Kugel Sita, Feldman Jessica L, Klein Mark A, Silberman Dafne M, Sebastián Carlos, Mermel Craig, Dobersch Stephanie, Clark Abbe R, Getz Gad, Denu John M, Mostoslavsky Raul
The Massachusetts General Hospital Cancer Center, Harvard Medical School, Boston, MA 02114, USA.
The Department of Biomolecular Chemistry and the Wisconsin Institute for Discovery, University of Wisconsin, Madison, WI 53715, USA.
Cell Rep. 2015 Oct 20;13(3):479-488. doi: 10.1016/j.celrep.2015.09.022. Epub 2015 Oct 8.
Chromatin factors have emerged as the most frequently dysregulated family of proteins in cancer. We have previously identified the histone deacetylase SIRT6 as a key tumor suppressor, yet whether point mutations are selected for in cancer remains unclear. In this manuscript, we characterized naturally occurring patient-derived SIRT6 mutations. Strikingly, all the mutations significantly affected either stability or catalytic activity of SIRT6, indicating that these mutations were selected for in these tumors. Further, the mutant proteins failed to rescue sirt6 knockout (SIRT6 KO) cells, as measured by the levels of histone acetylation at glycolytic genes and their inability to rescue the tumorigenic potential of these cells. Notably, the main activity affected in the mutants was histone deacetylation rather than demyristoylation, pointing to the former as the main tumor-suppressive function for SIRT6. Our results identified cancer-associated point mutations in SIRT6, cementing its function as a tumor suppressor in human cancer.
染色质因子已成为癌症中最常发生失调的蛋白质家族。我们之前已将组蛋白脱乙酰酶SIRT6鉴定为一种关键的肿瘤抑制因子,但癌症中是否会选择点突变尚不清楚。在本论文中,我们对天然存在的患者来源的SIRT6突变进行了表征。令人惊讶的是,所有突变均显著影响了SIRT6的稳定性或催化活性,表明这些突变在这些肿瘤中被选择。此外,通过糖酵解基因处的组蛋白乙酰化水平以及它们无法挽救这些细胞的致瘤潜力来衡量,突变蛋白无法挽救sirt6基因敲除(SIRT6 KO)细胞。值得注意的是,突变体中受影响的主要活性是组蛋白去乙酰化而非肉豆蔻酰化,这表明前者是SIRT6的主要肿瘤抑制功能。我们的结果确定了SIRT6中与癌症相关的点突变,巩固了其在人类癌症中作为肿瘤抑制因子的功能。