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人α1-抗胰蛋白酶基因在大鼠肝癌×人胎儿肝细胞杂种中的激活取决于人14号染色体的存在。

Activation of human alpha 1-antitrypsin gene in rat hepatoma x human fetal liver cell hybrids depends on presence of human chromosome 14.

作者信息

Pearson S J, Tetri P, George D L, Francke U

出版信息

Somatic Cell Genet. 1983 Sep;9(5):567-92. doi: 10.1007/BF01574259.

Abstract

In order to study the involvement of human chromosomes in the expression of liver-specific functions, we have produced somatic cell hybrids between a rat hepatoma (7777) cell line and human diploid skin fibroblasts (series XIX) or human fetal liver cells (series XXII). Production of human serum proteins was detected by immunoelectrophoretic analyses of concentrated serum-free hybrid culture supernatants. Human alpha 1-antitrypsin (AAT) was secreted by a subset of hybrids but not by the parental cells. The activated human AAT phenotype segregated concordantly with human chromosome 14 in 18 primarily HAT-selected and five azaguanine back-selected series XXII hybrids. All other chromosomes were excluded as playing a role in AAT expression. Therefore, the AAT gene (PI) is assigned to chromosome 14. This quasi-constitutive expression of a liver-specific function was not observed for the other serum proteins studied, nor was it seen in the skin fibroblast-derived hybrids (series XIX) although AAT was produced by some of them.

摘要

为了研究人类染色体在肝脏特异性功能表达中的作用,我们构建了大鼠肝癌(7777)细胞系与人类二倍体皮肤成纤维细胞(XIX系列)或人类胎儿肝细胞(XXII系列)之间的体细胞杂种。通过对浓缩的无血清杂种培养上清液进行免疫电泳分析来检测人血清蛋白的产生。人α1-抗胰蛋白酶(AAT)由一部分杂种分泌,但亲本细胞不分泌。在18个主要经次黄嘌呤-氨基蝶呤-胸腺嘧啶核苷(HAT)选择和5个氮杂鸟嘌呤回选的XXII系列杂种中,活化的人AAT表型与人类14号染色体一致分离。所有其他染色体被排除在AAT表达中起作用。因此,AAT基因(PI)定位于14号染色体。在所研究的其他血清蛋白中未观察到这种肝脏特异性功能的准组成型表达,在皮肤成纤维细胞来源的杂种(XIX系列)中也未观察到,尽管其中一些杂种产生了AAT。

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