AU765034B2 - Method and apparatus for performing surgery inside the human retina using fluidic internal limiting membrane (ILM) separation (films) - Google Patents
Method and apparatus for performing surgery inside the human retina using fluidic internal limiting membrane (ILM) separation (films) Download PDFInfo
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- AU765034B2 AU765034B2 AU26122/02A AU2612202A AU765034B2 AU 765034 B2 AU765034 B2 AU 765034B2 AU 26122/02 A AU26122/02 A AU 26122/02A AU 2612202 A AU2612202 A AU 2612202A AU 765034 B2 AU765034 B2 AU 765034B2
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S&FRef: 535684D1
AUSTRALIA
PATENTS ACT 1990 COMPLETE SPECIFICATION FOR A STANDARD PATENT
ORIGINAL
Name and Address of Applicant: Actual Inventor(s): Address for Service: Invention Title: Robert E. Morris 3204 Argyle Road Birmingham Alabama 35213 United States of America Robert E. Morris Spruson Ferguson St Martins Tower,Level 31 Market Street Sydney NSW 2000 (CCN 3710000177) Method and Apparatus for Performing Surgery Inside the Human Retina Using Fluidic Internal Limiting Membrane (ILM) Separation (Films) The following statement is a full description of this invention, including the best method of performing it known to me/us:- IPAustraia Docurm,:- on i 8 MAR 200z Z -o:i 5845c
DESCRIPTION
Method And Apparatus For Performing Surgery Inside The Human Retina Using Fluidic Internal Limiting Membrane (Ilm) Separation (Films) Background Of The Invention 1. Field Of The Invention The present invention is directed generally to a device to be used in medical procedures and, more particularly to a device to be used in a medical procedure for removal of the innermost layer of the human retina (internal limiting membrane) from the underlying neural retina at the center of vision (macula).
2. Background Art The rays of light entering the eye (FIG. 1) and bearing the pattern of the object being looked upon pass through the 15 cornea 32, the aqueous humor, the pupil, the lens 34, and the vitreous humor, then fall upon the retina 26. The retina is the light sensitive film lining the back twothirds of the eye. Its appearance is similar to that of wet tissue paper. Its layers consist of the internal limiting membrane (ILM), the neurosensory retina, and the retinal pigment epithelium; the ILM, being innermost, is the retinal border with the vitreous gel cavity 42. If the parts of the eye are normal and the lens is properly adjusted, the image will be focused upon the retina. This condition results in 25 clear vision. At the back of the eye or, more specifically, the back part of the retina is the macula lutea 36 having at its center the fovea centralis. The macula is a small orange-yellow, oval area (about 3 mm by 5 mm) of the retina adjacent to the optic nerve 38. Vision in which the image of the object looked upon falls upon the macula is the sharpest vision and is called macular vision or central vision, as opposed to gross, peripheral vision.
A wrinkling of the internal limiting membrane and the neural retina is called macular pucker. This can cause loss of fine vision to the level of legal blindness. The wrinkling is caused by contractile cells or fibrocellular membranes (epimacular proliferation or EMP) and is usually a process associated with aging.
Macular distortion and macular edema, with resultant macular dysfunction, are recognized sequelae of EMP. Often, the macula will have a "wrinkled cellophane" appearance.
According to one theory, this appearance represents internal limiting membrane (ILM) distortion by surface proliferative cells without a distinct epimacular proliferative membrane overlying the ILM, which might be surgically removed. This ILM cellophaning may persist or occur months after seemingly 15 successful removal of EMP, limiting visual recovery.
Specimens analyzed after vitrectomy (the surgical removal of a portion of the vitreous body and/or associated epiretinal or fibrous membranes) using a microscope for epimacular membrane removal often contain retinal ILM 20 fragments that have been intentionally or unintentionally removed to treat "traction maculopathy," a term introduced by Morris, Kuhn, Witherspoon, ("Retinal folds and hemorrhagic macular cysts in Terson's syndrome," Ophthalmology (1994) 101:1). Written reports differ on whether the presence of ILM fragments correlate with the visual outcome. (Trese, M. et al., "Macular pucker Ultrastructure," Graefe's Arch Clin Exp phthamol. (1983) 221:16-26; De Bustros, S. et al., "Vitrectomy for Macular Pucker: Use after treatment of retinal tears or retinal detachment," Arch Ophthalmol. (1988) 106:758-760; Sivalingam, A. et al., "Visual prognosis correlated with the presence of internal limiting membrane in histophathologic specimens obtained from epiretinal membrane surgery," Ophthalmology. (1990) 97:1549-1552). More recently, William Hutton and others have implicated even relatively small amounts of traction as exacerbating diabetic macular edema.
Additionally, Logan Brooks and Tom Rice have advocated the intentional removal of the macular ILM in macular hole surgery. (Brooks, "ILM peeling in full thickness macular hole surgery," Vitreoretinal Surgery and Technology.
(1995) 7:2; Rice, "Technique of removal of the inner retinal surface in macular hole surgery," Retina Society 2 8 t h Annual Meeting. Santa Fe, New Mexico, 1995). A macular hole is thought to occur as a result of tangential traction on the retina at the macula, usually leading to legal blindness Thus, there are many advocates of the importance of ILM removal in macular hole surgery. Previous methods as shown in FIG.2, developed over a period of about twenty years, have removed the macular ILM 54 and EMP 50 utilizing the manual, mechanical method with grasping forceps 52. This 15 forceps procedure is the most delicate surgical maneuver performed on the human body. The procedure requires ideal surgical conditions and expert skill. Ideally, cataracts and any other opacity obscuring surgical view will have been eliminated for safe and predictable EMP/ILM removal.
S 20 Electron microscopy of surgical specimens frequently demonstrates cellular proliferation contracting the ILM. It is believed that the increased mobility of an ILM denuded macula contributes to successful hole closure.
Furthermore, the results with ILM maculorhexis in macular hole surgery were encouraging. In a consecutive series of 32 idiopathic holes with less than two years duration, a 97% closure was achieved. Previous macular hole edges were rarely discernible. Visual acuity improved at least two Snellen lines in 91% of eyes, and 41% of eyes achieved 20/40 or better visual acuity at the last follow-up (Morris, Witherspoon, "Internal Limiting Membrane Maculorhexis for Traction Maculopathy," Vitreoretinal Surgery and Technology (1997) All of the above-described conditions may be considered forms of traction maculopathy as first described by Morris et al. The ultimate goal of all surgery to cure traction maculopathy is to return the neural retina to its normally smooth contour, allowing resumption of fine vision and relief from distorted vision.
In a very rare disease called Terson's syndrome, blood under pressure from a ruptured vein or capillary spontaneously lifts the ILM, resulting in what is called a hemorrhagic macular cyst (HMC) (Morris, Kuhn, F., Witherspoon, American Academy of Opthalmology, 1990).
The hemorrhage usually then breaks through the ILM into the vitreous. Vitreous and subinternal limiting membrane hemorrhage occurs as a result of abrupt intracranial hemorrhage from an aneurysm or closed head trauma. Although the exact mechanism for these hemorrhages is unknown, it is thought that the sudden increased intracranial pressure is 15 transmitted via the optic nerve to retinal venules and capillaries, rupturing them. If bleeding has occurred at the macula, it will appear as a circular or boat shaped cyst (HMC) on the surface of the retina. The HMC is usually encircling the macula. Its diameter and height vary, as does its color, depending on the longevity of the hemorrhage. Early intervention for amblyopia prevention in infants) finds a reddish cyst. A few months after the incident, the surgeon encounters a yellow lesion (degenerated blood products), a clear membrane spanning an optically empty cavity, or a collapsed membrane. A perimacular fold may form along the edge of the separation of the ILM from the neurosensory retina at the cyst margin.
Sub ILM hemorrhagic macular cysts are almost pathognomic to Terson's syndrome. Fourteen cases of retinal folds from shaken baby syndrome or consequent to direct head trauma were analyzed from various literature reports, each had intracranial hemorrhage and various forms of intraocular hemorrhage, including HMC. The HMC's occur not only in traumatically induced cases of Terson's syndrome but also in patients with spontaneous subarachnoid hemorrhage.
Accordingly, it has been proposed that intracranial hemorrhage, from whatever source, is the common denominator in the formation of both HMC's and their accompanying perimacular folds.
In the series originally presented at the Annual Meeting of the American Academy of Ophthalmology in 1990, it was found that of 25 eyes undergoing vitrectomy for Terson's syndrome, 8 demonstrated HMC's (Morris, Kuhn, F., Witherspoon, "Hemorrhagic Macular Cysts in Terson's Syndrome and its Implications for Macular Surgery," Developments in Opthalmology (1997) 29:44). After careful clinical examinations and light or electron microscopic evaluations, it was concluded that the ILM had formed the anterior cyst wall in five eyes. While several literature reports have characterized these hemorrhagic lesions as 15 being subvitreous or under a proliferative membrane, it is believed by Morris et al. (see above) that the majority of .i hemorrhagic macular cysts in Terson's syndrome are in fact submembranous (beneath the ILM) rather than subvitreous (preretinal).
S 20 Although rare, submembranous HMC's in Terson's syndrome are the most frequent lesion in which the macular ILM is spontaneously lifted from the underlying neurosensory retina as a result of a disease process. Thus, it was postulated that if the denuded macula retains good function without reparative surface proliferation developing, similar nontraumatic surgical removal of the ILM during vitrectomy in certain cases of traction maculopathy might be endorsed.
(Morris, Kuhn, Witherspoon, "Retinal folds and hemorrhagic macular cysts in Terson's syndrome," Ophthalmology (1994) 101:1). For example, in none of the five Terson's eyes in a series evaluated by the inventor and colleagues did reparative proliferation develop during an average follow up of 32 months (range: 6-70 months), and all adult eyes reached and maintained excellent 20/25 visual acuity.
Therefore, the desirability of developing procedures for the atraumatic surgical removal of the macular ILM in certain forms of traction maculopathy was suggested.
("Hemorrhagic Macular Cysts in Terson's Syndrome and its Implications for Macular Surgery," Developments in Ophthalmology (1997) 29:44). Even minimal ILM surface traction has been increasingly implicated in many forms of maculopathy and often the EMP/ILM layers become, in effect, fused together, not allowing surgical removal of EMP alone.
Additionally, long-term macular function appears to be stable or improved even without the ILM. ("Hemorrhagic Macular Cysts in Terson's Syndrome and its Implications for :i Macular Surgery," Developments in Ophthalmology (1997) 29:44). Thus, ILM removal is an important technique in the 15 treatment of all forms of traction maculopathy because only the removal of the ILM with all cellular and membrane proliferation on its surface ensures total relief from all traction on the underlying nerve fibers at the center of vision. However, the methods thus far developed for such 20 ILM removal have certain deficiencies. The method of mechanical pulling tearing away the macular ILM with forceps can cause severe trauma to the macula and the resultant injury can cause ocular damage of equal severity to the problem the surgery is meant to correct.
The current method employed for removal of both EMP and the macular ILM consists of cutting and then grasping, or directly grasping, the macular EMP/ILM with specially designed micro-forceps, 1 mm in maximum diameter, and slowly pulling it apart from the neural retina. This is done with great care in order to avoid engaging the neurosensory retina.
One problem with the current method of tearing and peeling away the macular ILM is the physical trauma associated with pulling on the ILM until it separates thereby unavoidably stressing the underlying nerve tissue, sometimes causing irreparable nerve damage with worsened vision than may have been present preoperatively.
Accordingly, the surgeon may proceed slowly and carefully but if too slowly the retina may be injured from light toxicity coming from the fiberoptic probe inside the eyeball enabling the surgeon's view. If the surgeon grasps too shallow then his movements are ineffectual, adding to the time of surgery and the chance of light toxicity. If the surgeon grasps too deep, permanent nerve damage and hemorrhage results. The difference is usually a matter of microns of forceps movement, causing the surgeon's mindset to be what has justly been described as "nerve-wracking." The mass of the forceps, although ever so small, often obscures the surgeon's view, further adding to the chance of surgical damage to the retina. As a result of the above 15 factors, complete traction release is the exception rather than the rule. Finally, even in the unusual case of complete tractibn release, the nerve tissue will usually require several months to resume a smooth contour with best vision returning. Thus, for some twenty years, the removal S 20 of epimacular proliferation so as to restore central vision in the eyes that are approaching legal blindness has remained a vexing problem for vitreoretinal surgeons worldwide. The potential surgical risks and the uncertain benefits, as well as the high level of skill required to perform such surgery has caused many surgeons to be reluctant to intervene until vision is substantially lost.
This has been true, despite the knowledge that persistence of EMP causes permanent destruction of nerve function at the center of vision, such that visual acuity is only partially restorable, and progressively less so, as the EMP is allowed to persist.
Solutions have been diligently sought over this twentyyear period, including progressively smaller and finer forceps. Finally, as an illustration of surgeons' frustration, in 1997, a new concept was introduced by Tano to surgically rub or scrape the surface of the retina at or near the macula with a flexible, rubber instrument upon which has been glued innumerable diamond chips so as to allow the device to purchase a hold on these barely visible membranes and/or ILM. This device was introduced and has been substantially used, despite the obvious risk of damage to the neural retina which underlays these thin membranes by rubbing or scraping the retinal surface with an intentionally roughened instrument, as well as the risk of diamond chips dislodging and permanently remaining on the retinal surface within the eye. These risks have been tolerated in the more or less desperate search for effective remedies for traction maculopathy because the device adds an additional means to gain a surgical edge against the all too frequent need to conclude the operation before achieving complete release of traction.
Wang US Patent No. 5,066,276, described injecting viscous material into the eye using a standard glue injector. Wang, however, did not apply this surgical procedure within the retina itself. Rather, Wang described injecting the viscous material between a 15 glia cell membrae and a retina. Wang described his procedure as one in which the ee S•pressure applied to the retina is very diffuse and not localized in one small are is order to reduce stresses on the retina.
There remains a need for improved methods for removal of both epimacular proliferations and the abnormal ILM of the retina to completely relieve all forms of traction maculopathy in which the ILM is contributory. Such a method must be based upon minimizing surgical traction on the underlying nerve tissue at the center of vision .i (fovea).
Object of the Invention It is an object of the present invention to substantially overcome or at least ameliorate one or more of the disadvantages of the prior art, or at least to provide a useful alternative.
[R:\LIBD]02866.doc:JMT Summary of the Invention The present invention provides an apparatus to be used in performing surgery inside the human retina using fluidic internal limiting membrane separation comprising: a hollow microcannula having a distal end, a proximal end, a central longitudinal axis, and a distal tip, said microcannula being shaped at its distal end to conform tangentially to the surface to the retina near the macula when inserted through an eyeball entrance site at the pars plana, and adapted to discharge a fluid substance from the distal tip of the microcannula to effectuate separation of the retinal internal limiting membrane at or near the macula from the neural retinal layer.
wherein said microcannula has an outside diameter of approximately 800 microns at its proximal end and an outside diameter of approximately 100 microns at its distal end, and is thus sufficiently microscopic as to not substantially injure the neural retina when introduced under said internal limiting membrane, wherein said distal end of said microcannula has a continuous curvature designed :to conform tangentially to the surface of the retina near the macula when inserted through an eyeball entrance site at the pars plana, wherein said tip of said microcannula is beveled and sharpened to allow optimal penetration of the internal limiting membrane and optical occlusion of the lumen by the overlying internal limiting membrane upon minimal insertion, and wherein the distal most end of said tip is located on the outer curve of said microcannula having the largest radius.
The preferred embodiment(s) provides a novel method for performing surgery inside the human retina using fluidic ILM.
9 o *o~o [R:\LIBD]02866.doc:JMT:caa separation (FILMS) and simultaneous retinal smoothing to overcome the disadvantages of the previously known methods.
Briefly, the preferred embodiment is directed to a device for separating the ILM layer of the retina from the neural layer of the retina in order to remove the macular internal limiting membrane and all EMP on its surface. The device has a hollow microcannula, considerably smaller than any such cannula heretofore, which is shaped at its distal end to conform tangentially to the surface of the retina, between the retinal ILM and the neural retina.
After the microcannula is inserted, a sterile fluid is injected at a pressure of about 25 mm Hg through the microcannula between the ILM layer of the retina and the neural layer of the retina. The fluid pressure lifts the macular internal limiting membrane layer away from the neural layer of the retina, separating it in the process of lifting away and allowing for its easy forceps removal from the eye without inflicting any physical trauma upon the neural retina. The lifted macular internal limiting 20 membrane is removed by grasping the free-floating macular internal limiting membrane with forceps and extending the macular internal limiting membrane separation as distant from the fovea as desired before tearing Circumferentially about the fovea and removing from the eye. The present invention allows for the removal of the macular internal 6* limiting membrane without mechanically peeling or tearing it away from the fovea, so as to minimize foveal traction and the resultant physical trauma to the fovea. Moreover, the present invention simultaneously actively smoothes the 30 underlying distorted and wrinkled neural retina by an intentional build-up of localized pressure within the confines of the developing FILMS cyst of which it is the posterior border. Thus, visual recovery, the ultimate surgical goal, is substantially accelerated as compared to the months needed for passive, spontaneous retinal smoothing after forceps traction removal. The preferred substance for use in practicing the invention and achieving complete removal of the macular internal limiting membrane is sodium hyaluronate (Healon®), as manufactured by Pharmacia Upjohn Inc. or chondroitin sodium hyaluronate (Viscoat®) as manufactured by Alcon, Inc.
The preferred embodiment allows surgeons to operate, for the first time, inside the human retina (intraretinal) rather than above its surface. In so doing, it enables the surgeon to gently, predictably, and rapidly remove the ILM and all EMP adhered to the neural retina. The device eliminates risk of mechanical traction from pulling on the nerve fibers. The use of the device takes typically 4 minutes as opposed to 15 mintures, substantially reducing the risk of light toxicity. The device allows for a more certain benefit from the surgery. Moreover, the device affords a significant decrease in the surgical skill level needed to treat traction maculopathy and makes visual recovery more rapid, more certain, and more complete. The sum effect is to enable patients suffering visual loss due to traction maculopathy of any type to seek and find earlier and more certain relief from distorted and reduced visual acuity, while the associated neural retinal abnormality is still reversible.
Brief Description of the Drawings e A preferred form of the present invention will now be described by way of 20 example with reference to the accompanying drawings, wherein: i FIG. 3 is a representation of the microcannula apparatus to [R:\LIBD]03505.doc:caa be used to perform fluidic ILM separation (FILMS). FIG. 4 is the interior of the posterior half of the left eye as viewed through an ophthalmoscope. The area of most acute vision, the macula, is shown with the fovea centralis at its center. FIG. 5 is a cross-sectional view of the eye undergoing a macular FILMS procedure in accordance with the method of the present invention.
Detailed Description Of The Preferred Embodiments Definitions S 10 "Maculorhexis" is the removal of the macular internal limiting membrane (ILM) by the production of a circular, 3600 ILM tear concentric with the fovea, while minimizing foveal traction. This procedure is used to relieve all forms of traction maculopathy in which the ILM is contributory, as a result of its innate inelasticity or its action as a scaffold for fibrocellular proliferation (EMP).
"Traction Maculopathy" is a pathological dysfunction of the macula partially or entirely secondary to abnormal tangential or anteroposterior forces macular hole, 20 epeimacular proliferation, vitreomacular traction syndrome, diffuse diabetic macular edema, cellophane maculopathy).
"Fluid" is a substance whose molecules move easily across one another; a liquid or a gas.
"Neural Retina" is the middle layer of the retina, 25 between the ILM and the pigment epithelial layers, which is composed of nerve tissue and which generates and transmits the electrical signals ultimately recognized as vision.
Preferred Embodiments Disclosed herein is a novel device allowing surgery within the human retina to remove the internal limiting membrane utilizing fluidic separation. With reference to FIG. 4, to begin the process of ILM removal, an optimal starting point is chosen within the arcade vessels but remote from the fovea. Additionally, the chosen starting point site should not overlie the papillomacular bundle.
Furthermore, the starting point is selected on the basis of the appearance of the ILM, and for surgical convenience. In a preferred embodiment, referring to FIG. 3, the specially designed hollow microcannula (microcannula and fluid injector) has a proximal end 18 and a distal end 12. The microcannula has an outside diameter of approximately 800 microns (0.8 mm) at its proximal end 18 stepwise tapering to an outside diameter of approximately 100 microns (0.1 mm) at its distal end 12. The microcannula is shaped at its distal end 12 to conform tangentially 10 to the surface of the retina 26. The microcannula is beveled at the distal tip 14 to promote an effective entry through the macular ILM retinal layer 22 (FIG. 5) at the surface of the retina 26 15 and is adapted at the distal tip 14 to discharge a substance which is contained in a reservoir 16 attached to the microcannula of FIG. 3. The point of insertion 28 of the microcannula is at the surface of the retina 26 and through the macular ILM retinal layer 22. A sterile substance 20 stored in the reservoir 16 attached to the microcannula is injected at a pressure of about 25 mm Hg through the microcannula so as to discharge from the distal tip 14 beneath the macular ILM 22 within the retinal tissue. The actual injection pressure is selected by the surgeon immediately prior to microcannula introduction into the eye, so that said injection pressure moves the injectate fluid through said FILMS microcannula at the desired rate of flow for effective but non-traumatic cleavage between the ILM and neural layers of the retina. The substance 20 then cleaves the human retina by lifting the macular ILM 22 away from the neural retina, allowing for its subsequent forceps removal without inflicting any physical trauma upon the neural retina due to adhesion of the macular ILM 22 to the surface of the neural retina. The separated macular ILM 22 is removed by grasping said macular ILM 22 with forceps and extending its separation by gentle traction beyond the macula, then tearing said macular ILM 22 in a circular, 3600 fashion concentric with the fovea.
The preferred substance 20 to discharge from the distal tip of the microcannula 14 and achieve complete fluidic separation of the macular ILM 22 from the neural retina is a thick clear fluid such as sodium hyaluronate (Healon®) or chondroitin sodium hyaluronate (Viscoat®). These are preferred because their thickness helps form the FILMS cyst, lifting the macular ILM 22 and simultaneously smoothing the neural retina without detrimental leakage at the FILMS microcannula insertion site. Furthermore, sodium hyaluronate creates a clear field of vision thereby facilitating intra-operative inspection of the retina.
However, it is possible that a different fluid, such as 15 sterile saline, or a gas could be used.
The free-floating raised macular ILM 22 is then grasped by forceps. When the forceps are then used to grasp the macular ILM 22 separated from the surface of the retina 26, the maneuver becomes predictable and non-traumatic because 20 there is no need to tear or peel the macular ILM 22 away from any direct adhesion to the fovea and surrounding macular surface of the retina 26, eliminating any vertical or tangential force vectors as placed upon the fovea by forceps ILM removal, substituting in its stead a very gentle and precisely controlled tamponad pressure. Then, a (smooth-edged continuous tear) "rhexis" is created by slowly tearing the ILM in a circular pattern concentric with the fovea, at a distance from the fovea as selected by the surgeon after further mechanical stripping of the ILM beyond the macular FILMS cyst. A surgeon can often create the complete 3600 rhexis in one motion. However, if the tear is incomplete, the ILM is simply regrasped at the new edge, and the rhexis is resumed.
The problem of adhesion and the necessity to tear and peel the macular ILM from the surface of the retina (fovea and macular center of vision) and the resultant physical 14 trauma impressed upon these areas is completely avoided. By injecting a fluid substance within the retina tissue, the macular ILM is separated from contact with the neura-l retina prior to grasping and removing it from the retina.
Therefore, the macular ILM is never actually torn or peeled away from the retina and there is no physical trauma caused by adhesion of the macular ILM to the neural retina because the injected fluid lifts the membrane away from the surface of the retina before it is removed using the forceps.
While embodiments and applications of this invention have been here shown and described, it would be apparent to those skilled in the art that many more modifications are possible without departing from the inventive concepts herein.
e. Examples It must be noted that as used herein the singular forms "and" and "the" include the plural references unless the context clearly 20 dictates otherwise. Thus, for example, reference to "a formulation" includes mixtures of different formulations and reference to "the method of treatment" includes reference to I equivalent steps and methods known to those skilled in the art, and so forth.
V. 25 Unless defined otherwise, all technical and scientific terms used herein have the same meaning as commonly .:-understood by one of ordinary skill in the art to which this invention belongs.
Claims (2)
1. An apparatus to be used in performing surgery inside the human retina using fluidic internal limiting membrane separation comprising: a hollow microcannula having a distal end, a proximal end, a central longitudinal axis, and a distal tip, said microcannula being shaped at its distal end to conform tangentially to the surface to the retina near the macula when inserted through an eyeball entrance site at the pars plana, and adapted to discharge a fluid substance from the distal tip of the microcannula to effectuate separation of the retinal internal limiting membrane at or near the macula from the neural retinal layer. wherein said microcannula has an outside diameter of approximately 800 microns at its proximal end and an outside diameter of approximately 100 microns at its distal end, and is thus sufficiently microscopic as to not substantially injure the neural retina when introduced under said internal limiting membrane, wherein said distal end of said microcannula has a continuous curvature designed to conform tangentially to the surface of the retina near the macula when inserted through an eyeball entrance site at the pars plana, o wherein said tip of said microcannula is beveled and sharpened to allow optimal penetration of the internal limiting membrane and optical occlusion of the lumen by the 20 overlying internal limiting membrane upon minimal insertion, and wherein the distal most end of said tip is located on the outer curve of said microcannula having the largest radius.
2. An apparatus to be used in performing surgery inside the human retina 25 using fluidic internal limiting membrane separation, said apparatus being substantially as hereinbefore described with reference to the accompanying drawings. Dated 5 June, 2003 Robert E. Morris 30 Patent Attorneys for the Applicant/Nominated Person SPRUSON FERGUSON [R:\LIBD]03505.doc:caa
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| Application Number | Priority Date | Filing Date | Title |
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| AU26122/02A AU765034B2 (en) | 1998-07-06 | 2002-03-18 | Method and apparatus for performing surgery inside the human retina using fluidic internal limiting membrane (ILM) separation (films) |
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| US09/111146 | 1998-07-06 | ||
| AU47042/99A AU747462B2 (en) | 1998-07-06 | 1999-06-21 | Method and apparatus for performing surgery inside the human retina using fluidic internal limiting membrane (ILM) separation (Films) |
| AU26122/02A AU765034B2 (en) | 1998-07-06 | 2002-03-18 | Method and apparatus for performing surgery inside the human retina using fluidic internal limiting membrane (ILM) separation (films) |
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| AU47042/99A Division AU747462B2 (en) | 1998-07-06 | 1999-06-21 | Method and apparatus for performing surgery inside the human retina using fluidic internal limiting membrane (ILM) separation (Films) |
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Citations (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| WO1992008406A1 (en) * | 1990-11-14 | 1992-05-29 | The University Of Rochester | Intraretinal delivery and withdrawal instruments |
| WO1994021205A1 (en) * | 1993-03-16 | 1994-09-29 | Photogenesis, Incorporated | Method for preparation and transplantation of volute grafts and surgical instrument therefor |
| WO1996026759A1 (en) * | 1995-02-28 | 1996-09-06 | Photogenesis, Incorporated | Method for preparation and transplantation of planar implants and surgical instruments therefor |
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Patent Citations (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| WO1992008406A1 (en) * | 1990-11-14 | 1992-05-29 | The University Of Rochester | Intraretinal delivery and withdrawal instruments |
| WO1994021205A1 (en) * | 1993-03-16 | 1994-09-29 | Photogenesis, Incorporated | Method for preparation and transplantation of volute grafts and surgical instrument therefor |
| WO1996026759A1 (en) * | 1995-02-28 | 1996-09-06 | Photogenesis, Incorporated | Method for preparation and transplantation of planar implants and surgical instruments therefor |
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