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Aflatoxin serum levels and risk of hepatoeellular carcinoma in a nested case-control study in the United States

机译:美国一项巢式病例对照研究中的黄曲霉毒素血清水平和肝细胞癌风险

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Background Aflatoxin is one of the most powerful chemical carcinogens known. While it is well known that ingestion or exposure to high levels of aflatoxin is associated with a greater risk of hepatocellular carcinoma (HCC), particularly among chronic HBV carriers, no studies have examined this association in a low exposure region with exposure measured prospectively. Aims To address this gap, we conducted a nested case-control study within the Multiphasic Health Check-up (MHC) cohort at Kaiser Permanente Northern California (KPNC). Methods The study population was defined as the MHC participants who provided a serum sample between 1964 and 1985 with serum available. HCC cases (n=193) that occurred after MHC exam date were identified by linkage to the KPNC Cancer Registry. Controls (n=578) were randomly selected and matched to cases on age, sex, race/ethnicity and date of MHC exam (serum draw). Serum aflatoxin-albumin (AF-alb) adduct levels were determined by an enzyme-linked immunosorbent assay (EUSA) after albumin extraction, digestion and purification with the limit of detection at 0.5 pg AF-lysine equivalent per mg albumin. Results 118 participants had levels of AF-alb above the detection limit (16.1% of the cases and 15.1% of the controls). Among individuals with detectable levels, the range of AF-alb levels was 0.70 to 138.00 pg/mg. The majority of detectable levels were near the limits of detection, where the assay is least precise. Only a single case (0.5%) and 12 controls (2%) had levels >10.00 pg/mg. In a conditional logistic regression model, the odds ratio for having a detectable serum AF-alb level in relation to risk of HCC was 1.19 (95% confidence interval 0.76-1.87). Conclusions This study provides no evidence that low exposure levels of aflatoxin found in this U.S. sample are associated with.
机译:背景黄曲霉毒素是已知的最强大的化学致癌物之一。众所周知,摄入或暴露于高水平的黄曲霉毒素会增加肝细胞癌(HCC)的风险,尤其是在慢性HBV携带者中,但尚无研究在低暴露区域与前瞻性测得的这种联系进行研究。目的为了解决这一差距,我们在北加州凯撒永久医疗中心(KPNC)的多相健康检查(MHC)队列中进行了嵌套的病例对照研究。方法将研究人群定义为MHC参与者,他们在1964年至1985年之间提供了血清样本并提供了血清。通过与KPNC癌症登记处建立联系,确定在MHC考试日期之后发生的HCC病例(n = 193)。随机选择对照组(n = 578),并与年龄,性别,种族/民族和MHC检查日期(血清抽签)的病例相匹配。在白蛋白提取,消化和纯化后,通过酶联免疫吸附测定(EUSA)测定血清黄曲霉毒素-白蛋白(AF-alb)加合物的水平,检测极限为每毫克白蛋白0.5 pg AF-赖氨酸当量。结果118名参与者的AF-alb水平高于检测极限(16.1%的病例和15.1%的对照)。在可检测水平的个体中,AF-alb水平范围为0.70至138.00 pg / mg。大多数可检测水平接近检测极限,在此检测是最不精确的。只有一个病例(0.5%)和12个对照(2%)的水平> 10.00 pg / mg。在条件逻辑回归模型中,血清可检测的AF-alb水平与HCC风险的比值比为1.19(95%置信区间0.76-1.87)。结论这项研究没有证据表明该美国样品中黄曲霉毒素的低暴露水平与之相关。

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