靶向 FANCJ-BRCA1 相互作用可促进从重组到依赖于聚合酶 eta 的旁路的转变。
Targeting the FANCJ-BRCA1 interaction promotes a switch from recombination to poleta-dependent bypass.
机构信息
Department of Cancer Biology, University of Massachusetts Medical School, Women's Cancers Program, UMASS Memorial Cancer Center, Worcester, MA 01605, USA.
出版信息
Oncogene. 2010 Apr 29;29(17):2499-508. doi: 10.1038/onc.2010.18. Epub 2010 Feb 22.
Abstract
BRCA1 and the DNA helicase FANCJ (also known as BACH1 or BRIP1) have common functions in breast cancer suppression and DNA repair. However, the functional significance of the direct interaction between BRCA1 and FANCJ remains unclear. Here, we have discovered that BRCA1 binding to FANCJ regulates DNA damage repair choice. Thus, when FANCJ binding to BRCA1 is ablated, the molecular mechanism chosen for the repair of damaged DNA is dramatically altered. Specifically, a FANCJ protein that cannot be phosphorylated at serine 990 or bind BRCA1 inhibits DNA repair via homologous recombination and promotes poleta-dependent bypass. Furthermore, the poleta-dependent bypass promoted by FANCJ requires the direct binding to the mismatch repair (MMR) protein, MLH1. Together, our findings implicate that in human cells BRCA1 binding to FANCJ is critical to regulate DNA repair choice and promote genomic stability. Moreover, unregulated FANCJ function could be associated with cancer and/or chemoresistance.
摘要
BRCA1 和 DNA 解旋酶 FANCJ(也称为 BACH1 或 BRIP1)在乳腺癌抑制和 DNA 修复方面具有共同的功能。然而,BRCA1 和 FANCJ 之间直接相互作用的功能意义尚不清楚。在这里,我们发现 BRCA1 与 FANCJ 的结合调节 DNA 损伤修复的选择。因此,当 FANCJ 与 BRCA1 的结合被消除时,用于修复受损 DNA 的分子机制会发生显著改变。具体而言,无法在丝氨酸 990 位点磷酸化或与 BRCA1 结合的 FANCJ 蛋白通过同源重组抑制 DNA 修复,并促进依赖于 poleta 的旁路修复。此外,FANCJ 促进的依赖于 poleta 的旁路修复需要与错配修复(MMR)蛋白 MLH1 的直接结合。总之,我们的研究结果表明,在人类细胞中,BRCA1 与 FANCJ 的结合对于调节 DNA 修复选择和促进基因组稳定性至关重要。此外,不受调节的 FANCJ 功能可能与癌症和/或化疗耐药性有关。
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