Predictive value in the analysis of RNASEL genotypes in relation to prostate cancer

被引:10
|
作者
Alvarez-Cubero, M. J. [1 ]
Entrala, C. [2 ]
Fernandez-Rosado, F. [2 ]
Martinez-Gonzalez, L. J. [3 ]
Alvarez, J. C. [1 ,3 ]
Suarez, A. [4 ]
Lorente, J. A. [1 ,3 ]
Cozar, J. M. [4 ]
机构
[1] Univ Granada, Fac Med, Lab Genet Identificat, Legal Med & Toxicol Dept, E-18071 Granada, Spain
[2] Ciencias Salud BIC, PT, R&D Div, LORGEN GP, Granada, Spain
[3] Univ Granada, Pfizer Ctr, Biomed Res Ctr, Junta Andalucia Genom & Oncol Res, E-18071 Granada, Spain
[4] Univ Hosp Virgen de las Nieves, Serv Urol, Granada, Spain
关键词
genetic profile; RNASEL; South European population; GENE; RISK; ASSOCIATION; VARIANTS; MUTATION; POLYMORPHISMS; 471DELAAAG; HEREDITARY;
D O I
10.1038/pcan.2011.56
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
BACKGROUND: We would like to compare the different RNASEL genotypes with the stage of the cancer using parameters such as PSA levels, Gleason score and T-stage, and to develop a clinical protocol for the monitoring of the disease for trying a better evolution of the patient. METHODS: A total of 231 patients with sporadic prostate cancer and 100 of controls were genotyped in RNASEL gene by sequencing the exons 1 and 3. A survey of clinical information was collected by a specialist following the Helsinki protocol. All patients and controls were interviewed by a researcher and signed their informed consent to participation in the study, which was approved by Ethics Committee of the hospital. The genetic information was processed and collected with an ABI PRISM Genetic Analyser 3130 using SeqScape software v. 2.6. All the patients were analysed by comparing the genetic and clinical data. chi(2)-tests, Monte Carlo, Fisher tests and contigency tables were performed using SPSS v. 15.0 and ARLEQUIN v. 3.5 software on patient population. RESULTS: Significant differences were found only between patients and controls in D541E, R461Q and I97L genotypes, the remainder of the variants did not seem relevant to our population in contrast to other populations, such as north-Caucasians, Afro Americans and Ashkenazi Jews. The genotypes associated with the worst prognoses are G/G in D541E, A/A in R462Q and A/G in I97L. The controls were included in our study to determine an approximation of the genotype in our population compared with the patients, but they did not account for the statistical process. CONCLUSIONS: The genetic profile of patients with this cancer combined with other parameters could be used as a prognosis factor in deciding to give more radical and frequent treatments, depending on personal genotype.
引用
收藏
页码:144 / 149
页数:6
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