Patent Grant
9149356
This invention relates generally to an interior bag for implantation in the natural capsular bag of an eye and an injector therefor and, more particularly, to an apparatus and method for preventing the condition of posterior capsular opacification (PCO), a condition occurring in about 25 percent of cataract surgery patients, and for preventing and/or treating other conditions of the eye.
A cataract is a clouding of the lens of the eye, the lens being responsible for focusing and producing sharp images. Cataracts are the leading cause of vision loss among adults 55 and older. Eye injuries, diseases, and certain medications are believed to accelerate the formation of cataracts.
The lens is contained inside the natural capsular bag in a human eye. Alteration of the structure of the lens over time causes lens opacification or clouding, which makes images look blurred or fuzzy. This process is a natural result of aging and can be accelerated due to injury, disease or medication.
PCO can occur after cataract surgery and cause patients to experience symptoms similar to those from the original cataract. During cataract surgery, a patient's natural lens is replaced with a small artificial lens, called an intraocular lens or IOL. Unfortunately, proteins and/or cells, such as lens epithelial cells retained in the capsular bag following surgery, may proliferate and migrate to the posterior surface inside the capsular bag causing PCO, thereby making clarity of vision difficult.
In an effort to treat PCO patients, surgeons have focused on methods of treating the cells on the inside of the capsular bag. Methods used in the past have included lysing, freezing, polishing, and laser treatment. Unfortunately, some of these methods carry a higher risk of developing a retinal detachment in the future. Additionally, some of these methods may also cause the intraocular lens to dislocate and necessitate surgical repositioning and, in unfortunate cases, result in the destruction of the capsular bag. Moreover, each of these methods does not adequately limit future cell formation inside the capsular bag because aqueous humor fluid flow through the capsular bag continues to provide an environment friendly to cell growth or even cell migration into the posterior part of the bag via fluid flow causing PCO. There is a need in the art to provide a means for inhibiting PCO.
There is also a need to provide a means for retaining the shape of the capsular bag and for reducing or eliminating shrinkage of the capsular bag following cataract surgery. In addition, experiments are now underway to inject silicone or other transparent materials into the capsular bag following cataract surgery to form a replacement lens in situ rather than using a conventional IOL and the present invention may facilitate the use of such a lens. The present invention may further provide a reservoir for retaining and releasing a time release pharmaceutical agent for treatment of glaucoma or infection such as iritis or uvitis.
It is in view of the above problems that the present invention was developed. Generally, the invention is an interior bag for placement in a capsular bag of an eye and an injector for placing the interior bag within the capsular bag. The interior bag is a discriminatingly permeable (or even impermeable) interior bag that reduces aqueous humor fluid flow volume through the capsular bag to provide a less favorable growth environment for cells that cause PCO, that aids in properly positioning an intraocular lens and in maintaining a proper position, and that may aid in removing PCO cellular buildup within the capsular bag. The interior bag may further provide support for the capsular bag to prevent or reduce shrinkage and to maintain the natural shape of the capsular bag following cataract surgery, and provide a reservoir for containing the silicone or other materials used in forming an injectable lens. It may also provide a reservoir for a pharmaceutical agent to treat certain conditions of the eye.
An injector for the interior bag is used to insert the interior bag into the capsular bag. The injector is adapted to hold the interior bag and may also hold an IOL. The injector has a housing that is further adapted to hold a pressurizing fluid in a fluid containment reservoir. A plunger for ejecting a volume of fluid from the fluid containment reservoir is disposed in the housing for ejecting the interior bag with the fluid into the capsular bag of the eye.
A method for inserting an interior bag inside an injector and injecting the interior bag into a capsular bag requires first that an interior bag be inserted or placed into an opening of the housing of the injector. The housing now holds the interior bag and the fluid containment reservoir is empty. Surgical or optical fluid or gel is then placed inside the fluid containment reservoir, in some cases either before or after a refractive device such as an IOL is placed inside the reservoir. The injector is now ready to deploy the interior bag. The interior bag is ejected from the injector by moving the plunger through the reservoir to collapse and invert the interior bag, eject it through an open distal end of the reservoir and fill it with the fluid or gel. A closed system is then created inside the interior bag. Finally, the interior bag is positioned and secured inside the capsular bag.
Further features and advantages of the present invention, as well as the structure and operation of various embodiments of the present invention, are described in detail below with reference to the accompanying drawings.
The accompanying drawings, which are incorporated in and form a part of the specification, illustrate the embodiments of the present invention and together with the description, serve to explain the principles of the invention. In the drawings:
Referring to the accompanying drawings in which like reference numbers indicate like elements,
The interior bag 22 may be impermeable, semi-permeable or permeable, depending on the desired use and the circumstances of the particular case. Permeability of the interior bag is determined relative to the ability to permit aqueous humor or other fluids to pass through the wall of the interior bag. By its placement within the capsular bag 26, the interior bag 22 occupies a substantial portion of the volume of the capsular bag 26 and thereby inhibits the free flow of floating aqueous humor through the capsular bag 26. The interior bag 22 includes an irregularly contoured outer surface 30. As shown in
It is emphasized that projections 32 serve to maintain the interior bag 22 in a relatively constant position with respect to the capsular bag 26. This is a key feature of the present invention. Accordingly, the position of the refractive device 50 may be reliably maintained relative to the capsular bag 26. This eliminates the common problem of a skewed or tilted position of the refractive device 50 within the capsular bag 26 after surgery, which often necessitates another surgery to correct the position of the refractive device 50. In addition, the projections 32 (or projections 32A-32E) maintain a stable position, but as the capsular bag 26 moves, the position of the projections 32 (or projections 32A-32E) also may experience slight displacement along the wall of the capsular bag 26, at least prior to formation of fibrosis. As this occurs, the projections 32 (or projections 32A-32E) may scrub or file the interior surface 24 of the capsular bag 26 of PCO cellular buildup. After fibrosis formation, slight movement may still occur between the projections 32 to scrub the interior surface 24 of capsular bag 26.
The interior bag 22 is a thin, optically clear, biologically compatible, rounded bag (rounded to approximate the dimensions of the capsular bag 26) and is adapted to hold a refractive device 50, such as a compressible disc lens, a traditional lens with two or more haptics or a material forming an injectable lens. The interior bag 22, although being impermeable or semi-permeable to limit the flow of aqueous humor through the capsular bag 26, must be thin and optically clear in order to allow light transmission to the back of the eye 28. In addition, in order to reduce the possibility for rejection, the interior bag 22 must be made of a biologically compatible material and it must be strong enough to protect the refractive device 50 and prevent it from tearing capsular bag 26. Examples of suitable materials are silicones, hydrogels and other materials commonly used in the manufacture of IOLs and other ocular implants.
The reduction of mass flow rate of aqueous humor fluid flow through the capsular bag 26 is important as it limits the deposition of excess proteins inside the capsular bag 26, and even on a refractive device, thus reducing the probability of a patient contracting PCO. Since the interior bag 22 is discriminatingly permeable (not permitting or reducing the flow of aqueous humor through the wall of the interior bag 22), the flow of aqueous humor into the interior bag 22 is also reduced. This is a key feature of the present invention because the aqueous humor transports the cells and proteins that can deposit on the interior of the bag 22 and on refractive device 50 and reduce their light transmitting properties. The interior bag 22, however, still allows sufficient fluid flow inside the capsular bag 26 to permit the capsular bag 26 to continue to receive the nourishment it needs.
As noted, there may be several friction-fitting projections employed on the interior bag 22, for example, projections 32 (or projections 32A-32E). These may, for example, include a single or multiple rims, beads, crimps, points, etc. that extend around a portion or the entire outer periphery of interior bag 22. As such, the number of friction-fitting features used may vary, as conditions require. The only limitations to the friction fitting features is that they assist in maintaining the relative position of the interior bag 22 with respect to the capsular bag 26, and reduce or interrupt aqueous humor flow in the space between the outer surface of interior bag 22 and interior surface 24 of the capsular bag 26 to reduce or eliminate the potential for PCO.
A bridge or support structure 60, adapted to hold a refractive device 50 such as an IOL, is formed inside the interior bag 22. The IOL has haptics 51 that fit between and engage opposed surfaces of the support 60 to hold the IOL 50 securely in place inside the interior bag 22. The refractive device 50 preferably has an index of refraction greater than or equal to a natural human lens. It is understood that the bridge or support structure 60 may be any apparatus that is capable of holding the IOL and is biologically compatible to body. The support structure 60 prevents the tilting of the haptics of the IOL 50, e.g. wherein one haptic can be tilted over the equator, and the other haptic tilted under the equator. It is estimated that eighty percent (80%) of IOLs have some tilting. It is very important to note that while the preferred embodiment places the support structure 60 on the equator, the structure 60 does not have to be placed on the equator of the capsular bag 26 or on the equator of the interior bag 22. Instead, the structure 60 may be in front or in back of the equator to permit accurate adjustment of the power of the IOL based upon the distance between the IOL and the cornea. For example, while high power lenses are available, they are thick and may therefore be undesirable. By proper placement of the structure 60, high power may be achieved using thinner lenses. An estimated additional accommodation of between one and three diopters can be achieved by vitreous pressure in the posterior part of the capsular bag pushing the structure 60 (and thus the position of the refractive device 50) forward. In addition, multiple IOLs, including multifocal and piggyback lenses, could be held by one or more support structures 60 as necessary to obtain higher magnification needed for treating patients, for example, having macular degeneration. Alternatively, an optical fluid or gel may constitute the refractive device, the fluid or gel having an index of refraction of between about 1.43 to 1.46 or such other power of refraction as is necessary to provide acceptable vision. In this case, the optical fluid or gel would be injected directly into and fill the interior bag 22 and the support structure 60 would be eliminated.
Accommodation is the ability of the eye to sharply focus on both near and far objects. With a natural lens, the ciliary muscles, acting through the zonules, cause the capsular bag to flatten or elongate in the direction of the optical axis to change the focal length of the lens to sharply focus an image on the retina irrespective of the distance of the object from the eye.
Using the injector of
In order to insert the interior bag 22 into the capsular bag 26 of the human eye 28, the inside surface 54 of the interior bag 22 is pressurized by moving the plunger 46 and piston 47 from a first position to a more distal second position. Applying pressure to the interior bag 22 causes the interior bag 22 to invert and move through the opening 49 at the distal end 48 of the injector 40 and into the capsular bag 26 through an incision 29 (
The interior bag 22 enters the incision 29 in the eye 28 as it moves through the distal end 48 of the injector 40. As the interior bag 22 passes through the opening 49 at the distal end 48 of the injector 40, the interior bag inverts or turns itself inside out and orients itself inside the capsular bag 26. This is apparent when viewing
As noted, pressurizing the inside surface 54 of the interior bag causes the interior bag 22 to collapse inside the fluid containment reservoir and then invert and move through the opening end 49 at the distal end 48 of the injector 40, through the incision 29 and into the capsular bag 26. It should be noted that the volume of fluid or gel injected into the interior bag 22 should be monitored to ensure that the interior bag's volume does not exceed the volume of capsular bag 26. Filling interior bag 22 with the optical fluid or gel causes enough curvature for achieving an index of refraction as a result of the curvature of the interior bag 22, as well as the volume of optical fluid contained within interior bag 22, to obtain the desired refraction.
If a soft IOL 50 is to be implanted, the IOL is transported by the fluid or gel flow and is squeezed through opening 49 and incision 29 into the interior bag 22. As this occurs, the roll 52 remains attached to the distal end 48 of the injector 40, and the interior bag 22 and refractive device 50 are oriented by the surgeon to the position shown in
To create the closed system inside the interior bag 22, the roll 52 is unrolled. Unrolling the roll 52 allows a surgeon to have slack in the end of the roll to work with. This is important because the surgeon must next glue the ends of the roll 52 together to fully close the interior bag 22. The surgeon may, for example, use a fibrinogen and thrombin combination to make a fibrin glue. After the closed system is created, the excess of the unrolled end of the bag 22 is removed or trimmed and the interior bag is secured by positioning and friction fitting the irregularly contoured outer surface 30 of the interior bag 22 with the inside surface 24 of the capsular bag 26. The friction fit should occur naturally, as the interior bag 22 is filled and pressurized to the extent that it fits the capsular bag 26. Finally, the surgeon closes the surgical incision.
In view of the foregoing, it will be seen that the several advantages of the invention are achieved and attained.
The embodiments were chosen and described in order to best explain the principles of the invention and its practical application to thereby enable others skilled in the art to best utilize the invention in various embodiments and with various modifications as are suited to the particular use contemplated.
As various modifications could be made in the constructions and methods herein described and illustrated without departing from the scope of the invention, it is intended that all matter contained in the foregoing description or shown in the accompanying drawings shall be interpreted as illustrative rather than limiting. For example, the method of the invention is described in a series of steps described in a preferred order, but the most important aspect is not the actual order of the steps, but the end result, enabling an interior bag 22 to be forced out of injector 40 with the use of pressurizing fluid. Thus, the breadth and scope of the present invention should not be limited by any of the above-described exemplary embodiments, but should be defined only in accordance with the following claims appended hereto and their equivalents.
This application is a continuation application of U.S. Pat. No. 8,556,967, issued on Oct. 15, 2013, which may be related to U.S. patent application Ser. No. 10/307,679 filed Dec. 2, 2002, now U.S. Pat. No. 7,662,179, which was a continuation-in-part of U.S. patent application Ser. No. 09/288,560 filed Apr. 9, 1999, now U.S. Pat. No. 6,488,708, each of which is incorporated herein in its entirety.
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| Number | Date | Country | |
|---|---|---|---|
| 20140046438 A1 | Feb 2014 | US |
| Number | Date | Country | |
|---|---|---|---|
| Parent | 11653084 | Jan 2007 | US |
| Child | 14054129 | US |
