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A组链球菌M蛋白的结构明确的多肽片段诱导人γ干扰素的产生。

Induction of human gamma interferon by structurally defined polypeptide fragments of group A streptococcal M protein.

作者信息

Weigent D A, Beachey E H, Huff T, Peterson J W, Stanton G J, Baron S

出版信息

Infect Immun. 1984 Jan;43(1):122-6. doi: 10.1128/iai.43.1.122-126.1984.

Abstract

The presence of interferon (IFN) has been demonstrated previously (i) in fluids obtained from the middle ears of children with Streptococcus pneumoniae infections, (ii) from the serum of mice injected intraperitoneally with either S. pneumoniae or Streptococcus pyogenes, and (iii) from human lymphoid cell cultures treated with a variety of bacteria. In this study, we showed that highly purified peptic extracts of three different serotypes of group A streptococcal M protein (pep M5, pep M6, and pep M24) stimulated human peripheral leukocytes to produce IFN. IFN production was apparent by 10 h and peaked 24 h after exposure. Dose-response experiments indicated that IFN could be detected in cultures treated with concentrations of M protein as low as 6 micrograms/ml, whereas maximum IFN production occurred at a concentration of 200 micrograms/ml. The IFN had antigenic and physicochemical characteristics of IFN-gamma. Preliminary leukocyte fractionation studies revealed that the IFN-producing cell was a nonadherent lymphocyte with receptors for sheep erythrocytes (T cell). Rabbit antisera specific for these structurally defined polypeptide fragments of streptococcal M protein (pep M5, pep M6, and pep M24) blocked IFN induction by each of the polypeptides. The data suggest that the different serotypes of streptococcal M protein may induce IFN by a common structural determinant shared by each of the polypeptide fragments tested.

摘要

先前已证实,在以下情况中存在干扰素(IFN):(i)从患有肺炎链球菌感染的儿童中耳获取的液体中;(ii)从腹腔注射肺炎链球菌或化脓性链球菌的小鼠血清中;(iii)从用多种细菌处理过的人淋巴细胞培养物中。在本研究中,我们发现,A组链球菌M蛋白三种不同血清型的高度纯化胃蛋白酶提取物(pep M5、pep M6和pep M24)刺激人外周血白细胞产生IFN。暴露10小时后IFN产生明显,并在24小时达到峰值。剂量反应实验表明,在用低至6微克/毫升的M蛋白浓度处理的培养物中可检测到IFN,而最大IFN产生发生在200微克/毫升的浓度下。该IFN具有IFN-γ的抗原和物理化学特性。初步白细胞分级研究表明,产生IFN的细胞是一种对绵羊红细胞有受体的非贴壁淋巴细胞(T细胞)。针对链球菌M蛋白这些结构明确的多肽片段(pep M5、pep M6和pep M24)的兔抗血清可阻断每种多肽诱导的IFN。数据表明,链球菌M蛋白的不同血清型可能通过所测试的每个多肽片段共有的共同结构决定簇诱导IFN。

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