遗传性共济失调SCAN1细胞在修复转录依赖性拓扑异构酶I切割复合物方面存在缺陷。

Hereditary ataxia SCAN1 cells are defective for the repair of transcription-dependent topoisomerase I cleavage complexes.

作者信息

Miao Ze-Hong, Agama Keli, Sordet Olivier, Povirk Lawrence, Kohn Kurt W, Pommier Yves

机构信息

Laboratory of Molecular Pharmacology, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

DNA Repair (Amst). 2006 Dec 9;5(12):1489-94. doi: 10.1016/j.dnarep.2006.07.004. Epub 2006 Aug 28.

DOI:10.1016/j.dnarep.2006.07.004

PMID:16935573

Abstract

Hereditary spinocerebellar ataxia with axonal neuropathy (SCAN1) is caused by an inactivating mutation (H493R) in the enzyme tyrosyl-DNA phosphodiesterase (Tdp1), which removes blocked 3'-termini at DNA strand breaks. Using SCAN1 cells treated with the specific topoisomerase I (Top1) inhibitor camptothecin, we find enhanced levels of Top1 cleavage complexes (Top1cc) and defective reversal of Top1cc in SCAN1 Tdp1-deficient cells, indicating a direct involvement of Tdp1 in the repair of Top1cc. Because the defective removal of Top1cc and the hypersensitivity of SCAN1 cells to camptothecin are not affected by aphidicolin, we propose that Tdp1 is involved in the repair of Top1cc associated with transcription damage in SCAN1 cells.

摘要

遗传性伴轴索性神经病的脊髓小脑共济失调（SCAN1）由酪氨酸-DNA磷酸二酯酶（Tdp1）的失活突变（H493R）引起，该酶可去除DNA链断裂处的受阻3'末端。使用经特异性拓扑异构酶I（Top1）抑制剂喜树碱处理的SCAN1细胞，我们发现SCAN1 Tdp1缺陷细胞中Top1切割复合物（Top1cc）水平升高且Top1cc的逆转存在缺陷，这表明Tdp1直接参与Top1cc的修复。由于Top1cc的缺陷性去除以及SCAN1细胞对喜树碱的超敏反应不受阿非科林的影响，我们提出Tdp1参与了SCAN1细胞中与转录损伤相关的Top1cc的修复。

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Hereditary ataxia SCAN1 cells are defective for the repair of transcription-dependent topoisomerase I cleavage complexes.遗传性共济失调SCAN1细胞在修复转录依赖性拓扑异构酶I切割复合物方面存在缺陷。

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遗传性共济失调SCAN1细胞在修复转录依赖性拓扑异构酶I切割复合物方面存在缺陷。

Hereditary ataxia SCAN1 cells are defective for the repair of transcription-dependent topoisomerase I cleavage complexes.

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