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致癌性V599E和V599K突变在B-raf激酶结构域中的优势在黑色素瘤淋巴结转移中增强。

Preponderance of the oncogenic V599E and V599K mutations in the B-raf kinase domain is enhanced in melanoma lymph node metastases.

作者信息

Kirschner Martin, Helmke Burkhard, Starz Hans, Benner Axel, Thome Marianne, Deichmann Martin

机构信息

Department of Dermatology, Heidelberg University Clinics, Arnsburger Weg 1, 63571 Gelnhausen, Germany.

出版信息

Melanoma Res. 2005 Oct;15(5):427-34. doi: 10.1097/00008390-200510000-00011.

Abstract

Downstream of Ras, the serine/threonine kinase B-raf has been reported to be mutated, amongst other carcinomas, in a substantial subset of primary melanomas, with a preponderance of mutations within the kinase domain, including the activating V599E and V599K transitions. We investigated a representative series of 54 resection specimens of melanoma lymph node metastases for the presence of mutations within the activation segment (exon 15) of the B-raf kinase domain by polymerase chain reaction (PCR) and single-strand conformational polymorphism (SSCP) gel electrophoresis. Sequencing of cloned PCR-SSCP amplicons resulted in 24 (44%) samples harbouring somatic mutations, which is not significantly different from the mutation frequency found in recently investigated primary cutaneous melanomas (Deichmann M, Thome M, Benner A, Näher H. B-raf exon 15 mutations are common in primary melanoma resection specimens but not associated with clinical outcome. Oncology 2004; 66:411-419). The activating mutation T1796A was present in 20 (83%) of these resection specimens, followed in frequency by the oncogenic g1795A mutation in five (21%) cases. With regard to the B-raf protein sequence, the acidic amino acid transitions V599E and V599K were predicted in 15 (62%) and five (21%) of the 24 positive metastases, respectively. The detection of mutations at this hot spot codon was significantly associated with subsequent visceral metastasis (P=0.03; Fisher's exact test). During the transition from primary melanomas (see reference above) to lymph node metastases, the spectrum of B-raf mutations narrows significantly (P=0.00047). The oncogenic B-raf mutations V599E and V599K, as early events in melanocyte transformation, persist throughout metastasis with important prognostic implications.

摘要

在Ras下游,丝氨酸/苏氨酸激酶B-raf已被报道在多种癌症中发生突变,在原发性黑色素瘤的相当一部分病例中也有突变,激酶结构域内存在大量突变,包括激活型V599E和V599K转换。我们通过聚合酶链反应(PCR)和单链构象多态性(SSCP)凝胶电泳,研究了一系列具有代表性的54例黑色素瘤淋巴结转移切除标本,以检测B-raf激酶结构域激活区(第15外显子)内的突变情况。对克隆的PCR-SSCP扩增子进行测序后发现,24例(44%)样本存在体细胞突变,这与最近研究的原发性皮肤黑色素瘤中的突变频率无显著差异(Deichmann M, Thome M, Benner A, Näher H. B-raf第15外显子突变在原发性黑色素瘤切除标本中常见,但与临床结局无关。肿瘤学2004;66:411 - 419)。激活突变T1796A存在于20例(83%)这些切除标本中,其次是致癌性g1795A突变,有5例(21%)。就B-raf蛋白序列而言,在24例阳性转移病例中,分别有15例(62%)和5例(21%)预测存在酸性氨基酸转换V599E和V599K。该热点密码子处突变的检测与随后的内脏转移显著相关(P = 0.03;Fisher精确检验)。在从原发性黑色素瘤(见上述参考文献)向淋巴结转移的转变过程中,B-raf突变谱显著变窄(P = 0.00047)。致癌性B-raf突变V599E和V599K作为黑素细胞转化的早期事件,在整个转移过程中持续存在,具有重要的预后意义。

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