Beiderbeck-Noll A B, Sturkenboom M C J M, van der Linden P D, Herings R M C, Hofman A, Coebergh J W W, Leufkens H G M, Stricker B H Ch
Department of Pharmacoepidemiology & Pharmacotherapy, Utrecht Institute for Pharmaceutical Sciences (UIPS), Utrecht, The Netherlands.
Eur J Cancer. 2003 Jan;39(1):98-105. doi: 10.1016/s0959-8049(02)00157-0.
The association between the use of calcium channel blockers (CCB) and cancer has received ample attention, but is still controversial. In this study, we have tested the hypothesis that the observed association between CCB and cancer in earlier studies could be explained by residual confounding or by misclassification of exposure because of the use of cross-sectional data on drug use. Data from the Rotterdam Study, a prospective population-based cohort study in the municipal area Ommoord, were used. The study population consisted of a cohort of 3204 participants aged 71 years or older who were followed from a baseline interview in the period 1991-1993 for the occurrence of incident cancer. Data on drug use were gathered at baseline and through the seven community pharmacies which served the Ommoord region during the study period between 1 January 1991 and 1 January 1999. Incident cancer events were gathered from a nationwide registry of hospitalisation data and from a specialised cancer centre in the Rotterdam region. We performed three analyses. First, we followed the method, and adjusted for the same risk factors, as in the earlier studies. In the second analysis, we included all risk factors that were univariately associated with cancer in the Rotterdam Study. In the third analysis, we included exposure to CCBs as time-varying co-variates, while adjusting for potential confounders. The relative risk (RR) of cancer associated with CCB was 1.4 (95% Confidence Interval (CI): 0.9-2.0) in the first analysis and lowered to 1.2 (95% CI: 0.8-1.8) upon adjustment for the different co-variates in the second. In both analyses, however, verapamil was significantly associated with cancer with RRs of 2.1 (95% CI: 1.1-4.0) and 2.0 (1.01-3.9), respectively, whereas no associations were found with the other CCB in this study, i.e. diltiazem and nifedipine. A significantly increased risk of cancer was found for intermediate daily doses of verapamil and diltiazem. Intake of other antihypertensives such as beta-blocking agents, diuretics and ACE-inhibitors was not associated with cancer. In the third analysis with exposure to CCB as time-varying co-variates, the risk increase was non-significant for use of 2 years or less, 1.0 (95% CI: 0.7-1.5), and for use for a cumulative period of more than 2 years, 1.3 (95% CI: 0.8-2.0). However, in all models the hazard ratio was statistically significantly increased for verapamil, but not for diltiazem and nifedipine. On the basis of these analyses, we found no increase in cancer in users of diltiazem and nifedipine, nor in users of other antihypertensives. In line with earlier studies, however, we found an increased risk of cancer in users of verapamil. At variance with the conclusions from several other studies, we think that it is too early to conclude that CCB are not associated with cancer.
钙通道阻滞剂(CCB)的使用与癌症之间的关联已受到广泛关注,但仍存在争议。在本研究中,我们检验了这样一个假设,即早期研究中观察到的CCB与癌症之间的关联可能是由残余混杂因素或因使用药物使用的横断面数据导致的暴露误分类所解释。我们使用了鹿特丹研究的数据,这是一项在奥莫德市辖区基于人群的前瞻性队列研究。研究人群包括3204名年龄在71岁及以上的参与者组成的队列,他们从1991 - 1993年的基线访谈开始,随访新发癌症的发生情况。药物使用数据在基线时收集,并通过在1991年1月1日至1999年1月1日研究期间为奥莫德地区服务的七家社区药店收集。新发癌症事件从全国范围的住院数据登记处和鹿特丹地区的一家专业癌症中心收集。我们进行了三项分析。首先,我们遵循早期研究的方法,并对相同的风险因素进行了调整。在第二项分析中,我们纳入了在鹿特丹研究中与癌症单因素相关的所有风险因素。在第三项分析中,我们将CCB的暴露作为随时间变化的协变量纳入,同时对潜在混杂因素进行调整。在第一项分析中,与CCB相关的癌症相对风险(RR)为1.4(95%置信区间(CI):0.9 - 2.0),在第二项分析中对不同协变量进行调整后降至1.2(95% CI:0.8 - 1.8)。然而,在这两项分析中,维拉帕米与癌症均显著相关,RR分别为2.1(95% CI:1.1 - 4.0)和2.0(1.01 - 3.9),而在本研究中未发现其他CCB(即地尔硫䓬和硝苯地平)与癌症有关联。发现中等日剂量的维拉帕米和地尔硫䓬患癌风险显著增加。其他抗高血压药物如β受体阻滞剂、利尿剂和ACE抑制剂的摄入与癌症无关。在将CCB暴露作为随时间变化协变量的第三项分析中,使用2年或更短时间的风险增加不显著,为1.0(95% CI:0.7 - 1.5),使用累计超过2年的风险为1.3(95% CI:0.8 - 2.0)。然而,在所有模型中,维拉帕米的风险比在统计学上显著增加,而地尔硫䓬和硝苯地平则不然。基于这些分析,我们发现地尔硫䓬和硝苯地平使用者以及其他抗高血压药物使用者的癌症发病率没有增加。然而,与早期研究一致,我们发现维拉帕米使用者患癌风险增加。与其他几项研究的结论不同,我们认为现在就得出CCB与癌症无关的结论还为时过早。
