体细胞高频突变过程中缺失和重复的频繁发生:对癌基因易位和重链病的影响
Frequent occurrence of deletions and duplications during somatic hypermutation: implications for oncogene translocations and heavy chain disease.
作者信息
Goossens T, Klein U, Küppers R
机构信息
Institute for Genetics, University of Cologne, 50931 Cologne, Germany.
出版信息
Proc Natl Acad Sci U S A. 1998 Mar 3;95(5):2463-8. doi: 10.1073/pnas.95.5.2463.
Abstract
Human naive and germinal center (GC) B cells were sorted by flow cytometry and rearranged VH region genes were amplified and sequenced from single cells. Whereas no deletions or insertions were found in naive B cells, approximately 4% of in-frame and >40% of out-of-frame rearrangements of GC B cells harbored deletions and/or insertions of variable length. The pattern of deletions/insertions and their restriction to mutated V genes strongly suggests that they result from somatic hypermutation. Deletions and insertions account for approximately 6% of somatic mutations introduced into rearranged VH region genes of GC B cells. These deletions/insertions seem to be the main cause for the generation of heavy chain disease proteins. Furthermore, it appears that several types of oncogene translocations (like c-myc translocations in Burkitt's lymphoma) occur as a byproduct of somatic hypermutation within the GC-and not during V(D)J recombination in the bone marrow as previously thought.
摘要
通过流式细胞术对人幼稚和生发中心(GC)B细胞进行分选,从单细胞中扩增并重排VH区域基因并进行测序。在幼稚B细胞中未发现缺失或插入,而GC B细胞中约4%的框内重排和>40%的框外重排存在可变长度的缺失和/或插入。缺失/插入的模式及其对突变V基因的限制强烈表明它们是由体细胞超突变导致的。缺失和插入约占引入GC B细胞重排VH区域基因的体细胞突变的6%。这些缺失/插入似乎是重链病蛋白产生的主要原因。此外,似乎几种类型的癌基因易位(如伯基特淋巴瘤中的c-myc易位)是GC内体细胞超突变的副产物——而不是如先前认为的那样发生在骨髓中的V(D)J重组期间。
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