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Blocking of the induction and expression of immunologically functional T lymphocytes by rat antiactivated T-cell serum
Authors:R Effros  J Fan  J Hiserodt  S Kessler  I Scher  B Bonavida
Institution:1. Washington University School of Medicine at The Jewish Hospital of St. Louis, Department of Surgery (Urology), 216 South Kingshighway, St. Louis, Missouri 63110 USA;2. St. Louis University School of Medicine at Veterans Medical Center, Department of Biochemistry, St. Louis, Missouri 63125 USA
Abstract:A hybridoma, F133, that produces macrophage activation factor (MAF) after mitogen stimulation was developed by fusing the AKR-derived BW5147 thymoma with alloantigen-stimulated C3H/HeJ splenocytes. F133 supernatants were shown to contain MAF, migration inhibition factor, and a factor capable of suppressing the plaque-forming response to sheep erythrocytes but not lymphotoxin, interleukin II, or interferon. Both concanavalin A (Con A) and phytohemagglutinin (PHA) induced MAF production by F133. Time course and dose-response experiments showed that maximal concentrations of MAF were present 48 hr after stimulation with either 1.5 μg/ml Con A or 6 μg/ml PHA. F133 and normal splenocyte MAF preparations shared physicochemical properties in that heating at 100 °C for 30 min abolished MAF activity while 56 °C for 30 min or 100 °C for 2 min had little effect. In addition, both MAF preparations were dependent on the presence of lipopolysaccharide for macrophage activation and each was inactivated by pH 4.0 or pH 10 treatment while pH 6.0 and pH 8.0 had little effect. Also, pretreatment of both MAF preparations with either trypsin or chymotrypsin inactivated MAF activity.
Keywords:Author to whom reprint requests should be addressed  
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