Contact lens drug depot

Abstract

A method includes placing a contact lens over a cornea of an eye. The contact lens includes a central convex disc, a peripheral curved portion that extends radially from the disc, an annular groove formed in the disc on the posterior portion, and one or more apertures formed in the groove. A drug substance is placed over the anterior portion of the contact lens. The groove is in contact with the cornea and is a depot for the drug substance. The groove is in fluid connection with the anterior portion of the lens via the one or more apertures. The drug substance moves in an undiluted manner to the groove and the contact lens holds the drug substance in contact with the cornea, unaffected by blinking or tear exchange, facilitating enhanced bioavailability to the cornea of the drug substance.

Claims

1. A method comprising: placing a contact lens over a cornea of an eye, said contact lens having a posterior portion in contact with the cornea and an anterior portion facing an external environment which is external to the eye, and wherein said contact lens comprises a central convex disc, a peripheral curved portion that extends radially from said disc, an annular groove formed in said disc on said posterior portion, and one or more apertures formed in said groove; and placing a drug substance over the anterior portion of said contact lens, wherein said groove on said posterior portion that is in contact with the cornea is a depot for the drug substance, said groove being in fluid connection with said anterior portion via said one or more apertures, such that the drug substance moves to said groove which is in contact with the cornea and said contact lens holds the drug substance in contact with the cornea, without detrimental effects from blinking or tear exchange, facilitating enhanced bioavailability to the cornea of the drug substance.

2. The method according to claim 1, wherein said drug substance comprises a hypertonic solution.

3. The method according to claim 1, further comprising using said lens to provide increased contact time of said drug substance with the eye.

4. The method according to claim 1, further comprising using said lens to treat recurrent corneal erosion syndrome (RCE).

5. The method according to claim 1, further comprising using said lens to treat dry eye syndrome.

6. The method according to claim 1, further comprising using said lens to treat uveitis.

7. The method according to claim 1, further comprising using said lens to treat an allergy.

8. The method according to claim 1, further comprising using said lens in a corneal collagen cross-linking procedure, for intra-operative use or reducing procedure time.

9. The method according to claim 1, wherein an inner surface of said groove contacts the cornea.

Description

BRIEF DESCRIPTION OF THE DRAWINGS

(1) The present invention will be understood and appreciated more fully from the following detailed description taken in conjunction with the drawings in which:

(2) FIG. 1 is a simplified front view illustration of a contact lens, constructed and operative in accordance with an embodiment of the present invention.

(3) FIG. 2 is a cross sectional view of the contact lens.

(4) FIG. 3 is an enlarged cross-section of a hole and annular groove of the lens.

(5) FIG. 4 is a simplified side view of the contact lens mounted on an eye, in accordance with an embodiment of the present invention.

(6) FIG. 5 is a simplified side view of a contact lens mounted on an eye, in accordance with another embodiment of the present invention.

DETAILED DESCRIPTION OF EMBODIMENTS

(7) Reference is now made to FIG. 1, which illustrates a contact lens 10, constructed and operative in accordance with an embodiment of the present invention.

(8) Contact lens 10 includes a central convex disc 12 from which radially extends a peripheral curved portion 14. Central convex disc 12 and peripheral curved portion 14 can have the same curvature or different curvatures. An annular groove 16 is formed at the interior (i.e., posterior side) junction of disc 12 and peripheral curved portion 14. In an alternative embodiment, annular groove 16 may be radially inwards of this junction. In another alternative embodiment, annular groove 16 may be radially outwards of this junction. One or more apertures (through holes) 18 may be formed in groove 16. In an alternative embodiment, the one or more apertures 18 may be radially inwards of annular groove 16. In another alternative embodiment, the one or more apertures 18 may be radially outwards of annular groove 16. In one embodiment, there are 6 apertures 18; in another embodiment there are 8 apertures 18, but the invention is not limited to these numbers.

(9) Central convex disc 12 is made of a material that is oxygen permeable and dimensionally stable for use as a contact lens. A preferred example is G4X p-GMA/HEMA (hioxifilcon D), with water content in the range of approximately 50-75%, commercially available from Benz Research & Development, Sarasota, Fla., US. The invention is not limited to this material and other suitable soft or hard materials may be used (e.g., GP PMMA—gas permeable polymethylmethacrylate). For example, the lens may be made of CONTAFLEX GM, commercially available from Contamac Ltd., UK, which is a highly water retentive terpolymer based on glycerol methacrylate.

(10) In one embodiment, the inner volume of lens 10, preferably that of central convex disc 12, defines a reservoir 20 (which may be a hyper-osmotic chamber, but in some embodiments is not hyper-osmotic) (seen in FIG. 2) for supporting therein a substance 22 (FIG. 4), which may be a hyper-osmotic transparent medium such as, but not limited to, dry hydrogel, etc., or solution such as, but not limited to, glycerol, salt solution, etc., or non-hyper-osmotic substances, and which may include antibiotics, steroids and other medicinal substances. Substance 22 may also have suitable refraction and transparency properties, which may be selected for modifying vision of a patient.

(11) If substance 22 is hyper-osmotic, substance 22 creates a molecular concentration gradient and thus osmotic pressure gradient between the cornea and hyper-osmotic chamber 20. The osmotic pressure gradient results in a net flow of fluid from the cornea directly into hyper-osmotic chamber 20 by osmosis, thus dehydrating the cornea. Lens 10 can be constructed to reach a steady state net fluid flow or not to reach steady state.

(12) Lens 10 has a suitable volume to enable functioning for a sufficient duration until it is full. Accordingly, contact lens 10 may be used for daily treatment, partial daily treatment or overnight treatment, or any other treatment period which is needed for the patient treatment when it is mounted upon a cornea in an edematous state. Contact lens 10 may be sized to fit over the cornea to the limbus, or alternatively may extend over the limbus.

(13) In another embodiment, chamber 20 is not filled with any substance 22, but instead simply fits over the cornea or cornea and limbus or beyond the limbus. It has been found that the chamber 20 defined by central convex disc 12, even when initially empty (that is, devoid of a hyper-osmotic substance, but, for example, containing air), can create an osmotic pressure gradient that results in a net flow of fluid from the cornea directly into hyper-osmotic chamber 20 by osmosis, thus dehydrating the cornea. A tear film is created, due to the osmotic pressure gradient, between the lens 10 and the cornea. Due to the groove 16 and apertures 18, the tear film creates a surface tension underneath the lens 10 which is relatively trapped and slow to escape. (The apertures 18 are small so the drops do not flow past them but instead are trapped due to surface tension). The entrapped salty tear film increases the hyper-osmotic pressure, which synergistically increases dehydration of the cornea. The structure of the apertures and lens is such that any liquid drop that placed on the exterior surface of the lens will be drawn through the relatively unidirectional apertures 18 to the interior of the lens. Thus, the lens serves as a trap for fluids, such as a hypertonic solution or any other drug.

(14) Optionally, the lens 10 can be heavier at its bottom portion, which may increase the stability of the lens against any torsional movement and maintain the lens in place.

(15) Reference is now made to FIGS. 2 and 4. Non-limiting, exemplary values of lens dimensions are now described.

(16) In one embodiment of the invention, the parameters are as follows:

(17) A overall lens diameter (including peripheral curved portion 14)=11.50 mm

(18) D diameter of aperture 18=0.5 mm

(19) B reservoir diameter (diameter of hyper-osmotic chamber 20)=7.50 mm

(20) C thickness of annular groove 16=0.40 mm

(21) CT center thickness=0.4 mm (see FIG. 3)

(22) RP peripheral eye radius

(23) RB reservoir radius is 0.3 mm steeper than central eye flat meridian

(24) RD radius (curvature) of central convex disc 12=8.60 mm

(25) RCP radius (curvature) of peripheral curved portion 14=8.60 mm

(26) In another embodiment of the invention, the parameters are as follows:

(27) A overall lens diameter (including peripheral curved portion 14)=15.00 mm

(28) D diameter of aperture 18=1.50 mm

(29) B reservoir diameter (diameter of hyper-osmotic chamber 20)=9.50 mm

(30) C thickness of annular groove 16=0.40 mm

(31) CT center thickness=0.25 mm

(32) RP peripheral eye radius

(33) RB reservoir radius is 0.3 mm steeper than central eye flat meridian

(34) RD radius (curvature) of central convex disc 12=7.80 mm

(35) RCP radius (curvature) of peripheral curved portion 14=9.60 mm

(36) In still another embodiment of the invention, the parameters are as follows:

(37) A overall lens diameter (including peripheral curved portion 14)=14.00 mm

(38) D diameter of aperture 18=0.5 mm

(39) B reservoir diameter (diameter of hyper-osmotic chamber 20)=9.50 mm

(40) C thickness of annular groove 16=0.40 mm

(41) CT center thickness=0.4 mm

(42) RP peripheral eye radius

(43) RB reservoir radius is 0.3 mm steeper than central eye flat meridian

(44) RD radius (curvature) of central convex disc 12=8.60 mm

(45) RCP radius (curvature) of peripheral curved portion 14=8.60 mm

(46) In yet another embodiment of the invention, the parameters are as follows:

(47) A overall lens diameter (including peripheral curved portion 14)=11.00 mm

(48) D diameter of aperture 18=0.5 mm

(49) B reservoir diameter (diameter of hyper-osmotic chamber 20)=7.50 mm

(50) C thickness of annular groove 16=0.30 mm

(51) CT center thickness=0.4 mm

(52) RP peripheral eye radius

(53) RB reservoir radius is 0.3 mm steeper than central eye flat meridian

(54) RD radius (curvature) of central convex disc 12=8.60 mm

(55) RCP radius (curvature) of peripheral curved portion 14=8.80 mm

(56) It is noted that in the first and fourth examples, the lens basically covers just the cornea, whereas in the second and third embodiments the lens extends to the limbus and beyond.

(57) As shown in broken lines in FIG. 1, as another option one or more arcuate grooves 40 may be formed at least partially in the spherical longitudinal direction across the inner surface of central convex disc 12. Grooves 40 may extend from apertures 18.

(58) Reference is now made to FIG. 5, which illustrates a contact lens 50, constructed and operative in accordance with another embodiment of the present invention.

(59) Contact lens 50 includes an anterior lens 52 that is mounted over a posterior lens 54, which in turn is mounted on the cornea C of the eye. A tear film 55 may be present between posterior lens 54 and the cornea. Without limitation, anterior lens 52 and posterior lens 54 may be made of G4X p-GMA/HEMA (hioxifilcon D), respectively with 73% and 54% water content; they may be made alternatively of CONTAFLEX GM. Dimensions of anterior lens 52 may be similar to the first above example, whereas posterior lens 54 may be similar to the second above example. The invention is not limited to these values.

(60) The hyper-osmotic contact lens described above is a contact lens that creates a cavity above the center of the cornea. Without limitation, the cavity volume is estimated at ˜10 μl and is generally at a height between 0-200 μm above the corneal surface. This cavity can store substances, such as but not limited to, hypertonic drops, for a long duration and by doing so extracts fluids by osmosis from the cornea.

(61) In one application, the contact lens of the invention is used as a drug depot to enable the drug, regardless of its chemistry, to remain in contact with the cornea as long as possible to enhance the bioavailability of the drug. In order to enhance the bioavailability the drug needs to remain relatively static, unaffected by the blink and at full concentration for as long as possible. The contact lens 10 serves as a drug depot by means of the groove 16 or 40 on the inner portion of the lens which is in contact with the corneal surface and act as a “lake” or depot for the drug. The groove 16 or 40 is connected to the anterior portion of contact lens 10, which is in contact with the external environment through fenestration 18 (aperture 18) which acts as another channel allowing for fluids placed on the anterior surface of the lens 10 to move in a relatively undiluted manner to the posterior surface groove 16 or 40 which is in contact with the anterior corneal surface. Contact lens 10 holds the drug in contact with the cornea, relatively unaffected by the blink or tear exchange, facilitating enhanced bioavailability to the cornea and allowing for greater concentrations of the drug to be in contact with the corneal surface for longer periods of time.

(62) The contact lens can be used in a variety of applications. The lens provides increased contact time of the medication (any drug substance) with the eye in order to maximize the treatment effect. For example, the lens may be used to treat corneal infections, uveitis, dry eye, allergic conjunctivitis and any other condition requiring the medication to be in contact for a longer period of time than a topical drop. The contact lens can also be used in a corneal collagen cross-linking procedure, for intra-operative use to enhance the procedure by holding riboflavin in place on the corneal surface rather than the current technique requiring continuous application of drops to the cornea for approximately 20 minutes.