Small-molecules that bind to the ubiquitin-binding motif of REV1 inhibit REV1 interaction with K164-monoubiquitinated PCNA and suppress DNA damage tolerance

Vanarotti Murugendra; Evison Benjamin J.; Actis Marcelo L.; Inoue Akira; McDonald Ezelle T.; Shao Youming; Heath Richard J.; Fujii Naoaki

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Small-molecules that bind to the ubiquitin-binding motif of REV1 inhibit REV1 interaction with K164-monoubiquitinated PCNA and suppress DNA damage tolerance

机译：与Rev1的泛素结合基序结合的小分子抑制Rev1与K164-单突相关PCNA相互作用，抑制DNA损伤耐受性

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REV1 protein is a mutagenic DNA damage tolerance (DDT) mediator and encodes two ubiquitin-binding motifs (i.e., UBM1 and UBM2) that are essential for the DDT function. REV1 interacts with K164-monoubiquitinated PCNA (UbPCNA) in cells upon DNA-damaging stress. By using AlphaScreen assays to detect inhibition of REV1 and UbPCNA protein interactions along with an NMR-based strategy, we identified small-molecule compounds that inhibit the REV1/UbPCNA interaction and that directly bind to REV1 UBM2. In cells, one of the compound prevented recruitment of REV1 to PCNA foci on chromatin upon cisplatin treatment, delayed removal of UV-induced cyclopyrimidine dimers from nuclei, prevented UV-induced mutation of HPRT gene, and diminished clonogenic survival of cells that were challenged by cyclophosphamide or cisplatin. This study demonstrates the potential utility of a small-molecule REV1 UBM2 inhibitor for preventing DDT. (C) 2018 Elsevier Ltd. All rights reserved.

机译：Rev1蛋白是一种诱变DNA损伤耐受性（DDT）介质，并编码两个对DDT功能必不可少的两个泛素结合基序（即，UBM1和UBM2）。 Rev1在DNA损伤应力时与K164-MONOUBIMINDEND pCNA（UBPCNA）相互作用。通过使用基于NMR的策略来检测Rev1和Ubpcna蛋白相互作用的α和Ubpcna蛋白相互作用的抑制，我们确定了抑制Rev1 / Ubpcna相互作用的小分子化合物，并且直接结合Rev1 UBM2。在细胞中，在顺铂处理时，其中一种化合物在染色质上募集了Rev1至PCNA焦点的PCNA焦点，延迟除去核诱导的核，预防紫外线诱导的HPRT基因突变，并致置于攻击的细胞的克隆因存活率降低环磷酰胺或顺铂。本研究证明了小分子Rev1 UBM2抑制剂防止DDT的潜在效用。（c）2018年elestvier有限公司保留所有权利。

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《Bioorganic and medicinal chemistry》 |2018年第9期|共9页
作者
Vanarotti Murugendra; Evison Benjamin J.; Actis Marcelo L.; Inoue Akira; McDonald Ezelle T.; Shao Youming; Heath Richard J.; Fujii Naoaki;
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作者单位

St Jude Childrens Res Hosp Dept Chem Biol &

Therapeut 332 N Lauderdale St Memphis TN 38105 USA;

St Jude Childrens Res Hosp Dept Chem Biol &

Therapeut 332 N Lauderdale St Memphis TN 38105 USA;

St Jude Childrens Res Hosp Dept Chem Biol &

Therapeut 332 N Lauderdale St Memphis TN 38105 USA;

St Jude Childrens Res Hosp Dept Chem Biol &

Therapeut 332 N Lauderdale St Memphis TN 38105 USA;

St Jude Childrens Res Hosp Prot Prod Facil 332 N Lauderdale St Memphis TN 38105 USA;

St Jude Childrens Res Hosp Prot Prod Facil 332 N Lauderdale St Memphis TN 38105 USA;

St Jude Childrens Res Hosp Dept Chem Biol &

Therapeut 332 N Lauderdale St Memphis TN 38105 USA;

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原文格式 PDF
正文语种 eng
中图分类药学;
关键词
REV1; Ubiquitin-binding motif; PCNA; Small-molecule; Protein-protein interaction;

机译：Rev1;泛素结合基序;PCNA;小分子;蛋白质 - 蛋白质相互作用;

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专利

1. Small-molecules that bind to the ubiquitin-binding motif of REV1 inhibit REV1 interaction with K164-monoubiquitinated PCNA and suppress DNA damage tolerance [J] . Vanarotti Murugendra, Evison Benjamin J., Actis Marcelo L., Bioorganic and medicinal chemistry . 2018,第9期

机译：与Rev1的泛素结合基序结合的小分子抑制Rev1与K164-单突相关PCNA相互作用，抑制DNA损伤耐受性
2. Structures of REV1 UBM2 Domain Complex with Ubiquitin and with a Small-Molecule that Inhibits the REV1 UBM2–Ubiquitin Interaction [J] . Murugendra Vanarotti, Christy R. Grace, Darcie J. Miller, Journal of Molecular Biology . 2018,第17期

机译：Rev1 UBM2结构域复合物与泛素和抑制Rev1 UBM2-泛素相互作用的小分子
3. DNA-damage tolerance mediated by PCNA center dot Ub fusions in human cells is dependent on Rev1 but not Pol eta [J] . Qin Zhoushuai, Lu Mengxue, Xu Xin, Nucleic Acids Research . 2013,第15期

机译：人细胞中PCNA中心点Ub融合介导的DNA损伤耐受性取决于Rev1，而不取决于Pol eta
4. Towards an understanding of protein-protein interaction network hierarchies. Analysis of DnaN (β)-binding peptide motifs in members of protein families interacting with the eubacterial processivity clamp, the β subunit of DNA Polymerase III [C] . Brian P. Dalrymple, Gene Wijffels, Kritaya Kongsuwan, Asia-Pacific Bioinformatics Conference(APBC 2003); 200302; Adelaide(AU) . 2003

机译：对蛋白质-蛋白质相互作用网络层次结构的理解。蛋白质家族成员与DNA聚合酶III的优生过程性钳位相互作用的DnaN（β）结合肽基序分析
5. The cellular roles of the translesion polymerases Eta, REV1 and Zeta in bypass and repair of DNA damage induced by anti-cancer agents. [D] . Hicks, James Kevin. 2010

机译：跨病变的聚合酶Eta，REV1和Zeta在旁路和修复抗癌药诱导的DNA损伤中的细胞作用。
6. Small-molecules that bind to the ubiquitin-binding motif of REV1 inhibit REV1 interaction with K164-monoubiquitinated PCNA and suppress DNA damage tolerance [O] . Murugendra Vanarotti, Benjamin J. Evison, Marcelo L. Actis, -1

机译：结合REV1泛素结合基序的小分子抑制REV1与K164单泛素化PCNA的相互作用并抑制DNA损伤耐受性
7. Small-molecules that bind to the ubiquitin-binding motif of REV1 inhibit REV1 interaction with K164-monoubiquitinated PCNA and suppress DNA damage tolerance [O] . Murugendra Vanarotti, Benjamin J. Evison, Marcelo L. Actis, 2018

机译：与Rev1的泛素结合基序结合的小分子抑制Rev1与K164-单突相关PCNA相互作用并抑制DNA损伤耐受性

Small-molecules that bind to the ubiquitin-binding motif of REV1 inhibit REV1 interaction with K164-monoubiquitinated PCNA and suppress DNA damage tolerance

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