Author: Oldstone, Michael B. A.
Title: Molecular mimicry and immuneâ€mediated diseases Cord-id: qg0sp2oj Document date: 1998_10_1
ID: qg0sp2oj
Snippet: Molecular mimicry has been proposed as a pathogenetic mechanism for autoimmune disease, as well as a probe useful in uncovering its etiologic agents. The hypothesis is based in part on the abundant epidemiological, clinical, and experimental evidence of an association of infectious agents with autoimmune disease and observed crossâ€reactivity of immune reagents with host ‘self’ antigens and microbial determinants. For our purpose, molecular mimicry is defined as similar structures shared by
Document: Molecular mimicry has been proposed as a pathogenetic mechanism for autoimmune disease, as well as a probe useful in uncovering its etiologic agents. The hypothesis is based in part on the abundant epidemiological, clinical, and experimental evidence of an association of infectious agents with autoimmune disease and observed crossâ€reactivity of immune reagents with host ‘self’ antigens and microbial determinants. For our purpose, molecular mimicry is defined as similar structures shared by molecules from dissimilar genes or by their protein products. Either the molecules' linear amino acid sequences or their conformational fits may be shared, even though their origins are as separate as, for example, a virus and a normal host–self determinant. An immune response against the determinant shared by the host and virus can evoke a tissueâ€specific immune response that is presumably capable of eliciting cell and tissue destruction. The probable mechanism is generation of cytotoxic crossâ€reactive effector lymphocytes or antibodies that recognize specific determinants on target cells. The induction of crossâ€reactivity does not require a replicating agent, and immuneâ€mediated injury can occur after the immunogen has been removed—a hitâ€andâ€run event. Hence, the viral or microbial infection that initiates the autoimmune phenomenon may not be present by the time overt disease develops. By a complementary mechanism, the microbe can induce cellular injury and release self antigens, which generate immune responses that crossâ€react with additional but genetically distinct self antigens. In both scenarios, analysis of the T cells or antibodies specifically engaged in the autoimmune response and disease provides a fingerprint for uncovering the initiating infectious agent.—Oldstone, M. B. A. Molecular mimicry and immuneâ€mediated diseases. FASEB J. 12, 1255–1265 (1998)
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