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- W1970229594 abstract "Abstract. The first step towards understanding the cellular interaction which results in autoimmune disease is to determine what triggers the recognition between a specific autoimmune antigen determinant and the cellular receptor. In this review, we have focused on the antigen inducing experimental allergic encephalitis (EAE) because the antigen has been characterized and a relatively large body of information on its biological activities has been accumulated. Clearly, a specific allergic encephalitis-producing determinant is present and is represented on a relatively small portion of the molecule. The determinant induces a wide variety of biological reactivities, some of which are classed as cellular mediated. An attempt is made to dissect activities such as blast transformation (BT), migration inhibitory factor (MIF), in vivo delayed type hypersensitivity reaction (DTH) and EAE and to relate them to the structural requirements which the determinants possess. The complexities which arise indicate that subpopulations of cells with different receptor activities may respond selectively and that recognition of the receptor is produced by an EAE determinant consisting of three amino acids in a specific linear sequence. Furthermore, under experimental circumstances the EAE activity can be dissociated from the other activities (BT, MIF, DTH), indicating that while these tests are used generally to follow various human autoimmune disease activities, they may represent the reaction of a broad spectrum of cells." @default.
- W1970229594 created "2016-06-24" @default.
- W1970229594 creator A5006252520 @default.
- W1970229594 creator A5025585907 @default.
- W1970229594 date "1977-05-01" @default.
- W1970229594 modified "2023-09-27" @default.
- W1970229594 title "Autoimmune disease antigens1" @default.
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- W1970229594 doi "https://doi.org/10.1111/j.1600-0714.1977.tb01877.x" @default.
- W1970229594 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/68112" @default.
- W1970229594 hasPublicationYear "1977" @default.
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