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Alternative Splicing Increases Sirtuin Gene Family Diversity and Modulates Their Subcellular Localization and Function

机译:替代剪接增加了Sirtuin基因家族的多样性并调节其亚细胞定位和功能

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摘要

Alternative splicing generates multiple distinct isoforms that increase transcriptome and proteome diversity. There are seven sirtuin genes in humans, each consists of multiple exons that are likely to undergo alternative splicing. Our aim was to characterize the effect of alternative splicing on the sirtuin genes. Here, we report the identification of 23 human sirtuin isoforms, most of which were not previously reported. Five of the sirtuin genes had more than one isoform, whereas sirtuin-6 had nine isoforms. Exon skipping was the main event. Most of the sirtuin isoforms were deficient in parts of the protein domains, including the catalytic domain, the N- or C-terminus, nuclear localization signal or mitochondrial targeting signal. The domain loss caused potential structural changes. Three SIRT1 isoforms had a differential effect on the mitochondrial oxygen consumption rate. Age-related changes in the expression of SIRT1 isoforms were observed in the human heart in fetus, adults, and very old individuals. We also identified 15 sirtuin isoforms in mice. Our data indicate that alternative splicing increases sirtuin gene diversity and may modulate subcellular localization and function, thereby adding complexity to the gene regulation of mitochondrial respiration, metabolism, and cardiac function during maturation and aging.
机译:替代剪接产生多种不同的同种型,其增加转录组和蛋白质组多样性。人类中有七个Sirtuin基因,每个Sirtuin基因由多种外显子组成,可能发生替代剪接。我们的目标是表征替代剪接对Sirtuin基因的影响。在这里,我们报告鉴定23例人类Sirtuin同种型,其中大多数未报告。六胞苷基因中有五种同种型,而Sirtuin-6有九种同种型。外显子跳过是主要的活动。大多数Sirtuin同种型缺乏蛋白质结构域的部分,包括催化结构域,N-或C-末端,核定位信号或线粒体靶向信号。域损失导致潜在的结构变化。三种SIRT1同种型对线粒体氧消耗率具有差异影响。在胎儿,成人和非常老年人的人体中观察到SIRT1同种型表达的年龄相关变化。我们还确定了小鼠中的15个Sirtuin同种型。我们的数据表明,替代剪接增加了Sirtuin基因的多样性,并且可以调节亚细胞定位和功能,从而增加了在成熟和老化期间对线粒体呼吸,代谢和心脏功能的基因调节的复杂性。

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