Thielmann H W, Popanda O, Edler L, Jung E G
Institute of Biochemistry, German Cancer Research Center, Heidelberg.
Cancer Res. 1991 Jul 1;51(13):3456-70.
Sixty-one xeroderma pigmentosum (XP) patients living in the Federal Republic of Germany were investigated. Clinical symptoms were correlated with DNA repair parameters measured in fibroblasts grown from skin biopsies. Classification according to the international complementation groups revealed that of the 61 patients 3 belonged to group A, 26 to group C, 16 to group D, 3 to group E, and 2 to group F; 11 were of the XP variant type. A striking clinical aspect was the frequency of histogenetically different skin tumors varying from one XP complementation group to the other: squamous and basal cell carcinomas predominated in XP group C; lentigo maligna melanomas were most frequent in group D; basal cell carcinomas occurred preferentially in group E and XP variants. Three DNA repair parameters were determined for 46 fibroblast strains: colony-forming ability (D0); DNA repair synthesis (G0); and DNA-incising capacity (E0). Dose-response experiments with up to 13 dose levels were performed throughout to achieve sufficient experimental accuracy. DNA-damaging treatments included UV light, the "UV-like" carcinogen N-acetoxy-2-acetylaminofluorene, and the alkylating carcinogens methyl methanesulfonate and N-methyl-N-nitrosourea. Comparison of clinical signs and repair data was made on the basis of D0, G0, and E0 values of both individual cell strains and weighted means of XP complementation groups. Despite considerable clinical and biochemical heterogeneity within complementation groups distinctive features emerged. In general, D0, G0, and E0 values of all XP strains investigated, including XP variants, were found to be reduced upon treatment with UV light or N-acetoxy-2-acetylaminofluorene. After treatment with UV light or N-acetoxy-2-acetylaminofluorene, cell strains in which DNA-incising capacity was reduced also showed a similar reduction in both colony-forming ability and DNA repair synthesis. Consequently, the weighted mean D0, G0, and E0 values of XP complementation groups and XP variants correlated with each other. Furthermore, the onset of both early dermatological symptoms of XP and tumor growth correlated with the extent of DNA repair defects. Of 45 XP fibroblast strains checked for colony-forming ability after treatment with methyl methanesulfonate only 3 cell strains from group D were found to be more sensitive than normal controls, suggesting that overall repair in XP strains was equal to that in controls. Weighted means of DNA repair synthesis of XP complementation groups, however, showed reductions hinting at impaired excision of distinct alkylated bases.(ABSTRACT TRUNCATED AT 400 WORDS)
对居住在德意志联邦共和国的61例着色性干皮病(XP)患者进行了调查。临床症状与从皮肤活检组织培养的成纤维细胞中测量的DNA修复参数相关。根据国际互补组分类显示,61例患者中,3例属于A组,26例属于C组,16例属于D组,3例属于E组,2例属于F组;11例为XP变异型。一个显著的临床现象是,不同XP互补组中组织发生学上不同的皮肤肿瘤发生率各异:C组XP患者中鳞状细胞癌和基底细胞癌占主导;D组中恶性雀斑样痣黑色素瘤最为常见;E组和XP变异型中基底细胞癌优先发生。对46个成纤维细胞株测定了三个DNA修复参数:集落形成能力(D0);DNA修复合成(G0);以及DNA切割能力(E0)。全程进行了多达13个剂量水平的剂量反应实验,以获得足够的实验准确性。DNA损伤处理包括紫外线、“类紫外线”致癌物N-乙酰氧基-2-乙酰氨基芴,以及烷化致癌物甲磺酸甲酯和N-甲基-N-亚硝基脲。根据各个细胞株的D0、G0和E0值以及XP互补组的加权平均值,对临床症状和修复数据进行了比较。尽管互补组内存在相当大的临床和生化异质性,但仍出现了显著特征。总体而言,发现所有研究的XP株,包括XP变异型,在用紫外线或N-乙酰氧基-2-乙酰氨基芴处理后,D0、G0和E0值均降低。在用紫外线或N-乙酰氧基-2-乙酰氨基芴处理后,DNA切割能力降低的细胞株在集落形成能力和DNA修复合成方面也出现类似降低。因此,XP互补组和XP变异型的加权平均D0、G0和E0值相互关联。此外,XP的早期皮肤症状和肿瘤生长的发生均与DNA修复缺陷的程度相关。在用甲磺酸甲酯处理后检查集落形成能力的45个XP成纤维细胞株中,仅发现D组的3个细胞株比正常对照更敏感,这表明XP株的总体修复与对照相当。然而,XP互补组的DNA修复合成加权平均值显示降低,提示特定烷基化碱基的切除受损。(摘要截短于400字)
