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胸苷酸合成酶缺陷的中国仓鼠细胞:一种用于人类18号染色体的选择系统以及用于研究胸苷酸合成酶调控和脆性X表达的实验系统。

Thymidylate synthase-deficient Chinese hamster cells: a selection system for human chromosome 18 and experimental system for the study of thymidylate synthase regulation and fragile X expression.

作者信息

Nussbaum R L, Walmsley R M, Lesko J G, Airhart S D, Ledbetter D H

出版信息

Am J Hum Genet. 1985 Nov;37(6):1192-205.

Abstract

Chinese hamster lung (CHL) V79 cells already deficient in hypoxanthine phosphoribosyltransferase were exposed to uv light and selected for mutations causing deficiency of thymidylate synthase (TS) by their resistance to aminopterin in the presence of thymidine and limiting amounts of methyl tetrahydrofolate. Three of seven colonies chosen for initial study were shown to be thymidylate synthase deficient (TS-) by enzyme assay, thymidine auxotrophy, and their inability to incorporate labeled deoxyuridine into their DNA in vivo. Complementation analysis of human X TS- hamster hybrids revealed that TS activity segregated with human chromosome 18. Southern analysis of a panel of 14 human X hamster hybrids probed with complementary DNA from mouse TS confirmed the chromosome assignment of TS to human chromosome 18; quantitative Southern blotting using unbalanced human cell lines further localized the gene to 18q21.31----qter. Another hybrid was generated that contained a human X chromosome with the Xq28 folate-dependent fragile site as its only human chromosome in a hamster TS- background. The fragile site could be easily and reproducibly expressed in this hybrid without the use of antimetabolites simply by removing exogenous thymidine from the medium. These TS-deficient cells are useful for: somatic cell genetics as a unique selectable marker for human chromosome 18, studies on regulation of the TS gene, and analysis of the fragile (X) chromosome and other folate-dependent fragile sites.

摘要

已经缺乏次黄嘌呤磷酸核糖转移酶的中国仓鼠肺(CHL)V79细胞暴露于紫外线,并在胸苷存在和有限量的甲基四氢叶酸的情况下,通过对氨甲蝶呤的抗性选择导致胸苷酸合成酶(TS)缺乏的突变。通过酶测定、胸苷营养缺陷以及它们在体内无法将标记的脱氧尿苷掺入其DNA中,证明最初选择进行研究的七个菌落中有三个是胸苷酸合成酶缺陷型(TS-)。对人X TS-仓鼠杂种的互补分析表明,TS活性与人类18号染色体分离。用来自小鼠TS的互补DNA探测一组14个人X仓鼠杂种的Southern分析证实了TS基因定位于人类18号染色体;使用不平衡人类细胞系的定量Southern印迹进一步将该基因定位到18q21.31----qter。产生了另一种杂种,其在仓鼠TS-背景中包含一条带有Xq28叶酸依赖性脆性位点的人类X染色体作为其唯一的人类染色体。通过简单地从培养基中去除外源性胸苷,无需使用抗代谢物,就可以在这种杂种中轻松且可重复地表达脆性位点。这些TS缺陷细胞可用于:作为人类18号染色体的独特选择标记用于体细胞遗传学、研究TS基因的调控以及分析脆性(X)染色体和其他叶酸依赖性脆性位点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/68b5/1684722/2859e986216b/ajhg00162-0152-a.jpg

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