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利用三氟胸苷(TFT)从L5178Y/TK+/-小鼠淋巴瘤细胞中筛选胸苷激酶缺陷(TK-/-)突变体。

The utilization of trifluorothymidine (TFT) to select for thymidine kinase-deficient (TK-/-) mutants from L5178Y/TK+/- mouse lymphoma cells.

作者信息

Moore-Brown M M, Clive D, Howard B E, Batson A G, Johnson K O

出版信息

Mutat Res. 1981 Oct;85(5):363-78. doi: 10.1016/0165-1161(81)90227-2.

Abstract

Trifluorothymidine (TFT), a thymidine analog, was analyzed for its ability to select for thymidine kinase-deficient (TK-/-) mutants. In comparison with BUdR, the traditional selective agent for TK-/- cells, it was determined that TFT at 1/50th the dose (1 microgram/ml vs. 50 microgram/ml) is a more effective and versatile selective agent for TK-/- mutants arising from the TK+/- -3.7.2C heterozygote of L5178Y mouse lymphoma cells. Since TFT acts more rapidly than BUdR, it can be utilized in procedures (such as the analysis of the phenotypic lag) requiring the fast arrest of cell division. Reconstruction analyses of effective TK-/- mutant recovery indicate that TFT can be used to recover mutants from significantly higher densities of TK+/- cells than can BUdR. In addition, TK-/- mutants can attain larger colony size in TFT than in BudR where severe stunting of growth occurs at high TK-/- cell densities. 190 of 194 isolated TFT-resistant large and small colony mutants (both spontaneous and induced).

摘要

三氟胸苷(TFT),一种胸苷类似物,被分析其选择胸苷激酶缺陷(TK-/-)突变体的能力。与用于TK-/-细胞的传统选择剂溴脱氧尿苷(BUdR)相比,已确定剂量为其1/50(1微克/毫升对50微克/毫升)的TFT对于源自L5178Y小鼠淋巴瘤细胞的TK+/- -3.7.2C杂合子产生的TK-/-突变体是一种更有效且用途更广的选择剂。由于TFT比BUdR作用更快,它可用于需要快速阻止细胞分裂的程序(如表型延迟分析)。有效TK-/-突变体回收率的重建分析表明,与BUdR相比,TFT可用于从密度显著更高的TK+/-细胞中回收突变体。此外,TK-/-突变体在TFT中比在BUdR中能形成更大的集落,在BUdR中当TK-/-细胞密度高时会出现严重的生长发育迟缓。194个分离出的抗TFT的大小集落突变体(包括自发和诱导的)中有190个。

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