Human Transcriptional Coactivator PC4 Stimulates DNA End Joining and Activates DSB Repair Activity |
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| Authors: | Kiran Batta Kunio Takeyasu |
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| Affiliation: | 1 Transcription and Disease Laboratory, Molecular Biology and Genetics Unit, Jawaharlal Nehru Center for Advanced Scientific Research, Jakkur, PO Bangalore 560064, India
2 Laboratory of Plasma Membrane and Nuclear Signaling, Graduate School of Biostudies, Kyoto University, Sakyo-ku, Kyoto, Japan |
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| Abstract: | Human transcriptional coactivator PC4 is a highly abundant nuclear protein that is involved in diverse cellular processes ranging from transcription to chromatin organization. Earlier, we have shown that PC4, a positive activator of p53, overexpresses upon genotoxic insult in a p53-dependent manner. In the present study, we show that PC4 stimulates ligase-mediated DNA end joining irrespective of the source of DNA ligase. Pull-down assays reveal that PC4 helps in the association of DNA ends through its C-terminal domain. In vitro nonhomologous end-joining assays with cell-free extracts show that PC4 enhances the joining of noncomplementary DNA ends. Interestingly, we found that PC4 activates double-strand break (DSB) repair activity through stimulation of DSB rejoining in vivo. Together, these findings demonstrate PC4 as an activator of nonhomologous end joining and DSB repair activity. |
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| Keywords: | DSB, double-strand break NHEJ, nonhomologous end joining BSA, bovine serum albumin AFM, atomic force microscopy CTD, C-terminal domain ssDNA, single-stranded DNA dsDNA, double-stranded DNA dNTP, deoxyribonucleotide triphosphate HMGB1, high-mobility group box 1 EDTA, ethylenediaminetetraacetic acid |
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