孟德尔随机化研究证实强迫症的遗传易感性与阿尔茨海默病的风险有关。

IF 2.6 3区 心理学 Q2 BEHAVIORAL SCIENCES Brain and Behavior Pub Date : 2024-09-30 DOI:10.1002/brb3.70081
Si Cao, Han Su, Xiaoyi Zhang, Chao Fang, Nayiyuan Wu, Youjie Zeng, Minghua Chen
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引用次数: 0

摘要

背景:观察性研究表明,强迫症(OCD)可能与阿尔茨海默病(AD)有关。然而,强迫症是否是阿尔茨海默病的因果风险因素仍不清楚。本研究旨在通过进行双样本孟德尔随机化(MR)分析,评估强迫症对阿尔茨海默病风险的因果效应:获得了强迫症(包括 2688 例病例和 7037 例对照)和 AD 的全基因组关联汇总统计数据,包括 Kunkle 等人研究中的 21,982 例病例和 41,944 例对照,以及 Wightman 等人研究中的 39,918 例病例和 358,140 例对照。根据两种不同的阈值,强迫症相关遗传变异被筛选为工具变量(IV),用于后续的 MR 分析。反方差权衡是主要的 MR 方法。MR-Egger、加权中位数和加权模式被用作辅助MR方法。各种敏感性测试评估了 MR 结果的可靠性:在严格的 IV 选择阈值的基础上,反方差加权法(IVW)在两个不同的来源中发现了强迫症遗传责任与 AD 风险增加之间的显著因果关系((i) Kunkle 等人:几率比 [OR] = 1.070,95% 置信区间 [CI]:1.015-1.127, p = 0.012;(ii) Wightman et al:OR = 1.051,95% CI:1.014-1.090,p = 0.007)。其他三种辅助 MR 方法的结果与 IVWs 相似(OR > 1)。此外,所有结果都在基于宽松的 IV 选择阈值的 MR 分析中得到了重复。敏感性测试表明,MR 结果稳定,不受显著水平多效性的影响:这项全面的磁共振研究表明,强迫症的遗传易感性是导致注意力缺失症的一个因果风险因素。对强迫症患者进行早期干预可能有利于预防未来的注意力缺失症进展。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Mendelian Randomization Study Supports Genetic Liability to Obsessive–Compulsive Disorder Associated With the Risk of Alzheimer's Disease

Background

Observational studies have suggested that obsessive–compulsive disorder (OCD) may be associated with Alzheimer's disease (AD). However, whether OCD is a causal risk factor for AD remains unclear. This study aimed to assess the causal effect of OCD on AD risk by performing a two-sample Mendelian randomization (MR) analysis.

Methods

Genome-wide association summary statistics were obtained for OCD, comprising 2688 cases and 7037 controls, as well as for AD, including 21,982 cases and 41,944 controls from Kunkle et al.’s study, and 39,918 cases and 358,140 controls from Wightman et al.’s study. On the basis of two diverse thresholds, OCD-associated genetic variants were screened as instrumental variables (IVs) for subsequent MR analyses. Inverse variance weighed was the primary MR method. MR-Egger, weighted median, and weighted mode were used as supplementary MR methods. Various sensitivity tests assessed the reliability of MR results.

Results

On the basis of strict IV selecting thresholds, inverse-variance weighted (IVW) identified significant causal associations between genetic liability to OCD and increased risk of AD in two different sources ((i) Kunkle et al.: odds ratio [OR] = 1.070, 95% confidence interval [CI]: 1.015–1.127, p = 0.012; (ii) Wightman et al. 0.012; (iii) Wightman et al.: OR = 1.051, 95% CI: 1.014–1.090, p = 0.007). Three other supplementary MR methods yielded similar results to IVWs (OR > 1). Furthermore, all results were replicated in MR analyses based on lenient IV selecting thresholds. The sensitivity tests indicated that MR results were stable and not affected by significant horizontal pleiotropy.

Conclusions

This comprehensive MR study suggests that genetic liability to OCD is a causal risk factor for AD. Early intervention in patients with OCD may be beneficial in preventing future AD progression.

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来源期刊
Brain and Behavior
Brain and Behavior BEHAVIORAL SCIENCES-NEUROSCIENCES
CiteScore
5.30
自引率
0.00%
发文量
352
审稿时长
14 weeks
期刊介绍: Brain and Behavior is supported by other journals published by Wiley, including a number of society-owned journals. The journals listed below support Brain and Behavior and participate in the Manuscript Transfer Program by referring articles of suitable quality and offering authors the option to have their paper, with any peer review reports, automatically transferred to Brain and Behavior. * [Acta Psychiatrica Scandinavica](https://publons.com/journal/1366/acta-psychiatrica-scandinavica) * [Addiction Biology](https://publons.com/journal/1523/addiction-biology) * [Aggressive Behavior](https://publons.com/journal/3611/aggressive-behavior) * [Brain Pathology](https://publons.com/journal/1787/brain-pathology) * [Child: Care, Health and Development](https://publons.com/journal/6111/child-care-health-and-development) * [Criminal Behaviour and Mental Health](https://publons.com/journal/3839/criminal-behaviour-and-mental-health) * [Depression and Anxiety](https://publons.com/journal/1528/depression-and-anxiety) * Developmental Neurobiology * [Developmental Science](https://publons.com/journal/1069/developmental-science) * [European Journal of Neuroscience](https://publons.com/journal/1441/european-journal-of-neuroscience) * [Genes, Brain and Behavior](https://publons.com/journal/1635/genes-brain-and-behavior) * [GLIA](https://publons.com/journal/1287/glia) * [Hippocampus](https://publons.com/journal/1056/hippocampus) * [Human Brain Mapping](https://publons.com/journal/500/human-brain-mapping) * [Journal for the Theory of Social Behaviour](https://publons.com/journal/7330/journal-for-the-theory-of-social-behaviour) * [Journal of Comparative Neurology](https://publons.com/journal/1306/journal-of-comparative-neurology) * [Journal of Neuroimaging](https://publons.com/journal/6379/journal-of-neuroimaging) * [Journal of Neuroscience Research](https://publons.com/journal/2778/journal-of-neuroscience-research) * [Journal of Organizational Behavior](https://publons.com/journal/1123/journal-of-organizational-behavior) * [Journal of the Peripheral Nervous System](https://publons.com/journal/3929/journal-of-the-peripheral-nervous-system) * [Muscle & Nerve](https://publons.com/journal/4448/muscle-and-nerve) * [Neural Pathology and Applied Neurobiology](https://publons.com/journal/2401/neuropathology-and-applied-neurobiology)
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