首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Structural studies on induced antibodies with defined idiotypic specificities. IX. Framework differences in the heavy- and light-chain- variable regions of monoclonal anti-p-azophenylarsonate antibodies from A/J mice differing with respect to a cross-reactive idiotype
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Structural studies on induced antibodies with defined idiotypic specificities. IX. Framework differences in the heavy- and light-chain- variable regions of monoclonal anti-p-azophenylarsonate antibodies from A/J mice differing with respect to a cross-reactive idiotype

机译:具有确定的独特型特异性的诱导抗体的结构研究。九。来自A / J小鼠的抗p-偶氮苯基砷酸单克隆抗体的重链和轻链可变区的构架差异在交叉反应性独特型方面有所不同

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摘要

Amino terminal amino acid sequence analyses have been performed on the heavy and light chains of induced monoclonal antibodies with specificity for the hapten p-azophenylarsonate. Four of the eight antibodies react with conventional antisera to the previously described A/J anti-arsonate cross-reactive idiotype (CRI). Of the 16 chains analyzed, all but one contain sequence differences in their first framework segment (residues 1-30) that distinguish them from the heavy- and light-chain sequences found in anti-arsonate antibodies isolated from A/J serum or ascites fluid. The presence of such framework differences appears to be independent of whether or not the hybridoma antibodies bear the CRI. In spite of the framework substitutions, all four of the CRI-positive hybridoma antibodies have variable (V)-region frameworks that are very similar to each other and to the CRI-positive molecules found in A/J serum. Two of the four CRI-negative molecules are also structurally similar to the serum antibodies. Two others, however, are strikingly different from any serum anti-arsonate antibody thus far described and appear to reflect a completely separate repertoire of anti-arsonate antibodies in the A/J MOUSE. In addition, serological analyses with an anti-idiotypic antiserum generated against a CRI-positive hybridoma product suggest that each monoclonal antibody may possess individual antigenic specificities different from the determinant(s) detected with the conventional rabbit anti-CRI. The consistent appearance of framework substitutions in what has been thought to be a homogeneous antibody population has important implications for our understanding of the generation of antibody diversity and for the precise chemical definition of an idiotype.
机译:已对诱导的单克隆抗体的重链和轻链进行了氨基末端氨基酸序列分析,这些抗体对半抗原对偶氮苯基ar酸酯具有特异性。八种抗体中的四种与常规抗血清反应,形成先前描述的A / J抗砷酸盐交叉反应性独特型(CRI)。在分析的16条链中,除一条以外的所有链均在其第一个构架区段(残基1-30)中包含序列差异,这些差异将它们与从A / J血清或腹水分离的抗ar抗体中发现的重链和轻链序列区分开来。 。这种框架差异的存在似乎与杂交瘤抗体是否带有CRI无关。尽管框架被替换,所有四种CRI阳性杂交瘤抗体都具有可变的(V)区框架,这些框架彼此非常相似,并且与A / J血清中的CRI阳性分子非常相似。四个CRI阴性分子中的两个在结构上也与血清抗体相似。然而,另外两个与迄今所描述的任何血清抗砷酸盐抗体显着不同,并且似乎反映了A / J MOUSE中抗砷酸盐抗体的完全独立的库。另外,用针对CRI阳性杂交瘤产品产生的抗独特型抗血清的血清学分析表明,每种单克隆抗体可能具有与常规兔抗CRI检测到的决定簇不同的抗原特异性。在被认为是同质抗体群体中,框架取代的一致出现对于我们对抗体多样性的产生以及独特型的精确化学定义的理解具有重要意义。

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