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A cis-Acting Diversification Activator Both Necessary and Sufficient for AID-Mediated Hypermutation

机译:AID介导的超突变所需和充分的顺式作用多样化活化剂

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摘要

Hypermutation of the immunoglobulin (Ig) genes requires Activation Induced cytidine Deaminase (AID) and transcription, but it remains unclear why other transcribed genes of B cells do not mutate. We describe a reporter transgene crippled by hypermutation when inserted into or near the Ig light chain (IgL) locus of the DT40 B cell line yet stably expressed when inserted into other chromosomal positions. Step-wise deletions of the IgL locus revealed that a sequence extending for 9.8 kilobases downstream of the IgL transcription start site confers the hypermutation activity. This sequence, named DIVAC for diversification activator, efficiently activates hypermutation when inserted at non-Ig loci. The results significantly extend previously reported findings on AID-mediated gene diversification. They show by both deletion and insertion analyses that cis-acting sequences predispose neighboring transcription units to hypermutation.
机译:免疫球蛋白(Ig)基因的超突变需要激活诱导的胞苷脱氨酶(AID)和转录,但是尚不清楚为什么B细胞的其他转录基因不会突变。我们描述了一种记者转基因,当插入或靠近DT40 B细胞系的Ig轻链(IgL)基因座时,由于超突变而受损,而当插入其他染色体位置时却稳定表达。 IgL基因座的逐步删除显示,在IgL转录起始位点下游延伸9.8公里碱基的序列赋予了超突变活性。当插入非Ig基因座时,该序列被称为DIVAC,用于多样化激活子,可有效激活超突变。该结果大大扩展了先前报道的有关AID介导的基因多样化的发现。他们通过缺失和插入分析表明顺式作用序列使邻近的转录单位易于发生超突变。

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