Messmer Bradley T, Albesiano Emilia, Efremov Dimitar G, Ghiotto Fabio, Allen Steven L, Kolitz Jonathan, Foa Robin, Damle Rajendra N, Fais Franco, Messmer Davorka, Rai Kanti R, Ferrarini Manlio, Chiorazzi Nicholas
North Shore-LIJ Research Institute, 350 Community Dr., Manhasset, NY 11030, USA.
J Exp Med. 2004 Aug 16;200(4):519-25. doi: 10.1084/jem.20040544.
Previous studies suggest that the diversity of the expressed variable (V) region repertoire of the immunoglobulin (Ig)H chain of B-CLL cells is restricted. Although limited examples of marked constraint in the primary structure of the H and L chain V regions exist, the possibility that this level of restriction is a general principle in this disease has not been accepted. This report describes five sets of patients, mostly with unmutated or minimally mutated IgV genes, with strikingly similar B cell antigen receptors (BCRs) arising from the use of common H and L chain V region gene segments that share CDR3 structural features such as length, amino acid composition, and unique amino acid residues at recombination junctions. Thus, a much more striking degree of structural restriction of the entire BCR and a much higher frequency of receptor sharing exists among patients than appreciated previously. The data imply that either a significant fraction of B-CLL cells was selected by a limited set of antigenic epitopes at some point in their development and/or that they derive from a distinct B cell subpopulation with limited Ig V region diversity. These shared, stereotyped Ig molecules may be valuable probes for antigen identification and important targets for cross-reactive idiotypic therapy.
先前的研究表明,B - CLL细胞免疫球蛋白(Ig)H链表达的可变(V)区序列的多样性受到限制。尽管在H链和L链V区的一级结构中存在有限的显著限制实例,但这种限制程度是该疾病普遍规律的可能性尚未被接受。本报告描述了五组患者,大多数患者的IgV基因未发生突变或仅有微小突变,他们使用共同的H链和L链V区基因片段,产生了惊人相似的B细胞抗原受体(BCR),这些基因片段共享CDR3结构特征,如长度、氨基酸组成以及重组连接处的独特氨基酸残基。因此,与之前的认识相比,患者之间整个BCR的结构限制程度更为显著,受体共享频率也更高。数据表明,要么相当一部分B - CLL细胞在其发育的某个阶段被有限的一组抗原表位所选择,和/或它们源自具有有限Ig V区多样性的独特B细胞亚群。这些共享的、定型的Ig分子可能是用于抗原识别的有价值探针,也是交叉反应性独特型疗法的重要靶点。
