Smanik P A, Furminger T L, Mazzaferri E L, Jhiang S M
Department of Physiology and Internal Medicine, Ohio State University, Columbus 43210, USA.
Hum Mol Genet. 1995 Dec;4(12):2313-8. doi: 10.1093/hmg/4.12.2313.
The ret/PTC oncogene, rearranged form of the ret proto-oncogene (c-ret), has been detected specifically in a minority of papillary thyroid carcinomas. Three forms of the ret/PTC oncogene have been identified; the two most common forms, ret/PTC-1 and ret/PTC-3, both result from a paracentric inversion, of the long arm of chromosome 10. In this study, we have successfully amplified the chimeric introns resulting from these inversions, ranging from 1.4 to 10 kb, from four of five tumors known to contain the ret/PTC-1 oncogene (where c-ret rearranges with the H4 gene), and from 1/1 tumors containing the ret/PTC-3 oncogene (where c-ret rearranges with the ele1 gene). We localized the breakpoints within the chimeric introns using nested PCR, and determined the exact nucleotide sequence at the breakpoint for each tumor. Our results indicate that the breakpoints in c-ret occur at sites distributed across intron 11, where breaks in H4 intron 1 appear more frequently at the 5'- end of the intron. Interestingly, in all tumors that we investigated, the breakpoints occurred at sits of two or three nucleotide matches between the contributing germline sequences. In summary, we describe a simple, convenient way to investigate the ret/PTC breakpoints, and have revealed several common features of the breakpoints which warrant further investigations.
ret/PTC癌基因是原癌基因ret(c-ret)的重排形式,已在少数甲状腺乳头状癌中被特异性检测到。已鉴定出ret/PTC癌基因的三种形式;两种最常见的形式,ret/PTC-1和ret/PTC-3,均由10号染色体长臂的臂间倒位产生。在本研究中,我们成功地从已知含有ret/PTC-1癌基因(其中c-ret与H4基因重排)的五例肿瘤中的四例,以及含有ret/PTC-3癌基因(其中c-ret与ele1基因重排)的1/1例肿瘤中,扩增出了由这些倒位产生的长度在1.4至10 kb之间的嵌合内含子。我们使用巢式PCR将断点定位在嵌合内含子内,并确定了每个肿瘤断点处的确切核苷酸序列。我们的结果表明,c-ret中的断点发生在11号内含子分布的位点,其中H4内含子1中的断点在该内含子的5'端出现得更频繁。有趣的是,在我们研究的所有肿瘤中,断点发生在相关种系序列之间有两到三个核苷酸匹配的位点。总之,我们描述了一种简单、便捷的方法来研究ret/PTC断点,并揭示了断点的几个共同特征,值得进一步研究。
