Rass Knuth, Reichrath Jörg
Clinic for Dermatology, Venerology and Allergology, The Saarland University Hospital, 66421 Homburg/Saar, Germany.
Adv Exp Med Biol. 2008;624:162-78. doi: 10.1007/978-0-387-77574-6_13.
Exposition of the skin with solar ultraviolet radiation (UV) is the main cause of skin cancer development. The consistently increasing incidences of melanocytic and nonmelanocytic skin tumors are believed to be at least in part associated with recreational sun exposure. Epidemiological data indicate that excessive or cumulative sunlight exposition takes place years and decades before the resulting malignancies arise. The most important defense mechanisms that protect human skin against UV radiation involve melanin synthesis and active repair mechanisms. DNA is the major target of direct or indirect UV-induced cellular damage. Low pigmentation capacity in white Caucasians and rare congenital defects in DNA repair are mainly responsible for protection failures. The important function of nucleotide excision DNA repair (NER) to protect against skin cancer becomes obvious by the rare genetic disease xeroderma pigmentosum, in which diverse NER genes are mutated. In animal models, it has been demonstrated that UVB is more effective to induce skin cancer than UVA. UV-induced DNA photoproducts are able to cause specific mutations (UV-signature) in susceptible genes for squamous cell carcinoma (SCC) and basal cell carcinoma (BCC). In SCC development, UV-signature mutations in the p513 tumor suppressor gene are the most common event, as precancerous lesions reveal approximately 80% and SCCs > 90% UV-specific p53 mutations. Mutations in Hedgehog pathway related genes, especially PTCH1, are well known to represent the most significant pathogenic event in BCC. However, specific UV-induced mutations can be found only in approximately 50% of sporadic BCCs. Thus, cumulative UVB radiation can not be considered to be the single etiologic risk factor for BCC development. During the last decades, experimental animal models, including genetically engineered mice, the Xiphophorus hybrid fish, the south american oppossum and human skin xenografts, have further elucidated the important role of the DNA repair system in the multi-step process of UV-induced melanomagenesis. An increasing body of evidence now indicates that nucleotide excision repair is not the only DNA repair pathway that is involved in UV-induced tumorigenesis of melanoma and nonmelanoma skin cancer. An interesting new perspective in DNA damage and repair research lies in the participation of mammalian mismatch repair (MMR) in UV damage correction. As MMR enzyme hMSH2 displays a p53 target gene, is induced by UVB radiation and is involved in NER pathways, studies have now been initiated to elucidate the physiological and pathophysiological role of MMR in malignant melanoma and nonmelanoma skin cancer development.
皮肤暴露于太阳紫外线辐射(UV)是皮肤癌发生的主要原因。黑素细胞性和非黑素细胞性皮肤肿瘤的发病率持续上升,人们认为这至少部分与休闲时的阳光暴露有关。流行病学数据表明,在由此导致的恶性肿瘤出现之前的数年甚至数十年就发生了过度或累积的阳光暴露。保护人类皮肤免受紫外线辐射的最重要防御机制包括黑色素合成和主动修复机制。DNA是紫外线直接或间接诱导细胞损伤的主要靶点。白种人的色素沉着能力低以及DNA修复方面罕见的先天性缺陷是导致保护失败的主要原因。罕见的遗传性疾病着色性干皮病中多种核苷酸切除修复(NER)基因发生突变,这表明核苷酸切除DNA修复在预防皮肤癌方面的重要作用。在动物模型中,已证明UVB比UVA更易诱导皮肤癌。紫外线诱导的DNA光产物能够在鳞状细胞癌(SCC)和基底细胞癌(BCC)的易感基因中引起特定突变(紫外线特征)。在SCC发生过程中,p53肿瘤抑制基因中的紫外线特征突变是最常见的事件,因为癌前病变中约80%以及SCC中>90%存在紫外线特异性p53突变。众所周知,刺猬信号通路相关基因的突变,尤其是PTCH1的突变,是BCC中最重要的致病事件。然而,仅在约50%的散发性BCC中能发现特定的紫外线诱导突变。因此,累积的UVB辐射不能被视为BCC发生的唯一病因风险因素。在过去几十年中,包括基因工程小鼠、剑尾鱼杂交鱼、南美负鼠和人皮肤异种移植在内的实验动物模型,进一步阐明了DNA修复系统在紫外线诱导黑色素瘤发生的多步骤过程中的重要作用。现在越来越多的证据表明,核苷酸切除修复并不是参与紫外线诱导黑色素瘤和非黑色素瘤皮肤癌肿瘤发生的唯一DNA修复途径。DNA损伤与修复研究中一个有趣的新观点在于哺乳动物错配修复(MMR)参与紫外线损伤校正。由于MMR酶hMSH2是p53的靶基因,受UVB辐射诱导并参与NER途径,目前已开始研究以阐明MMR在恶性黑色素瘤和非黑色素瘤皮肤癌发生中的生理和病理生理作用。
