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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >The importance of making ends meet: mutations in genes and altered expression of proteins of the MRN complex and cancer.
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The importance of making ends meet: mutations in genes and altered expression of proteins of the MRN complex and cancer.

机译:收支相抵的重要性:MRN复合体和癌症的基因突变和蛋白质表达的改变。

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摘要

The MRN protein complex, consisting of MRE1, RAD50 and NBS1, plays a crucial role in sensing DNA double-strand breaks (DSBs), and it is involved in cell cycle control. This makes the MRN complex an important guard of genome stability. Hypomorphic mutations in NBS1 result in the Nijmegen breakage syndrome (NBS), which is characterized by, among other things, an increased predisposition to malignancies, especially leukemia/lymphoma. Relatives of NBS patients carrying heterozygous mutations are also more prone to cancer development. This review summarizes several studies searching for associations between heterozygous mutations in NBS1, MRE11, and RAD50 and cancer and examining the levels of expression of proteins coded by these genes in tumor tissues. The results indicate that both decreased and increased expression of NBS1 may contribute to tumorigenesis, whereas overexpressed RAD50 has an anti-tumoric effect. MRE11 and RAD50 are also affected in tumors with microsatellite instability. However, the outcomes of association studies, which concerned primarily lymphomas/leukemias and breast cancer, were inconclusive. Heterozygous NBS1 mutations and molecular variants 657del5, I171V, R215W and E185Q were most commonly analyzed. Among these, an association with cancer was found most frequently for 657del5 (in leukemia/lymphoma and breast cancer) and I171V (in leukemia, breast, head and neck and colorectal cancers); however, other studies gave contradictory results. For other NBS1 as well as MRE11 and RAD50 variants, too little data were available to assess their role in cancer risk. Overall, the results suggest that heterozygous MRN complex mutations and molecular variants may contribute only to a limited fraction of tumors. This may be caused by several factors: various frequencies of the variants in specific populations, different criteria used for selection of control groups, possible effects of environmental factors, and potential interactions with variants of other low-risk genes. These issues, as well as the impact of the alterations on protein function, need to be addressed in future studies.
机译:由MRE1,RAD50和NBS1组成的MRN蛋白复合物在检测DNA双链断裂(DSB)中起关键作用,并且参与细胞周期控制。这使MRN复杂体成为基因组稳定性的重要保障。 NBS1的亚型突变会导致奈梅亨断裂综合征(NBS),其特征之一是对恶性肿瘤尤其是白血病/淋巴瘤的易感性增加。携带杂合突变的NBS患者的亲属也更容易患癌症。这篇综述总结了几项研究,以寻找NBS1,MRE11和RAD50中的杂合突变与癌症之间的关联,并研究这些基因编码的蛋白质在肿瘤组织中的表达水平。结果表明,NBS1表达的降低和升高均可能有助于肿瘤发生,而过表达的RAD50具有抗肿瘤作用。 MRE11和RAD50在微卫星不稳定性肿瘤中也受到影响。然而,主要涉及淋巴瘤/白血病和乳腺癌的关联研究的结果尚无定论。最常分析杂合NBS1突变和657del5,I171V,R215W和E185Q的分子变异。其中,与癌症的关联最常见的是657del5(在白血病/淋巴瘤和乳腺癌中)和I171V(在白血病,乳腺癌,头颈癌和结肠直肠癌中)。但是,其他研究却得出了矛盾的结果。对于其他NBS1以及MRE11和RAD50变体,只有很少的数据可用来评估其在癌症风险中的作用。总体而言,结果表明杂合的MRN复合物突变和分子变异可能仅对有限比例的肿瘤起作用。这可能是由多种因素引起的:特定人群中变体的频率不同,用于对照组的选择标准不同,环境因素的可能影响以及与其他低风险基因变体的潜在相互作用。这些问题以及这些改变对蛋白质功能的影响,需要在未来的研究中加以解决。

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