Literature DB >> 21149617

Polymorphisms inside microRNAs and microRNA target sites predict clinical outcomes in prostate cancer patients receiving androgen-deprivation therapy.

Bo-Ying Bao1, Jiunn-Bey Pao, Chun-Nung Huang, Yeong-Shiau Pu, Ta-Yuan Chang, Yu-Hsuan Lan, Te-Ling Lu, Hong-Zin Lee, Shin-Hun Juang, Lu-Min Chen, Chi-Jeng Hsieh, Shu-Pin Huang.   

Abstract

PURPOSE: Recent evidence indicates that small noncoding RNA molecules, known as microRNAs (miRNAs), are involved in cancer initiation and progression. We hypothesized that genetic variations in miRNAs and miRNA target sites could be associated with the efficacy of androgen-deprivation therapy (ADT) in men with prostate cancer. EXPERIMENTAL
DESIGN: We systematically evaluated 61 common single nucleotide polymorphisms (SNPs) inside miRNAs and miRNA target sites in a cohort of 601 men with advanced prostate cancer treated with ADT. The prognostic significance of these SNPs on disease progression, prostate cancer-specific mortality (PCSM) and all-cause mortality (ACM) after ADT were assessed by Kaplan-Meier analysis and Cox regression model.
RESULTS: Four, seven, and four SNPs were significantly associated with disease progression, PCSM, and ACM, respectively, after ADT in univariate analysis. KIF3C rs6728684, CDON rs3737336, and IFI30 rs1045747 genotypes remained as significant predictors for disease progression; KIF3C rs6728684, PALLD rs1071738, GABRA1 rs998754, and SYT9 rs4351800 remained as significant predictors for PCSM; and SYT9 rs4351800 remained as a significant predictor for ACM in multivariate models that included clinicopathologic predictors. Moreover, strong combined genotype effects on disease progression and PCSM were also observed. Patients with a greater number of unfavorable genotypes had a shorter time to progression and worse prostate cancer-specific survival during ADT (P for trend < 0.001).
CONCLUSION: SNPs inside miRNAs and miRNA target sites have a potential value to improve outcome prediction in prostate cancer patients receiving ADT. ©2010 AACR.

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Year:  2010        PMID: 21149617     DOI: 10.1158/1078-0432.CCR-10-2648

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


  34 in total

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2.  Does primary androgen-deprivation therapy delay the receipt of secondary cancer therapy for localized prostate cancer?

Authors:  Grace L Lu-Yao; Peter C Albertsen; Hui Li; Dirk F Moore; Weichung Shih; Yong Lin; Robert S DiPaola; Siu-Long Yao
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3.  Vitamin D receptor gene variants and clinical outcomes after androgen-deprivation therapy for prostate cancer.

Authors:  Jiunn-Bey Pao; Ying-Pi Yang; Chun-Nung Huang; Shu-Pin Huang; Tzyh-Chyuan Hour; Ta-Yuan Chang; Yu-Hsuan Lan; Te-Ling Lu; Hong-Zin Lee; Shin-Hun Juang; Chao-Yuan Huang; Bo-Ying Bao
Journal:  World J Urol       Date:  2011-12-23       Impact factor: 4.226

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Authors:  Jinliang Xing; Shaogui Wan; Feng Zhou; Falin Qu; Bingshan Li; Ronald E Myers; Xiaoying Fu; Juan P Palazzo; Xianli He; Zhinan Chen; Hushan Yang
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Review 7.  Genetic variation: effect on prostate cancer.

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Journal:  Cancer Discov       Date:  2015-02-17       Impact factor: 39.397

10.  PTBP1 Genetic Variants Affect the Clinical Response to Androgen-deprivation Therapy in Patients With Prostate Cancer.

Authors:  Shu-Pin Huang; Lih-Chyang Chen; Yei-Tsung Chen; Cheng-Hsueh Lee; Chao-Yuan Huang; Chia-Cheng Yu; Victor C Lin; Te-Ling Lu; Bo-Ying Bao
Journal:  Cancer Genomics Proteomics       Date:  2021 May-Jun       Impact factor: 4.069

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