Autoimmune Disease and the Eye
Items in BOLD discussed in detail at the bottom of outline
I.Introduction
A.Important for Optometrist to recognize what ocular complications can manifest from autoimmune disease for appropriate treatment, testing, and referral.
II.Goals
A.Recognize signs/symptoms of autoimmune disease affecting the eye
B.Understand systemic complications of autoimmune disease
C.Learn how/when to refer to specialist
III.This lecture is designed to examine the eye (anterior to posterior) and learn how autoimmune disease affects each structure. This is similar to how an Optometrist would discover autoimmune related disease in the eye.
IV.External
A.Ptosis
1.Myasthenia Gravis
a)Chronic autoimmune neuromuscular disease causing muscle weakness
b)Antibodies destroy or alter receptors for acetylcholine. This prevents muscle contraction from occurring.
c)Some patients develop thymoma - need to check thymus gland
d)Eyelid muscles first affected in most cases
e)Test
(1)Tensilon
(2)Ice-pack test
(3)Acetylcholine receptor antibodies
(4)Anti-MuSK antibody
f)Treat
(1)Neostigmine
(2)Pyridostigmine
B.Exophthalmos
1.Graves’ Disease
C.Diplopia
1.Graves’Disease
2.Myasthenia Gravis
3.Multiple Sclerosis
a)Inflammatory (? infectious) disease that causes nerve demylenation
b)Can cause many problems including optic neuropathy and diplopia
c)Typically recover from diplopia without treatment
d)If diplopia appears atypical or combined with other symptoms (numbness, tingling, heat intolerance) - may consider MS testing
4.Giant Cell Arteritis
V.Episclera
A.Not as likely as Scleritis to have systemic association
1.If nodular and/or recurrent, consider list given with Scleritis
VI.Sclera
A.Scleritis
1.Rheumatoid Arthritis
a)Inflammatory damage to small joints in hands and feet
b)Leads to pain, swelling and possible deformity
c)Can cause pain in larger joins such as hip, shoulder, knees, ankles, and elbows
d)Often diagnosed with a combination of blood work, x-ray, and clinical signs/symptoms
e)Treated with NSAIDs for mild cases
f)Can use steroids, DMARDs, and/or immune modulating drugs
g)Most likely systemic cause of scleritis is RA
(1)Keep in mind that only 50% of patients with scleritis have associated condition
(2)Patients with RA and scleritis have a more widespread and aggressive systemic disease and may need more aggressive therapy
2.Lupus
a)Lupus is an autoimmune disease that can affect: joints, skin, kidneys, blood cells, brain, heart and lungs
b)Signs and symptoms often include: fatigue, shortness of breath, chest pain, classic “butterfly”rash on cheeks and nose
c)Most commonly seen in women of childbearing age
d)Difficult to diagnose
e)Treated with NSAID, steroid, Plaquenil, immune suppression
3.HLA-B27 Disease (not as likely) - see discussion on Uveitis for diagnosis strategy
a)Ulcerative Colitis
b)Ankylosing Spondylitis
c)Reactive Arthritis
d)Psoriatic Arthritis
VII.Cornea/Dry Eye
A.Sjogren’s
1.Autoimmune disease that mainly causes: dry eye and dry mouth
2.Can also have joint pain, fatigue, persistent cough
3.Typically in women over 40
4.Can have association with RA or Lupus
5.Diagnosis is made by signs/symptoms, blood test, lip biopsy?
6.Treat specific symptoms
7.Treat salivation (pilocarpine), may also use Plaquenil
B.Graves’Disease
C.Lupus
D.Rheumatoid Arthritis
VIII.Uvea/Uveitis
A.Ulcerative Colitis
B.Ankylosing Spondylitis
C.Reactive Arthritis
D.Psoriatic Arthritis
E.Rarely Lupus
F.Sarcoidosis
IX.Retina
A.Vasculitis
1.How to recognize vasculitis
2.Who to refer to
B.Plaquenil Retinopathy
C.Arterial Disease
1.Giant Cell Arteritis
X.Optic Nerve
A.Multiple Sclerosis
B.Sarcoidosis
C.Lupus
D.Giant Cell Arteritis
1. Graves’ Disease
I.Graves Disease (GD) is an autoimmune disease that targets 3 tissues
i.Orbit
ii.Thyroid
iii.Skin
a.Previous thinking was that GD damaged the thyroid gland which led to ophthalmic complications
b.Current knowledge states that GD is an autoimmune disease that can affect orbit, thyroid, and skin independently. It is not the thyroid directly leading to ocular damage.
II.Pathogenesis
a.Body produces autoantibodies to TSH receptor which chronically stimulates synthesis.
i. Leads to abnormally high T3 and T4
ii.Negative feedback loop decreases TSH which increases T3 and T4
b.Simultaneously affects orbit fat and muscle
i.Fibroblasts
ii.Myofibroblasts
III.Ocular Signs and Symptoms
a.Exophthalmos –always bilateral though often asymmetric
i.Most common cause at 50%
b.Dry eye
i.Foreign body sensation, Epiphora
ii.If severe enough can lead to corneal complications
c.Eye Pain
d.Diplopia–possible muscle restriction
e.Eyelid retraction - from overactive sympathetic innervations to upper eyelid
f.Redness
g.Rarely Optic Nerve Compression
IV.Thyroid Labs
a.Hyperthyroidism
i.Majority of patients with GD get this ~80%
ii.Nervousness
iii.Heat Intolerance/Sweating
iv.Tremor
v.Increased appetite
b.Hypothyroidism
i.Uncommon in GD –but up to 15%
ii.Lethargic
iii.Low appetite
iv.Low sex drive
v.Weight gain
vi.Cold, clammy
c.Euthyroid
i.Uncommon in GD ~ 5%
ii.No thyroid symptoms
iii.Skin Manifestations
iv.Pre-tibial
V.Treatment
a.Most patients stabilize over 8-36 months
b.Systemic Steroids
c.Radiotherapy
d.Anti-thyroid medication
e.Thyroidectomy
f.Psychiatric Medication
i.Quality of Life
g.Orbital Decompression
i.Likely need strabismus surgery also due to diplopia
1.As high as 64% after decompression
h.Topical Lubrication
i.Treating exposure keratopathy
i.Smoking cessation!
i.Helps progression of disease
ii.Helps prognosis for recovery
iii.Non-smokers (or those who quit) do better with treatment
iv.Weight loss
j.Neuropsychological and Mental Health
i.Often overlooked symptom of Graves’
ii.Depression
iii.Tension
iv.Anxiety
2. Giant Cell Arteritis
a.Giant Cell Arteritis (GCA) is an Immune-Mediated Vasculitis
b.Affects Medium and Large Arteries
i.In eye mostly Posterior Ciliary Artery (PCA), then Central Retinal Artery (CRA), rarely Ophthalmic Artery (OA)
ii.Explain why GCA affects eyes
iii.Called GCA because of granulomatous inflammation. Arteries lined with multinucleated giant cells: macrophages, lymphocytes, and fibroblasts
c.Incidence of 2.3/100,000 in 6th decade. Increases with Age.
d.Happens mostly to those > 50 years old
i.Age range
e.Predilection for North European, Scandinavian descent. Typically Caucasian though can happen in other races
f.Why is it important?
i.Profound vision loss
1.Causes A-AION
2.Can become bilateral in 14 days in 1/3 if untreated
3.Treatable
g.CRAO and Cilioretinal artery occlusion can occur
h.A-AION
i.Sudden painless vision loss
ii.Unilateral Optic Disc Edema
iii.1/10 patients (> 50 years old) with optic disc edema are A-AION. Other 9/10 NA-AION
i.Systemic Symptoms
i.Jaw Claudication (Odds Ratio 9.0)
ii.Neck Pain (Odds Ratio 3.4)
iii.Anorexia
iv.Less predictable symptoms
1.Headache
2.Fever
3.Scalp Tenderness
4.Malaise
v.Average number of symptoms =
j.Visual Symptoms/Signs
i.Sudden, painless vision loss
ii.31% had amaurosisfugax 1-2 weeks before
1.This can be misleading. Not saying 31% of patients with AmaurosisFugax have GCA
iii.6% diplopia
iv.8% ocular pain
v.Optic Disc Edema “chalky white pallor”
k.Lab Testing
i.ESR –86% sensitive
ii.CRP –100% sensitive, 82% specific
iii.Combined ESR and CRP –99% sensitive, 97% specific
iv.CBC with differential looking for disease that can affect Red Blood Cells (i.e. Anemia, Polycythemia Vera)
l.Other Diagnostic Testing
i.Fluorescein Angiography (FA) –characteristic late filling of choroid in the 2 weeks after Optic Disc Edema starts
ii.Ultrasound, PET, MRI of limited benefit
iii.Temporal Artery Biopsy –especially indicated if clinical symptoms highly suggestive but either ESR or CRP are inconclusive
m.Contralateral optic nerve can give us clues to A-AION vs. NA-AION
i.Go through Bayesian analysis
1.If C/D is > 0.4 1/5 have A-AION
2.If C/D is < 0.3 1/15 have A-AION
n.Treatment
i.Most studied and likely still most effective is oral steroid
1.80-100 mg/day until labs normalize
2.Then taper for VERY long (years!)
3.Evidence still lacks because not ethical to have a placebo group
ii.No evidence that IV steroid in mega dose any more effective
iii.Limited evidence for TNF blockers, Methotrexate and other immune modulators
3. Uveitis
II.The Goal of Treatment
A.Improve patient’s quality of life
III.Associated Conditions
A.What is the purpose of evaluating for associated conditions?
1.Find something that once found will help alleviate uveitis and prevent recurrence.
2.Correctly name a condition that was previously named incorrectly –leading to better treatment of non-ophthalmic condition
3.Should leave the patient better after the testing
B.We need a thoughtful approach that matches the description of uveitis with patient’s symptoms.
C.A “scatter”approach is not good medical care because:
1.It is no more beneficial to patient than tailored approach
2.There is added expense
3.There is added anxiety
4.Increase in false positives
V.A tailored workup should be specific to your patient. It requires that you know:
A.A working list of common associated conditions
B.The characteristics of the uveitis of those conditions
1.Acute vs. Chronic –Can be acute and recur. Recurrent does not mean Chronic
2.Anterior vs. Posterior (or Panuveitis)
3.Unilateral vs. Bilateral (or Alternating)
4.Granulomatous vs. Non-Granulomatous–Often difficult to distinguish. Look for Granulomas, Bussaca nodules or Mutton Fat KP
C.The history and physical findings that might manifest in a patient with one of these conditions
D.What specialized testing used to identify these conditions (if indicated)
E.The appropriate referral/treatment when a condition is diagnosed or suspected
F.Meshing these five areas will allow for appropriate testing and eliminate unnecessary tests. (e.g. a patient with acute, unilateral, non-granulomatous uveitis should not be tested for Sarcoid.)
VI.Common associated conditions and their characteristics
A.Ankylosing Spondylitis, Reactive Arthritis, Psoriasis - Acute, anterior, unilateral, nongranulomatous.
B.Inflammatory Bowel Diseases–Typically unilateral and non-granulomatous. However, some report up to 50% bilateral. Forty percent of uveitis is anterior (40% is panuveitis, 20% posterior)
C. Juvenile Idiopathic Arthritis–Chronic, anterior, unilateral or bilateral, nongranulomatous, asymptomatic. “White eye uveitis.”
D.Sarcoid –Chronic, anterior (can be posterior or pan), bilateral, granulomatous
VII.Signs/Symptoms, Follow-up Testing, and Treatment of Associated Conditions
A.Ankylosing Spondylitis
1.Lower back pain/stiffness in morning > 30 minutes, back pain improves with exercise, awakening in second half of night from back pain. All back pain is worse with rest.
2.Sacro-iliac joint x-ray and referral
3.Treatment typically NSAID. TNF Blockers work very well but are very expensive
B.Reactive Arthritis
1.Most patients with Reactive Arthritis lack the full triad of “Reiter’s Syndrome.”Acute, asymmetric oligoarthritis (typically knee, ankle, foot). Can also have symptoms of urethritis, diarrhea, or cutaneous lesions (usually soles of hands or palms of hands). Musculoskeletal symptoms follow GI or GU symptoms by 2-4 weeks.
2.Refer to Rheumatology. Laboratory tests are not indicated for diagnosis.
3.Treatment is pain management. This includes, but not limited to, Physical Therapy, NSAID, Steroid, Anti-rheumatic medication.
C.Inflammatory Bowel Disease
1.GI symptoms such as stomach cramps, diarrhea, bloody stools
2.Refer to GI
3.Treatment has a multi-step approach: Fiber, Aminosalicylates, and Corticosteroids
D.Psoriasis
1. Plaques on skin - red with white scaly top
2.Can affect scalp, skin near joints
3.Refer to dermatology
4.Treatment includes shampoos, ointments, immune modulation
E.Juvenile Idiopathic Arthritis
1.Suspect in children with non-traumatic iritis. Usually found with unilateral cataract and white eye uveitis.
2.Possible joint pain/stiffness
3.Refer to pediatrician
4.Treatment typically NSAID.
F.Sarcoid
1.Skin involvement (Macules, Papules, Granulomas), pulmonary symptoms such as dyspnea or cough
2.Order chest x-ray. Refer. ACE is a non-specific test with a poor sensitivity.
3.Treatment: Immune suppression. Typically Corticosteroids.
4. Plaquenil Retinopathy
VI.Hydroxychloroquine (Plaquenil)
a.Used for
i.Lupus
ii.Rheumatoid Arthritis
iii.Sjogren’s
iv.Lyme arthritis
b.Several side effects. Mostly worried about vision changes
c.Damages Ganglion cells, Photoreceptors, RPE
i.Leads to atrophy of macular tissue 5-10 degrees from fovea
ii.Paracentral scotoma
iii.Irreversible damage
d.Risk Factors
i.Age > 60*
ii.Retinal Disease? –possibly
iii.Renal and/or Liver Disease
iv.Daily Dose
v.Cumulative Dosage
e.Daily Dose
i.Typically 400 mg/day
ii.Used to worry about weight
iii.Does not store in fatty tissue
iv.Concern now with height/ideal weight
f.Cumulative Dosage
i.1000 g = 400 mg/day for >5-7 years
ii.If patient takes for less than 5 years, risk is 1/1000
iii.If patient takes for greater than 5 years risk is 1/100
VII.Testing
a.Should not be confused with “screening”
b.Several tests are widely used
i.Amsler Grid
ii.Color vision
iii.10-2 Visual Field
iv.Multifocal ERG (MFERG)
v.Fundus Autofluoresence (FAF)
vi.OCT
vii.Fundus examination
c.The following tests are not recommended
i.Time domain OCT
ii.Fluorescein Angiography
iii.Full Field ERG
iv.EOG
v.Amsler Grid/Color Vision –not sensitive enough
d.MFERG
i.Pros
1.Objective
2.Reliable
3.Targets macula
ii.Cons
1.Interpretation
2.Expense
3.Hassle
4.Accessibility
e.FAF
i.Pros
1.Objective
2.View changes over time
ii.Cons
1.Interpretation
2.Availability
3.Not as reliable as 10-2, SD-OCT, ERG
f.10-2 Visual Field
i.Pros
1.Available
2.Inexpensive
3.Easy interpretation
ii.Cons
1.Subjective
2.Patients dislike
3.False positives!!
g.SD-OCT –Look for Flying Saucer sign
i.Pros
1.Available
2.Objective
3.Interpretation easy
4.Good Specificity
ii.Cons
1.Early detection may be difficult
2.Poor sensitivity
3.Cost
VIII.American Academy of Ophthalmology 2002 recommendations
a.Patient is high risk if > 6.5 mg/kg/day
b.Color vision
c.10-2 or Amsler Grid
IX.American Academy of Ophthalmology 2011 recommendations
a.High risk if 1000g cumulative dose
b.Consider height
c.No color vision or Amsler Grid testing
d.Should do 10-2 combined with
i.SD-OCT, FAF, mfERG
e.Recommend baseline exam
i.If high risk, test yearly
ii.If low risk, test again after 5 years
II.American Academy of Ophthalmology 2011 recommendations
a.High risk if 1000g cumulative dose
b.Consider height
i.5'5" for men
ii.5'7" for women
iii.For every 2" below ideal, subtract 1 tablet per week
c.Consider weight
i.180 lbs for 400mg
ii.Subtract 1 tablet per week for every 13 lbs less
d.No color vision or Amsler Grid testing
e.Should do 10-2 combined with
i.SD-OCT, FAF, mfERG
e.Recommend baseline exam
i.If high risk, test yearly
ii.If low risk, test again after 5 years
X.Frustrations with diagnosing and managing Plaquenil Maculopathy
a.False positives
b.There is no gold standard
c.We are the authority –often the eye doctor will dictate who gets taken off meds
d.Difficult to balance risks/benefits of Plaquenil
e.It is possible that we are taking many patients off Plaquenil that would greatly benefit from the medication. These patients may have discontinued it due to our recommendations. We may have arrived at the recommendation from false positive testing. Optometrists need to understand our role in this diagnosis and management and be very careful before recommending stopping a potentially very helpful medicine.