Department of Homeostatic Regulation, Division of Cellular and Molecular Biology, Research Institute for Microbial Diseases, Osaka University, Suita, Osaka, 565-0871, Japan.
Institute for Molecular & Cellular Regulation, Gunma University, Gunma, 371-8512, Japan.
Nat Commun. 2022 Mar 18;13(1):1417. doi: 10.1038/s41467-022-29061-6.
Most tumours are thought to arise through oncogenic cell generation followed by additional mutations. How a new oncogenic cell primes tumorigenesis by acquiring additional mutations remains unclear. We show that an additional TP53 mutation stimulates primary tumorigenesis by switching oncogene-induced senescence from a tumour suppressor to a driver. Zebrafish imaging reveals that a newly emerged oncogenic cell with the Ras mutation becomes senescent and is eliminated from the epithelia, which is prevented by adding a TP53 gain-of-function mutation (TP53) into Ras cells. Surviving Ras-TP53 double-mutant cells senesce and secrete senescence-associated secretory phenotype (SASP)-related inflammatory molecules that convert neighbouring normal cells into SASP factor-secreting senescent cells, generating a heterogeneous tumour-like cell mass. We identify oncogenic cell behaviours that may control the initial human tumorigenesis step. Ras and TP53 mutations and cellular senescence are frequently detected in human tumours; similar switching may occur during the initial step of human tumorigenesis.
大多数肿瘤被认为是通过致癌细胞的产生,然后再加上额外的突变而形成的。新的致癌细胞如何通过获得额外的突变来引发肿瘤发生仍然不清楚。我们发现,额外的 TP53 突变通过将致癌基因诱导的衰老从肿瘤抑制因子转换为驱动因子,刺激原发性肿瘤发生。斑马鱼成像显示,具有 Ras 突变的新出现的致癌细胞会衰老并从上皮中消除,而通过向 Ras 细胞中添加 TP53 功能获得性突变 (TP53) 可以防止这种情况发生。存活的 Ras-TP53 双突变细胞衰老并分泌衰老相关分泌表型 (SASP) 相关的炎症分子,将邻近的正常细胞转化为分泌 SASP 因子的衰老细胞,从而产生异质性的肿瘤样细胞团。我们确定了可能控制人类肿瘤起始步骤的致癌细胞行为。Ras 和 TP53 突变以及细胞衰老经常在人类肿瘤中检测到;类似的转换可能发生在人类肿瘤起始的最初步骤中。
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