The human eye comprises several layers. The white outer layer is the sclera, which surrounds the choroid layer. The retina is interior to the choroid layer. The sclera contains collagen and elastic fiber, providing protection to the choroid and retina. The choroid layer includes vasculature providing oxygen and nourishment to the retina. The retina comprises light sensitive tissue, including rods and cones. The macula is located at the center of the retina at the back of the eye, generally centered on an axis passing through the centers of the lens and cornea of the eye (i.e., the optic axis). The macula provides central vision, particularly through cone cells.
Macular degeneration is a medical condition that affects the macula, such that people suffering from macular degeneration may experience lost or degraded central vision while retaining some degree of peripheral vision. Macular degeneration may be caused by various factors such as age (also known as “AMD”) and genetics. Macular degeneration may occur in a “dry” (nonexudative) form, where cellular debris known as drusen accumulates between the retina and the choroid, resulting in an area of geographic atrophy. Macular degeneration may also occur in a “wet” (exudative) form, where blood vessels grow up from the choroid behind the retina. Even though people having macular degeneration may retain some degree of peripheral vision, the loss of central vision may have a significant negative impact on the quality of life. Moreover, the quality of the remaining peripheral vision may be degraded and in some cases may disappear as well. It may therefore be desirable to provide treatment for macular degeneration in order to prevent or reverse the loss of vision caused by macular degeneration. In some cases it may be desirable to provide such treatment in a highly localized fashion, such as by delivering a therapeutic substance in the subretinal layer (under the neurosensory layer of the retina and above the retinal pigment epithelium) directly adjacent to the area of geographic atrophy, near the macula. However, since the macula is at the back of the eye and underneath the delicate layer of the retina, it may be difficult to access the macula in a practical fashion.
While a variety of surgical methods and instruments have been made and used to treat an eye, it is believed that no one prior to the inventors has made or used the invention described in the appended claims.
While the specification concludes with claims which particularly point out and distinctly claim this technology, it is believed this technology will be better understood from the following description of certain examples taken in conjunction with the accompanying drawings, in which like reference numerals identify the same elements and in which:
The drawings are not intended to be limiting in any way, and it is contemplated that various embodiments of the technology may be carried out in a variety of other ways, including those not necessarily depicted in the drawings. The accompanying drawings incorporated in and forming a part of the specification illustrate several aspects of the present technology, and together with the description serve to explain the principles of the technology; it being understood, however, that this technology is not limited to the precise arrangements shown.
The following description of certain examples of the technology should not be used to limit its scope. Other examples, features, aspects, embodiments, and advantages of the technology will become apparent to those skilled in the art from the following description, which is by way of illustration, one of the best modes contemplated for carrying out the technology. As will be realized, the technology described herein is capable of other different and obvious aspects, all without departing from the technology. Accordingly, the drawings and descriptions should be regarded as illustrative in nature and not restrictive.
It is further understood that any one or more of the teachings, expressions, embodiments, examples, etc. described herein may be combined with any one or more of the other teachings, expressions, embodiments, examples, etc. that are described herein. The following-described teachings, expressions, embodiments, examples, etc. should therefore not be viewed in isolation relative to each other. Various suitable ways in which the teachings herein may be combined will be readily apparent to those of ordinary skill in the art in view of the teachings herein. Such modifications and variations are intended to be included within the scope of the claims.
For clarity of disclosure, the terms “proximal” and “distal” are defined herein relative to a surgeon or other operator grasping a surgical instrument having a distal surgical end effector. The term “proximal” refers the position of an element closer to the surgeon or other operator and the term “distal” refers to the position of an element closer to the surgical end effector of the surgical instrument and further away from the surgeon or other operator.
In the present example, cannula (50) comprises a flexible material such as Polyether block amide (PEBA), which may be manufactured under the trade name PEBAX. Of course, any other suitable material or combination of materials may be used. Also in the present example, cannula (50) has a cross-sectional profile dimension of approximately 2.0 mm by 0.8 mm, with a length of approximately 80 mm. Alternatively, any other suitable dimensions may be used. As will be described in greater detail below, cannula (50) is flexible enough to conform to specific structures and contours of the patient's eye, yet cannula (50) has sufficient column strength to permit advancement of cannula (50) between the sclera and choroid of patient's eye without buckling. By way of example only, cannula (50) may be configured and operable in accordance with at least some of the teachings of U.S. Pub. No. 2015/0223977, entitled “Method and Apparatus for Subretinal Administration of Therapeutic Agent,” published Aug. 13, 2015, the disclosure of which is incorporated by reference herein.
As can be seen in
As best seen in
Needle (100) of the present example has a sharp distal tip (102) and defines a lumen (104). Distal tip (102) of the present example has a lancet configuration. In some other versions, distal tip (102) has a tri-bevel configuration or any other configuration as described in U.S. Pub. No. 2015/0223977, entitled “Method and Apparatus for Subretinal Administration of Therapeutic Agent,” published Aug. 13, 2015, the disclosure of which is incorporated by reference herein. Still other suitable forms that distal tip (102) may take will be apparent to those of ordinary skill in the art in view of the teachings herein. Needle (100) of the present example comprises a stainless steel hypodermic needle that is sized to deliver the therapeutic agent while being small enough to minimize incidental trauma as needle (100) penetrates tissue structures of the patient's eye, as will be described in greater detail below. While stainless steel is used in the present example, it should be understood that any other suitable material(s) may be used, including but not limited to nitinol, etc.
By way of example only, needle (100) may be 35 gauge with a 100 μm inner diameter, although other suitable sizes may be used. For instance, the outer diameter of needle (100) may fall within the range of 27 gauge to 45 gauge; or more particularly within the range of 30 gauge to 42 gauge; or more particularly within the range of 32 gauge to 39 gauge. As another merely illustrative example, the inner diameter of needle (100) may fall within the range of approximately 50 μm to approximately 200 μm; or more particularly within the range of approximately 50 μm to approximately 150 μm; or more particularly within the range of approximately 75 μm to approximately 125 μm.
Needle (100) is slidably disposed within lumen (64) of needle guide (60). Needle guide (60) is generally configured to direct needle (100) upwardly along an exit axis (EA) that is obliquely oriented relative to the longitudinal axis (LA) of cannula (50) through lateral opening (56) of cannula (50). This is shown in the sequence depicted in
It should be understood that the depiction of exit axis (EA) in
As shown in
In the present example, knob (26) is rotatable through a complete range of motion that corresponds to advancement of needle (100) to a position relative to cannula (50) to a predetermined amount of penetration within an eye of a patient. In other words, instrument (10) is configured such that an operator rotates knob (26) until knob (26) can no longer rotate, or until knob (26) begins to slip or “freewheel” in a clutch assembly, to properly position needle (100) within an eye of a patient. In some examples, the predetermined amount of advancement of needle (100) relative to cannula (50) is between approximately 0.25 mm to approximately 10 mm; or more particularly within the range of approximately 0.1 mm to approximately 10 mm; or more particularly within the range of approximately 2 mm to approximately 6 mm; or more particularly to approximately 4 mm.
In addition or in the alternative, instrument (10) may be equipped with certain tactile feedback features to indicate to an operator when needle (100) has been advanced to certain predetermined distances relative to cannula (50). Accordingly, an operator may determine the desired depth of penetration of needle (100) into a patient's eye based on direct visualization of indicia on instrument and/or based on tactile feedback from instrument (10). Of course, such tactile feedback features may be combined with the present example, as will be apparent to those of ordinary skill in the art in view of the teachings herein.
As also shown in
It should be understood that the features and operability of instrument (10) may be varied in numerous ways. By way of example only, needle (100) may be replaced with needle (200) as described in greater detail below. In addition, cannula (50) may be replaced with cannula (400) as will be described in greater detail below. In addition, instrument (10) may be modified in accordance with at least some of the teachings of U.S. Pub. No. 2015/0223977, entitled “Method and Apparatus for Subretinal Administration of Therapeutic Agent,” published Aug. 13, 2015, the disclosure of which is incorporated by reference herein; U.S. Pub. No. 2015/0351958, entitled “Therapeutic Agent Delivery Device with Convergent Lumen,” published Dec. 10, 2015, the disclosure of which is incorporated by reference herein; U.S. Pub. No. 2015/0351959, entitled “Sub-Retinal Tangential Needle Catheter Guide and Introducer,” published Dec. 10, 2015, the disclosure of which is incorporated by reference herein; U.S. Pub. No. 2016/0074212, entitled “Method and Apparatus for Sensing Position Between Layers of an Eye,” published Mar. 17, 2016, the disclosure of which is incorporated by reference herein; U.S. Pub. No. 2016/0074217, entitled “Motorized Suprachoroidal Injection of Therapeutic Agent,” published Mar. 17, 2016, the disclosure of which is incorporated by reference herein; U.S. Pub. No. 2016/0074211, entitled “Therapeutic Agent Delivery Device with Advanceable Cannula and Needle,” published Mar. 17, 2016, the disclosure of which is incorporated by reference herein; and/or U.S. Pub. No. 2016/0081849, entitled “Therapeutic Agent Delivery Device,” published Mar. 24, 2016, the disclosure of which is incorporated by reference herein. Other suitable modifications will be apparent to those of ordinary skill in the art in view of the teachings herein.
In the present example, the procedure begins by an operator immobilizing tissue surrounding a patient's eye (301) (e.g., the eyelids) using a speculum, and/or any other instrument suitable for immobilization. While immobilization described herein with reference to tissue surrounding eye (301), it should be understood that eye (301) itself may remain free to move. Once the tissue surrounding eye (301) has been immobilized, an eye chandelier port (314) is inserted into eye (301), as shown in
In the present example, only chandelier port (314) is inserted at the stage shown in
Once eye chandelier port (314) has been positioned, the sclera (304) may be accessed by dissecting the conjunctiva by incising a flap in the conjunctiva and pulling the flap posteriorly. After such a dissection is completed, the exposed surface (305) of the sclera (304) may optionally be blanched using a cautery tool to minimize bleeding. Once conjunctiva dissection is complete, the exposed surface (305) of the sclera (304) may optionally be dried using a WECK-CEL or other suitable absorbent device. A template may then be used to mark eye (301), as described in U.S. Pub. No. 2015/0223977, entitled “Method and Apparatus for Subretinal Administration of Therapeutic Agent,” published Aug. 13, 2015, the disclosure of which is incorporated by reference herein. An operator may then use a visual guide created using the template to attach a suture loop assembly (332) and to perform a sclerotomy, as shown in
With the sclerotomy procedure performed, an operator may insert cannula (50) of instrument (10) through incision (316) and into the space between sclera (304) and choroid (306). As can be seen in
Although not shown, it should be understood that in some examples cannula (50) may include one or more markers on the surface of cannula (50) to indicate various depths of insertion. While merely optional, such markers may be desirable to aid an operator in identifying the proper depth of insertion as cannula (50) is guided along an atraumatic path. For instance, the operator may visually observe the position of such markers in relation to suture loop assembly (332) and/or in relation to the incision in the sclera (304) as an indication of the depth to which cannula (50) is inserted in eye (301). By way of example only, one such marker may correspond to an approximately 6 mm depth of insertion of cannula (50).
As shown in
Once cannula (50) has been advanced to the delivery site as shown in
In the present example, after the operator has confirmed that needle (100) has been properly advanced by visualizing the tenting effect described above, the operator infuses a balanced salt solution (BSS) or other similar solution as needle (100) is advanced relative to cannula (50). Such a BSS may form a leading bleb (340) ahead of needle (100) as needle (100) is advanced through choroid (306). Leading bleb (340) may be desirable for two reasons. First, as shown in
Once the operator visualizes leading bleb (340), the operator may cease infusion of BSS, leaving a pocket of fluid as can be seen in
In the present example, the amount of therapeutic agent (341) that is ultimately delivered to the delivery site is approximately 50 μL, although any other suitable amount may be delivered. In some versions, a foot pedal is actuated in order to drive agent (341) out from needle (100). Alternatively, other suitable features that may be used to drive agent (341) out from needle (100) will be apparent to those of ordinary skill in the art in view of the teachings herein. Delivery of therapeutic agent (341) may be visualized by an expansion of the pocket of fluid as can be seen in
Once delivery is complete, needle (100) may be retracted by rotating knob (26) in a direction opposite to that used to advance needle (100); and cannula (50) may then be withdrawn from eye (301). It should be understood that because of the size of needle (100), the site where needle (100) penetrated through choroid (306) is self sealing, such that no further steps need be taken to seal the delivery site through choroid (306). Suture loop assembly (332) and chandelier (314) may be removed, and the incision in the sclera (304) may be closed using any suitable conventional techniques.
As noted above, the foregoing procedure may be carried out to treat a patient having macular degeneration. In some such instances, the therapeutic agent (341) that is delivered by needle (100) may comprise cells that are derived from postpartum umbilicus and placenta. As noted above, and by way of example only, the therapeutic agent (341) may be provided in accordance with at least some of the teachings of U.S. Pat. No. 7,413,734, entitled “Treatment of Retinitis Pigmentosa with Human Umbilical Cord Cells,” issued Aug. 19, 2008, the disclosure of which is incorporated by reference herein. Alternatively, needle (100) may be used to deliver any other suitable substance or substances, in addition to or in lieu of those described in U.S. Pat. No. 7,413,734 and/or elsewhere herein. By way of example only, therapeutic agent (341) may comprise various kinds of drugs including but not limited to small molecules, large molecules, cells, and/or gene therapies. It should also be understood that macular degeneration is just one merely illustrative example of a condition that may be treated through the procedure described herein. Other biological conditions that may be addressed using the instruments and procedures described herein will be apparent to those of ordinary skill in the art.
It should also be understood that the procedure described above may be carried out in accordance with any of the teachings of U.S. Pub. No. 2015/0223977, entitled “Method and Apparatus for Subretinal Administration of Therapeutic Agent,” published Aug. 13, 2015, the disclosure of which is incorporated by reference herein; U.S. Pub. No. 2015/0351958, entitled “Therapeutic Agent Delivery Device with Convergent Lumen,” published Dec. 10, 2015, the disclosure of which is incorporated by reference herein; U.S. Pub. No. 2015/0351959, entitled “Sub-Retinal Tangential Needle Catheter Guide and Introducer,” published Dec. 10, 2015, the disclosure of which is incorporated by reference herein; U.S. Pub. No. 2016/0074212, entitled “Method and Apparatus for Sensing Position Between Layers of an Eye,” published Mar. 17, 2016, the disclosure of which is incorporated by reference herein; U.S. Pub. No. 2016/0074217, entitled “Motorized Suprachoroidal Injection of Therapeutic Agent,” published Mar. 17, 2016, the disclosure of which is incorporated by reference herein; U.S. Pub. No. 2016/0074211, entitled “Therapeutic Agent Delivery Device with Advanceable Cannula and Needle,” published Mar. 17, 2016, the disclosure of which is incorporated by reference herein; and/or U.S. Pub. No. 2016/0081849, entitled “Therapeutic Agent Delivery Device,” published Mar. 24, 2016, the disclosure of which is incorporated by reference herein.
Several variables may affect the relationship between the exit angle (EA) of needle (100) and the choroid (306) of any given patient. It should be understood that the choroid (306) and the retina (308) are very thin and have relatively little structural integrity. Thus, even when a very flexible cannula (50) is used, cannula (50) may tend to provide substantial separation between the choroid (306) and the sclera (304) as cannula (50) is inserted between the choroid (306) and the sclera (304). The degree of separation may vary from patient to patient (e.g., based on normal anatomical variation and/or based on the patient's disease state, etc.). In cases where the separation is truly substantial, the exit angle (EA) of needle (100) may be insufficient to result in distal tip (102) passing fully through the choroid (306). In other words, needle (100) may continue through the suprachoroidal space without fully penetrating the choroid (306).
If the operator determines (e.g., based on the absence of a choroidal “tenting” observation as described above) that needle (100) has not fully penetrated the choroid (306) despite needle (100) being advanced fully distally, the operator may retract needle (100) proximally, slightly reposition cannula (50) and/or another portion of instrument (10) in order to provide a better orientation for the exit angle (EA), and then try advancing needle (100) distally again. Even with such efforts, it may still be very difficult or even impossible in some cases to successfully penetrate the choroid (306) with needle (100). Even in cases where efforts to reposition are successful, the success rate may be highly dependent on the skill of the operator, and the repositioning efforts will add time to the procedure. Moreover, the repositioning may increase the risk of tissue trauma, increase the risk of bleb collapse, and/or increase the risk of cell egress into the suprachoroidal space.
It may seem apparent to address the above-noted issues by simply modifying needle guide (60) to provide a steeper exit angle (EA). However, this kind of modification may be unsuitable for many patients. In particular, increasing the exit angle (EA) by providing a more pronounced bend in distal end (62) of needle guide (60) may increase the risk of needle (100) perforating the retina (308) in some patients, particularly in those where the gap (305) created by cannula (50) between the sclera (304) and the choroid (306) is less pronounced than the gap (305) shown in
Needle (200) is configured to provide bent portion (214) as a preformed feature, such that needle (200) is resiliently biased to assume the configuration shown in
While the radius of curvature of bent portion (214) is constant in the present example, in some other versions the radius of curvature may be variable. For instance, some variations of needle (200) may provide a larger radius of curvature in a region of needle (200) that remains disposed in cannula (50), even when needle (200) is in a distally extended position; with a smaller radius of curvature in a region of needle (200) that extends distally from cannula (50) when needle (200) is in a distally extended position. This kind of configuration may impart a slight precurvature to cannula (50), which may further assist in cannula (50) conforming to the curved inner wall of sclera (304), which may in turn reduce the occurrence (or magnitude) of gap (305).
As shown in
As the operator continues to advance needle (200) distally relative to cannula (50), more of needle (200) protrudes distally from lateral opening (56), as shown in
As shown in
As noted above, the exit angle (EA) of needle (200) varies based on the extent to which needle (200) is extended from cannula (50). It should be understood that this variation in the exit angle (EA) will allow the operator to control the optimal exit angle (EA) by controlling the amount of needle (200) extension. This may allow for shallower angles (less extension) for some patients and steeper angles (more extension) for other patients, to more consistently be able to achieve penetration of the choroid (306) in a relatively safe and efficient manner, eliminating the need for other mitigations or workarounds that would otherwise be required from the scenario depicted in
As noted above, cannula (50) includes a closed distal end (54) and a lateral opening (56) that is located proximal to distal end (54). In some instances, it may be desirable to provide an alternative cannula that has an open distal end, without a lateral opening. By way of example only, this may provide simplified manufacturing processes. Since it may still be desirable to have a needle exit the cannula at such that the distal tip of the needle is oriented along an axis that is oblique to the longitudinal axis of the cannula, it may be desirable to use a needle with a preformed curve in versions where the cannula has an open distal end.
An insert (408) is positioned within cannula (400). Insert (408) may be secured within cannula (400) by a press or interference fit, by adhesives, by mechanical locking mechanisms, and/or in any other suitable fashion. In the present example, insert (408) is formed of a polyimide material, though it should be understood that any other suitable biocompatible material(s) may be used. Insert (408) of the present example is substantially straight yet may bend with cannula (400). Needle (200) is slidably disposed in a lumen (410) defined by insert (408). When needle (200) is in a proximal position as shown in
The following examples relate to various non-exhaustive ways in which the teachings herein may be combined or applied. It should be understood that the following examples are not intended to restrict the coverage of any claims that may be presented at any time in this application or in subsequent filings of this application. No disclaimer is intended. The following examples are being provided for nothing more than merely illustrative purposes. It is contemplated that the various teachings herein may be arranged and applied in numerous other ways. It is also contemplated that some variations may omit certain features referred to in the below examples. Therefore, none of the aspects or features referred to below should be deemed critical unless otherwise explicitly indicated as such at a later date by the inventors or by a successor in interest to the inventors. If any claims are presented in this application or in subsequent filings related to this application that include additional features beyond those referred to below, those additional features shall not be presumed to have been added for any reason relating to patentability.
An apparatus, comprising: (a) a body; (b) a cannula extending distally from the body, wherein the cannula is flexible; and (c) a needle slidably disposed in the cannula, wherein the needle includes: (i) a sharp distal tip, wherein the needle is configured to translate relative to the cannula between a proximal position and a distal position, wherein the distal tip is configured to be positioned inside the cannula when the needle is in the proximal position, wherein the distal tip is configured to be positioned outside the cannula when the needle is in the distal position, and (ii) a curved portion, wherein the needle is resiliently biased to extend along a curve through the curved portion.
The apparatus of Example 1, wherein the cannula includes: (i) a closed distal end, and (ii) a lateral opening located proximal to the closed distal end.
The apparatus of Example 2, wherein the cannula further includes a ramp feature, wherein the ramp feature extends from an interior region of the cannula to the lateral opening.
The apparatus of any one or more of Examples 1 through 3, wherein the curved portion is resiliently biased to define a constant radius of curvature.
The apparatus of Example 4, wherein the radius of curvature is between approximately 7 mm and approximately 12 mm.
The apparatus of Example 4, wherein the radius of curvature is between approximately 4 mm and approximately 15 mm.
The apparatus of Example 4, wherein the radius of curvature is between approximately 9 mm and approximately 10 mm.
The apparatus of any one or more of Examples 1 through 7, wherein the curved portion is configured to position the distal tip at a progressively increasing exit angle relative to a longitudinal axis of the cannula, based on a distance to which the needle is advanced distally relative to the cannula.
The apparatus of any one or more of Examples 1 through 8, wherein the curved portion comprises a first curved region and a second curved region, wherein the first curved region is located near a distal portion of the needle, wherein the second curved region is located proximal to the first curved region.
The apparatus of Example 9, wherein the first curved region has a first radius of curvature, wherein the second curved region has a second radius of curvature, wherein the second radius of curvature is greater than the first radius of curvature.
The apparatus of any one or more of Examples 9 through 10, wherein the first curved region is configured to not impart a curvature to the cannula, wherein the second curved region is configured to impart a curvature to the cannula.
The apparatus of any one or more of Examples 1 through 11, wherein the needle further includes a straight proximal portion and a straight distal portion, wherein the curved portion is longitudinally positioned between the straight proximal portion and the straight distal portion.
The apparatus of any one or more of Examples 1 through 12, wherein the cannula defines an open distal end.
The apparatus of Example 13, wherein the needle is configured to protrude from the open distal end of the cannula when the needle is in the distal position.
The apparatus of any one or more of Examples 1 through 14, further comprising a source of liquid therapeutic agent, wherein the needle is operable to deliver the liquid therapeutic agent.
The apparatus of Example 15, wherein the body includes: (i) a needle actuator, wherein the actuator is operable to drive the needle longitudinally relative to the cannula, and (ii) a valve member, wherein the valve member is operable to selectively provide fluid communication from the source of liquid therapeutic agent to the needle.
An apparatus, comprising: (a) a body; (b) a cannula extending distally from the body, wherein the cannula is flexible, wherein the cannula includes: (i) a closed distal end, and (ii) a lateral opening located proximal to the closed distal end; and (c) a needle slidably disposed in the cannula, wherein the needle includes: (i) a sharp distal tip, wherein the needle is configured to translate relative to the cannula between a proximal position and a distal position, wherein the distal tip is configured to be positioned inside the cannula when the needle is in the proximal position, wherein the distal tip is configured extend past the lateral opening when the needle is in the distal position, and (ii) a curved portion, wherein the curved portion is configured to provide an oblique exit angle to a portion of the needle extending past the lateral opening when the needle is in the distal position.
The apparatus of Example 17, wherein the curved portion is resiliently biased to assume a curved configuration, wherein the curved portion is further configured to deform to a substantially straight configuration within the cannula when the needle is in the proximal position.
A method of administering a therapeutic agent to an eye of a patient, wherein the eye includes a sclera, a choroid, and a retina, the method comprising: (a) inserting a flexible cannula between the sclera and the choroid; (b) advancing a needle relative to the cannula, thereby penetrating the choroid with a distal tip of the needle, wherein the needle includes a preformed curve, wherein the curve guides the needle toward a targeted region of the choroid; and (c) administering the therapeutic agent to a region between the choroid and the retina via the needle.
The method of Example 19, wherein the act of advancing the needle includes: (i) advancing the needle to a first longitudinal position relative to the cannula, wherein the needle defines a first exit angle relative to the cannula at the first longitudinal position, and (ii) advancing the needle further distally to a second longitudinal position relative to the cannula, wherein the needle defines a second exit angle relative to the cannula at the second longitudinal position, wherein the second exit angle is greater than the first exit angle.
It should be understood that any of the versions of the instruments described herein may include various other features in addition to or in lieu of those described above. By way of example only, any of the devices herein may also include one or more of the various features disclosed in any of the various references that are incorporated by reference herein.
It should be understood that any one or more of the teachings, expressions, embodiments, examples, etc. described herein may be combined with any one or more of the other teachings, expressions, embodiments, examples, etc. that are described herein. The above-described teachings, expressions, embodiments, examples, etc. should therefore not be viewed in isolation relative to each other. Various suitable ways in which the teachings herein may be combined will be readily apparent to those of ordinary skill in the art in view of the teachings herein. Such modifications and variations are intended to be included within the scope of the claims.
It should be appreciated that any patent, publication, or other disclosure material, in whole or in part, that is said to be incorporated by reference herein is incorporated herein only to the extent that the incorporated material does not conflict with existing definitions, statements, or other disclosure material set forth in this disclosure. As such, and to the extent necessary, the disclosure as explicitly set forth herein supersedes any conflicting material incorporated herein by reference. Any material, or portion thereof, that is said to be incorporated by reference herein, but which conflicts with existing definitions, statements, or other disclosure material set forth herein will only be incorporated to the extent that no conflict arises between that incorporated material and the existing disclosure material.
Versions described above may be designed to be disposed of after a single use, or they can be designed to be used multiple times. Versions may, in either or both cases, be reconditioned for reuse after at least one use. Reconditioning may include any combination of the steps of disassembly of the device, followed by cleaning or replacement of particular pieces, and subsequent reassembly. In particular, some versions of the device may be disassembled, and any number of the particular pieces or parts of the device may be selectively replaced or removed in any combination. Upon cleaning and/or replacement of particular parts, some versions of the device may be reassembled for subsequent use either at a reconditioning facility, or by an operator immediately prior to a procedure. Those skilled in the art will appreciate that reconditioning of a device may utilize a variety of techniques for disassembly, cleaning/replacement, and reassembly. Use of such techniques, and the resulting reconditioned device, are all within the scope of the present application.
By way of example only, versions described herein may be sterilized before and/or after a procedure. In one sterilization technique, the device is placed in a closed and sealed container, such as a plastic or TYVEK bag. The container and device may then be placed in a field of radiation that can penetrate the container, such as gamma radiation, x-rays, or high-energy electrons. The radiation may kill bacteria on the device and in the container. The sterilized device may then be stored in the sterile container for later use. A device may also be sterilized using any other technique known in the art, including but not limited to beta or gamma radiation, ethylene oxide, or steam.
Having shown and described various embodiments of the present invention, further adaptations of the methods and systems described herein may be accomplished by appropriate modifications by one of ordinary skill in the art without departing from the scope of the present invention. Several of such potential modifications have been mentioned, and others will be apparent to those skilled in the art. For instance, the examples, embodiments, geometrics, materials, dimensions, ratios, steps, and the like discussed above are illustrative and are not required. Accordingly, the scope of the present invention should be considered in terms of the following claims and is understood not to be limited to the details of structure and operation shown and described in the specification and drawings.
This application is a divisional of U.S. Non-Provisional patent application Ser. No. 15/438,918, entitled “Apparatus for Subretinal Administration of Therapeutic Agent via a Curved Needle,” filed Feb. 22, 2017, issued as U.S. Pat. No. 10,478,553 on Nov. 19, 2019; which claims priority to U.S. Provisional Patent Application No. 62/305,767, entitled “Curved Needle Choroidal Penetration,” filed Mar. 9, 2016, the disclosure of which is incorporated by reference herein.
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Number | Date | Country | |
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20200078514 A1 | Mar 2020 | US |
Number | Date | Country | |
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Number | Date | Country | |
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Parent | 15438918 | Feb 2017 | US |
Child | 16599206 | US |