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Mutational analysis of the transforming growth factor beta receptor type I gene in primary non-small cell lung cancer |
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| Authors: | Zhang Hong-Tao Fei Qing-Yan Chen Feng Qi Qing-Yuan Zou Wei Wang Jiu-Cun Zhang Rong-Mei Tao Shi-Heng Chen Xiao-Feng Luo Ze-Wei |
| Affiliation: | a Laboratory of Population and Quantitative Genetics, The State Key Laboratory of Genetic Engineering, Institute of Genetics, Morgan –Tan International Center for Life Sciences, Fudan University, Shanghai 200433, P.R, China b Department of Surgery, Shanghai Hospital for Pulmonary Diseases, Shanghai 200433, P.R, China c School of Biosciences, The University of Birmingham, Edgbaston, Birmingham B15 2TT, UK |
| Abstract: | Transforming growth factor-β receptor-dependent signals are critical for cell growth and differentiation and are often disrupted during tumorigenesis. The entire coding region of TGFβRI and flanking intron sequences from 53 primary non-small cell lung cancer (NSCLC) tissues were examined for alterations using SSCP and direct sequencing. No somatic point mutations other than two silent mutations and a polymorphism were found in the TGFβRI gene. The two silent mutations located at codon 344 (AAT to AAC) and codon 406 (TTA to CTA), respectively, and the polymorphism was at the 24th base of intron 7 (G to A). To investigate whether the presence of this polymorphism is associated with NSCLC, we determined its allele distribution in all the 53 carcinomas and 89 normal controls. Interestingly, we found that the subjects with homozygous genotype A/A displayed more than 3-fold increased risk of developing NSCLC than the common wild genotype G/G. As the first report, the present study showed that TGFβRI gene is not a frequent site of spontaneous mutational inactivation while the detected polymorphism is frequent in the pathogenesis of NSCLC. |
| Keywords: | TGFβRI NSCLC PCR-SSCP Mutation Polymorphism |
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