UVSSA 促进转录偶联修复 DNA 链间交联。

UVSSA facilitates transcription-coupled repair of DNA interstrand crosslinks.

机构信息

Institute for Cancer Genetics, Columbia University Vangelos College of Physicians and Surgeons, New York, NY, USA.

Institute for Cancer Genetics, Columbia University Vangelos College of Physicians and Surgeons, New York, NY, USA; Agilent Technologies, La Jolla, CA 92037, USA.

出版信息

DNA Repair (Amst). 2024 Nov;143:103771. doi: 10.1016/j.dnarep.2024.103771. Epub 2024 Oct 9.

DOI:10.1016/j.dnarep.2024.103771

PMID:39383571

Abstract

DNA interstrand crosslinks (ICLs) are covalent bonds between bases on opposing strands of the DNA helix which prevent DNA melting and subsequent DNA replication or RNA transcription. Here, we show that Ultraviolet Stimulated Scaffold Protein A (UVSSA) is critical for ICL repair in human cells, at least in part via the transcription coupled ICL repair (TC-ICR) pathway. Inactivation of UVSSA sensitizes human cells to ICL-inducing drugs, and delays ICL repair. UVSSA is required for replication-independent repair of a single ICL in a fluorescence-based reporter assay. UVSSA localizes to chromatin following ICL damage, and interacts with transcribing Pol II, CSA, CSB, and TFIIH. Specifically, UVSSA interaction with TFIIH is required for ICL repair and transcription inhibition blocks localization of transcription coupled repair factors to ICL damaged chromatin. Finally, UVSSA expression positively correlates with ICL-based chemotherapy resistance in human cancer cell lines. Our data strongly suggest that UVSSA is a novel ICL repair factor functioning in TC-ICR. These results provide further evidence that TC-ICR is a bona fide ICL repair mechanism that contributes to crosslinker drug resistance independently of replication-coupled ICL repair.

摘要

DNA 链间交联（ICLs）是 DNA 双螺旋中碱基之间的共价键，可防止 DNA 解链以及随后的 DNA 复制或 RNA 转录。在这里，我们表明紫外线刺激支架蛋白 A（UVSSA）在人类细胞中的 ICL 修复中至关重要，至少部分通过转录偶联 ICL 修复（TC-ICR）途径。UVSSA 的失活使人类细胞对 ICL 诱导药物敏感，并延迟 ICL 修复。在基于荧光的报告测定中，UVSSA 是复制非依赖性修复单个 ICL 所必需的。UVSSA 在 ICL 损伤后定位于染色质，并与转录 Pol II、CSA、CSB 和 TFIIH 相互作用。具体而言，UVSSA 与 TFIIH 的相互作用是 ICL 修复所必需的，并且转录抑制会阻止转录偶联修复因子定位到 ICL 受损的染色质。最后，UVSSA 的表达与人癌细胞系中基于 ICL 的化疗耐药性呈正相关。我们的数据强烈表明，UVSSA 是一种新型的 ICL 修复因子，在 TC-ICR 中起作用。这些结果进一步证明 TC-ICR 是一种真正的 ICL 修复机制，它独立于复制偶联的 ICL 修复而有助于交联剂药物耐药性。