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首页> 外文期刊>Carcinogenesis >Multidirectional tumor-suppressive activity of AIMP2/p38 and the enhanced susceptibility of AIMP2 heterozygous mice to carcinogenesis.
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Multidirectional tumor-suppressive activity of AIMP2/p38 and the enhanced susceptibility of AIMP2 heterozygous mice to carcinogenesis.

机译:AIMP2 / p38的多向肿瘤抑制活性和AIMP2杂合小鼠对癌变的敏感性增加。

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Aminoacyl-transfer ribonucleic acid (tRNA) synthetases-interacting multifunctional protein (AIMP) 2 is a factor associated with the macromolecular protein synthesis machinery consisting of nine different aminoacyl-tRNA synthetases and three non-enzymatic factors. However, it was shown to work as a multifaceted regulator through the versatile interactions with diverse signal mediators. For instance, it can mediate pro-apoptotic response to DNA damage and tumor necrosis factor-alpha (TNF-alpha) stimulus and growth-arresting signal by transforming growth factor (TGF)-beta. Considering that these pathways are critically implicated in the control of tumorigenesis, AIMP2 is expected to work as a potent tumor suppressor with broad coverage against different cancer types. Here we investigated whether AIMP2 would give gene dosage effect on its pro-apoptotic and anti-proliferative activities using the wild-type, hetero- and homozygous AIMP2 cells and whether AIMP2 would be critical in preventing tumorigenesis using different in vivo tumor models. Both the apoptotic responses to DNA damage and TNF-alpha and sensitivity to growth arresting TGF-beta signal were reduced in AIMP2 hetero- and homozygous cells compared with the wild-type cells in dose-dependent manner. In all the in vivo carcinogenesis experiments, reduction of AIMP2 level in heterozygous AIMP2 mice provided higher susceptibility to tumor formation. Thus, this work proves the functional significance of AIMP2 in determination of cell proliferation and death, and as a haploinsufficient tumor suppressor.
机译:氨基酰基转移核糖核酸(tRNA)合成酶多功能蛋白(AIMP)2是与大分子蛋白质合成机制相关的因子,该机制由9种不同的氨酰基tRNA合成酶和3种非酶因子组成。但是,通过与各种信号介体的多功能交互,它被证明可以用作多面调节器。例如,它可以通过转化生长因子(TGF)-β介导对DNA损伤和肿瘤坏死因子-α(TNF-α)刺激以及生长抑制信号的促凋亡反应。考虑到这些途径在肿瘤发生的控制中至关重要,AIMP2有望作为有效的抑癌剂,广泛针对不同类型的癌症。在这里,我们调查了AIMP2是否会使用野生型,杂合和纯合AIMP2细胞对其促凋亡和抗增殖活性赋予基因剂量效应,以及AIMP2对于使用不同的体内肿瘤模型预防肿瘤发生是否至关重要。与野生型细胞相比,AIMP2杂合和纯合细胞对DNA损伤和TNF-α的凋亡反应和对生长停滞的TGF-β信号的敏感性均以剂量依赖性方式降低。在所有体内致癌实验中,杂合AIMP2小鼠中AIMP2水平的降低为肿瘤形成提供了更高的敏感性。因此,这项工作证明了AIMP2在确定细胞增殖和死亡以及作为单倍型肿瘤抑制因子方面的功能意义。

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