In vitro effects of HgCl2 on murine lymphocytes. II. Selective activation of T cells expressing certain v{beta}TCR |
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Authors: | Jiang, Yun Moller, Goran |
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Affiliation: | Department of Immunology, The Wenner-Gren Institute, Arrhenius Laboratories for natural Sciences, Stockolm University 106 91 Stockholm, Sweden |
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Abstract: | In vivo administration of HgCI2 causes autoimmune manifestationsin susceptible rats and mice. We have, previously shown thatmercury is a unique molecule that can primarily activate murineT lymphocytoes to transformation and proliferation in vitro.To test whether a specific TCR repertoire predisposes the autoimmunedevelopment induced by HgCI2 and our hypothesis that mercurymay, function as a superantigen, we examined the TCR Vßrepertoire in HgCI2-stimulated T cells from the responder BALB/cor SJL mice and the non-responder DBA/2 mice. We found a selectiveactivation of T cells bearing a certain set of TCR Vßchains in response to HgCI2, e.g. Vß6, Vß8,Vß10, and Vß14 in the BALB/c strain. Moreover,depletion of Vß8+ T cells, a family predoininantlyexpanded in the BALB/c strain upon HgCI2 stimulation, profoundlyinhibited the response to HgCI2 in this strain. An alternativeselection of Vß segments, involving Vß6,Vß7 and Vß14, was observed in the SJL strainin which the Vß8 family is genetically deleted. Mechanism(s)whereby mercury modulates the immune system under a stringentgenetic control and a possible therapeutic regime against mercury-inducedautoimmune disease by administration of antibody specific tothe TCR Vß region are discussed. |
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Keywords: | autoimmunity, mercuric chloride, T lymphocyte, Vß repertoire |
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