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γ-谷氨酰转肽酶的表达使肿瘤细胞在生理浓度的胱(硫)氨酸条件下具有选择性生长优势。

Expression of gamma-glutamyl transpeptidase provides tumor cells with a selective growth advantage at physiologic concentrations of cyst(e)ine.

作者信息

Hanigan M H

机构信息

Department of Cell Biology, University of Virginia Health Sciences Center, Charlottesville 22908.

出版信息

Carcinogenesis. 1995 Feb;16(2):181-5. doi: 10.1093/carcin/16.2.181.

DOI:10.1093/carcin/16.2.181
PMID:7859346
Abstract

Cells from the GGT-negative mouse hepatoma cell line, Hepa 1-6, were transfected with a human GGT cDNA and stably transformed clones were isolated. In standard tissue culture medium the GGT-positive cells and GGT-negative controls grew equally well. However, when the cysteine concentration of the medium was reduced to physiologic levels the GGT-positive cells had a growth advantage. Further investigation revealed that the medium of the GGT-negative Hepa 1-6 cells contained glutathione that had been excreted by the cells, but no glutathione was present in the medium of the GGT-positive cells. We have previously shown that expression of GGT enables cells to use extracellular glutathione as a source of cysteine (Hanigan and Ricketts, Biochem., 32:6302, 1993). These new data reveal that physiologic levels of cysteine can be limiting for cell growth and expression of GGT can provide the cells with a selective growth advantage. These data explain the observation that cells transfected with GGT grow at the same rate as the GGT-negative controls in tissue culture medium which contains a high level of cysteine, but the GGT-positive cells grow more rapidly than the GGT-negative cells when transplanted into animals (Warren et al., Proc. Soc. Exp. Biol. Med., 202:9, 1993). GGT-positive tumor cells have a selective growth advantage in vivo in comparison to GGT-negative tumor cells because they are able to use serum glutathione as a secondary source of cysteine thereby overcoming the growth restriction imposed by serum levels of cysteine.

摘要

用人类γ-谷氨酰转肽酶(GGT)cDNA转染GGT阴性的小鼠肝癌细胞系Hepa 1-6的细胞,并分离出稳定转化的克隆。在标准组织培养基中,GGT阳性细胞和GGT阴性对照生长得同样良好。然而,当培养基中的半胱氨酸浓度降至生理水平时,GGT阳性细胞具有生长优势。进一步研究发现,GGT阴性的Hepa 1-6细胞的培养基中含有细胞分泌的谷胱甘肽,但GGT阳性细胞的培养基中不存在谷胱甘肽。我们之前已经表明,GGT的表达使细胞能够利用细胞外谷胱甘肽作为半胱氨酸的来源(哈尼根和里基茨,《生物化学》,32:6302,1993)。这些新数据表明,生理水平的半胱氨酸可能会限制细胞生长,而GGT的表达可以为细胞提供选择性生长优势。这些数据解释了以下观察结果:在含有高水平半胱氨酸的组织培养基中,用GGT转染的细胞与GGT阴性对照以相同的速率生长,但当移植到动物体内时,GGT阳性细胞比GGT阴性细胞生长得更快(沃伦等人,《实验生物学与医学学会会刊》,202:9,1993)。与GGT阴性肿瘤细胞相比,GGT阳性肿瘤细胞在体内具有选择性生长优势,因为它们能够利用血清谷胱甘肽作为半胱氨酸的次要来源,从而克服血清半胱氨酸水平对生长的限制。

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Expression of gamma-glutamyl transpeptidase provides tumor cells with a selective growth advantage at physiologic concentrations of cyst(e)ine.γ-谷氨酰转肽酶的表达使肿瘤细胞在生理浓度的胱(硫)氨酸条件下具有选择性生长优势。
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