Mutational analysis of PINX1 in hereditary prostate cancer |
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| Authors: | Hawkins Gregory A Chang Bao-Li Zheng S Lilly Isaacs Sarah D Wiley Kathleen E Bleecker Eugene R Walsh Patrick C Meyers Deborah A Xu Jianfeng Isaacs William B |
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| Affiliation: | Center for Human Genomics, Wake Forest University School of Medicine, Winston-Salem, North Carolina, USA. |
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| Abstract: | ![]()
BACKGROUND: Telomerase activity is increased in most tumors. PinX1 has recently been identified as a critical component in regulating telomerase activity. The PinX1 gene is located within chromosomal region 8p22-23, a region associated with LOH and potentially linked to increased prostate cancer risk. METHODS: PINX1 was re-sequenced in 159 hereditary prostate cancer (HPC) probands. Four non-synonymous coding variants were genotyped in 159 HPC families. RESULTS: Thirty-nine polymorphisms were identified in the HPC screening panel. Ten coding polymorphisms were identified, seven (Gln50His, Leu91Met, Gln206His, Arg215Ile, Thr220Ala, Ser254Cys, and Glu414Ala) of which were non-synonymous. The most common variants Thr220Ala and Ser254Cys were not significantly over-transmitted from affected parent to affected offspring. CONCLUSIONS: Based on these results, we conclude that PINX1 is not a major factor for HPC risk. |
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| Keywords: | prostate cancer telomerase PinX1 polymorphisms |
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