首页> 外文期刊>Oncogene >FRA16D common chromosomal fragile site oxido-reductase (FOR|[sol]|WWOX) protects against the effects of ionizing radiation in Drosophila
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FRA16D common chromosomal fragile site oxido-reductase (FOR|[sol]|WWOX) protects against the effects of ionizing radiation in Drosophila

机译:FRA16D常见的染色体脆性位点氧化还原酶(用于|ρ|型Wwox)可防止电离辐射在果蝇中的影响

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摘要

Fragile sites are chromosomal structures that have been proposed to have a determining role in cancer-associated DNA instability. The human WWOX gene spans the FRA16D chromosomal fragile site, the common minimal region of homozygous deletion found in adenocarcinomas and three out of five translocation breakpoints in multiple myeloma. Transcripts from the alternatively spliced WWOX gene encode proteins with common N-terminal WW domains and variable homology to the oxidoreductase family of proteins. In this study, the Drosophila orthologue of the WWOX gene was identified and subjected to mutagenesis via homologous recombination. The resultant DmWWOX1 mutants were viable but exhibited an increased sensitivity to ionizing radiation. This radiation sensitivity was rescued by reintroduction and expression of either the wild-type Drosophila or human WWOX genes. Thus, the protective function of DmWWOX in response to irradiation in Drosophila is conserved with human WWOX (hWWOX). This is consistent with a protective role for hWWOX where aberrant expression, as a result of breakage at the associated fragile site, could contribute directly to cancer progression.
机译:脆弱的位点是已经提出的染色体结构,其在癌症相关的DNA不稳定性中具有确定作用。人WWOX基因跨越FRA16D染色体脆弱位点,在腺癌中发现的纯合缺失的常见区域和多种骨髓瘤中的五个易位断裂点中的三个。可替代的Wwox基因对蛋白质的转录物与常见的N-末端WW结构域编码和可变同源物与氧化还原酶的蛋白质。在该研究中,通过同源重组鉴定了Wwox基因的果蝇原理和对诱变进行诱变。所得DMWWOX1突变体是可行的,但表现出对电离辐射的敏感性增加。通过重新引入和表达野生型果蝇或人WWOX基因来拯救这种辐射敏感性。因此,DMWWOX响应于果蝇在果蝇的辐射响应的保护功能被人类威毒(HWWOX)保守。这与HWWOO的保护作用一致,其中由于相关脆弱位点的破裂而导致异常表达,可以直接促进癌症进展。

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