Przygodzki R M, Finkelstein S D, Keohavong P, Zhu D, Bakker A, Swalsky P A, Soini Y, Ishak K G, Bennett W P
Laboratory of Human Carcinogenesis, National Cancer Institute, National Institutes of Health, Bethesda, Maryland, USA.
Lab Invest. 1997 Jan;76(1):153-9.
Hepatic angiosarcoma (HA) is an uncommon neoplasm associated with known etiologic factors in 25% to 42% of cases. It is, however, one of the most common sarcomas found in the liver. The aim of this study was to find was to find mutations in the K-ras-2 oncogene in sporadic and Thorotrast (TT)-induced HA. Point mutations in K-ras-2 were sought in archival, formalin-fixed tissue blocks from 24 patients with angiosarcoma. Of these, 19 cases were sporadic and 5 were TT-induced. Mutational analysis was performed by topographic microdissection with PCR amplification followed by genotyping. Specific mutations were determined by two independent methods: (a) direct sequencing of the PCR product confirmed by rePCR and by using a different sequencing primer, and (b) PCR-based selective enrichment of mutant DNA by endonuclease digestion followed by heteroduplex DNA analysis using denaturing gradient gel electrophoresis. Eleven K-ras-2 point mutations were detected in 7 of 24 (29%) tumors, including 5 of 19 (26%) sporadic HA and 2 of 5 (40%) TT-induced HA. There were seven G:C > A:T and four G:C > T:A mutations. All seven mutated tumors contained a codon 12-aspartate amino acid substitution. In addition, a second codon 12-cysteine mutant cell population was present in one of two codon 12-aspartate mutated TT-induced HA and in three of five codon 12-aspartate sporadic tumors. Of these four tumors, three contained both aspartate and cysteine mutations and were composed of multiple nodules; the fourth was a single mass. Seventeen tumors had multiple nodules; whereas 5 had a K-ras-2 mutation, 12 were wild-type. The molecular pathology of both sporadic and TT-induced HA is characterized by a high rate of K-ras-2 mutations characteristic of oxidative damage (ie, G:C > A:T and G:C > T:A mutations) resulting in two mutated population sets: codon 12 GGT > GAT and GGT > TGT (glycine to aspartic acid and cysteine). This is, to date, the first study to characterize the K-ras-2 gene mutations within human sporadic and TT-induced HA by direct sequence analysis and denaturing gradient gel electrophoresis. These data further support the hypothesis linking adduct-forming vinyl chloride exposure to HA containing a much higher frequency of K-ras-2 mutations and a mutational spectrum characteristic of chloroethylene oxide, a carcinogenic metabolite of vinyl chloride.
肝血管肉瘤(HA)是一种罕见的肿瘤,25%至42%的病例有已知病因。然而,它是肝脏中最常见的肉瘤之一。本研究的目的是在散发性和钍造影剂(TT)诱发的HA中寻找K-ras-2癌基因的突变。在24例血管肉瘤患者的存档福尔马林固定组织块中寻找K-ras-2的点突变。其中,19例为散发性,5例为TT诱发。通过拓扑显微切割结合PCR扩增,然后进行基因分型来进行突变分析。通过两种独立方法确定特定突变:(a)对PCR产物进行直接测序,通过再PCR并用不同测序引物进行确认,以及(b)通过核酸内切酶消化对突变DNA进行基于PCR的选择性富集,然后使用变性梯度凝胶电泳进行异源双链DNA分析。在24个肿瘤中的7个(29%)检测到11个K-ras-2点突变,包括19个散发性HA中的5个(26%)和5个TT诱发的HA中的2个(40%)。有7个G:C>A:T和4个G:C>T:A突变。所有7个突变肿瘤均含有密码子12-天冬氨酸氨基酸替代。此外,在两个密码子12-天冬氨酸突变的TT诱发的HA中的一个以及5个密码子12-天冬氨酸散发性肿瘤中的三个中存在第二个密码子12-半胱氨酸突变细胞群体。在这四个肿瘤中,三个同时含有天冬氨酸和半胱氨酸突变,且由多个结节组成;第四个是单个肿块。17个肿瘤有多个结节;其中5个有K-ras-2突变,12个为野生型。散发性和TT诱发的HA的分子病理学特征均为K-ras-2突变率高,具有氧化损伤特征(即G:C>A:T和G:C>T:A突变),导致两个突变群体:密码子12 GGT>GAT和GGT>TGT(甘氨酸到天冬氨酸和半胱氨酸)。这是迄今为止第一项通过直接序列分析和变性梯度凝胶电泳对人类散发性和TT诱发的HA中的K-ras-2基因突变进行特征描述的研究。这些数据进一步支持了将形成加合物的氯乙烯暴露与含有更高频率K-ras-2突变以及氯乙烯致癌代谢物环氧乙烷特征性突变谱的HA联系起来的假说。
