ANKK1、TTC12 和 NCAM1 多态性与海洛因依赖:考虑药物暴露的重要性。

ANKK1, TTC12, and NCAM1 polymorphisms and heroin dependence: importance of considering drug exposure.

机构信息

Department of Psychiatry, Washington University School of Medicine, St Louis, Missouri 63110, USA.

出版信息

JAMA Psychiatry. 2013 Mar;70(3):325-33. doi: 10.1001/jamapsychiatry.2013.282.

Abstract

CONTEXT

The genetic contribution to liability for opioid dependence is well established; identification of the responsible genes has proved challenging.

OBJECTIVE

To examine association of 1430 candidate gene single-nucleotide polymorphisms (SNPs) with heroin dependence, reporting here only the 71 SNPs in the chromosome 11 gene cluster (NCAM1, TTC12, ANKK1, DRD2) that include the strongest observed associations.

DESIGN

Case-control genetic association study that included 2 control groups (lacking an established optimal control group).

SETTING

Semistructured psychiatric interviews.

PARTICIPANTS

A total of 1459 Australian cases ascertained from opioid replacement therapy clinics, 531 neighborhood controls ascertained from economically disadvantaged areas near opioid replacement therapy clinics, and 1495 unrelated Australian Twin Registry controls not dependent on alcohol or illicit drugs selected from a twin and family sample.

MAIN OUTCOME MEASURE

Lifetime heroin dependence.

RESULTS

Comparison of cases with Australian Twin Registry controls found minimal evidence of association for all chromosome 11 cluster SNPs (P ≥ .01); a similar comparison with neighborhood controls revealed greater differences (P ≥ 1.8 × 10(-4)). Comparing cases (n = 1459) with the subgroup of neighborhood controls not dependent on illicit drugs (n = 340), 3 SNPs were significantly associated (correcting for multiple testing): ANKK1 SNP rs877138 (most strongly associated; odds ratio = 1.59; 95% CI, 1.32-1.92; P = 9.7 × 10(-7)), ANKK1 SNP rs4938013, and TTC12 SNP rs7130431. A similar pattern of association was observed when comparing illicit drug-dependent (n = 191) and nondependent (n = 340) neighborhood controls, suggesting that liability likely extends to nonopioid illicit drug dependence. Aggregate heroin dependence risk associated with 2 SNPs, rs877138 and rs4492854 (located in NCAM1), varied more than 4-fold (P = 2.7 × 10(-9) for the risk-associated linear trend).

CONCLUSIONS

Our results provide further evidence of association for chromosome 11 gene cluster SNPs with substance dependence, including extension of liability to illicit drug dependence. Our findings highlight the necessity of considering drug exposure history when selecting control groups for genetic investigations of illicit drug dependence.

摘要

背景

阿片类药物依赖的遗传易感性已得到充分证实;但鉴定相关基因具有挑战性。

目的

本研究旨在检测 1430 个候选基因单核苷酸多态性(SNP)与海洛因依赖的相关性,此处仅报告染色体 11 基因簇(NCAM1、TTC12、ANKK1、DRD2)中观察到的最强关联的 71 个 SNP。

设计

病例对照遗传关联研究,包含 2 个对照组(缺乏既定的最佳对照组)。

环境

半结构化精神科访谈。

参与者

共纳入 1459 名来自阿片类药物替代治疗诊所的澳大利亚病例、531 名来自阿片类药物替代治疗诊所附近经济贫困地区的邻里对照组,以及 1495 名来自澳大利亚双胞胎登记处的无关对照组,这些对照组未依赖酒精或非法药物,是从双胞胎和家庭样本中选择的。

主要观察指标

终生海洛因依赖。

结果

与澳大利亚双胞胎登记处对照组相比,所有染色体 11 簇 SNP 的比较均显示出最小的关联证据(P≥0.01);与邻里对照组的类似比较显示出更大的差异(P≥1.8×10(-4))。与病例(n=1459)相比,邻里对照组中不依赖非法药物的亚组(n=340),有 3 个 SNP 显著相关(校正多重检验):ANKK1 SNP rs877138(最强相关;优势比=1.59;95%CI,1.32-1.92;P=9.7×10(-7))、ANKK1 SNP rs4938013 和 TTC12 SNP rs7130431。当比较依赖和不依赖非法药物的邻里对照组(n=191 和 n=340)时,观察到类似的关联模式,表明易感性可能扩展到非阿片类非法药物依赖。与 2 个 SNP(位于 NCAM1 的 rs877138 和 rs4492854)相关的海洛因依赖总风险差异超过 4 倍(与风险相关的线性趋势的 P=2.7×10(-9))。

结论

我们的结果为染色体 11 基因簇 SNP 与物质依赖的相关性提供了进一步的证据,包括将易感性扩展到非法药物依赖。我们的研究结果强调了在选择遗传研究非法药物依赖的对照组时,需要考虑药物暴露史。

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