Investigation of Genetic Polymorphisms Related to the Outcome of Radiotherapy for Prostate Cancer Patients

Author:

Cintra Hellen Silva12,Pinezi Juliana Castro Dourado34,Machado Graziella Dias Pinheiro24,Carvalho Gustavo Moura de23,Carvalho Ana Terra Silva12,dos Santos Thalles Eduardo Dias23,Marciano Ricardo Duarte23,Soares Renata de Bastos Ascenço123

Affiliation:

1. Programa de Mestrado em Genética, Pontifícia Universidade Católica de Goiás, Avenida Universitária 1440 Setor Universitário, 74605-010 Goiânia, GO, Brazil

2. Laboratório de Oncogenética e Radiobiologia, Associação de Combate ao Câncer em Goiás, Rua 239 N.52 Lt.29, Setor Universitário, 74605-070 Goiânia, GO, Brazil

3. Departamento de Medicina, Pontifícia Universidade Católica de Goiás, Avenida Universitária 1440 Setor Universitário, 74605-010 Goiânia, GO, Brazil

4. Serviço de Radioterapia, Hospital Araújo Jorge, Associação de Combate ao Câncer em Goiás, Rua 239 N.52 Lt.181, Setor Universitário, 74605-070 Goiânia GO, Brazil

Abstract

The purpose of this study was to evaluate the association betweenATM,TP53 andMDM2 polymorphisms in prostate cancer patients and morbidity after radiotherapy. The presence ofATM(rs1801516),TP53 (rs1042522, rs1800371, rs17878362, rs17883323, and rs35117667), andMDM2 (rs2279744) polymorphisms was assessed by direct sequencing of PCR fragments from 48 patients with histologically proven prostate adenocarcinoma and treated with external beam radiation. The side effects were classified according to the Radiation Therapy Oncology Group (RTOG) score. The results showed no association between clinical characteristics and the development of radiation toxicities (P> 0.05). The C>T transition in the position 16273 (intron 3) of TP53 (rs35117667) was significantly associated with the risk of acute skin toxicity (OR: 0.0072, 95% CI 0.0002–0.227,P= 0.003). The intronic TP53 polymorphism at position 16250 (rs17883323) was associated with chronic urinary toxicity (OR: 0.071, 95%CI 0.006–0.784,P= 0.032). No significant associations were found for the remaining polymorphisms (P> 0.05). The results show that clinical characteristics were not determinant on the developing of radiation sensitivity in prostate cancer patients, and intronic TP53 polymorphisms would be associated with increased acute and chronic radiation toxicities. These observations corroborate the importance of investigating the genetic profile to predict adverse side effects in patients undergoing radiotherapy.

Funder

Financiadora de Estudos e Projetos

Publisher

Hindawi Limited

Subject

Biochemistry (medical),Clinical Biochemistry,Genetics,Molecular Biology,General Medicine

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