首页> 外文OA文献 >Idiotype profile of an immune response. II. Reversal of the relative dominance of major and minor cross-reactive idiotypes in arsonate- specific T-independent responses
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Idiotype profile of an immune response. II. Reversal of the relative dominance of major and minor cross-reactive idiotypes in arsonate- specific T-independent responses

机译:免疫反应的独特型概况。二。逆转特定的T-独立反应中主要和次要交叉反应独特型的相对优势

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摘要

Two different cross-reactive idiotype (CRI) groups are distinguishable in the Ab response of A/J mice to the p-azobenzenearsonate (ABA) hapten: CRIA and CRIm. These two groups showed distinct patterns of relative dominance in the ensuing response depending on whether the inducing Ag was a T cell-dependent (TD) form of ABA, such as ABA-KLH or ABA-CGG, or a T-independent type 1 (TI-1) form, such as ABA-Brucella abortus or ABA-lipopolysaccharide (LPS), and on whether the response was elicited in vivo or in vitro. The CRI+ component of primary in vivo plaque-forming cell (PFC) responses to TD ABA Ags was largely (greater than 90%) CRIA+ as was, to a slightly lesser extent (greater than 75%) the CRI+ portion of secondary or hyperimmune serum Ab or PFC responses to the same Ags. In contrast, in vivo primary and hyperimmune PFC responses to ABA-Bru or ABA-LPS showed a significantly lower CRIA/CRI ratio, averaging 0.5-0.6, with some individual mice giving figures as low as 0.2, indicating predominance of CRIm over CRIA. Serological analysis of hyperimmune anti-ABA Abs from a group of 5 A/J mice immunized with ABA-Bru gave a figure of less than 0.5 for the CRIA/CRI ratio. The most striking disparity from the TD pattern was seen in primary in vitro PFC responses to the TI ABA Ags; here ratios of less than 0.2 were generally seen. Since T cell removal did not alter the Id pattern in the TI responses, CRIA-specific Ts cells do not account for the weak expression of CRIA in such responses. We propose a model that explains these results on the basis of differential expression of IdX dominance by two distinct B cell subpopulations--equatable to the Lyb- 5+ and Lyb-5- B cell subsets--along with differential relative activation of these subsets in different types of responses. Examination of anti-ABA PFC responses of F1 progeny of CBA/N and A/J mice to ABA-Bru lends support to this hypothesis since CRIA expression was significantly lower in mice with the xid defect.
机译:在A / J小鼠对对偶氮苯磺酸盐(ABA)半抗原的Ab反应中,两个不同的交叉反应独特型(CRI)组是可区分的:CRIA和CRIm。根据诱导的Ag是ABA的T细胞依赖性(TD)形式(例如ABA-KLH或ABA-CGG),还是T非依赖性1型,这两组在随后的反应中表现出明显的相对优势模式。 TI-1)形式,例如ABA流产布鲁氏菌或ABA-脂多糖(LPS),以及是否在体内或体外引发反应。对TD ABA Ags的主要体内噬菌斑形成细胞(PFC)反应的CRI +成分在很大程度上(大于90%)CRIA +,而在次级或超免疫血清中CRI +部分则稍少(大于75%) Ab或PFC对相同Ag的响应。相比之下,体内对ABA-Bru或ABA-LPS的原发性和超免疫性PFC反应显示出显着较低的CRIA / CRI比,平均为0.5-0.6,一些单独的小鼠给出的数字低至0.2,表明CRIm优于CRIA。来自一组用ABA-Bru免疫的5只A / J小鼠的超免疫抗ABA抗体的血清学分析得出CRIA / CRI比值小于0.5。与TD模式最显着的差异是在对TI ABA Ags的体外PFC初始反应中发现的。在此通常看到小于0.2的比率。由于去除T细胞不会改变TI反应中的Id模式,因此CRIA特异性Ts细胞不能解释此类反应中CRIA的弱表达。我们提出了一个模型,根据两个不同的B细胞亚群(相当于Lyb-5 +和Lyb-5- B细胞亚群)对IdX优势的差异表达,以及这些亚群的相对相对激活,来解释这些结果在不同类型的响应中。 CBA / N和A / J小鼠的F1子代对ABA-Bru的抗ABA PFC反应的研究为这一假设提供了支持,因为在xid缺陷小鼠中CRIA表达明显较低。

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