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相隔 15 年采集的预诊断样本中的循环 sCD27 和 sCD30 与未来非霍奇金淋巴瘤风险。

Circulating sCD27 and sCD30 in pre-diagnostic samples collected fifteen years apart and future non-Hodgkin lymphoma risk.

机构信息

Division of Cancer Epidemiology and Genetics, National Cancer Institute, Rockville, Maryland.

Johns Hopkins Bloomberg School of Public Health, Baltimore, Maryland.

出版信息

Int J Cancer. 2019 Apr 15;144(8):1780-1785. doi: 10.1002/ijc.31879. Epub 2018 Dec 19.

Abstract

Elevated serum sCD27 and sCD30 from a single banked sample have been associated with future non-Hodgkin lymphoma risk (NHL); however, the etiologic relevance of this finding is unclear. To address this question, we conducted a case-control study (235 cases, 235 controls) nested within the CLUE-I and CLUE-II cohorts, which enrolled participants in 1974 and 1989 respectively in Washington County, Maryland. Our study features a subset of 102 cases and 102 controls with two banked pre-diagnostic samples each, collected 15 years apart. In analyses involving an individual sample per subject, both sCD27 and sCD30 were associated with NHL diagnosed up to 20 years later. In analyses involving repeated samples, cases were significantly more likely than controls to have higher analyte levels in the CLUE-II vs. CLUE-I sample for sCD27 (p = 0.006) but not sCD30 (p = 0.16). In joint analyses of dichotomized analyte levels in both samples, the strongest NHL association observed for sCD27 was for having below-median levels in CLUE-I and above-median levels in CLUE-II [odds ratio (OR) 3.6, 95% confidence interval (CI) 1.4-9.2 vs. below-median levels in both). In joint analyses for sCD30, the strongest NHL association was observed for having above-median levels in both samples (OR 1.7, 95% CI 0.8-3.7), particularly for cases diagnosed >10 years after the CLUE-II sample (OR 2.4, 95% CI 0.9-6.7). Our findings suggest that sCD27 is a disease marker for NHL and add to the weight of evidence that elevated circulating sCD30 is a marker of increased NHL susceptibility.

摘要

从单个储存样本中检测到的血清 sCD27 和 sCD30 水平升高与未来非霍奇金淋巴瘤(NHL)风险相关;然而,这一发现的病因学相关性尚不清楚。为了解决这个问题,我们在 CLUE-I 和 CLUE-II 队列中进行了一项病例对照研究(235 例病例,235 例对照),该队列分别于 1974 年和 1989 年在马里兰州华盛顿县招募参与者。我们的研究具有一个亚组,包括 102 例病例和 102 例对照,每个个体有两个相隔 15 年采集的储存预诊断样本。在涉及每个受试者单个样本的分析中,sCD27 和 sCD30 均与 20 年后诊断出的 NHL 相关。在涉及重复样本的分析中,与 CLUE-I 样本相比,CLUE-II 样本中 sCD27 分析物水平较高的病例显著多于对照(p=0.006),但 sCD30 则不然(p=0.16)。在对两个样本中分析物水平进行二分类的联合分析中,sCD27 与 NHL 相关性最强的是在 CLUE-I 中低于中位数水平而在 CLUE-II 中高于中位数水平[比值比(OR)3.6,95%置信区间(CI)1.4-9.2 与在两个样本中均低于中位数水平相比]。在 sCD30 的联合分析中,与 NHL 相关性最强的是在两个样本中均处于中位数以上水平(OR 1.7,95%CI 0.8-3.7),尤其是在 CLUE-II 样本采集后 10 年以上诊断出的病例(OR 2.4,95%CI 0.9-6.7)。我们的研究结果表明 sCD27 是非霍奇金淋巴瘤的疾病标志物,并进一步增加了证据表明循环 sCD30 升高是非霍奇金淋巴瘤易感性增加的标志物。

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