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B-raf基因第15外显子突变在原发性黑色素瘤切除标本中很常见,但与临床结果无关。

B-raf exon 15 mutations are common in primary melanoma resection specimens but not associated with clinical outcome.

作者信息

Deichmann Martin, Thome Marianne, Benner Axel, Näher Helmut

机构信息

Department of Dermatology, University Clinics of Heidelberg, Heidelberg, Germany.

出版信息

Oncology. 2004;66(5):411-9. doi: 10.1159/000079490.

Abstract

Downstream of Ras, the serine/threonine kinase B-raf has recently been reported to be mutated, among other carcinomas, in a majority of melanoma cell lines with a preponderance of mutations within the kinase domain including the activating V599E transition. We therefore investigated a representative number of 50 primary melanoma resection specimens for the presence of mutations within the activation segment (exon 15) of the B-raf kinase domain. Applying polymerase chain reaction and single-strand conformation polymorphism gel electrophoresis, followed by DNA cloning and sequencing, we found 19 cases (38%) to harbor somatic B-raf exon 15 mutations. With respect to the B-raf protein sequence, the V599E mutation was predicted in 63% of these positive melanomas, followed in frequency by the V599K transition (31%). Detection of B-raf exon 15 mutations or prediction of the activating mutation V599E were not statistically associated with the risk for subsequent metastasis in the follow-up of patients. Altogether, the B-raf oncogene is affected in a substantial subset of melanoma resection specimens. As B-raf alterations possibly affect melanocyte-specific pathways controlling proliferation and differentiation, activation of this oncogene may contribute to the development of melanoma.

摘要

在Ras下游,丝氨酸/苏氨酸激酶B-raf最近被报道在多种癌症中发生突变,在大多数黑色素瘤细胞系中也有突变,激酶结构域内的突变占优势,包括激活型V599E转变。因此,我们研究了50例原发性黑色素瘤切除标本,以检测B-raf激酶结构域激活片段(第15外显子)内是否存在突变。应用聚合酶链反应和单链构象多态性凝胶电泳,随后进行DNA克隆和测序,我们发现19例(38%)存在体细胞B-raf第15外显子突变。就B-raf蛋白序列而言,在这些阳性黑色素瘤中,63%预测存在V599E突变,其次是V599K转变(31%)。在患者随访中,检测到B-raf第15外显子突变或预测激活型突变V599E与随后转移的风险无统计学关联。总之,在相当一部分黑色素瘤切除标本中,B-raf癌基因受到影响。由于B-raf改变可能影响控制增殖和分化的黑素细胞特异性途径,该癌基因的激活可能有助于黑色素瘤的发生。

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