共济失调毛细血管扩张症突变基因（ATM）错义变体P1054R易患前列腺癌。

ATM missense variant P1054R predisposes to prostate cancer.

作者信息

Meyer Andreas, Wilhelm Bettina, Dörk Thilo, Bremer Michael, Baumann Rolf, Karstens Johann Hinrich, Machtens Stefan

机构信息

Department of Radiation Oncology, Hannover Medical School, Germany.

出版信息

Radiother Oncol. 2007 Jun;83(3):283-8. doi: 10.1016/j.radonc.2007.04.029. Epub 2007 May 14.

DOI:10.1016/j.radonc.2007.04.029

PMID:17502119

Abstract

BACKGROUND

Prostate cancer is associated with defective DNA strand break repair after DNA damage leading to genetic instability and prostate cancer progression. The ATM (ataxia-telangiectasia mutated) gene product is known to play an important role in cell cycle regulation and maintenance of genomic integrity. We investigated whether the prevalence of the ATM missense substitution P1054R is increased in a hospital-based series of prostate cancer patients and whether carriers are at increased risk for treatment-related side effects.

MATERIALS AND METHODS

A consecutive series of 261 patients treated for early-stage prostate cancer with I-125 brachytherapy (permanent seed implantation) between 10/2000 and 04/2006 at our institution and a comparison group of 460 male control individuals were screened for the presence of the P1054R variant. Outcome of therapy regarding morbidity was assessed prospectively and compared between carriers vs. non-carriers with the International Prostate Symptom Score (IPSS), a Quality-of-Life-index (QoL) and the International Index of Erectile Function (IIEF-15) with its subgroups (IIEF-5 and EF).

RESULTS

The proportion of carriers of the P1054R variant was significantly higher among prostate cancer patients than in the general population (25 out of 261 vs. 22 out of 460; OR 2.1; 95% CI 1.2-3.8, p<0.01). A subgroup of the carriers additionally harboured the ATM missense variant F858L that was associated with a similar risk (OR=2.2; 95% CI 1.1-4.6; p=0.03). After a mean follow-up of 18 months there were no statistically significant differences regarding IPSS (p=0.48), QoL (p=0.61), IIEF-15 score (p=0.78), IIEF-5 score (p=0.83), and EF score (p=0.80), respectively.

CONCLUSIONS

The ATM missense variant P1054R confers an about twofold increased risk for prostate cancer in our series. The subgroup of patients with the second-site variant F858L is not at significantly higher risk. After 18 months, there was no evidence for an increased adverse radiotherapy response in P1054R carriers.

摘要

背景

前列腺癌与DNA损伤后DNA链断裂修复缺陷相关，这会导致基因不稳定和前列腺癌进展。已知共济失调毛细血管扩张症突变（ATM）基因产物在细胞周期调控和基因组完整性维持中起重要作用。我们调查了在一组以医院为基础的前列腺癌患者中，ATM错义替代P1054R的发生率是否增加，以及携带者是否有更高的治疗相关副作用风险。

材料与方法

对2000年10月至2006年4月期间在我们机构接受I-125近距离放射治疗（永久性粒子植入）的261例早期前列腺癌患者的连续系列，以及460名男性对照个体组成的比较组，筛查P1054R变体的存在情况。前瞻性评估治疗关于发病率的结果，并使用国际前列腺症状评分（IPSS）、生活质量指数（QoL）和国际勃起功能指数（IIEF-15）及其亚组（IIEF-5和EF）比较携带者与非携带者之间的情况。

结果

前列腺癌患者中P1054R变体携带者的比例显著高于普通人群（261例中有25例，460例中有22例；比值比2.1；95%可信区间1.2 - 3.8，p<0.01）。携带者的一个亚组还携带与类似风险相关的ATM错义变体F858L（比值比=2.2；95%可信区间1.1 - 4.6；p = 0.03）。平均随访18个月后，在IPSS（p = 0.48）、QoL（p = 0.61）、IIEF-15评分（p = 0.78）、IIEF-5评分（p = 0.83）和EF评分（p = 0.80）方面分别没有统计学上的显著差异。