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Evi-2,一个参与小鼠髓系白血病发生的常见整合位点。

Evi-2, a common integration site involved in murine myeloid leukemogenesis.

作者信息

Buchberg A M, Bedigian H G, Jenkins N A, Copeland N G

机构信息

Mammalian Genetics Laboratory, NCI-Frederick Cancer Research and Development Center, Frederick, Maryland 21702.

出版信息

Mol Cell Biol. 1990 Sep;10(9):4658-66. doi: 10.1128/mcb.10.9.4658-4666.1990.

Abstract

BXH-2 mice have the highest incidence of spontaneous retrovirally induced myeloid leukemia of any known inbred strain and, as such, represent a valuable model system for identifying cellular proto-oncogenes involved in myeloid disease. Chronic murine leukemia viruses often induce disease by insertional activation or mutation of cellular proto-oncogenes. These loci are identified as common viral integration sites in tumor DNAs. Here we report on the characterization of a novel common viral integration site in BXH-2 myeloid leukemias, designated Evi-2. Within the cluster of viral integration sites that define Evi-2, we identified a gene that has the potential for encoding a novel protein of 223 amino acids. This putative proto-oncogene possesses all of the structural features of a transmembrane protein. Within the transmembrane domain is a "leucine zipper," suggesting that Evi-2 is involved in either homopolymer or heteropolymer formation, which may play an important role in the normal functioning of Evi-2. Interestingly, the human homolog of Evi-2 has recently been shown to be tightly linked to the von Recklinghausen neurofibromatosis locus, suggesting a role for Evi-2 in human disease as well.

摘要

BXH-2小鼠在所有已知近交系中,由逆转录病毒自发诱导的髓系白血病发病率最高,因此,它是用于鉴定参与髓系疾病的细胞原癌基因的宝贵模型系统。慢性鼠白血病病毒通常通过细胞原癌基因的插入激活或突变来诱发疾病。这些基因座在肿瘤DNA中被确定为常见的病毒整合位点。在此,我们报告BXH-2髓系白血病中一个新的常见病毒整合位点Evi-2的特征。在定义Evi-2的病毒整合位点簇中,我们鉴定出一个有潜力编码223个氨基酸的新蛋白质的基因。这个假定的原癌基因具有跨膜蛋白的所有结构特征。在跨膜结构域内有一个“亮氨酸拉链”,这表明Evi-2参与同聚物或异聚物的形成,这可能在Evi-2的正常功能中起重要作用。有趣的是,最近发现Evi-2的人类同源物与冯雷克林霍增氏神经纤维瘤病基因座紧密连锁,这也表明Evi-2在人类疾病中也发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bea3/361055/3c67ae05cd95/molcellb00045-0233-a.jpg

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