Optic neuritis: Difference between revisions

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===Physical Examination===
===Physical Examination===
Ophthalmic examinations including slit lamp examination and pupillary reactions (RAPD) in unilateral or bilateral asymmetric conditions allows a quantitative measurement of whether the optic neuropathy is stable, improving, or worsening [1,31,32]. Aided visual acuity (V.A) is measured for near vision by near vision plates and for distance vision by ETDRS (early treatment diabetic retinopathy chart) or retro-illuminated Bailey-Lovie chart at a distance of 4m and Snellen at 6m [31,32]. Those unable to read any letters at one meter are further examined by counting fingers, identifying hand movements or perceiving light [7]. Color vision, where V.A and central visual function allows, can be recorded using FM-100 hue test (Farnsworth Munsell 100) or Ishihara pseudoisochromatic color vision plates [1,7,9]. Contrast sensitivity can be recorded using Pelli-Robson charts at a distance of 1m [7,31] or Cambridge low contrast gratings [32]. Low-contrast letter acuity (Sloan charts) and contrast sensitivity (Pelli–Robson chart) show a strong relationship with brain MRI and RNFL thickness, by OCT [2]. Visual field determination, where aided V.A permits, recorded for both eyes by Goldmann perimeter to evaluate peripheral visual field and Humphrey field analyzer to evaluate central 30 degrees [7,31,32]. Fluorescein angiography and electroretinography (ERG) is done in case of retinal diseases [4]. Optical Coherence Tomography (OCT) is used to measure the thickness of retinal tissues which are thinned in the affected eye by ON [10,14,25,33,34]. Reduction in RNFL thickness correlates with visual acuity, visual field, color vision, contrast sensitivity and visual evoked potential (VEP) amplitude [33,34].
Physical examination of patients with optic neuritis is usually remarkable for:
 
*
Neurological examinations including orbital and brain MRI is performed with or without gadolinium (Gd) preferably within two weeks after the onset of symptoms [9,10,32]. Contrast enhancement of the optic nerve is a sensitive finding in acute ON but does not correlate with the degree of visual recovery [8,16] (Fig. ​'''1A1A''').
* Ophthalmic examination findings:
** [[Papillitis]] with swollen [[optic disc]]
** Normal [[optic disc]] appearance (2/3 of cases) in retrobulbar neuritis type of optic neuritis
** Perineuritis, which involves the [[optic nerve]] sheath while the optic disc may or may not be swollen
** Neuroretinitis with optic disc oedema and macular star exudates.


===Laboratory Findings===
===Laboratory Findings===

Revision as of 19:26, 27 November 2018

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Mohamadmostafa Jahansouz M.D.[2]

Overview

Historical Perspective

Discovery

Classification

Optic neuritis may be classified into atypical or typical subtypes based on its clinical features.[2]

  • Atypical optic neuritis entails clinical manifestations that deviate from classic pattern of optic neuritis features.[3]
  • Atypical features to consider include:[3]
    • Lack of pain
    • Simultaneous or near-simultaneous onset
    • Lack of response to or relapse upon tapering from corticosteroids
    • Optic neuritis due nerve head or peripapillary hemorrhages

Pathophysiology

Pathogenesis

Causes

The following autoimmune are associated with optic neuritis:[7][8][9]

Differentiating Optic Neuritis from other Diseases

Optic neuritis must be differentiated from other diseases that cause sudden eye pain and vision loss such as:[2]

  1. Leber’s Hereditary Optic Neuropathy (LHON)[2] which results from point mutations in mitochondrial DNA and subsequent mitochondrial dysfunction, causing bilateral central vision loss.[10]
  2. Nonarteritic Anterior Ischemic Optic Neuropathy (AION)[2]

Epidemiology and Demographics

Incidence

  • The incidence of optic neuritis is approximately 5 to 6.4 per 100 000 individuals in US.[7][11][12]

Age

  • Optic neuritis commonly affects patients between the ages of 15 and 49.[13]

Race

  • Optic neuritis usually affects individuals of the Caucasians race eight times more frequently than Blacks and Asians.[7][14][15][16]
  • Black populations individuals are less likely to develop optic neuritis.[7][14][15][16]

Gender

  • Women are more commonly affected by optic neuritis than men.[2]

Region

  • The incidence of optic neuritis is highest in populations located at higher latitudes such as:[7][17][18]
    • Northern United States
    • Northern and Western Europe
    • New Zealand and Southern Australia

Risk Factors

Common Risk Factors

Natural History, Complications and Prognosis

Natural History

  • The symptoms of optic neuritis usually develop in the second decade of life, and start with symptoms such as pain on movement of the eyes, followed by a worsening of vision.[28]
  • Common symptoms of optic neuritis include:[28][29]
    1. Pain on movement of the eyes which is sever and so disturbing
    2. Seeing things darkly, unclearly, and with poor contrast
    3. Dirty and pale Colors
    4. Visual field loss
    5. Disturbed color vision
    6. Flashing lights
  • After a sub acute onset, the patient’s visual acuity continues to deteriorate for a few more days; in the untreated course of the disease, it generally reaches its nadir in one to two weeks and then improves again.[28]

Complications

Prognosis

  • The long-term visual prognosis of idiopathic optic neuritis is generally good.[31]
  • More than 90% of the patients recover a visual acuity of 20/40 or better by 6 months.[31]
  • Findings associated with poor visual outcome at 6 months include:[32][31]
    • A cut-off level of vision ≤ 20/50
    • Contrast sensitivity of <1.0 log units
    • A visual field mean deviation of ≤ – 15 dB after 1 month in the Optic Neuritis Treatment Trial.
  • Despite the relatively good visual outcome, most patients show a degree of long-lasting damage to the optic nerve, such as:[31]

Diagnosis

Diagnosis studies

The diagnosis of typical optic neuritis is usually made clinically.[2]

The classic triad for diagnosis of optic neuritis consist of:[2][17][33]

  1. Visual loss
  2. Periocular pain
  3. Dyschromatopsia

MRI is the diagnosis study of choice for visualising the optic nerve.

The following result of MRI is confirmatory of optic neuritis:

  • Swollen retrobulbar intra-orbital segment of the optic nerve with a high T2 signal. High T2 signal persists and may be permanent;
  • Atrophied nerve in chronic cases

Other diagnosis studies which may help to diagnosis of optic neuritis include:[34][35][36]

Symptoms

  • The symptoms of optic neuritis usually develop in the second decade of life, and start with symptoms such as pain on movement of the eyes, followed by a worsening of vision.[28]
  • Common symptoms of optic neuritis include:[28][29][37]
    1. Pain on movement of the eyes which is sever and so disturbing
    2. Seeing things darkly, unclearly, and with poor contrast
    3. Dirty and pale Colors
    4. Visual field loss
    5. Disturbed color vision
    6. Flashing lights
  • After a sub acute onset, the patient’s visual acuity continues to deteriorate for a few more days; in the untreated course of the disease, it generally reaches its nadir in one to two weeks and then improves again.[28]

Physical Examination

Physical examination of patients with optic neuritis is usually remarkable for:

  • Ophthalmic examination findings:
    • Papillitis with swollen optic disc
    • Normal optic disc appearance (2/3 of cases) in retrobulbar neuritis type of optic neuritis
    • Perineuritis, which involves the optic nerve sheath while the optic disc may or may not be swollen
    • Neuroretinitis with optic disc oedema and macular star exudates.

Laboratory Findings

Imaging Findings

Other Diagnostic Studies

Treatment

Medical Therapy

Surgery

Prevention

References

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  3. 3.0 3.1 Gaier ED, Boudreault K, Rizzo JF, Falardeau J, Cestari DM (December 2015). "Atypical Optic Neuritis". Curr Neurol Neurosci Rep. 15 (12): 76. doi:10.1007/s11910-015-0598-1. PMID 26467052.
  4. 4.0 4.1 4.2 Hoorbakht H, Bagherkashi F (2012). "Optic neuritis, its differential diagnosis and management". Open Ophthalmol J. 6: 65–72. doi:10.2174/1874364101206010065. PMC 3414716. PMID 22888383.
  5. 5.0 5.1 5.2 Toosy AT, Mason DF, Miller DH (January 2014). "Optic neuritis". Lancet Neurol. 13 (1): 83–99. doi:10.1016/S1474-4422(13)70259-X. PMID 24331795.
  6. Taniguchi S, Kawano T, Kakunaga T, Baba T (May 1986). "Differences in expression of a variant actin between low and high metastatic B16 melanoma". J. Biol. Chem. 261 (13): 6100–6. PMID 3700386.
  7. 7.0 7.1 7.2 7.3 7.4 7.5 7.6 7.7 7.8 Marechal F, Berthiot G, Deltour G (1988). "Serum levels of CA-50, CA-19.9, CA-125, CA-15.3, enolase and carcino-embryonic antigen in non neoplastic diseases of the lung". Anticancer Res. 8 (4): 677–80. PMID 3178158.
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  9. 9.0 9.1 9.2 Balcer LJ (March 2006). "Clinical practice. Optic neuritis". N. Engl. J. Med. 354 (12): 1273–80. doi:10.1056/NEJMcp053247. PMID 16554529.
  10. Fujimori H (December 1973). "[Pulmonary tuberculosis--keypoints in nursing of pregnant and puerperal patients]". Josanpu Zasshi (in Japanese). 27 (12): 40–3. PMID 4492634.
  11. Rodriguez M, Siva A, Cross SA, O'Brien PC, Kurland LT (February 1995). "Optic neuritis: a population-based study in Olmsted County, Minnesota". Neurology. 45 (2): 244–50. PMID 7854520.
  12. Percy AK, Nobrega FT, Kurland LT (February 1972). "Optic neuritis and multiple sclerosis. An epidemiologic study". Arch. Ophthalmol. 87 (2): 135–9. PMID 5057861.
  13. 13.0 13.1 Self SG, Grossman EA (September 1986). "Linear rank tests for interval-censored data with application to PCB levels in adipose tissue of transformer repair workers". Biometrics. 42 (3): 521–30. PMID 3105615.
  14. 14.0 14.1 14.2 14.3 Bhigjee AI, Moodley K, Ramkissoon K (November 2007). "Multiple sclerosis in KwaZulu Natal, South Africa: an epidemiological and clinical study". Mult. Scler. 13 (9): 1095–9. doi:10.1177/1352458507079274. PMID 17967837.
  15. 15.0 15.1 15.2 15.3 Mbonda E, Larnaout A, Maertens A, Appel B, Lowenthal A, Mbede J, Evrard P (1990). "Multiple sclerosis in a black Cameroonian woman". Acta Neurol Belg. 90 (4): 218–22. PMID 2124032.
  16. 16.0 16.1 16.2 16.3 Phillips PH, Newman NJ, Lynn MJ (February 1998). "Optic neuritis in African Americans". Arch. Neurol. 55 (2): 186–92. PMID 9482360.
  17. 17.0 17.1 Shams PN, Plant GT (September 2009). "Optic neuritis: a review". Int MS J. 16 (3): 82–9. PMID 19878630.
  18. Kurtzke JF (July 1985). "Optic neuritis or multiple sclerosis". Arch. Neurol. 42 (7): 704–10. PMID 4015470.
  19. Adam MP, Ardinger HH, Pagon RA, Wallace SE, Bean L, Stephens K, Amemiya A, Yu-Wai-Man P, Chinnery PF. PMID 20301353. Vancouver style error: initials (help); Missing or empty |title= (help)
  20. 20.0 20.1 Chan JW (September 2002). "Optic neuritis in multiple sclerosis". Ocul. Immunol. Inflamm. 10 (3): 161–86. PMID 12789593.
  21. Haslbeck M (November 1974). "[Insulin secretion after glucose loading. Studies on insulin secretion in healthy and diabetic subjects after administration of glucose]". Fortschr. Med. (in German). 92 (32): 1317–8. PMID 4457437.
  22. Sawicka-Pierko A, Obuchowska I, Mariak Z (2014). "Nutritional optic neuropathy". Klin Oczna. 116 (2): 104–10. PMID 25345287.
  23. Primicerio B (January 1971). "[Competitions for the position of sanitary personnel in hospitals]". Policlinico Prat (in Italian). 78 (2): 72–7. PMID 5546777.
  24. Dyras M, Stós B, Zemowski W (1989). "[Possibilities of combined maxillary-orthopaedic and prosthetic treatment of malocclusion in adult patients]". Protet Stomatol (in Polish). 39 (3): 134–9. PMID 2701125.
  25. Warren SA, Warren KG (August 1983). "Optic neuritis, diabetes mellitus and multiple sclerosis: a three-way association". Can. J. Ophthalmol. 18 (5): 228–32. PMID 6354403.
  26. Holmberg D, Lundkvist I, Forni L, Ivars F, Coutinho A (1985). "Absence of immunoglobulin heavy chain expression results in altered kappa/lambda light chain ratios". J. Mol. Cell. Immunol. 2 (1): 51–6. PMID 3939751.
  27. Dabholkar AS, Tewari HB (1968). "The functional significance of the presence of acid phosphatase at the nucleic-acid synthesizing sites in the nuclei of the neurons of the cephalothoracic ganglionic masses of palaemnius". Acta Neurol. Scand. 44 (5): 533–41. PMID 4177903.
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  30. "Henry Edmund Seiler". Lancet. 2 (8092 Pt 1): 747. September 1978. PMID 80680.
  31. 31.0 31.1 31.2 31.3 Sagalovich V, Solov'eva IP, Kunichan AD, Nemsadze MN (1987). "[Effectiveness of single and fractional administration of isoniazid in the treatment of dogs infected with isoniazid-resistant strains of Mycobacterium tuberculosis]". Probl Tuberk (in Russian) (7): 49–53. PMID 3116540. Vancouver style error: initials (help)
  32. Achiron A, Kishner I, Sarova-Pinhas I, Raz H, Faibel M, Stern Y, Lavie M, Gurevich M, Dolev M, Magalashvili D, Barak Y (October 2004). "Intravenous immunoglobulin treatment following the first demyelinating event suggestive of multiple sclerosis: a randomized, double-blind, placebo-controlled trial". Arch. Neurol. 61 (10): 1515–20. doi:10.1001/archneur.61.10.1515. PMID 15477504.
  33. Wells H (1988). "A discussion of the KDI Quik Test Drug Screen". J Anal Toxicol. 12 (2): 111. PMID 3379920.
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