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Methylation of histone H3 lysine 9 occurs during translation

机译:组蛋白H3赖氨酸9的甲基化在翻译过程中发生

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Histone post-translational modifications are key contributors to chromatin structure and function, and participate in the maintenance of genome stability. Understanding the establishment and maintenance of these marks, along with their misregulation in pathologies is thus a major focus in the field. While we have learned a great deal about the enzymes regulating histone modifications on nucleosomal histones, much less is known about the mechanisms establishing modifications on soluble newly synthesized histones. This includes methylation of lysine 9 on histone H3 (H3K9), a mark that primes the formation of heterochromatin, a critical chromatin landmark for genome stability. Here, we report that H3K9 mono- and dimethylation is imposed during translation by the methyltransferase SetDB1. We discuss the importance of these results in the context of heterochromatin establishment and maintenance and new therapeutic opportunities in pathologies where heterochromatin is perturbed.
机译:组蛋白翻译后修饰是染色质结构和功能的关键因素,并参与基因组稳定性的维持。因此,了解这些标记的建立和维护以及它们在病理学中的失调是该领域的主要重点。尽管我们已经了解了许多有关调节核小体组蛋白上的组蛋白修饰的酶,但对在可溶性新合成组蛋白上建立修饰的机理的了解还很少。这包括组蛋白H3(H3K9)上赖氨酸9的甲基化,这是引发异染色质形成的标记,异染色质是基因组稳定性的关键染色质标志。在这里,我们报告H3K9单和二甲基化是由甲基转移酶SetDB1在翻译过程中强加的。我们讨论了异染色质建立和维持以及在异染色质受到干扰的病理学中新的治疗机会的背景下这些结果的重要性。

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