Department of Toxicogenetics, Leiden University Medical Center, 2300 RC Leiden, The Netherlands.
Proc Natl Acad Sci U S A. 2009 Dec 22;106(51):21836-41. doi: 10.1073/pnas.0909507106. Epub 2009 Dec 10.
The induction of skin cancer involves both mutagenic and proliferative responses of the epidermis to ultraviolet (UV) light. It is believed that tumor initiation requires the mutagenic replication of damaged DNA by translesion synthesis (TLS) pathways. The mechanistic basis for the induction of proliferation, providing tumor promotion, is poorly understood. Here, we have investigated the role of TLS in the initiation and promotion of skin carcinogenesis, using a sensitive nucleotide excision repair-deficient mouse model that carries a hypomorphic allele of the error-prone TLS gene Rev1. Despite a defect in UV-induced mutagenesis, skin carcinogenesis was accelerated in these mice. This paradoxical phenotype was caused by the induction of inflammatory hyperplasia of the mutant skin that provides strong tumor promotion. The induction of hyperplasia was associated with mild and transient replicational stress of the UV-damaged genome, triggering DNA damage signaling and senescence. The concomitant expression of Interleukin-6 (IL-6) is in agreement with an executive role for IL-6 and possibly other cytokines in the autocrine induction of senescence and the paracrine induction of inflammatory hyperplasia. In conclusion, error-prone TLS suppresses tumor-promoting activities of UV light, thereby controlling skin carcinogenesis.
皮肤癌的诱导涉及表皮对紫外线 (UV) 光的诱变和增殖反应。人们认为肿瘤的起始需要通过跨损伤合成 (TLS) 途径对受损 DNA 进行诱变复制。增殖诱导的机制基础,为肿瘤促进提供了基础,目前了解甚少。在这里,我们使用一种敏感的核苷酸切除修复缺陷型小鼠模型,该模型携带易错 TLS 基因 Rev1 的低功能等位基因,研究了 TLS 在皮肤癌发生的起始和促进中的作用。尽管存在 UV 诱导的诱变缺陷,但这些小鼠的皮肤癌发生速度加快。这种矛盾的表型是由突变皮肤的炎症性增生引起的,这种增生为肿瘤的促进提供了强大的作用。增生的诱导与 UV 损伤基因组的轻微和短暂的复制应激有关,触发了 DNA 损伤信号和衰老。白细胞介素 6 (IL-6) 的同时表达与 IL-6 及其它细胞因子在衰老的自分泌诱导和炎症性增生的旁分泌诱导中的执行作用一致。总之,易错 TLS 抑制了 UV 光的促肿瘤活性,从而控制了皮肤癌的发生。