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UVEA- 1
Dr. K. Srikanth M.S,D.O, DNB
• At the end of the session you will be able to
• Understand the basics of Uveitis
• Know various types of uveitis
• How to manage a case of uveitis
• Know the causes of defective vision in uveitis
Uvea
Middle, pigmented, structures of the eye
includes the iris, ciliary body, and choroid
Highly vascular layer
 Various functions
1. Regulation of entry of light
2. Accommodation
3. Production of aqueous
4. Nutrition to outer layers of retina
Clinical Approach to Uveitis
• Uveitis inflammation (ie, -itis) of the uvea
broadly categorized
• Infectious and non-infectious
• Frequently associated with systemic disease,
Classification of Uveitis
• based on anatomy(the portion of the uvea
involved),
• clinical course (acute, chronic, or recurrent),
• etiology(infectious or noninfectious),
• histology (granulomatous ,nongranulomatous)
The SUN Working Group
• Etiologic categories (infectious or noninfectious)
• Anatomical classification into 4 groups
• anterior uveitis
• intermediate uveitis
• posterior uveitis
• panuveitis
The SUN Working Group Anatomical
Classification of Uveitis
Type Primary Site of Inflammation Includes
• Anterior uveitis Anterior chamber Iritis
Iridocyclitis
Anterior cyclitis
• Intermediate uveitis Vitreous Pars planitis
Posterior cyclitis
Hyalitis
• Posterior uveitis Retina or choroid Focal, multifocal, or diffuse
Choroiditis
Chorioretinitis
Retinochoroiditis
Retinitis
Neuroretinitis
• Panuveitis Anterior chamber, vitreous,
and retina or choroid
Descriptors in Uveitis
Category Descriptor Comment
• Onset Sudden
Insidious
• Duration limited < 3 months' duration
Persistent >3 months' duration
• Course Acute sudden onset limited duration
Recurrent Repeated episodes separated by
periods of inactivity without
treatment >3 months' duration
Chronic Persistent uveitis with relapse
<3 months after discontinuing
treatment
Granulomatous
• Mutton fat KPs
• Dense PS
• Iris nodules
• Invasion by live
organism/hypersensi
tivity
• Insidious onset,
chronic course
Non Granulomatous
• Fine KPs
• Filiform PS
• No nodules
• Allergic/exudative
• Acute onset, short
duration
Anterior Uveitis
• The anterior chamber is the primary site of
inflammation.
• iritis -Inflammation confined to the anterior
chamber
• iridocyclitis -If it spills over into the retrolental
space
• keratouveitis -if it involves the cornea
• sclerouveitis -if the inflammatory reaction
involves the sclera and uveal tract
Intermediate Uveitis
• Major site of inflammation is the vitreous.
• Inflammation of the middle portion (posterior
ciliary body, pars plana) of the eye
• Manifests primarily as floaters-affecting vision;
• The eye frequently appears quiet externally.
• Visual loss is primarily a result of chronic
cystoid macular edema (CME) or cataract
Posterior Uveitis
• intraocular inflammation primarily involving the
retina and/or choroid.
• Inflammatory cells may be observed diffusely
throughout the vitreous cavity, overlying foci of
active inflammation, or on the posterior vitreous
face.
Ocular examination reveals
• focal, multifocal, or diffuse areas of retinitis or
choroiditis, with
• varying degrees of vitreous cellular activity
Pan uveitis
• primary sites of inflammation in panuveitis
(diffuse uveitis) are the anterior chamber,
vitreous, and retina or choroid.
• Associated with many systemic infectious and
non-infectious diseases
Clinical Course
• Acute, chronic or recurrent :
• acute - episodes of sudden onset and limited duration that usually
resolve within a few weeks to months.
• chronic uveitis - persistent. with relapse in less than 3 months after
discontinuing treatment.
• Recurrent uveitis is characterized by repeated episodes separated
by periods of inactivity without treatment 3 months or longer in
duration
• May occur in one or both eyes. or it may alternate between them.
• The distribution of ocular involvement- focal. multi focal. or diffuse
• Non-granulomatous inflammation typically has a lymphocytic
• and plasma cell infiltrate
• granulomatous reactions also include epithelioid and giant cells
Symptoms of Uveitis
• Depend on which part of the uveal tract is inflamed,
the rapidity of onset (sudden or insidious), the duration
of the disease (limited or persistent). and the course of
the disease (acute. chronic. or recurrent)
• Acute-onset anterior uveitis (iridocyclitis)
• Pain, photophobia, redness and blurred vision
• Pain -acute onset of inflammation in the region of the
iris as in acute iritis or from secondary glaucoma.
• Referred pain that seems to radiate over the larger
area served by cranial nerve V (the trigeminal nerve).
• Epiphora, redness and photophobia are usually
present when inflammation involves the iris, cornea,
or iris-ciliary body.
• chronic iridocyclitis (in patients with
juvenile idiopathic arthritis)
• May not be associated with any symptoms at all
• Blurred vision may develop as a result of calcific band
keratopathy, cataract, or CME
• Intermediate uveitis
• Symptoms of floaters and blurred vision.
• Floaters result from the shadows cast by vitreous
cells and snowballs on the retina.
• Blurred vision may be caused by CME or vitreous
opacities in the visual axis
Posterior uveitis
• painless decreased visual acuity, floaters, photopsia,
metamorphopsia, scotomata, nyctalopia, or a combination of these.
Blurred vision may be caused by the retinitis or choroiditis
• CME, epiretinal membrane, retinal ischemia, and choroidal
neovascularization.
• from refractive error such as a myopic or
hyperopic shift associated with macular edema
• Blurred vision include opacities in the visual axis from inflammatory
cells, fibrin, or protein in the anterior chamber; keratic precipitates
(KPs); secondary cataract; vitreous debris; macular edema; and
retinal atrophy
Signs of Uveitis
Signs of Uveitis
Anterior Segment
• keratic precipitates
• Inflammatory cells
• Flare
• Hypopyon
• pigment dispersion
• pupillary miosis
• Iris nodules synechiae, both anterior and
posterior
• Band keratopathy (seen with long-standing
uveitis)
Keratic precipitates
• Collections of inflammatory cells on the corneal endothelium.
• When newly formed, they tend to be white and smoothly rounded, but
they then become crenated ( shrunken),pigmented, or glassy Large,
yellowish K Ps are described as
• mutton-fat K Ps; usually associated with granulomatous types of
inflammation
• Number of inflammatory cells seen in a I-mm x I
-mm high powered beam at full intensity at a
45°_60° angle
Iris involvement :
• anterior or posterior synechiae,
• iris nodules (Koeppe nodules at the pupillary border, Busacca
nodules within the iris stroma, and Berlin
nodules in the angle)
• iris granulomas,
• heterochromia (eg, Fuchs heterochromic iridocyclitis), or stromal
atrophy (eg, herpetic uveitis)
• Intraocular pressure (lOP) -often low
secondary to decreased aqueous production
or increased alternative outflow
• lOP may increase - if the meshwork becomes
clogged by inflammatory cells or debris or
trabeculitis
• Pupillary block with iris bombe and secondary
angle closure - acute rise in lOP
Intermediate Segment
• vitreal inflammatory cells , vitreous haze
• snowball opacities, which are common with
sarcoidosis or intermediate uveitis
• Exudates over the pars plana (snowbank).
Active snowbanks have a fluffy or shaggy
appearance
• vitreal strands
• Chronic uveitis may be associated with cyclitic
membrane formation, secondary ciliary body
detachment, and hypotony
Posterior Segment
• Retinal and choroidal signs may be unifocal, multifocal,
or diffuse
• Retinal or choroidal inflammatory infiltrates
• Inflammatory sheathing of arteries or veins
• Exudative, tractional, or rhegmatogenous retinal
detachment
• Retinal pigment epithelial hypertrophy or atrophy'
• atrophy or swelling of the retina, choroid, or optic
nerve head‘
• preretinal or sub retinal fibrosis
• Retinal or choroidal neovascularization
Laboratory and Medical Evaluation
• Medical history, review of systems , thorough
ophthalmologic and general physical examination
• There is no one standardized battery of tests that needs to
be ordered for all patients with uveitis
• When the history and physical examination
• do not clearly indicate the cause rule out the most common
causes. which include syphilis, sarcoidosis and tuberculosis
• Purified protein derivative (PPD) skin test
• serum angiotensin-converting enzyme (ACE)
• syphilis serologies
• chest radiograph or chest computed tomography
Ancillary testing
• Fluorescein angiography (FA)- for evaluating eyes
with chorioretinal disease and structural complications
caused by posterior uveitis
• CME ( Flower petal pattern of
• Leakage)
• retinal vasculitis
• secondary choroidal or retinal neovascularization
• areas of optic nerve, retinal, and choroidal inflammation
• Optical coherence tomography (OCT)
• OCT has become a standard of care for the objective
measurement of
• Uveitic CME ,
• Retinal thickening,
• subretinal fluid associated with choroidal
neovascularization,
• serous retinal detachments
• limited by media opacities
Fundus autofluorescence imaging - emerging noninvasive modality
• utilizes the fluorescent properties of lipofuscin to assess the viability of
the retinal pigment epithelium (RPE)- photoreceptor complex in
inflammatory chorioretinopathies
lndocyanine green angiography-patterns of hypofluorescence in the
presence of inflammatory choroidal vasculopathies
Ultrasonography - useful in demonstrating
• vitreous opacities,
• choroidal thickening,
• retinal detachment,
• cyclitic membrane formation, particularly if media opacities preclude a
view of the posterior segment
Anterior chamber paracentesis
Vitreous biopsy
Chorioretinal biopsy
Medical Management of Uveitis
Goal
• effectively control inflammation
• eliminate or reduce the risk of vision loss from
structural and functional complications that
result from uncontrolled inflammation
Includes
• topical cycloplegics,
• topical or systemic nonsteroidal anti-inflammatory drugs
• topical or systemic corticosteroids
Mydriatic and Cycloplegic Agents
• Beneficial for breaking or preventing the
formation of posterior synechiae
• For relieving photophobia secondary to ciliary
spasm.
• Cycloplegics commnly used.
• Cyclopentolate hydrochloride 1%
• Atropine 1%
• Homatropine 2%
• Tropicamide 0.5%
Nonsteroidal Anti-Inflammatory
Drugs
• work by inhibiting cyclooxygenase (COX)
isoforms l and 2 or 2 alone
• Reduce the synthesis of prostaglandins that
mediate inflammation
• Ketorolac and 2 newer agents bromfenac and
nepafenac - used for the treatment of CME.
Corticosteroids
• Mainstay of uveitis therapy
• Treatment of active inflammation in the eye
• Prevention or treatment of complications such as
CME
• Reduction of inflammatory infiltration of the retina,
choroid, or optic nerve
Topical administration
• Effective primarily for anterior uveitis
• .
• Routes of Administration
• Topical
• Oral
• Sub tenon
• Intra vitreal
Systemic administration
• Supplement or replace other routes of administration
• Used for vision-threatening chronic uveitis when
topical corticosteroids are insufficient or when systemic
disease also requires therapy
• The dosing and taper should be individualized to the
patient
• If corticosteroid therapy is required for longer than 3
months. Immuno-modulatory therapy (IMT) is
indicated
• 1- 2 mg/kg/day of oral prednisone
• Gradually tapered every 1 to 2 weeks until the
disease is quiescent.
• ,
• Blockers or proton pump inhibitors to prevent
gastric and peptic ulcers
• Long-term corticosteroid therapy -
supplement the diet with calcium and vitamin
D to lessen the chances of osteoporosis.
lmmunomodulatory Medications
• severe, Sight-threatening uveitis
• who are resistant to or cannot tolerate
corticosteroids
• Work by killing the rapidly dividing clones of
lymphocytes that are responsible for the
inflammation
Indications :
• vision-threatening intraocular inflammation
• Reversibility of the disease process
• Inadequate response to corticosteroid treatment
• Failure of therapy
• corticosteroids contraindicated because of systemic
problems
• unacceptable corticosteroid side effects
• chronic corticosteroid dependence
• antimetabolites.
• inhibitors of T-cell signaling
• alkylating agents
• biologic response modifiers
• Renal and hepatic toxicity,
• Bone marrow suppression, and increased
susceptibility to infection
• Blood monitoring including complete blood
count and liver and renal function tests
ANTERIOR UVEITIS
Symptoms:
• Acute
– Pain
– Photophobia
– Conjunctival injection
– Decreased vision
• Chronic
– Decreased vision
Aetiopathogenesis
• Inflammatory
infective exogenous infections(perf wound/ulcer)
secondary infections(cornea/sclera/retina)
endogenous(blood stream)
immune related(sensitization of ocular tissue to unknown Ag)
• Neoplastic
Masquerade syndrome
• Traumatic
blunt/penetrating
surgical
Associated Diseases
• Non granulomatous uveitis - Acute:
Idiopathic
Infections
HLA-B27 associated
IBD
Lens induced
Posner Schlossmann syndrome
Trauma
Chronic :
JIA
Fuch’s heterochromic iridocyclitis
Associated Diseases
• Granulomatous Uveitis -Acute: Rare
• Chronic :
Sarcoidosis
TB
Syphilis
Leprosy
HSV,HZV
Brucellosis
Phacoanaphylactic
IRITIS
• CCC
• Hyperemia,exudation &swelling of iris
 Pupil constriction
 Sluggishly acting pupil
 Pattern of iris-blurred & indistinct (Muddy iris)
• Albuminous exudate into the AC
 Flare/cells/KPs/PS
IRITIS
• Profuse exudation-Plastic iridocyclitis
• Ectropion uvae(contraction of organising exudates upon
iris)
• Seclusio pupillae (Annular/Ring synechiae)
• Iris bombe - PAS - Sec.ACG
• Occlusio pupillae
• Cyclitic membrane
• Phthisis bulbi
Cyclitis
• KPs
• Anterior vitreous opacities
• Total PS
• Cyclitic membrane
• Hypotony(destruction of ciliary processes)
• Phthisis bulbi
KPs
Fibrin
Posterior synechiae
Hypopyon
Ciliary flush
Flare
Possible questions
• Classify Uveitis,List the various forms of uvitis
• List the various clinical features of irido cyclitis
• Discuss the management of a case of chronic
irido cyclitis
• List the differnces between Granulomatous
and Non –granulomatous irdo cyclitis
• List the various factors which lead to defective
vision in a case of iridocyclitis

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Classifications of etio pathogenesis of ueitis, anterior uieitis-dr.k.srikanth 17.03.16

  • 1. UVEA- 1 Dr. K. Srikanth M.S,D.O, DNB
  • 2. • At the end of the session you will be able to • Understand the basics of Uveitis • Know various types of uveitis • How to manage a case of uveitis • Know the causes of defective vision in uveitis
  • 3. Uvea Middle, pigmented, structures of the eye includes the iris, ciliary body, and choroid Highly vascular layer  Various functions 1. Regulation of entry of light 2. Accommodation 3. Production of aqueous 4. Nutrition to outer layers of retina
  • 4. Clinical Approach to Uveitis • Uveitis inflammation (ie, -itis) of the uvea broadly categorized • Infectious and non-infectious • Frequently associated with systemic disease,
  • 5. Classification of Uveitis • based on anatomy(the portion of the uvea involved), • clinical course (acute, chronic, or recurrent), • etiology(infectious or noninfectious), • histology (granulomatous ,nongranulomatous)
  • 6. The SUN Working Group • Etiologic categories (infectious or noninfectious) • Anatomical classification into 4 groups • anterior uveitis • intermediate uveitis • posterior uveitis • panuveitis
  • 7. The SUN Working Group Anatomical Classification of Uveitis Type Primary Site of Inflammation Includes • Anterior uveitis Anterior chamber Iritis Iridocyclitis Anterior cyclitis • Intermediate uveitis Vitreous Pars planitis Posterior cyclitis Hyalitis • Posterior uveitis Retina or choroid Focal, multifocal, or diffuse Choroiditis Chorioretinitis Retinochoroiditis Retinitis Neuroretinitis • Panuveitis Anterior chamber, vitreous, and retina or choroid
  • 8. Descriptors in Uveitis Category Descriptor Comment • Onset Sudden Insidious • Duration limited < 3 months' duration Persistent >3 months' duration • Course Acute sudden onset limited duration Recurrent Repeated episodes separated by periods of inactivity without treatment >3 months' duration Chronic Persistent uveitis with relapse <3 months after discontinuing treatment
  • 9. Granulomatous • Mutton fat KPs • Dense PS • Iris nodules • Invasion by live organism/hypersensi tivity • Insidious onset, chronic course Non Granulomatous • Fine KPs • Filiform PS • No nodules • Allergic/exudative • Acute onset, short duration
  • 10. Anterior Uveitis • The anterior chamber is the primary site of inflammation. • iritis -Inflammation confined to the anterior chamber • iridocyclitis -If it spills over into the retrolental space • keratouveitis -if it involves the cornea • sclerouveitis -if the inflammatory reaction involves the sclera and uveal tract
  • 11. Intermediate Uveitis • Major site of inflammation is the vitreous. • Inflammation of the middle portion (posterior ciliary body, pars plana) of the eye • Manifests primarily as floaters-affecting vision; • The eye frequently appears quiet externally. • Visual loss is primarily a result of chronic cystoid macular edema (CME) or cataract
  • 12. Posterior Uveitis • intraocular inflammation primarily involving the retina and/or choroid. • Inflammatory cells may be observed diffusely throughout the vitreous cavity, overlying foci of active inflammation, or on the posterior vitreous face. Ocular examination reveals • focal, multifocal, or diffuse areas of retinitis or choroiditis, with • varying degrees of vitreous cellular activity
  • 13. Pan uveitis • primary sites of inflammation in panuveitis (diffuse uveitis) are the anterior chamber, vitreous, and retina or choroid. • Associated with many systemic infectious and non-infectious diseases
  • 14. Clinical Course • Acute, chronic or recurrent : • acute - episodes of sudden onset and limited duration that usually resolve within a few weeks to months. • chronic uveitis - persistent. with relapse in less than 3 months after discontinuing treatment. • Recurrent uveitis is characterized by repeated episodes separated by periods of inactivity without treatment 3 months or longer in duration • May occur in one or both eyes. or it may alternate between them. • The distribution of ocular involvement- focal. multi focal. or diffuse • Non-granulomatous inflammation typically has a lymphocytic • and plasma cell infiltrate • granulomatous reactions also include epithelioid and giant cells
  • 15. Symptoms of Uveitis • Depend on which part of the uveal tract is inflamed, the rapidity of onset (sudden or insidious), the duration of the disease (limited or persistent). and the course of the disease (acute. chronic. or recurrent) • Acute-onset anterior uveitis (iridocyclitis) • Pain, photophobia, redness and blurred vision • Pain -acute onset of inflammation in the region of the iris as in acute iritis or from secondary glaucoma. • Referred pain that seems to radiate over the larger area served by cranial nerve V (the trigeminal nerve). • Epiphora, redness and photophobia are usually present when inflammation involves the iris, cornea, or iris-ciliary body.
  • 16. • chronic iridocyclitis (in patients with juvenile idiopathic arthritis) • May not be associated with any symptoms at all • Blurred vision may develop as a result of calcific band keratopathy, cataract, or CME • Intermediate uveitis • Symptoms of floaters and blurred vision. • Floaters result from the shadows cast by vitreous cells and snowballs on the retina. • Blurred vision may be caused by CME or vitreous opacities in the visual axis
  • 17. Posterior uveitis • painless decreased visual acuity, floaters, photopsia, metamorphopsia, scotomata, nyctalopia, or a combination of these. Blurred vision may be caused by the retinitis or choroiditis • CME, epiretinal membrane, retinal ischemia, and choroidal neovascularization. • from refractive error such as a myopic or hyperopic shift associated with macular edema • Blurred vision include opacities in the visual axis from inflammatory cells, fibrin, or protein in the anterior chamber; keratic precipitates (KPs); secondary cataract; vitreous debris; macular edema; and retinal atrophy
  • 19. Signs of Uveitis Anterior Segment • keratic precipitates • Inflammatory cells • Flare • Hypopyon • pigment dispersion • pupillary miosis • Iris nodules synechiae, both anterior and posterior • Band keratopathy (seen with long-standing uveitis)
  • 20. Keratic precipitates • Collections of inflammatory cells on the corneal endothelium. • When newly formed, they tend to be white and smoothly rounded, but they then become crenated ( shrunken),pigmented, or glassy Large, yellowish K Ps are described as • mutton-fat K Ps; usually associated with granulomatous types of inflammation
  • 21.
  • 22. • Number of inflammatory cells seen in a I-mm x I -mm high powered beam at full intensity at a 45°_60° angle
  • 23. Iris involvement : • anterior or posterior synechiae, • iris nodules (Koeppe nodules at the pupillary border, Busacca nodules within the iris stroma, and Berlin nodules in the angle) • iris granulomas, • heterochromia (eg, Fuchs heterochromic iridocyclitis), or stromal atrophy (eg, herpetic uveitis)
  • 24. • Intraocular pressure (lOP) -often low secondary to decreased aqueous production or increased alternative outflow • lOP may increase - if the meshwork becomes clogged by inflammatory cells or debris or trabeculitis • Pupillary block with iris bombe and secondary angle closure - acute rise in lOP
  • 25. Intermediate Segment • vitreal inflammatory cells , vitreous haze • snowball opacities, which are common with sarcoidosis or intermediate uveitis • Exudates over the pars plana (snowbank). Active snowbanks have a fluffy or shaggy appearance • vitreal strands • Chronic uveitis may be associated with cyclitic membrane formation, secondary ciliary body detachment, and hypotony
  • 26. Posterior Segment • Retinal and choroidal signs may be unifocal, multifocal, or diffuse • Retinal or choroidal inflammatory infiltrates • Inflammatory sheathing of arteries or veins • Exudative, tractional, or rhegmatogenous retinal detachment • Retinal pigment epithelial hypertrophy or atrophy' • atrophy or swelling of the retina, choroid, or optic nerve head‘ • preretinal or sub retinal fibrosis • Retinal or choroidal neovascularization
  • 27. Laboratory and Medical Evaluation • Medical history, review of systems , thorough ophthalmologic and general physical examination • There is no one standardized battery of tests that needs to be ordered for all patients with uveitis • When the history and physical examination • do not clearly indicate the cause rule out the most common causes. which include syphilis, sarcoidosis and tuberculosis • Purified protein derivative (PPD) skin test • serum angiotensin-converting enzyme (ACE) • syphilis serologies • chest radiograph or chest computed tomography
  • 28. Ancillary testing • Fluorescein angiography (FA)- for evaluating eyes with chorioretinal disease and structural complications caused by posterior uveitis • CME ( Flower petal pattern of • Leakage) • retinal vasculitis • secondary choroidal or retinal neovascularization • areas of optic nerve, retinal, and choroidal inflammation
  • 29. • Optical coherence tomography (OCT) • OCT has become a standard of care for the objective measurement of • Uveitic CME , • Retinal thickening, • subretinal fluid associated with choroidal neovascularization, • serous retinal detachments • limited by media opacities
  • 30. Fundus autofluorescence imaging - emerging noninvasive modality • utilizes the fluorescent properties of lipofuscin to assess the viability of the retinal pigment epithelium (RPE)- photoreceptor complex in inflammatory chorioretinopathies lndocyanine green angiography-patterns of hypofluorescence in the presence of inflammatory choroidal vasculopathies Ultrasonography - useful in demonstrating • vitreous opacities, • choroidal thickening, • retinal detachment, • cyclitic membrane formation, particularly if media opacities preclude a view of the posterior segment Anterior chamber paracentesis Vitreous biopsy Chorioretinal biopsy
  • 31. Medical Management of Uveitis Goal • effectively control inflammation • eliminate or reduce the risk of vision loss from structural and functional complications that result from uncontrolled inflammation Includes • topical cycloplegics, • topical or systemic nonsteroidal anti-inflammatory drugs • topical or systemic corticosteroids
  • 32. Mydriatic and Cycloplegic Agents • Beneficial for breaking or preventing the formation of posterior synechiae • For relieving photophobia secondary to ciliary spasm. • Cycloplegics commnly used. • Cyclopentolate hydrochloride 1% • Atropine 1% • Homatropine 2% • Tropicamide 0.5%
  • 33. Nonsteroidal Anti-Inflammatory Drugs • work by inhibiting cyclooxygenase (COX) isoforms l and 2 or 2 alone • Reduce the synthesis of prostaglandins that mediate inflammation • Ketorolac and 2 newer agents bromfenac and nepafenac - used for the treatment of CME.
  • 34. Corticosteroids • Mainstay of uveitis therapy • Treatment of active inflammation in the eye • Prevention or treatment of complications such as CME • Reduction of inflammatory infiltration of the retina, choroid, or optic nerve Topical administration • Effective primarily for anterior uveitis • .
  • 35. • Routes of Administration • Topical • Oral • Sub tenon • Intra vitreal
  • 36. Systemic administration • Supplement or replace other routes of administration • Used for vision-threatening chronic uveitis when topical corticosteroids are insufficient or when systemic disease also requires therapy • The dosing and taper should be individualized to the patient • If corticosteroid therapy is required for longer than 3 months. Immuno-modulatory therapy (IMT) is indicated
  • 37. • 1- 2 mg/kg/day of oral prednisone • Gradually tapered every 1 to 2 weeks until the disease is quiescent. • ,
  • 38. • Blockers or proton pump inhibitors to prevent gastric and peptic ulcers • Long-term corticosteroid therapy - supplement the diet with calcium and vitamin D to lessen the chances of osteoporosis.
  • 39. lmmunomodulatory Medications • severe, Sight-threatening uveitis • who are resistant to or cannot tolerate corticosteroids • Work by killing the rapidly dividing clones of lymphocytes that are responsible for the inflammation
  • 40. Indications : • vision-threatening intraocular inflammation • Reversibility of the disease process • Inadequate response to corticosteroid treatment • Failure of therapy • corticosteroids contraindicated because of systemic problems • unacceptable corticosteroid side effects • chronic corticosteroid dependence
  • 41. • antimetabolites. • inhibitors of T-cell signaling • alkylating agents • biologic response modifiers • Renal and hepatic toxicity, • Bone marrow suppression, and increased susceptibility to infection • Blood monitoring including complete blood count and liver and renal function tests
  • 42. ANTERIOR UVEITIS Symptoms: • Acute – Pain – Photophobia – Conjunctival injection – Decreased vision • Chronic – Decreased vision
  • 43. Aetiopathogenesis • Inflammatory infective exogenous infections(perf wound/ulcer) secondary infections(cornea/sclera/retina) endogenous(blood stream) immune related(sensitization of ocular tissue to unknown Ag) • Neoplastic Masquerade syndrome • Traumatic blunt/penetrating surgical
  • 44. Associated Diseases • Non granulomatous uveitis - Acute: Idiopathic Infections HLA-B27 associated IBD Lens induced Posner Schlossmann syndrome Trauma Chronic : JIA Fuch’s heterochromic iridocyclitis
  • 45. Associated Diseases • Granulomatous Uveitis -Acute: Rare • Chronic : Sarcoidosis TB Syphilis Leprosy HSV,HZV Brucellosis Phacoanaphylactic
  • 46. IRITIS • CCC • Hyperemia,exudation &swelling of iris  Pupil constriction  Sluggishly acting pupil  Pattern of iris-blurred & indistinct (Muddy iris) • Albuminous exudate into the AC  Flare/cells/KPs/PS
  • 47. IRITIS • Profuse exudation-Plastic iridocyclitis • Ectropion uvae(contraction of organising exudates upon iris) • Seclusio pupillae (Annular/Ring synechiae) • Iris bombe - PAS - Sec.ACG • Occlusio pupillae • Cyclitic membrane • Phthisis bulbi
  • 48. Cyclitis • KPs • Anterior vitreous opacities • Total PS • Cyclitic membrane • Hypotony(destruction of ciliary processes) • Phthisis bulbi
  • 50. Possible questions • Classify Uveitis,List the various forms of uvitis • List the various clinical features of irido cyclitis • Discuss the management of a case of chronic irido cyclitis • List the differnces between Granulomatous and Non –granulomatous irdo cyclitis • List the various factors which lead to defective vision in a case of iridocyclitis