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前淋巴细胞白血病中表达的VH基因体细胞突变频率高。

High frequency of somatic mutations in the VH genes expressed in prolymphocytic leukemia.

作者信息

Davi F, Maloum K, Michel A, Pritsch O, Magnac C, Macintyre E, Salomon-Nguyen F, Binet J L, Dighiero G, Merle-Béral H

机构信息

Département d'Hématologie, Hôpital Pitié-Salpêtrière, Paris, France.

出版信息

Blood. 1996 Nov 15;88(10):3953-61.

PMID:8916962
Abstract

Prolymphocytic leukemia (PLL) is a chronic lymphoproliferative disorder, characterized by prominent splenomegaly, prolymphocytes accounting for more than 55% of circulating lymphocytes, and short-term survival. To better characterize the nature of the cellular origin in this disease, we analyzed lg heavy chain variable region (VH) genes in eleven cases of de novo PLL Leukemic cells expressed a skewed repertoire characterized by predominant use of the V3 family members (73%), with preferential use of the V3-23 gene (50% of the VH3 genes). All sequences from expressed VH genes diverged from their putative germline counterpart, and in eight cases the divergence was greater than 5%. In seven cases, which expressed the V3-23 gene and VH4 family members, nucleotide substitutions could be confidently attributed to somatic mutations. The type and distribution of these mutations clearly indicated that in three cases the cells had been subjected to an antigen selection process. Taken together, these results suggest that B-PLL cells display a skewed repertoire of lg VH regions and probably represent, at least in some instances, expansion of postgerminal center cells that have undergone antigen driven selection.

摘要

幼淋巴细胞白血病(PLL)是一种慢性淋巴细胞增殖性疾病,其特征为显著脾肿大、幼淋巴细胞占循环淋巴细胞的55%以上以及生存期短。为了更好地描述该疾病细胞起源的本质,我们分析了11例初发PLL患者的Ig重链可变区(VH)基因。白血病细胞表达的谱系存在偏倚,其特征为主要使用V3家族成员(73%),优先使用V3-23基因(占VH3基因的50%)。所有表达的VH基因序列均与其推定的种系对应序列不同,在8例中差异大于5%。在7例表达V3-23基因和VH4家族成员的病例中,核苷酸替换可明确归因于体细胞突变。这些突变的类型和分布清楚地表明,在3例中细胞经历了抗原选择过程。综上所述,这些结果表明B-PLL细胞显示出Ig VH区谱系偏倚,并且至少在某些情况下可能代表经历了抗原驱动选择的生发中心后细胞的扩增。

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