RadGenomics Project, National Institute of Radiological Sciences, Chiba, Japan.
Int J Radiat Oncol Biol Phys. 2011 Nov 15;81(4):1144-52. doi: 10.1016/j.ijrobp.2010.09.012. Epub 2010 Nov 2.
This study sought to associate polymorphisms in genes related to cell cycle regulation or genome maintenance with radiotherapy (RT)-induced an early adverse reaction (EAR) in patients with cervical cancer.
This study enrolled 243 cervical cancer patients who were treated with pelvic RT. An early gastrointestinal reaction was graded using the National Cancer Institute Common Toxicity Criteria, version 2. Clinical factors of the enrolled patients were analyzed, and 208 patients were grouped for genetic analysis according to their EAR (Grade ≤1, n = 150; Grade ≥2, n = 58). Genomic DNA was genotyped, and association with the risk of EAR for 44 functional single-nucleotide polymorphisms (SNPs) of 19 candidate genes was assessed by single-locus, haplotype, and multilocus analyses.
Our analysis revealed two haplotypes to be associated with an increased risk of EAR. The first, comprising rs625120C, rs189037T, rs228589A, and rs183460G, is located between the 5' ends of NPAT and ATM (OR = 1.86; 95% CI, 1.21-2.87), whereas the second is located in the AURKA gene and comprises rs2273535A and rs1047972G (OR = 1.75; 95% CI, 1.10-2.78). A third haplotype, rs2273535T and rs1047972A in AURKA, was associated with a reduced EAR risk (OR = 0.42; 95% CI, 0.20-0.89). The risk of EAR was significantly higher among patients with both risk diplotypes than in those possessing the other diplotypes (OR = 3.24; 95% CI, 1.52-6.92).
Individual radiosensitivity of intestine may be determined by haplotypes in the NPAT-ATM and AURKA genes. These variants should be explored in larger association studies in cervical cancer patients.
本研究旨在探讨与细胞周期调控或基因组维护相关的基因多态性与宫颈癌患者放疗(RT)诱导的早期不良反应(EAR)之间的关系。
本研究纳入了 243 例接受盆腔 RT 的宫颈癌患者。采用国立癌症研究所常见毒性标准(版本 2)对早期胃肠道反应进行分级。分析了纳入患者的临床因素,根据 EAR(Grade≤1,n=150;Grade≥2,n=58)将 208 例患者分为两组进行遗传分析。对基因组 DNA 进行基因分型,并通过单基因座、单体型和多基因座分析评估 19 个候选基因的 44 个功能单核苷酸多态性(SNP)与 EAR 风险的相关性。
我们的分析显示,有两个单体型与 EAR 风险增加相关。第一个单体型由 rs625120C、rs189037T、rs228589A 和 rs183460G 组成,位于 NPAT 和 ATM 的 5'端之间(OR=1.86;95%CI,1.21-2.87),而第二个单体型位于 AURKA 基因中,由 rs2273535A 和 rs1047972G 组成(OR=1.75;95%CI,1.10-2.78)。AURKA 基因中的 rs2273535T 和 rs1047972A 单体型与 EAR 风险降低相关(OR=0.42;95%CI,0.20-0.89)。与携带其他单体型的患者相比,同时携带两种风险单体型的 EAR 风险显著更高(OR=3.24;95%CI,1.52-6.92)。
肠道的个体放射敏感性可能由 NPAT-ATM 和 AURKA 基因中的单体型决定。这些变体应该在更大的宫颈癌患者关联研究中进行探索。
