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T-cell-independent and T-cell-dependent B-cell responses to exposed variant surface glycoprotein epitopes in trypanosome-infected mice.

机译:在锥虫体感染的小鼠中T细胞非依赖性和T细胞非依赖性B细胞对暴露的变异表面糖蛋白表位的反应。

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摘要

The T-cell dependency of B-cell responses to variant surface glycoprotein (VSG) epitopes exposed in their native surface conformation on Trypanosoma brucei rhodesiense clone LouTat 1 was investigated. T-cell requirements were examined by analyses of gamma globulin preparations derived from trypanosome-infected BALB/c nude (nuu) and thymus-intact (nu/+) mice. A radioimmunoassay was used to selectively quantitate antibody binding to native VSG 1 epitopes present on the surface of viable trypanosomes. Such analyses of VSG-specific antibody in infected mice demonstrated that in the absence of T cells there was a significant B-cell response to exposed VSG epitopes; however, in the presence of T cells these surface epitope-specific responses were greatly enhanced. In contrast to infection, immunization of mice with purified VSG 1 or paraformaldehyde-fixed parasites elicited significant VSG surface epitope-specific responses only in the presence of T cells (i.e., in nu/+ mice only). VSG-specific antibody responses in mice infected with three other clonal T. brucei rhodesiense populations (LouTat 1.2, 1.5, and 1.9) were found to be similar in this pattern, although not identical, to the anti-LouTat 1 responses. An important exception was that mice infected with LouTat 1.8 required T cells to produce VSG surface-specific antibody. Thus, the VSG surface epitope-specific B-cell responses in trypanosome-infected mice represent composite T-cell-independent and T-cell-dependent processes, and a significantly stronger response is made in the presence of T cells. However, immunization with VSG in the absence of infection elicited only T-cell-dependent responses. Since the relative contribution of T-cell-independent and T-cell-dependent processes to the total VSG-specific antibody produced during infection was variable (as seen with the absence of a T-cell-independent response to LouTat 1.8), this may reflect differences in the primary structure or display of VSG molecules on the trypanosome membrane or may represent active parasite interference with some epitope-specific B-cell responses.
机译:研究了布鲁氏锥虫克隆LouTat 1上B细胞对天然表面构象暴露的变异表面糖蛋白(VSG)表位的T细胞依赖性。通过分析源自锥虫体感染的BALB / c裸鼠(nu / nu)和完整胸腺(nu / +)小鼠的γ球蛋白制剂来检查T细胞的需求。使用放射免疫测定法来选择性地定量与活锥虫体表面上存在的天然VSG 1表位结合的抗体。对受感染小鼠的VSG特异性抗体的此类分析表明,在不存在T细胞的情况下,对暴露的VSG表位有明显的B细胞反应。然而,在存在T细胞的情况下,这些表面表位特异性反应大大增强。与感染相反,仅在T细胞存在的情况下(仅在nu / +小鼠中),用纯化的VSG 1或低聚甲醛固定的寄生虫免疫小鼠才会引起明显的VSG表面表位特异性反应。发现在感染了其他三个布鲁氏罗氏梭菌种群(LouTat 1.2、1.5和1.9)的小鼠中,VSG特异性抗体反应在这种模式下与抗LouTat 1反应相似,尽管并不相同。一个重要的例外是感染LouTat 1.8的小鼠需要T细胞才能产生VSG表面特异性抗体。因此,锥虫感染的小鼠中VSG表面抗原决定簇特异性B细胞反应代表复合T细胞独立和T细胞依赖过程,并且在存在T细胞的情况下产生明显更强的响应。但是,在没有感染的情况下用VSG免疫仅引起T细胞依赖性反应。由于在感染过程中T细胞非依赖性和T细胞非依赖性过程对产生的总VSG特异性抗体的相对贡献是可变的(如不存在对LouTat 1.8的T细胞非依赖性应答),这可能反映了锥虫体膜上VSG分子的一级结构或展示的差异,或可能代表了对某些表位特异性B细胞反应的主动寄生虫干扰。

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