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Polypoidal Choroidal
Vasculopathy
Dr. Md Mominul Islam
Fellow Vitreo - Retina
Introduction
 PCV is an exudative maculopathy with features similar
to neovascular AMD with hemorrhage, pigment
epithelium detachment and neurosensory
detachment.
 Pathogenesis mostly unknown
 It remains controverial as to weather PCV represents a
sub type of neovascular AMD
History
• In 1982 By Yannuzzi et al
• At annual meeting of American academy of
ophthalmology as :-
 Polypoidal , subretinal, vascular lesions associated
with serous and hemorrhagic detachments of the RPE
in a series of patients (10/11 patients were woman).
 The entitity was initially called Idiopathic
polypoidal choroidal vasculopathy.
History (contd) In 1984 Kleiner et al Described as:-
 A peculiar hemorrhagic disorder of the macula and
sub retinal pigment epithelium bleeding in middle
aged black woman ,which they term posterior uveal
bleeding syndrome.
 Later a study from the same group of authors showed
an expanded clinical spectrum for PCV
Pathogenesis
 It is a primary abnormality of the choroidal
circulation, characterized by :-
 An inner choroidal vascular network of vessels ending
in an aneurysmal bulged or outward projection often
visible as a reddish – orange, spheroid ,polyp like
structure.
 PCV primarily involves the inner choroidal vasculature
that is well differentiated from the middle and larger
choroidal vessels by histology.
Histopathological Features
 Kuroiwa reported from surgically excised specimens
from 5 patients with PCV had been diagnosed by ICGA
:--
 Results - arteriosclerosis appears to be an important
pathological feature in the choroidal vessels of PCV
subjects.
Histopathological Features (Contd)
In another histopathologic group :
• Nakashizuka et al, who also examined from surgically
excised specimens from 5 patients with PCV
Results :- little granulation tissue from any of the
specimens.
On the other hand all the specimen exhibited:-
• Massive exudative change and leaking ,all the vessels
exhibited hyalinization and chorio-capillaris had
disappeared ,in which RPE had been preserved.
Immuno ChemistryThis group demonstrated that :
• PCV is not the same as choroidal neovascularization.
• CD-34 is a marker of vascular endothelial growth factor
• CD-34 staining revealed
 Discontinuity in the vascular
endothelium.
 Smooth muscle actin was negative in
hyalinized vessels
 There was disruption and injury of
smooth cells causing dilation of vessels
Demography
Prevalence of PCV in presumed neovascular AMD
• US -7.8%
• Belgian – 4.0%
• Italian - 9.8 %
• Greek – 8.2%
• Japanese – 23.0-54.7%
• Chinese – 22.3%
• Korean – 24.6%
Demography (contd)
 Varies with age
 Predominantly middle aged ,one or two decade earlier
than classical AMD
 Commonly occur both gender ( more in Asian man
than woman)
 More prevalent in black, Japanese and other Asian
than in white.
 Incidence is high in Asian.
Course
Natural course of disease is Variable:-
 May be relatively stable
 May repeated bleeding and leakage with vision loss and
chorioretinal atrophy
 With or without fibroitic scarring
 Reddish- orange nodules alone or nodule and small sub-
retinal hemorrhage and absence of hard exudates.
 May association with other condition like
thrombocytopenia and massive hemorrhage has been
reported
 Also association with sickle cell disease and irradiation.
Clinical feature Usually bilateral
 Protruding orange –red elevated lesion often with
nodular elevations of RPE.
 Also described as –
 Polypoidal lesion ,polyp like or grasp like
 Association serous exudation and hemorrhage
, that may lead to detachment of the RPE and
sometimes neurosensory retina
 Sometime associated features recurrent
hemorrhage and vitreous hemorrhage.
Clinical feature (contd)
Location of the lesion:
 In the macular area -69.5%
 Under the temporal retinal vascular arcade
15%
 Peripapillary area (within one disc
diameter of disc edge -4.5%.
 Also mid peripheral area
Clinical feature (contd)Lesions may active or inactive.
• Lesions considered as active on the evidence of
clinical, OCT, FFA any one of the following:
1. Vision loss of 5 or more letters (ETDRS
chart)
2. Subretinal fluid with or without
intraretinal fluid.
3. PED
4. Subretinal hemorrhage or fluorescence
leakage.
ICGA :-
• Accepted as the gold standared for diagnosis of PCV.
• Better visualization in ICGA than FFA
 ICG absorbs and
emit near infrared
light, which readily
penetrates the RPE
and enhancing veiwing
of choroidal lesions
 ICG binding affinity
with plasma
proteins, that means –
it does not leak from
chorio-capillaries in the
same way as
fluorescence, so
choroidal lesions are
less obscured.
Characteristics feature of PCV in ICGA:-
 A branching network of inner choroidal vessels.
 Nodular polypoidal aneurysm or dilations at the edge
of these abnormal vessels network, which correspond
to orange sub-retinal nodules.
 Presence of single or multiple focal nodular areas of
hyperfluorescence arising from choroidal circulation
within the first 6 minutes
Classification
According to Japanese group on PCV
Quiescent: Polyps in the absence of subretinal or intraretinal fluid
or hemorrhage.
Exudative : Exudation without hemorrhage, which may include
sensory retinal thickening, Neuro-sensory retinal
detachment, PED, subretinal lipid exudation.
Hemorrhagic: Any hemorrhage with or without other exudative
characteristics
Differential Diagnosis
 AMD
 CSCR
Treatment
Thermal laser Photocoagulation:
To be beneficial ,albeit it with short term follow up
and for extra foveal lesion.
In some studies
 Improve and stabilize vision- in 55-100%
 Vision loss – in 13-45%
 Whole lesion compared with polyps only appears to
be more efficacious.
Photodynamic therapy:
 Regression or resolution of the polyp by in angio
occlusive mechanism of action
 Restrict loss of letters on ETDRS chart to less than
15 letters or improved vision 80-100% patient after 1
year.
Anti VEGF therapy:
 Intravitreal Ranibizumab resolving the macular
oedema, polypoidal complexes decreased in 4/12 (33%)
eyes.
 Intravitreal Bevacizumab 1/11 (9.09%) eyes
Combination therapy:
 Both combination therapy and vertiporfin PDT
monotherapy superior to ranibizumab monotherapy
in achieving complete polyp regression at 6 months.
 Improvement in BCVA and central retinal thickness
also favored combination therapy.
THANK YOU

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Polypoidal Choroidal

  • 1. Polypoidal Choroidal Vasculopathy Dr. Md Mominul Islam Fellow Vitreo - Retina
  • 2. Introduction  PCV is an exudative maculopathy with features similar to neovascular AMD with hemorrhage, pigment epithelium detachment and neurosensory detachment.  Pathogenesis mostly unknown  It remains controverial as to weather PCV represents a sub type of neovascular AMD
  • 3.
  • 4. History • In 1982 By Yannuzzi et al • At annual meeting of American academy of ophthalmology as :-  Polypoidal , subretinal, vascular lesions associated with serous and hemorrhagic detachments of the RPE in a series of patients (10/11 patients were woman).  The entitity was initially called Idiopathic polypoidal choroidal vasculopathy.
  • 5. History (contd) In 1984 Kleiner et al Described as:-  A peculiar hemorrhagic disorder of the macula and sub retinal pigment epithelium bleeding in middle aged black woman ,which they term posterior uveal bleeding syndrome.  Later a study from the same group of authors showed an expanded clinical spectrum for PCV
  • 6. Pathogenesis  It is a primary abnormality of the choroidal circulation, characterized by :-  An inner choroidal vascular network of vessels ending in an aneurysmal bulged or outward projection often visible as a reddish – orange, spheroid ,polyp like structure.  PCV primarily involves the inner choroidal vasculature that is well differentiated from the middle and larger choroidal vessels by histology.
  • 7. Histopathological Features  Kuroiwa reported from surgically excised specimens from 5 patients with PCV had been diagnosed by ICGA :--  Results - arteriosclerosis appears to be an important pathological feature in the choroidal vessels of PCV subjects.
  • 8. Histopathological Features (Contd) In another histopathologic group : • Nakashizuka et al, who also examined from surgically excised specimens from 5 patients with PCV Results :- little granulation tissue from any of the specimens. On the other hand all the specimen exhibited:- • Massive exudative change and leaking ,all the vessels exhibited hyalinization and chorio-capillaris had disappeared ,in which RPE had been preserved.
  • 9. Immuno ChemistryThis group demonstrated that : • PCV is not the same as choroidal neovascularization. • CD-34 is a marker of vascular endothelial growth factor • CD-34 staining revealed  Discontinuity in the vascular endothelium.  Smooth muscle actin was negative in hyalinized vessels  There was disruption and injury of smooth cells causing dilation of vessels
  • 10. Demography Prevalence of PCV in presumed neovascular AMD • US -7.8% • Belgian – 4.0% • Italian - 9.8 % • Greek – 8.2% • Japanese – 23.0-54.7% • Chinese – 22.3% • Korean – 24.6%
  • 11. Demography (contd)  Varies with age  Predominantly middle aged ,one or two decade earlier than classical AMD  Commonly occur both gender ( more in Asian man than woman)  More prevalent in black, Japanese and other Asian than in white.  Incidence is high in Asian.
  • 12. Course Natural course of disease is Variable:-  May be relatively stable  May repeated bleeding and leakage with vision loss and chorioretinal atrophy  With or without fibroitic scarring  Reddish- orange nodules alone or nodule and small sub- retinal hemorrhage and absence of hard exudates.  May association with other condition like thrombocytopenia and massive hemorrhage has been reported  Also association with sickle cell disease and irradiation.
  • 13. Clinical feature Usually bilateral  Protruding orange –red elevated lesion often with nodular elevations of RPE.  Also described as –  Polypoidal lesion ,polyp like or grasp like  Association serous exudation and hemorrhage , that may lead to detachment of the RPE and sometimes neurosensory retina  Sometime associated features recurrent hemorrhage and vitreous hemorrhage.
  • 14. Clinical feature (contd) Location of the lesion:  In the macular area -69.5%  Under the temporal retinal vascular arcade 15%  Peripapillary area (within one disc diameter of disc edge -4.5%.  Also mid peripheral area
  • 15. Clinical feature (contd)Lesions may active or inactive. • Lesions considered as active on the evidence of clinical, OCT, FFA any one of the following: 1. Vision loss of 5 or more letters (ETDRS chart) 2. Subretinal fluid with or without intraretinal fluid. 3. PED 4. Subretinal hemorrhage or fluorescence leakage.
  • 16. ICGA :- • Accepted as the gold standared for diagnosis of PCV. • Better visualization in ICGA than FFA  ICG absorbs and emit near infrared light, which readily penetrates the RPE and enhancing veiwing of choroidal lesions  ICG binding affinity with plasma proteins, that means – it does not leak from chorio-capillaries in the same way as fluorescence, so choroidal lesions are less obscured.
  • 17. Characteristics feature of PCV in ICGA:-  A branching network of inner choroidal vessels.  Nodular polypoidal aneurysm or dilations at the edge of these abnormal vessels network, which correspond to orange sub-retinal nodules.  Presence of single or multiple focal nodular areas of hyperfluorescence arising from choroidal circulation within the first 6 minutes
  • 18.
  • 19.
  • 20. Classification According to Japanese group on PCV Quiescent: Polyps in the absence of subretinal or intraretinal fluid or hemorrhage. Exudative : Exudation without hemorrhage, which may include sensory retinal thickening, Neuro-sensory retinal detachment, PED, subretinal lipid exudation. Hemorrhagic: Any hemorrhage with or without other exudative characteristics
  • 22. Treatment Thermal laser Photocoagulation: To be beneficial ,albeit it with short term follow up and for extra foveal lesion. In some studies  Improve and stabilize vision- in 55-100%  Vision loss – in 13-45%  Whole lesion compared with polyps only appears to be more efficacious.
  • 23.
  • 24. Photodynamic therapy:  Regression or resolution of the polyp by in angio occlusive mechanism of action  Restrict loss of letters on ETDRS chart to less than 15 letters or improved vision 80-100% patient after 1 year.
  • 25. Anti VEGF therapy:  Intravitreal Ranibizumab resolving the macular oedema, polypoidal complexes decreased in 4/12 (33%) eyes.  Intravitreal Bevacizumab 1/11 (9.09%) eyes
  • 26. Combination therapy:  Both combination therapy and vertiporfin PDT monotherapy superior to ranibizumab monotherapy in achieving complete polyp regression at 6 months.  Improvement in BCVA and central retinal thickness also favored combination therapy.