Ocular implant and delivery system

Description

TECHNICAL FIELD

The present disclosure pertains generally, but not by way of limitation, to medical devices, and methods for manufacturing medical devices. The present invention relates generally to devices that are implanted within the eye. More particularly, the present invention relates to devices that facilitate the transfer of fluid from within one area of the eye to another area of the eye. Additionally, the present disclosure relates to systems, devices and methods for delivering ocular implants into the eye.

BACKGROUND

According to a draft report by The National Eye Institute (NEI) at The United States National Institutes of Health (NIH), glaucoma is now the leading cause of irreversible blindness worldwide and the second leading cause of blindness, behind cataract, in the world. Thus, the NEI draft report concludes, “it is critical that significant emphasis and resources continue to be devoted to determining the pathophysiology and management of this disease.” Glaucoma researchers have found a strong correlation between high intraocular pressure and glaucoma. For this reason, eye care professionals routinely screen patients for glaucoma by measuring intraocular pressure using a device known as a tonometer. Many tonometers make this measurement by blowing a sudden puff of air against the outer surface of the eye.

The eye can be conceptualized as a ball filled with fluid. There are two types of fluid inside the eye. The cavity behind the lens is filled with a viscous fluid known as vitreous humor. The cavity in front of the lens is filled with a fluid known as aqueous humor. Whenever a person views an object, he or she is viewing that object through both the vitreous humor and the aqueous humor.

Whenever a person views an object, he or she is also viewing that object through the cornea and the lens of the eye. In order to be transparent, the cornea and the lens can include no blood vessels. Accordingly, no blood flows through the cornea and the lens to provide nutrition to these tissues and to remove wastes from these tissues. Instead, these functions are performed by the aqueous humor. A continuous flow of aqueous humor through the eye provides nutrition to portions of the eye (e.g., the cornea and the lens) that have no blood vessels. This flow of aqueous humor also removes waste from these tissues.

Aqueous humor is produced by an organ known as the ciliary body. The ciliary body includes epithelial cells that continuously secrete aqueous humor. In a healthy eye, aqueous humor flows out of the anterior chamber of the eye through the trabecular meshwork and into Schlemm's canal as new aqueous humor is secreted by the epithelial cells of the ciliary body. The exited aqueous humor enters the episcleral venous system from Schlemm's canal and is carried along with the venous blood leaving the eye.

When the natural drainage mechanisms of the eye stop functioning properly, the pressure inside the eye begins to rise. Researchers have theorized prolonged exposure to high intraocular pressure causes damage to the optic nerve that transmits sensory information from the eye to the brain. This damage to the optic nerve typically results in loss of peripheral vision initially. As glaucoma progresses, more and more of the visual field is lost until the patient is completely blind.

In addition to drug treatments, a variety of surgical treatments for glaucoma have been performed. For example, shunts were implanted to direct aqueous humor from the anterior chamber to the extraocular vein (Lee and Scheppens, “Aqueous-venous shunt and intraocular pressure,” Investigative Opthalmology (February 1966)). Other early glaucoma treatment implants led from the anterior chamber to a sub-conjunctival bleb (e.g., U.S. Pat. Nos. 4,968,296 and 5,180,362). Still others were shunts leading from the anterior chamber to a point just inside Schlemm's canal (Spiegel et al., “Schlemm's canal implant: a new method to lower intraocular pressure in patients with POAG?” Ophthalmic Surgery and Lasers (June 1999); U.S. Pat. Nos. 6,450,984; 6,450,984).

SUMMARY

The invention provides design, material, and manufacturing method alternatives for medical devices.

In a first illustrative example, an ocular implant adapted to reside at least partially in a portion of Schlemm's canal of an eye may comprise a tubular body having an inner surface and an outer surface, the tubular body extending in a curved volume whose longitudinal axis forms an arc of a circle. A plurality of open areas and strut areas may be formed in the tubular body, the strut areas surrounding the plurality of open areas. A polymer rod may be disposed within the curved volume of the tubular body; at least one therapeutic agent may be disposed within an interstitial space of the polymer rod. The tubular body may have a diameter of between 0.005 inches and 0.04 inches.

In another illustrative example, an ocular implant adapted to reside at least partially in a portion of Schlemm's canal of an eye may comprise an elongated polymeric body extending in a curved volume whose longitudinal axis forms an arc of a circle. At least one therapeutic agent may be disposed within an interstitial space of the polymeric body. The polymeric body may have a diameter of between 0.005 inches and 0.04 inches.

In another illustrative example, a system may comprise a cannula defining a passageway extending from a proximal end to a distal end. The cannula may have a distal opening extending through a side wall and the distal end of the cannula to form a trough, a curved distal portion, a curved intermediate portion, and a proximal portion. The system may further comprise an ocular implant including a polymeric element containing a therapeutic agent disposed within the passageway of the cannula. The system may further comprise a delivery tool having a distal interlocking portion engaging a complementary interlocking portion of the ocular implant.

The above summary of some examples and embodiments is not intended to describe each disclosed embodiment or every implementation of the present disclosure. The Brief Description of the Drawings, and Detailed Description, which follow, more particularly exemplify these embodiments, but are also intended as exemplary and not limiting.

BRIEF DESCRIPTION OF THE DRAWINGS

The disclosure may be more completely understood in consideration of the following detailed description of various embodiments in connection with the accompanying drawings, in which:

FIG. 1 is a stylized perspective view depicting a portion of a human eye and a portion of an ocular implant disposed in Schlemm's canal.

FIG. 2A is an enlarged perspective view showing a portion of the implant of FIG. 1.

FIG. 2B is another enlarged perspective view showing a portion of the implant of FIG. 1 including a coating.

FIG. 3 is a perspective view showing a volume defined by the body of the ocular implant of FIGS. 1 and 2.

FIG. 4 is a perspective view showing a first plane intersecting the body of an ocular implant.

FIG. 5 is a perspective view showing a bending moment being applied to an ocular implant.

FIG. 6A is an enlarged perspective view of a portion of the ocular implant including a pressure sensor.

FIG. 6B is a cross-sectional view of the illustrative pressure sensor of FIG. 6A, taken at line B-B.

FIG. 6C is an enlarged perspective view of another portion of the ocular implant including a pressure sensor.

FIG. 7 is stylized view of an electronic device receiving data from an implanted ocular implant.

FIG. 8 is a side view of another illustrative ocular implant;

FIG. 9A is an enlarged cross-sectional view of the ocular implant of FIG. 8 taken along section line A-A of FIG. 8.

FIG. 9B is an enlarged cross-sectional view of the ocular implant of FIG. 8 taken along section line B-B of FIG. 8.

FIG. 10 is a side view of another illustrative ocular implant;

FIG. 11 is an enlarged cross-sectional view of the ocular implant of FIG. 10 taken along section line A-A of FIG. 10.

FIG. 12 is a side view of another illustrative ocular implant;

FIG. 13 is an enlarged cross-sectional view of the ocular implant of FIG. 12 taken along section line A-A of FIG. 12.

FIG. 14 is a side view of another illustrative ocular implant;

FIG. 15 is an enlarged cross-sectional view of the ocular implant of FIG. 14 taken along section line A-A of FIG. 14.

FIG. 16 is an illustrative plug for use with any of the illustrative ocular implants.

FIG. 17 is a stylized representation of a medical procedure in accordance with this DETAILED DESCRIPTION.

FIG. 18 is an enlarged perspective view further illustrating the delivery system and the eye shown in FIG. 17.

FIG. 19A is a perspective view showing a delivery system including an ocular implant and a cannula defining a passageway that is dimensioned to slidingly receive the ocular implant.

FIG. 19B is an enlarged detail view further illustrating the ocular implant and the cannula 108 shown in FIG. 19A.

FIG. 20 is a perspective view of a cannula in accordance with the detailed description.

FIG. 21 is a perspective view of an assembly including the cannula shown in FIG. 20 and an ocular implant that is resting in a passageway defined by the cannula.

FIG. 22 is a stylized perspective view including the assembly shown in FIG. 21.

FIG. 23 is an enlarged perspective view showing a portion of the cannula shown in the assembly of FIG. 22.

FIG. 24 is an additional perspective view showing the ocular implant and the cannula shown in the previous FIG. 23.

FIG. 25 is an additional perspective view showing the ocular implant and the cannula shown in FIG. 24.

FIG. 26 is an additional perspective view showing the ocular implant and the cannula shown in FIGS. 24 and 25.

FIG. 27 is a perspective view of Schlemm's canal after the cannula shown in FIG. 24 has been withdrawn leaving an inlet portion of the ocular implant in the anterior chamber of the eye and the remainder of ocular implant in Schlemm's canal.

FIG. 28A is a perspective view showing another illustrative delivery system including an ocular implant and a cannula defining a passageway that is dimensioned to slidingly receive the ocular implant.

FIG. 28B is an enlarged detail view further illustrating the ocular implant and the cannula shown in FIG. 28A.

FIG. 29 is an enlarged perspective view further illustrating the delivery system shown in FIG. 28 and an eye.

FIG. 30 is a perspective view further illustrating delivery system shown in FIG. 28.

FIG. 31 is a side view further illustrating the cannula shown in FIG. 38.

FIG. 31A is an additional side view illustrating the cannula shown in FIG. 28.

FIG. 32 is an enlarged detail view further illustrating the cannula shown in FIG. 28.

FIG. 33 is an enlarged perspective view further illustrating the distal portion of the cannula shown in FIG. 28.

While the disclosure is amenable to various modifications and alternative forms, specifics thereof have been shown by way of example in the drawings and will be described in detail. It should be understood, however, that the intention is not to limit the invention to the particular embodiments described. On the contrary, the intention is to cover all modifications, equivalents, and alternatives falling within the spirit and scope of the disclosure.

DETAILED DESCRIPTION

The following description should be read with reference to the drawings, which are not necessarily to scale, wherein like reference numerals indicate like elements throughout the several views. The detailed description and drawings are intended to illustrate but not limit the claimed invention. Those skilled in the art will recognize that the various elements described and/or shown may be arranged in various combinations and configurations without departing from the scope of the disclosure. The detailed description and drawings illustrate example embodiments of the claimed invention.

Definitions of certain terms are provided below and shall be applied, unless a different definition is given in the claims or elsewhere in this specification.

All numeric values are herein assumed to be modified by the term “about,” whether or not explicitly indicated. The term “about” generally refers to a range of numbers that one of skill in the art would consider equivalent to the recited value (i.e., having the same or substantially the same function or result). In many instances, the terms “about” may include numbers that are rounded to the nearest significant figure. Other uses of the term “about” (i.e., in a context other than numeric values) may be assumed to have their ordinary and customary definition(s), as understood from and consistent with the context of the specification, unless otherwise specified.

The recitation of numerical ranges by endpoints includes all numbers within that range (e.g., 1 to 5 includes 1, 1.5, 2, 2.75, 3, 3.80, 4, and 5).

As used in this specification and the appended claims, the singular forms “a,” “an,” and “the” include or otherwise refer to singular as well as plural referents, unless the content clearly dictates otherwise. As used in this specification and the appended claims, the term “or” is generally employed to include “and/or,” unless the content clearly dictates otherwise.

It is noted that references in the specification to “an embodiment”, “some embodiments”, “other embodiments”, etc., indicate that the embodiment(s) described may include a particular feature, structure, or characteristic, but every embodiment may not necessarily include the particular feature, structure, or characteristic. Moreover, such phrases are not necessarily referring to the same embodiment. Further, when a particular feature, structure, or characteristic is described in connection with an embodiment, it would be within the knowledge of one skilled in the art to affect such feature, structure, or characteristic in connection with other embodiments, whether or not explicitly described, unless clearly stated to the contrary. That is, the various individual elements described below, even if not explicitly shown in a particular combination, are nevertheless contemplated as being combinable or able to be arranged with each other to form other additional embodiments or to complement and/or enrich the described embodiment(s), as would be understood by one of ordinary skill in the art.

The following detailed description should be read with reference to the drawings, in which similar elements in different drawings are identified with the same reference numbers. The drawings, which are not necessarily to scale, depict illustrative embodiments and are not intended to limit the scope of the disclosure.

FIG. 1 is a stylized perspective view depicting a portion of a human eye 20. Eye 20 can be conceptualized as a fluid filled ball having two chambers. Sclera 22 of eye 20 surrounds a posterior chamber 24 filled with a viscous fluid known as vitreous humor. Cornea 26 of eye 20 encloses an anterior chamber 30 that is filled with a fluid know as aqueous humor. The cornea 26 meets the sclera 22 at a limbus 28 of eye 20. A lens 32 of eye 20 is located between anterior chamber 30 and posterior chamber 24. Lens 32 is held in place by a number of ciliary zonules 34. Whenever a person views an object, he or she is viewing that object through the cornea, the aqueous humor, and the lens of the eye. In order to be transparent, the cornea and the lens can include no blood vessels. Accordingly, no blood flows through the cornea and the lens to provide nutrition to these tissues and to remove wastes from these tissues. Instead, these functions are performed by the aqueous humor. A continuous flow of aqueous humor through the eye provides nutrition to portions of the eye (e.g., the cornea and the lens) that have no blood vessels. This flow of aqueous humor also removes waste from these tissues.

Aqueous humor is produced by an organ known as the ciliary body. The ciliary body includes epithelial cells that continuously secrete aqueous humor. In a healthy eye, a stream of aqueous humor flows out of the eye as new aqueous humor is secreted by the epithelial cells of the ciliary body. This excess aqueous humor eventually enters the blood stream and is carried away by venous blood leaving the eye.

In a healthy eye, aqueous humor flows out of the anterior chamber 30 through the trabecular meshwork 36 and into Schlemm's canal 38, located at the outer edge of the iris 42. Aqueous humor exits Schlemm's canal 38 by flowing through a number of outlets 40. After leaving Schlemm's canal 38, aqueous humor is absorbed into the venous blood stream.

In FIG. 1, an ocular implant 100 is disposed in Schlemm's canal 38 of eye 20. Ocular implant 100 has a body 102 including a plurality of tissue supporting frames 104 and a plurality of spines 106. Body 102 also includes a first edge 120 and a second edge 122 that define a first opening 124. First opening 124 is formed as a slot and fluidly communicates with an elongate channel 126 defined by an inner surface 128 of body 102. With reference to FIG. 1, it will be appreciated that first opening 124 is disposed on an outer side 130 of body 102. Accordingly, channel 126 opens in a radially outward direction 132 via first opening 124.

Ocular implant 100 may be inserted into Schlemm's canal of a human eye to facilitate the flow of aqueous humor out of the anterior chamber. This flow may include axial flow along Schlemm's canal, flow from the anterior chamber into Schlemm's canal, and flow leaving Schlemm's canal via outlets communicating with Schlemm's canal. When in place within the eye, ocular implant 100 will support trabecular mesh tissue and Schlemm's canal tissue and will provide for improved communication between the anterior chamber and Schlemm's canal (via the trabecular meshwork) and between pockets or compartments along Schlemm's canal. As shown in FIG. 1, the implant is preferably oriented so that the first opening 124 is disposed radially outwardly within Schlemm's canal.

FIG. 2A is an enlarged perspective view showing a portion of ocular implant 100 shown in the previous figure. Ocular implant 100 has a body 102 that extends along a generally curved longitudinal axis 134. Body 102 has a plurality of tissue supporting frames 104 and a plurality of spines 106. As shown in FIG. 2A, these spines 106 and frames 104 are arranged in a repeating AB pattern in which each A is a tissue supporting frame and each B is a spine. In the embodiment of FIG. 2A, one spine extends between each adjacent pair of frames 104

The frames 104 of body 102 include a first frame 136 of ocular implant 100 that is disposed between a first spine 140 and a second spine 142. In the embodiment of FIG. 2A, first frame 136 is formed as a first strut 144 that extends between first spine 140 and second spine 142. First frame 136 also includes a second strut 146 extending between first spine 140 and second spine 142. In the exemplary embodiment of FIG. 2A, each strut undulates in a circumferential direction as it extends longitudinally between first spine 140 and second spine 142.

In the embodiment of FIG. 2A, body 102 has a longitudinal radius 150 and a lateral radius 148. Body 102 of ocular implant 100 includes a first edge 120 and a second edge 122 that define a first opening 124. First opening 124 fluidly communicates with an elongate channel 126 defined by an inner surface 128 of body 102. A second opening is defined by a second edge 122A of a first strut 144 and a second edge 122B of a second strut 146. First opening 124, second opening 138 and additional openings defined by ocular implant 100 allow aqueous humor to flow laterally across and/or laterally through ocular implant 100. The outer surfaces 127 of body 102 defines a volume 152.

In some instances, the ocular implant 100 may further include a coating 129 disposed on the inner surfaces 128 and/or outer surfaces 127 of the implant 100, as shown in FIG. 2B. While the coating 129 is illustrated on both the outer and inner surfaces 127, 128, the coating 129 may be on only one of the outer surface 127 or the inner surface 128. Further, while the coating 129 is illustrated as extending over the entirety of the outer surface and the inner surface 127, 128, in some embodiments, the coating 129 may cover only a portion of the outer and/or inner surfaces 127, 128. For example, the coating 129 may cover 10% or more, 25% or more, 50% or more, or 75% or more of the surface area of the ocular implant 100. These are just examples. In some instances, the coating 129 may cover less than 10% or more than 75% of the surface area of the implant 100, as desired.

The coating 129 may be formed of, or otherwise include, a therapeutic agent. In some embodiments, the coating 129 may release the therapeutic agent. The coating 129 may release the therapeutic agent controllably over a period of time. In some embodiments, the therapeutic agent may be applied directly to the ocular implant 100 while in other embodiments, the ocular implant may be dispersed within a matrix material. For example, the therapeutic agent may be dispersed within a biocompatible or biodegradable polymeric material. The concentration of therapeutic agent within the matrix material may vary depending on the desired treatment.

The biocompatible polymeric material used to form the bioactive agent-polymer composite layer(s) may include any polymeric material capable of forming a solidified composite layer in the presence of the bioactive material. The polymeric material of the present invention may be hydrophilic or hydrophobic, and is, for example, polycarboxylic acids, cellulosic polymers, including cellulose acetate and cellulose nitrate, gelatin, polyvinylpyrrolidone, cross-linked polyvinylpyrrolidone, polyanhydrides including maleic anhydride polymers, polyamides, polyvinyl alcohols, polyolefins, copolymers of vinyl monomers such as EVA, polyvinyl ethers, polyvinyl aromatics, polyethylene oxides, glycosaminoglycans, polysaccharides, polyesters including polyethylene terephthalate, polyacrylamides, polyethers, polyether sulfone, polycarbonate, polyalkylenes including polypropylene, polyethylene and high molecular weight polyethylene, halogenated polyalkylenes including polytetrafluoroethylene, polyurethanes, polyorthoesters, proteins, polypeptides, silicones, siloxane polymers, polylactic acid (PLA), polyglycolic acid (PLGA), polycaprolactone, polyhydroxybutyrate valerate and blends and copolymers thereof as well as other biodegradable, bioabsorbable and biostable polymers and copolymers. Coatings from polymer dispersions such as polyurethane dispersions (BAYHDROL®, etc.) and acrylic latex dispersions are also within the scope of the present invention. The polymer may be a protein polymer, fibrin, collagen and derivatives thereof, polysaccharides such as celluloses, starches, dextrans, alginates and derivatives of these polysaccharides, an extracellular matrix component, hyaluronic acid, or another biologic agent or a suitable mixture of any of these, for example. The coating 129 can include of a single polymer or copolymer. The coating 129 may also include copolymers or physical blends of any of the materials indicated above.

The therapeutic agents utilized with the ocular implant, may include one or more drugs provided below, either alone or in combination. The drugs utilized may also be the equivalent of, derivatives of, or analogs of one or more of the drugs provided below. The drugs may include but are not limited to pharmaceutical agents including anti-glaucoma medications, ocular agents, antimicrobial agents (e.g., antibiotic, antiviral, antiparasitic, antifungal agents), anti-inflammatory agents (including steroids or non-steroidal anti-inflammatory), biological agents including hormones, enzymes or enzyme-related components, antibodies or antibody-related components, oligonucleotides (including DNA, RNA, shortinterfering RNA, antisense oligonucleotides, and the like), DNA/RNA vectors, viruses (either wild type or genetically modified) or viral vectors, peptides, proteins, enzymes, extracellular matrix components, and live cells configured to produce one or more biological components. The use of any particular drug is not limited to its primary effect or regulatory body-approved treatment indication or manner of use. Drugs also include compounds or other materials that reduce or treat one or more side effects of another drug or therapeutic agent. As many drugs have more than a single mode of action, the listing of any particular drug within any one therapeutic class below is only representative of one possible use of the drug and is not intended to limit the scope of its use with the ophthalmic implant system.

The therapeutic agents may be combined with any number of excipients as is known in the art. In addition to the biodegradable polymeric excipients discussed above, other excipients may be used, including, but not limited to, benzyl alcohol, ethylcellulose, methylcellulose, hydroxymethylcellulose, cetyl alcohol, croscarmellose sodium, dextrans, dextrose, fructose, gelatin, glycerin, mono glycerides, diglycerides, kaolin, calcium chloride, lactose, lactose monohydrate, maltodextrins, polysorbates, pregelatinized starch, calcium stearate, magnesium stearate, silicon dioxide, cornstarch, talc, and the like. The one or more excipients may be included in total amounts as low as about 1%, 5%, or 10% and in other embodiments may be included in total amounts as high as 50%, 70% or 90%.

Examples of drugs may include various anti-secretory agents; antimitotics and other antiproliferative agents, including among others, anti-angiogenesis agents such as angiostatin, anecortave acetate, thrombospondin, VEGF receptor tyrosine kinase inhibitors and anti-vascular endothelial growth factor (anti-VEGF) drugs such as ranibizumab (LUCENTIS®) and bevacizumab (AVASTIN®), pegaptanib (MACUGEN®) sunitinib and sorafenib and any of a variety of known small-molecule and transcription inhibitors having anti-angiogenesis effect: classes of known ophthalmic drugs, including: glaucoma agents, such as adrenergic antagonists, including for example, beta-blocker agents such as atenolol propranolol, metipranolol, betaxolol, betaxolol hydrochloride carteolol, levobetaxolol, levobunolol, levobunolol hydrochloride, timolol, timolol hemihydrate, and timolol maleate; adrenergic agonists or sympathomimetic agents such as epinephrine, dipivefrin, clonidine, apraclonidine, and brimonidine; parasympathomimetics or cholinergic agonists such as pilocarpine, carbachol, phospholene iodine, and physostigmine, salicylate, acetylcholine chloride, eserine, diisopropyl fluorophosphate, demecarium bromide); muscarinics; carbonic anhydrase inhibitor agents, including topical and/or systemic agents, for example acetozolamide, brinzolamide, dorzolamide and methazolamide, ethoxzolamide, diamox, and dichlorphenamide; mydriatic-cycloplegic agents such as atropine, cyclopentolate, succinylcholine, homatropine, phenylephrine, scopolamine and tropicamide; prostaglandins such as prostaglandin F2 alpha, antiprostaglandins, prostaglandin precursors, or prostaglandin analog agents such as bimatoprost, latanoprost, travoprost, tafluprost and unoprostone; docosanoid compounds such as unoprostone.

Other examples of drugs may also include anti-inflammatory agents including for example glucocorticoids and corticosteroids such as betamethasone, cortisone, dexamethasone, dexamethasone 21-phosphate, methylprednisolone, prednisolone 21-phosphate, prednisolone acetate, prednisolone, fluorometholone, loteprednol, medrysone, fluocinolone acetonide, triamcinolone acetonide, triamcinolone, triamcinolone acetonide, beclomethasone, budesonide, flunisolide, fluorometholone, fluticasone, hydrocortisone, hydrocortisone acetate, loteprednol, rimexolone and non-steroidal anti-inflammatory agents including, for example, diclofenac, flurbiprofen, ibuprofen, bromfenac, nepafenac, and ketorolac, salicylate, indomethacin, ibuprofen, naxopren, piroxicam, nabumetone, and aldehyde traps; anti-infective or antimicrobial agents such as antibiotics including, for example, tetracycline, chlortetracycline, bacitracin, neomycin, polymyxin, gramicidin, cephalexin, oxytetracycline, chloramphenicol, rifampicin, ciprofloxacin, tobramycin, gentamycin, erythromycin, penicillin, sulfonamides, sulfadiazine, sulfacetamide, sulfamethizole, sulfisoxazole, nitrofurazone, sodium propionate, aminoglycosides such as gentamicin and tobramycin; fluoroquinolones such as ciprofloxacin, gatifloxacin, levofloxacin, moxifloxacin, norfloxacin, ofloxacin; bacitracin, erythromycin, fusidic acid, neomycin, polymyxin B, gramicidin, trimethoprim and sulfacetamide; antifungals such as amphotericin B and miconazole; antivirals such as idoxuridine trifluorothymidine, acyclovir, gancyclovir, interferon; antimycotics; immune-modulating agents such as antiallergenics, including, for example, sodium chromoglycate, antazoline, methapyriline, chlorpheniramine, cetirizine, pyrilamine, prophenpyridamine anti-histamine agents such as azelastine, emedastine and levocabastine; immunological drugs (such as vaccines and immune stimulants); MAST cell stabilizer agents such as cromolyn sodium, ketotifen, lodoxamide, nedocromil, olopatadine and pemirolastciliary body ablative agents, such as gentamicin and cidofovir; and other ophthalmic agents such as verteporfin, proparacaine, tetracaine, cyclosporine and pilocarpine; inhibitors of cell-surface glycoprotein receptors; decongestants such as phenylephrine, naphazoline, tetrahydrozoline; lipids or hypotensive lipids; dopaminergic agonists and/or antagonists such as quinpirole, fenoldopam, and ibopamine; vasospasm inhibitors; vasodilators; antihypertensive agents; angiotensin converting enzyme (ACE) inhibitors; angiotensin-! receptor antagonists such as olmesartan; microtubule inhibitors; molecular motor (dynein and/or kinesin) inhibitors; actin cytoskeleton regulatory agents such as cyctchalasin, latrunculin, swinholide A, ethacrynic acid, H-7, and Rho-kinase (ROCK) inhibitors; remodeling inhibitors; modulators of the extracellular matrix such as tert-butylhydro-quinolone and AL-3037A; adenosine receptor agonists and/or antagonists such as dicyanopyridines, N-6-cylclophexyladenosine and (R)-phenylisopropyladenosine; serotonin agonists; hormonal agents such as estrogens, estradiol, progestational hormones, progesterone, insulin, calcitonin, parathyroid hormone, peptide and vasopressin hypothalamus releasing factor; growth factor antagonists or growth factors, including, for example, epidermal growth factor, fibroblast growth factor, platelet derived growth factor, transforming growth factor beta, somatotropin, fibronectin, connective tissue growth factor, bone morphogenic proteins (BMPs); cytokines such as interleukins, CD44, cochlin, and serum amyloids, such as serum amyloid A.

Other therapeutic agents may include neuroprotective agents such as lubezole, nimodipine and related compounds, and including blood flow enhancers, sodium channels blockers, glutamate inhibitors such as memantine, neurotrophic factors, nitric oxide synthase inhibitors; free radical scavengers or anti-oxidants; chelating compounds; apoptosis-related protease inhibitors; compounds that reduce new protein synthesis; radiotherapeutic agents; photodynamic therapy agents; gene therapy agents; genetic modulators; and dry eye medications such as cyclosporine A, demulcents, and sodium hyaluronate. Other therapeutic agents that may be used include: other beta-blocker agents such as acebutolol, atenolol, bisoprolol, carvedilol, asmolol, labetalol, nadolol, penbutolol, and pindolol; other corticosteroidal and non-steroidal anti-inflammatory agents such aspirin, betamethasone, cortisone, diflunisal, etodolac, fenoprofen, fludrocortisone, flurbiprofen, hydrocortisone, ibuprofen, indomethacine, ketoprofen, meclofenamate, mefenamic acid, meloxicam, methylprednisolone, nabumetone, naproxen, oxaprozin, prednisolone, prioxicam, salsalate, sulindac and tolmetin; COX-2 inhibitors like celecoxib, rofecoxib and Valdecoxib; other immune-modulating agents such as aldesleukin, adalimumab (HUMIRA®), azathioprine, basiliximab, daclizumab, etanercept (ENBREL®), hydroxychloroquine, infliximab (REMICADE®), leflunomide, methotrexate, mycophenolate mofetil, and sulfasalazine; other anti-histamine agents such as loratadine, desloratadine, cetirizine, diphenhydramine, chlorpheniramine, dexchlorpheniramine, clemastine, cyproheptadine, fexofenadine, hydroxyzine and promethazine; other anti-infective agents such as aminoglycosides such as amikacin and streptomycin; anti-fungal agents such as amphotericin B, caspofungin, clotrimazole, fluconazole, itraconazole, ketoconazole, voriconazole, terbinafine and nystatin; anti-malarial agents such as chloroquine, atovaquone, mefloquine, primaquine, quinidine and quinine; anti-mycobacterium agents such as ethambutol, isoniazid, pyrazinamide, rifampin and rifabutin; anti-parasitic agents such as albendazole, mebendazole, thiabendazole, metronidazole, pyrantel, atovaquone, iodoquinol, ivermectin, paromycin, praziquantel, and trimetrexate; other anti-viral agents, including anti-CMV or anti-herpetic agents such as acyclovir, cidofovir, famciclovir, ganciclovir, valacyclovir, valganciclovir, vidarabine, trifluridine and foscamet; protease inhibitors such as ritonavir, saquinavir, lopinavir, indinavir, atazanavir, amprenavir and nelfinavir; nucleotide/nucleoside/nonnucleoside reverse transcriptase inhibitors such as abacavir, ddl, 3TC, d4T, ddC, tenofovir and emtricitabine, delavirdine, efavirenz and nevirapine; other anti-viral agents such as interferons, ribavirin and trifluridine; other anti-bacterial agents, including carbapenems like ertapenem, imipenem and meropenem; cephalosporins such as cefadroxil, cefazolin, cefdinir, cefditoren, cephalexin, cefaclor, cefepime, cefoperazone, cefotaxime, cefotetan, cefoxitin, cefpodoxime, cefprozil, ceftazidime, ceftibuten, ceftizoxime, ceftriaxone, cefuroxime and loracarbef; other macro !ides and ketolides such as azithromycin, clarithromycin, dirithromycin and telithromycin; peniciiiis (with and without clavulanate) including amoxiciiiin, ampicillin, pivampicillin, dicloxacillin, nafcillin, oxacillin, piperacillin, and ticarcillin; tetracyclines such as doxycycline, minocycline and tetracycline; other anti-bacterials such as aztreonam, chloramphenicol, clindamycin, linezolid, nitrofurantoin and vancomycin; alpha blocker agents such as doxazosin, prazosin and terazosin; calcium-channel blockers such as amlodipine, bepridil, diltiazem, felodipine, isradipine, nicardipine, nifedipine, nisoldipine and verapamil; other anti-hypertensive agents such as clonidine, diazoxide, fenoldopan, hydralazine, minoxidil, nitroprusside, phenoxybenzamine, epoprostenol, tolazoline, treprostinil and nitrate-based agents; anti-coagulant agents, including heparins and heparinoids such as heparin, dalteparin, enoxaparin, tinzaparin and fondaparinux; other anti-coagulant agents such as hirudin, aprotinin, argatroban, bivalirudin, desirudin, lepirudin, warfarin and ximelagatran; anti-platelet agents such as abciximab, clopidogrel, dipyridamole, optifibatide, ticlopidine and tirofiban; prostaglandin PDE-5 inhibitors and other prostaglandin agents such as alprostadil, carboprost, sildenafil, tadalafil and vardenafil; thrombin inhibitors; antithrombogenic agents; anti-platelet aggregating agents; thrombolytic agents and/or fibrinolytic agents such as alteplase, anistreplase, reteplase, streptokinase, tenecteplase and urokinase; anti-proliferative agents such as sirolimus, tacrolimus, everolimus, zotarolimus, paclitaxel and mycophenolic acid; hormonal-related agents including levothyroxine, fluoxymestrone, methyltestosterone, nandrolone, oxandrolone, testosterone, estradiol, estrone, estropipate, clomiphene, gonadotropins, hydroxyprogesterone, levonorgestrel, medroxyprogesterone, megestrol, mifepristone, norethindrone, oxytocin, progesterone, raloxifene and tamoxifen; anti-neoplastic agents, including alkylating agents such as carmustine lomustine, melphalan, cisplatin, fluorouracil3, and procarbazine antibiotic-like agents such as bleomycin, daunorubicin, doxorubicin, idarubicin, mitomycin and plicamycin; anti proliferative agents (such as 1,3-cis retinoic acid, 5-fluorouracil, taxol, rapamycin, mitomycin C and cisplatin); antimetabolite agents such as cytarabine, fludarabine, hydroxyurea, mercaptopurine and 5-flurouracil (5-FU); immune modulating agents such as aldesleukin, imatinib, rituximab and tositumomab; mitotic inhibitors docetaxel, etoposide, vinblastine and vincristine; radioactive agents such as strontium-89; and other anti-neoplastic agents such as irinotecan, topotecan and mitotane.

FIG. 3 is an additional perspective view showing volume 152 defined by the body of the ocular implant shown in the previous figure. With reference to FIG. 3, it will be appreciated that volume 152 extends along a generally curved longitudinal axis 134. Volume 152 has a longitudinal radius 150, a lateral radius 148, and a generally circular lateral cross section 153.

FIG. 4 is a perspective view showing a first plane 154 and a second plane 155 that both intersect ocular implant 100. In FIG. 4, first plane 154 is delineated with hatch marks. With reference to FIG. 4, it will be appreciated that spines 106 of body 102 are generally aligned with one another and that first plane 154 intersects all spines 106 shown in FIG. 4. In the embodiment of FIG. 4, body 102 of ocular implant 100 is generally symmetric about first plane 154.

In the embodiment of FIG. 4, the flexibility of body 102 is at a maximum when body 102 is bending along first plane 154, and body 102 has less flexibility when bending along a plane other than first plane 154 (e.g., a plane that intersects first plane 154). For example, in the embodiment shown in FIG. 4, body 102 has a second flexibility when bending along second plane 155 that is less than the first flexibility that body 102 has when bending along first plane 154.

Stated another way, in the embodiment of FIG. 4, the bending modulus of body 102 is at a minimum when body 102 is bent along first plane 154. Body 102 has a first bending modulus when bent along first plane 154 and a greater bending modulus when bent along a plane other than first plane 154 (e.g., a plane that intersects first plane 154). For example, in the embodiment shown in FIG. 4, body 102 has a second bending modulus when bent along second plane 155 that is greater than the first bending modulus that body 102 has when bent along first plane 154.

FIG. 5 is an enlarged perspective view showing a portion of ocular implant 100 shown in the previous figure. In the exemplary embodiment of FIG. 5, a bending moment M is being applied to body 102 of ocular implant 100. Bending moment M acts about a first axis 156 that is generally orthogonal to first plane 154. A second axis 158 and a third axis 160 are also shown in FIG. 5. Second axis 158 is generally perpendicular to first axis 156. Third axis 160 is skewed relative to first axis 156.

An inner surface 128 of body 102 defines a channel 126. Body 102 of ocular implant 100 includes a first edge 120 and a second edge 123 that define a first opening 124. Channel 126 of ocular implant 100 fluidly communicates with first opening 124. A second opening 138 is defined by a second edge 122A of a first strut 144 and a second edge 122B of a second strut 146. First opening 124, second opening 138 and additional openings defined by ocular implant 100 allow aqueous humor to flow laterally across and/or laterally through ocular implant 100.

As shown in FIG. 5, ocular implant 100 has a first spine 140 and a second spine 142. First strut 144 and a second strut 146 form a first frame 136 of ocular implant 100 that extends between first spine 140 and second spine 142. In the exemplary embodiment of FIG. 5, each strut undulates in a circumferential direction as it extends longitudinally between first spine 140 and second spine 142.

In the embodiment of FIG. 5, the flexibility of body 102 is at a maximum when body 102 is bent by a moment acting about first axis 156, and body 102 has less flexibility when bent by a moment acting about an axis other than first axis 156 (e.g., second axis 158 and third axis 160). Stated another way, the bending modulus of body 102 is at a minimum when body 102 is bent by a moment acting about first axis 156, and body 102 has a greater bending modulus when bent by a moment acting about an axis other than first axis 156 (e.g., second axis 158 and third axis 160). Some illustrative ocular implants having a similar structure are described in commonly assigned U.S. Provisional Application 62/267,794, titled “OCULAR IMPLANT AND DELIVERY SYSTEM” which is hereby incorporated by reference.

FIG. 6A is an enlarged perspective view showing a portion of ocular implant 100 shown in the FIGS. 2 and 4. The ocular implant 100 may further include an intraocular pressure sensor 180 mounted to the inner surface 128 of the ocular implant 100 adjacent to an outlet of the implant 100, as shown in Detail A. While the pressure sensor 180 is illustrated as mounted to an inner surface 128 of the ocular implant 100 it is contemplated that the pressure sensor 180 may be mounted within one of the openings 124, 138 or on an outer surface of the ocular implant 100, as desired. The pressure sensor 180 may continuously measure the intraocular pressure of a patient, once the ocular implant 100 has been implanted.

The pressure sensor 180 may be a Micro-Electro-Mechanical System (MEMS) pressure sensor. While the pressure sensor 180 has been described as a MEMS pressure sensor, it is contemplated that other pressure sensors may be used in place of, or in addition to, a MEMS pressure sensor. In some instances, the pressure sensor 180 may have a width in the range of approximately 0.02 millimeters (20 micrometers) to approximately 1.0 millimeters. However, it is contemplated that the pressure sensors 180 are smaller than 20 micrometers, or larger than 1.0 millimeter. In some instances, the pressure sensor 180 may have a width dimension in the nanometer range. Further, while only a single pressure sensor 180 has been illustrated, the ocular implant 100 may include more than one pressure sensor 180, as desired. For example, a first pressure sensor may be placed at a first end of the ocular implant 100 and a second pressure sensor may be placed at a second end of the ocular implant. In some instances, the is pressure sensor 180 may be provided in the channel 128 adjacent to the proximal end 101 of the implant 100, as shown in FIG. 6C. It is contemplated that the pressure sensor 180 may include a protective cover to prevent the delivery device (not explicitly shown) from damaging the sensor 180 during delivery of the ocular implant 100, although this is not required.

MEMS pressure sensors are often formed by anisotropically etching a recess into a back side of a silicon substrate die, leaving a thin flexible diaphragm 182. In operation, at least one surface of the diaphragm 182 is exposed to an input pressure (e.g. the ocular pressure). The diaphragm 182 deflects according to the magnitude of the input pressure, which may be detected by one or more electrical components or sense elements 186 (e.g. piezoresistors) positioned on or embedded within the diaphragm 182. The change in resistance of the piezoresistors 186 is reflected as a change in an output voltage signal from a resistive bridge formed at least in part by the piezoresistors. In some cases, the diaphragm may be made thinner with the addition of support bosses, which may help increase the sensitivity of the diaphragm over a flat plate diaphragm. Circuit elements may be connected so that sensor elements 186 to provide some level of signal processing before providing an output signal to bond pads 188 of the pressure sensor 180. The signal processing may filter, amplify, linearize, calibrate and/or otherwise process the raw sensor signal produced by the sensor elements (e.g. piezoresistors 186). While the sense elements 186 have been described as piezoresistors, it is contemplated that the sense elements may be selected to provide a capacitive pressure sensor 180.

The pressure sensor 180 may include a first substrate 185 and a second substrate 183, as shown in FIG. 6B, which is a cross-section of the illustrative pressure sensor 180 taken at line B-B in FIG. 6A. In some instances, the first substrate 185 may be a layered silicon-insulator-silicon substrate or wafer formed with silicon on insulator (SOI) technology, although this is not required. It is contemplated that other substrates may be used, as desired. The first substrate 185 may include a first silicon layer. An insulating, or oxide, layer 187 may be disposed on the first silicon layer 185. In some instances, the insulating layer 187 may be formed from silicon dioxide, silicon nitride, sapphire, and/or any other suitable insulating material. While not explicitly shown, the pressure sensor 180 may include a second silicon layer disposed on the insulating layer. In some instances, the second silicon layer may be thinned or removed such that the oxide layer 187 is exposed at the side facing away from the second substrate 183. Alternatively, and in some cases, the second silicon layer and oxide layer 187 are not provided from the start.

The second substrate 183 may be any semi-conductor wafer (e.g. silicon or germanium) or other substrate as desired. It is contemplated that either or both the first substrate 185 or the second substrate 183 may be doped with an impurity to provide an n-type or p-type extrinsic semiconductor. For example, the first substrate 185 may be an n-type substrate while the second substrate 183 may be a p-type substrate. The reverse configuration is also contemplated, or both substrates may be doped the same polarity. In some instances, the first substrate 185 and/or the second substrate 183 may include an epitaxial layer.

A portion of the first substrate 185, such as a portion of the first silicon layer, may be removed, leaving a thin, flexible diaphragm 182 over a cavity or recess 181. In some cases, piezoresistors 186 may be located in or on the diaphragm 182 to measure deflection/stress of the diaphragm 182 to form a pressure sensor. During operation, at least one surface of the diaphragm 182 may be exposed to an input pressure. The diaphragm 182 may then deflect according to a magnitude of the pressure on the diaphragm 182. A deflection of the diaphragm 182 then creates changes in resistance in the piezoresistors 186. A change in resistance of the piezoresistors 186 may be reflected as a change in an output voltage signal of a resistive bridge that is formed at least partially by the piezoresistors 186. The output voltage provides a measure of the input pressure exerted on the diaphragm 182.

It is contemplated that the second substrate 183 may be flexible to allow the substrate 183 to be mounted flush against the inner surface 128 of the ocular implant 100. Alternatively, or additionally, the second substrate 183 may have a curved outer surface (facing away from the diaphragm 182) shaped to generally correspond to the curved inner surface 128 of the ocular implant 100. It is further contemplated that the materials forming the pressure sensor 180 may be selected such that the pressure sensor 180 is biocompatible.

As noted above, while the pressure sensor 180 has been described as a MEMS pressure sensor, it is contemplated that pressure sensor 180 may take other suitable forms. In one alternative example, the pressure sensor may be formed in such a way that radio waves can be used to detect changes in pressure without sensor elements incorporated into the device. Such a pressure sensor may include a flexible base substrate, a bottom inductive coil positioned on the base substrate, a layer of pressure sensitive rubber pyramids positioned over the bottom inductive coil, a top inductive coil positioned on top of the rubber pyramids, and a top substrate positioned over the top inductive coil. As a pressure is exerted on the sensor, the inductive coils move close together. Radio waves (from an applied source) reflected by the inductive coils have a lower resonance frequency when the coils are positioned closer together. Thus, the frequency of the radio waves can indicate the distance between the coils which is then correlated to the pressure exerted on the device.

The pressure sensor 180 may be further provided with an antenna or inductor 184 to allow the data from the pressure sensor 180 to be wirelessly communicated to a readout device. In some instances, the pressure sensor 180 may use radiofrequency communication protocols, such as, but not limited to cellular communication, ZigBee®, Bluetooth®, WiFi®, IrDA, dedicated short range communication (DSRC), EnOcean®, Z-Wave, or any other suitable wireless protocols, as desired to transmit the data from the pressure sensor 180 to another device located outside the body. The data may be transmitted to any number so suitably enabled devices, including, but not limited to, cellular phones, tablet or laptop computers, desktop computers, portable handheld devices, such a personal digital assistant (PDA), or a specially designed device, such as, but not limited to a medical device. This may allow a physician, patient, or other interested party to monitor the ocular pressure without the use of a tonometer. In some instances, the pressure data may be automatically transmitted to a physician from the remote device. For example, as shown in FIG. 7, once the ocular implant 100 with the pressure sensor 180 has been implanted, an enabled remote device 192 may be brought within communication range of the patient's 190 eye. This may allow the enabled device 192 to receive the ocular pressure data recorded at the pressure sensor 180. The enabled device 192 may be configured to automatically transmit the data to a physician, for example, to a second remote device.

In addition to, or in place of, an ocular implant, such as implant 100, configured and positioned to facilitate the flow of aqueous humor out of the anterior chamber, an ocular implant may be provided to deliver an intraocular pressure reducing drug (or any other therapeutic agent, including, but not limited to, those described herein with respect to coating 129). FIG. 8 is a perspective view of an illustrative implant 200 which may be used to deliver a therapeutic agent to the eye over a length of time. It is contemplated that the implant 200 may be configured to deliver the therapeutic agent at a controlled dosage or rate for a period of hours, days, weeks, or even years. In some instances, it is contemplated the therapeutic agent may be delivered for a period of one to twenty years, five to fifteen years, or about 10 years. In some instances, the implant 200 may be configured to deliver a therapeutic agent for less than a year, or more than twenty years, as desired. It is contemplated that the length of time the implant 200 is capable of delivering a therapeutic agent may depend on the size of the implant, the quantity of the therapeutic agent loaded into the stent, the delivery rate of the therapeutic agent, other biological factors dependent on the patient, and/or combinations thereof.

The implant 200 may include a body portion 202 similar in form and function to the body 102 and frame 104 described above with respect to ocular implant 100. The body portion 202 may include a frame 206 having a plurality of splines 204 and a plurality of struts 208 extending between the splines 204. The frame 206 may include a first opening 210 (or plurality of openings) configured to be positioned in a radially outward positioned (similar to opening 124 described above). The frame 206 may include a second opening 212 (or plurality of openings) configured to be poisoned in a radially inward position (e.g., facing the anterior chamber 30). A longitudinally extending channel 220 extends from a proximal end 216 of the implant 200 to a distal end 218 of the implant 200.

A polymer rod 214 loaded with a therapeutic agent 218 is positioned within the longitudinally extending channel 220. For example, the polymer rod 214 may be formed from a biocompatible polymer such as, but not limited to polysiloxanes (e.g., silicone), polyurethane, polylactic acid (PLA), polyvinyl alcohol, poly(lactic-co-glycolic) acid (PLGA), polyethylene, polyethylene oxide, polyethylene terephthalate, or polyester, or mixtures, combinations, blends or co-polymers thereof, or the like. In some cases, it may be desirable to use a cross-linked polymer system to avoid polymer creep, although this is not required. In some cases, all or a portion of the polymer rod 214 may be porous thereby allowing certain substances to permeate or diffuse through a side wall of the polymer rod 214 and into pores or interstitial spaces within the rod 214. The porosity (e.g., the percentage of interstitial volume to total volume) of the polymer rod 214 may be about 10% or more, about 20% or more, about 30% or more, about 40% or more, about 50% or more, about 60% or more, about 70% or more, or about 80% or more, for example.

The polymer rod 214 may be loaded with a therapeutic agent 218 (see, for example, FIGS. 9A and 9B). For instance, the interstitial spaces of the polymer rod 214 may be filled with one or more therapeutic agent 218. It is contemplated that the polymer rod 214 may be filled with a therapeutic agent 218 such that the rod 214 has a precise quantity of the therapeutic agent. Once implanted in a body, the therapeutic agent 218 may diffuse through the porous sidewall of the polymer rod 214 over a predetermined period of time dictated, at least in part, by the average pore size of the porous sidewall of the rod 214. Thus, the rate of release of the therapeutic agent 218 may be known and dictated, at least in part, by the porosity of the rod 214. For instance, the porosity of the rod 214 may be chosen to controllably release the therapeutic agent 218 over a period of minutes, hours, days, weeks, months, years, etc. In some embodiments, the duration of release of the therapeutic agent 218 from the rod 214 may be about 1 hour, about 2 hours, about 3 hours, about 4 hours, about 5 hours, about 6 hours, about 12 hours, about 1 day, about 2 days, about 3 days, about 4 days, about 5 days, about 6 days, about 1 week, about 2 weeks, about 3 weeks, about 1 month, about 2 months, about 3 months, about 4 months, about 5 months, about 6 months, about 1 year, about 2 years, about 5 years, about 10 years, or longer. Thus, the polymer rod 214 may be chosen for its porosity such that a desired rate of therapeutic agent release is provided.

In some instances, the therapeutic agent 218 and the monomer or polymer for forming the polymer rod 214 may be injected into the channel 220 as a liquid or slurry and solidified within the channel 220. It is contemplated that solidification of the polymer may include exposing the device 200 to a cross-link initiator, such as a UV light source, heat, reagents, etc. In other cases, the polymer rod 214 and therapeutic agent 218 may be formed outside of the channel 220 and is subsequently loaded into the channel 220.

FIG. 9A is a lateral cross-sectional view of ocular implant 200 taken along section line A-A shown in FIG. 8. Section line A-A intersects a pair of struts 208 of the frame 206 at the point where the circumferential undulation of these struts is at its maximum. The polymer rod 214 is positioned within the channel 220. A first opening 212 fluidly communicates with channel 126. FIG. 9B is a lateral cross-sectional view of ocular implant 200 taken along section line B-B shown in the FIG. 8. Section line B-B intersects a spine 204 of ocular implant 200. In some cases, the frame 206 and/or polymer rod 214 may be wrapped with a sleeve 216 to hold the rod 214 in place. The sleeve 216 may be a silicone sleeve, or other porous material, configured to control elution, although this is not required. It is contemplated that the sleeve 216 may have a pore size selected to control the release of the therapeutic agent 218. The sleeve 216 and/or frame 206 may be provided with additional openings or windows on the radially inwards surface to direct the therapeutic agent 218 towards the anterior chamber of the eye. In some cases, the sleeve 216, if so provided, or the outer surface of the frame 206 and rod 214 may be coated with heparin or a heparin related coating to prevent the adhesion of tissue or other debris on the surface of the device 200 which may inhibit drug elution.

The ocular implant 200 may be inserted into Schlemm's canal such that it is fixed and not free floating (as it may if placed in the anterior chamber). This may reduce the likelihood of the implant 200 damaging the cornea or other structures through movement. Further, the placement of the implant 200 in Schlemm's canal may place the therapeutic agent 218 in continuous contact with the aqueous humor that reaches the implant 200 by the trabecular meshwork.

FIG. 10 is a perspective view of another illustrative implant 300 which may be used to deliver a therapeutic agent to the eye over a length of time either in addition to or in place of an ocular implant, such as implant 100, configured and positioned to facilitate the flow of aqueous humor out of the anterior chamber. It is contemplated that the implant 300 may be configured to deliver the therapeutic agent at a controlled dosage or rate for a period of hours, days, weeks, or even years. In some instances, it is contemplated the therapeutic agent may be delivered for a period of one to twenty years, five to fifteen years, or about 10 years. In some instances, the implant 300 may be configured to deliver a therapeutic agent for less than a year, or more than twenty years, as desired. It is contemplated that the length of time the implant 300 is capable of delivering a therapeutic agent may depend on the size of the implant, the quantity of the therapeutic agent loaded into the stent, the delivery rate of the therapeutic agent, other biological factors dependent on the patient, and/or combinations thereof.

The implant 300 may include an elongated tubular body 302 extending from a proximal end 306 to a distal end 304. A lumen 308 extends from the proximal end 306 to the distal end 304. In some cases, the distal end 304 may be tapered or pointed to facilitate advancement through the eye, although this is not required. The proximal end 306 may include interlocking features 314 configured to engage mating features on a delivery device, similar to that described with respect to FIGS. 19A and 19B. The elongated tubular body 302 may be curved along its longitudinal axis in a similar manner to the implant 100 described above. The elongated tubular body 302 may a nitinol, stainless steel, or other material, as desired. The elongated tubular body 302 may include a plurality of micro pores extending from an inner surface to an outer surface of the tubular body 302 (e.g., from the lumen 308 top a point exterior to the tubular body 302) to allow a therapeutic agent to pass from the lumen 308 to a point exterior to the elongated tubular body 302. In some cases, the micro pores may be present on the radially inwards portions of the tubular member 302 to direct a therapeutic agent towards the anterior chamber of the eye. However, this is not required. The micro pores may be on a radially outward portion of the tubular body 302, the entire tubular body 302, a portion of a length of the tubular body 302, and/or a portion of the circumference the tubular body 302, as desired.

A polymer rod 310 loaded with a therapeutic agent 312 is positioned within the lumen 308, as shown in FIG. 11 which illustrates a lateral cross-sectional view of ocular implant 300 taken along section line A-A shown in FIG. 10. The polymer rod 310 may be formed from a biocompatible polymer such as, but not limited to polysiloxanes (e.g., silicone), polyurethane, polylactic acid (PLA), polyvinyl alcohol, poly(lactic-co-glycolic) acid (PLGA), polyethylene, polyethylene oxide, polyethylene terephthalate, or polyester, or mixtures, combinations, blends or co-polymers thereof, or the like. In some cases, it may be desirable to use a cross-linked polymer system to avoid polymer creep, although this is not required. In some cases, all or a portion of the polymer rod 310 may be porous thereby allowing certain substances to permeate or diffuse through a side wall of the polymer rod 310 and into pores or interstitial spaces within the rod 310. The porosity (e.g., the percentage of interstitial volume to total volume) of the polymer rod 310 may be about 10% or more, about 20% or more, about 30% or more, about 40% or more, about 50% or more, about 60% or more, about 70% or more, or about 80% or more, for example.

The polymer rod 310 may be loaded with a therapeutic agent 312. The therapeutic agent may be an intraocular pressure reducing drug (or any other therapeutic agent, including, but not limited to, those described herein with respect to coating 129). For instance, the interstitial spaces of the polymer rod 310 may be filled with one or more therapeutic agent 312. It is contemplated that the polymer rod 310 may be filled with a therapeutic agent 312 such that the rod 310 has a precise quantity of the therapeutic agent. Once implanted in a body, the therapeutic agent 312 may diffuse through the porous sidewall of the polymer rod 310 and the porous wall of the tubular body 302 over a predetermined period of time dictated, at least in part, by the average pore size of the porous sidewall of the rod 310 and/or the tubular body 302. Thus, the rate of release of the therapeutic agent 312 may be known and dictated, at least in part, by the porosity of the rod 310. For instance, the porosity of the rod 310 and/or tubular body 302 may be chosen to controllably release the therapeutic agent 312 over a period of minutes, hours, days, weeks, months, years, etc. In some embodiments, the duration of release of the therapeutic agent 312 from the rod 310 may be about 1 hour, about 2 hours, about 3 hours, about 4 hours, about 5 hours, about 6 hours, about 12 hours, about 1 day, about 2 days, about 3 days, about 4 days, about 5 days, about 6 days, about 1 week, about 2 weeks, about 3 weeks, about 1 month, about 2 months, about 3 months, about 4 months, about 5 months, about 6 months, about 1 year, about 2 years, about 5 years, about 10 years, or longer. Thus, the polymer rod 310 and/or tubular body 302 may be chosen for its porosity such that a desired rate of therapeutic agent release is provided.

In some instances, the therapeutic agent 312 and the monomer or polymer for forming the polymer rod 310 may be injected into the lumen 308 as a liquid or slurry and solidified within the lumen 308. It is contemplated that solidification of the polymer may include exposing the device 300 to a cross-link initiator, such as a UV light source, heat, reagents, etc. In other cases, the polymer rod 310 and therapeutic agent 312 may be formed outside of the lumen 308 and is subsequently loaded into the lumen 308.

In some cases, the elongated tubular body 302 may be coated with heparin or a heparin related coating to prevent the adhesion of tissue or other debris on the surface of the implant 300 which may inhibit drug elution. The ocular implant 300 may be inserted into Schlemm's canal such that it is fixed and not free floating (as it may if placed in the anterior chamber). This may reduce the likelihood of the implant 300 damaging the cornea or other structures through movement. Further, the placement of the implant 300 in Schlemm's canal may place the therapeutic agent 312 in continuous contact with the aqueous humor that reaches the implant 300 by the trabecular meshwork.

FIG. 12 is a perspective view of another illustrative implant 330 which may be used to deliver a therapeutic agent to the eye over a length of time either in addition to or in place of an ocular implant, such as implant 100, configured and positioned to facilitate the flow of aqueous humor out of the anterior chamber. It is contemplated that the implant 330 may be configured to deliver the therapeutic agent at a controlled dosage or rate for a period of hours, days, weeks, or even years. In some instances, it is contemplated the therapeutic agent may be delivered for a period of one to twenty years, five to fifteen years, or about 10 years. In some instances, the implant 330 may be configured to deliver a therapeutic agent for less than a year, or more than twenty years, as desired. It is contemplated that the length of time the implant 330 is capable of delivering a therapeutic agent may depend on the size of the implant, the quantity of the therapeutic agent loaded into the stent, the delivery rate of the therapeutic agent, other biological factors dependent on the patient, and/or combinations thereof.

The implant 330 may include an elongated body 332 extending from a proximal end 336 to a distal end 334. The proximal end 336 may include interlocking features 338 configured to engage mating features on a delivery device, similar to that described with respect to FIGS. 19A and 19B. The elongated body 332 may have a generally porous but otherwise substantially solid cross-section (see, for example, FIG. 13, which illustrates a lateral cross-sectional view of ocular implant 300 taken along section line A-A shown in FIG. 12). In other words, the elongated body 332 may lack the elongated lumen and/or channels of other implants described herein. The elongated body 332 may be curved along its longitudinal axis in a similar manner to the implant 100 described above. The elongated body 332 may be formed from a biocompatible polymer such as, but not limited to polysiloxanes (e.g., silicone), polyurethane, polylactic acid (PLA), polyvinyl alcohol, poly(lactic-co-glycolic) acid (PLGA), polyethylene, polyethylene oxide, polyethylene terephthalate, or polyester, or mixtures, combinations, blends or co-polymers thereof, or the like. In some embodiments, the polymer may be biodegradable. In some cases, it may be desirable to use a cross-linked polymer system to avoid polymer creep, although this is not required. In some cases, all or a portion of the elongated body 332 may be porous thereby allowing certain substances to permeate or diffuse through a side wall of the elongated body 332 and into pores or interstitial spaces within the elongated body 332. The porosity (e.g., the percentage of interstitial volume to total volume) of the elongated body 332 may be about 10% or more, about 20% or more, about 30% or more, about 40% or more, about 50% or more, about 60% or more, about 70% or more, or about 80% or more, for example.

The elongated body 332 may be loaded with a therapeutic agent 340. The therapeutic agent may be an intraocular pressure reducing drug (or any other therapeutic agent, including, but not limited to, those described herein with respect to coating 129). For instance, the interstitial spaces of the elongated body 332 may be filled with one or more therapeutic agent 340. It is contemplated that the elongated body 332 may be filled with a therapeutic agent 340 such that the elongated body 332 has a precise quantity of the therapeutic agent. Once implanted in a body, the therapeutic agent 340 may diffuse through the porous sidewall of the elongated body 332 and the porous wall of the tubular body 332 over a predetermined period of time dictated, at least in part, by the average pore size of the porous sidewall of the elongated body 332 and/or the tubular body 332. Thus, the rate of release of the therapeutic agent 340 may be known and dictated, at least in part, by the porosity of the elongated body 332. For instance, the porosity of the elongated body 332 and/or tubular body 332 may be chosen to controllably release the therapeutic agent 340 over a period of minutes, hours, days, weeks, months, years, etc. In some embodiments, the duration of release of the therapeutic agent 340 from the elongated body 332 may be about 1 hour, about 2 hours, about 3 hours, about 4 hours, about 5 hours, about 6 hours, about 12 hours, about 1 day, about 2 days, about 3 days, about 4 days, about 5 days, about 6 days, about 1 week, about 2 weeks, about 3 weeks, about 1 month, about 2 months, about 3 months, about 4 months, about 5 months, about 6 months, about 1 year, about 2 years, about 5 years, about 10 years, or longer. Thus, the elongated body 332 and/or tubular body 332 may be chosen for its porosity such that a desired rate of therapeutic agent release is provided.

In some cases, the elongated tubular body 332 may be coated with heparin or a heparin related coating to prevent the adhesion of tissue or other debris on the surface of the implant 330 which may inhibit drug elution. The ocular implant 330 may be inserted into Schlemm's canal such that it is fixed and not free floating (as it may if placed in the anterior chamber). This may reduce the likelihood of the implant 330 damaging the cornea or other structures through movement. Further, the placement of the implant 400 in Schlemm's canal may place the therapeutic agent 340 in continuous contact with the aqueous humor that reaches the implant 330 by the trabecular meshwork.

FIG. 14 is a perspective view of another illustrative implant 350, which may be used to deliver a therapeutic agent to the eye over a length of time either in addition to or in place of an ocular implant, such as implant 100, configured and positioned to facilitate the flow of aqueous humor out of the anterior chamber. It is contemplated that the implant 350 may be configured to deliver the therapeutic agent at a controlled dosage or rate for a period of hours, days, weeks, or even years. In some instances, it is contemplated the therapeutic agent may be delivered for a period of one to twenty years, five to fifteen years, or about 10 years. In some instances, the implant 350 may be configured to deliver a therapeutic agent for less than a year, or more than twenty years, as desired. It is contemplated that the length of time the implant 350 is capable of delivering a therapeutic agent may depend on the size of the implant, the quantity of the therapeutic agent loaded into the stent, the delivery rate of the therapeutic agent, other biological factors dependent on the patient, and/or combinations thereof.

The implant 300 may include an elongated tubular body 352 extending from a proximal end 356 to a distal end 354. A lumen 358 extends from the proximal end 356 to the distal end 354. In some cases, the distal end 354 may be tapered or pointed to facilitate advancement through the eye, although this is not required. The proximal end 356 may include interlocking features 360 configured to engage mating features on a delivery device, similar to that described with respect to FIGS. 19A and 19B. The elongated tubular body 352 may be curved along its longitudinal axis in a similar manner to the implant 100 described above. The elongated tubular body 352 may a nitinol, stainless steel, or other material, as desired.

A therapeutic agent 362 may be loaded within the lumen 358, as shown in FIG. 15 which illustrates a lateral cross-sectional view of ocular implant 300 taken along section line A-A shown in FIG. 14. The therapeutic agent 362 may be an intraocular pressure reducing drug (or any other therapeutic agent, including, but not limited to, those described herein with respect to coating 129). For instance, the lumen 358 of the implant 350 may be filled with one or more therapeutic agents 362. It is contemplated that the lumen 358 may be filled with a therapeutic agent 362 such that the implant 350 has a precise quantity of the therapeutic agent 362.

The lumen 358 may be blocked or plugged adjacent the distal and/or proximal ends 354, 356 using a removable plug, cap, or stopper such as the plug 364 illustrated in FIG. 16. In some cases, the plug 364 may have a tapered configuration. In other embodiments, the plug 364 may have a uniform diameter from a first end to a second end thereof. It is contemplated that the plug 364 may form a friction fit within the lumen 358 to substantially block the flow of therapeutic agent from the lumen 358 of the implant 350. The plug 364 may formed, at least in part, from a polymer configured to limit or control diffusion of the therapeutic agent 362. For example, the plug 364 may be formed from a biocompatible polymer such as, but not limited to polysiloxanes (e.g., silicone), polyurethane, polylactic acid (PLA), polyvinyl alcohol, poly(lactic-co-glycolic) acid (PLGA), polyethylene, polyethylene oxide, polyethylene terephthalate, or polyester, or mixtures, combinations, blends or co-polymers thereof, or the like. In some embodiments, the polymer may be biodegradable. In some cases, it may be desirable to use a cross-linked polymer system to avoid polymer creep, although this is not required. In some cases, all or a portion of the plug 364 may be porous thereby allowing certain substances to permeate or diffuse through the plug 364. The porosity (e.g., the percentage of interstitial volume to total volume) of the plug 364 may be about 10% or more, about 20% or more, about 30% or more, about 40% or more, about 50% or more, about 60% or more, about 70% or more, or about 80% or more, for example. In some cases, the polymer may be injected into a metal cap or frame. In other cases, the plug 356 may be formed entirely from the polymeric material. It is contemplated that in some cases, the body 352 of the implant 302 may also be porous, as described herein, to further control diffusion of the therapeutic agent 362.

Once implanted in a body, the therapeutic agent 362 may diffuse through the porous plug 364 over a predetermined period of time dictated, at least in part, by the average pore size of the plug 364. Thus, the rate of release of the therapeutic agent 362 may be known and dictated, at least in part, by the porosity of the plug 364. For instance, the porosity of the plug 364 may be chosen to controllably release the therapeutic agent 362 over a period of minutes, hours, days, weeks, months, years, etc. In some embodiments, the duration of release of the therapeutic agent 362 from the implant 350 may be about 1 hour, about 2 hours, about 3 hours, about 4 hours, about 5 hours, about 6 hours, about 12 hours, about 1 day, about 2 days, about 3 days, about 4 days, about 5 days, about 6 days, about 1 week, about 2 weeks, about 3 weeks, about 1 month, about 2 months, about 3 months, about 4 months, about 5 months, about 6 months, about 1 year, about 2 years, about 5 years, about 10 years, or longer. Thus, the polymer rod 310 and/or tubular body 352 may be chosen for its porosity such that a desired rate of therapeutic agent release is provided.

In some cases, the elongated tubular body 352 may be coated with heparin or a heparin related coating to prevent the adhesion of tissue or other debris on the surface of the implant 300 which may inhibit drug elution. The ocular implant 350 may be inserted into Schlemm's canal such that it is fixed and not free floating (as it may if placed in the anterior chamber). This may reduce the likelihood of the implant 350 damaging the cornea or other structures through movement. Further, the placement of the implant 350 in Schlemm's canal may place the therapeutic agent 362 in continuous contact with the aqueous humor that reaches the implant 350 by the trabecular meshwork.

FIG. 17 is a stylized representation of a medical procedure in accordance with this detailed description. In the procedure of FIG. 17, a physician is treating an eye 400 of a patient P. In the procedure of FIG. 17, the physician is holding a hand piece of a delivery system 450 in his or her right hand RH. The physician's left hand (not shown) may be used to hold the handle H of a gonio lens 402. Alternatively, some physicians may prefer holding the delivery system hand piece in the left hand and the gonio lens handle H in the right hand RH. Further details of ocular implant delivery systems may be found in U.S. application Ser. No. 11/943,289, filed Nov. 20, 2007, now U.S. Pat. No. 8,512,404, the disclosure of which is incorporated herein by reference.

During the procedure illustrated in FIG. 17, the physician may view the interior of the anterior chamber using gonio lens 402 and a microscope 404. Detail A of FIG. 17 is a stylized simulation of the image viewed by the physician. A distal portion of a cannula 452 is visible in Detail A. A shadow-like line indicates the location of Schlemm's canal SC which is lying under various tissues (e.g., the trabecular meshwork) that surround the anterior chamber. A distal opening 454 of cannula 452 is positioned near Schlemm's canal SC of eye 400.

Methods in accordance with this detailed description may include the step of advancing the distal end of cannula 452 through the cornea of eye 400 so that a distal portion of cannula 452 is disposed in the anterior chamber of the eye. Cannula 452 may then be used to access Schlemm's canal of the eye, for example, by piercing the wall of Schlemm's canal with the distal end of cannula 452. Distal opening 454 of cannula 452 may be placed in fluid communication with a lumen defined by Schlemm's canal. The ocular implant may be advanced out of distal opening 454 and into Schlemm's canal. Insertion of the ocular implant into Schlemm's canal may facilitate the flow of aqueous humor out of the anterior chamber of the eye.

FIG. 18 is an enlarged perspective view further illustrating delivery system 450 and eye 400 shown in the previous figure. In FIG. 18, cannula 452 of delivery system 450 is shown extending through a cornea 426 of eye 400. A distal portion of cannula 452 is disposed inside the anterior chamber defined by cornea 426 of eye 400. In the embodiment of FIG. 18, cannula 452 is configured so that a distal opening 454 of cannula 452 can be placed in fluid communication with Schlemm's canal.

In the embodiment of FIG. 18, an ocular implant is disposed in a passageway defined by cannula 452. Delivery system 450 includes a mechanism that is capable of advancing and retracting the ocular implant along the length of cannula 452. The ocular implant may be placed in Schlemm's canal of eye 400 by advancing the ocular implant through the distal opening of cannula 452 while the distal opening is in fluid communication with Schlemm's canal.

FIG. 19A is a perspective view showing a delivery system 500 including an ocular implant 550 and a cannula 508 defining a passageway that is dimensioned to slidingly receive ocular implant 550. Delivery system 500 may be used to advance ocular implant 550 into a target location in the eye of a patient. Examples of target locations that may be suitable in some applications include areas in and around Schlemm's canal, the trabecular meshwork, the suprachoroidal space, and the anterior chamber of the eye. FIG. 19B is an enlarged detail view further illustrating ocular implant 550 and cannula 508 of delivery system 500.

Delivery system 500 of FIG. 19A is capable of controlling the advancement and retraction of ocular implant 550 within cannula 508. Ocular implant 550 may be placed in a target location (e.g., Schlemm's canal) by advancing the ocular implant through a distal opening 532 of cannula 508 while the distal opening is in fluid communication with Schlemm's canal. In the embodiment of FIG. 19A, ocular implant 550 has been advanced through distal opening 532 of cannula 508 for purposes of illustration.

Delivery system 500 of FIG. 19A includes a housing 502, a sleeve 504, and an end cap 510. A tracking wheel 506 extends through a wall of housing 502 in FIG. 19A. Tracking wheel 506 is part of a mechanism that is capable of advancing and retracting a delivery tool 552 of delivery system 500. The delivery tool 552 extends through a distal opening of cannula 508 of FIG. 19B. Rotating the tracking wheel will cause delivery tool 552 to move in an axial direction along a passageway defined by cannula 508. The axial direction may be in a distal direction D or a proximal direction P. The delivery tool 552 and the mechanism for moving the delivery tool 552 are described in commonly assigned application Ser. No. 62/024,295, which is herein incorporated by reference.

In the embodiment of FIG. 19A, housing 502 is configured to be gripped with one hand while providing control over the axial advancement and retraction of ocular implant via tracking wheel 506. The housing of delivery system 500 results in an advantageous ergonomic relationship of the fingers relative to the hand. This design provides a configuration that will allow a user, such as a physician, to stabilize the device using part of the hand, while leaving the middle or index finger free move independently from the remainder of the hand. The middle or index finger is free to move independently to rotate the wheel for advancing and/or retract the ocular implant.

FIG. 19B is an enlarged detail view further illustrating ocular implant 550 and a cannula 508 of delivery system 500. Cannula 508 comprises a generally tubular member 598 having proximal portion 540, a distal end 534, and a distal portion 544 extending between distal end 534 and proximal portion 540. In the embodiment of FIG. 19, distal portion 544 is curved. In some useful embodiments, distal portion 544 is dimensioned and configured to be received in the anterior chamber of the eye.

FIG. 19B shows delivery tool 552 of delivery system 500 extending through distal opening 532 of cannula 508. Delivery tool 552 includes an interlocking portion 560 that is configured to form a connection with a complementary interlocking portion 562 of ocular implant 550, as explained in more detail below. In the embodiment of FIG. 19, rotating the tracking wheel will cause delivery tool 552 and ocular implant 550 to move along a path defined by cannula 508. Cannula 508 is sized and configured so that the distal end of cannula 508 can be advanced through the trabecular meshwork of the eye and into Schlemm's canal. Positioning cannula 508 in this way places distal opening 532 in fluid communication with Schlemm's canal. Ocular implant 550 may be placed in Schlemm's canal by advancing the ocular implant through distal opening 532 of cannula 508 while the distal opening is in fluid communication with Schlemm's canal. The distal portion of the cannula may include a cutting portion configured to cut through the trabecular meshwork and the wall of Schlemm's canal, such as by providing distal end 534 with a sharp edge adapted to cut through such tissue.

FIG. 20 is a perspective view of a cannula 508 in accordance with the present detailed description. Cannula 508 of FIG. 20 comprises a generally tubular member 598 having a central axis 596. Generally tubular member 598 of FIG. 20 comprises a proximal portion 540, a distal end 534, and a distal portion 544 extending between distal end 534 and proximal portion 540. A distal opening surface 542 surrounds a distal opening 532 extending through the distal end 534 and through a side wall of cannula 508. A beveled edge 565 is disposed at the distal end of distal opening surface 542, extending from the distal end 534 to a proximal extent 567 of beveled edge 565. Tubular member 598 defines distal opening 532, a proximal opening 536, and a passageway 538 extending between proximal opening 536 and distal opening 532.

In the embodiment of FIG. 20, proximal portion 540 of cannula 508 is substantially straight, distal portion 544 of cannula 508 is curved, and central axis 596 defines a curvature plane 548. Curvature plane 548 may be referred to as a plane of curvature. Curvature plane 548 divides cannula 508 into a first portion PA and a second portion PB. In the embodiment of FIG. 20, second portion PB is substantially a mirror image of first portion PA. In FIG. 20, distal portion 544 is shown extending between distal end 534 and proximal portion 540 with no intervening elements. In the embodiment of FIG. 20, distal portion 544 is curved along its entire length.

A method in accordance with this detailed description may include the step of advancing the distal end 534 of cannula 508 through the cornea of a human eye so that distal end 534 is disposed in the anterior chamber of the eye. Cannula 508 may then be used to access Schlemm's canal of the eye, for example, by piercing the wall of Schlemm's canal with the distal end 534 of cannula 508. The beveled edge 565 may be inserted into Schlemm's canal to place at least part of distal opening 532 of cannula 508 in communication with Schlemm's canal, as discussed in more detail below. The ocular implant may be advanced out of a distal port of the cannula and into Schlemm's canal.

In the embodiment of FIG. 20, distal portion 544 of cannula 508 defines a trough 554. In some useful embodiments, trough 554 is configured to receive the entire external cross section of an ocular implant as the ocular implant is being advanced into Schlemm's canal. When this is the case, trough 554 may have a depth dimension that is deeper than a width of the ocular implant. This cannula configuration advantageously prevents the ocular implant from intersecting the layers of the trabecular meshwork as the ocular implant is advanced into Schlemm's canal. Trough 554 may also be configured to allow the proximal portion of the ocular implant to be released from the delivery tool, as discussed below.

The cannula 508 may further include a pressure sensor 580 disposed within the trough 554. The pressure sensor 580 may be similar in form and function to pressure sensor 180 described above. While the pressure sensor 580 is illustrated as mounted within the trough 554 of the cannula, it is contemplated that the pressure sensor 580 may be mounted at other locations within or on the cannula 508. The pressure sensor 580 may provide an instantaneous pressure reading during implantation of the ocular implant 550 or shortly thereafter. In some instances, the pressure reading obtained from the pressure sensor 580 on the cannula 508 can be compared to a pressure reading obtained from a pressure sensor mounted on the ocular implant 550, if so provided.

The pressure sensor 580 may be a Micro-Electro-Mechanical System (MEMS) pressure sensor. While the pressure sensor 580 has been described as a MEMS pressure sensor, it is contemplated that other pressure sensors may be used in place of, or in addition to, a MEMS pressure sensor. Further, while only a single pressure sensor 580 has been illustrated, the cannula 508 may include more than one pressure sensor 580, as desired. MEMS pressure sensors are often formed by anisotropically etching a recess into a back side of a silicon substrate die, leaving a thin flexible diaphragm. In operation, at least one surface of the diaphragm is exposed to an input pressure (e.g. the ocular pressure). The diaphragm deflects according to the magnitude of the input pressure, which may be detected by one or more electrical components or sense elements (e.g. piezoresistors) positioned on or embedded within the diaphragm. The change in resistance of the piezoresistors is reflected as a change in an output voltage signal from a resistive bridge formed at least in part by the piezoresistors. In some cases, the diaphragm may be made thinner with the addition of support bosses, which may help increase the sensitivity of the diaphragm over a flat plate diaphragm. Circuit elements may be connected so that sensor elements to provide some level of signal processing before providing an output signal to bond pads of the pressure sensor. The signal processing may filter, amplify, linearize, calibrate and/or otherwise process the raw sensor signal produced by the sensor elements (e.g. piezoresistors). While the sense elements have been described as piezoresistors, it is contemplated that the sense elements may be selected to provide a capacitive pressure sensor 580.

The pressure sensor 580 may be further provided with an antenna or inductor to allow the data from the pressure sensor 580 to be wirelessly communicated to a readout device. In some instances, the pressure sensor 580 may use radiofrequency communication protocols, such as, but not limited to cellular communication, ZigBee®, Bluetooth®, WiFi®, IrDA, dedicated short range communication (DSRC), EnOcean®, or any other suitable wireless protocols, as desired to transmit the data from the pressure sensor 580 to another device located outside the body. The data may be transmitted to any number so suitably enabled devices, including, but not limited to, cellular phones, tablet computers, computers, portable handheld devices, such a personal digital assistant (PDA), or a specially designed device. This may allow a physician, patient, or other interested party to monitor the ocular pressure without the use of a tonometer.

FIG. 21 is a perspective view of an assembly including cannula 508 shown in the previous figure. For purposes of illustration, cannula 508 is cross-sectionally illustrated in FIG. 26. In FIG. 21, an ocular implant 550 can be seen resting in a passageway 538 defined by cannula 508. With reference to FIG. 21, it will be appreciated that distal portion 544 of cannula 508 is curved so that central axis 596 of cannula 508 defines a curvature plane 548. With reference to FIG. 26, it will be appreciated that curvature plane 548 divides cannula 508 into a first portion and a second portion PB. Only second portion PB of cannula 508 is shown in the illustrative embodiment of FIG. 21.

FIG. 22 is a stylized perspective view including the assembly shown in the previous figure. In the embodiment of FIG. 22, a distal portion of cannula 508 is shown extending through the wall of Schlemm's canal SC. The distal tip of cannula 508 may include a sharp portion configured for cutting and/or piercing the trabecular meshwork and the wall of Schlemm's canal so that the passageway defined by the cannula can be placed in fluid communication with the lumen defined by Schlemm's canal. With the passageway of the cannula placed in fluid communication with the lumen of Schlemm's canal, ocular implant 550 can be advanced out of the distal opening of the cannula and into Schlemm's canal. In FIG. 22, a distal portion of ocular implant 550 can be seen through distal opening 532 of cannula 508.

For purposes of illustration, a hypothetical window W is cut through the wall of cannula 508 in FIG. 22. An interlocking portion 560 of a delivery tool 552 and a complementary interlocking portion 562 of ocular implant 550 are visible through window W. In the embodiment of FIG. 22, interlocking portion 560 of delivery tool 552 and complementary interlocking portion 562 of ocular implant 550 are engaging each other so that a proximal end 549 of ocular implant 550 is proximal to the distal end 551 of delivery tool 552. Surface 561 of delivery tool 552 rests against the wall of cannula 508 to prevent interlocking portion 560 of delivery tool 552 and complementary interlocking portion 562 of ocular implant 550 from disengaging one another. When they are connected in this fashion, delivery tool 552 and ocular implant 550 move together as the delivery tool is advanced and retracted relative to cannula 508 by the delivery system mechanism.

FIG. 23 is an enlarged perspective view showing a portion of cannula 508 shown in the previous figure. In some useful embodiments, cannula 508 is curved to achieve substantially tangential entry into Schlemm's canal SC. In the embodiment of FIG. 23, cannula 508 is contacting an outer major wall of Schlemm's canal SC at a point of tangency PT. Also in the embodiment of FIG. 23, a curved distal portion of cannula 508 is dimensioned to be disposed within the anterior chamber of the eye.

As shown in FIG. 23, the distal tip 534 and beveled edge of the cannula 508 have been inserted into Schlemm's canal up to the proximal extent 567 of beveled edge 565. In this position, ocular implant 550 can be seen extending into trough 554. In some useful embodiments, the ocular implant has a radius of curvature that is larger than the radius of curvature of the cannula. This arrangement ensures that the ocular implant will track along trough 554 as the ocular implant is urged in a distal direction by delivery system 500.

FIG. 24 is an additional perspective view showing ocular implant 550 and cannula 508 shown in the previous figure. By comparing FIG. 24 with the previous figure, it will be appreciated that ocular implant 550 has been advanced in a distal direction D while cannula 508 has remained stationary so that a distal portion of ocular implant 550 is disposed inside Schlemm's canal SC. Trough 554 opens into an elongate opening 532 defined by edge 542 at the distal portion of cannula 508. In the embodiment of FIG. 24, the elongate opening defined by the cannula provides direct visualization of the ocular implant as it is advanced into Schlemm's canal. A configuration allowing direct visualization of the ocular implant has a number of clinical advantages. During a medical procedure, it is often difficult to monitor the progress of the implant by viewing the implant through the trabecular meshwork. For example, blood reflux may push blood into Schlemm's canal obstructing a physician's view the portion of the implant that has entered Schlemm's canal. With reference to FIG. 24, ocular implant 550 tracks along trough 554 as it is advanced distally along cannula 508. The trough opening allows the physician to monitor the progress of the implant by viewing the implant structures as they advance through the trough prior to entering Schlemm's canal. The trough opening also allows the physician to identify the position of the proximal end of the ocular implant with respect to the incision made by the cannula to access Schlemm's canal.

FIG. 25 is an additional stylized perspective view showing ocular implant 550 and cannula 508. In the embodiment of FIG. 25, the interlocking portions 560 and 562 of the delivery tool 552 and ocular implant 550, respectively, can be seen entering the distal opening 532 defined by cannula 508. As shown, ocular implant 550 has been advanced in a distal direction D (relative to the embodiment shown in the previous figure) so that more of ocular implant 550 is disposed inside Schlemm's canal SC. Surface 561 opposite interlocking portion 560 of delivery tool 552 still rests against the inner wall of cannula 508 to keep the delivery tool interlocked with ocular implant 550.

FIG. 26 is an additional stylized perspective view showing ocular implant 550 and cannula 508. As shown in FIG. 26, the ocular implant 550 and delivery tool 552 have advanced further distally so that delivery tool surface 561 and part of the reduced diameter portion 563 have now passed into opening 532, thereby permitting the delivery tool curved portion 553 to move toward its curved at-rest shape so that the delivery tool engagement surface 560 disengages and moves away from its complementary engagement surface 562 on the ocular implant 550.

In some useful embodiments, the delivery tool may be colored to provide visual differentiation from the implant. After the disengaging from the ocular implant, cannula 508 and delivery tool 552 can be withdrawn from Schlemm's canal SC leaving the ocular implant 550 in the fully deployed position shown in FIG. 26. After delivery of ocular implant 550 is complete, the delivery tool and the cannula may be removed from the eye, leaving at least a distal portion of the ocular implant in Schlemm's canal.

FIG. 27 is a perspective view of Schlemm's canal SC after the cannula (seen in the previous figure) has been withdrawn leaving an inlet portion of ocular implant 550 in the anterior chamber of the eye and the remainder of ocular implant 550 in Schlemm's canal. The presence of ocular implant 550 in Schlemm's canal may facilitate the flow of aqueous humor out of the anterior chamber. This flow may include axial flow along Schlemm's canal, flow from the anterior chamber into Schlemm's canal, and flow leaving Schlemm's canal via outlets communicating with Schlemm's canal. When in place within the eye, ocular implant 550 will support the trabecular meshwork and Schlemm's canal tissue and will provide for improved communication between the anterior chamber and Schlemm's canal (via the trabecular meshwork) and between pockets or compartments along Schlemm's canal.

In some instances, it may be desirable to deliver an ocular implant to Schlemm's canal in conjunction with another corrective surgery, such as, but not limited to, cataract surgery. When the ocular implant is placed during another surgical procedure, it may be desirable to insert the ocular implant through the same incision used for the other procedure. FIG. 28A is a perspective view showing another illustrative delivery system 600 that may be used to advance ocular implant 650 into a target location in the eye of a patient through an incision location created for another procedure, such as, but not limited to cataract surgery. The delivery system 600 may include an ocular implant 650 and a cannula 608 defining a passageway that is dimensioned to slidingly receive ocular implant 650. It is contemplated that aspects of delivery system 600 may be similar in form and function to delivery system 500. Examples of target locations that may be suitable in some applications include areas in and around Schlemm's canal, the trabecular meshwork, the suprachoroidal space, and the anterior chamber of the eye. FIG. 28B is an enlarged detail view further illustrating ocular implant 650 and cannula 608 of delivery system 600.

Delivery system 600 of FIG. 28A is capable of controlling the advancement and retraction of ocular implant 650 within cannula 608. Ocular implant 650 may be placed in a target location (e.g., Schlemm's canal) by advancing the ocular implant 650 through a distal opening 632 of cannula 608 while the distal opening is in fluid communication with Schlemm's canal. In the embodiment of FIG. 28A, ocular implant 650 has been advanced through distal opening 632 of cannula 608 for purposes of illustration.

Delivery system 600 of FIG. 28A includes a housing 602, a sleeve 604, and an end cap 610. A tracking wheel 606 extends through a wall of housing 602 in FIG. 28A. Tracking wheel 606 is part of a mechanism that is capable of advancing and retracting a delivery tool 652 of delivery system 600. The delivery tool 652 is slidably disposed within cannula 608 and configured to extend through a distal opening of cannula 608. Rotating the tracking wheel will cause delivery tool 652 to move in an axial direction along a passageway defined by cannula 608. The axial direction may be in a distal direction D or a proximal direction P. Delivery tool 652 may be similar in form and function to delivery tool 152.

In the embodiment of FIG. 28A, housing 602 is configured to be gripped with one hand while providing control over the axial advancement and retraction of ocular implant via tracking wheel 606. The features of housing 602 result in an advantageous ergonomic relationship of the fingers relative to the hand. This design provides a configuration that will allow a user, such as a physician, to stabilize the device using part of the hand, while leaving the middle or index finger free move independently from the remainder of the hand. The middle or index finger is free to move independently to rotate the wheel for advancing and/or retract the ocular implant.

FIG. 28B is an enlarged detail view further illustrating ocular implant 650 and a cannula 608 of delivery system 600. Cannula 608 comprises a generally tubular member 698 having proximal portion 640, an intermediate portion 645, a distal portion 644, and a distal end 634. The intermediate portion 645 may extend distally from a first point 643 distal to the proximal end 641 to a second point 647 proximal to the distal end 634. The distal portion 644 may extend between distally from the second point 647 to distal end 634 of cannula 608 (shown in FIG. 31). In the embodiment of FIG. 28, both distal portion 644 and intermediate portion 645 may be curved. In some instances, distal portion 644 may have a smaller radius of curvature, and thus a higher curvature, than the intermediate portion 645, although this is not required. In some useful embodiments, distal portion 644 and intermediate portion 645 may be dimensioned and configured to be received in the anterior chamber of the eye.

In some instances, it may be desirable to place the ocular implant 650 during another ocular procedure, such as, but not limited to cataract surgery. It is contemplated that the optimal position for an incision for cataract surgery may not be the same as the optimal position of an incision for solely placing an ocular implant, such as implant 650, into Schlemm's canal. With previous ocular implant delivery system designs, in order to allow for substantially tangential entry of the cannula into Schlemm's canal two separate incisions may be required when the implant is placed in combination with another ocular procedure. The curved configuration of both the distal portion 644 may be configured to allow for substantially tangential entry of the cannula 608 into Schlemm's canal. It is further contemplated that the curved configuration of the intermediate portion 645 may allow the cannula 608 to be advanced through typical incisions associated with and/or optimized for cataract surgery, such as, but not limited to, a sclerocorneal tunnel incision, while still allowing for substantially tangential entry of the cannula 608 into Schlemm's canal. This may allow for two or more ocular procedures to be performed using a single incision. It is further contemplated that performing multiple procedures through a single incision may reduce patient discomfort and recovery time. FIG. 28B shows delivery tool 652 of delivery system 600 extending through distal opening 632 of cannula 608. Delivery tool 652 includes an interlocking portion 660 that is configured to form a connection with a complementary interlocking portion 662 of ocular implant 650, as explained in more detail below. In the embodiment of FIG. 28, rotating the tracking wheel will cause delivery tool 652 and ocular implant 650 to move along a path defined by cannula 608. Cannula 608 is sized and configured so that the distal end of cannula 608 can be advanced through the trabecular meshwork of the eye and into Schlemm's canal. Positioning cannula 608 in this way places distal opening 632 in fluid communication with Schlemm's canal. Ocular implant 650 may be placed in Schlemm's canal by advancing the ocular implant through distal opening 632 of cannula 608 while the distal opening is in fluid communication with Schlemm's canal. The distal portion of the cannula 608 may include a cutting portion configured to cut through the trabecular meshwork and the wall of Schlemm's canal, such as by providing distal end 634 with a sharp edge adapted to cut through such tissue.

FIG. 29 is an enlarged perspective view further illustrating delivery system 600 shown in the previous figure and an eye 601. In FIG. 29, cannula 608 of delivery system 600 is shown extending through a cornea 603 of eye 601. A distal portion of cannula 608 is disposed inside the anterior chamber defined by cornea 603 of eye 601. In the embodiment of FIG. 29, cannula 608 is configured so that a distal opening 632 of cannula 608 can be placed in fluid communication with Schlemm's canal. For example, distal portion 644 and intermediate portion 645 of cannula 608 may be dimensioned and configured such that cannula 608 may be advanced through an incision 607 created for another optical surgical procedure.

In the embodiment of FIG. 29, an ocular implant is disposed in a passageway defined by cannula 608. Delivery system 600 includes a mechanism that is capable of advancing and retracting the ocular implant along the length of cannula 608. The ocular implant may be placed in Schlemm's canal of eye 601 by advancing the ocular implant through the distal opening of cannula 608 while the distal opening is in fluid communication with Schlemm's canal.

FIG. 30 is a perspective view further illustrating delivery system 600 shown in the previous figure. In FIG. 30, a portion of housing 602 has been removed for purposes of illustration. Delivery system 600 includes a delivery tool subassembly 670 and a cannula subassembly 680. Delivery tool subassembly 670 includes rotating rack gear 620 and a delivery tool (not shown). In the embodiment of FIG. 30, the delivery tool extends into a passageway defined by a cannula 608. Cannula 608 can be seen extending beyond sleeve 604 in FIG. 30. Cannula subassembly 680 includes cannula 608, a hub 672, and an extension tube (not shown). In the embodiment of FIG. 30, the extension tube of cannula subassembly 680 is disposed inside a lumen defined by rotating rack gear 620.

Delivery system 600 includes a mechanism 617 that controls the movement of delivery tool subassembly 670. Mechanism 617 includes a number of components that are located inside housing 602, including tracking wheel 606, an idler gear 622, and the rotating rack gear 620. In the embodiment of FIG. 30, tracking wheel 606 and idler gear 622 are both rotatably supported by housing 602. Gear teeth on tracking wheel 606 engage gear teeth on idler gear 622, which in turn engage gear teeth on the rotating rack gear 620. Rotating tracking wheel 606 in a counter clockwise direction CCW causes idler gear 622 to rotate in a clockwise direction CW, which in turn causes the rotating rack gear 620 to move in a distal direction D. Rotating tracking wheel 606 in a clockwise direction CW causes idler gear 622 to rotate in a counter clockwise direction CCW, which in turn causes the rotating rack gear 620 to move in a proximal direction P. In other embodiments, the idler gear 622 may be eliminated from the device, which would cause counter-clockwise movement of the tracking wheel to move the rack gear proximally.

In the embodiment of FIG. 30, a sleeve 604 is fixed to cannula subassembly 680. Sleeve 604 may be rotated by the user to change the orientation of cannula 608 with respect to housing 602. The sleeve 604 may include gripping features, such as grooves (as shown), a rubber coating, or other frictional surfaces to facilitate this use. In some applications, correct alignment between the cannula and iris is advantageous to ensure that the core tube and/or ocular implant is advanced at the correct trajectory relative to Schlemm's canal or other anatomy in the eye into which the ocular implant is to be implanted. The device is configured in a manner that keeps the ocular implant aligned within the device during rotation. Selected groups of components are keyed together to ensure that they rotate as a single body while simultaneously allowing axial movement of the ocular implant. In the embodiment of FIG. 30, cannula subassembly 680 and delivery tool subassembly 670 may rotate in unison with sleeve 604 relative to housing 602.

In the embodiment of FIG. 30, rotating rack gear 620 is configured to rotate with sleeve 604 while maintaining the ability to move axially in the distal and proximal directions before, during, and after rotation. As the rotating rack gear 620 moves distally and/or proximally, it causes corresponding movement of the delivery tool relative to cannula 608. This movement is transferred to ocular implant 650 when delivery tool 652 is coupled to ocular implant 650. Delivery tool subassembly 670 and cannula subassembly 680 engage one another in a keyed arrangement, as described in more detail below. This keyed arrangement causes delivery tool subassembly 670 and cannula subassembly 680 to maintain a constant rotational orientation relative to each other while, at the same time, allowing delivery tool subassembly 670 to translate in a distal direction D and a proximal direction P relative to cannula subassembly 680.

In some embodiments, delivery tool 652 is formed from shape memory material (such as, e.g., nitinol), and at least a portion of delivery tool 652 assumes a curved at-rest shape when no external forces are acting on it. Delivery tool 652 can be urged to assume a straightened shape, for example, by inserting delivery tool 652 through a straight portion of the passageway defined by cannula 608. When the delivery tool 652 is confined, such as within cannula 608, the interlocking portion can engage the complementary interlocking portion to join the delivery tool and ocular implant together, and allow the delivery tool and ocular implant to move together through the cannula 608, as described in more detail below.

FIGS. 28, 29, and 30 illustrate more detailed views of cannula 608. FIG. 31 is a side view of a cannula 608 in accordance with the present detailed description, FIG. 32 is an enlarged detail view of cannula 608, and FIG. 33 is an enlarged perspective view further illustrating a portion of distal portion 644 of cannula 608. Cannula 608 comprises a generally tubular member 698 having a central axis 696. Generally, tubular member 698 comprises a proximal end 641, a proximal portion 640, an intermediate portion 645, a distal portion 644, and a distal end 634. Cannula 608 may extend a distance D1 between proximal end 641 and distal end 634. Tubular member 698 may have a length along central axis 696 that is longer than distance D1 between proximal end 641 and distal end 634. For purposes of example, It is contemplated that distance D1 may be in the range of 1.50 to 3.50 inches (3.81 to 8.89 centimeters), 2.0 to 3.0 inches (5.08 to 7.62 centimeters) or around 2.50 inches (6.35 centimeters). It is contemplated cannula 608 may span any distance D1 desired. Proximal portion 640 may extend over a distance D2 from proximal end 641 to a point 643 distal to proximal end 641. Proximal portion 640 may be generally straight such that distance D2 is approximately equal to or equal to a length of proximal portion 640 measured along central axis 696. Distance D2 may be in the range of 1.50 to 2.50 inches (3.81 to 6.35 centimeters), 1.75 to 2.25 inches (4.652 to 5.72 centimeters), or around 2.0 inches (5.08 centimeters). Intermediate portion 645 may extend between first point 643 and a second point 647 located proximal to distal end 634 of cannula 608. Intermediate portion 645 may span a distance D3 extending from point 643 and point 647. Distance D3 may be in the range of 0.15 to 0.50 inches (0.38 to 1.27 centimeters), 0.25 to 0.40 inches (0.64 to 1.02 centimeters), or around 0.33 inches (0.84 centimeters). Intermediate portion 645 may have a length along central axis 696 of tubular member 698 that is longer than distance D3. The difference in the length of intermediate portion 645 and the distance D3 may be determined by the degree of curvature of intermediate portion 645, as will be discussed in more detail below. Distal portion 644 may extend between second point 647 and distal end 634. Distal portion 644 may span a distance D4 extending from point 647 and distal end point 634. Distance D4 may be in the range of 0.05 to 0.30 inches (0.13 to 0.76 centimeters), 0.13 to 0.23 inches (0.33 to 0.58 centimeters), or around 0.17 inches (0.43 centimeters). Distal portion 644 may have a length along central axis 696 of tubular member 698 that is longer than distance D4. The difference in the length of distal portion 644 and the distance D4 may be determined by the degree of curvature of distal portion 644, as will be discussed in more detail below.

A distal opening surface 642 surrounds a distal opening 632 extending through the distal end 634 and through a side wall of cannula 608. A beveled edge 665 is disposed at the distal end of distal opening surface 642, extending from the distal end 634 to a proximal extent 667 of beveled edge 665. Tubular member 698 defines distal opening 632, a proximal opening 636, and a passageway 638 extending between proximal opening 636 and distal opening 632.

Proximal portion 640 of cannula 608 is substantially straight while intermediate portion 645 and distal portion 644 of cannula 608 may be curved. In the embodiment of FIG. 31, distal portion 644 is curved along its entire length and intermediate portion 645 is curved along its entire length. Intermediate portion 645 may define a curve having a first radius R1 measured from central axis 696 and defining a first radius of curvature. The length of intermediate portion 645 along central axis 696 may be determined by the measure of the arc (in degrees) and the radius of the curve using Equation 1 below:

$\begin{matrix} L_{arc} = θ (\frac{π}{180}) r & Equation 1 \end{matrix}$

where L_arcis the length of the arc, θ is the angle measure of the arc (in degrees), and r is the radius of the circle. In some instances, the angle measure of intermediate portion 645 may be in the range of 10° to 25°, although other angles are possible. Distal portion 644 may define a curve having a second radius R2 and defining a second radius of curvature. The length of distal portion 644 along central axis 696 may be determined by the measure of the arc (in degrees) and the radius of the curve using Equation 1 above. In some instances, the angle measure of distal portion 644 may be in the range of 90° to 110°, although other angles are possible. It is contemplated that the first radius R1 may be larger than the second radius R2 such that the distal portion 644 has a higher curvature than the intermediate portion 645. This configuration may advance the ocular implant at the correct trajectory relative to Schlemm's canal or other anatomy in the eye into which the ocular implant is to be implanted. For example, the configuration may allow the cannula 608 to be advanced through an incision generally along a major axis of the visible eye and allowing for substantially tangential entry of cannula 608 into Schlemm's canal. It is contemplated that first radius R1 and second radius R2 may be selected to facilitate delivery of implant 650 to other anatomical locations.

FIG. 31A is an additional side view and illustrates a sectioned view of the cannula shown in FIG. 28. For purposes of example, cannula 608 comprises a generally tubular member 698 having a central axis 696. Generally tubular member 698 comprises a proximal end 641, a proximal portion 640, an intermediate portion 645, a distal portion 644, and a distal end 634. Additionally, for example, the central axis 696 of proximal portion 640 is tangential to the tangential line at first point 643 of intermediate portion 645. Further, the tangential line at second point 647 of intermediate portion 645 is tangential to the tangential line of the second point 647 of distal portion 644. The tangential line at distal end 634 of distal portion 644 and the central axis 696 of proximal portion may have third radius R3, for example, having an angle approximately in the range of 90° to 165°.

A method in accordance with this detailed description may include the step of advancing the distal end 634 of cannula 608 through the cornea of a human eye so that distal end 634 is disposed in the anterior chamber of the eye. Cannula 608 may then be used to access Schlemm's canal of the eye, for example, by piercing the wall of Schlemm's canal with the distal end 634 of cannula 608. The beveled edge 665 may be inserted into Schlemm's canal to place at least part of distal opening 632 of cannula 608 in communication with Schlemm's canal. For example, cannula 608 may be advanced until the distal tip 634 and beveled edge 665 of cannula 608 have been inserted into Schlemm's canal up to the proximal extent 667 of beveled edge 665. With the passageway of the cannula 608 placed in fluid communication with the lumen of Schlemm's canal, the ocular implant may be advanced out of a distal port of the cannula 608 and into Schlemm's canal.

In the embodiment of FIG. 32 and further illustrated in FIG. 33, distal portion 644 of cannula 608 defines a trough 654. In some embodiments, trough 654 is configured to receive the entire external cross section of an ocular implant as the ocular implant is being advanced into Schlemm's canal. When this is the case, trough 654 may have a depth dimension that is deeper than a width of the ocular implant. This cannula configuration advantageously prevents the ocular implant from intersecting the layers of the trabecular meshwork as the ocular implant is advanced into Schlemm's canal. Trough 654 may also be configured to allow the proximal portion of the ocular implant to be released from the delivery tool in a manner similar to trough 554 described above.

Referring briefly to FIG. 28B, while not explicitly shown, during advancement of ocular implant 650 interlocking portion 660 of delivery tool 652 and complementary interlocking portion 662 of ocular implant 650 may be engaged with each other so that a proximal end of ocular implant 650 is proximal to the distal end of delivery tool 652. Surface 661 of delivery tool 652 rests against the wall of cannula 608 to prevent interlocking portion 660 of delivery tool 652 and complementary interlocking portion 662 of ocular implant 650 from disengaging one another. When they are connected in this fashion, delivery tool 652 and ocular implant 650 move together as the delivery tool is advanced and retracted relative to cannula 608 by the delivery system mechanism. In some embodiments, the ocular implant 650 has a radius of curvature that is larger than the radius of curvature of the distal portion 644 of cannula 608. This arrangement ensures that the ocular implant will track along trough 654 as the ocular implant is urged in a distal direction by delivery system 600.

Once cannula 608 has been positioned in the desired location, ocular implant 650 may be advanced distally while cannula 608 is held stationary. Elongate opening 632 may provide direct visualization of ocular implant 650 as it is advanced into Schlemm's canal. A configuration allowing direct visualization of the ocular implant has a number of clinical advantages. During a medical procedure, it is often difficult to monitor the progress of the implant by viewing the implant through the trabecular meshwork. For example, blood reflux may push blood into Schlemm's canal obstructing a physician's view the portion of the implant that has entered Schlemm's canal. Ocular implant 650 tracks along trough 654 as it is advanced distally along cannula 608. The trough opening allows the physician to monitor the progress of the implant by viewing the implant structures as they advance through the trough prior to entering Schlemm's canal. The trough opening also allows the physician to identify the position of the proximal end of the ocular implant with respect to the incision made by the cannula to access Schlemm's canal.

Delivery tool 652 may advance ocular implant 650 distally until delivery tool surface 661 and part of the reduced diameter portion 663 have now passed into opening 632, thereby permitting the delivery tool curved portion to move toward its curved at-rest shape so that the delivery tool engagement surface 660 disengages and moves away from its complementary engagement surface 662 on the ocular implant 650. After the disengaging from the ocular implant, cannula 608 and delivery tool 652 can be withdrawn from Schlemm's canal leaving the ocular implant 650 in the fully deployed position. After delivery of ocular implant 650 is complete, the delivery tool 652 and the cannula 608 may be removed from the eye, leaving at least a distal portion of the ocular implant 650 in Schlemm's canal. An inlet portion of ocular implant 650 may be positioned in the anterior chamber of the eye and the remainder of ocular implant 650 in Schlemm's canal. The presence of ocular implant 650 in Schlemm's canal may facilitate the flow of aqueous humor out of the anterior chamber. This flow may include axial flow along Schlemm's canal, flow from the anterior chamber into Schlemm's canal, and flow leaving Schlemm's canal via outlets communicating with Schlemm's canal. When in place within the eye, ocular implant 650 will support the trabecular meshwork and Schlemm's canal tissue and will provide for improved communication between the anterior chamber and Schlemm's canal (via the trabecular meshwork) and between pockets or compartments along Schlemm's canal.

The cannula 608 may further include a pressure sensor 690 disposed within the trough 654. The pressure sensor 690 may be similar in form and function to pressure sensor 180 described above. While the pressure sensor 690 is illustrated as mounted within the trough 654 of the cannula, it is contemplated that the pressure sensor 690 may be mounted at other locations within or on the cannula 608. The pressure sensor 690 may provide an instantaneous pressure reading during implantation of the ocular implant 650 or shortly thereafter. In some instances, the pressure reading obtained from the pressure sensor 690 on the cannula 608 can be compared to a pressure reading obtained from a pressure sensor mounted on the ocular implant 650, if so provided.

The pressure sensor 690 may be a Micro-Electro-Mechanical System (MEMS) pressure sensor. While the pressure sensor 690 has been described as a MEMS pressure sensor, it is contemplated that other pressure sensors may be used in place of, or in addition to, a MEMS pressure sensor. Further, while only a single pressure sensor 690 has been illustrated, the cannula 608 may include more than one pressure sensor 690, as desired. MEMS pressure sensors are often formed by anisotropically etching a recess into a back side of a silicon substrate die, leaving a thin flexible diaphragm. In operation, at least one surface of the diaphragm is exposed to an input pressure (e.g. the ocular pressure). The diaphragm deflects according to the magnitude of the input pressure, which may be detected by one or more electrical components or sense elements (e.g. piezoresistors) positioned on or embedded within the diaphragm. The change in resistance of the piezoresistors is reflected as a change in an output voltage signal from a resistive bridge formed at least in part by the piezoresistors. In some cases, the diaphragm may be made thinner with the addition of support bosses, which may help increase the sensitivity of the diaphragm over a flat plate diaphragm. Circuit elements may be connected so that sensor elements to provide some level of signal processing before providing an output signal to bond pads of the pressure sensor. The signal processing may filter, amplify, linearize, calibrate and/or otherwise process the raw sensor signal produced by the sensor elements (e.g. piezoresistors). While the sense elements have been described as piezoresistors, it is contemplated that the sense elements may be selected to provide a capacitive pressure sensor 690.

The pressure sensor 690 may be further provided with an antenna or inductor to allow the data from the pressure sensor 690 to be wirelessly communicated to a readout device. In some instances, the pressure sensor 690 may use radiofrequency communication protocols, such as, but not limited to cellular communication, ZigBee®, Bluetooth®, WiFi®, IrDA, dedicated short range communication (DSRC), EnOcean®, or any other suitable wireless protocols, as desired to transmit the data from the pressure sensor 690 to another device located outside the body. The data may be transmitted to any number so suitably enabled devices, including, but not limited to, cellular phones, tablet computers, computers, portable handheld devices, such a personal digital assistant (PDA), or a specially designed device. This may allow a physician, patient, or other interested party to monitor the ocular pressure without the use of a tonometer.

Components of ocular device may be made from a metal, metal alloy, polymer (some examples of which are disclosed below), a metal-polymer composite, ceramics, combinations thereof, and the like, or other suitable material. Some examples of suitable polymers may include polytetrafluoroethylene (PTFE), ethylene tetrafluoroethylene (ETFE), fluorinated ethylene propylene (FEP), polyoxymethylene (POM, for example, DELRIN® available from DuPont), polyether block ester, polyurethane (for example, Polyurethane 85A), polypropylene (PP), polyvinylchloride (PVC), polyether-ester (for example, ARNITEL® available from DSM Engineering Plastics), ether or ester based copolymers (for example, utylene/poly(alkylene ether) phthalate and/or other polyester elastomers such as HYTREL® available from DuPont), polyamide (for example, DURETHAN® available from Bayer or CRISTAMID® available from Elf Atochem), elastomeric polyamides, block polyamide/ethers, polyether block amide (PEBA, for example available under the trade name PEBAX®), ethylene vinyl acetate copolymers (EVA), silicones, polyethylene (PE), Marlex high-density polyethylene, Marlex low-density polyethylene, linear low density polyethylene (for example REXELL®), polyester, polybutylene terephthalate (PBT), polyethylene terephthalate (PET), polytrimethylene terephthalate, polyethylene naphthalate (PEN), polyetheretherketone (PEEK), polyimide (PI), polyetherimide (PEI), polyphenylene sulfide (PPS), polyphenylene oxide (PPO), poly praraphenylene terephthalamide (for example, KEVLAR), polysulfone, nylon, nylon-12 (such as GRILAMID® available from EMS American Grilon), perfluoro(propyl vinyl ether) (PFA), ethylene vinyl alcohol, polyolefin, polystyrene, epoxy, polyvinylidene chloride (PVdC), poly(styrene-b-isobutylene-b-styrene) (for example, SIBS and/or SIBS 50A), polycarbonates, ionomers, biocompatible polymers, other suitable materials, or mixtures, combinations, copolymers thereof, polymer/metal composites, and the like. In some embodiments the sheath can be blended with a liquid crystal polymer (LCP). For example, the mixture can contain up to about 6 percent LCP.

Some examples of suitable metals and metal alloys include stainless steel, such as 304V, 304L, and 316LV stainless steel; mild steel; nickel-titanium alloy such as linear-elastic and/or super-elastic nitinol; other nickel alloys such as nickel-chromium-molybdenum alloys (e.g., UNS: N06625 such as INCONEL® 625, UNS: N06022 such as HASTELLOY® C-22®, UNS: N10276 such as HASTELLOY® C276®, other HASTELLOY® alloys, and the like), nickel-copper alloys (e.g., UNS: N04400 such as MONEL® 400, NICKELVAC® 400, NICORROS® 400, and the like), nickel-cobalt-chromium-molybdenum alloys (e.g., UNS: R30035 such as MP35-N® and the like), nickel-molybdenum alloys (e.g., UNS: N10665 such as HASTELLOY® ALLOY B2®), other nickel-chromium alloys, other nickel-molybdenum alloys, other nickel-cobalt alloys, other nickel-iron alloys, other nickel-copper alloys, other nickel-tungsten or tungsten alloys, and the like; cobalt-chromium alloys; cobalt-chromium-molybdenum alloys (e.g., UNS: R30003 such as ELGILOY®, PHYNOX®, and the like); platinum enriched stainless steel; titanium; combinations thereof; and the like; or any other suitable material.

As alluded to herein, within the family of commercially available nickel-titanium or nitinol alloys, is a category designated “linear elastic” or “non-super-elastic” which, although may be similar in chemistry to conventional shape memory and super elastic varieties, may exhibit distinct and useful mechanical properties. Linear elastic and/or non-super-elastic nitinol may be distinguished from super elastic nitinol in that the linear elastic and/or non-super-elastic nitinol does not display a substantial “superelastic plateau” or “flag region” in its stress/strain curve like super elastic nitinol does. Instead, in the linear elastic and/or non-super-elastic nitinol, as recoverable strain increases, the stress continues to increase in a substantially linear, or a somewhat, but not necessarily entirely linear relationship until plastic deformation begins or at least in a relationship that is more linear that the super elastic plateau and/or flag region that may be seen with super elastic nitinol. Thus, for the purposes of this disclosure linear elastic and/or non-super-elastic nitinol may also be termed “substantially” linear elastic and/or non-super-elastic nitinol.

In some cases, linear elastic and/or non-super-elastic nitinol may also be distinguishable from super elastic nitinol in that linear elastic and/or non-super-elastic nitinol may accept up to about 2-5% strain while remaining substantially elastic (e.g., before plastically deforming) whereas super elastic nitinol may accept up to about 8% strain before plastically deforming. Both of these materials can be distinguished from other linear elastic materials such as stainless steel (that can also can be distinguished based on its composition), which may accept only about 0.2 to 0.44 percent strain before plastically deforming.

In some embodiments, the linear elastic and/or non-super-elastic nickel-titanium alloy is an alloy that does not show any martensite/austenite phase changes that are detectable by differential scanning calorimetry (DSC) and dynamic metal thermal analysis (DMTA) analysis over a large temperature range. For example, in some embodiments, there may be no martensite/austenite phase changes detectable by DSC and DMTA analysis in the range of about −60 degrees Celsius (° C.) to about 120° C. in the linear elastic and/or non-super-elastic nickel-titanium alloy. The mechanical bending properties of such material may therefore be generally inert to the effect of temperature over this very broad range of temperature. In some embodiments, the mechanical bending properties of the linear elastic and/or non-super-elastic nickel-titanium alloy at ambient or room temperature are substantially the same as the mechanical properties at body temperature, for example, in that they do not display a super-elastic plateau and/or flag region. In other words, across a broad temperature range, the linear elastic and/or non-super-elastic nickel-titanium alloy maintains its linear elastic and/or non-super-elastic characteristics and/or properties.

In some embodiments, the linear elastic and/or non-super-elastic nickel-titanium alloy may be in the range of about 50 to about 60 weight percent nickel, with the remainder being essentially titanium. In some embodiments, the composition is in the range of about 54 to about 57 weight percent nickel. One example of a suitable nickel-titanium alloy is FHP-NT alloy commercially available from Furukawa Techno Material Co. of Kanagawa, Japan. Some examples of nickel titanium alloys are disclosed in U.S. Pat. Nos. 5,238,004 and 6,508,803, which are incorporated herein by reference. Other suitable materials may include ULTANIUM™ (available from Neo-Metrics) and GUM METAL™ (available from Toyota). In some other embodiments, a superelastic alloy, for example a superelastic nitinol can be used to achieve desired properties.

It is to be understood that even though numerous characteristics of various embodiments have been set forth in the foregoing description, together with details of the structure and function of various embodiments, this detailed description is illustrative only, and changes may be made in detail, especially in matters of structure and arrangements of parts illustrated by the various embodiments to the full extent indicated by the broad general meaning of the terms in which the appended claims are expressed.

Claims

1. An ocular implant adapted to reside at least partially in a portion of Schlemm's canal of an eye, the implant comprising: a tubular body having an inner surface and an outer surface and comprising a plurality of struts extending along a longitudinal axis of the tubular body and a plurality of open areas surrounded by the plurality of struts, the tubular body extending in a curved volume whose longitudinal axis forms an arc of a circle;a polymer rod disposed within the curved volume of the tubular body;at least one therapeutic agent disposed within an interstitial space of the polymer rod; andthe tubular body having a diameter of between 0.005 inches and 0.04 inches.
2. The implant of claim 1, further comprising a sleeve disposed over an outer surface of the tubular body and the polymer rod.
3. The implant of claim 2, wherein the sleeve is porous.
4. The implant of claim 1, wherein the therapeutic agent is an intraocular pressure reducing drug.
5. The implant of claim 1, wherein when implanted the therapeutic agent is configured to elute from the polymer rod over a period of 1 to 15 years.
6. The implant of claim 1, further comprising a heparin related coating disposed over an outer surface of the tubular body and the polymer rod.
7. The implant of claim 3, wherein an elution rate of the therapeutic agent, when implanted, is controlled by a size of one or more pores in the sleeve.

CROSS-REFERENCE TO RELATED APPLICATIONS

This application is a National Stage of International Application Serial No. PCT/US2019/018559, filed Feb. 19, 2019, which claims the benefit of priority under 35 U.S.C. § 119 of U.S. Provisional Application Ser. No. 62/633,823, filed Feb. 22, 2018, the entirety of which are incorporated herein by reference.

PCT Information

Filing Document	Filing Date	Country	Kind
PCT/US2019/018559	2/19/2019	WO

Publishing Document	Publishing Date	Country	Kind
WO2019/164834	8/29/2019	WO	A

US Referenced Citations (588)

Number	Name	Date	Kind
703296	Arnold	Jun 1902	A
1601709	Windom	Oct 1926	A
2716983	George et al.	Sep 1955	A
3071135	Baldwin et al.	Jan 1963	A
3788327	Donowitz et al.	Jan 1974	A
3811442	Maroth	May 1974	A
3858577	Bass et al.	Jan 1975	A
3884236	Krasnov	May 1975	A
3948271	Akiyama	Apr 1976	A
3958558	Dunphy et al.	May 1976	A
3982541	L'Esperance	Sep 1976	A
4037604	Newkirk	Jul 1977	A
4134405	Smit	Jan 1979	A
4273109	Enderby	Jun 1981	A
4391275	Fankhauser et al.	Jul 1983	A
4428746	Mendez	Jan 1984	A
4457757	Molteno	Jul 1984	A
4461294	Baron	Jul 1984	A
4470407	Hussein	Sep 1984	A
4497319	Sekine et al.	Feb 1985	A
4501274	Skjaerpe	Feb 1985	A
4517973	Sunago et al.	May 1985	A
4538608	L'Esperance	Sep 1985	A
4548205	Armeniades et al.	Oct 1985	A
4551129	Coleman et al.	Nov 1985	A
4558698	O'Dell	Dec 1985	A
4559942	Eisenberg	Dec 1985	A
4566438	Liese et al.	Jan 1986	A
4580559	L'Esperance	Apr 1986	A
4583539	Karlin et al.	Apr 1986	A
4601713	Fuquo	Jul 1986	A
4604087	Joseph	Aug 1986	A
4633866	Peyman et al.	Jan 1987	A
4658816	Ector	Apr 1987	A
4660546	Herrick et al.	Apr 1987	A
4671273	Lindsey	Jun 1987	A
4689040	Thompson	Aug 1987	A
4699140	Holmes et al.	Oct 1987	A
4706669	Schlegel	Nov 1987	A
4722350	Armeniades et al.	Feb 1988	A
4722724	Schocket	Feb 1988	A
4729373	Peyman	Mar 1988	A
4733665	Palmaz	Mar 1988	A
4750901	Molteno	Jun 1988	A
4770654	Rogers et al.	Sep 1988	A
4791927	Menger	Dec 1988	A
4826478	Schocket	May 1989	A
4846172	Berlin	Jul 1989	A
4861341	Woodburn	Aug 1989	A
4876250	Clark	Oct 1989	A
4880000	Holmes et al.	Nov 1989	A
4886488	White	Dec 1989	A
4919130	Stoy et al.	Apr 1990	A
4925299	Meisberger et al.	May 1990	A
4934363	Smith et al.	Jun 1990	A
4934809	Volk	Jun 1990	A
4936825	Ungerleider	Jun 1990	A
4946436	Smith	Aug 1990	A
4968296	Ritch et al.	Nov 1990	A
4994060	Rink et al.	Feb 1991	A
5034010	Kittrell et al.	Jul 1991	A
5092837	Ritch et al.	Mar 1992	A
5123902	Muller et al.	Jun 1992	A
5127901	Odrich	Jul 1992	A
5129895	Vassiliadis et al.	Jul 1992	A
5178604	Baerveldt et al.	Jan 1993	A
5180362	Worst	Jan 1993	A
5190552	Kelman	Mar 1993	A
5213569	Davis	May 1993	A
5238004	Sahatjian et al.	Aug 1993	A
5246452	Sinnott	Sep 1993	A
5254112	Sinofsky et al.	Oct 1993	A
5273056	McLaughlin et al.	Dec 1993	A
5290267	Zimmermann	Mar 1994	A
5300020	L'Esperance	Apr 1994	A
5359685	Waynant et al.	Oct 1994	A
5360399	Stegmann	Nov 1994	A
5371078	Clark et al.	Dec 1994	A
5372577	Ungerleider	Dec 1994	A
5445637	Bretton	Aug 1995	A
5454796	Krupin	Oct 1995	A
5458615	Klemm et al.	Oct 1995	A
5501274	Nguyen et al.	Mar 1996	A
5536259	Utterberg	Jul 1996	A
5575780	Saito	Nov 1996	A
5591223	Lock et al.	Jan 1997	A
5607966	Hellberg et al.	Mar 1997	A
5613972	Lee et al.	Mar 1997	A
5626558	Suson	May 1997	A
5643250	O'Donnell	Jul 1997	A
5653753	Brady et al.	Aug 1997	A
5657760	Ying et al.	Aug 1997	A
5676669	Colvard	Oct 1997	A
5704907	Nordquist et al.	Jan 1998	A
5713844	Peyman	Feb 1998	A
5722970	Colvard et al.	Mar 1998	A
5738676	Hammer et al.	Apr 1998	A
5738677	Colvard et al.	Apr 1998	A
5785658	Benaron et al.	Jul 1998	A
5792099	DeCamp et al.	Aug 1998	A
5792103	Schwartz et al.	Aug 1998	A
5807302	Wandel	Sep 1998	A
5811453	Yanni et al.	Sep 1998	A
5865831	Cozean et al.	Feb 1999	A
5868697	Richter et al.	Feb 1999	A
5873835	Hastings et al.	Feb 1999	A
5879319	Pynson et al.	Mar 1999	A
5885279	Bretton	Mar 1999	A
5893837	Eagles et al.	Apr 1999	A
5895831	Brasier et al.	Apr 1999	A
5919171	Kira et al.	Jul 1999	A
5948427	Yamamoto et al.	Sep 1999	A
5966058	Richter et al.	Oct 1999	A
5990099	Clark	Nov 1999	A
5993438	Juhasz et al.	Nov 1999	A
5997531	Loeb et al.	Dec 1999	A
6002480	Izatt et al.	Dec 1999	A
6007511	Prywes	Dec 1999	A
6050970	Baerveldt	Apr 2000	A
6083193	Kadziauskas et al.	Jul 2000	A
6099521	Shadduck	Aug 2000	A
6102045	Nordquist et al.	Aug 2000	A
6142990	Burk	Nov 2000	A
6146375	Juhasz et al.	Nov 2000	A
6177544	Kanal et al.	Jan 2001	B1
6186974	Allan et al.	Feb 2001	B1
6217584	Nun	Apr 2001	B1
6221078	Bylsma	Apr 2001	B1
6238409	Hojeibane	May 2001	B1
6241721	Cozean et al.	Jun 2001	B1
D444874	Haffner et al.	Jul 2001	S
6297228	Clark	Oct 2001	B1
6319274	Shadduck	Nov 2001	B1
6328747	Nun	Dec 2001	B1
6375642	Grieshaber et al.	Apr 2002	B1
6398809	Hoffmann et al.	Jun 2002	B1
6409752	Boatman et al.	Jun 2002	B1
6450984	Lynch	Sep 2002	B1
6464724	Lynch et al.	Oct 2002	B1
6471666	Odrich	Oct 2002	B1
6494857	Neuhann	Dec 2002	B1
6508779	Suson	Jan 2003	B1
6508803	Horikawa et al.	Jan 2003	B1
6517523	Kaneko et al.	Feb 2003	B1
6524275	Lynch et al.	Feb 2003	B1
6533764	Haffner et al.	Mar 2003	B1
6533768	Hill	Mar 2003	B1
6544208	Ethier et al.	Apr 2003	B2
6544249	Yu et al.	Apr 2003	B1
6551289	Higuchi et al.	Apr 2003	B1
6626858	Lynch et al.	Sep 2003	B2
6638239	Bergheim et al.	Oct 2003	B1
6666841	Gharib et al.	Dec 2003	B2
6689085	Rubenstein	Feb 2004	B1
6699210	Williams et al.	Mar 2004	B2
6699211	Savage	Mar 2004	B2
6702790	Ross	Mar 2004	B1
6726676	Stegmann et al.	Apr 2004	B2
D490152	Myall et al.	May 2004	S
6730056	Ghaem et al.	May 2004	B1
6736791	Tu et al.	May 2004	B1
6780164	Bergheim et al.	Aug 2004	B2
6783544	Lynch et al.	Aug 2004	B2
6827699	Lynch et al.	Dec 2004	B2
6827700	Lynch et al.	Dec 2004	B2
6881198	Brown	Apr 2005	B2
6899717	Weber et al.	May 2005	B2
6939298	Brown et al.	Sep 2005	B2
6955656	Bergheim et al.	Oct 2005	B2
6962573	Wilcox	Nov 2005	B1
6981958	Gharib et al.	Jan 2006	B1
6989007	Shadduck	Jan 2006	B2
7018376	Webb et al.	Mar 2006	B2
7094225	Tu et al.	Aug 2006	B2
7125119	Farberov	Oct 2006	B2
7133137	Shimmick	Nov 2006	B2
7135009	Tu et al.	Nov 2006	B2
7147650	Lee	Dec 2006	B2
7163543	Smedley et al.	Jan 2007	B2
7186232	Smedley et al.	Mar 2007	B1
7192412	Zhou et al.	Mar 2007	B1
7207965	Simon	Apr 2007	B2
7207980	Christian et al.	Apr 2007	B2
7220238	Lynch	May 2007	B2
7273475	Tu et al.	Sep 2007	B2
7297130	Bergheim et al.	Nov 2007	B2
7331984	Tu et al.	Feb 2008	B2
7355216	Yang	Apr 2008	B2
7488303	Haffner et al.	Feb 2009	B1
7699882	Stamper et al.	Apr 2010	B2
7740604	Schieber et al.	Jun 2010	B2
7931596	Rachlin et al.	Apr 2011	B2
7967772	McKenzie et al.	Jun 2011	B2
8012115	Karageozian	Sep 2011	B2
8123729	Yamamoto et al.	Feb 2012	B2
8172899	Silvestrini et al.	May 2012	B2
8267882	Euteneuer et al.	Sep 2012	B2
8282592	Schieber et al.	Oct 2012	B2
8308701	Horvath et al.	Nov 2012	B2
8337509	Schieber et al.	Dec 2012	B2
8372026	Schieber et al.	Feb 2013	B2
8414518	Schieber et al.	Apr 2013	B2
8425449	Wardle et al.	Apr 2013	B2
8475374	Irazoqui et al.	Jul 2013	B2
8512404	Frion et al.	Aug 2013	B2
8529494	Euteneuer et al.	Sep 2013	B2
8540659	Berlin	Sep 2013	B2
8551166	Schieber et al.	Oct 2013	B2
8629161	Mizuno et al.	Jan 2014	B2
8636647	Silvestrini et al.	Jan 2014	B2
8647659	Robinson et al.	Feb 2014	B2
8657776	Wardle et al.	Feb 2014	B2
8663150	Wardle et al.	Mar 2014	B2
8663303	Horvath et al.	Mar 2014	B2
8734377	Schieber et al.	May 2014	B2
8808222	Schieber et al.	Aug 2014	B2
8939906	Huang et al.	Jan 2015	B2
8939948	De Juan, Jr. et al.	Jan 2015	B2
8945038	Yablonski	Feb 2015	B2
8951221	Stegmann et al.	Feb 2015	B2
8961447	Schieber et al.	Feb 2015	B2
8974511	Horvath et al.	Mar 2015	B2
9039650	Schieber et al.	May 2015	B2
9050169	Schieber et al.	Jun 2015	B2
9066750	Wardle et al.	Jun 2015	B2
9066783	Euteneuer et al.	Jun 2015	B2
9107897	Klassen et al.	Aug 2015	B2
9155655	Wardle et al.	Oct 2015	B2
9211213	Wardle et al.	Dec 2015	B2
9226852	Schieber et al.	Jan 2016	B2
9301875	Tu et al.	Apr 2016	B2
9351874	Schieber et al.	May 2016	B2
9358156	Wardle et al.	Jun 2016	B2
9402767	Schieber et al.	Aug 2016	B2
9510973	Wardle	Dec 2016	B2
9554940	Haffner	Jan 2017	B2
9579234	Wardle et al.	Feb 2017	B2
9603741	Berlin	Mar 2017	B2
9610196	Schieber et al.	Apr 2017	B2
9636254	Yu et al.	May 2017	B2
9642746	Berlin	May 2017	B2
9693899	Wardle et al.	Jul 2017	B2
9693901	Horvath et al.	Jul 2017	B2
9693902	Euteneuer et al.	Jul 2017	B2
9730638	Haffner et al.	Aug 2017	B2
9757276	Penhasi	Sep 2017	B2
9775729	McClain et al.	Oct 2017	B2
9782293	Doci	Oct 2017	B2
9788999	Schaller	Oct 2017	B2
9795503	Perez Grossmann	Oct 2017	B2
9808373	Horvath et al.	Nov 2017	B2
9820883	Berlin	Nov 2017	B2
9833357	Berlin	Dec 2017	B2
9931243	Wardle et al.	Apr 2018	B2
10159601	Berlin	Dec 2018	B2
10335314	Berlin	Jul 2019	B2
10363168	Schieber et al.	Jul 2019	B2
10390993	Berlin	Aug 2019	B1
10406025	Wardle et al.	Sep 2019	B2
10492949	Wardle et al.	Dec 2019	B2
10537474	Euteneuer et al.	Jan 2020	B2
10617558	Schieber et al.	Apr 2020	B2
10687978	Berlin	Jun 2020	B2
10709547	Schieber	Jul 2020	B2
20010002438	Sepetka et al.	May 2001	A1
20020003546	Mochimaru et al.	Jan 2002	A1
20020013546	Grieshaber et al.	Jan 2002	A1
20020013572	Berlin	Jan 2002	A1
20020026200	Savage	Feb 2002	A1
20020052653	Durgin	May 2002	A1
20020072673	Yamamoto et al.	Jun 2002	A1
20020082591	Haefliger	Jun 2002	A1
20020133168	Smedley et al.	Sep 2002	A1
20020143284	Tu et al.	Oct 2002	A1
20020165504	Sharp et al.	Nov 2002	A1
20020165522	Holmen	Nov 2002	A1
20020193805	Ott et al.	Dec 2002	A1
20030004457	Andersson	Jan 2003	A1
20030014092	Neuhann	Jan 2003	A1
20030040754	Mitchell et al.	Feb 2003	A1
20030055372	Lynch et al.	Mar 2003	A1
20030060748	Baikoff	Mar 2003	A1
20030060752	Bergheim et al.	Mar 2003	A1
20030060784	Hilgers et al.	Mar 2003	A1
20030093084	Nissan et al.	May 2003	A1
20030097151	Smedley et al.	May 2003	A1
20030105456	Lin	Jun 2003	A1
20030125351	Azuma et al.	Jul 2003	A1
20030167031	Odland	Sep 2003	A1
20030175324	Robinson	Sep 2003	A1
20030181848	Bergheim et al.	Sep 2003	A1
20030187384	Bergheim et al.	Oct 2003	A1
20030212387	Kurtz et al.	Nov 2003	A1
20030220603	Lynch	Nov 2003	A1
20030229303	Haffner et al.	Dec 2003	A1
20030236483	Ren	Dec 2003	A1
20030236484	Lynch et al.	Dec 2003	A1
20040024345	Gharib et al.	Feb 2004	A1
20040024453	Castillejos	Feb 2004	A1
20040030302	Kamata et al.	Feb 2004	A1
20040070761	Horvath et al.	Apr 2004	A1
20040082939	Berlin	Apr 2004	A1
20040088048	Richter et al.	May 2004	A1
20040092856	Dahan	May 2004	A1
20040098124	Freeman et al.	May 2004	A1
20040102729	Haffner et al.	May 2004	A1
20040106975	Solovay et al.	Jun 2004	A1
20040111050	Smedley et al.	Jun 2004	A1
20040116909	Neuberger et al.	Jun 2004	A1
20040122380	Utterberg	Jun 2004	A1
20040127843	Tu et al.	Jul 2004	A1
20040147870	Burns et al.	Jul 2004	A1
20040193095	Shadduck	Sep 2004	A1
20040193262	Shadduck	Sep 2004	A1
20040199149	Myers et al.	Oct 2004	A1
20040199171	Akahoshi	Oct 2004	A1
20040210181	Vass et al.	Oct 2004	A1
20040210185	Tu	Oct 2004	A1
20040216749	Tu	Nov 2004	A1
20040225250	Yablonski	Nov 2004	A1
20040225357	Worst et al.	Nov 2004	A1
20040228013	Goldstein et al.	Nov 2004	A1
20040249333	Bergheim et al.	Dec 2004	A1
20040254517	Quiroz-Mercado et al.	Dec 2004	A1
20040254519	Tu et al.	Dec 2004	A1
20040254520	Porteous et al.	Dec 2004	A1
20040260228	Lynch et al.	Dec 2004	A1
20050041200	Rich	Feb 2005	A1
20050043722	Lin	Feb 2005	A1
20050049578	Tu et al.	Mar 2005	A1
20050090806	Lynch et al.	Apr 2005	A1
20050090807	Lynch et al.	Apr 2005	A1
20050101967	Weber et al.	May 2005	A1
20050107734	Coroneo	May 2005	A1
20050119601	Lynch et al.	Jun 2005	A9
20050119636	Haffner et al.	Jun 2005	A1
20050125003	Pinchuk et al.	Jun 2005	A1
20050131514	Hijlkema et al.	Jun 2005	A1
20050149114	Cartledge et al.	Jul 2005	A1
20050154443	Linder et al.	Jul 2005	A1
20050165385	Simon	Jul 2005	A1
20050192527	Gharib et al.	Sep 2005	A1
20050197667	Chan et al.	Sep 2005	A1
20050203542	Weber et al.	Sep 2005	A1
20050209549	Bergheim et al.	Sep 2005	A1
20050209550	Bergheim et al.	Sep 2005	A1
20050240168	Neuberger et al.	Oct 2005	A1
20050244464	Hughes	Nov 2005	A1
20050245916	Connor	Nov 2005	A1
20050250788	Tu et al.	Nov 2005	A1
20050260186	Bookbinder et al.	Nov 2005	A1
20050266047	Tu et al.	Dec 2005	A1
20050271704	Tu et al.	Dec 2005	A1
20050273033	Grahn et al.	Dec 2005	A1
20050277864	Haffner	Dec 2005	A1
20050277912	John	Dec 2005	A1
20050279369	Lin	Dec 2005	A1
20050283108	Savage	Dec 2005	A1
20050288619	Gharib et al.	Dec 2005	A1
20050288745	Andersen et al.	Dec 2005	A1
20060015089	Meglin	Jan 2006	A1
20060020247	Kagan et al.	Jan 2006	A1
20060021623	Miller et al.	Feb 2006	A1
20060032507	Tu	Feb 2006	A1
20060052879	Kolb	Mar 2006	A1
20060069340	Simon	Mar 2006	A1
20060074375	Bergheim et al.	Apr 2006	A1
20060079828	Brown	Apr 2006	A1
20060084907	Bergheim et al.	Apr 2006	A1
20060084954	Zadoyan et al.	Apr 2006	A1
20060093642	Ranade	May 2006	A1
20060106370	Baerveldt et al.	May 2006	A1
20060110428	deJuan et al.	May 2006	A1
20060116626	Smedley et al.	Jun 2006	A1
20060117859	Liu et al.	Jun 2006	A1
20060129141	Lin	Jun 2006	A1
20060149194	Conston et al.	Jul 2006	A1
20060154382	Basceri et al.	Jul 2006	A1
20060154981	Klimko et al.	Jul 2006	A1
20060155238	Shields	Jul 2006	A1
20060155265	Juhasz et al.	Jul 2006	A1
20060155300	Stamper et al.	Jul 2006	A1
20060167421	Quinn	Jul 2006	A1
20060167466	Dusek	Jul 2006	A1
20060173397	Tu	Aug 2006	A1
20060173399	Rodgers et al.	Aug 2006	A1
20060178674	McIntyre	Aug 2006	A1
20060189915	Camras et al.	Aug 2006	A1
20060189916	Bas et al.	Aug 2006	A1
20060189917	Mayr et al.	Aug 2006	A1
20060195055	Bergheim et al.	Aug 2006	A1
20060195056	Bergheim et al.	Aug 2006	A1
20060195187	Stegmann et al.	Aug 2006	A1
20060200113	Haffner et al.	Sep 2006	A1
20060204738	Dubrow	Sep 2006	A1
20060224146	Lin	Oct 2006	A1
20060241749	Tu et al.	Oct 2006	A1
20060259021	Lin	Nov 2006	A1
20060264971	Akahoshi	Nov 2006	A1
20060276759	Kinast et al.	Dec 2006	A1
20070010827	Tu et al.	Jan 2007	A1
20070021725	Villette	Jan 2007	A1
20070027452	Varner et al.	Feb 2007	A1
20070073275	Conston et al.	Mar 2007	A1
20070088432	Solovay et al.	Apr 2007	A1
20070093794	Wang et al.	Apr 2007	A1
20070093796	Raksi et al.	Apr 2007	A1
20070106200	Levy	May 2007	A1
20070106236	Coroneo	May 2007	A1
20070112292	Tu et al.	May 2007	A1
20070118147	Smedley et al.	May 2007	A1
20070121120	Schachar	May 2007	A1
20070135681	Chin et al.	Jun 2007	A1
20070173791	Raksi	Jul 2007	A1
20070179520	West	Aug 2007	A1
20070191863	De Juan, Jr. et al.	Aug 2007	A1
20070202186	Yamamoto et al.	Aug 2007	A1
20070208325	Kurtz	Sep 2007	A1
20070219509	Tashiro et al.	Sep 2007	A1
20070219541	Kurtz	Sep 2007	A1
20070235543	Zadoyan et al.	Oct 2007	A1
20070236771	Zadoyan et al.	Oct 2007	A1
20070265582	Kaplan et al.	Nov 2007	A1
20070270945	Kobayashi et al.	Nov 2007	A1
20070276315	Haffner et al.	Nov 2007	A1
20070276316	Haffner	Nov 2007	A1
20070282244	Tu et al.	Dec 2007	A1
20070282245	Tu et al.	Dec 2007	A1
20070282247	Desai	Dec 2007	A1
20070293807	Lynch	Dec 2007	A1
20070293872	Peyman	Dec 2007	A1
20070298068	Badawi et al.	Dec 2007	A1
20080009781	Anwar	Jan 2008	A1
20080015488	Tu	Jan 2008	A1
20080027519	Guerrero	Jan 2008	A1
20080039768	Francis	Feb 2008	A1
20080045878	Bergheim et al.	Feb 2008	A1
20080051691	Dragoon	Feb 2008	A1
20080058704	Hee et al.	Mar 2008	A1
20080058777	Kurtz et al.	Mar 2008	A1
20080082088	Kurtz et al.	Apr 2008	A1
20080091224	Griffis et al.	Apr 2008	A1
20080119827	Kurtz et al.	May 2008	A1
20080125838	Francis	May 2008	A1
20080139959	Miethke et al.	Jun 2008	A1
20080228127	Burns et al.	Sep 2008	A1
20080278687	Somani	Nov 2008	A1
20080288082	Deal	Nov 2008	A1
20080312661	Downer et al.	Dec 2008	A1
20090005852	Gittings et al.	Jan 2009	A1
20090028953	Yamamoto et al.	Jan 2009	A1
20090030363	Gellman	Jan 2009	A1
20090030381	Lind et al.	Jan 2009	A1
20090036843	Erskine	Feb 2009	A1
20090043321	Conston et al.	Feb 2009	A1
20090054723	Khairkhahan et al.	Feb 2009	A1
20090069786	Vesely et al.	Mar 2009	A1
20090082862	Schieber et al.	Mar 2009	A1
20090104248	Rapacki	Apr 2009	A1
20090118716	Brownell	May 2009	A1
20090118717	Brownell et al.	May 2009	A1
20090118718	Raksi et al.	May 2009	A1
20090131921	Kurtz et al.	May 2009	A1
20090137988	Kurtz	May 2009	A1
20090138081	Bergheim et al.	May 2009	A1
20090157062	Hauger et al.	Jun 2009	A1
20090171327	Kurtz et al.	Jul 2009	A1
20090182421	Silvestrini et al.	Jul 2009	A1
20090198248	Yeung et al.	Aug 2009	A1
20090204053	Nissan et al.	Aug 2009	A1
20090247955	Yamamoto et al.	Oct 2009	A1
20090259126	Saal et al.	Oct 2009	A1
20090281520	Highley et al.	Nov 2009	A1
20090281530	Kom	Nov 2009	A1
20090291423	Hara	Nov 2009	A1
20100004580	Lynch et al.	Jan 2010	A1
20100036488	Juan et al.	Feb 2010	A1
20100057072	Roman et al.	Mar 2010	A1
20100114309	de Juan, Jr.	May 2010	A1
20100137981	Silvestrini et al.	Jun 2010	A1
20100173866	Hee et al.	Jul 2010	A1
20100191176	Ho et al.	Jul 2010	A1
20100191177	Chang et al.	Jul 2010	A1
20100234726	Sirimanne et al.	Sep 2010	A1
20100234790	Tu et al.	Sep 2010	A1
20100262174	Sretavan et al.	Oct 2010	A1
20100324543	Kurtz et al.	Dec 2010	A1
20100331858	Simaan et al.	Dec 2010	A1
20110028948	Raksi et al.	Feb 2011	A1
20110028949	Raksi et al.	Feb 2011	A1
20110028950	Raksi et al.	Feb 2011	A1
20110028951	Raksi et al.	Feb 2011	A1
20110028952	Raksi et al.	Feb 2011	A1
20110028953	Raksi et al.	Feb 2011	A1
20110028954	Raksi et al.	Feb 2011	A1
20110028955	Raksi	Feb 2011	A1
20110028957	Raksi et al.	Feb 2011	A1
20110028958	Raksi et al.	Feb 2011	A1
20110098809	Wardle et al.	Apr 2011	A1
20110125090	Peyman	May 2011	A1
20110144559	Lafdi	Jun 2011	A1
20110196487	Badawi et al.	Aug 2011	A1
20110218523	Robl	Sep 2011	A1
20110224597	Stegmann et al.	Sep 2011	A1
20110319806	Wardle	Dec 2011	A1
20120010702	Stegmann et al.	Jan 2012	A1
20120021397	Van Dalen et al.	Jan 2012	A1
20120022424	Yamamoto et al.	Jan 2012	A1
20120035524	Silvestrini	Feb 2012	A1
20120078362	Haffner et al.	Mar 2012	A1
20120165933	Haffner et al.	Jun 2012	A1
20120191064	Conston et al.	Jul 2012	A1
20120271272	Hammack et al.	Oct 2012	A1
20120283557	Berlin	Nov 2012	A1
20120302861	Marshall et al.	Nov 2012	A1
20120310137	Silvestrini	Dec 2012	A1
20120323159	Wardle	Dec 2012	A1
20130023837	Becker	Jan 2013	A1
20130090534	Burns et al.	Apr 2013	A1
20130182223	Wardle et al.	Jul 2013	A1
20130184631	Pinchuk	Jul 2013	A1
20130195806	Gay et al.	Aug 2013	A1
20130231603	Wardle	Sep 2013	A1
20130253402	Badawi et al.	Sep 2013	A1
20130253403	Badawi et al.	Sep 2013	A1
20130253437	Badawi et al.	Sep 2013	A1
20130253438	Badawi et al.	Sep 2013	A1
20130253528	Haffner et al.	Sep 2013	A1
20130267887	Kahook et al.	Oct 2013	A1
20130281908	Schaller et al.	Oct 2013	A1
20130289467	Haffner et al.	Oct 2013	A1
20140018720	Horvath et al.	Jan 2014	A1
20140066821	Freidland et al.	Mar 2014	A1
20140066831	Silvestrini et al.	Mar 2014	A1
20140081195	Clauson et al.	Mar 2014	A1
20140186309	Klassen et al.	Jul 2014	A1
20140213958	Clauson	Jul 2014	A1
20140248454	Lafdi	Sep 2014	A1
20140249463	Wardle	Sep 2014	A1
20140275923	Haffner et al.	Sep 2014	A1
20140303544	Haffner et al.	Oct 2014	A1
20140371624	Ziale et al.	Dec 2014	A1
20150018746	Hattenbach	Jan 2015	A1
20150022780	John et al.	Jan 2015	A1
20150038893	Haffner et al.	Feb 2015	A1
20150045714	Horvath et al.	Feb 2015	A1
20150057583	Gunn et al.	Feb 2015	A1
20150057591	Horvath et al.	Feb 2015	A1
20150065940	Rangel-Friedman et al.	Mar 2015	A1
20150148836	Heeren	May 2015	A1
20150166624	Tseng et al.	Jun 2015	A1
20150290033	Wardle et al.	Oct 2015	A1
20150305939	Vera et al.	Oct 2015	A1
20150305940	Vera et al.	Oct 2015	A1
20150313759	Vera et al.	Nov 2015	A1
20160063898	Bernal	Mar 2016	A1
20160250072	Wardle et al.	Sep 2016	A1
20160310020	Warnking et al.	Oct 2016	A1
20170127941	Ostermeier et al.	May 2017	A1
20170143541	Badawi et al.	May 2017	A1
20170164831	Choo et al.	Jun 2017	A1
20170172794	Varner et al.	Jun 2017	A1
20170172795	Lerner	Jun 2017	A1
20170172797	Horvath et al.	Jun 2017	A1
20170172798	Horvath et al.	Jun 2017	A1
20170172799	Horvath	Jun 2017	A1
20170172800	Romoda et al.	Jun 2017	A1
20170202708	Berlin	Jul 2017	A1
20170239272	Ambati et al.	Aug 2017	A1
20170251921	Phan et al.	Sep 2017	A1
20170280997	Lai et al.	Oct 2017	A1
20170281409	Haffner	Oct 2017	A1
20170348150	Horvath et al.	Dec 2017	A1
20170360609	Schieber et al.	Dec 2017	A9
20180360655	Berlin	Dec 2018	A1
20180369017	Schieber et al.	Dec 2018	A1
20190076296	Van Meter et al.	Mar 2019	A1
20190343679	Wardle et al.	Nov 2019	A1
20190380874	Schieber et al.	Dec 2019	A1
20200060876	Wardle et al.	Feb 2020	A1
20200085620	Euteneuer	Mar 2020	A1
20200197221	Schieber et al.	Jun 2020	A1
20200222238	Schieber et al.	Jul 2020	A1
20200261270	Berlin	Aug 2020	A1
20210030590	Blanda	Feb 2021	A1
20210330499	Wardle	Oct 2021	A1
20210361479	Wardle et al.	Nov 2021	A1
20220054314	Van Meter	Feb 2022	A1

Foreign Referenced Citations (94)

Number	Date	Country
199876197	Feb 1999	AU
107530190	Jan 2018	CN
4226476	Aug 1993	DE
102012221350	May 2014	DE
0168201	Jun 1988	EP
0957949	Nov 1996	EP
0766544	May 1998	EP
1615604	Aug 2009	EP
2193821	Jun 2010	EP
1715827	Dec 2010	EP
2380622	Oct 2011	EP
2468327	Jun 2012	EP
2471563	Jul 2012	EP
1833440	Aug 2012	EP
3164061	May 2017	EP
2996648	Jun 2017	EP
1732484	Aug 2017	EP
1740153	Aug 2017	EP
3076948	Aug 2017	EP
3205333	Aug 2017	EP
3060180	Sep 2017	EP
3082570	Sep 2017	EP
10504978	May 1998	JP
11123205	May 1999	JP
2002542872	Dec 2002	JP
2006517848	Aug 2006	JP
2006289075	Oct 2006	JP
2009523545	Jun 2009	JP
2010509003	Mar 2010	JP
2011502649	Jan 2011	JP
2012527318	Nov 2012	JP
2015517836	Jun 2015	JP
2017517363	Jun 2017	JP
WO9620742	Jul 1996	WO
9818509	May 1998	WO
WO9901063	Jan 1999	WO
WO9945868	Sep 1999	WO
WO0007525	Feb 2000	WO
WO0064389	Nov 2000	WO
WO0064393	Nov 2000	WO
WO0067687	Nov 2000	WO
WO0189437	Nov 2001	WO
WO0197727	Dec 2001	WO
WO0236052	May 2002	WO
WO02074052	Sep 2002	WO
WO02080811	Oct 2002	WO
WO03015659	Feb 2003	WO
WO03045290	Jun 2003	WO
WO2004054643	Jul 2004	WO
WO2004093761	Nov 2004	WO
WO2005105197	Nov 2005	WO
WO2006066103	Jun 2006	WO
WO2007035356	Mar 2007	WO
WO2007047744	Apr 2007	WO
WO2007087061	Aug 2007	WO
WO2008002377	Jan 2008	WO
WO2008005873	Jan 2008	WO
WO2009120960	Oct 2009	WO
2010093945	Aug 2010	WO
2010135369	Nov 2010	WO
WO2011053512	May 2011	WO
WO2011057283	May 2011	WO
WO2011106781	Sep 2011	WO
WO2011150045	Dec 2011	WO
WO2012051575	Apr 2012	WO
2012071476	May 2012	WO
WO2012083143	Jun 2012	WO
2012158910	Nov 2012	WO
2013040079	Mar 2013	WO
2013074681	May 2013	WO
2013148275	Oct 2013	WO
WO2013147978	Oct 2013	WO
2013074681	Nov 2013	WO
2014011813	Jan 2014	WO
2014150292	Sep 2014	WO
2014151070	Sep 2014	WO
2014164569	Oct 2014	WO
2015073571	May 2015	WO
2015085251	Jun 2015	WO
WO-2015085251	Jun 2015	WO
2015108970	Jul 2015	WO
WO2016154066	Sep 2016	WO
2016159999	Oct 2016	WO
WO2017030902	Feb 2017	WO
WO2017030917	Feb 2017	WO
WO2017062347	Apr 2017	WO
WO2017087713	May 2017	WO
2017106517	Jun 2017	WO
WO2017095825	Jun 2017	WO
WO-2017106517	Jun 2017	WO
WO2017132418	Aug 2017	WO
WO2017132647	Aug 2017	WO
WO2017156530	Sep 2017	WO
WO2019106803	Jun 2019	WO

Non-Patent Literature Citations (43)

Entry
Bahler, et al.; Trabecular bypass stents decrease intraocular pressure in cultured human anterior segments; Amer. Journal of Ophthalmology; vol. 138, No. 6; pp. 988-994.e2; Dec. 2004.
Cambridge Dictionary; Sensor (definition); 2 pages; retrived from the internet (http://dictionary.cambridge.org/define.asp?dict=CALD&key=71811 >) on Aug. 14, 2018.
Camras et al.; A novel schlemm's canal scaffold increases outflow facility in a human anterior segment perfusion model; Invest. Opthalmol. Vis. Sci. ; 53(10); pp. 6115-6121; Sep. 1, 2012.
D'Ermo, et al.; Our results with the operation of ab externo trabeculotomy; Ophthalmologica; vol. 163; pp. 347-355; Feb. 1971.
Dietlein et al.; Morphological variability of the trabecular meshwork in glaucoma patients: implications for non-perforating glaucoma surgery: British Journal of Ophthalmology; 84(12); pp. 1354-1359; Dec. 2000.
Ellingsen et al.; Trabeculotomy and sinusotomy in enucleated human eyes; Investigative Ophthalmology; vol. 11; pp. 21-28; Jan. 1972.
Grant; Experimental aqueous perfusion in enucleated human eyes; Archives of Ophthalmology; vol. 69; pp. 783-801; Jun. 1963.
Gulati et al; A novel 8-mm schlemm's canal scaffold reduces outflow resistance in a human anterior segment perfusion model; Invest. Ophthalmol. Vis. Sci.; 54(3); pp. 1698-1704; Mar. 5, 2013.
Hays et al.; Improvement in outflow facility by two novel microinvasive glaucoma surgery implants; Invest. Ophthalmol. Vis. Sci.; 55(3); pp. 1893-1900; Mar. 1, 2014.
Huang et al.; Optical coherence tomography; Science; 254(5035); pp. 1178-1181; 12 pages (Author Manuscript); Nov. 1991.
Johnstone et al.; “Microsurgery of Schlemm's Canal and the Human Aqueous Outflow System;” American Journal of Ophthalmology, vol. 76 (6): 906-917; Dec. 1973.
Johnstone et al.; Effects of a schlemm canal scaffold on collector channel ostia in human anterior segments; Exp. Eye. Res.; 119; pp. 70-76; Feb. 2014.
Johnstone; Aqueous humor outflow system overview; Becker-Shaffer's Diagnosis and Therapy of the Glaucomas; Part 2 Aqueous Humor Dynamics; Chapter 3; pp. 25-46; Mosby Elseveir; (year of pub. sufficiently earlier than effective US filing date and any foreign priority date) 2009.
Kirkness et al.; The Use of Silicone Drainage Tubing to Control Post-Keratoplasty Glaucoma; Eye; 2 (pt 5); pp. 583-590; Apr. 1988.
Lee et al.; Aqueous-venous shunt and intraocular pressure. Preliminary report of animal studies; Investigative Ophthalmology; vol. 5; No. 1; pp. 59-64; Feb. 1966.
Lee et al.; Short-pulsed neodymium-YAG laser trabeculotomy. An in vivo morphological study in the human eye; Investigative Ophthalmology and Visual Science; 29(11); pp. 1698-1707; Nov. 1988.
Lynch, Mary G.; U.S. Appl. No. 60/131,030 entitled “Devices and methods for treating glaucoma by enhancing aqueous outflow through schlemm's canal and anterior chamber angle,” filed Apr. 26, 1999.
Macmilla Online Dictionary; Detector (definition); Macmilla on Line Dictionary; 2 pages; retrived from the internet (https://www.macmillandictionary.com/dictionary/british/detector) on Aug. 14, 2018.
Mäepea et al.; The pressures in the episcleral veins, schlemm's canal and the trabecular meshwork in monkeys: effects of changes in intraocular pressure; Exp. Eye Res.; vol. 49; pp. 645-663; Oct. 1989.
Molteno et al.; Long Tube Implants in the Management of Glaucoma; SA Medical Journal; 26; pp. 1062-1066; Jun. 1976.
Molteno; New implant for drainage in glaucoma; Brit. J. Ophthal; 53; pp. 606-615; Sep. 1969.
Moses, Robert; The effect of intraocular pressure on resistance to outflow; Survey of Ophthalmology; vol. 22; No. 2; pp. 88-100; Sep.-Oct. 1977.
Nakamura et al.; Femtosecond laser photodisruption of primate trabecular meshwork; an ex vivo study; Investigative Ophthalmology and Visual Science; 50(3); pp. 1198-1204; Mar. 2009.
Owen; A moving-mirror gonioscope for retinal surgery; British Journal of Ophthalmology; 61(3); pp. 246-247; Mar. 1977.
Oxford Dictionaries; Detector (definition); 1 page; retrieved from the internet (https://en.oxforddictionaries.com/definition/detector) on Aug. 14, 2018.
Oxford Dictionaries; Sensor (definition); 1 page; retrieved from te internet (http://www.askoxford.com/concise_oed/sensor?view=uk>) on Aug. 14, 2018.
Radhakrishnan et al.; Real-time optical coherence tomography of the anterior segment at 1310 nm; Archives of Opthhalmology; 119(8); pp. 1179-1185; Aug. 2001.
Rosenquist et al.; Outflow resistance of enucleated human eyes at two different perfusion pressures and different extents of trabeculotomy; Current Eye Res.; vol. 8; No. 12; pp. 1233-1240; Dec. 1989.
Savage, James; Gonioscopy in the management of glaucoma; Am. Academy of Ophthalmology; Focal Points; vol. XXIV; No. 3; pp. 1-14; Mar. 2006.
Schocket et al.; Anterior Chamber Tube Shunt to an Encircling Band in the Treatment of Neovascular Glaucoma and other Refractory Glaucomas; Ophthalmology; 92; pp. 553-562; Apr. 1985.
Schultz, Jared; Canaloplasty procedure shows promise for open-angle glaucoma in European study; Ocular Surgery News; vol. 34; Mar. 1, 2007.
Smit et al.; Effects of viscoelastic injection into schlemm's canal in primate and human eyes; J. Am. Academy of Ophthalmology; vol. 109; No. 4; pp. 786-792; Apr. 2002.
Spiegel et al.; Schlemm's canal implant: a new method to lower intraocular pressure in patients with POAG?; Ophthalmic Surgery and Lasers; vol. 30; No. 6; pp. 492-494; Jun. 1999.
Sugiyama et al.; Micro-Diaphragm Pressure Sensor; 1986 International Electron Devices Meeting; pp. 184-187; Dec. 7, 1986.
Toyran et al.; Femtosecond laser photodisruption of human trabecular meshwork: an in vitro study; Experimental Eye Research; 81(3); pp. 298-305; Sep. 2005.
Wilcox et al.; Hypothesis for Improving Accessory Filtration by Using Geometry; Journal of Glaucoma; 3; pp. 244-247; Fall 1994.
Yuan et al.; Mathematical modeling of outflow facility increase with trabecular meshwork bypass and schlemm canal dilation; J. Glaucoma; 10 pgs.; Mar. 24, 2015 (Epub ahead of print).
Lazarus et al.; Farrofluid-based stretchable magnetic core inductors; In Journal of Physics: Conference Series; 660(1); Jan. 2007; 5 pages; retrieved from the internet (https://iopscience.iop.org/article/10.1088/1742-6596/660/1/012007/pdf) on Oct. 27, 2020.
Wardle et al.; U.S. Appl. No. 17/548,212 entitled “Single operator device for delivering an ocular implant,” filed Dec. 10, 2021.
Noda et al.; U.S. Appl. No. 17/572,064 entitled “Systems and methods for viscoelastic delivery,” filed Jan. 10, 2022.
Lee, “Aqueous-Venous Shunt and Intraocular Pressure,” Investigative Opthalmology, vol. 5, No. 1, pp. 59-64, Feb. 1966. Accessed on Nov. 9, 2020.
Spiegel et al; “Schlemm's Canal Implant: A New Method to Lower Intraocular Pressure in Patients with POAG?” Ophthalmic Surgery and Lasers Imaging Retina, vol. 30 (6), pp. 492-494. Jun. 1999, Accessed on Nov. 9, 2020.
International Preliminary Report on Patentability, dated Sep. 3, 2020 for International Application PCT/US2019/018559.

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	Number	Date	Country
	20210030590 A1	Feb 2021	US

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	Number	Date	Country
	62633823	Feb 2018	US

Ocular implant and delivery system

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