Serum sickness
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Serum sickness
Pathology
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Neonatal sepsis
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Hypersensitivity reactions
Type I hypersensitivity
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Autoimmune hemolytic anemia
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Goodpasture syndrome
Rheumatic heart disease
Myasthenia gravis
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Serum sickness
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Immune system pathology review
Blood transfusion reactions and transplant rejection: Pathology review
Immunodeficiencies: T-cell and B-cell disorders: Pathology review
Immunodeficiencies: Combined T-cell and B-cell disorders: Pathology review
Immunodeficiencies: Phagocyte and complement dysfunction: Pathology review
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Serum sickness
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First Aid
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Arthralgias
serum sickness p. 111
Lymphadenopathy
serum sickness p. 111
Proteinuria p. 619
serum sickness p. 111
Urticaria p. 487, 489
serum sickness p. 111
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Transcript
Contributors
Sarah Clifford, BMBS, BSc (Hons)
Thomas Bush
Sam Gillespie, BSc
Let's imagine for a minute that you found yourself in the somewhat unfavorable position of having been bitten by a venomous snake.
Now, to treat that, you might get injected with anti-venom, which is the serum, or just the liquid part of blood and it’s had the coagulation proteins removed, and it comes from another animal, like a mouse, and that mouse has already encountered that particular venom and so it’s developed antibodies against it. These antibodies can bind to the venom molecules and render them harmless.
Now normally that's the end of that, but in serum sickness, your immune system actually mounts an attack against the foreign serum. It’s just like attacking a friendly police officer that’s trying to help you out. Serum sickness is a type III hypersensitivity reaction, which means that it’s mediated by immune complexes, which are combinations of antibodies and soluble antigens, in this case the antigens are the foreign antibodies in the serum.
Now normally, antibodies, which are sometimes called immunoglobulins, are produced by plasma cells, which are fully mature and differentiated B cells. B cells have multiple IgM antibodies on their surface and they act like receptors. When an antigen binds to two of these receptors it’s called cross-linking. This triggers the B cell to take in the antigen, break it all apart, and present a piece on the surface on a protein called MHC class II, which stands for major histocompatibility complex class II. Nearby T helper cells can then bind to the MHC class II protein via their T cell receptor, this happens along with costimulatory molecule CD4.
The B cell’s CD40 also binds to the T cell’s CD40 ligand, and that causes the T cell to release cytokines, which then results in B cell activation and class switching, or isotype switching. This means that it changes from producing IgM antibodies to producing IgG antibodies instead.
Summary
Serum sickness is a type III hypersensitivity reaction in which a foreign blood serum causes an allergy-like response. This happens when small, soluble foreign serum, elicits the production of antibodies, and those antigens and antibodies bind together to form immune complexes. These immune complexes then build up on the basement membrane of blood vessels in various parts of the body, and then the complement system is activated and this causes inflammation in and damage to nearby tissues. Symptoms include fever, urticaria, arthralgia, proteinuria, and lymphadenopathy. The treatment for serum sickness is generally to use antihistamines and analgesics which help with symptoms and to avoid the serum that triggered the reaction in the future.
Sources
- "Harrison's Principles of Internal Medicine, Twentieth Edition (Vol.1 & Vol.2)" McGraw-Hill Education / Medical (2018)
- "CURRENT Medical Diagnosis and Treatment 2020" McGraw-Hill Education / Medical (2019)
- "Yen & Jaffe's Reproductive Endocrinology" Saunders W.B. (2018)
- "Robbins Basic Pathology" Elsevier (2017)
- "Serum sickness-like reaction associated with cefazolin" BMC Clinical Pharmacology (2006)
- "Serum Sickness" Encyclopedia of Immunology (1998)
- "Serum Sickness" Pediatric Clinical Advisor (2007)
- "Serum Sickness" Pediatric Emergency Medicine (2008)
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