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滤泡性淋巴瘤中t(14;18)染色体易位的后果:嵌合且突变的BCL-2基因表达失调。

Consequences of the t(14;18) chromosomal translocation in follicular lymphoma: deregulated expression of a chimeric and mutated BCL-2 gene.

作者信息

Hua C, Zorn S, Jensen J P, Coupland R W, Ko H S, Wright J J, Bakhshi A

机构信息

Metabolism Branch, National Institutes of Health, Bethesda, MD 20892.

出版信息

Oncogene Res. 1988 Feb;2(3):263-75.

PMID:3285301
Abstract

The t(14;18) chromosomal translocation of human follicular lymphoma recombines the candidate transforming gene bcl-2, located at 18q21, with the immunoglobulin (Ig) H-chain joining region (JH) at 14q32. To elucidate the consequences of this translocation, we cloned bcl-2 cDNAs from a pre-B cell line (Nall-1) and a t(14;18) lymphoma cell line (SU-DHL-6) and compared these sequences with their genomic counterparts. These studies revealed the complexity of bcl-2 gene expression in which six potential polyadenylation signals in exon 3 and two different 5' exons (exons 1 and 2) and promoters are alternatively used to generate different sized bcl-2 mRNAs. A single open reading frame (ORF), at the junction of exons 2 and 3, predicts a 239 amino acid, 26 kD protein. Most chromosome 18 breakpoints cluster within a 150 bp region of exon 3. In SU-DHL-6 the t(14;18) translocation juxtaposes a truncated bcl-2 gene with J6 in a tail-to-head configuration, resulting in the deregulated expression of chimeric bcl-2/Ig transcripts. Importantly, the SU-DHL-6 bcl-2 cDNA also contained several point mutations in the ORF, two of which altered the primary amino acid sequence. The deregulated expression of an altered bcl-2 gene may play a critical role in the disordered growth and differentiation of follicular B cell lymphoma.

摘要

人类滤泡性淋巴瘤的t(14;18)染色体易位使位于18q21的候选转化基因bcl-2与位于14q32的免疫球蛋白(Ig)重链连接区(JH)发生重组。为了阐明这种易位的后果,我们从一个前B细胞系(Nall-1)和一个t(14;18)淋巴瘤细胞系(SU-DHL-6)中克隆了bcl-2 cDNA,并将这些序列与其基因组对应序列进行了比较。这些研究揭示了bcl-2基因表达的复杂性,其中外显子3中的六个潜在聚腺苷酸化信号以及两个不同的5'外显子(外显子1和2)和启动子被交替使用以产生不同大小的bcl-2 mRNA。在外显子2和3的交界处有一个单一的开放阅读框(ORF),预测有一个239个氨基酸、26 kD的蛋白质。大多数18号染色体断点聚集在外显子3的一个150 bp区域内。在SU-DHL-6中,t(14;18)易位以尾对首的构型将一个截短的bcl-2基因与J6并列,导致嵌合的bcl-2/Ig转录本的表达失调。重要的是,SU-DHL-6的bcl-2 cDNA在ORF中也包含几个点突变,其中两个改变了一级氨基酸序列。改变的bcl-2基因的表达失调可能在滤泡性B细胞淋巴瘤的无序生长和分化中起关键作用。

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