Association between polymorphisms in sex hormones synthesis and metabolism and prostate cancer aggressiveness

Inmaculada Robles-Fernandez; Luis Javier Martinez-Gonzalez; Manrique Pascual-Geler; Jose Manuel Cozar; Ignacio Puche-Sanz; Maria Jose Serrano; Jose Antonio Lorente; Maria Jesus Alvarez-Cubero

doi:10.1371/journal.pone.0185447

Association between polymorphisms in sex hormones synthesis and metabolism and prostate cancer aggressiveness

PLoS One. 2017 Oct 5;12(10):e0185447. doi: 10.1371/journal.pone.0185447. eCollection 2017.

Authors

Inmaculada Robles-Fernandez¹, Luis Javier Martinez-Gonzalez¹, Manrique Pascual-Geler², Jose Manuel Cozar², Ignacio Puche-Sanz², Maria Jose Serrano^{1

3}, Jose Antonio Lorente^{1

4}, Maria Jesus Alvarez-Cubero^{1

5}

Affiliations

¹ GENYO. Centre for Genomics and Oncological Research: Pfizer / University of Granada /Andalusian Regional Government. Granada, Spain.
² Urology Department, University Hospital Virgen de las Nieves. Granada, Spain.
³ Integral Oncology Division, Clinical University Hospital. Granada, Spain.
⁴ Laboratory of Genetic Identification, University of Granada-Department of Legal Medicine-Faculty of Medicine, Granada, Spain.
⁵ Cell Biology Department, University of Granada- Faculty of Sciences, Granada, Spain.

Abstract

Novel biomarkers for prostate cancer (PCa) diagnosis and prognosis are necessary to improve the accuracy of current ones employed in clinic. We performed a retrospective study between the association of several polymorphisms in the main genes involved in the synthesis and metabolism of sex hormones and PCa risk and aggressiveness. A total of 311 Caucasian men (155 controls and 156 patients) were genotyped for 9 SNPs in AR, CYP17A1, LHCGR, ESR1 and ESR2 genes. Diagnostic PSA serum levels, Gleason score, tumor stage, D´Amico risk and data of clinical progression were obtained for patients at the moment of the diagnosis and after 54 months of follow-up. Chi-squared test were used for comparisons between clinical variables groups, logistic regression for clinical variables associations between SNPs; and Kaplan-Meier for the association between SNPs and time to biochemical progression. We found 5 variants (CYP17A1) rs743572, rs6162, rs6163; (LHCGR) rs2293275 and (ESR2) rs1256049 that were statistically significant according to clinical variables (PSA, D´Amico risk and T stage) on a case-case analysis. Moreover, the presence of A and G alleles in rs743572 and rs6162 respectively, increase the risk of higher PSA levels (>10 ng/μl). With respect to D´Amico risk rs743572 (AG-GG), rs6162 (AG-AA) and rs6163 (AC-AA) were associated with an increased risk; and last, AC and AA genotypes for rs6163 were associated with a shorter biochemical recurrence free survival (BRFS) in patients with radical prostatectomy. In multigene analysis, several variants in SNPs rs2293275, rs6152, rs1062577, rs6162, rs6163, rs1256049 and rs1004467 were described to be associated with a more aggressiveness in patients. However, none of the selected SNPs show significant values between patients and controls. In conclusion, this study identified inherited variants in genes CYP17A1, LHCGR and ESR2 related to more aggressiveness and/or a poor progression of the disease. According to this study, new promise PCa biomarkers for clinical management could be included in these previous SNPs.

MeSH terms

Case-Control Studies
Gonadal Steroid Hormones / biosynthesis*
Humans
Male
Multigene Family
Polymorphism, Single Nucleotide*
Prostatic Neoplasms / genetics
Prostatic Neoplasms / metabolism
Prostatic Neoplasms / pathology*
Recurrence

Substances

Gonadal Steroid Hormones

Grants and funding

The author(s) received no specific funding for this work.