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普鲁卡因胺引发选择性自身抗体免疫反应。

Procainamide elicits a selective autoantibody immune response.

作者信息

Rubin R L, Reimer G, McNally E M, Nusinow S R, Searles R P, Tan E M

出版信息

Clin Exp Immunol. 1986 Jan;63(1):58-67.

Abstract

The specificity of the in vivo humoral immune response elicited by procainamide was examined by solid-phase assays, immunofluorescence, immunoprecipitation and a cytotoxicity assay. Serial samples obtained from patients during their procainamide therapy showed a progressive increase in antibodies to histones and denatured DNA, and both activities decreased after discontinuation of therapy. In contrast antibodies to tetanus, human IgG (rheumatoid factor) and heterologous lymphocytes were unaffected by procainamide treatment, indicating that they were not drug-induced. Of 29 sera examined by protein-A-facilitated immunoprecipitation, four sera had antibody to ribosomal RNA and three sera immunoprecipitated a 40kD protein. Antinuclear antibodies were invariably present but absorption studies showed that these activities were due to anti-histone antibodies. These results indicate that procainamide-induced autoimmunity is characterized predominantly by an anti-histone and anti-denatured DNA immune response.

摘要

通过固相测定、免疫荧光、免疫沉淀和细胞毒性测定,研究了普鲁卡因胺引发的体内体液免疫反应的特异性。在接受普鲁卡因胺治疗的患者中获取的系列样本显示,抗组蛋白和变性DNA抗体逐渐增加,且在治疗中断后这两种活性均下降。相比之下,抗破伤风抗体、人IgG(类风湿因子)和异源淋巴细胞不受普鲁卡因胺治疗的影响,表明它们不是药物诱导的。在通过蛋白A促进的免疫沉淀检测的29份血清中,4份血清有抗核糖体RNA抗体,3份血清免疫沉淀出一种40kD蛋白。抗核抗体始终存在,但吸收研究表明这些活性是由抗组蛋白抗体引起的。这些结果表明,普鲁卡因胺诱导的自身免疫主要以抗组蛋白和抗变性DNA免疫反应为特征。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e0d7/1577356/9696a226f5c7/clinexpimmunol00124-0070-a.jpg

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