首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >PNAS Plus: FASN regulates cellular response to genotoxic treatments by increasing PARP-1 expression and DNA repair activity via NF-κB and SP1
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PNAS Plus: FASN regulates cellular response to genotoxic treatments by increasing PARP-1 expression and DNA repair activity via NF-κB and SP1

机译:PNAS Plus:FASN通过增加PARP-1表达和通过NF-κB和SP1的DNA修复活性来调节细胞对遗传毒性治疗的反应

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摘要

Fatty acid synthase (FASN), the sole cytosolic mammalian enzyme for de novo lipid synthesis, is crucial for cancer cell survival and associates with poor prognosis. FASN overexpression has been found to cause resistance to genotoxic insults. Here we tested the hypothesis that FASN regulates DNA repair to facilitate survival against genotoxic insults and found that FASN suppresses NF-κB but increases specificity protein 1 (SP1) expression. NF-κB and SP1 bind to a composite element in the poly(ADP-ribose) polymerase 1 (PARP-1) promoter in a mutually exclusive manner and regulate PARP-1 expression. Up-regulation of PARP-1 by FASN in turn increases Ku protein recruitment and DNA repair. Furthermore, lipid deprivation suppresses SP1 expression, which is able to be rescued by palmitate supplementation. However, lipid deprivation or palmitate supplementation has no effect on NF-κB expression. Thus, FASN may regulate NF-κB and SP1 expression using different mechanisms. Altogether, we conclude that FASN regulates cellular response against genotoxic insults by up-regulating PARP-1 and DNA repair via NF-κB and SP1.
机译:脂肪酸合酶(FASN)是用于从头合成脂质的唯一胞质哺乳动物酶,对癌细胞存活至关重要,并与不良预后相关。已经发现FASN过表达引起对遗传毒性侮辱的抗性。在这里,我们测试了FASN调节DNA修复以促进针对遗传毒性损伤的生存的假设,并发现FASN抑制NF-κB但增加了特异性蛋白1(SP1)的表达。 NF-κB和SP1以相互排斥的方式与聚(ADP-核糖)聚合酶1(PARP-1)启动子中的复合元件结合,并调节PARP-1的表达。 FASN对PARP-1的上调反过来会增加Ku蛋白募集和DNA修复。此外,脂质剥夺抑制了SP1的表达,可以通过补充棕榈酸酯来挽救SP1的表达。然而,脂质剥夺或棕榈酸酯补充对NF-κB表达没有影响。因此,FASN可能使用不同的机制调节NF-κB和SP1的表达。总之,我们得出结论,FASN通过上调PARP-1和通过NF-κB和SP1的DNA修复来调节针对遗传毒性损伤的细胞反应。

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