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ANATOMY & PHYSIOLOGY 
OF CORNEA 
Presented By – Dr. Om Patel 
Moderator – Dr. Jyoti Puri
ANATOMY OF CORNEA 
Cornea has the following physical characteristics: 
• Transparent 
• Avascular 
• Watchglass like structure 
• It forms anterior 1/6th of the 
outer fibrous coat of the eyeball 
2
DIMENSIONS 
• Anterior surface 
– Elliptical, 11.7 mm horizontally, 11 
mm vertical 
• Posterior surface 
–Circular about 11.7mm in diameter, 
1% wider in males 
• Central Thickness – 0.52mm 
• Peripheral Thickness – 0.67mm 
• Anterior radius of curvature – 
7.8mm 
• Posterior radius of curvature – 
6.5mm
• Optical zone - central third 
• Refractive power 
– 43 D (3/4th of total refractive power of eye) 
• Refractive index – 1.37
Composed of 6 layers ( ant to post.) are 
1. EPITHELIUM 
2. BOWMANS MEMBRANE 
3. SUBSTANTIA PROPRIA/STROMA 
4. DUA’S LAYER 
5. DESCEMENTS MEMBRANE 
6. ENDOTHELIUM 
HISTOLOGY
EPITHELIUM 
• Stratified, Squamous, Non-keratinized 
• 10% of total corneal thickness 
• 50-90microns thick, 5-6 layers of nucleated cells namely 
 Flattened surface cells ( superior 2 layers) 
 Wing cells ( next 2 to 3 layers) 
 Basal cell layer 
 Basement Membrane
FLATTENED SURFACE CELLS 
• Superficial 2 layers 
• Flat and polygonal 
• Surface covered with microvilli 
• Plays important role in tear film stability
WING CELLS 
• Polyhedral shape 
• 2-3 layers 
• Rich in intracellular tonofilaments composed of 
keratin 
• Numerous desmosomes and gap junctions are present 
between the cells
BASAL CELL LAYER 
• Tall columnar cells 
• Forms the germinal layer of epithelium 
• Secretes the basement membrane 
• Basal cells are firmly joined laterally to other basal cells and 
anteriorly to wing cells by desmosomes and maculae 
occludentes – these tight intracellular junctions account for 
epithelial transparency as well as its barrier function 
• Absence of hemi-desmosomes of the basal epithelial cells is 
responsible for recurrent corneal erosions
BASEMENT MEMBRANE 
• Secreted by the basal cell layer 
• PAS +ve 
• Consist mainly of type IV collagen & laminin 
• Blends indistinctly into bowman's membrane 
• Responsible for maintainence of well organised corneal 
epithelium 
• Defective BM is associated with recurrent erosion and 
epithelial defect
BOWMAN’S MEMBRANE 
• 8-14 microns 
• Also known as Anterior limiting lamina 
• Acellular mass of condensed collagen fibrils 
• Condensed superficial part of stroma 
• Collagen fibrils are primarily type I and type III 
• Shows considerable resistance to infection and injury 
• Once destroyed it does not regenerate
STROMA/SUBSTANTIA PROPRIA 
• 500 microns 
• Forms the largest portion of cornea 90% of total thickness 
• Consists of keratocytes and extracellular matrix 
• Keratocytes are corneal fibroblasts, found throughout 
stroma 
• Keratocytes produce the extracellular matrix 
• The extracellular matrix is made up of collagen fibrils and 
GAG.
• Most abundant GAG is keratan sulfate (65%) 
• The collagen fibrils are arranged in many layers with highly 
uniform diameter (22.5 to 35 nm) & inter fibrillary distance ( 
41.5 nm) 
• Fibrils are arranged parallel to each other and the corneal 
plane 
• Extends to periphery where the fibrils adopt a concentric 
configuration to form weave at the limbus 
• This imparts considerable strength to peripheral cornea & 
permits it to maintain curvature & optical properties
DUA’S LAYER 
• The existence of a new layer of cornea was suggested by 
Harminder Singh Dua et al in 2013 
• The existence of the layer was proved by injecting bubbles 
in the specific pre-descement layer of cornea with the help 
of surgical techniques 
• The experimental results were studied by optical 
and electron microscopy. The images showed a thin layer of 
corneal collagen between the corneal stroma and Descemet's 
membrane
• It is hypothetically 15 microns (0.00059 inches) thick, the 
fourth caudal layer, and located between the corneal 
stroma and Descemet's membrane 
• Despite its thinness, the layer is very strong and impervious 
to air
DESCEMENT’S MEMBRANE 
• Appears at the second month of gestation. 
• 3 microns at birth and 10-12 microns in young 
adults 
• Synthesis continues throughout adult life 
• Basal lamina of the corneal endothelium 
• Very resistant to chemical agents, trauma, infection, 
pathological process and enzymatic degradation
• Has regenerative power unlike Bowman’s membrane 
• It is sharply defined from the corneal stroma unlike Bowman’s 
membrane. There is in fact a plane of separation between them 
which is made use of in lamellar keratoplasty 
• Peripherally it appears to end at the anterior limit of trabecular 
meshwork as Schwalbe’s line 
• Posterior surface shows rounded wart like excrescences 
peripherally called Hassel Henle bodies which increase with 
advancing age 
• Similar central excrescenes are found in Fuch’s dystrophy known 
as Guttate
ENDOTHELIUM 
• Single layer of flat polygonal cells 
• Cell density is about 6000 cells/mm sq. at birth which 
goes on decreasing with age and comes around 2400- 
3000 cells/mm sq. in young adults 
• In adults these cells lose the ability to divide 
• Defect left by dying cells is filled by enlargement of 
remaining cells- POLYMEGATHISM 
• Cell diameter varies from 18-20 microns in early life to 
40 microns in aged
• Corneal decompensation – when more than 75% of adult age cells 
lost ( <500 cells/mm sq) 
• Cells are attached to each other & DM by tight junctional complexes 
and hemidesmosomes which closes the intercelluar space from the 
anterior chamber
BLOOD SUPPLY OF CORNEA 
• Cornea is an avascular tissue 
• The limbal region contains a vascular arcade which supplies the 
cornea with blood components 
• The vascular arcade is formed by the anastamoses b/w the 
anterior ciliary artery (branch of ophthalmic artery) & branches 
of external carotid artery 
• It invades periphery for about 1 mm & provide nourishment to 
cornea 
• It is actually present in the sub - conjunctival tissue which 
overlaps the cornea
NERVE SUPPLY OF CORNEA 
• Cornea is one of the most heavily innervated tissues in the 
body 
• Innervational density is highest near the centre & gradually 
decreases towards the periphery 
• Trigeminal N.  Ophthalmic division  Nasociliary nerve 
 Long ciliary nerves
Long ciliary nerve 
↓ 
Enter the eyeball around the Optic nerve 
↓ 
Run forward in suprachoroidal space 
↓ 
Pierces the sclera close to the limbus 
↓ 
Forms a PERICORNEAL PLEXUS OF NERVES with 
conjuctival nerves 
↓ 
Enters the cornea at various depths viz. sclera, episclera & 
conjunctiva
↓ 
Loses their myelin sheath after traversing 1-2 mm to form a 
STROMAL PLEXUS 
↓ 
Anteriorly forms a SUBEPITHELIAL PLEXUS 
↓ 
Penetrates the pores in Bowman’s membrane, 
divides into filaments under the basal layer of epithelium & extends 
between the cells of all layers of epithelium to form 
INTRAEPITHELIAL PLEXUS 
↓ 
Ends in epithelium as fine beaded filaments
Subepithelial and Intraepithelial Plexus
CORNEAL PHYSIOLOGY 
Physiological functions of cornea are : 
• To act as a powerful refracting lens of fixed focus that 
transmits light in an orderly fashion for proper image 
formation 
• To protect intraocular contents 
• Absorption of topically applied drugs
Physiological processes concerned in carrying out 
these functions are: 
• BIOCHEMICAL COMPOSITION AND 
METABOLISM OF CORNEA 
• CORNEAL TRANSPARENCY 
• DRUG PERMEABILITY THROUGH THE CORNEA 
• CORNEAL WOUND HEALING
CORNEAL METABOLISM 
• Cornea requires energy for normal metabolic activities as 
well as for maintaining transparency & dehydration 
• Energy is generated by the breakdown of glucose in form 
of ATP 
• Most actively metabolising layers – Epithelium & 
Endothelium
Sources of Nutrients 
1) Oxygen 
 Epithelium 
– Mainly from atmosphere through tear 
film 
- Limbal Capillaries 
 Endothelium 
- Through aqueous humour 
• Minimum oxygen tension for normal corneal 
hydration is 11-19 mm Hg. Below this range 
cornea will hydrate and swell
2) Glucose 
• Mainly from the aqueous humour 
• In case of deprivation stored glycogen or even fatty 
acids are utilised as a source of glucose 
3) Amino Acids 
• Principal source is passive diffusion from aqueous 
• Required for synthesis of protein needed for 
epithelial turnover
METABOLIC PATHWAYS 
• GLYCOLYSIS 
- Many enzymes of the EMP or the TCA/Krebs cycle are 
present in cornea 
- There is accumulation of lactate even in aerobic 
conditions due to high glycolytic activity but limited TCA 
cycle activity 
- Lactate is eliminated from the cornea by diffusion 
through the epithelium
• HMP SHUNT 
- This occurs without a net gain in the ATP 
- Its purpose is to produce NADPH which is utilized for the 
biosynthesis of lipids by corneal epithelium 
- Ribose produced may be used to build DNA & RNA
CORNEAL TRANSPARENCY 
Factors affecting corneal transparency are: 
1. Corneal epithelium & tear film 
2. Arrangement of stromal lamellae 
3. Corneal vascularization 
4. Corneal hydration 
5. IOP
CORNEAL EPITHELIUM & TEAR FILM 
• It has homogenous refractive index 
• The various cells at different layers are firmly attached 
with each other 
• Tight intercellular junctions contribute to transparency
2. ARRANGEMENT OF STROMAL 
LAMELLAE 
Two theories are proposed 
1) MAURICE THEORY -(1957) 
The regular lattice arrangement destroys the scattered 
light by mutual interference. The collagen fibrils are separated 
by less than a wavelength of light.
2) Theory of GOLDMAN et al. 
• Lattice arrangement not necessary 
• Cornea is transparent because the fibrils are small in relation to 
light & do not interfere with light transmission unless they are 
larger than one half the wavelength of light 
• However these theories fail to explain the occurrence of rapid 
clouding of cornea associated with acute rise in IOP & the 
rapid clearing of cornea with reduction of IOP
CORNEAL VASCULARIZATION 
• Corneal vascularisation occurs as a defence mechanism in 
response to noxious stimulus which interferes with the 
transparency 
• Various chemical and mechanical theories have been suggested 
to explain the vascularisation of cornea in response to noxious 
stimuli
CORNEAL HYDRATION 
• The normal corneal water content is 80% 
• Increase in the water content leads to increased central 
corneal thickness and will compromise the corneal 
transparency 
• It is kept constant by balance of various factors
• Factor which draws water inside cornea 
- Swelling pressure of stromal matrix 
• Factor preventing the flow of water inside cornea 
- Barrier function of epithelium & 
endothelium 
• Factor drawing water out of the cornea 
- Active pump mechanisms of endothelium
STROMAL SWELLING PRESSURE 
• Pressure (60 mm Hg) exerted by the GAGs of the corneal 
stroma which act like a sponge 
• Due to the electrostatic repulsion of the anionic charges on 
the GAG molecule, a negative but equal pressure called 
imbibition pressure is developed 
• This is the negative pressure by which the level of 
interfibrillar tension is maintained 
• However in practice imbibition pressure 
IP = ( IOP - SP )i.e. 17 - 60 = - 43 mm hg
BARRIER FUNCTION OF EPITHELIUM 
AND ENDOTHELIUM 
• Functions as barriers to excessive flow of water and diffusion of 
electrolytes into the stroma due to their semipermeable nature 
• Corneal transparency decreases and thickness increases when 
the corneal endothelium is damaged and to a lesser extent when 
the epithelium is damaged
ACTIVE PUMP MECHANISM OF 
ENDOTHELIUM 
The corneal endothelium plays an important role in 
controlling fluid transport across itself due to the presence of 
several enzyme pump mechanisms namely 
• Na+/K+ ATPase Pump 
• Bicarbonate dependant ATPase 
• Na+/H+ exchanger 
• Carbonic Anhydrase enzyme system
INTRAOCULAR PRESSURE 
• Epithelial edema occurs when IOP increases more than 
stromal swelling pressure 
• Clinically detectable corneal edema can be seen with IOP 
more than 50 mm Hg 
• However in endothelial dystrophy corneal oedema can 
occur with normal IOP also due to decreased swelling 
pressure
DRUG PERMEABILITY ACROSS 
THE CORNEA 
Factors affecting this are: 
1) Lipid & water solubility of drug 
– Drug should be amphipathic to readily penetrate 
cornea as epithelium & endothelium are lipophilic while the 
stroma is hydrophilic 
2) Molecular size, weight & concentration of drug – 
- Lipophilic molecules can easily cross epithelium 
while hydrophilic molecules only smaller than 0.4 nm 
can cross through the pores in the cell membrane 
48
- Substances with molecular weight of less than 100 
daltons can easily pass through the cell membrane while 
those with more than 500 cannot 
- Drugs with large molecular size in high concentration 
can cross the cornea following laws of mass action 
3) Ionic forms of the drug 
– Drug must have the capacity to exist in both ionized & 
non-ionized forms for a better penetration through cornea 
49
KINSEY MODEL FOR DRUG IONIZATION AND 
PERMEABILITY
4) pH of the solution 
– Within a range of pH 4-10, epithelial permeability is 
not affected but beyond this range, the permeability 
increases 
5) Tonicity of the solution 
– Hypotonic solutions greatly increase the permeability 
of the epithelium 
6) Surface active agents 
– Agents that reduce surface tension, increase corneal 
wetting & thus present more drug for absorption
7) Pro-drug 
– Prodrug forms are lipophilic & after absorption 
through epithelium are converted into proper drugs that can 
easily pass through stroma. E.g.. Dipivefrin- Epinephrine
EFFECT OF CONTACT LENS WEAR 
ON CORNEAL PHYSIOLOGY 
• CL affect the function of epithelium 
• Epithelium gets oxygen from tears & 
glucose from aqueous & limbal vessels 
• CL shifts the balance from aerobic  
anaerobic metabolism  increases lactate 
& CO2 production 
• Leads to acidosis  Stromal hydration
• CL types are based on their oxygen flux defined as the DK 
value 
• Oxygen flux = DK/L * DP 
D = Diffusion Coefficient 
K = Solubility 
L = Thickness of lens 
DP = Change in the partial pressure 
of oxygen across the material 
• HEMA and PMMA have low oxygen flux 
• Hydrogen and Silicon lenses have high flux 
• Both DK value and thickness of lens determines the 
suitability for use
• Rigid CL (PMMA) 
• Reduces O2 availability 
• Deplete glycogen stores 
• Reduces direct glucose utilization by the cornea 
• Affect corneal transparency 
• Tear film instability 
• Soft CL permits extended wear due to their permeability 
to O2 & CO2 
• RGP combines the reduced toxicity of PMMA and high 
gas transfer capability
• Deleterious effects of CL  Due to low O2 permeability 
• Epithelial thinning 
• Reduction in the hemidesmosome density 
• Reduction in anchoring fibrils 
• Reduce adhesion of the epithelium to the basement 
membrane 
• Severe cases produce epithelial edema and punctate epithelial 
erosions
CORNEAL WOUND HEALING
58

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Corneal anatomy and physiology 2

  • 1. ANATOMY & PHYSIOLOGY OF CORNEA Presented By – Dr. Om Patel Moderator – Dr. Jyoti Puri
  • 2. ANATOMY OF CORNEA Cornea has the following physical characteristics: • Transparent • Avascular • Watchglass like structure • It forms anterior 1/6th of the outer fibrous coat of the eyeball 2
  • 3. DIMENSIONS • Anterior surface – Elliptical, 11.7 mm horizontally, 11 mm vertical • Posterior surface –Circular about 11.7mm in diameter, 1% wider in males • Central Thickness – 0.52mm • Peripheral Thickness – 0.67mm • Anterior radius of curvature – 7.8mm • Posterior radius of curvature – 6.5mm
  • 4. • Optical zone - central third • Refractive power – 43 D (3/4th of total refractive power of eye) • Refractive index – 1.37
  • 5. Composed of 6 layers ( ant to post.) are 1. EPITHELIUM 2. BOWMANS MEMBRANE 3. SUBSTANTIA PROPRIA/STROMA 4. DUA’S LAYER 5. DESCEMENTS MEMBRANE 6. ENDOTHELIUM HISTOLOGY
  • 6. EPITHELIUM • Stratified, Squamous, Non-keratinized • 10% of total corneal thickness • 50-90microns thick, 5-6 layers of nucleated cells namely  Flattened surface cells ( superior 2 layers)  Wing cells ( next 2 to 3 layers)  Basal cell layer  Basement Membrane
  • 7.
  • 8. FLATTENED SURFACE CELLS • Superficial 2 layers • Flat and polygonal • Surface covered with microvilli • Plays important role in tear film stability
  • 9. WING CELLS • Polyhedral shape • 2-3 layers • Rich in intracellular tonofilaments composed of keratin • Numerous desmosomes and gap junctions are present between the cells
  • 10. BASAL CELL LAYER • Tall columnar cells • Forms the germinal layer of epithelium • Secretes the basement membrane • Basal cells are firmly joined laterally to other basal cells and anteriorly to wing cells by desmosomes and maculae occludentes – these tight intracellular junctions account for epithelial transparency as well as its barrier function • Absence of hemi-desmosomes of the basal epithelial cells is responsible for recurrent corneal erosions
  • 11. BASEMENT MEMBRANE • Secreted by the basal cell layer • PAS +ve • Consist mainly of type IV collagen & laminin • Blends indistinctly into bowman's membrane • Responsible for maintainence of well organised corneal epithelium • Defective BM is associated with recurrent erosion and epithelial defect
  • 12. BOWMAN’S MEMBRANE • 8-14 microns • Also known as Anterior limiting lamina • Acellular mass of condensed collagen fibrils • Condensed superficial part of stroma • Collagen fibrils are primarily type I and type III • Shows considerable resistance to infection and injury • Once destroyed it does not regenerate
  • 13. STROMA/SUBSTANTIA PROPRIA • 500 microns • Forms the largest portion of cornea 90% of total thickness • Consists of keratocytes and extracellular matrix • Keratocytes are corneal fibroblasts, found throughout stroma • Keratocytes produce the extracellular matrix • The extracellular matrix is made up of collagen fibrils and GAG.
  • 14. • Most abundant GAG is keratan sulfate (65%) • The collagen fibrils are arranged in many layers with highly uniform diameter (22.5 to 35 nm) & inter fibrillary distance ( 41.5 nm) • Fibrils are arranged parallel to each other and the corneal plane • Extends to periphery where the fibrils adopt a concentric configuration to form weave at the limbus • This imparts considerable strength to peripheral cornea & permits it to maintain curvature & optical properties
  • 15.
  • 16. DUA’S LAYER • The existence of a new layer of cornea was suggested by Harminder Singh Dua et al in 2013 • The existence of the layer was proved by injecting bubbles in the specific pre-descement layer of cornea with the help of surgical techniques • The experimental results were studied by optical and electron microscopy. The images showed a thin layer of corneal collagen between the corneal stroma and Descemet's membrane
  • 17. • It is hypothetically 15 microns (0.00059 inches) thick, the fourth caudal layer, and located between the corneal stroma and Descemet's membrane • Despite its thinness, the layer is very strong and impervious to air
  • 18. DESCEMENT’S MEMBRANE • Appears at the second month of gestation. • 3 microns at birth and 10-12 microns in young adults • Synthesis continues throughout adult life • Basal lamina of the corneal endothelium • Very resistant to chemical agents, trauma, infection, pathological process and enzymatic degradation
  • 19. • Has regenerative power unlike Bowman’s membrane • It is sharply defined from the corneal stroma unlike Bowman’s membrane. There is in fact a plane of separation between them which is made use of in lamellar keratoplasty • Peripherally it appears to end at the anterior limit of trabecular meshwork as Schwalbe’s line • Posterior surface shows rounded wart like excrescences peripherally called Hassel Henle bodies which increase with advancing age • Similar central excrescenes are found in Fuch’s dystrophy known as Guttate
  • 20. ENDOTHELIUM • Single layer of flat polygonal cells • Cell density is about 6000 cells/mm sq. at birth which goes on decreasing with age and comes around 2400- 3000 cells/mm sq. in young adults • In adults these cells lose the ability to divide • Defect left by dying cells is filled by enlargement of remaining cells- POLYMEGATHISM • Cell diameter varies from 18-20 microns in early life to 40 microns in aged
  • 21. • Corneal decompensation – when more than 75% of adult age cells lost ( <500 cells/mm sq) • Cells are attached to each other & DM by tight junctional complexes and hemidesmosomes which closes the intercelluar space from the anterior chamber
  • 22. BLOOD SUPPLY OF CORNEA • Cornea is an avascular tissue • The limbal region contains a vascular arcade which supplies the cornea with blood components • The vascular arcade is formed by the anastamoses b/w the anterior ciliary artery (branch of ophthalmic artery) & branches of external carotid artery • It invades periphery for about 1 mm & provide nourishment to cornea • It is actually present in the sub - conjunctival tissue which overlaps the cornea
  • 23. NERVE SUPPLY OF CORNEA • Cornea is one of the most heavily innervated tissues in the body • Innervational density is highest near the centre & gradually decreases towards the periphery • Trigeminal N.  Ophthalmic division  Nasociliary nerve  Long ciliary nerves
  • 24.
  • 25. Long ciliary nerve ↓ Enter the eyeball around the Optic nerve ↓ Run forward in suprachoroidal space ↓ Pierces the sclera close to the limbus ↓ Forms a PERICORNEAL PLEXUS OF NERVES with conjuctival nerves ↓ Enters the cornea at various depths viz. sclera, episclera & conjunctiva
  • 26. ↓ Loses their myelin sheath after traversing 1-2 mm to form a STROMAL PLEXUS ↓ Anteriorly forms a SUBEPITHELIAL PLEXUS ↓ Penetrates the pores in Bowman’s membrane, divides into filaments under the basal layer of epithelium & extends between the cells of all layers of epithelium to form INTRAEPITHELIAL PLEXUS ↓ Ends in epithelium as fine beaded filaments
  • 28. CORNEAL PHYSIOLOGY Physiological functions of cornea are : • To act as a powerful refracting lens of fixed focus that transmits light in an orderly fashion for proper image formation • To protect intraocular contents • Absorption of topically applied drugs
  • 29. Physiological processes concerned in carrying out these functions are: • BIOCHEMICAL COMPOSITION AND METABOLISM OF CORNEA • CORNEAL TRANSPARENCY • DRUG PERMEABILITY THROUGH THE CORNEA • CORNEAL WOUND HEALING
  • 30. CORNEAL METABOLISM • Cornea requires energy for normal metabolic activities as well as for maintaining transparency & dehydration • Energy is generated by the breakdown of glucose in form of ATP • Most actively metabolising layers – Epithelium & Endothelium
  • 31. Sources of Nutrients 1) Oxygen  Epithelium – Mainly from atmosphere through tear film - Limbal Capillaries  Endothelium - Through aqueous humour • Minimum oxygen tension for normal corneal hydration is 11-19 mm Hg. Below this range cornea will hydrate and swell
  • 32. 2) Glucose • Mainly from the aqueous humour • In case of deprivation stored glycogen or even fatty acids are utilised as a source of glucose 3) Amino Acids • Principal source is passive diffusion from aqueous • Required for synthesis of protein needed for epithelial turnover
  • 33. METABOLIC PATHWAYS • GLYCOLYSIS - Many enzymes of the EMP or the TCA/Krebs cycle are present in cornea - There is accumulation of lactate even in aerobic conditions due to high glycolytic activity but limited TCA cycle activity - Lactate is eliminated from the cornea by diffusion through the epithelium
  • 34. • HMP SHUNT - This occurs without a net gain in the ATP - Its purpose is to produce NADPH which is utilized for the biosynthesis of lipids by corneal epithelium - Ribose produced may be used to build DNA & RNA
  • 35. CORNEAL TRANSPARENCY Factors affecting corneal transparency are: 1. Corneal epithelium & tear film 2. Arrangement of stromal lamellae 3. Corneal vascularization 4. Corneal hydration 5. IOP
  • 36. CORNEAL EPITHELIUM & TEAR FILM • It has homogenous refractive index • The various cells at different layers are firmly attached with each other • Tight intercellular junctions contribute to transparency
  • 37. 2. ARRANGEMENT OF STROMAL LAMELLAE Two theories are proposed 1) MAURICE THEORY -(1957) The regular lattice arrangement destroys the scattered light by mutual interference. The collagen fibrils are separated by less than a wavelength of light.
  • 38.
  • 39. 2) Theory of GOLDMAN et al. • Lattice arrangement not necessary • Cornea is transparent because the fibrils are small in relation to light & do not interfere with light transmission unless they are larger than one half the wavelength of light • However these theories fail to explain the occurrence of rapid clouding of cornea associated with acute rise in IOP & the rapid clearing of cornea with reduction of IOP
  • 40. CORNEAL VASCULARIZATION • Corneal vascularisation occurs as a defence mechanism in response to noxious stimulus which interferes with the transparency • Various chemical and mechanical theories have been suggested to explain the vascularisation of cornea in response to noxious stimuli
  • 41. CORNEAL HYDRATION • The normal corneal water content is 80% • Increase in the water content leads to increased central corneal thickness and will compromise the corneal transparency • It is kept constant by balance of various factors
  • 42. • Factor which draws water inside cornea - Swelling pressure of stromal matrix • Factor preventing the flow of water inside cornea - Barrier function of epithelium & endothelium • Factor drawing water out of the cornea - Active pump mechanisms of endothelium
  • 43. STROMAL SWELLING PRESSURE • Pressure (60 mm Hg) exerted by the GAGs of the corneal stroma which act like a sponge • Due to the electrostatic repulsion of the anionic charges on the GAG molecule, a negative but equal pressure called imbibition pressure is developed • This is the negative pressure by which the level of interfibrillar tension is maintained • However in practice imbibition pressure IP = ( IOP - SP )i.e. 17 - 60 = - 43 mm hg
  • 44. BARRIER FUNCTION OF EPITHELIUM AND ENDOTHELIUM • Functions as barriers to excessive flow of water and diffusion of electrolytes into the stroma due to their semipermeable nature • Corneal transparency decreases and thickness increases when the corneal endothelium is damaged and to a lesser extent when the epithelium is damaged
  • 45. ACTIVE PUMP MECHANISM OF ENDOTHELIUM The corneal endothelium plays an important role in controlling fluid transport across itself due to the presence of several enzyme pump mechanisms namely • Na+/K+ ATPase Pump • Bicarbonate dependant ATPase • Na+/H+ exchanger • Carbonic Anhydrase enzyme system
  • 46.
  • 47. INTRAOCULAR PRESSURE • Epithelial edema occurs when IOP increases more than stromal swelling pressure • Clinically detectable corneal edema can be seen with IOP more than 50 mm Hg • However in endothelial dystrophy corneal oedema can occur with normal IOP also due to decreased swelling pressure
  • 48. DRUG PERMEABILITY ACROSS THE CORNEA Factors affecting this are: 1) Lipid & water solubility of drug – Drug should be amphipathic to readily penetrate cornea as epithelium & endothelium are lipophilic while the stroma is hydrophilic 2) Molecular size, weight & concentration of drug – - Lipophilic molecules can easily cross epithelium while hydrophilic molecules only smaller than 0.4 nm can cross through the pores in the cell membrane 48
  • 49. - Substances with molecular weight of less than 100 daltons can easily pass through the cell membrane while those with more than 500 cannot - Drugs with large molecular size in high concentration can cross the cornea following laws of mass action 3) Ionic forms of the drug – Drug must have the capacity to exist in both ionized & non-ionized forms for a better penetration through cornea 49
  • 50. KINSEY MODEL FOR DRUG IONIZATION AND PERMEABILITY
  • 51. 4) pH of the solution – Within a range of pH 4-10, epithelial permeability is not affected but beyond this range, the permeability increases 5) Tonicity of the solution – Hypotonic solutions greatly increase the permeability of the epithelium 6) Surface active agents – Agents that reduce surface tension, increase corneal wetting & thus present more drug for absorption
  • 52. 7) Pro-drug – Prodrug forms are lipophilic & after absorption through epithelium are converted into proper drugs that can easily pass through stroma. E.g.. Dipivefrin- Epinephrine
  • 53. EFFECT OF CONTACT LENS WEAR ON CORNEAL PHYSIOLOGY • CL affect the function of epithelium • Epithelium gets oxygen from tears & glucose from aqueous & limbal vessels • CL shifts the balance from aerobic  anaerobic metabolism  increases lactate & CO2 production • Leads to acidosis  Stromal hydration
  • 54. • CL types are based on their oxygen flux defined as the DK value • Oxygen flux = DK/L * DP D = Diffusion Coefficient K = Solubility L = Thickness of lens DP = Change in the partial pressure of oxygen across the material • HEMA and PMMA have low oxygen flux • Hydrogen and Silicon lenses have high flux • Both DK value and thickness of lens determines the suitability for use
  • 55. • Rigid CL (PMMA) • Reduces O2 availability • Deplete glycogen stores • Reduces direct glucose utilization by the cornea • Affect corneal transparency • Tear film instability • Soft CL permits extended wear due to their permeability to O2 & CO2 • RGP combines the reduced toxicity of PMMA and high gas transfer capability
  • 56. • Deleterious effects of CL  Due to low O2 permeability • Epithelial thinning • Reduction in the hemidesmosome density • Reduction in anchoring fibrils • Reduce adhesion of the epithelium to the basement membrane • Severe cases produce epithelial edema and punctate epithelial erosions
  • 58. 58

Notes de l'éditeur

  1. Horizontal – 11 to 12 Vertical 9 to 11
  2. Non inonized for epithelium and endothelium’ Ionized form for stroma
  3. Hema - hydroxyethyl methacrylate