AU780010B2 - Biomedical compositions - Google Patents

Biomedical compositions Download PDF

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AU780010B2
AU780010B2 AU61404/00A AU6140400A AU780010B2 AU 780010 B2 AU780010 B2 AU 780010B2 AU 61404/00 A AU61404/00 A AU 61404/00A AU 6140400 A AU6140400 A AU 6140400A AU 780010 B2 AU780010 B2 AU 780010B2
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polymer
macromonomer
lens
macromonomers
range
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Anthony Brian Clayton
Gordon Francis Meijs
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Commonwealth Scientific and Industrial Research Organization CSIRO
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Commonwealth Scientific and Industrial Research Organization CSIRO
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Description

WO 01/08603 PCT/AU00/00915 1 BIOMEDICAL COMPOSITIONS Technical Field of the Invention This invention relates to ethylenically unsaturated macromonomers that are suitable for use as precursors for polymers in biomedical applications.
Background of the Invention The use of polymeric prostheses and biomedical mouldings has grown rapidly in recent times. Such mouldings may be used for contact lenses or for specific ophthalmic purposes. For example, they may be used for intraocular lenses and eye bandages. They may also be used for surgical mouldings such as heart valves and artificial arteries. Other applications include wound dressings, biomedical adhesives and tissue scaffolds. Use in drug delivery is a further application.
Diseases of the lens material of the eye are often in the form of cataracts.
The ideal cataract procedure is considered to be one where the lens capsule bag is maintained with the cataractous lens material removed through a small opening in the capsule. The residual lens epithelial cells are removed chemically and/or with ultrasound or lasers. A biocompatible material with appropriate optical clarity, refractive index and mechanical properties is inserted into the capsular bag to restore the qualities of the original crystalline lens. The desired refractive index is 1.41.
There have been recent advances in methods of inserting intraocular lens.
For example, US Patent number 5,772,667 assigned to Pharmacia Lovision Inc, discloses a novel intraocular lens injector. This device compresses an intraocular lens by rolling the lens into a tight spiral. The device then injects the compressed lens through a relatively small incision in the eye, approximately 2- 3 millimetres in length, resulting from a phacoemulsification procedure. The intraocular lens is inserted into a receiving channel of the injector device in an uncompressed state and is urged into a cylindrical passageway. As the intraocular lens advances into the cylindrical passageway, the lens rolls upon itself into a tightly rolled spiral within the confines of the cylindrical passageway. An insertion rod is then inserted into an open end of the cylindrical passageway and advances the compressed lens down the WO 01/08603 PCT/AU00/00915 2 passageway. As the lens exits the passageway and enters the eye, the lens will expand back to its uncompressed state.
To avoid the need for such injection devices, it has been proposed that intraocular lenses be formed in situ after being injected as a liquid flowable form into the lens capsule bag. However, while this concept is attractive in that smaller incisions would be required, it raises further difficulties in that further chemical reactions are required to cure the injectable material and these are required to be not harmful to the patient. It is also a requirement that the chemical reactions can take place over a relatively short time under mild reaction conditions. It is desirable that the reaction is also not significantly inhibited by oxygen. A still further requirement is that no by-products or residues are produced that may have an adverse biological effect on the patient.
As adults age the accommodative power of the eye decreases leading to the onset of presbyopia. This age-related decrease in accommodative power is believed to be caused by a decrease in the elasticity of the lens material. This decrease is probably caused by cross-linking of the lens material. Thus the loss of accommodation results from a change in elasticity rather than a decrease in the action of the ciliary muscles. The replacement of the original lens with a synthetic polymer having the elasticity equivalent to the lens of a young adult offers the prospect of being able to use a surgical procedure to replace the need for glasses to correct presbyopia.
US Patent No. 5,079,319 assigned to Ciba-Geigy Corporation discloses vinyl unsaturated macromonomers that are prepared via a two stage process. In the first stage of this process copolymers are prepared by addition polymerisation of ethylenically unsaturated monomers. The monomers are selected such that the polymer chain includes polysiloxane units pendant from a carbon backbone.
Ethylenic unsaturation is introduced into the copolymer in the second stage by reaction of an active hydrogen in the polymer chain with an unsaturated isocyanate.
The unsaturated macromonomer so formed may be subsequently crosslinked in a mould to form contact lenses. This invention is described as being an improvement over US Patent No. 4,605,712 which has a common assignee. The improvement is WO 01/08603 PCT/AU00/00915 3 described as being the ability to introduce higher concentrations of siloxane groups without the problems of phase-separation and opacity associated with the compositions of 4,605,712. Patent number 5,079,319 asserts that addition polymerisation in the first stage leads to more random introduction of siloxane groups and thus the avoidance of large incompatible domains.
Silicones containing pendant (meth)acrylic or (meth)acrylamide groups are particularly suitable for rapid crosslinking using radical photoinitiating systems.
US Patent No. 4,563,539 assigned to Dow Coring Corporation, discloses the synthesis of acrylofunctional siloxanes.
International Publication No. W099/47185 in the name of Pharmacia Upjohn Groningen BV proposes intraocular compositions comprising aqueous dispersions of polymerisable microgels. This application relies upon the microgel structure to obtain the rapid crosslinking required for intraocular lens procedures.
The invention of this application is distinguished from this invention as it uses oligomers and solution polymers. The citation claims that it is not possible to achieve the required balance of speed of crosslinking, refractive index and mechanical properties necessary for intraocular procedures with such polymers.
Summary Of The Invention This invention provides in one form an ethylenically unsaturated macromonomer comprising units of Formula I: Me Me Me Me I I I
I
M e -Si- -3SiO--Si Si-Me Me Me L Me
Z
where L is a linker group Z is an ethylenically unsaturated free radical polymerisable group yis 2 x is WO 01/08603 PCT/AU00/00915 4 and wherein the ethylenically unsaturated groups are provided by (meth)acrylamide moieties.
The linker group, L, functions as a spacing group which allows the required ethylenic unsaturated group Z to be attached to the copolymer backbone. It may be a linear, branched or cyclic hydro carbyl chain. It may contain hetero atoms as well as carbonyl and other substituted atoms.
In an alternative form this invention provides an ethylenically unsaturated macromonomer comprising units of Formula I wherein the molecular weight of the macromonomer is in the range 3,000 80,000, and wherein the ethylenically unsaturated groups are provided by (meth)acrylamide, (meth)acrylate and styrenic moieties.
In a further alternative form this invention provides an ethylenically unsaturated macromonomer comprising units of Formula I wherein the macromonomer has a viscosity at 25 0 C in the range 1,000 20,000 cSt, and more preferably 1,000 10,000 cSt and after polymerisation has an E modulus in the range 0.01 100 kPa, preferably 0.1 10kPa and more preferably 0.5 In an alternative embodiment this invention provides polymers for biomedical application wherein polymers are polymerised from macromonomers as defined above.
In a still further alternative form this invention provides a method of preparing intraocular lenses in situ by injecting a flowable macromonomer composition of Formula I into a lens capsule bag where: L is a linker group; Z is an ethylenically unsaturated free radical polymerisable group; yis 2 and x is 2 and wherein the macromonomer has a viscosity at 25 0 C in the range 1,000 20,000 cSt, and more preferably 1,000 10,000 cSt and polymerising the macromonomer to provide a polymer having an E modulus in the range 0.01 100 kPa, preferably 0.1 10kPa and more preferably 0.5 WO 01/08603 PCT/AU00/00915 In a further embodiment this invention provides a method of treating presbyopia by making an incision into the cornea of a patient, removing the lens material and injecting a flowable macromonomer composition of Formula I where the macromonomer has a viscosity at 25 0 C in the range 1,000 20,000 cSt, and more preferably 1,000 10,000 cSt and polymerising the macromonomer to provide a polymer having an E modulus in the range 0.01 100 kPa, preferably 0.1 10kPa and more preferably 0.5 Detailed Description Of The Invention The most effective process for producing the preferred (meth)acrylamidebased macromonomers involves the attachment of acrylamide functional groups to poly(dimethylsiloxane-co-aminoalkylsiloxane) copolymers by reaction with 2vinyl-4,4-dimethylazlactone in solution as set out below in the scheme of reaction.
However, treatment of the poly(dimethylsiloxane-co-aminoalkylsiloxane) copolymers with acryloyl chloride or other such reagents is an alternative means of synthesis.
Me Me Me- Me Me-Si--Si--S 0 -Si Me Me Me Me 2,vinyl-4,4dimethylazlactone polydimethyl-aminopropylsiloxane copolymer dichlromethane WO 01/08603 PCT/AU00/00915 6 Me Me Me Me Me- I -O- S I i
O
i-Me Me Me Me
NH
HN/r y=0 acrylamide-functionalised polydimethyl-aminopropylsiloxane copolymer The macromonomers set out in the above scheme of reaction as well as in Formula I are preferably random copolymers. However block type copolymers also fall within the scope of the present invention.
While generally the compositions of the present invention do not usually involve the use of other macromonomers, these may be optionally included. This can be an advantage when the refractive index or viscosity needs to be adjusted.
Preferably the compositions comprise at least 50%, more preferably at least by weight of macromonomers as defined in the present invention.
The macromonomers of this invention may be polymerised by free radical polymerisation to form crosslinked or cured polymers. The mechanical and optical properties of the polymers are preferably matched to those of the natural biological material. In the case of lens material for the eye the refractive index should be close to 1.41. The modulus of the polymer is measured by a Bohlin controlled stress rheometer in the range 0.01 100 kPa, preferably 0.1 10 kPa and most preferably 5kPa. The E modulus is influenced by the number of ethylenically unsaturated groups per macromonomer and also the spacing of the ethylenically unsaturated groups. Generally as the number of ethylenically unsaturated groups WO 01/08603 PCT/AU00/00915 7 per macromonomer molecule increases or the spacing between ethylenically unsaturated groups decreases the elasticity of the cured polymer decreases.
The crosslinking process is preferably carried out in such a way that the macromonomer comprising cross-linkable groups is free or essentially free from undesired constituents, in particular from monomeric, oligomeric or polymeric starting compounds used for the preparation of the cross-linkable macromonomer.
The polymer product should also be free from by-products formed during the preparation of the crosslinked polymer. The macromonomer is preferably used without the addition of a comonomer although this is allowed.
In the case of photo cross-linking, it is expedient to add an initiator which is capable of initiating free-radical crosslinking. Examples thereof are known to the person skilled in the art; suitable photoinitiators which may be* mentioned specifically are benzoins, such as benzoin, benzoin ethers, such as benzoin methyl ether, benzoin ethyl ether, benzoin isopropyl ether and benzoin phenyl ether, and benzoin acetate; acetophenones, such as acetophenone, 2,2-dimethoxyacetophenone and 1,1-dichloroacetophenone; benzil, benzil ketals, such as benzil dimethyl ketal and benzil diethyl ketal, camphorquinone, anthraquinones, such as 2methylanthraquinone, 2-ethylanthraquinone, 2-tert-butylanthraquinone, 1chloroanthraquinone and 2-amylanthraquinone; furthermore triphenylphosphine, benzoylphosphine oxides, for example 2,4,6-trimethylbenzoyl-diphenylphosphine oxide, benzophenones, such as benzophenone and 4,4'-bis(N,Ndimethylamino)benzophenone; thioxanthones and xanthenes; acridine derivatives; phenazine derivatives; quinoxaline derivatives and l-phenyl-1,2-propanedione benzoyl oxime; 1-aminophenyl ketones and 1-hydroxyphenyl ketones, such as 1hydroxycyclohexylphenyl ketone, phenyl 1 -hydroxyisopropyl ketone, 4isopropylphenyl 1-hydroxyisopropyl 1-hydroxyisopropyl ketone, 2-hydroxy-1-[4- 2(-hydroxyethoxy)phenyl]-2-methylpropan- 1-one, 1 -phenyl-2-hydroxy-2methylpropan-1-one, and 2,2-dimethoxy-1,2-diphenylethanone, all of which are known compounds.
Particularly suitable photoinitiators, which are usually used with UV lamps as light sources, are acetophenones, such as 2,2-dialkoxybenzophenones and WO 01/08603 PCT/AU00/00915 8 hydroxyphenyl ketones, in particular the initiators known under the trade names IRGACURE®819 and IRGACURE®184. A particularly preferred photoinitiator is IRGACURE® 651.
Another class of photoinitiators usually employed when argon ion lasers are used are benzil ketals, for example benzil dimethyl ketal.
The photoinitiators are added in effective amounts, expediently in amounts from about 0.05 to about 2.0% by weight, in particular from 0.1 to 0.5% by weight, based on the total amount of cross-linkable macromonomer.
The resultant cross-linkable macromonomer can be introduced into a mould using methods known per se, such as, in particular, conventional metering, for example dropwise. Alternatively, the macromonomers may be cured in situ, as for example in the case of an injectable lens. In this case the macromonomer is cured or crosslinked in the lens capsule after injection.
The cross-linkable macromonomers which are suitable in accordance with the invention can be crosslinked by irradiation with ionising or actinic radiation, for example electron beams, X-rays, UV or VIS light, ie electromagnetic radiation or particle radiation having a wavelength in the range from about 280 to 650 nm. Also suitable are UV lamps, He/Dc, argon ion or nitrogen or metal vapour or NdYAG laser beams with multiplied frequency. It is known to the person skilled in the art that each selected light source requires selection and, if necessary, sensitisation of the suitable photoinitiator. It has been recognised that in most cases the depth of penetration of the radiation into the cross-linkable macromonomer and the rate of curing are in direct correlation with the absorption coefficient and concentration of the photoinitiator. As well as photoinitiation, redox and thermal initiators may be used satisfactorily.
If desired, the crosslinking can also be initiated thermally. It should be emphasised that the crosslinking can take place in a very short time in accordance with the invention, for example, in less than five minutes, preferably in less than one minute, more preferably in less than 30 seconds. It will be appreciated that while the macromonomers of this invention may be used alone to form the lenses and other biocompatible materials, other materials may also be present. For WO 01/08603 PCT/AU00/00915 9 example, diluents may be present as well as other monomers including other macromonomers. When used as an injectable material the macromonomers should have a viscosity in the range 1,000 20,000 cSt and more preferably 1,000 10,000 cSt at 25 0 C. Instruments such as the Brookfield rheometer or the Bohlin controlled stress rheometer may be conveniently used for measurement.
The invention will be further described by reference to the following examples where all parts are expressed as parts by weight.
Example 1 This example illustrates the preparation of an acrylamide macromonomer.
An acrylamidoorganosilicon macromonomer of Formula I, where y 3, x and having a molecular weight in the range from 4,000 to 5,000, containing three acrylamido radicals A, having the formula -C(O)-C(CH 3 2
-NHC(O)CH=CH
2 was prepared as follows:
(CH
3 3 SiO((CH 3 )2SiO)x(O CH 3 Si(CH 2 3 NHA)yOSi(CH 3 3
I
Into a 25ml flask equipped with a stirrer bar and containing 10ml dry dichloromethane is placed 2.4g of a commercially available aminopropylmethylsiloxane-dimethysiloxane copolymer (available from Gelest, Inc., Tullytown, PA as Product AMS-162). To this is added 0.23g of distilled 2vinyl-4,4-dimethylazlactone. The reaction mixture is stirred for 18 hours, after which the infra red spectrum is recorded to confirm complete consumption of the vinylazlactone. Dichloromethane solvent is then removed in vacuo to yield a macromonomer of viscosity 250 centiStokes (cSt).
Example 2 This example illustrates the preparation of a crosslinked polymer using the macromonomer prepared in Example 1.
The acrylamide-functionalised siloxane and Irgacure 651 photoinitiator (Ciba Speciality Chemicals) were separately dissolved in chloroform in the proportions given below. The solutions were combined and the chloroform was removed in WO 01/08603 PCT/AU00/00915 vacuo. The following example was placed into polypropylene moulds (designed to give a flat polymeric disc of 20.7mm diameter and 1.0mm depth) and polymerised for ten minutes under irradiation from a 365nm UV lamp. All parts are by weight.
Macromonomer of 100 parts Formula I (x 60, y 3) Irgacure 651 0.3 parts After polymerisation was complete, a transparent, rubbery polymer disc was removed from the moulds. The shear modulus of the polymer was measured with a Bohlin controlled stress rheometer (CS-10) as 220 kPa.
Example 3 This example illustrates that the synthetic procedure outlined in Example 1 may be extended to other amino group containing polydimethylsiloxane copolymers.
Macro Mole Molecular Percent Shear Modulus Viscosity r.i.
monomer amino weight azlactone (kPa) (cSt) groups substitution after of amino polymerisation groups 2A' 2-4 28,000- 47% 85 14,600 1.4132 32,000 2B 2-4 28,000 25% 2.5 250 1.4239 32,000 1. Prepared from Aminoethylaminopropyl Methylsiloxane-Dimethylsiloxane Copolymer (Gelest Systems, Inc. Product AMS-233).
Macromonomers 2A and 2B were prepared in a similar fashion to macromonomer 1.
Example 4 WO 01/08603 PCT/AU00/00915 11 This example illustrates the preparation of cured polymers from macromonomers prepared according to Example 3.
Macromonomers 2A and 2B were placed into polypropylene moulds and polymerised for ten minutes under irradiation from a 365nm UV lamp. 100 parts Macromonomer and 0.3 parts Irgacure 651 photoinitiator were used in both examples. The difference in shear moduli for examples 2A and 2B shows that the mechanical properties of the polymer can be varied as desired by changing the degree of acrylamide substitution.
Example This example illustrates the preparation of a macromonomer where the ethylenically unsaturated groups are provided by acrylate moieties and the polymerisation of this macromonomer to a polymer.
A silicone acrylate compound of Formula II, where the average value of x 790, and the average value of y 60, and the molecular weight of the macromonomer is 62,000 containing an average of 60 acrylate radicals, A, having the formula -C(=O)-O-CH=CH 2 was prepared as follows:
(CH
3 3 SiO((CH 3 2 SiO)(OSi (CH 3 A) OSi(CH 3 3
II
In a 250ml round-bottom flask equipped with a reflux condenser and drying tube, methylhydrosiloxane-dimethylsiloxane copolymer (available from Gelest, Inc., Tullytown, PA as Product HMS-064) (20.03g, 18.91 mmol SiH groups) and allyl chloride (Aldrich, 1.45g, 18.9 mmol) were dissolved in 50ml dry toluene and then 95 microlitres of a 0.02M solution of hexachloroplatinic acid in isopropanol was added. The reaction mixture was then stirred for 18 h at 80 0 C. Consumption of the silicone hydride (SiH) groups was verified by treating an aliquot of the reaction mixture with ethanolic KOH solution no hydrogen evolution was observed.
The reaction mixture was then cooled to 5 0 C and butylated hydroxytoluene (25mg) and dry pyridine (1.5g, 18.96mmol) were added. A solution of 2hydroxyethyl acrylate (2.196g, 18.90mmol) in 10ml dry toluene was then added WO 01/08603 PCT/AU00/00915 12 dropwise at such a rate so as to maintain the reaction temperature below 5°C. The macromonomer was washed twice with methanol (100ml) and then left for four days in a dark environment. Irgacure 651 photoinitiator (Ciba Speciality Chemicals) was dissolved in dry toluene and combined -with the acrylatefunctionalised siloxane in dry toluene to give a concentration of photoinitiator to macromonomer identical to that for Example 4.
The formulation (viscosity 7,300 cSt) was then placed into polypropylene moulds designed to give a flat polymeric disc (refractive index 1.4107) of 20.7mm diameter and 1.0mm depth, (obtained from CIBA Vision, Atlanta) and polymerised for ten minutes under irradiation from a 365nm UV lamp. After polymerisation was complete, a transparent, rubbery polymer disc (refractive index 1.4107) was removed from the mould. The shear modulus of the polymer was measured with a Bohlin controlled stress rheometer (CS-10) as 44.5 kPa.
Example 6 S: 15 This example illustrates the preparation of a macromonomer where the ethylenically unsaturated groups are provided by methacrylate moieties and the polymerisation of this macromonomer to a polymer.
A silicone methacrylate compound of Formula I, where the average value of x 730, and the average value of y 7, and the molecular weight of the 20 macromonomer is 55,000 containing an average of 7 methacrylate radicals, A, *having the formula C(=O)-O-(CH 3
)CH=CH
2 was prepared as follows:
S**
(CH
3 3 SiO((CH 3 2 SiO)x(O(CH 3 )Si(CH 2 3 A)yOSi(CH3)3 Il Into a 50ml flask equipped with a stirrer bar and containing 20ml dry toluene is placed 2.6543g (0.36 mmol SiH groups) of a commercially available methylhydrosiloxane-dimethylsiloxane copolymer (available from Gelest, Inc., Tullytown, PA as Product HMS-013) and 0.2g (1.59 mmol) of allyl methacrylate.
100 microlitres of a 0.02M solution of hexachloroplatinic acid in isopropanol is then added. The reaction mixture is stirred for 72 hours, after which the 1H NMR spectrum is recorded to confirm complete reaction of the silicone hydride group WO 01/08603 PCT/AU00/00915 13 (8 4.7ppm).
The methacrylate-functionalised siloxane and Irgacure 651 photoinitiator (Ciba Specialty Chemicals) (in proportions identical to that used in Example 4) were separately dissolved in toluene. The solutions were combined and the toluene removed in vacuo, to yield a macromonomer of viscosity 3,300 cSt.
The formulation was then placed into polypropylene moulds (designed to give a flat polymeric disc of 20.7 mm diameter and 1.0mm depth, obtained from CIBA Vision, Atlanta) and polymerised for ten minutes under irradiation from a 365nm UV lamp. After polymerisation was complete, a transparent, rubbery polymer disc (refractive index 1.4086) was removed from the mould. The shear modulus of the polymer was measured with a Bohlin controlled stress rheometer as 22.5 kPa.
Example 7 This example illustrates the in vivo use of macromonomers according to this invention as intraocular lenses.
After initial softening by techniques such as phacoemulsification,.
endolenticular fragmentation, laser phacolysis, the existing lens material of a patient is removed via aspiration through a small (less than 1.2mm, but preferably equal to or less than 0.5mm) capsulorhexis at the periphery of the lens, with minimal damage to the capsule and peripheral tissue. The interior of the capsular bag is then cleaned and aspirated to remove cellular debris which may contribute to opacification of the posterior capsule subsequent to surgery a number of viscoelastic fluids e.g. hyaluronic acid may be used to flush the lens capsule. Other techniques photodynamic therapy) may be used at this time to provide an additional means of decreasing the incidence of posterior capsule opacification.
The macromonomer from Example 1 that is to form the substitute lens material is then introduced into the capsular bag through the capsulorhexis via a narrow gauge cannula. Optionally, an additional valve device may be positioned on the exterior of the empty lens capsule to enable injection of the substitute lens material without leakage prior to cure of the material. After refilling of the lens 004385566v7 14 capsule, the material is cured by UV irradiation. Other means including, but not limited to visible irradiation, thermal or redox reaction could also have been used.
The incision in the cornea is sutured and allowed to heal.
Reference to any prior art in the specification is not, and should not be taken as, an acknowledgment, or any form of suggestion, that this prior art forms part of the common general knowledge in Australia or any other jurisdiction or that this prior art could reasonably be expected to be ascertained, understood and regarded as relevant by a person skilled in the art.
*o *oo *o *o *o o *o *ooo

Claims (2)

1.39-1.44. A method of preparing intraocular lenses in situ by injecting a flowable macromonomer according to any one of claims 1 to 14 into a lens capsular bag and polymerising the macromonomer to provide a polymer, wherein the macromonomer has a viscosity at 25 0 C in the range 1,000 20,000 cSt, and wherein after polymerisation to form a polymer, the polymer has an E modulus in the range of 0.01 100 kPa. 16 A method of treating presbyopia by removing the lens material and injecting a flowable macromonomer according to any one of claims 1 to 14 into a lens capsular bag and polymerising the macromonomer to provide a polymer, wherein the macromonomer has a viscosity at 25 0 C in the range 1,000 20,000 cSt, and wherein after polymerisation to form a polymer, the polymer has an E modulus in the range of 0.01 100 kPa. 0** 20 17 A method according to claim 15 or 16 further comprising adding a photoinitiator. 18 A method according to claim 17 in which the amount of photoinitiator is between 0.05% and 2% by weight. 19 A polymer comprising macromonomers according to any one of claims 1 to
14. A polymer according to claim 18 in which macromonomers according to claims 1 to 14 comprise at least 50% by weight. 004571085v5.doc 21 A polymer according to claim 17 in which macromonomers according to claims 1 to 14 comprise at least 80% by weight. 22 A polymer according to any one of claims 19 to 21 further comprising other macromonomers to adjust the refractive index of the polymer. 23 A polymer according to any one of claims 19 to 21 further comprising other macromonomers to adjust the viscosity of the polymer. 24 An intraocular lens comprising a polymer according to any one of claims to 23. .o *a 25 An ethylenically unsaturated macromonomer substantially as described herein with reference to any one or more of the examples. 26 A method of preparing intraocular lenses in situ by injecting a flowable macromonomer according to any one of claims 1 to 14 into a lens capsular bag substantially as described herein with reference to any one or more of the examples. 20 27 A method of treating presbyopia by removing the lens material and injecting a flowable macromonomer according to any one of claims 1 to 14 into a lens capsular bag substantially as described herein with reference to any one or more of the examples. Commonwealth Scientific and Industrial Research Organisation By its registered patent attorneys Freehills Patent Trade Mark Attorneys 10 December 2004
AU61404/00A 1999-08-02 2000-08-02 Biomedical compositions Ceased AU780010B2 (en)

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AUPQ1978 1999-08-02
AUPQ1978A AUPQ197899A0 (en) 1999-08-02 1999-08-02 Biomedical compositions
AU61404/00A AU780010B2 (en) 1999-08-02 2000-08-02 Biomedical compositions
PCT/AU2000/000915 WO2001008603A1 (en) 1999-08-02 2000-08-02 Biomedical compositions

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Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5346946A (en) * 1992-08-26 1994-09-13 Menicon Co., Ltd Ocular lens material
US5610257A (en) * 1994-11-08 1997-03-11 L'oreal Photoprotective/cosmetic compositions comprising benzotriazole-substituted polyorganosiloxanes/polyorganosilanes
WO2000022460A1 (en) * 1998-10-13 2000-04-20 Pharmacia Groningen Bv Photocurable siloxane polymers

Patent Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5346946A (en) * 1992-08-26 1994-09-13 Menicon Co., Ltd Ocular lens material
US5610257A (en) * 1994-11-08 1997-03-11 L'oreal Photoprotective/cosmetic compositions comprising benzotriazole-substituted polyorganosiloxanes/polyorganosilanes
WO2000022460A1 (en) * 1998-10-13 2000-04-20 Pharmacia Groningen Bv Photocurable siloxane polymers

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