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一个人类基因位点的X连锁,该位点可纠正tsC1AGOH小鼠细胞中的DNA合成损伤。

X-linkage of a human genetic locus that corrects the DNA synthesis lesion in tsC1AGOH mouse cells.

作者信息

Giles R E, Ruddle F H

出版信息

Genetics. 1979 Dec;93(4):975-96. doi: 10.1093/genetics/93.4.975.

Abstract

GM 126 diploid fibroblasts were fused with a heat-sensitive mouse cell mutant defective in DNA synthesis, and primary hybrids were selected at permissive and nonpermissive temperatures in HAT medium. Primary hybrids, primary hybrid clones back-selected in 8-azaguanine at the permissive temperature, and subclones of heat-resistant primary hybrids isolated under nonselective conditions or after 8-azaguanine treatment were tested for heat sensitivity, the expression of 26 human enzymes assigned to 19 different human chromosomes, and the presence of human chromosomes. Only the human X chromosome and X-linked marker enzymes exhibited a clear pattern of concordant segregation with the heat-resistant phenotype. On the basis of these observations, we have defined the human genetic locus that corrects the heat-sensitive lesion in tsC1AGOH as hrC1AGOH and have assigned this locus to the X chromosome. This observation provides the first instance where two selectable markers (heat resistance and 8-azaguanine sensitivity) are found on a single human chromosome and suggests that these markers may prove to be a valuable push-pull selective system of use in determining the linear arrangement of genes on human chromosomes by somatic cell genetics.

摘要

将GM 126二倍体成纤维细胞与DNA合成缺陷的热敏小鼠细胞突变体融合,并在允许温度和非允许温度下于HAT培养基中筛选初级杂种。对初级杂种、在允许温度下于8-氮杂鸟嘌呤中反向选择的初级杂种克隆,以及在非选择性条件下或经8-氮杂鸟嘌呤处理后分离的耐热初级杂种的亚克隆,进行热敏感性、分配到19条不同人类染色体上的26种人类酶的表达以及人类染色体存在情况的检测。只有人类X染色体和X连锁标记酶与耐热表型呈现出明显的一致分离模式。基于这些观察结果,我们将校正tsC1AGOH中热敏损伤的人类遗传位点定义为hrC1AGOH,并将该位点定位于X染色体。这一观察结果首次表明在单个人类染色体上发现了两个选择标记(耐热性和8-氮杂鸟嘌呤敏感性),并表明这些标记可能被证明是一种有价值的推拉选择系统,可用于通过体细胞遗传学确定人类染色体上基因的线性排列。

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本文引用的文献

1
Isolation of temperature-sensitive mutants of L-cells.
Proc Natl Acad Sci U S A. 1970 Jun;66(2):377-84. doi: 10.1073/pnas.66.2.377.
10
Temperature-sensitive mutations in animal cells.
Adv Cancer Res. 1977;24:223-66. doi: 10.1016/s0065-230x(08)61016-7.

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