Proteomics

Dataset Information

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RNF114 Co-IP experiments to identify binding partners


ABSTRACT: To identify the substrates of RNF114 in the context of PARylation-mediated DDR, we performed an IP-MS (immunoprecipitation coupled with MS) experiment, using cells treated with either H2O2 or H2O2+Talazoparib. We identified a large number of PARP1 peptides from the RNF114 immunoprecipitants only in H2O2-treated cells.

INSTRUMENT(S):

ORGANISM(S): Homo Sapiens (human)

TISSUE(S): Cell Culture

SUBMITTER: Chiho Kim  

LAB HEAD: Yonghao Yu

PROVIDER: PXD045231 | Pride | 2024-01-26

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
F08927.csv Csv
F08927.raw Raw
F08930.csv Csv
F08930.raw Raw
F08933.csv Csv
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Publications

Nimbolide targets RNF114 to induce the trapping of PARP1 and synthetic lethality in <i>BRCA</i>-mutated cancer.

Li Peng P   Zhen Yuanli Y   Kim Chiho C   Liu Zhengshuai Z   Hao Jianwei J   Deng Heping H   Deng Hejun H   Zhou Min M   Wang Xu-Dong XD   Qin Tian T   Yu Yonghao Y  

Science advances 20231025 43


Recent studies have pointed to PARP1 trapping as a key determinant of the anticancer effects of PARP1 inhibitors (PARPi). We identified RNF114, as a PARylation-dependent, E3 ubiquitin ligase involved in DNA damage response. Upon sensing genotoxicity, RNF114 was recruited, in a PAR-dependent manner, to DNA lesions, where it targeted PARP1 for degradation. The blockade of this pathway interfered with the removal of PARP1 from DNA lesions, leading to profound PARP1 trapping. We showed that a natura  ...[more]

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