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26/02/2008
   Only place in the body where blood vessels can
    be visualized directly
   Mirror the status of the systemic circulation
   Continuity of nerve fibers and meninges
   Reflects specific changes in systemic diseases
   Contribute to diagnosis
   Direct ophthalmoscopy




   Indirect opthalmoscopy
      Sterioscopical view possible
   Ideally fundus should be examined
    in a darkened room
   Patient should be asked to fix their gaze on a
    distant object
   Examine with corresponding eyes
   The ideal line of approach should bring the
    optic disc straight in to view
   If only blood vessels on a pink background are
    seen they should be followed , the disk will
    eventually come in to view
   Media- hazy, clear
   Disc- size, shape, colour, margin, physiological
    cup, neuroretinal rim
   Blood vessels- caliber, tortousity, irregularities,
    changes in the vessel wall, aneurism,
    neovascularisation
   Exudates
   Haemorrhage
   Uniform red to pink
   Disc-pale pink
   1.5 mm in diameter
   Nasal margin slightly blurred
   Vessels emanate from optic cup
   Consist of central cup and
    peripheral neuroretinal rim
   Macula temporally
   Fovea 2.5mm-diameter, darker
   Uniform red to pink
   Disc-pale pink
   1.5 mm in diameter
   Nasal margin slightly blurred
   Vessels emanate from optic cup
   Consist of central cup and
    peripheral neuroretinal rim
   Macula temporally
   Fovea 2.5mm-diameter, darker
   Uniform red to pink
   Disc-pale pink
   1.5 mm in diameter
   Nasal margin slightly blurred
   Vessels emanate from optic cup
   Consist of central cup and
    peripheral neuroretinal rim
   Macula temporally
   Fovea 2.5mm-diameter, darker
   Uniform red to pink
   Disc-pale pink
   1.5 mm in diameter
   Nasal margin slightly blurred
   Vessels emanate from optic cup
   Consist of central cup and
    peripheral neuroretinal rim
   Macula temporally
   Fovea 2.5mm-diameter, darker
   Uniform red to pink
   Disc-pale pink
   1.5 mm in diameter
   Nasal margin slightly blurred
   Vessels emanate from optic cup
   Consist of central cup and
    peripheral neuroretinal rim
   Macula temporally
   Fovea 2.5mm-diameter, darker
   Uniform red to pink
   Disc-pale pink
   1.5 mm in diameter
   Nasal margin slightly blurred
   Vessels emanate from optic cup
   Consist of central cup and
    peripheral neuroretinal rim
   Macula temporally
   Fovea 2.5mm-diameter, darker
   Uniform red to pink
   Disc-pale pink
   1.5 mm in diameter
   Nasal margin slightly blurred
   Vessels emanate from optic cup
   Consist of central cup and
    peripheral neuroretinal rim
   Macula temporally
   Fovea 2.5mm-diameter, darker
   Uniform red to pink
   Disc-pale pink
   1.5 mm in diameter
   Nasal margin slightly blurred
   Vessels emanate from optic cup
   Consist of central cup and
    peripheral neuroretinal rim
   Macula temporally
   Fovea 2.5mm-diameter, darker
   Tygroid fundus
   Deeply pigmented choroid
   Choroidal vessels are seen
   Polygonal pigmented areas
    in between
   Dot haemorrhages
     Deep within the retina
     Leakage of capillaries, venules
     Common in diabetes

   Flame haemorrhages
     Superficial nerve fibre layer
     Leakage of capillaries, venules
      that are ischemic or, in the case of
      veins, under high pressure
   Boat haemorrhages (pre-retinal)
       Interface between retina & vitreous
   Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
   Dot haemorrhages
     Deep within the retina
     Leakage of capillaries, venules
     Common in diabetes

   Flame haemorrhages
     Superficial nerve fibre layer
     Leakage of capillaries, venules
      that are ischemic or, in the case of
      veins, under high pressure
   Boat haemorrhages (pre-retinal)
       Interface between retina & vitreous
   Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
   Dot haemorrhages
     Deep within the retina
     Leakage of capillaries, venules
     Common in diabetes

   Flame haemorrhages
     Superficial nerve fibre layer
     Leakage of capillaries, venules
      that are ischemic or, in the case of
      veins, under high pressure
   Boat haemorrhages (pre-retinal)
       Interface between retina & vitreous
   Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
   Dot haemorrhages
     Deep within the retina
     Leakage of capillaries, venules
     Common in diabetes

   Flame haemorrhages
     Superficial nerve fibre layer
     Leakage of capillaries, venules
      that are ischemic or, in the case of
      veins, under high pressure
   Boat haemorrhages (pre-retinal)
       Interface between retina & vitreous
   Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
   Dot haemorrhages
     Deep within the retina
     Leakage of capillaries, venules
     Common in diabetes

   Flame haemorrhages
     Superficial nerve fibre layer
     Leakage of capillaries, venules
      that are ischemic or, in the case of
      veins, under high pressure
   Boat haemorrhages (pre-retinal)
       Interface between retina & vitreous
   Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
   Dot haemorrhages
     Deep within the retina
     Leakage of capillaries, venules
     Common in diabetes

   Flame haemorrhages
     Superficial nerve fibre layer
     Leakage of capillaries, venules
      that are ischemic or, in the case of
      veins, under high pressure
   Boat haemorrhages (pre-retinal)
       Interface between retina & vitreous
   Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
   Hard exudate
     Deep yellow with sharp margins
     Often circinate
     Leakage from pre-capillary arterioles
     DM, HTN, VHL disease, radiation
     „Macular star‟

   Soft exudate(cotton wool spot)
     Fluffygray-white, near optic disc
     Retinal nerve fiber layer microinfarction
     HTN, DM, connective tissue disease,HIV
   Hard exudate
     Deep yellow with sharp margins
     Often circinate
     Leakage from pre-capillary arterioles
     DM, HTN, VHL disease, radiation
     „Macular star‟

   Soft exudate(cotton wool spot)
     Fluffygray-white, near optic disc
     Retinal nerve fiber layer microinfarction
     HTN, DM, connective tissue disease,HIV
   Hard exudate
     Deep yellow with sharp margins
     Often circinate
     Leakage from pre-capillary arterioles
     DM, HTN, VHL disease, radiation
     „Macular fan‟

   Soft exudate(cotton wool spot)
     Fluffygray-white, near optic disc
     Retinal nerve fiber layer microinfarction
     HTN, DM, connective tissue disease,HIV
   White centered retinal haemorrhages
   CWS surrounded by h‟mage
   CWS- ischaemic axons
   H‟maghe- precapillary arterioles
   Sub acute bacterial endocarditis
   Leukaemia
   Diabetes
   Deposition in ganglion cell layer
   Thickening & loss of
    transparency of retina
   Foveola-ganglion cells absent,
    thin, so contrast
   Sphingolipidoses
   Central retinal artery occlusion
   Berlins edema
   Crack like dehiscence in brusch‟ membrane
   Degenerative process combined with calcium
    deposition
   Linear reddish brown lesion
   Lies beneath normal blood vessels
   “Pseu d‟orange”
   Salmon spots, optic nerve drusen
   Pseudoxanthoma elasticum, EDS
   Paget‟s, Hemoglobinopathies
   Papillopheblitis (optic disc vasculitis)
     Affects healthyindividuals <50
     Disc edema, cotton wool spots
     Venous dilatation and tortousity
     Retinal haemorrhages
   Retinal vasculitis
     Occurs in sarcoidosis, Behcet‟s disease,
      Multiple sclerosis, idiopathic
     Extremely rare in lupus
     Perivenous lymphocytic infiltration
      (sheathing)
   Diffuse retinal dystrophy(rods)
   Classic clinical triad
     Arteriolarattenuation
     Retinal bone-spicule pigmentation
     Waxy disc pallor
   Starts at mid periphery
   Maculopathy
   Associations
     Bassen-Kornzwieg   syndrome,
      Refsum‟s disease, Kearn-sayre
      syndrome , Usher‟s syndrome
      Muchopolysaccharidoses, Lauren‟s
      moon biedel syndrome, Friederisch
      ataxia
   Attempt at vascularising ischaemic tissue
   Lacks bifurcating pattern
   Bleed spontaneously
   Diabetic retinopathy
   Retinal vein occlusion
   Radiation
   Sickle cell retinopathy
   Retinopathy of prematurity
   Separation of sensory retina from
    pigment epithelium
   Rhegmatogenous RD
   Non-rhegmatogenous RD
     Tractional- PDR, ROP, sickle cell
      retinopathy, penetrating posterior
      segment trauma
     Exudative- choroidal tumours,
      exophytic retinoblastoma, harada
      disease, posterior scleritis, subretinal
      neovascularisation, severe
      hypertension
   Elevated sheath of retinal tissue
    with folds
   Separation of sensory retina from
    pigment epithelium
   Rhegmatogenous RD
   Non-rhegmatogenous RD
     Tractional- PDR, ROP, sickle cell
      retinopathy, penetrating posterior
      segment trauma
     Exudative- choroidal tumours,
      exophytic retinoblastoma, harada
      disease, posterior scleritis, subretinal
      neovascularisation, severe
      hypertension
   Elevated sheath of retinal tissue
    with folds
   Atherosclerosis, embolism
   Retina appears white
   Attenuation of arteries and
    veins
   Cherry red spot
   Investigate for
   Valvular heart disease,
    endocarditis, mural thrombi,
    Carotid artery disease, systemic
    vasculitis, hematological
    disorders
Cholesterol       Fibrinoplatelet   Calcific
(Hollenhorst plaques)
   Atherosclerosis, embolism
   Retina appears white
   Attenuation of arteries and
    veins
   Cherry red spot
   Investigate for
    Valvular heart disease,
    endocarditis, mural thrombi,
    Carotid artery disease, systemic
    vasculitis, hematological
    disorders
   Atherosclerosis, embolism          Cattle-trucking
   Retina appears white
   Attenuation of arteries and
    veins
   Cherry red spot
   Investigate for
    Valvular heart disease,
    endocarditis, mural thrombi,
    Carotid artery disease, systemic
    vasculitis, hematological
    disorders
   Embolism, periarteritis
   Retinal cloudiness
    corresponding to the areas of
    ischemia
   Narrowing of arteries and
    veins
   One or more emboli may be
    present
   Present in 20% of population
   It may be isolated, combined
    CRVO, combined AION
   Localised cloudiness- macula
    and papillomacular bundle
   Occlusion of short posterior ciliary arteries
   Disc is pale
   Diffuse or sectoral edema
   Splinter shaped h‟mages
   „Pseudo-Foster kennedy syndrome‟
   Giant cell arteritis
   Cotton wool spots are uncommon
   Cilioretinal artery occlusion
   Central artery occlusion
   Etiology
    Arteriosclerosis
    Increasing age
    Hypertension
    Diabetes mellitus
    Blood dyscrasiasis
    Periphlebitis
    Raised intraocular tension
   Dilatation & tortousity
    of all branches of CRV
   Retinal h‟age- superficial
    & deep throughout
   “Blood and thunder”
   Cotton wool spots
   Optic disc edema
   Macular edema
   Venous dilatation and
    tortousity peripheral to
    the site of occlusion
   Hemorrhages
   Retinal edema
   Cotton wool spots
   Neovascularisation
   Most common cause of legal blindness in 20-65 yrs
   Type 1>Type 2 (40% , 20%)
   Risk factors
     Duration of diabetes
     Poor metabolic control
     Pregnancy
     Hypertension
     Nephropathy
     Smocking
     Obesity
     Hyperlipidaemia
   Micro vascular occlusion      Microvascular leakage
Eva kohner‟s classification

   Non-proliferative diabetic retinopathy
   Pre-proliferative diabetic retinopathy
   Proliferative diabetic retinopathy
   Micro aneurysms
    (earliest lesion)
   Hard exudates
   Retinal edema
   Haemorrhages
   Cotton wool spots
   Intra retinal micro vascular abnormalities(IRMA)
   Venous changes
     Dilatation,looping
     Beading, segmentation

   Arterial changes
     Narrowing,  occlusion
     Silver wiring

   Dark blot haemorrhages
   Involvement of fovea
   Perifoveal hard exudates
   Dark blot hemorrhages
Neovascularisation
                           Venous looping


                     NVD


                           Venous beading

                     NVE
NVD   NVE
   Primary response to HTN- vasoconstriction
   Narrowing depend on pre-existing sclerosis
   Narrowing seen in its pure form only in
    young individuals
   Sustained HTN-inner BRB disrupted
   Increased vascular permeability
   Narrowing and sclerosis suggests duration of
    hypertension
   GRADE 1                     GRADE2
   Generalised arteriolar      Exaggeration of light reflex
    narrowing                   AV crossing changes
                                     (Salus sign)
   GRADE 1               GRADE2
   Focal arteriolar      Exaggeration of light reflex
    narrowing             AV crossing changes
                               (Salus sign)
   GRADE 3                   GRADE 4
   Prominent AV changes      Features of grade 3
    (Bonnet, Gunn signs)      Papilloedema
   Retina edema, CWS
   Flame h‟mages
Grade 0




Grade 4             Grade 1




Grade 3             Grade 2
   Rare, occurs in hypertensive crisis
   „Elschnig spots‟
   „Siegrist streaks‟
   Exudative retinal detachment
   Creamy appearance of the
    vessels in the posterior
    pole and peripheral area
   Triglycerides >2500mg/dl
   Micro vascular occlusion and
    ischemia
   Severe head trauma, chest
    compression injury, Embolism,
    a/c pancreatitis, carcinoma,
    connective tissue diseases,
    Lymphoma, TTP, Bone
    marrow transplantation
   Multiple superficial white
    retinal patches
   Superficial pericapillary
    haemorrhages
   Sickle cell anaemia & Sickle cell thalassemia
    are associated severe ocular manifestations
   Proliferative changes
   Seafan neovascularisation
   Haemorrhages
STAGING

5       1   1.   Peripheral arteriolar
                 occlusion
            2.   Peripheral AV
                 anastomosis
4       2   3.   Sprouting new vessels
            4.   Vitreous haemorrhage
            5.   Retinal detachment
    3
   Venous tortousity
   Silver wiring of arterioles
   „Salmon patches‟
   „Black sunbursts‟
   Macular depression sign
   Peripheral retinal holes
   Artery & vein occlusion
   Angioid streaks
   Venous tortousity
   Silver wiring of arterioles
   „Salmon patches‟
   „Black sunbursts‟
   Macular depression sign
   Peripheral retinal holes
   Artery & vein occlusion
   Angioid streaks
   Rarely diagnostic importance
   Duration &type don‟t influence
   Pale fundus
   Haemorrhages
   Cotton wool spots
   Roth spot
   Venous tortousity-related severity of anemia
   More common in a/c leukaemia
   Primary- infiltration
   Secondary- anemia, thrombocytopaenia,
    hyperviscosity, infection
   Superficial haemorrhages
   Roth spot
   Cotton wool spot
   Peripheral retinal vascularisation
   Pigment epitheliopathy- ‛leopard spot‟
   Venous dilatation
   Segmentation
   Venous tortousity
   Retinal haemorrhages
   Viral
     CMV
     HIV
     Rubella

   Bacterial
     Tuberculosis
     Syphilis

   Parasitic
     Toxoplasmosis

   Fungal
   Most common ocular infection in AIDS
   Indolent retinitis
     Startsin the periphery
     Mild granular opacification

   Fulminating retinitis
     Dense white opacification
     Vasculitis, mild vitritis
     Hemorrhages
     Extension along blood vessels
     Involve optic nerve head
   60% of AIDS patients
   Retinal microangiopathy
   Multiple cotton wool spots
   Non infectious
   Salt & pepper retinopathy,
    most marked at macula
   Disc & vessels normal
   Pigmentery disturbance at
    posterior pole
   Optic neuritis
   Intractable chronic uveitis
   Focal/multi focal choroiditis
   Choroidal granuloma
   Periphlebits
   Panuveitis
   Quiscent
       Bilateral/unilateral healed chorio
        retinal scars
   Reactivation retinochoroiditis
     Adjacent to old scar
      (satellite lesion)
     Vasculitis,
     Severe vitritis
      (headlight in the fog‟ appearance)
   Papillitis (secondary to
    juxtapapillary retinitis)
   Atypical lesions
   Quiscent
       Bilateral/unilateral healed chorio
        retinal scars
   Reactivation retinochoroiditis
     Adjacent to old scar
      (satellite lesion)
     Vasculitis,
     Severe vitritis
      (headlight in the fog‟ appearance)
   Papillitis (secondary to
    juxtapapillary retinitis)
   Atypical lesions
   Quiscent
       Bilateral/unilateral healed chorio
        retinal scars
   Reactivation retinochoroiditis
     Adjacent to old scar
      (satellite lesion)
     Vasculitis,
     Severe vitritis
      (headlight in the fog‟ appearance)
   Papillitis (secondary to
    juxtapapillary retinitis)
   Atypical lesions
   Retinal periphlebitis
   „Candle wax drippings‟
   Branch retinal vein occlusion
   Cotton ball vitreous opacities
   Haemorrhages,
   Granulomas
   Optic nerve edema and
    granuloma
   Optic disc granuloma      Retinal granuloma
                                 ‟Landers sign‟
   Optic disc granuloma      Retinal granuloma
                                 ‟Landers sign‟
   A/c recurrent Hypopyon uveitis
   Retinitis- superficial infiltrates
   Retinal vasculitis
     Periphlebitis& periarteritis
     Vascular occlusion

   Vascular leakage
   Optic disc edema
   Retinal exudation
   Vitritis
   Optic disc edema
   Multifocal detachments of
    the sensory retina
   Exudative retinal
    detachment
   Numerous, residual, small,
    atrophic scars
    (‛sunset glow‟ fundus)
   No typical features
   Retinopathy
   Haemorrhages
   Cotton wool spots
   Vascular occlusions
   Hyaline like calcific material within optic disc
   Often bilateral, 0.3%
   Buried drusen
     Elevated disc, scalloped margin
     No physiological cup
     No hyperaemia
     Vessels not obscured
     Venous pulsation present

   Exposed drusen
     Waxy   pearl like irregularities
   Hyaline like calcific material within optic disc
   Often bilateral, 0.3%
   Buried drusen
     Elevated disc, scalloped margin
     No physiological cup
     No hyperaemia
     Vessels not obscured
     Venous pulsation present

   Exposed drusen
     Waxy   pearl like irregularities
   Hyaline like calcific material within optic disc
   Often bilateral, 0.3%
   Buried drusen
     Elevated disc, scalloped margin
     No physiological cup
     No hyperaemia
     Vessels not obscured
     Venous pulsation present

   Exposed drusen
     Waxy   pearl like irregularities
   Incomplete closure of the choroid fissure
   Discrete, focal, glistening, white,
    bowl shaped excavation
   Disc may enlarged
   Retinal vasculature normal
   Complication- RD
   Trisomy 13, 18, 22
   CHARGE
   Visual acuity very poor
   Enlarged disc with funnel shaped excavation
   Central core -whitish glial tissue
   Spokes of wheel appearance
   Complication- RD
   Frontonasal dysplasia
   Neurofibromatosis type-2
   Myelination extend to retina
   Don‟t interfere with vision
   Larger & denser than CWS
   Always connected to optic disc
   No overlying vitreous haze
Normal vertical cup-disc ratio 0.3 or less
   Inflammatory, infective or demyelinating process
   Retrobulbar neuritis
     Opticdisc normal
     Most common type in adult, MS

   Papillitis
     Hyperemia & edema of optic disc
     Flame h‟mage

   Neuroretinitis
     Papiiltiswith retinal nerve fibre layer inflammation
     Macular star
     Viral infection , cat scratch fever, syphilis
   Inflammatory, infective or demyelinating process
   Retrobulbar neuritis
     Opticdisc normal
     Most common type in adult, MS

   Papillitis
     Hyperemia & edema of optic disc
     Flame h‟mage

   Neuroretinitis
     Papiiltiswith retinal nerve fibre layer inflammation
     Macular star
     Viral infection , cat scratch fever, syphilis
   Inflammatory, infective or demyelinating process
   Retrobulbar neuritis
     Opticdisc normal
     Most common type in adult, MS

   Papillitis
     Hyperemia & edema of optic disc
     Flame h‟mage

   Neuroretinitis
     Papiiltiswith retinal nerve fibre layer inflammation
     Macular star
     Viral infection , cat scratch fever, syphilis
   Swelling of optic nerve head secondary to
    raised intracranial pressure
   Early papilloedema
     Optic disc- hyperemia
      & mild elevation
     Disk margins indistinct
     Loss of spontaneous
      venous pulsation
   Established papilloedema
     Hyperaemia   of optic disc
     Blurred, elevated margin
     Obliterated cup
     Venous engorgement
     Flame shaped hemorrhages
     Cotton wool spots
     Hard exudates-‛macular fan‟
   Chronic papilloedema
     Optic disc elevated and white
      ‛champagne cork appearance‟
     Usual cause chronic elevated ICT
     Corpora amylacea
     Irreversible visual loss
     Cotton wool spot & h‟mage
      absent
   Retro laminar portion of optic
    nerve to lateral geniculate body
   Lesion anterior to optic chiasma-
    unilateral
   RB neuritis, hereditary,
    compressive lesions, toxic&
    nutritional optic neuropathy
   Without antecedent swelling of
    optic disc
   Pale flat disc, clear margins
   Reduction in no. of small BV on
    the disc- „Kestenbaum sign‟
   Atrophy may be diffuse/sectoral
   Retro laminar portion of optic
    nerve to lateral geniculate body
   RB neuritis, hereditary,
    compressive lesions, toxic&
    nutritional optic neuropathy
   Without antecedent swelling of
    optic disc
   Lesion anterior to optic chiasma-
    unilateral
   Pale flat disc, clear margins
   Reduction in no. of small BV on
    the disc- „Kestenbaum sign‟
   Atrophy may be diffuse/sectoral
   Preceded by swelling
   Papilloedema, AION, Optic neuritis
   Dirty grey slightly raised disc
   Ill defined margins –gliosis
   Sheathed vessels
   Reduction in small vessels
   Clinical opthalmology- Jack J.Kanski 5th Ed.
   “The Eyes Have It”-University of Michigan
   Harrison‟s Principles of internal medicine 16th Ed.
   Parsons‟ Diseases of the Eye 20th Ed.
   New England Journal of Medicine
Optic fundus in clinical medicine

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Optic fundus in clinical medicine

  • 2. Only place in the body where blood vessels can be visualized directly  Mirror the status of the systemic circulation  Continuity of nerve fibers and meninges  Reflects specific changes in systemic diseases  Contribute to diagnosis
  • 3. Direct ophthalmoscopy  Indirect opthalmoscopy Sterioscopical view possible
  • 4. Ideally fundus should be examined in a darkened room  Patient should be asked to fix their gaze on a distant object  Examine with corresponding eyes  The ideal line of approach should bring the optic disc straight in to view  If only blood vessels on a pink background are seen they should be followed , the disk will eventually come in to view
  • 5. Media- hazy, clear  Disc- size, shape, colour, margin, physiological cup, neuroretinal rim  Blood vessels- caliber, tortousity, irregularities, changes in the vessel wall, aneurism, neovascularisation  Exudates  Haemorrhage
  • 6. Uniform red to pink  Disc-pale pink  1.5 mm in diameter  Nasal margin slightly blurred  Vessels emanate from optic cup  Consist of central cup and peripheral neuroretinal rim  Macula temporally  Fovea 2.5mm-diameter, darker
  • 7. Uniform red to pink  Disc-pale pink  1.5 mm in diameter  Nasal margin slightly blurred  Vessels emanate from optic cup  Consist of central cup and peripheral neuroretinal rim  Macula temporally  Fovea 2.5mm-diameter, darker
  • 8. Uniform red to pink  Disc-pale pink  1.5 mm in diameter  Nasal margin slightly blurred  Vessels emanate from optic cup  Consist of central cup and peripheral neuroretinal rim  Macula temporally  Fovea 2.5mm-diameter, darker
  • 9. Uniform red to pink  Disc-pale pink  1.5 mm in diameter  Nasal margin slightly blurred  Vessels emanate from optic cup  Consist of central cup and peripheral neuroretinal rim  Macula temporally  Fovea 2.5mm-diameter, darker
  • 10. Uniform red to pink  Disc-pale pink  1.5 mm in diameter  Nasal margin slightly blurred  Vessels emanate from optic cup  Consist of central cup and peripheral neuroretinal rim  Macula temporally  Fovea 2.5mm-diameter, darker
  • 11. Uniform red to pink  Disc-pale pink  1.5 mm in diameter  Nasal margin slightly blurred  Vessels emanate from optic cup  Consist of central cup and peripheral neuroretinal rim  Macula temporally  Fovea 2.5mm-diameter, darker
  • 12. Uniform red to pink  Disc-pale pink  1.5 mm in diameter  Nasal margin slightly blurred  Vessels emanate from optic cup  Consist of central cup and peripheral neuroretinal rim  Macula temporally  Fovea 2.5mm-diameter, darker
  • 13. Uniform red to pink  Disc-pale pink  1.5 mm in diameter  Nasal margin slightly blurred  Vessels emanate from optic cup  Consist of central cup and peripheral neuroretinal rim  Macula temporally  Fovea 2.5mm-diameter, darker
  • 14. Tygroid fundus  Deeply pigmented choroid  Choroidal vessels are seen  Polygonal pigmented areas in between
  • 15.
  • 16. Dot haemorrhages  Deep within the retina  Leakage of capillaries, venules  Common in diabetes  Flame haemorrhages  Superficial nerve fibre layer  Leakage of capillaries, venules that are ischemic or, in the case of veins, under high pressure  Boat haemorrhages (pre-retinal)  Interface between retina & vitreous  Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
  • 17. Dot haemorrhages  Deep within the retina  Leakage of capillaries, venules  Common in diabetes  Flame haemorrhages  Superficial nerve fibre layer  Leakage of capillaries, venules that are ischemic or, in the case of veins, under high pressure  Boat haemorrhages (pre-retinal)  Interface between retina & vitreous  Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
  • 18. Dot haemorrhages  Deep within the retina  Leakage of capillaries, venules  Common in diabetes  Flame haemorrhages  Superficial nerve fibre layer  Leakage of capillaries, venules that are ischemic or, in the case of veins, under high pressure  Boat haemorrhages (pre-retinal)  Interface between retina & vitreous  Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
  • 19. Dot haemorrhages  Deep within the retina  Leakage of capillaries, venules  Common in diabetes  Flame haemorrhages  Superficial nerve fibre layer  Leakage of capillaries, venules that are ischemic or, in the case of veins, under high pressure  Boat haemorrhages (pre-retinal)  Interface between retina & vitreous  Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
  • 20. Dot haemorrhages  Deep within the retina  Leakage of capillaries, venules  Common in diabetes  Flame haemorrhages  Superficial nerve fibre layer  Leakage of capillaries, venules that are ischemic or, in the case of veins, under high pressure  Boat haemorrhages (pre-retinal)  Interface between retina & vitreous  Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
  • 21. Dot haemorrhages  Deep within the retina  Leakage of capillaries, venules  Common in diabetes  Flame haemorrhages  Superficial nerve fibre layer  Leakage of capillaries, venules that are ischemic or, in the case of veins, under high pressure  Boat haemorrhages (pre-retinal)  Interface between retina & vitreous  Sub macular h‟ge, Preretinal h‟ge, Retinal h‟ge
  • 22. Hard exudate  Deep yellow with sharp margins  Often circinate  Leakage from pre-capillary arterioles  DM, HTN, VHL disease, radiation  „Macular star‟  Soft exudate(cotton wool spot)  Fluffygray-white, near optic disc  Retinal nerve fiber layer microinfarction  HTN, DM, connective tissue disease,HIV
  • 23. Hard exudate  Deep yellow with sharp margins  Often circinate  Leakage from pre-capillary arterioles  DM, HTN, VHL disease, radiation  „Macular star‟  Soft exudate(cotton wool spot)  Fluffygray-white, near optic disc  Retinal nerve fiber layer microinfarction  HTN, DM, connective tissue disease,HIV
  • 24. Hard exudate  Deep yellow with sharp margins  Often circinate  Leakage from pre-capillary arterioles  DM, HTN, VHL disease, radiation  „Macular fan‟  Soft exudate(cotton wool spot)  Fluffygray-white, near optic disc  Retinal nerve fiber layer microinfarction  HTN, DM, connective tissue disease,HIV
  • 25. White centered retinal haemorrhages  CWS surrounded by h‟mage  CWS- ischaemic axons  H‟maghe- precapillary arterioles  Sub acute bacterial endocarditis  Leukaemia  Diabetes
  • 26. Deposition in ganglion cell layer  Thickening & loss of transparency of retina  Foveola-ganglion cells absent, thin, so contrast  Sphingolipidoses  Central retinal artery occlusion  Berlins edema
  • 27. Crack like dehiscence in brusch‟ membrane  Degenerative process combined with calcium deposition  Linear reddish brown lesion  Lies beneath normal blood vessels  “Pseu d‟orange”  Salmon spots, optic nerve drusen  Pseudoxanthoma elasticum, EDS  Paget‟s, Hemoglobinopathies
  • 28. Papillopheblitis (optic disc vasculitis)  Affects healthyindividuals <50  Disc edema, cotton wool spots  Venous dilatation and tortousity  Retinal haemorrhages  Retinal vasculitis  Occurs in sarcoidosis, Behcet‟s disease, Multiple sclerosis, idiopathic  Extremely rare in lupus  Perivenous lymphocytic infiltration (sheathing)
  • 29. Diffuse retinal dystrophy(rods)  Classic clinical triad  Arteriolarattenuation  Retinal bone-spicule pigmentation  Waxy disc pallor  Starts at mid periphery  Maculopathy  Associations  Bassen-Kornzwieg syndrome, Refsum‟s disease, Kearn-sayre syndrome , Usher‟s syndrome Muchopolysaccharidoses, Lauren‟s moon biedel syndrome, Friederisch ataxia
  • 30. Attempt at vascularising ischaemic tissue  Lacks bifurcating pattern  Bleed spontaneously  Diabetic retinopathy  Retinal vein occlusion  Radiation  Sickle cell retinopathy  Retinopathy of prematurity
  • 31. Separation of sensory retina from pigment epithelium  Rhegmatogenous RD  Non-rhegmatogenous RD  Tractional- PDR, ROP, sickle cell retinopathy, penetrating posterior segment trauma  Exudative- choroidal tumours, exophytic retinoblastoma, harada disease, posterior scleritis, subretinal neovascularisation, severe hypertension  Elevated sheath of retinal tissue with folds
  • 32. Separation of sensory retina from pigment epithelium  Rhegmatogenous RD  Non-rhegmatogenous RD  Tractional- PDR, ROP, sickle cell retinopathy, penetrating posterior segment trauma  Exudative- choroidal tumours, exophytic retinoblastoma, harada disease, posterior scleritis, subretinal neovascularisation, severe hypertension  Elevated sheath of retinal tissue with folds
  • 33.
  • 34. Atherosclerosis, embolism  Retina appears white  Attenuation of arteries and veins  Cherry red spot  Investigate for  Valvular heart disease, endocarditis, mural thrombi, Carotid artery disease, systemic vasculitis, hematological disorders
  • 35. Cholesterol Fibrinoplatelet Calcific (Hollenhorst plaques)
  • 36. Atherosclerosis, embolism  Retina appears white  Attenuation of arteries and veins  Cherry red spot  Investigate for Valvular heart disease, endocarditis, mural thrombi, Carotid artery disease, systemic vasculitis, hematological disorders
  • 37. Atherosclerosis, embolism Cattle-trucking  Retina appears white  Attenuation of arteries and veins  Cherry red spot  Investigate for Valvular heart disease, endocarditis, mural thrombi, Carotid artery disease, systemic vasculitis, hematological disorders
  • 38. Embolism, periarteritis  Retinal cloudiness corresponding to the areas of ischemia  Narrowing of arteries and veins  One or more emboli may be present
  • 39. Present in 20% of population  It may be isolated, combined CRVO, combined AION  Localised cloudiness- macula and papillomacular bundle
  • 40. Occlusion of short posterior ciliary arteries  Disc is pale  Diffuse or sectoral edema  Splinter shaped h‟mages  „Pseudo-Foster kennedy syndrome‟
  • 41. Giant cell arteritis  Cotton wool spots are uncommon  Cilioretinal artery occlusion  Central artery occlusion
  • 42. Etiology Arteriosclerosis Increasing age Hypertension Diabetes mellitus Blood dyscrasiasis Periphlebitis Raised intraocular tension
  • 43. Dilatation & tortousity of all branches of CRV  Retinal h‟age- superficial & deep throughout  “Blood and thunder”  Cotton wool spots  Optic disc edema  Macular edema
  • 44. Venous dilatation and tortousity peripheral to the site of occlusion  Hemorrhages  Retinal edema  Cotton wool spots  Neovascularisation
  • 45. Most common cause of legal blindness in 20-65 yrs  Type 1>Type 2 (40% , 20%)  Risk factors  Duration of diabetes  Poor metabolic control  Pregnancy  Hypertension  Nephropathy  Smocking  Obesity  Hyperlipidaemia
  • 46. Micro vascular occlusion  Microvascular leakage
  • 47. Eva kohner‟s classification  Non-proliferative diabetic retinopathy  Pre-proliferative diabetic retinopathy  Proliferative diabetic retinopathy
  • 48. Micro aneurysms (earliest lesion)  Hard exudates  Retinal edema  Haemorrhages
  • 49. Cotton wool spots  Intra retinal micro vascular abnormalities(IRMA)  Venous changes  Dilatation,looping  Beading, segmentation  Arterial changes  Narrowing, occlusion  Silver wiring  Dark blot haemorrhages
  • 50. Involvement of fovea  Perifoveal hard exudates  Dark blot hemorrhages
  • 51. Neovascularisation Venous looping NVD Venous beading NVE
  • 52. NVD NVE
  • 53. Primary response to HTN- vasoconstriction  Narrowing depend on pre-existing sclerosis  Narrowing seen in its pure form only in young individuals  Sustained HTN-inner BRB disrupted  Increased vascular permeability  Narrowing and sclerosis suggests duration of hypertension
  • 54. GRADE 1  GRADE2  Generalised arteriolar  Exaggeration of light reflex narrowing  AV crossing changes (Salus sign)
  • 55. GRADE 1  GRADE2  Focal arteriolar  Exaggeration of light reflex narrowing  AV crossing changes (Salus sign)
  • 56. GRADE 3  GRADE 4  Prominent AV changes  Features of grade 3 (Bonnet, Gunn signs)  Papilloedema  Retina edema, CWS  Flame h‟mages
  • 57. Grade 0 Grade 4 Grade 1 Grade 3 Grade 2
  • 58. Rare, occurs in hypertensive crisis  „Elschnig spots‟  „Siegrist streaks‟  Exudative retinal detachment
  • 59. Creamy appearance of the vessels in the posterior pole and peripheral area  Triglycerides >2500mg/dl
  • 60. Micro vascular occlusion and ischemia  Severe head trauma, chest compression injury, Embolism, a/c pancreatitis, carcinoma, connective tissue diseases, Lymphoma, TTP, Bone marrow transplantation  Multiple superficial white retinal patches  Superficial pericapillary haemorrhages
  • 61.
  • 62. Sickle cell anaemia & Sickle cell thalassemia are associated severe ocular manifestations  Proliferative changes  Seafan neovascularisation  Haemorrhages
  • 63. STAGING 5 1 1. Peripheral arteriolar occlusion 2. Peripheral AV anastomosis 4 2 3. Sprouting new vessels 4. Vitreous haemorrhage 5. Retinal detachment 3
  • 64. Venous tortousity  Silver wiring of arterioles  „Salmon patches‟  „Black sunbursts‟  Macular depression sign  Peripheral retinal holes  Artery & vein occlusion  Angioid streaks
  • 65. Venous tortousity  Silver wiring of arterioles  „Salmon patches‟  „Black sunbursts‟  Macular depression sign  Peripheral retinal holes  Artery & vein occlusion  Angioid streaks
  • 66. Rarely diagnostic importance  Duration &type don‟t influence  Pale fundus  Haemorrhages  Cotton wool spots  Roth spot  Venous tortousity-related severity of anemia
  • 67. More common in a/c leukaemia  Primary- infiltration  Secondary- anemia, thrombocytopaenia, hyperviscosity, infection  Superficial haemorrhages  Roth spot  Cotton wool spot
  • 68. Peripheral retinal vascularisation  Pigment epitheliopathy- ‛leopard spot‟
  • 69. Venous dilatation  Segmentation  Venous tortousity  Retinal haemorrhages
  • 70. Viral  CMV  HIV  Rubella  Bacterial  Tuberculosis  Syphilis  Parasitic  Toxoplasmosis  Fungal
  • 71. Most common ocular infection in AIDS  Indolent retinitis  Startsin the periphery  Mild granular opacification  Fulminating retinitis  Dense white opacification  Vasculitis, mild vitritis  Hemorrhages  Extension along blood vessels  Involve optic nerve head
  • 72. 60% of AIDS patients  Retinal microangiopathy  Multiple cotton wool spots  Non infectious
  • 73. Salt & pepper retinopathy, most marked at macula  Disc & vessels normal  Pigmentery disturbance at posterior pole  Optic neuritis
  • 74. Intractable chronic uveitis  Focal/multi focal choroiditis  Choroidal granuloma  Periphlebits  Panuveitis
  • 75. Quiscent  Bilateral/unilateral healed chorio retinal scars  Reactivation retinochoroiditis  Adjacent to old scar (satellite lesion)  Vasculitis,  Severe vitritis (headlight in the fog‟ appearance)  Papillitis (secondary to juxtapapillary retinitis)  Atypical lesions
  • 76. Quiscent  Bilateral/unilateral healed chorio retinal scars  Reactivation retinochoroiditis  Adjacent to old scar (satellite lesion)  Vasculitis,  Severe vitritis (headlight in the fog‟ appearance)  Papillitis (secondary to juxtapapillary retinitis)  Atypical lesions
  • 77. Quiscent  Bilateral/unilateral healed chorio retinal scars  Reactivation retinochoroiditis  Adjacent to old scar (satellite lesion)  Vasculitis,  Severe vitritis (headlight in the fog‟ appearance)  Papillitis (secondary to juxtapapillary retinitis)  Atypical lesions
  • 78.
  • 79. Retinal periphlebitis  „Candle wax drippings‟  Branch retinal vein occlusion  Cotton ball vitreous opacities  Haemorrhages,  Granulomas  Optic nerve edema and granuloma
  • 80. Optic disc granuloma  Retinal granuloma ‟Landers sign‟
  • 81. Optic disc granuloma  Retinal granuloma ‟Landers sign‟
  • 82. A/c recurrent Hypopyon uveitis  Retinitis- superficial infiltrates  Retinal vasculitis  Periphlebitis& periarteritis  Vascular occlusion  Vascular leakage  Optic disc edema  Retinal exudation  Vitritis
  • 83. Optic disc edema  Multifocal detachments of the sensory retina  Exudative retinal detachment  Numerous, residual, small, atrophic scars (‛sunset glow‟ fundus)
  • 84. No typical features  Retinopathy  Haemorrhages  Cotton wool spots  Vascular occlusions
  • 85.
  • 86. Hyaline like calcific material within optic disc  Often bilateral, 0.3%  Buried drusen  Elevated disc, scalloped margin  No physiological cup  No hyperaemia  Vessels not obscured  Venous pulsation present  Exposed drusen  Waxy pearl like irregularities
  • 87. Hyaline like calcific material within optic disc  Often bilateral, 0.3%  Buried drusen  Elevated disc, scalloped margin  No physiological cup  No hyperaemia  Vessels not obscured  Venous pulsation present  Exposed drusen  Waxy pearl like irregularities
  • 88. Hyaline like calcific material within optic disc  Often bilateral, 0.3%  Buried drusen  Elevated disc, scalloped margin  No physiological cup  No hyperaemia  Vessels not obscured  Venous pulsation present  Exposed drusen  Waxy pearl like irregularities
  • 89. Incomplete closure of the choroid fissure  Discrete, focal, glistening, white, bowl shaped excavation  Disc may enlarged  Retinal vasculature normal  Complication- RD  Trisomy 13, 18, 22  CHARGE
  • 90. Visual acuity very poor  Enlarged disc with funnel shaped excavation  Central core -whitish glial tissue  Spokes of wheel appearance  Complication- RD  Frontonasal dysplasia  Neurofibromatosis type-2
  • 91. Myelination extend to retina  Don‟t interfere with vision  Larger & denser than CWS  Always connected to optic disc  No overlying vitreous haze
  • 92. Normal vertical cup-disc ratio 0.3 or less
  • 93. Inflammatory, infective or demyelinating process  Retrobulbar neuritis  Opticdisc normal  Most common type in adult, MS  Papillitis  Hyperemia & edema of optic disc  Flame h‟mage  Neuroretinitis  Papiiltiswith retinal nerve fibre layer inflammation  Macular star  Viral infection , cat scratch fever, syphilis
  • 94. Inflammatory, infective or demyelinating process  Retrobulbar neuritis  Opticdisc normal  Most common type in adult, MS  Papillitis  Hyperemia & edema of optic disc  Flame h‟mage  Neuroretinitis  Papiiltiswith retinal nerve fibre layer inflammation  Macular star  Viral infection , cat scratch fever, syphilis
  • 95. Inflammatory, infective or demyelinating process  Retrobulbar neuritis  Opticdisc normal  Most common type in adult, MS  Papillitis  Hyperemia & edema of optic disc  Flame h‟mage  Neuroretinitis  Papiiltiswith retinal nerve fibre layer inflammation  Macular star  Viral infection , cat scratch fever, syphilis
  • 96. Swelling of optic nerve head secondary to raised intracranial pressure  Early papilloedema  Optic disc- hyperemia & mild elevation  Disk margins indistinct  Loss of spontaneous venous pulsation
  • 97. Established papilloedema  Hyperaemia of optic disc  Blurred, elevated margin  Obliterated cup  Venous engorgement  Flame shaped hemorrhages  Cotton wool spots  Hard exudates-‛macular fan‟
  • 98. Chronic papilloedema  Optic disc elevated and white ‛champagne cork appearance‟  Usual cause chronic elevated ICT  Corpora amylacea  Irreversible visual loss  Cotton wool spot & h‟mage absent
  • 99. Retro laminar portion of optic nerve to lateral geniculate body  Lesion anterior to optic chiasma- unilateral  RB neuritis, hereditary, compressive lesions, toxic& nutritional optic neuropathy  Without antecedent swelling of optic disc  Pale flat disc, clear margins  Reduction in no. of small BV on the disc- „Kestenbaum sign‟  Atrophy may be diffuse/sectoral
  • 100. Retro laminar portion of optic nerve to lateral geniculate body  RB neuritis, hereditary, compressive lesions, toxic& nutritional optic neuropathy  Without antecedent swelling of optic disc  Lesion anterior to optic chiasma- unilateral  Pale flat disc, clear margins  Reduction in no. of small BV on the disc- „Kestenbaum sign‟  Atrophy may be diffuse/sectoral
  • 101. Preceded by swelling  Papilloedema, AION, Optic neuritis  Dirty grey slightly raised disc  Ill defined margins –gliosis  Sheathed vessels  Reduction in small vessels
  • 102.
  • 103. Clinical opthalmology- Jack J.Kanski 5th Ed.  “The Eyes Have It”-University of Michigan  Harrison‟s Principles of internal medicine 16th Ed.  Parsons‟ Diseases of the Eye 20th Ed.  New England Journal of Medicine