Difference between revisions of "Systemic Lupus Erythematosus"
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Skin changes include: periorbital alopecia, seborrhea, oral ulceration, [[Discoid Lupus Erythematosus]], mucocutaneous ulcerations, footpad ulceration, panniculitis and urticaria. Skin changes can be multifocal or generalised, and commonly involve skin poorly covered by hair. Lesions may be exacerbated by exposure to light. | Skin changes include: periorbital alopecia, seborrhea, oral ulceration, [[Discoid Lupus Erythematosus]], mucocutaneous ulcerations, footpad ulceration, panniculitis and urticaria. Skin changes can be multifocal or generalised, and commonly involve skin poorly covered by hair. Lesions may be exacerbated by exposure to light. | ||
| − | Other common manifestations include: '''anaemia, leucopaenia, peripheral lymphadenopathy, splenomegaly'''. | + | Other common manifestations include: '''[[:Category:Anaemia|anaemia]], leucopaenia, peripheral lymphadenopathy, splenomegaly'''. |
| − | Other reported syndromes include: pericarditis, | + | Other reported syndromes include: [[pericarditis]], [[thrombocytopaenia]], polymyositis, myocarditis, pneumonitis, pleuritis, neurologic disorders ([[seizures]], meningitis, psychosis) and lymphoedema. |
<u>Cats</u>: no age predilection, but Siamese, Himalayan and Persian breeds may be predisposed. | <u>Cats</u>: no age predilection, but Siamese, Himalayan and Persian breeds may be predisposed. | ||
| − | + | Syndromes reported include: haematological abnormalities, neurological abnormalities, fever, lymphadenopathy, polyarthritis, myopathy, oral ulceration, conjunctivitis, [[:Category:Renal failure|'''renal failure''']] and subclinical pulmonary disease. | |
| − | Only 20% of cats will have skin lesions such as seborrhea, erythema, alopecia and scarring on the face, pinnae and paws. | + | Only 20% of cats will have skin lesions such as seborrhea, erythema, [[alopecia]] and scarring on the face, pinnae and paws. |
==Diagnosis== | ==Diagnosis== | ||
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The most widely accepted diagnostic criteria for the disease is that an animal should have at least '''2 separate clinically and serologically defined manifestations of autoimmunity in addition to a high serum titre of ANA'''. | The most widely accepted diagnostic criteria for the disease is that an animal should have at least '''2 separate clinically and serologically defined manifestations of autoimmunity in addition to a high serum titre of ANA'''. | ||
| − | '''Haematology and biochemistry''' may reveal: anaemia with or without a positive direct Coombs' test result, thrombocytopaenia, leucopaenia or leucocytosis, proteinuria and hypergammaglobulinaemia. | + | '''Haematology and biochemistry''' may reveal: anaemia with or without a positive direct [[Coagulation Tests|Coombs' test result]], thrombocytopaenia, leucopaenia or leucocytosis, proteinuria and hypergammaglobulinaemia. |
| − | The '''ANA test''' is considered the most sensitive serological test for SLE. However it is not the most specific of tests, and can be positive in up to 20% of dogs with infectious diseases, particularly leishmaniasis. It is important to record the titre and compare it with normal values for the same laboratory. | + | The '''ANA test''' is considered the most sensitive serological test for SLE. However, it is not the most specific of tests, and can be positive in up to 20% of dogs with infectious diseases, particularly [[leishmaniasis]]. It is important to record the titre and compare it with normal values for the same laboratory. |
The Lupus Erythematosus '''(LE) test''' is not as valuable, varies from day to day, and lacks specificity and sensitivity. | The Lupus Erythematosus '''(LE) test''' is not as valuable, varies from day to day, and lacks specificity and sensitivity. | ||
| − | '''Pathology''' findings in the skin include: lymphohistiocytic interface dermatitis, thickened basement membrane, vasculitis, subepidermal vesicles, basal cell degeneration | + | '''Pathology''' findings in the skin include: lymphohistiocytic interface dermatitis, thickened basement membrane, vasculitis, subepidermal vesicles, basal cell degeneration. |
==Treatment== | ==Treatment== | ||
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Other drugs may be useful in combination if the response is not satisfactory, and '''azathioprine or cyclophosphamide''' can be used. Typically the dose can be tapered once the condition is under control. | Other drugs may be useful in combination if the response is not satisfactory, and '''azathioprine or cyclophosphamide''' can be used. Typically the dose can be tapered once the condition is under control. | ||
| − | '''Splenectomy''' may be necessary in animals with severe anaemia and thrombocytopaenia. ''' | + | '''Splenectomy''' may be necessary in animals with severe anaemia and thrombocytopaenia. '''Vincristine''' can be useful when thrombocytopaenia is severe. |
Animals with SLE are prone to infections and therefore any infections must be identified and dealt with effectively and quickly. | Animals with SLE are prone to infections and therefore any infections must be identified and dealt with effectively and quickly. | ||
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|flashcards = [[Veterinary Dentistry Q&A 15]] | |flashcards = [[Veterinary Dentistry Q&A 15]] | ||
| + | |literature search = [http://www.cabdirect.org/search.html?q=title%3A%28systemic+lupus+erythematosus%29+OR+title%3A%28multisystemic+immune+mediated+disease%29&fq=sc%3A%22ve%22 Systemic Lupus Erythematosus publications] | ||
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==References== | ==References== | ||
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Pasquini, C. (1999) '''Tschauner's Guide to Small Animal Clinics''' ''Sudz Publishing'' | Pasquini, C. (1999) '''Tschauner's Guide to Small Animal Clinics''' ''Sudz Publishing'' | ||
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| − | [[Category: | + | {{review}} |
| + | [[Category:Expert Review]] | ||
[[Category:Integumentary System - Autoimmune Reactions]] | [[Category:Integumentary System - Autoimmune Reactions]] | ||
[[Category:Antibody Mediated Autoimmune Diseases]] | [[Category:Antibody Mediated Autoimmune Diseases]] | ||
[[Category:Immunological Diseases - Cat]][[Category:Immunological Diseases - Dog]] | [[Category:Immunological Diseases - Cat]][[Category:Immunological Diseases - Dog]] | ||
| + | [[Category:Immunological Diseases - Horse]] | ||
Revision as of 23:08, 13 October 2011
Also known as: SLE
Introduction
Systemic Lupus Erythematous is an immune-mediated disease which can affect many different organ systems. It is an primary autoimmune disease in which the body loses 'self-tolerance' towards autoantigens and mounts an inappropriate attack on various target tissues of the body. The pathology can be attributed to true autoantibody binding, immune complex deposition causing a type III hypersensitivity reaction, or cell-mediated autoimmunity.
The most well-studied autoantibodies formed are the Anti-Nuclear Antibodies (ANA) which are found in up to 100% of cases reported and are important in the diagnosis of the disease. These target a number of nuclear components, including double-stranded DNA, histones and extractable nuclear antigens.
The aetiology of the disease is multifactorial, involving genetics, immunological disorder, viral infection and hormonal and ultraviolet light modulation.
The condition is uncommon in dogs and rare in cats and horses.
Clinical Signs
Clinical signs are varied and changeable. SLE is able to mimic numerous diseases and is sometimes called 'the great imitator'.
Dogs: there is no age predilection, but male are more commonly affected.
The most common manifestations are: fever (constant or cyclic), polyarthritis (non-erosive, non-deforming), proteinuria and skin disease.
Skin changes include: periorbital alopecia, seborrhea, oral ulceration, Discoid Lupus Erythematosus, mucocutaneous ulcerations, footpad ulceration, panniculitis and urticaria. Skin changes can be multifocal or generalised, and commonly involve skin poorly covered by hair. Lesions may be exacerbated by exposure to light.
Other common manifestations include: anaemia, leucopaenia, peripheral lymphadenopathy, splenomegaly.
Other reported syndromes include: pericarditis, thrombocytopaenia, polymyositis, myocarditis, pneumonitis, pleuritis, neurologic disorders (seizures, meningitis, psychosis) and lymphoedema.
Cats: no age predilection, but Siamese, Himalayan and Persian breeds may be predisposed.
Syndromes reported include: haematological abnormalities, neurological abnormalities, fever, lymphadenopathy, polyarthritis, myopathy, oral ulceration, conjunctivitis, renal failure and subclinical pulmonary disease.
Only 20% of cats will have skin lesions such as seborrhea, erythema, alopecia and scarring on the face, pinnae and paws.
Diagnosis
Diagnosis of SLE is made on a combination of clinical findings, haemotologic, serum biochemistry and immunological testing results. Diagnosis can be challenging as the condition can mimic a number of other diseases. Ruling out differential diagnoses will help in securing a definitive diagnosis.
The most widely accepted diagnostic criteria for the disease is that an animal should have at least 2 separate clinically and serologically defined manifestations of autoimmunity in addition to a high serum titre of ANA.
Haematology and biochemistry may reveal: anaemia with or without a positive direct Coombs' test result, thrombocytopaenia, leucopaenia or leucocytosis, proteinuria and hypergammaglobulinaemia.
The ANA test is considered the most sensitive serological test for SLE. However, it is not the most specific of tests, and can be positive in up to 20% of dogs with infectious diseases, particularly leishmaniasis. It is important to record the titre and compare it with normal values for the same laboratory.
The Lupus Erythematosus (LE) test is not as valuable, varies from day to day, and lacks specificity and sensitivity.
Pathology findings in the skin include: lymphohistiocytic interface dermatitis, thickened basement membrane, vasculitis, subepidermal vesicles, basal cell degeneration.
Treatment
Treatment is with immunosuppressive drugs.
The initial agent of choice is large doses of systemic glucocorticoids such as prednisolone.
Other drugs may be useful in combination if the response is not satisfactory, and azathioprine or cyclophosphamide can be used. Typically the dose can be tapered once the condition is under control.
Splenectomy may be necessary in animals with severe anaemia and thrombocytopaenia. Vincristine can be useful when thrombocytopaenia is severe.
Animals with SLE are prone to infections and therefore any infections must be identified and dealt with effectively and quickly.
Specific supportive care may be necessary for animals with renal disease, such as dietary manipulation.
ANA titres can be monitored throughout treatment as levels usually fall with clinical improvement, thought the antibody may persist at lower titres during clinical remission.
Prognosis
Prognosis is unpredictable and depends on the organs involved.
The earlier the diagnosis is made, the better the prognosis.
In general, dogs with muscle, joint and skin disease respond more reliably to medical treatment and remain in remission for longer than animals with severe haemolytic anaemia, thrombocytopaenia or glomerulonephritis.
Over 40% of dogs with SLE are dead within 1 year after the diagnosis is made, either from disease or from euthanasia.
| Systemic Lupus Erythematosus Learning Resources | |
|---|---|
 Test your knowledge using flashcard type questions |
Veterinary Dentistry Q&A 15 |
 Search for recent publications via CAB Abstract (CABI log in required) |
Systemic Lupus Erythematosus publications |
References
Blood, D.C. and Studdert, V. P. (1999) Saunders Comprehensive Veterinary Dictionary (2nd Edition) Elsevier Science
Merck & Co (2008) The Merck Veterinary Manual (Eighth Edition) Merial
Nelson, R.W. and Couto, C.G. (2009) Small Animal Internal Medicine (Fourth Edition) Mosby Elsevier
Muller, G. (2001) Small animal dermatology Elsevier Health Sciences
Pasquini, C. (1999) Tschauner's Guide to Small Animal Clinics Sudz Publishing
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This article has been peer reviewed but is awaiting expert review. If you would like to help with this, please see more information about expert reviewing. |