Mass M J, Jeffers A J, Ross J A, Nelson G, Galati A J, Stoner G D, Nesnow S
Carcinogenesis and Metabolism Branch, U.S. Environmental Protection Agency, Research Triangle Park, NC 27711.
Mol Carcinog. 1993;8(3):186-92. doi: 10.1002/mc.2940080309.
Strain A/J mice received intraperitoneal injections of benz[j]aceanthrylene (B[j]A) or benzo[a]pyrene (B[a]P). At 24, 48, and 72 h, lung tissues were removed for analysis of B[a]P- or B[j]A-derived DNA adduct formation during the first 3 d of exposure. One group of mice exposed to these hydrocarbons was kept for 8 mo to determine lung tumor multiplicity, the occurrence of mutations in codons 12 and 61 of the Ki-ras gene in the tumors that arose, the relationship between Ki-ras oncogene mutations in tumors, and the presence and quantity of genomic DNA adducts. The major DNA adduct in the lungs of mice exposed to B[a]P was N2-(10 beta-[+B, 7 alpha, 9 alpha-trihydroxy-7,8,9,10-tetrahydrobenzo[a]pyrene]yl)-deoxyguanosine (BPDE-I-dGuo) arising from bay-region diolepoxide activation of B[a]P and was consistent with the occurrence of tumors with mutations GGT-->TGT (56%), GGT-->GTT (25%), and GGT-->GAT (19%) in codon 12, all involving mutations of a guanine. B[j]A, a demethylated analogue of 3-methylcholanthrene (3-MCA) with an unsaturated cyclopenta ring, produced 16-to 60-fold more tumors at equivalent doses than did B[a]P; the mutations in tumors were GGT-->TGT (4%), GGT-->GTT (30%), and GGT-->CGT (65%). Analysis of adduction patterns in DNA suggested that B[j]A was activated to form DNA-binding derivatives in A/J mouse lungs primarily at the cyclopenta ring even though B[j]A contains a bay region. As reported in the published literature, the mutation spectrum induced by 3-MCA in Ki-ras codon 12 of mouse cells is similar to that of B[a]P but not to that of its close relative B[j]A. In contrast to B[j]A, 3-MCA is activated mostly via a bay-region diol-epoxide since its cyclopenta ring is saturated and not easily epoxidates. Therefore, we propose that the GGT-->CGT mutations produced by B[j]A in Ki-ras codon 12 were mostly the result of cyclopenta-ring-derived adducts.
A/J品系小鼠接受腹腔注射苯并[j]屈(B[j]A)或苯并[a]芘(B[a]P)。在24、48和72小时时,取出肺组织以分析暴露前3天内B[a]P或B[j]A衍生的DNA加合物形成情况。将一组暴露于这些碳氢化合物的小鼠饲养8个月,以确定肺肿瘤的多发性、所产生肿瘤中Ki-ras基因第12和61密码子的突变情况、肿瘤中Ki-ras癌基因突变之间的关系以及基因组DNA加合物的存在和数量。暴露于B[a]P的小鼠肺中的主要DNA加合物是N2-(10β-[+B, 7α, 9α-三羟基-7,8,9,10-四氢苯并[a]芘]基)-脱氧鸟苷(BPDE-I-dGuo),它由B[a]P的湾区二环氧物活化产生,并且与第12密码子中发生GGT→TGT(56%)、GGT→GTT(25%)和GGT→GAT(19%)突变的肿瘤情况一致,所有这些突变都涉及鸟嘌呤的突变。B[j]A是3-甲基胆蒽(3-MCA)的去甲基类似物,带有一个不饱和环戊环,在等效剂量下产生的肿瘤比B[a]P多16至60倍;肿瘤中的突变是GGT→TGT(4%)、GGT→GTT(30%)和GGT→CGT(65%)。对DNA加合模式的分析表明,尽管B[j]A含有一个湾区,但它在A/J小鼠肺中主要在环戊环处被活化以形成DNA结合衍生物。正如已发表文献中所报道的,3-MCA在小鼠细胞Ki-ras第12密码子中诱导的突变谱与B[a]P相似,但与其近亲B[j]A不同。与B[j]A相反,3-MCA主要通过湾区二醇环氧化物被活化,因为其环戊环是饱和的且不易环氧化。因此,我们提出B[j]A在Ki-ras第12密码子中产生的GGT→CGT突变主要是环戊环衍生加合物的结果。
