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基因组倍增作为对组织存活的适应性:来自哺乳动物心脏和肝脏基因表达的证据。

Genome multiplication as adaptation to tissue survival: evidence from gene expression in mammalian heart and liver.

作者信息

Anatskaya Olga V, Vinogradov Alexander E

机构信息

Institute of Cytology, Russian Academy of Sciences, Tikhoretsky Avenue 4, St. Petersburg 194064, Russia.

出版信息

Genomics. 2007 Jan;89(1):70-80. doi: 10.1016/j.ygeno.2006.08.014. Epub 2006 Oct 6.

DOI:10.1016/j.ygeno.2006.08.014
PMID:17029690
Abstract

To elucidate the functional significance of genome multiplication in somatic tissues, we performed a large-scale analysis of ploidy-associated changes in expression of non-tissue-specific (i.e., broadly expressed) genes in the heart and liver of human and mouse (6585 homologous genes were analyzed). These species have inverse patterns of polyploidization in cardiomyocytes and hepatocytes. The between-species comparison of two pairs of homologous tissues with crisscross contrast in ploidy levels allows the removal of the effects of species and tissue specificity on the profile of gene activity. The different tests performed from the standpoint of modular biology revealed a consistent picture of ploidy-associated alteration in a wide range of functional gene groups. The major effects consisted of hypoxia-inducible factor-triggered changes in main cellular processes and signaling pathways, activation of defense against DNA lesions, acceleration of protein turnover and transcription, and the impairment of apoptosis, the immune response, and cytoskeleton maintenance. We also found a severe decline in aerobic respiration and stimulation of sugar and fatty acid metabolism. These metabolic rearrangements create a special type of metabolism that can be considered intermediate between aerobic and anaerobic. The metabolic and physiological changes revealed (reflected in the alteration of gene expression) help explain the unique ability of polyploid tissues to combine proliferation and differentiation, which are separated in diploid tissues. We argue that genome multiplication promotes cell survival and tissue regeneration under stressful conditions.

摘要

为阐明体细胞组织中基因组倍增的功能意义,我们对人和小鼠心脏及肝脏中与倍性相关的非组织特异性(即广泛表达)基因的表达变化进行了大规模分析(共分析了6585个同源基因)。这些物种在心肌细胞和肝细胞中的多倍体化模式相反。对两对同源组织进行倍性水平交叉对比的种间比较,能够消除物种和组织特异性对基因活性谱的影响。从模块化生物学角度进行的不同测试揭示了广泛功能基因组中与倍性相关的一致变化情况。主要影响包括缺氧诱导因子引发的主要细胞过程和信号通路变化、对DNA损伤防御的激活、蛋白质周转和转录的加速,以及细胞凋亡受损、免疫反应和细胞骨架维持受损。我们还发现有氧呼吸严重下降,糖和脂肪酸代谢受到刺激。这些代谢重排产生了一种特殊的代谢类型,可被视为介于有氧代谢和无氧代谢之间的中间类型。所揭示的代谢和生理变化(反映在基因表达改变中)有助于解释多倍体组织结合增殖和分化的独特能力,而在二倍体组织中这两种过程是分开的。我们认为基因组倍增在应激条件下促进细胞存活和组织再生。

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