Winchester Danyelle A, Till Cathee, Goodman Phyllis J, Tangen Catherine M, Santella Regina M, Johnson-Pais Teresa L, Leach Robin J, Xu Jianfeng, Zheng S Lilly, Thompson Ian M, Lucia M Scott, Lippman Scott M, Parnes Howard L, Isaacs William B, De Marzo Angelo M, Drake Charles G, Platz Elizabeth A
Department of Epidemiology, Johns Hopkins Bloomberg School of Public Health, Baltimore, Maryland.
SWOG Statistical Center, Fred Hutchinson Cancer Research Center, Seattle, Washington.
Prostate. 2017 Jun;77(8):908-919. doi: 10.1002/pros.23346. Epub 2017 Mar 20.
We reported that some, but not all single nucleotide polymorphisms (SNPs) in select immune response genes are associated with prostate cancer, but not individually with the prevalence of intraprostatic inflammation in the Prostate Cancer Prevention Trial (PCPT) placebo arm. Here, we investigated whether these same SNPs are associated with risk of lower- and higher-grade prostate cancer in men randomized to finasteride, and with prevalence of intraprostatic inflammation among controls. Methods A total of 16 candidate SNPs in IL1β, IL2, IL4, IL6, IL8, IL10, IL12(p40), IFNG, MSR1, RNASEL, TLR4, and TNFA and 7 tagSNPs in IL10 were genotyped in 625 white prostate cancer cases, and 532 white controls negative for cancer on an end-of-study biopsy nested in the PCPT finasteride arm. We used logistic regression to estimate log-additive odds ratios (OR) and 95% confidence intervals (CI) adjusting for age and family history.
Minor alleles of rs2243250 (T) in IL4 (OR = 1.46, 95% CI 1.03-2.08, P-trend = 0.03), rs1800896 (G) in IL10 (OR = 0.77, 95% CI 0.61-0.96, P-trend = 0.02), rs2430561 (A) in IFNG (OR = 1.33, 95% CI 1.02-1.74; P-trend = 0.04), rs3747531 (C) in MSR1 (OR = 0.55, 95% CI 0.32-0.95; P-trend = 0.03), and possibly rs4073 (A) in IL8 (OR = 0.81, 95% CI 0.64-1.01, P-trend = 0.06) were associated with higher- (Gleason 7-10; N = 222), but not lower- (Gleason 2-6; N = 380) grade prostate cancer. In men with low PSA (<2 ng/mL), these higher-grade disease associations were attenuated and/or no longer significant, whereas associations with higher-grade disease were apparent for minor alleles of rs1800795 (C: OR = 0.70, 95% CI 0.51-0.94, P-trend = 0.02) and rs1800797 (A: OR = 0.72, 95% CI 0.53-0.98, P-trend = 0.04) in IL6. While some IL10 tagSNPs were associated with lower- and higher-grade prostate cancer, distributions of IL10 haplotypes did not differ, except possibly between higher-grade cases and controls among those with low PSA (P = 0.07). We did not observe an association between the studied SNPs and intraprostatic inflammation in the controls.
In the PCPT finasteride arm, variation in genes involved in the immune response, including possibly IL8 and IL10 as in the placebo arm, may be associated with prostate cancer, especially higher-grade disease, but not with intraprostatic inflammation. We cannot rule out PSA-associated detection bias or chance due to multiple testing.
我们曾报道,某些(而非全部)免疫反应基因中的单核苷酸多态性(SNP)与前列腺癌相关,但在前列腺癌预防试验(PCPT)安慰剂组中,这些SNP并非单独与前列腺内炎症的患病率相关。在此,我们研究了这些相同的SNP是否与随机接受非那雄胺治疗的男性患低级别和高级别前列腺癌的风险相关,以及与对照组中前列腺内炎症的患病率相关。方法:在PCPT非那雄胺组中进行的一项研究结束时的活检中,对625例白人前列腺癌病例和532例活检结果为癌症阴性的白人对照进行了IL1β、IL2、IL4、IL6、IL8、IL10、IL12(p40)、IFNG、MSR1、RNASEL、TLR4和TNFA中的16个候选SNP以及IL10中的7个标签SNP的基因分型。我们使用逻辑回归来估计对数相加比值比(OR)和95%置信区间(CI),并对年龄和家族史进行了调整。
IL4中rs2243250(T)的次要等位基因(OR = 1.46,95% CI 1.03 - 2.08,P趋势 = 0.03)、IL10中rs1800896(G)的次要等位基因(OR = 0.77,95% CI 0.61 - 0.96,P趋势 = 0.02)、IFNG中rs2430561(A)的次要等位基因(OR = 1.33,95% CI 1.02 - 1.74;P趋势 = 0.04)、MSR1中rs3747531(C)的次要等位基因(OR = 0.55,95% CI 0.32 - 0.95;P趋势 = 0.03)以及可能IL8中rs4073(A)的次要等位基因(OR = 0.81,95% CI 0.64 - 1.01,P趋势 = 0.06)与高级别(Gleason 7 - 10;N = 222)前列腺癌相关,但与低级别(Gleason 2 - 6;N = 380)前列腺癌无关。在前列腺特异性抗原(PSA)水平较低(<2 ng/mL)的男性中,这些与高级别疾病的关联减弱和/或不再显著,而IL6中rs1800795(C:OR = 0.70,95% CI 0.51 - 0.94,P趋势 = 0.02)和rs1800797(A:OR = 0.72,95% CI 0.53 - 0.98,P趋势 = 0.04)的次要等位基因与高级别疾病的关联明显。虽然一些IL10标签SNP与低级别和高级别前列腺癌相关,但IL10单倍型的分布没有差异,可能除了PSA水平较低者中高级别病例与对照组之间(P = 0.07)。我们未观察到所研究的SNP与对照组中前列腺内炎症之间存在关联。
在PCPT非那雄胺组中,参与免疫反应的基因变异,可能如安慰剂组中的IL8和IL10,可能与前列腺癌相关,尤其是高级别疾病,但与前列腺内炎症无关。我们不能排除因PSA相关的检测偏倚或多次检验导致的偶然性。
