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人类15号染色体赋予着色性干皮病F组细胞部分表型互补性。

Human chromosome 15 confers partial complementation of phenotypes to xeroderma pigmentosum group F cells.

作者信息

Saxon P J, Schultz R A, Stanbridge E J, Friedberg E C

机构信息

Department of Pathology, Stanford University School of Medicine, CA 94305.

出版信息

Am J Hum Genet. 1989 Apr;44(4):474-85.

Abstract

Microcell-mediated transfer of a single human chromosome from repair-proficient human cells to genetic complementation group F cells from the hereditary disease xeroderma pigmentosum (XP) results in partial complementation of repair-defective phenotypes. The complementing chromosome was identified by cytogenetic and molecular analysis as human chromosome 15. Transfer of this chromosome to XP-F cells restores approximately 20% of the resistance of wild-type cells to killing by UV radiation or by the UV-mimetic chemical 4-nitroquinoline-1-oxide (4NQO), as well as partial repair synthesis of DNA measured as unscheduled DNA synthesis. Additionally, complemented XP-F cells have an enhanced capacity for reactivation of the plasmid-borne E. coli cat gene following its inactivation by UV radiation. Phenotypic complementation of XP cells by chromosome 15 is specific to genetic complementation group F; no effect on the UV sensitivity of XP-A, XP-C, or XP-D cells was detected. The observation that phenotypic complementation is partial is open to several interpretations and does not allow the definitive conclusion that the XP-F locus is carried on chromosome 15.

摘要

通过微细胞介导,将一条人类染色体从具有修复能力的人类细胞转移至遗传性疾病色素性干皮病(XP)的F组基因互补细胞中,结果导致修复缺陷表型得到部分互补。通过细胞遗传学和分子分析确定,这条互补染色体为人类15号染色体。将该染色体转移至XP - F细胞后,可使野生型细胞对紫外线辐射或紫外线模拟化学物质4 - 硝基喹啉 - 1 - 氧化物(4NQO)杀伤的抗性恢复约20%,同时还能使以非预定DNA合成来衡量的DNA部分修复合成得以恢复。此外,经互补的XP - F细胞在质粒携带的大肠杆菌cat基因被紫外线辐射灭活后,具有增强的再激活能力。15号染色体对XP细胞的表型互补作用对F组基因互补具有特异性;未检测到对XP - A、XP - C或XP - D细胞紫外线敏感性的影响。表型互补是部分互补这一观察结果有多种解释,且无法得出XP - F基因座位于15号染色体上的确切结论。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ffea/1715561/7122bb30752b/ajhg00114-0046-a.jpg

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