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组蛋白去乙酰化酶家族成员的转录分析揭示了分化和衰老精原干细胞之间的相似性。

Transcriptional analysis of histone deacetylase family members reveal similarities between differentiating and aging spermatogonial stem cells.

机构信息

Human Molecular Genetics Program, Children's Memorial Research Center, Chicago, IL 60614, USA.

出版信息

Stem Cell Rev Rep. 2013 Feb;9(1):59-64. doi: 10.1007/s12015-012-9392-5.

Abstract

The differentiation of adult stem cells involves extensive chromatin remodeling, mediated in part by the gene products of histone deacetylase (HDAC) family members. While the transcriptional downregulation of HDACs can impede stem cell self-renewal in certain contexts, it may also promote stem cell maintenance under other circumstances. In self-renewing, differentiating, and aging spermatogonial stem cells (SSCs), the gene expression dynamics of HDACs have not yet been characterized. To gain further insight with these studies, we analyzed the transcriptional profiles of six HDAC family members, previously identified to be the most highly expressed in self-renewing SSCs, during stem cell differentiation and aging. Here we discovered that in both differentiating and aging SSCs the expression of Sirt4 increases, while the expression of Hdac2, Hdac6, and Sirt1 decreases. When SSCs are exposed to the lifespan-enhancing drug rapamycin in vivo, the resultant HDAC gene expression patterns are opposite of those seen in the differentiating and aging SSCs, with increased Hdac2, Hdac6, and Sirt1 and decreased Hdac8, Hdac9, and Sirt4. Our findings suggest that HDACs important for stem cell maintenance and oxidative capacity are downregulated as adult stem cells differentiate or age. These results provide important insights into the epigenetic regulation of stem cell differentiation and aging in mammals.

摘要

成体干细胞的分化涉及广泛的染色质重塑,部分由组蛋白去乙酰化酶 (HDAC) 家族成员的基因产物介导。虽然 HDAC 的转录下调在某些情况下会阻碍干细胞的自我更新,但在其他情况下也可能促进干细胞的维持。在自我更新、分化和衰老的精原干细胞 (SSC) 中,HDAC 的基因表达动态尚未得到表征。为了更深入地了解这些研究,我们分析了六个 HDAC 家族成员的转录谱,这些成员之前被确定为自我更新的 SSC 中表达最高的。在这里,我们发现,在分化和衰老的 SSC 中,Sirt4 的表达增加,而 Hdac2、Hdac6 和 Sirt1 的表达减少。当 SSCs 在体内暴露于延长寿命的药物雷帕霉素时,HDAC 基因的表达模式与分化和衰老的 SSC 中所见的相反,Hdac2、Hdac6 和 Sirt1 增加,Hdac8、Hdac9 和 Sirt4 减少。我们的发现表明,在成体干细胞分化或衰老过程中,维持干细胞和氧化能力的重要 HDAC 被下调。这些结果为哺乳动物干细胞分化和衰老的表观遗传调控提供了重要的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8f10/3605728/63c7c88d55ee/nihms443946f1.jpg

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