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DNA 聚合酶 β 在关键的线粒体碱基切除修复活动中优于 DNA 聚合酶 γ。

DNA polymerase β outperforms DNA polymerase γ in key mitochondrial base excision repair activities.

机构信息

Laboratory of Molecular Gerontology, National Institute on Aging, 251 Bayview Blvd., Baltimore, MD, 21224, USA.

Laboratory of Molecular Gerontology, National Institute on Aging, 251 Bayview Blvd., Baltimore, MD, 21224, USA.

出版信息

DNA Repair (Amst). 2021 Mar;99:103050. doi: 10.1016/j.dnarep.2021.103050. Epub 2021 Jan 21.

Abstract

DNA polymerase beta (POLβ), well known for its role in nuclear DNA base excision repair (BER), has been shown to be present in the mitochondria of several different cell types. Here we present a side-by-side comparison of BER activities of POLβ and POLγ, the mitochondrial replicative polymerase, previously thought to be the only mitochondrial polymerase. We find that POLβ is significantly more proficient at single-nucleotide gap filling, both in substrates with ends that require polymerase processing, and those that do not. We also show that POLβ has a helicase-independent functional interaction with the mitochondrial helicase, TWINKLE. This interaction stimulates strand-displacement synthesis, but not single-nucleotide gap filling. Importantly, we find that purified mitochondrial extracts from cells lacking POLβ are severely deficient in processing BER intermediates, suggesting that mitochondrially localized DNA POLβ may be critical for cells with high energetic demands that produce greater levels of oxidative stress and therefore depend upon efficient BER for mitochondrial health.

摘要

DNA 聚合酶 β(POLβ)以其在核 DNA 碱基切除修复(BER)中的作用而闻名,现已证实其存在于多种不同细胞类型的线粒体中。在这里,我们将 POLβ和 POLγ(线粒体复制聚合酶)的 BER 活性进行了并排比较,POLγ之前被认为是唯一的线粒体聚合酶。我们发现 POLβ在单核苷酸缺口填充方面明显更有效率,无论是在需要聚合酶处理的末端的底物中,还是在不需要的底物中。我们还表明,POLβ与线粒体解旋酶 TWINKLE 具有独立于解旋酶的功能相互作用。这种相互作用刺激链置换合成,但不刺激单核苷酸缺口填充。重要的是,我们发现缺乏 POLβ的细胞的纯化线粒体提取物在 BER 中间产物的加工中严重缺乏,这表明定位于线粒体的 DNA POLβ对于具有高能量需求的细胞可能是至关重要的,这些细胞会产生更高水平的氧化应激,因此需要有效的 BER 来维持线粒体健康。

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