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正常或癌变的乳腺组织细胞在缺乏精氨酸时表现出不同的生长特性。

Cells derived from normal or cancer breast tissue exhibit different growth properties when deprived of arginine.

机构信息

Dipartimento di Biologia e Patologia Cellulare e Molecolare L. Califano, University of Naples Federico II, 80131, Naples, Italy.

出版信息

Med Oncol. 2012 Dec;29(4):2543-51. doi: 10.1007/s12032-011-0130-7. Epub 2011 Dec 20.

Abstract

Arginine deprivation impairs cell proliferation more strong in cancer than in normal cells; thus, it has been proposed that such an effect could be exploited for cancer therapy. We have compared the effect of arginine deprivation on normal and cancer cells, studying growth rate, morphology, and protein expression patterns in immortalized human MCF10a cells and in MCF7 cells. Arginine deprivation forces MCF10a cells into irreversible senescence while the vast majority of MCF7 cells become quiescent and resume normal growth following arginine re-addition. Arginine deprivation induced a significant burst of p21cip1 in both cell lines that were reversible in MCF7 and irreversible in MCF10 cells. In the latter cells, p21cip1 increase was accompanied by a time-dependent increase of p16INK4A. Similar effects could be obtained by treating both cell types with α-difluoro-methyl-ornithine, but not with Nω-hydroxy-L-arginine, drugs that interfere specifically but differently with the major pathways of arginine metabolism. Our data suggest that derangement in polyamine synthesis is the main consequence of arginine starvation.

摘要

精氨酸缺乏在癌症细胞中比正常细胞更强烈地抑制细胞增殖;因此,有人提出这种效应可以被用来进行癌症治疗。我们比较了精氨酸缺乏对正常细胞和癌细胞的影响,研究了永生人 MCF10a 细胞和 MCF7 细胞的生长速度、形态和蛋白质表达模式。精氨酸剥夺使 MCF10a 细胞不可逆地衰老,而绝大多数 MCF7 细胞在精氨酸再添加后进入静止状态并恢复正常生长。精氨酸剥夺在两种细胞系中都诱导了 p21cip1 的显著爆发,在 MCF7 中是可逆的,而在 MCF10 细胞中是不可逆的。在后一种细胞中,p21cip1 的增加伴随着 p16INK4A 的时间依赖性增加。用 α-二氟甲基-鸟氨酸处理两种细胞类型也可以获得类似的效果,但用 Nω-羟基-L-精氨酸处理则不行,这两种药物特异性地但以不同的方式干扰精氨酸代谢的主要途径。我们的数据表明,多胺合成的紊乱是精氨酸饥饿的主要后果。

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