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Pretreatment of P815 mastocytoma cells with inhibitors of protein synthesis reduces their susceptibility to lysis by cytotoxic thymus-derived lymphocytes
Authors:A D D'Angeac  A H Hale
Affiliation:1. Department of Biology and the Center for Cancer Research, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139, USA;2. Department of Microbiology and Immunology, The Bowman Gray School of Medicine, Winston-Salem, North Carolina 27103 USA
Abstract:
Protein synthesis inhibitors like cycloheximide, emetine, and puromycin diminish the ability of P815, a mastocytoma of DBA/2 mice, to react with anti-H-2d cytotoxic thymus-derived lymphocytes (CTLs). Compared to untreated P815, tumor cells incubated with the protein synthesis inhibitors exhibited a reduced sensitivity to lysis and a reduced ability to inhibit lysis of untreated P815 cells. Consistent with this reduced reactivity of cycloheximide-treated P815 cells with CTLs was the inability of anti-H-2d CTLs to form T cell-target cell conjugates with treated P815 cells. As evaluated by the binding of an anti-H-2d serum, treated P815 cells expressed the same amount of H-2 membrane antigen as untreated cells. However, treated cells were still lysed by CTLs in the presence of the agglutinator, concanavalin A (Con A).
Keywords:
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