Ophthalmology Notes: NEURO OPHTHALMOLOGY NOTES

NEUROPHTHALMOLOGY

AFFERENT PUPILLARY DEFECT-

Absolute APD – AMAUROTIC PUPIL
Relative APD- MARCUS GUNN PUPIL

ABSOLUTE APD-

Complete ON lesion
Inv eye- No PL
Both pupils- equal in size
When the affected eye is stimulated→ neither pupil reacts
When the nml eye is stimulated→ both pupils react nmlly
Near reflex is nml

RELATIVE APD-

Caused by –incomplete ON lesion

-Sev retinal dis

-NEVER by a dense cataract

* Swinging flashlight test-

When nml eye is stimulated→ Both pupils constrict

When abnml eye is stimulated→ Both pupils dilate

This paradoxical dilatation of pupils occurs b’cos the dilatation produced by withdrawing the light from the nml eye outweighs the constriction produced by stimulating the abnml eye.
Afferent /sensory lesions- Pupils are equal in size
Efferent/ motor lesions-Anisocoria [unequal pupil size]

APD-

Causes of APD-

AION
Optic neuritis
Glaucoma
CRAO / CRVO
Lesion of optic chiasma / optic tract
Amblyopia
VH
Macular degeneration
BRVO /BRAO

10.RD

OPTIC NERVE-

Length- 50mm

Intraocular -1mm
Intraorbital -25-30mm
Intracanalicular- 6mm
Intracranial- 10mm

OPTIC ATROPHY-case

DEF-

A condition characterized by loss of conducting function of the ON with pallor of the disc d/t gliosis & loss of capillaries.

PATHOGENESIS-

Degeneration of optic N fib→ Proliferation of astrocytes & glial tiss [Loss of transparency ] →When light enters the disc, instead of refraction , it gets reflected back→ so the disc appears pale.

VIVA-

CLASSIFICATION-

A] PATHOLOGICAL-

1. Ascending OA

2. Descending OA

3. Inherited OA

B] OPHTHALMOSCOPIC-

1. primary OA

2. Secondary OA

3.Consecutive OA

4. Cavernous / glaucomatous OA

5. Segmental / partial OA

PATHOLOGICAL-

ASCENDING OA-

Also k/as Wallerian degeneration
Prim lesion- ret,ON & choroids
Atrophy proceeds towards the brain
Eg

RP
CRAO
Papilloedema
Glaucoma
Toxic amb
Choroiditis

DESCENDING OA-

Also k/as retrograde OA
Brain/eye→ ON
Eg- Chiasmal compression

-Retrobulbar neuritis

INHERITED OA-

Congenital / Infantile OA-

Recessive form-

OA shortly after birth
Profound LOV
Nystagmus
Defective CV

Dominant form-

-blindness seldom occurs

-Vision slowly decreases

-central & paracentral scotoma

Leber’s OA- X –linked recessive

-men

-2-3 decade

-ul sudden LOV

-Fundus- Disc edema + hyperaemia

-telangiectatic BV s around disc

-edematous NFL

-Sec OA later

-Fields- dense central /centrocaecal scotoma

-Mild spasticity & gait disturbance

behr’s OA-

-Infancy

-AR

- Incomplete BL OA

-Temporal pallor

-Cerebellar ataxia

-Spasticity

-Pyramidal tr lesion

OPHTHALMOSCOPIC CLASSN-

CONSECUTIVE OA-

Follows dis of retina , choroid & retinal vasculature.

-Disc-Waxy pallor

-nml margins

-Marked attenuation of As

-Nml physiological cup

-Asstd retinal pathology

RP
Choroiditis
Chorioretinitis
CRAO

TOXIC OA-

Tobacco ,ETB, streptomycin, INH, lead, arsenic.

Degeneration of axial portion of retrobulbar ON→ Fibrosis & gliosis in papillomacular bundle→ Temporal pallor.[ bcos PM fib enter the disc temporally]

PRIMARY OA-[viva]

-Orderly deg of nerve fib & replacement by glial tiss without alteration in the architecture of ONH

-Disc-chalky white

-Sharply defined margins

-Lamina cribrosa well seen

-surrounding ret is nml

-Retinal BVs- nml

-Retinal periphery-nml

Eg-

Pituitary tum
Retrobulbar neuritis
Demyelinating dis
Tabes dorsalis
Toxic & nutritional neuropathies
Hereditary neuropathies

-Lesions anterior to optic chiasma→ UL OA

-Lesions inv the chiasm & optic tract→ BL OA

BAND /BOWTIE OA-

Chiasmal lesion
-Pallor is on nasal & temporal side of disc ,sparing the sup & inf aspect
Inv the PM bundle which enters the disc temporally

KESTENBAUM SIGN-

Decrease in the number of capillaries on the disc surface

SECONDARY OA-

-Preceded by swelling of ONH

-Marked deg of optic n fib

-Excessive proliferation of glial tiss.

-Disc-

* Dirty grey pallor

* Poorly defined disc margin

* Physiological cup obliterated [Cup is filled with proliferating fibroglial tiss→ lamina cribrosa cannot be seen]

* Peripapillary sheathing of arteries

* Tortuous & narrowed veins

Papilloedema
Papillitis
AION

CAVERNOUS OA-

-Also k/as Glaucomatous / Schnabel’s OA

-Axonal deg without glial tiss proliferation→ Caverns → filled with hyaluronic acid

-Features-

* Vertical enlargement of the cup

* Notching of NRR

* Laminar dot sign

* Bayonetting sign

* Backward bowing of lamina cribrosa

* Nasal shifting of BV

* Baring of circumlinear BVs

* Splinter h’ages

* Saucerization of disc

Eg-

Glaucoma
Methyl alcohol poisoning

ALTITUDINAL DISC PALLOR-

-Segmental disc swelling fol by segmental OA

-AION

WEDGE SHAPED PALLOR-

BRVO

OPTIC NEURITIS-case

DEF-Inflamn of ON

CLASS-

Inflamn affecting the ophthalmoscopically visible part of the nerve at the disc & thus showing obvious signs of disease

Papillitis
Neuroretinitis

Inflamn which attacks the nerve proximal to this region & thus shows no ophthalmoscopic change.

Retrobulbar neuritis

PATHOLOGY-

3 types of neuritis-

1) PERINEURITIS / PERI-AXIAL NEURITIS-

Leptomeningitis of the optic n & may represent a spread from the brain / orbit & sinuses.It may extend along the pial septa into the nerve parenchyma affecting the extramacular fib

2) AXIAL NEURITIS-

-Affects the Macular fib

-Causes a centrocaecal scotoma & temporal pallor of the disc

Eg-

MS
Toxic & nutritional neuropathies

3) TRANSVERSE NEURITIS

Both axial & periaxial neuritis may progress to inv all the fib.

VIVA-

Q- MC type of ON in childn→ PAPILLITIS

Q-MCC of ON in childn→ POSTVIRAL

AETIO-

Idiopathic

2. Demyelinating disorders

Multiple sclerosis
Acute Disseminated Encephalomyelitis [ADEM]
Neuromyelitis optica [Devic’s dis]
Diffuse Periaxial Encephalitis [ Schilder’s dis ]

3.Infections-

Local-

Endophthalmitis
Orbital cellulitis
Sinusitis
Contiguous spread from meninges, brain & base of skull

Systemic-

Bacterial-

Tb
Syphillis
Cat-scratch dis
Lyme’s dis

Viral-

Influenza
Measles
Mumps
Chickenpox
HZV
Infectious mononucleosis
CMV

Protozoal-

Toxocariasis
Toxoplasmosis
Malaria
Pneumonia

Fungal-

Cryptococcosis
Histoplasmosis

Parasitic-Cysticercosis

4.Immune-mediated disorders

Local-

Uveitis
Sympathetic oph

Systemic-

Sarcoidosis
Wegener’s granulomatosis
Ac Disseminated encephalomyelitis

C/F-

Women
20-40 yrs
Visual loss-usually UL-adults

BL-childn

Pain- Increases on eye movt-elev & adduction [d/t inv of SR &MR which share the same sheath with optic N]
Uhthoff’s phen-Worsening of symptoms on exercise / rise in temp
Pulfrich’s phen- Altered perception of moving objects
Loss of colour vision [ Typically red desaturation]
Reduced perception of light intensity
RAPD
Visual fields- central / centrocaecal scotoma
Fundus-

-Vitreous opacities

-Retrobulbar neuritis-nml optic disc & NFL

-Papillitis- Disc-hyperaemia,

-Peripapillary flame shaped h’ages

-Neuroretinitis-Disc hyperaemia + macular star

INV-

Visual fields-perimetry-central/centrocaecal scotoma
VEP-Prolonged latency
Complete bld count
Rapid plasma reagin
C-reactive protein
ESR
Fluorescent treponemal antibody –absorption [FTA-ABS]test
Anti-nuclear antibody [ANA] test
MRI-brain & orbit with gadolinium enhancement→For MS → periventricular plaques
Tb-X-ray chest

-Montoux

-sputum

11.Sarcoidosis-X-ray chest

-Gallium scan

12.Bld sugar

13. Sinusitis-X-ray –PNS

ATYPICAL ON-

Out of typical age range
No pain on eye movt
Poor vision > 2wks

D/D-

Papilloedema
Optic N compression [Pituitary tum,meningioma]
AION
Toxic / nutritional def amblyopia
Non-organic visual loss
Leber’s hereditary OA

FEATURES	PAPILLOEDEMA	PAPILLITIS
LATERALITY	BL	UL
VISION	Transient LOV	Sudden LOV
OM	N	Restricted & painful
COLOR VISION	N	Affected
PUPILLARY REAC	N	RAPD
VITREOUS OPACITY	Absent	Present
DISC SWELLING	> + 3 D	+ 2D to + 3D
H’AGE & EXUD	More	Less
VISUAL FIELD	Constricted Enlarged blind spot	Central /centrocaecal scotoma
RECOVERY OF VISION	Usually not complete	Usually complete

T/T-

Pulsed steroid therapy-

IV Methyl prednisolone 1gm/day over 1 hour for 3 days→

Oral prednisolone 1 mg/kg/day for 11days

ISCHEAMIC OPTIC NEUROPATHY-case

DEF-Acute painless optic neuropathy occurring sec to optic N ischaemia.

2 types-

1] Anterior ischaemic ON

2] Posterior ischaemic ON

Anterior ION→ Arteritic

→ Non-arteritic

NO	FEATURES	ARTERITIC	NON-ARTERITIC
1.	AGE	70 YRS	60 YRS
2.	SEX	3F> M	M=F
3.	SYMPTOMS	Headache Scalp tenderness Jaw claudication	Pain
4.	V/A	Upto 76% <6/60	Upto 61% < 6/60
5.	DISC	More pale	More hyperaemic
6.	CUP	N	Small
7.	ESR	70	20-40
8.	FFA	Disc & choroids filling delay	Disc filling delay

OCULAR FEATURES-

rapid onset
Painless
UL LOV
Visual field-Altitudinal defect,Arcuate scot,centrocecal def
RAPD
Disc edema
Surface telangiectasia
Flame-shaped h’ages
Peri-papillary arterioles are narrowed

ARTERITC AION-

Giant cell arteritis-[ J-07-T/T]

Headache
Jaw claudication
Scalp tenderness
Prominent Temporal A
Occult temporal arteritis-visual loss in the absence of overt systemic symptoms
Pallor with disc edema
Choroidal ischaemia→ peripapillary pallor & edema
Fellow eye-N disc dia & cup

NON-ARTERITIC AION-

Unrelated to temporal arteritis
Visual impairment on awakening [Nocturnal hypotension]
Hyperemic disc edema
Telangiectasia-represents microvascular shunting from ischemic to non-ischemic region of ON→ c/as Luxury perfusion
C/L eye-disc-small & Cup –small/absent→ k/as-‘Disc at risk’

INV-

ESR
Serum C-reactive protein
Superficial temporal A biopsy-

Take biopsy from the ipsilateral side
Ideal location is the temple, bcos it avoids damage to a major br of Auriculotemporal N
Atleast 2.5cm section shud be taken & serial sections shud be examined b/o the pheno of ‘skip lesions’
Patho-Thickening of the intima,Chr inflame infiltrate with giant cells

4.FFA- Prolonged choroidal filling time

Risk factors-

HT
DM
IHD
Thyroid dis
COPD
Carotid occlusive dis
Vasculitis
Migraine
Nocturnal hypotension
Hyperopia
Smoking
HLA-A29
Hyperlipidemia

D/DS-

1.Non-arteritic ischemic ON-

-young

-less severe visual loss

-nml ESR

2. Optic neuritis-

-young

-painful ocular movts

-Hyperemic OD edema

3. Compressive optic N tum

-Slowly prog visual loss

4. CRVO

-Sev vis loss

-RAPD

-disc edema

-diffuse ret h’ages extending to periphery

5. CRAO-

-sudden painless,sev LOV

-RAPD

-no disc edema

-retinal edema

-cherry red spot

T/T-

Start systemic steroids.-Do not wait for temporal A biopsy report b’cos visual loss is permanent

IV methyl prednisolone 1 gm /day over 1 hour for 3 days

→ Foll by oral prednisolone 1mg/kg/day for 11 days

POSTERIOR ISCHEMIC ON-

D/t disorder of small pial Vs that supply the intraorbital portion of ON away from the eyeball.

ETIO-

Giant cell arteritis
SLE
Sys hypotension /Shock optic neuropathy

C/F-

Visual loss
RAPD
No disc edema
No h’ages

T/T- Same

PAPILLOEDEMA-case

CSF CIRCULATION-

CSF is formed by the choroid plexus in the ventricles of the brain
Choroidal plexus→ Lateral ventricles → Foramen of Monro→ III ventricle→ Aqueduct of Sylvius→ IV ventricle→ Foramen of Luschka & Magendie→ SAS→Absorption by the arachnoid villi into the cerebral venous drainage system

NORMAL CSF PRESSURE-

Infants- < 80 mm H2O
Childn- < 90 mmH2O
Adults- < 210 mmH2O

Papilloedema is also k/as ‘Choked disc’

DEF-

Swelling of the ONH d/t rise in ICP.

Passive edema without primary inflamn

Papilloedema→ Disc edema + rise in ICP

Disc swelling→ Disc edema - rise in ICP

PATHOGENESIS-

Lamina cribrosa divides the ON into –intraocular part & retroocular part.
Nmlly-Tiss press within the intraocular part is more than the retro-ocular part→ Disturbance in the press gradient across the lamina cribrosa→ i.e if the press in the IO part falls or press in the retro-ocular part becomes more→Disc edema
Increase in CSF press in cranial SAS transmitted to SAS around the ON→ Alters the press gradient across the lamina cribrosa→Stasis of axoplasm in pre-laminar reg→ venous congestion→ Disc edema

AETIO-

Ocular
Orbital
Intracranial
Systemic

OCULAR CAUSES-Hypotension

-Acute hypertension

Hypotension→ decrease tiss press in the pre-laminar region→ disc edema

Eg-

Ocular trauma
Parsplanitis
Irvine – Gas syn
CB & choroidal detachment

Acute hypertension-Eg –Acute angle closure glaucoma→ Obliteration of peripapillary Vs→ Anoxia→ disc edema

ORBITAL-

Tumours
Orbital abscess
Endocrine exophthalmos
Sinusitis

INTRACRANIAL-

Tumours-

Papilloedema + brain tum→”Plerocephalic edema”

Highest % in –Mid-brain

-Cerebellum

-Parieto-occipital region

2. Brain abscess

3. Cavernous sinus thrombosis

4 Aneurysm

5. SAH

6.Pseudotum cerebri

7. Malignant HT

8. Meningitis /Encephalitis

9. Tuberculomata & Gummata

10.Parasitic inf

11. Hydrocephalus

SYSTEMIC DIS-

HT
Bld dyscrasias- Pernicious anemia

-Polycythemia vera

-Thrombocytopenic purpura

-Leukemia

* Endocrine

UNILATERAL DISC EDEMA-

Papilloedema
Papillitis
AION
CRVO
Orbital tum
Ocular hypotony
Foster Kennedy syn→Frontal lobe tumour with I/L OA & C/L Papilloedema

PSEUDO FOSTER KENNEDY SYNDROME-

D/t giant cell arteritis involving both the discs at diff times.

BILATERAL DISC EDEMA-

papilloedema
HTR
Diabetic papillopathy
TED
CCF
Leber’s on
Anaemia & Hypoxemia

PSEUDOPAPILLOEDEMA-

Optic disc drusen
Hyperopia
Disc NV
Myelinated nerve fibres
Astrocytic hamartomas
Bergmister’s papilla

PATHOLOGY-

Edematous swelling of NFL
Infiltration of all the tiss with fld
Lamina cribrosa bows forward with ant convexity
Small / obliterated physiological cup
Peripapillary ret displaced laterally & thrown into folds
Both veins & capillaries distended
Peripapillary h’ages
SAS distended
Swollen NFL contains cytoid bodies

C/F-

SYMPTOMS-

Transient LOV –Blackouts [D/Ds]
Headache
Nausea/ vomitg
Diplopia [Rise in ICP→VI n palsy]

SIGNS-

1] EARLY PAPILLOEDEMA-

1. Symptoms are absent

2. V/A –N

3. Disc-Hyperaemia

-Blurred margins [ nasal to begin with]

4. Swelling of peripapillary NFL

5.Loss of spontaneous venous pulsation

2] ESTABLISHED PAPILLOEDEMA

* Transient LOV

* Disc-Sev hyperemia

-Mod elev

-indistinct margins

-Cup obscured

-Small Vs obscured

* Venous engorgement

* flame-shaped h’ages

* CW spots

*Circumferential ret folds

* Macular star [ DDs]

* Blind spot enlarged

TRANSIENT LOSS OF VISION- viva [MICA]

1] amaurosis fugax

2] Migraine

3] Impending CRVO & CRAO

4] Cerebrovascular insufficiency

MACULAR STAR –DDs-

HTR
DR
CRVO
CRAO
Macular edema
Neuroretinitis
Juxtapapillary choroiditis

3] LONGSTANDING [ VINTAGE] PAPILLOEDEMA-

* Variable V/A

* Visual fields begin to constrict

* Disc- markedly elevated-‘CHAMPAIGNE CORK’

* CW spots –nt

* H’ages-nt

* Optociliary shunts

4] ATROPHIC PAPILLOEDEMA-

* Sec OA [DDs]

* Vision –sev impaired

* disc- Dirty grey

-Slightly elevated

-few crossing BVs

-Indistinct margins

SECONDARY OA-{ D/Ds}

Papillitis
Papilloedema
AION

DD-Papilloedema-

Papillitis
Hyperopia
Medullated NF
Optic disc drusens

NYSTAGMUS-case

DEF-

Repetitive, Involuntary ,rhythmic ,to & fro oscillations of the eyeball. [RIRO]

SACCADES-

Fixate on objects

PURSUIT S-

Maintain fixation

CLASS-

JERKY NYSTAGMUS-

Saccadic
Slow defoveating movt & a fast refoveating movt.

PENDULAR NYSTAGMUS-

Non-saccadic
Both the foveating & defoveating movts are equal in velocity & amplitude.

Amplitude of nystagmus – means how far the eyes move

Frequency of nystagmus –means how often the eyes oscillate

MIXED NYSTAGMUS

Pendular nys in prim gaze & jerk nys on lateral gaze.

CLINICAL TYPES-

PHYSIOLOGICAL NYSTAGMUS- [ D-04]

END-GAZE NYSTAGMUS-

Fine jerky nystagmus in extreme gaze pos

B. OPTO-KINETIC NYSTAGMUS-

Jerk nys induced by moving repeatitive visual patterns across the visual field

C. VESTIBULAR NYSTAGMUS-

Jerk nys
Slow phase initiated by vestibular nuclei
Fast phase initiated by brainstem & frontomesencephalic pathway
COWS-
Cold water poured into right ear-->Left jerk nys
Warm water poured into right ear->Right jerk nys
Cold water poured into both ears simultaneously→ jerk nys with fast phase upwards
Warm water in both ears simultaneously→ Jerk nys with fast phase downwards.
COLD SLOWS THINGS DOWN

MOTOR IMBALANCE NYSTAGMUS-

1.CONGENITAL NYSTAGMUS-

* X-linked recessive or AD

* Jerk or pendular type

* Binocular & similar amplitude in both the eyes

* good V/A

* uniplanar

* Null zone present. So abnml head posture.

* High astigmatism→ Rx –contact lens

* Horizontal

* Dampened by eye closure [sleep] & convergence

* Persists thru out life.

2.SPASMAS MUTANS-

* Pendular nys

* Abnml head posture

* Head nodding

* Occurs bet 4mo & 2yrs of age

* diff in maintaining fixation

* Insufficient control d/t instable motor cortical centres

3.LATENT NYSTAGMUS-

* Bil, jerk & horizontal nys

* With both eyes open-No nys

* Nys on covering one eye

* Fast phase in dir of uncovered eye

* Asstd with-Esotropia & DVD

4.PERIODIC ALTERNATING NYSTAGMUS-

* Conjugate horizontal jerk nys that periodically reverses its direction

* Causes- Demyelination

-Brainstem dis

5.CONVERGENCE RETRACTION NYSTAGMUS-

* Caused by co-contraction of EO ms

* Jerk nys induced by passing an OKN tape downwards

* Upwards refixation saccade brings the two eyes towards each other

* Asstd with globe retraction

* Lesion-Pe-tectal area

DOWNBEAT NYSTAGMUS-

Vertical nys with fast phase downwards
Increases in lateral gaze
Lesion- Cervico-medullary juncn at the foramen magnum
Causes-Arnold Chiari malformn

-Syringobulbia

-Wernicke’s encephalopathy

-Hydrocephalus

-Demyelination

-Lithium,phenytoin,carbemazepine,barbiturates,alcohol

6.UPBEAT NYSTAGMUS-

* Vertical nys with fast phase upwards

* Causes- Posterior fossa lesion

-Wernicke’s encephalopathy

7.SEE-SAW NYSTAGMUS-

* Pendular nys in which one eye elevates & intorts & the other eye depresses & extorts.

* Cause- Chiasmal lesion with bitemporal hemianopia

-III ventricle

-syringobulbia

-brainstem stroke

ATAXIC NYSTAGMUS-

Horizontal jerk nys which occurs in the abducting eye.
* Cause-INO

9.MINER’S NYSTAGMUS-

* Rotatory rapid nys

* Defective vision at night with dancing movt of light objects.

* pendular nys in prim pos & later jerky nys in lateral gaze

* due to low illumination in mine workers

10.NYSTAGMUS BLOCKAGE SNY-

* Purposive esotropia dampens the nys

* compensatory phen

T/T-

A] General Rx-

* Rx of cause

* good food

* Visual hygiene

B] Specific Rx-

A) CONSERVATIVE-

1) OPTICAL-

* Correction of refractive error

* Stimulating accommodative convergence- by overcorrecting minus lenses

* Gallilean arrangement of contact lenses & spec

* CL-For high ref error.They give good visual stim for fusional control

B) PRISMOTHERAPY-

1. Base –out prism [7PD]- For fusional convergence→ Decreases nystagmus in congenital nys

2. Apex in prefered dir of gaze [ base towards face turn]

C) MEDICAL THERAPY-

1. Cyclopentolate 1 % BD

2. Botulinum A toxin –Retrobulbar space [ 10-25 U in 0.1-1ml every 3-4 mo]

3. Baclofen -5mg TDS

-Increase every 3days

-max 80 mg/day

- Periodic alternating nys

4. clonazepam- Downbeat nys

5. Carbamezepine- Sup obl myokymia

3. Propranolol- opsoclonus

D)ORTHOPTICS

1. Pleoptics

2. Penalization

3. Occlusion-

Partial occlusion of sound eye with a neutral density filter to reduce the V/A in the fixing eye below that of the amblyopic eye

B]SURGICAL-

1) Faden’s posterior fixation suture

Ind-

Abnml head posture
nystagmus blockage syn
for decreasing nys intensity

Tech- The muscle creating the nys is sutured to the sclera at the equator

2) Modified Kestenbaum surg-

-Indicated in all cases with 20 % face turn

- Recession-resection of all 4 recti [ equal amt of 5mm for all recti]

- Similarly vertical ms recession-resection for chin elevation / depression of 25 deg or more

VISUAL FIELD DEFECTS-spot

Notes-diag

OPTIC N-

A )CENTRAL SCOTOMA- Depressed area of visual field inv the fixation point.

UNILATERAL CENTRAL SCOTOMA-

Optic neuritis
Compressive lesion of ON

BILATERAL CENTRAL SCOTOMA-

Nutrional ON
Hereditary ON
Toxic ON

B )CECOCENTRAL SCOTOMA- Involves fixation pt + blind spot

Toxic ON
Serous RD
Optic pit

C ) ARCUATE SCOTOMA- Inv superior & inf arcuate nerve fibres

* Glaucoma

* AION

* Papilloedema

* Optic disc drusen

* Optic pits

* BRVO

D ) ALTITUDINAL SCOTOMA-Inv the upper / lower half of visual field in one / both eyes

1. AION

2.ONH Drusen

3. Chr papilloedema

4. ONH coloboma

5. Hemiretinal V occlusion

Strongly suggests a vascular etio

CHIASMAL LESIONS- BITEMPORAL HEMIANOPIA

Infrachiasmatic- Pituitary adenoma
Suprachiasmatic- Meningioma, craniopharyngioma
Intrachiasmatic-Glioma

PITUITARY ADENOMA-

Typical field defect- Bitemporal hemianopia
Bitemporal hemianopia→ Scotomatous

→ Non-scotomatous

Scotomatous-

Stops at the vertical meridian
Progresses Clockwise-RE

Anticlockwise-LE

-Junctional scotoma of Traquair-

Central scot in one eye & superotemporal scot in other eye.

D/t inv of Von Willibrandt’s knee [ i.e lower nasal fib of ipsilateral side loop into the C/L side]

Non-scotomatous –

Upper temporal quad are symmetrically depressed→ LT→ cross the vertical midline→ LN→ UN
Return of funcn is in opp dir.

SUPRACHIASMATIC-

Those that impinge on the chisma from anterosuperior dir→ Meningioma
Those that attack from posterosuperior dir→ Craniopharyngioma

INFRACHIASMATIC- Craniopharyngioma

PSEUDO-BITEMPORAL HEMIANOPIA-

Bil sectoral retinitis pigmentosa
Bil inferotemporal retinoschisis
Tilted disc

OPTIC TRACT-

Retrochiasmal lesions cause homonymous hemianopia i.e occur in each eye on the same side of visual field
Respect the vertical meridian
Nerve fib from corresponding retinal elements in each eye are not closely aligned in either the optic tract / LGB→ Incongruous homonymous hemiaopia [ i.e Dissimiliar field defect]

RETROGENICULATE-

OPTIC RADIATION-

Homonymous hemianopia
TEMPORAL LOBE- ‘PIE IN THE SKY’

-Inv inferior fib of optic radiation

-Lesion-Infarction

-Tum

-Abscess

-Seizures

-Visual hallucinations

* PARIETAL LOBE- ‘PIE ON THE FLOOR’

-Inv superior fib of optic radn

-Lesion-Infarction

-Tum

-Abscess

-Hemiparesis

Gertsman syn -Acalculia

-Agnosia

-Rt-Lt confusion

-Dyslexia-inability to read letters

GERTSMAN SYN-acalculia & inability to name fingers from left to right.

B. OCCIPITAL CORTEX-

* Extremely congruous

* Very complex, like pieces in a jig-saw puzzle

* Macular sparing.

Reasons-

Large macular projection in occipital cortex
Dual bld supply-Middle & posterior cerebral cir
Possibility of dual macular innervation also exists

Occipital lesions are vascular
Occipital lobe → Nml OKN
Parietal lobe→ Abnml OKN
RIDDOCH PHEN-

Specific for occipital lobe lesions

Ability to detect movts & not an object in an area of visual field.

CALCRINE FISSURE-

Lesion→ UL loss of temporal crescent
Sparing→ Preservation of temporal crescent
Thus preservatn or loss of temporal crescent proves that the lesion is in occipital cortex
CORTICAL BLINDNESS- ANTON’S SYN

Denial of blindness

Complete blindness + nml pupillary response

PUPILLARY REACTIONS

LIGHT REFLEX

Afferent- Optic N

Efferent- III N

Rods & cones → Ganglion cells → Optic N → optic chiasma [Nasal fib decussate & temporal fib remain uncrossed ]

→ Pre-tectal nucleus [Nasal fib go to C/L nu & temporal fib to I/L nu ]→ EW nu. These are the internuncial fib responsible for consensual light reflex.--> III N [inf div ]→

N to IO→ ciliary ganglion→ short ciliary Ns→ sphincter pupillae

* Normally, there is a tonic inhibitory input from the cerebral cortex to the EW nu.

* During sleep, there is dimunitionof this input resulting in papillary constriction.

FUNCTIONS OF LIGHT REFLEX-

Light ref→ pupillary constriction →less amt of light enters the eye → protects the eye against bleaching
Helps in light & dark adaptation

-Large pupil → admits more light → allows greater acuity in dim illumination.

-Small pupil → limits ref aberrations → greater acuity

WERNICKE’S PUPIL-

Lesion of optic tract
Light reflex [direct+consensual] is absent when light is thrown on the temporal retina of affected side & nasal retina of opposite side. Vice versa it is present

ILL-SUSTAINED PUPILLARY REAC-

Optic neuritis

OPTIC ATROPHY- Direct light rea -nt

-Consensual +nt

NEAR REFLEX-

TRIAD-Convergence

-Accomodation

-Pupillary constriction

SYMPATHETIC SUPPLY-

Post Hypothalamus [1st neuron ]→ Brainstem→ Ciliospinal centre of Budge [2nd neuron ]→ Sup cervical ganglion [3rd neuron ]→ ascends along the ICA→ skull→Joins oph div of V n→ via nasociliary & Long ciliary N→ ciliary body & dilator pupillae

LIGHT NEAR DISSOCIATION

Light reflex – absent / sluggish
Near reflex – nml

CAUSES-

UNILATERAL-

Afferent conduction defect
Adie’s pupil 3As + H
HZO
Aberrant regeneration of III N

BILATERAL-

Neurosyphyllis
DM
myotonic dystrophy
Parinaud’s dorsal midbrain syn
Familial amyloidosis
Encephalitis
Chr alcoholism

ARGYLL ROBERTSON PUPIL

Lesion –tectum-interfere with light reflex fibres
BL
pupils –small & irreg
Light rea- Absent
Accomodation rea – present
Good vision in both eyes
Atrophic depigmented patches on iris
Pupils do not dilate with mydriatics
Causes-

Syphillitic-tabes dorsalis

Non-syphyillitic-DM

-MS

-H’age

Tum of pre-tectal area

Site of lesion-Internuncial neuroes bet pre-tectal Nu & EW nu

ADIE’S TONIC PUPIL

Caused by denervation of the postganglionic supply to sphincter pupillae and ciliary ms
UL
Healthy young women
Pupil-large & regular-anisocoria
Light rea –absent / sluggish
Near ref –slow & tonic
Redilatation occurs slowly
Vermiform movts of pupillary border
With 0.125% pilocarpine-tonic pupil constricts rapidly

-nml pupil does not constrict

This is d/ super-sensitivity of cholinergic stim

With atropine-Tonic pupil dilates

-Argyll Robertson pupil does not

* HOLMES-ADIE PUPIL-

Adie’s pupil + Absent knee / ankle jerks

HIPPUS

Alternate rhythmic dilatation & constriction of pupil
Depends upon rhythmic activity of CNS
Seen in Multiple sclerosis

HORNER’S SYNDROME

Oculosympathetic syn

C/F-

Ptosis –d/t weakness of Muller’s ms
Elev of LL- d/t weakness of inferior tarsal ms
Miosis- d/t unopposed action of sphincter pupillae [ sphincter pup-III n,Dilator pup- Sympathetic chain ]
Nml rea to light & near
Anhydrosis
Hypochromic heterochromia
IOP is lower than 5mmHg on nml side
Accomodation is decreased
Enophthalmos

CAUSES-

CENTRAL [1st order neuron ]-post hypothalamus

Brainstem dis
Syringomyelia
Lateral medullary syn
Spinal cord tum

PRE-GANGLIONIC [2nd order ]-cilio-spinal centre of Budge

Pancoast tum
Carotid & aortic aneurysms & dissections
Neck lesions [glds,trauma,postsurg]

POSTGANGLIONIC [3rd neuron]-Superior cervical ganglion

Cluster headache
Internal carotid A dissection
Nasopharyngeal tum
Otitis media
Cavernous sinus mass

COCAINE TEST-

Cocaine 4 %- Nml pupil dilates

-Horner’s pupil does not dilate

Cocaine blocks the uptake of adrenaline that causes papillary dilatation. Since no adrenaline is available, no dilatation occurs in Horner’s syn.

HYDROXYAMPHETAMINE TEST [1%]-

To diff pre-ganglionic from post-ganglionic
Pre-ganglionic- Both pupils will dilate
Post-ganglionic-Horner’s pupil will not
Hydroxyamphetamine potentiates the release of NA from post-gang N endings.If the neuron is intact,[ 1st or 2nd order] NA will be released & pupil will dilate.In a lesion of III order neuron there will be no dilatation since the neuron is destroyed.

ADRENALINE 1: 1000-

-Opposite to the response in 1 % hydroxyamphetamine.

MIOSIS-

[< 2mm]

Bright light
Acute iritis
Opium
Morphine
Pontine H’age
Pilocarpine
Sleep

MYDRIASIS-

Dark
Angle closure glaucoma
Absolute glaucoma
Coma
Head inj
Mydriatics [atropine,homatropine]
OA
III n palsy

MIOTICS-spot

Cholinergic miotics
Sympathetic miotics

CHOLINERGIC / PARASYMPATHOMIMETIC /PARASYMPATHETIC MIOTICS-

2Types-

I] Direct stimulant at the myoneural junctn as acetylcholine-

* Pilocarpine

* Methacholine

II] Indirect stimulants-By abolishing the effect of cholinesterase [ Anticholinesterase]-

Eserine (0.25-1%)
Neostigmine
Demecarium bromide
Phospholine iodide (0.06-0.25%)

III] Combination of direct & indirect-

Carbachol
Urecholine

SYMPATHETIC MIOTICS-

Or sympatholytic
Adrenergic blocking agent→Inhibits pupillary dilatation→leaves the sphincter pupillae unopposed
Thymoxamine (0.5%)

USES OF MIOTICS-

Glaucoma
Accomodative esotropia
Accomodation failure
In cat surg before AC IOL implantation
Pre-operatively for keratoplasty
amblyopia Rx-penalisation

SIDE-EFFECTS

1.Impaired night vision

2.Reduced V/A in the presence of axial lens opacity

3.Generalised constriction of visual field

4.Spasm of accommodation→ myopia

5,Increased permeability of BAB→ Transfer of proteins, fibrin & cells into aq .In chr ant uveitis , this effect along with miosis promotes Post synechiae.

Systemic miotic→ Morphine

MYDRIATICS-spot

PARASYMPATHOLYTIC MYDRIATIC
SYMPATHOMIMETIC MYDRIATIC

PARASYMPATHOLYTIC MYDRIATIC-

Abolish the action of acetylcholine by destroying cholinesterase→ Paralysis of sphincter pupillae & ciliary ms

DRUGS-

Atropine 1%
Homatropine 1-2%
Hyosine 0.1-1%
Cyclopentolate 0.5-1%
Tropicamide 0.5-1%

USES-

1.Mydriatic uses-

* To dilate the pupil for fundus, lens,periphery & vitreous exam

* Fundus photography,FFA & photocoagn

* uveitis

* Nuclear sclerotic or posterior polar cat

* Pre-oper

2.Cycloplegic uses-

* Refraction

* Amblyopia

* Uveitis

* Post –oper

* Corneal abrasion

SIDE-EFFECTS-

Photophobia
Reduced accommodation
Acute ACG
Dry mucous memb
Tachycardia

ATROPINE-

Long-acting
Strongest
Complete dilatation in 30-40 min
Cycloplegia in 2 hrs
Effect lasts for 21 days

HOMATROPINE- 2%

short acting
Cycloplegia + mydriasis in 45-60 min
Effect lasts for 48 hrs

CYCLOPENTOLATE-1%

Short acting
Myd + cyc in 1 hr
Effect lasts for 6-12 hrs

TROPICAMIDE-1%

Short acting

SYMPATHOMIMETIC MYDRIATICS-

Act on postsynaptic receptors→release of NA→mydriasis

DRUGS-

Adrenaline [1 in 10,000] as intracameral
Phenyephrine 5-10%
Cocaine 2-4 %

SIDE-EFFECTS-

HT
Reflex bradycardia
headache,trembling,stinging
Liberate iris granules→ rise in IOP
Loss of cor microvilli
Desquamation of cells
Ischaemia d/t vessel blanching

USES-

Fundus exam
ECCE + / - PCIOL
Break post synechiae

C/I OF MYDRIATICS-

ACG
Very shallow AC
Iris –fixated IOL

CONGENITAL ON ANOMALIES

OPTIC DISC DRUSENS-

DEF- OD drusens composed of hyaline like calcific material within the substance of ONH

-Bil

-Result from intracellular calcification within the axons

C/F-

Buried drusens-

-Early childhood

-Elevated disc with scalloped margins

-Blurred disc margins

-No physiological cup

-No hyperaemia of disc surface

-surface Vs are not obscured

-Anomalous vascular pattern

-Spontaneous venous pulsation

Exposed drusens-

Early teens
Emerge on the disc surf as waxy pearl like irregularities

Complications-

1.Juxtapapillary CNV

Associations-

RP
Angioid streaks
Allagille syn

INV-

USG- high acoustic reflectivity

CT scan-less sensitive
FA-Exposed drusen show autofluorescence prior to dye injection & buried drusen- late localized hyperfluorescence

d/t staining

-no leakage

[papilloedema- hyperfluorescence & late leakage]

OPTIC DISC COLOBOMA

DEF-Results from incomplete closure of choroidal fissure

-Mostly sporadic, AD may occur

-UL /BL

C/F-

-Reduced V/A

-Disc- focal,discrete,white ,bowl shaped excavation,decentered inferiorly so that inf NRR is thin or absent & nml disc tiss is confined to a small superior wedge

-Retinal vasculature nml

-Fields- superior defect

COMPLICATIONS-

Serous RD at the macula
progressive enlargement of the excavation
RRD

OCULAR ASSOCN

Microphthalmos
coloboma –iris,CB & fundus

SYSTEMIC ASSOTN

Chromosomal anomalies-Patau’s syn

-Edward’s syn

- Cat’s eye synn

2. CHARGE-

C- Coloboma

H-Heart defect

A-choanal Atresia

R- Retarded growth

G- Genital anomalies

E –Ear anomalies

MORNING GLORY SYNDROME

-Very rare

-Usually UL & sporadic

-BL & hereditary are still rarer

C/F-

V/A –very poor
Disc- enlarged with a funnel shaped excavation

-central core of whitish glial tiss at the base of the excavation-represents persistent hyaloid remnants

-Disc is surrounded by an elevated annulus of chorioretinal pigmentary disturbance

-BVs emerge from the rim of the excavation like spokes of a wheel

COMPLICATION- Serous RD

SYSTEMIC ASSN-

1.Frontonasal dysplasia

2. NF-2

OPTIC NERVE HYPOPLASIA

-UL /BL

DEF- Decreased no of nerve fibres

Caused by ingestion of foll drugs by mother during gestation

-Alcohol

-LSD

-Quinine

- protamine zinc insulin

-steroids

-Diuretics

-cold remedies

-anticonvulsants

Superior segmental hypoplasia may be asstd with maternal DM

C/F-

V/A- normal to no PL
Disc –small & grey surrounded by a halo of hypopigmentation caused by concentric chorioretinal atrophy [double ring sign]
Distance from the fovea to the temporal border of the disc equals or exceeds 3 times the disc dia.This strongly suggests disc hypoplasia
BV?
s are of normal caliber
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Ophthalmology Notes

SECTIONS

Ophthalmology Notes @ OphthalNotes.blogspot.com

NEURO OPHTHALMOLOGY NOTES

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