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Pterygium and its management 
Dr Jyoti Prakash Behera
Anatomy of conjunctiva
Histology of normal conjunctiva
Pterygium- Definition 
• Derived from Greek word “Pterygos” means 
small wing 
• It is a non malignant slow growing 
proliferation of wing shaped fibrovascular 
tissue. 
• Arises from subconjunctival tissue. 
• May extend over the cornea thus disturbing 
the vision.
Pterygium- Incidence & Prevalence 
• Cameron's map- Shows a direct relationship 
between prevalence and proximity to the 
equator(warm and dry climate) 
• Factors other than geographic location 
– Male : female= 2:1 
– more common in farmers than in city dwellers 
– more who do not wear eyeglasses 
– elderly have the highest prevalence rate, but a much 
younger (20-to 40-year old) group has the highest 
incidence rate
• In India prevalence is 9.5%. 
• Morbidity: causes significant alteration in 
visual function in advanced cases.
ETIOPATHOGENESIS. 
• Strong association between UV light exposure 
and formation of pterygium. 
– More common- in patients who worked outdoors. 
– In welders than other factory workers. 
• Also associated with basal cell carcinoma, 
porphyria cutanea tarda, polymorphous light 
eruptions, xeroderma pigmentosa.
• ANGIOGENESIS FACTOR-(Wong) Prolonged UV 
exposure causes biological changes in the 
bowmans membrane 
• UV Exposure: May induce hyperplasia in 
limbal cells. These altered cells invade the 
cornea and limbus which moves centripetally 
with them
ALBEDO HYPOTHESIS 
• Light entering the temporal limbus at 90degree is 
concentrated at medial limbus (supported and 
demonstrated by Coroneo) 
• Related to corneal curvature. 
• This explains the predominance of medial 
pterygium.
Other theories 
• Scarpa, Friede, and Kamel believed that chronic 
inflammation in the form of conjunctivitis or 
episcleritis initiates the process 
• MICROTRAUMA: mechanical irritation by dust 
particles, enhanced by tear flow from lateral to 
medial. 
• IMMUNOLOGY: Cell bound IgE irritant complexes 
initiate the release of inflammatory mediators 
from mast cells→ Release of stimulatory 
factors→Development of pterygium.
• HYPOXIA: increase in non perfusion areas and 
attenuated vessels in nasal limbus during early 
stage of pterygium causes recruitment of 
progenitor cells. 
• Viral markers: infection with HPV and herpes 
virus is considered as risk factor(rare).
Genetic predisposition 
• Expression of vimentin. 
• P53 mutation leads to decreased apoptosis 
and increased TGF-b which leads to increased 
growth.
Pterygium- Degenerative or 
proliferative ??? 
• long been considered a chronic degenerative 
condition 
• Classically described as“elastotic degeneration” 
• Cˇilanova-Atanasova ascertained that the 
degenerative or dystrophic changes in pterygium 
were simply more pronounced than normal aging 
conjuctiva 
• In addition, pterygium tissue had proliferative 
components that included epithelial hyperplasia 
and the appearance of newly formed connective 
tissue, blood vessels and fibrous elements
• Cameron- showed the evidence of transformed, 
invading subconjuctival fibroblasts that grows 
centripetally 
• Austin and co-workers suggested- excessive 
production of elastin material by actinically 
damaged, proliferative subconjunctival fibroblasts 
• Primary Pterygium is definitely locally invasive 
• Also pterygium epithelium exhibits varying 
degrees of abnormality, ranging from mild 
dysplasia to carcinoma in situ
Limbal Stem Cell Deficiency and 
Epithelial Abnormalities 
• Kwok- propose that the initial biologic event in 
pterygium was an alteration of limbal stem cells 
due to chronic UV light exposure, resulting in 
concomitant breakdown of the limbal barrier and 
subsequent conjunctivalization of the cornea 
• primary and recurrent pterygia exhibit 
overexpression of the p53 tumor-suppressor 
gene 
• Presence of abberant apoptosis
Pterygium-Histopathology 
• Three basic elements characterize the histologic 
appearance 
1. Epithelial covering of atrophic conjuctiva extends 
beyond 
2. Degenerated connective tissue- a bulky mass of 
thickened, hypertrophied, and degenerated 
connective tissue 
– collagen component of which assumes a coiled, fibrillated 
pattern reminiscent of elastic tissue 
– The abnormal collagen shows basophilia and an affinity for 
elastic tissue stains, but is not digested by elastase 
– hence categorized as elastotic degeneration
Histology 
Normal conjunctiva Pterygium
Histology
3. Vascular element- New blood vessels, usually 
congested, are dispersed among the 
hypertrophied collagen fibers 
• The episcleral bed beneath the pterygium is 
hyperemic 
• Tenon’s capsule is incorporated into the body 
of the pterygium and contributes to its 
vasculature and bulk
Histopathology cont.. 
• Immediately in front of the head of the 
pterygium, an advancing row of fibroblasts 
penetrates the cornea between Bowman’s 
layer and the basement membrane of the 
epithelium (grey zone or cap) 
• Eventually tissue enters the cornea, Bowman's 
layer is pushed posteriorly and eventually 
becomes fragmented
Formed pterygium- schematic
Pterygium- Clinical feature 
• A pterygium appears as a fleshy triangular band 
of fibrovascular tissue 
• axis of the triangle gently slopes superiorly on the 
corneal side 
• It has several components 
– The cap 
– The head 
– The body 
– The base 
– Superior edge 
– Inferior edge
• The cap 
– The cap is a flat, grayish white avascular zone of 
variable size located in the subepithelial corneal 
tissue 
– Sometimes a round, gray, coin-like extensions of 
the cap precede it (“islets of Fuchs") 
– some cases, a golden-yellow iron line may be seen 
(Stocker's line) 
– Between the head and the cap there are small 
capillaries
Islets of Fuch’s 
Stocker's line
• The head 
– It is slightly elevated and 
white 
– It is the one site of firm 
adhesion to the globe 
• The body 
– fleshy sheet of pink, highly 
vascularized tissue 
– delineated from the normal 
conjunctiva superiorly and 
inferiorly by sharp folds 
– frequently reveals punctate 
staining over the epithelial 
surface of the body
• Clinical Grading of 
pterygium 
• As proposed by Donald 
T H Tan 
• Grade T1(atrophic)- 
pterygium in which 
episcleral vessels 
underlying the body of 
the pterygium were 
unobscured and clearly 
distinguished
• Grade T3(fleshy)- thick 
pterygium in which 
episcleral vessels 
underlying the body of 
the pterygium are 
totally obscured by 
fibrovascular tissue 
• Grade T2(intermediate)- 
All other pterygia that 
do not fall into these 
two categories
• Surgical recurrence correlated well with 
translucency 
– fleshy pterygium having the highest capacity for 
recurrence 
– Atrophic has the lowest
Clinical staging of pterygium 
CLINICAL STAGING PATHOLOGICAL 
STAGING 
Stage I Exposure 
conjunctivitis 
Size and number of 
Conjunctival vessels 
Mild – moderate congestion 
S/S of dryness 
No formed lesions 
Altered tear film 
Mild vascular 
response 
Stage II Pinguecula and 
pterygium 
Distinct raised lesion on bulbar 
conjunctiva 
With or w/o abnormal 
vascularization and inflammation 
Cell injury 
Inflammatory 
response
Stage III Limbal pterygium Head is on or across the 
limbus with or w/o an iron 
line at the conjunctival 
corneal interface 
Vascularization and fibrous 
proliferation 
Symptoms more 
pronounced 
Lesion organization 
Mixed proliferation 
and degeneration 
Stage IV Corneal pterygium Lesion 2mm or more into 
cornea 
Invasion of granulation 
tissue 
Zone of dellen 
Stocker’s line 
Infiltration of corneal 
nerves- pain 
Lesion b/w 
epithelium and 
bowman 
Mixed proliferative 
and degeneration
Stage V Compound pterygium Induced astigmatism 
Symptoms more 
frequent and severe 
Lesion extended 
into stroma 
Mixed proliferative 
and degeneration 
Proliferation- Small lymphocytes and plasma cells 
Degeneration- Swirls of type I collagen
Other types 
• Primary double pterygium. 
• Recurrent pterygium. 
• Pseudopterygium. 
• Malignant 
pterygium(rare):recurrent 
pterygium with restriction of 
ocular movements.
Symptoms 
• Asymptomatic 
• Foreign body sensation 
• Discomfort 
• Congestion(redness) 
• Irritation and grittiness-interference with 
precorneal tear film. 
• Interference with vision-obscuring visual axis 
-inducing astigmatism(WTR) 
• Cosmesis 
• Diplopia
Differential diagnosis 
Condition Signs and symptoms Tests 
Pseudopterygium Most often hx of previous 
infective, chemical, thermal, 
or traumatic injury to the 
cornea. 
May occur at multiple 
locations and is not restricted 
to the 3 and 9 o'clock 
(interpalpebral) positions. 
-Slit-lamp examination: reveals 
lesion to be adhesion of a fold 
of conjunctiva, which has 
occurred as a response to a 
previous peripheral corneal 
ulcer/inflammation. 
-Lesion typically only fixed at its 
apex to the cornea so that a 
probe may be passed 
underneath its body at the 
limbus, while a true pterygium 
adheres to the underlying 
cornea throughout its length. 
Thinning of the underlying 
cornea may be seen at its head.
Pinguecula Does not encroach on the 
cornea. 
Slit-lamp examination: reveals 
exact extent and nature of 
lesion. A pingueculum is 
limited to limbus and 
conjunctiva and does not 
encroach onto the cornea. 
Marginal keratitis Associated with blepharitis. 
Infiltrate on corneal surface 
is separated by a clear zone 
from the limbus. Occur at 2, 
4, 8, and 10 o'clock 
position. Does not have 
typical pterygium shape. 
Often superior and inferior. 
Corneal swab/scraping: 
microscopy and culture 
positive for infecting organism, 
but infecting organisms are 
often not detected, as many 
cases are due to an 
inflammatory reaction to 
staphylococcal proteins
Corneal micropannus Hx of trachoma or lack of 
corneal oxygenation due to 
excessive contact lens 
wear. 
Slit-lamp examination: 
reveals encroachment of 
fine blood vessels onto 
corneal surface. 
Conjunctival carcinoma in 
situ/ bowens epithlioma. 
Rare. Does not have typical 
pterygium shape. Not 
restricted to the 3 and 9 
o'clock (interpalpebral) 
positions and can occur at 
any position on the cornea. 
Slit-lamp examination: 
gelatinous-appearing mass. 
Biopsy: cytological features 
of a squamous cell 
carcinoma, but the basal 
membrane of the 
epithelium remains intact.
Squamous cell 
carcinoma 
Rare. Does not have typical 
pterygium shape. Not restricted 
to the 3 and 9 o'clock 
(interpalpebral) positions and can 
occur at any position on the 
cornea. May arise from a 
pterygium, carcinoma in situ, or 
de novo. 
Slit-lamp examination: 
surface may appear 
keratinised and friable. 
Biopsy: well-differentiated 
squamous cell carcinoma 
with invasion of the basal 
membrane. 
Limbal dermoid Benign choriostomatous tissue. 
MC site:inferior temporal 
quadrant. 
Histology contains 
abberant tissue like 
epidermal 
appendages,connective 
tissue,skin,fatmuscle teeth.
Treatment Options 
Managing the Menace
Historical aspects 
• Susruta,(before 1000 B.C.) 
the Indian physician who 
was the world’s first 
surgeon-ophthalmologist 
described his operative 
procedure, in which he 
combined surgical removal 
with adjunctive chemical 
therapy
• 1953, Rosenthal reviewed surgical treatments 
and stated that pterygia have been “incised, 
removed, split, transplanted, excised, 
cauterized, grafted, inverted, galvanized, 
heated, dissected, rotated, coagulated, 
repositioned and irradiated.”
Treatment 
• Medical Treatment 
– Symptomatic patients- Tear substitutes 
– Inflammation- Topical steroids 
– Sunglasses- to reduce UV exposure and decrease 
growth stimulus
Surgical management 
Indications for Surgery 
1. Extension to the visual axis and induced 
astigmatism. 
2. Recurrent irritation. 
3. Cosmetic- patient should be explained there is 
fairly high risk of recurrence, which may be 
more unsightly.
A variety of pterygium operations illustrated in 
1950 (Archs Ophthal, 1950,Vol. 44)
• Modern pterygium surgery divided into four 
main category 
1. Bare sclera excision 
2. Excision with conjunctival closure/transposition 
3. Excision with antimitotic adjunctive therapies 
4. Ocular surface transplantation techniques
1.Bare sclera excission 
• first described in 1948 by D’Ombrain 
• Principle- leaving a strip of bare sclera allowed the 
cornea, time to heal 
• Recurrence rate range from 24% to 89% 
• Recurrence is highly aggressive 
• Symblepharon, restriction of motility and gaze 
dependent diplopia may occur 
• Complication 
– Scleral thinning 
– Irregular astigmatism 
– Dellen formation at sceral bed
2.Excision with Conjunctival 
Closure/Transposition 
• Bare sclera- does not comply with general 
principles of wound healing and closure 
• Wound closure may be simple approximation 
of undermined conjunctival margins, with or 
without relaxing incisions 
• may be effected by conjunctival transposition 
by a rotational pedicle flap from above or 
below 
• Recurrence rates are similar
3.Excision with Adjunctive Medical 
Therapy 
• Sushruta- introduced chemicals or chemical cautery 
• Radiation therapy- Terson in 1911(radium) 
• Estrada used X-rays 
• Iliff (1947)- employed beta irradiation with the means 
of a radon applicator 
• Beta irradiation 
– Strontium 90 source 
– total doses varying from 2000 rads to 6000 rads 
– Treatment periods - single immediate postoperative dose 
to weekly doses for six weeks after surgery 
– Recurrence rate is around 10%
Beta Irradiation 
• Complications 
– Milder reactions 
– sectoral cataract formation 
– iris atrophy, scleral necrosis 
– Melting 
– Limbal stem cell deficiency 
• Use should be restricted to severe or repeated 
pterygium recurrences with a justifiable risk-benefit 
ratio
Mitomycin C 
• Kunimoto and Mori (1963) reported success with post-operative 
MMC 0.04% 
• inhibits DNA, RNA and protein synthesis 
• 0.01% twice a day for five days 
• Complications - Iritis, limbal avascularity, scleral melting 
or calcific plaque formation, corneal decompensation, 
scleral or corneal perforations, secondary glaucoma and 
cataract 
• surgeons now advocate a single intra-operative 
application of MMC 0.02% 
• Recurrence rate 2.3%
Thiotepa 
• Nitrogen mustard alkylating agent 
antimitotic property 
• Radiomimetic- obliterates vascular endothelial 
cells. 
• Dose:1:2000 every 3 hours for 6 weeks. 
• Used in bare sclera method. 
• Complication: scleral thinning. 
• Recurrence:10-16%
5-fluorouracil 
• Antiproliferative 
• Inhibits thymidylate synthetase, thus inhibits 
DNA. 
• Only cells in the synthesis phase are affected, 
allowing the remaining cells to continue to 
proliferate after exposure to 5-FU.
Cyclosporine A 
• Immunosuppresant drug. 
• Dose: 0.05% topical for 3 months following 
pterygium excision. 
• Safe and effective. 
• Low recurrence rate(3.4%)
Bevacizumab 
• Inhibit neovascularisation. 
• Stop the progression or prevent the 
recurrence. 
• Case reported by Wu and co workers. 
Topical bevacizumab eye drops 25mg/ml 4times 
for 3weeks. 
• No recurrence in 1year follow up period.
4. Ocular Surface Transplantation 
Techniques 
• transplantation procedures currently 
performed are: 
1. Conjunctival autograft transplantation 
2. Modifications of conjunctival autografting: 
a. Conjunctival rotational autografting 
b. Annular conjunctival autografting 
3. Conjunctival limbal autograft 
4. Amniotic membrane transplantation
Conjunctival Autografting(CAU) 
• Now recognized as procedure of choice for pterygium 
surgery in terms of the efficacy and safety 
• Recurrence rate is 2% 
• 1977, Thoft first described the procedure of 
conjunctival transplantation 
• 1931 Gomez-Marquez, utilized superior bulbar 
conjunctiva from the contralateral eye 
• 1985 Keynon proposed the current conjunctival 
autograft transplantation technique 
• low recurrence rate (2%)
Fibrin glue and conjunctival auto graft 
• Mechanism of action: it acts forming a fibrin clot 
between graft and host tissue. 
• Advantages : decreases the post op pain. 
reduces the surgical time as well 
as recurrence rate. 
Disadvantage : not FDA approved. 
graft dehiscence. 
infection, discomfort, cost 
Recurrence rate: less as compared to suture.
CAU-Post operative care 
• Avoid exposure to sunlight. 
• Use of dark sun glasses. 
• Topical steroid antibiotic drops, topical 
NSAIDS, artificial tears.
• Complete healing expected between 6- 
8weeks. 
• Topical medications should be tapered. 
Lubricants should remain for 3months. 
• Instruction to patient: avoid exposure to 
sunlight.
Complications 
• Graft failure. 
• Granuloma formation. 
• Conjunctival infection. 
• Suture detachment. 
• Delayed healing. 
• Recurrence.
Conjuctival limbal autograft (CLAU) 
• Principle- “corneal limbus as the source of 
limbal stem cells responsible for corneal 
epithelial cell maintenance” 
• similar to conjunctival autografting 
• Except that the limbal edge of the donor graft 
is extended to include limbal epithelium 
– superficial keratectomy 
– or by superficial lamellar dissection 
• Recurrence rate is similar or higher as to CAU
Amniotic Membrane Transplantation 
• As an alternative basement membrane substrate 
for use in ocular surface transplantation 
• effective in reducing scarring and fibrosis 
• recently has also been shown to suppress TGF-β 
signaling of fibroblasts 
• Advantages 
– Relatively easy 
– Good cosmetic result 
• Disadvantage 
– less efficient than conjunctival autografting 
(Prabhasawat reported a 13% recurrence rate)
Pterygium Recurrence 
• Growth of fibrovascular tissue across the limbus 
onto cornea after initial removal. 
• Excludes persistence of deeper corneal vessels 
and scarring which may remain even after 
adequate removal. 
• Bunching of conjunctiva and formation of parallel 
loops of vessels, which aim almost like an 
arrowhead at the limbus, usually denotes a 
conjunctival recurrence.
Proposed Recurrence Grading 
System 
• Grade 1 – normal appearing 
operative site. 
• Grade 2 – fine episcleral vessels in 
the site extending to the limbus. 
• Grade 3 – additional fibrous 
tissues in site. 
• Grade 4 – actual corneal 
recurrence.
Excision of Recurrent Pterygia 
• Why different?? 
– subconjunctival fibrous tissue is more abundant and is 
tightly bound to the underlying sclera 
– usually cannot be avulsed from the cornea and, therefore 
must be dissected 
– Important to resect all fibrous tissue and any symblephara 
• Treatment option 
– Superficial keratectomy 
– Deep lamellar keratectomy and inlay graft 
– Adjunctive therapy
Under trial 
• ANECORTANE ACETATE: 
Angiostatic steroid: Inhibits the blood vessels 
Topical 1% have inhibitory effect on pterygium 
regrowth following recurrenr pterygium 
excision.
THANK YOU

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Pterygium and its management

  • 1. Pterygium and its management Dr Jyoti Prakash Behera
  • 3. Histology of normal conjunctiva
  • 4. Pterygium- Definition • Derived from Greek word “Pterygos” means small wing • It is a non malignant slow growing proliferation of wing shaped fibrovascular tissue. • Arises from subconjunctival tissue. • May extend over the cornea thus disturbing the vision.
  • 5. Pterygium- Incidence & Prevalence • Cameron's map- Shows a direct relationship between prevalence and proximity to the equator(warm and dry climate) • Factors other than geographic location – Male : female= 2:1 – more common in farmers than in city dwellers – more who do not wear eyeglasses – elderly have the highest prevalence rate, but a much younger (20-to 40-year old) group has the highest incidence rate
  • 6. • In India prevalence is 9.5%. • Morbidity: causes significant alteration in visual function in advanced cases.
  • 7. ETIOPATHOGENESIS. • Strong association between UV light exposure and formation of pterygium. – More common- in patients who worked outdoors. – In welders than other factory workers. • Also associated with basal cell carcinoma, porphyria cutanea tarda, polymorphous light eruptions, xeroderma pigmentosa.
  • 8. • ANGIOGENESIS FACTOR-(Wong) Prolonged UV exposure causes biological changes in the bowmans membrane • UV Exposure: May induce hyperplasia in limbal cells. These altered cells invade the cornea and limbus which moves centripetally with them
  • 9. ALBEDO HYPOTHESIS • Light entering the temporal limbus at 90degree is concentrated at medial limbus (supported and demonstrated by Coroneo) • Related to corneal curvature. • This explains the predominance of medial pterygium.
  • 10. Other theories • Scarpa, Friede, and Kamel believed that chronic inflammation in the form of conjunctivitis or episcleritis initiates the process • MICROTRAUMA: mechanical irritation by dust particles, enhanced by tear flow from lateral to medial. • IMMUNOLOGY: Cell bound IgE irritant complexes initiate the release of inflammatory mediators from mast cells→ Release of stimulatory factors→Development of pterygium.
  • 11. • HYPOXIA: increase in non perfusion areas and attenuated vessels in nasal limbus during early stage of pterygium causes recruitment of progenitor cells. • Viral markers: infection with HPV and herpes virus is considered as risk factor(rare).
  • 12. Genetic predisposition • Expression of vimentin. • P53 mutation leads to decreased apoptosis and increased TGF-b which leads to increased growth.
  • 13. Pterygium- Degenerative or proliferative ??? • long been considered a chronic degenerative condition • Classically described as“elastotic degeneration” • Cˇilanova-Atanasova ascertained that the degenerative or dystrophic changes in pterygium were simply more pronounced than normal aging conjuctiva • In addition, pterygium tissue had proliferative components that included epithelial hyperplasia and the appearance of newly formed connective tissue, blood vessels and fibrous elements
  • 14. • Cameron- showed the evidence of transformed, invading subconjuctival fibroblasts that grows centripetally • Austin and co-workers suggested- excessive production of elastin material by actinically damaged, proliferative subconjunctival fibroblasts • Primary Pterygium is definitely locally invasive • Also pterygium epithelium exhibits varying degrees of abnormality, ranging from mild dysplasia to carcinoma in situ
  • 15. Limbal Stem Cell Deficiency and Epithelial Abnormalities • Kwok- propose that the initial biologic event in pterygium was an alteration of limbal stem cells due to chronic UV light exposure, resulting in concomitant breakdown of the limbal barrier and subsequent conjunctivalization of the cornea • primary and recurrent pterygia exhibit overexpression of the p53 tumor-suppressor gene • Presence of abberant apoptosis
  • 16. Pterygium-Histopathology • Three basic elements characterize the histologic appearance 1. Epithelial covering of atrophic conjuctiva extends beyond 2. Degenerated connective tissue- a bulky mass of thickened, hypertrophied, and degenerated connective tissue – collagen component of which assumes a coiled, fibrillated pattern reminiscent of elastic tissue – The abnormal collagen shows basophilia and an affinity for elastic tissue stains, but is not digested by elastase – hence categorized as elastotic degeneration
  • 19. 3. Vascular element- New blood vessels, usually congested, are dispersed among the hypertrophied collagen fibers • The episcleral bed beneath the pterygium is hyperemic • Tenon’s capsule is incorporated into the body of the pterygium and contributes to its vasculature and bulk
  • 20. Histopathology cont.. • Immediately in front of the head of the pterygium, an advancing row of fibroblasts penetrates the cornea between Bowman’s layer and the basement membrane of the epithelium (grey zone or cap) • Eventually tissue enters the cornea, Bowman's layer is pushed posteriorly and eventually becomes fragmented
  • 22. Pterygium- Clinical feature • A pterygium appears as a fleshy triangular band of fibrovascular tissue • axis of the triangle gently slopes superiorly on the corneal side • It has several components – The cap – The head – The body – The base – Superior edge – Inferior edge
  • 23. • The cap – The cap is a flat, grayish white avascular zone of variable size located in the subepithelial corneal tissue – Sometimes a round, gray, coin-like extensions of the cap precede it (“islets of Fuchs") – some cases, a golden-yellow iron line may be seen (Stocker's line) – Between the head and the cap there are small capillaries
  • 24. Islets of Fuch’s Stocker's line
  • 25. • The head – It is slightly elevated and white – It is the one site of firm adhesion to the globe • The body – fleshy sheet of pink, highly vascularized tissue – delineated from the normal conjunctiva superiorly and inferiorly by sharp folds – frequently reveals punctate staining over the epithelial surface of the body
  • 26. • Clinical Grading of pterygium • As proposed by Donald T H Tan • Grade T1(atrophic)- pterygium in which episcleral vessels underlying the body of the pterygium were unobscured and clearly distinguished
  • 27. • Grade T3(fleshy)- thick pterygium in which episcleral vessels underlying the body of the pterygium are totally obscured by fibrovascular tissue • Grade T2(intermediate)- All other pterygia that do not fall into these two categories
  • 28. • Surgical recurrence correlated well with translucency – fleshy pterygium having the highest capacity for recurrence – Atrophic has the lowest
  • 29. Clinical staging of pterygium CLINICAL STAGING PATHOLOGICAL STAGING Stage I Exposure conjunctivitis Size and number of Conjunctival vessels Mild – moderate congestion S/S of dryness No formed lesions Altered tear film Mild vascular response Stage II Pinguecula and pterygium Distinct raised lesion on bulbar conjunctiva With or w/o abnormal vascularization and inflammation Cell injury Inflammatory response
  • 30. Stage III Limbal pterygium Head is on or across the limbus with or w/o an iron line at the conjunctival corneal interface Vascularization and fibrous proliferation Symptoms more pronounced Lesion organization Mixed proliferation and degeneration Stage IV Corneal pterygium Lesion 2mm or more into cornea Invasion of granulation tissue Zone of dellen Stocker’s line Infiltration of corneal nerves- pain Lesion b/w epithelium and bowman Mixed proliferative and degeneration
  • 31. Stage V Compound pterygium Induced astigmatism Symptoms more frequent and severe Lesion extended into stroma Mixed proliferative and degeneration Proliferation- Small lymphocytes and plasma cells Degeneration- Swirls of type I collagen
  • 32. Other types • Primary double pterygium. • Recurrent pterygium. • Pseudopterygium. • Malignant pterygium(rare):recurrent pterygium with restriction of ocular movements.
  • 33. Symptoms • Asymptomatic • Foreign body sensation • Discomfort • Congestion(redness) • Irritation and grittiness-interference with precorneal tear film. • Interference with vision-obscuring visual axis -inducing astigmatism(WTR) • Cosmesis • Diplopia
  • 34. Differential diagnosis Condition Signs and symptoms Tests Pseudopterygium Most often hx of previous infective, chemical, thermal, or traumatic injury to the cornea. May occur at multiple locations and is not restricted to the 3 and 9 o'clock (interpalpebral) positions. -Slit-lamp examination: reveals lesion to be adhesion of a fold of conjunctiva, which has occurred as a response to a previous peripheral corneal ulcer/inflammation. -Lesion typically only fixed at its apex to the cornea so that a probe may be passed underneath its body at the limbus, while a true pterygium adheres to the underlying cornea throughout its length. Thinning of the underlying cornea may be seen at its head.
  • 35. Pinguecula Does not encroach on the cornea. Slit-lamp examination: reveals exact extent and nature of lesion. A pingueculum is limited to limbus and conjunctiva and does not encroach onto the cornea. Marginal keratitis Associated with blepharitis. Infiltrate on corneal surface is separated by a clear zone from the limbus. Occur at 2, 4, 8, and 10 o'clock position. Does not have typical pterygium shape. Often superior and inferior. Corneal swab/scraping: microscopy and culture positive for infecting organism, but infecting organisms are often not detected, as many cases are due to an inflammatory reaction to staphylococcal proteins
  • 36. Corneal micropannus Hx of trachoma or lack of corneal oxygenation due to excessive contact lens wear. Slit-lamp examination: reveals encroachment of fine blood vessels onto corneal surface. Conjunctival carcinoma in situ/ bowens epithlioma. Rare. Does not have typical pterygium shape. Not restricted to the 3 and 9 o'clock (interpalpebral) positions and can occur at any position on the cornea. Slit-lamp examination: gelatinous-appearing mass. Biopsy: cytological features of a squamous cell carcinoma, but the basal membrane of the epithelium remains intact.
  • 37. Squamous cell carcinoma Rare. Does not have typical pterygium shape. Not restricted to the 3 and 9 o'clock (interpalpebral) positions and can occur at any position on the cornea. May arise from a pterygium, carcinoma in situ, or de novo. Slit-lamp examination: surface may appear keratinised and friable. Biopsy: well-differentiated squamous cell carcinoma with invasion of the basal membrane. Limbal dermoid Benign choriostomatous tissue. MC site:inferior temporal quadrant. Histology contains abberant tissue like epidermal appendages,connective tissue,skin,fatmuscle teeth.
  • 39. Historical aspects • Susruta,(before 1000 B.C.) the Indian physician who was the world’s first surgeon-ophthalmologist described his operative procedure, in which he combined surgical removal with adjunctive chemical therapy
  • 40. • 1953, Rosenthal reviewed surgical treatments and stated that pterygia have been “incised, removed, split, transplanted, excised, cauterized, grafted, inverted, galvanized, heated, dissected, rotated, coagulated, repositioned and irradiated.”
  • 41. Treatment • Medical Treatment – Symptomatic patients- Tear substitutes – Inflammation- Topical steroids – Sunglasses- to reduce UV exposure and decrease growth stimulus
  • 42. Surgical management Indications for Surgery 1. Extension to the visual axis and induced astigmatism. 2. Recurrent irritation. 3. Cosmetic- patient should be explained there is fairly high risk of recurrence, which may be more unsightly.
  • 43. A variety of pterygium operations illustrated in 1950 (Archs Ophthal, 1950,Vol. 44)
  • 44. • Modern pterygium surgery divided into four main category 1. Bare sclera excision 2. Excision with conjunctival closure/transposition 3. Excision with antimitotic adjunctive therapies 4. Ocular surface transplantation techniques
  • 45. 1.Bare sclera excission • first described in 1948 by D’Ombrain • Principle- leaving a strip of bare sclera allowed the cornea, time to heal • Recurrence rate range from 24% to 89% • Recurrence is highly aggressive • Symblepharon, restriction of motility and gaze dependent diplopia may occur • Complication – Scleral thinning – Irregular astigmatism – Dellen formation at sceral bed
  • 46. 2.Excision with Conjunctival Closure/Transposition • Bare sclera- does not comply with general principles of wound healing and closure • Wound closure may be simple approximation of undermined conjunctival margins, with or without relaxing incisions • may be effected by conjunctival transposition by a rotational pedicle flap from above or below • Recurrence rates are similar
  • 47. 3.Excision with Adjunctive Medical Therapy • Sushruta- introduced chemicals or chemical cautery • Radiation therapy- Terson in 1911(radium) • Estrada used X-rays • Iliff (1947)- employed beta irradiation with the means of a radon applicator • Beta irradiation – Strontium 90 source – total doses varying from 2000 rads to 6000 rads – Treatment periods - single immediate postoperative dose to weekly doses for six weeks after surgery – Recurrence rate is around 10%
  • 48. Beta Irradiation • Complications – Milder reactions – sectoral cataract formation – iris atrophy, scleral necrosis – Melting – Limbal stem cell deficiency • Use should be restricted to severe or repeated pterygium recurrences with a justifiable risk-benefit ratio
  • 49. Mitomycin C • Kunimoto and Mori (1963) reported success with post-operative MMC 0.04% • inhibits DNA, RNA and protein synthesis • 0.01% twice a day for five days • Complications - Iritis, limbal avascularity, scleral melting or calcific plaque formation, corneal decompensation, scleral or corneal perforations, secondary glaucoma and cataract • surgeons now advocate a single intra-operative application of MMC 0.02% • Recurrence rate 2.3%
  • 50. Thiotepa • Nitrogen mustard alkylating agent antimitotic property • Radiomimetic- obliterates vascular endothelial cells. • Dose:1:2000 every 3 hours for 6 weeks. • Used in bare sclera method. • Complication: scleral thinning. • Recurrence:10-16%
  • 51. 5-fluorouracil • Antiproliferative • Inhibits thymidylate synthetase, thus inhibits DNA. • Only cells in the synthesis phase are affected, allowing the remaining cells to continue to proliferate after exposure to 5-FU.
  • 52. Cyclosporine A • Immunosuppresant drug. • Dose: 0.05% topical for 3 months following pterygium excision. • Safe and effective. • Low recurrence rate(3.4%)
  • 53. Bevacizumab • Inhibit neovascularisation. • Stop the progression or prevent the recurrence. • Case reported by Wu and co workers. Topical bevacizumab eye drops 25mg/ml 4times for 3weeks. • No recurrence in 1year follow up period.
  • 54. 4. Ocular Surface Transplantation Techniques • transplantation procedures currently performed are: 1. Conjunctival autograft transplantation 2. Modifications of conjunctival autografting: a. Conjunctival rotational autografting b. Annular conjunctival autografting 3. Conjunctival limbal autograft 4. Amniotic membrane transplantation
  • 55. Conjunctival Autografting(CAU) • Now recognized as procedure of choice for pterygium surgery in terms of the efficacy and safety • Recurrence rate is 2% • 1977, Thoft first described the procedure of conjunctival transplantation • 1931 Gomez-Marquez, utilized superior bulbar conjunctiva from the contralateral eye • 1985 Keynon proposed the current conjunctival autograft transplantation technique • low recurrence rate (2%)
  • 56. Fibrin glue and conjunctival auto graft • Mechanism of action: it acts forming a fibrin clot between graft and host tissue. • Advantages : decreases the post op pain. reduces the surgical time as well as recurrence rate. Disadvantage : not FDA approved. graft dehiscence. infection, discomfort, cost Recurrence rate: less as compared to suture.
  • 57. CAU-Post operative care • Avoid exposure to sunlight. • Use of dark sun glasses. • Topical steroid antibiotic drops, topical NSAIDS, artificial tears.
  • 58. • Complete healing expected between 6- 8weeks. • Topical medications should be tapered. Lubricants should remain for 3months. • Instruction to patient: avoid exposure to sunlight.
  • 59. Complications • Graft failure. • Granuloma formation. • Conjunctival infection. • Suture detachment. • Delayed healing. • Recurrence.
  • 60. Conjuctival limbal autograft (CLAU) • Principle- “corneal limbus as the source of limbal stem cells responsible for corneal epithelial cell maintenance” • similar to conjunctival autografting • Except that the limbal edge of the donor graft is extended to include limbal epithelium – superficial keratectomy – or by superficial lamellar dissection • Recurrence rate is similar or higher as to CAU
  • 61. Amniotic Membrane Transplantation • As an alternative basement membrane substrate for use in ocular surface transplantation • effective in reducing scarring and fibrosis • recently has also been shown to suppress TGF-β signaling of fibroblasts • Advantages – Relatively easy – Good cosmetic result • Disadvantage – less efficient than conjunctival autografting (Prabhasawat reported a 13% recurrence rate)
  • 62. Pterygium Recurrence • Growth of fibrovascular tissue across the limbus onto cornea after initial removal. • Excludes persistence of deeper corneal vessels and scarring which may remain even after adequate removal. • Bunching of conjunctiva and formation of parallel loops of vessels, which aim almost like an arrowhead at the limbus, usually denotes a conjunctival recurrence.
  • 63. Proposed Recurrence Grading System • Grade 1 – normal appearing operative site. • Grade 2 – fine episcleral vessels in the site extending to the limbus. • Grade 3 – additional fibrous tissues in site. • Grade 4 – actual corneal recurrence.
  • 64. Excision of Recurrent Pterygia • Why different?? – subconjunctival fibrous tissue is more abundant and is tightly bound to the underlying sclera – usually cannot be avulsed from the cornea and, therefore must be dissected – Important to resect all fibrous tissue and any symblephara • Treatment option – Superficial keratectomy – Deep lamellar keratectomy and inlay graft – Adjunctive therapy
  • 65. Under trial • ANECORTANE ACETATE: Angiostatic steroid: Inhibits the blood vessels Topical 1% have inhibitory effect on pterygium regrowth following recurrenr pterygium excision.