Causal relationships of grey matter structures in multiple sclerosis and neuromyelitis optica spectrum disorder: insights from Mendelian randomization.

IF 4.1 Q1 CLINICAL NEUROLOGY
Brain communications Pub Date : 2024-09-11 eCollection Date: 2024-01-01 DOI:10.1093/braincomms/fcae308
Jie Sun, Yingying Xie, Tongli Li, Yunfei Zhao, Wenjin Zhao, Zeyang Yu, Shaoying Wang, Yujie Zhang, Hui Xue, Yayuan Chen, Zuhao Sun, Zhang Zhang, Yaou Liu, Ningnannan Zhang, Feng Liu
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Abstract

Multiple sclerosis and neuromyelitis optica spectrum disorder are two debilitating inflammatory demyelinating diseases of the CNS. Although grey matter alterations have been linked to both multiple sclerosis and neuromyelitis optica spectrum disorder in observational studies, it is unclear whether these associations indicate causal relationships between these diseases and grey matter changes. Therefore, we conducted a bidirectional two-sample Mendelian randomization analysis to investigate the causal relationships between 202 grey matter imaging-derived phenotypes (33 224 individuals) and multiple sclerosis (47 429 cases and 68 374 controls) as well as neuromyelitis optica spectrum disorder (215 cases and 1244 controls). Our results suggested that genetically predicted multiple sclerosis was positively associated with the surface area of the left parahippocampal gyrus (β = 0.018, P = 2.383 × 10-4) and negatively associated with the volumes of the bilateral caudate (left: β = -0.020, P = 7.203 × 10-5; right: β = -0.021, P = 3.274 × 10-5) and putamen nuclei (left: β = -0.030, P = 2.175 × 10-8; right: β = -0.024, P = 1.047 × 10-5). In addition, increased neuromyelitis optica spectrum disorder risk was associated with an increased surface area of the left paracentral gyrus (β = 0.023, P = 1.025 × 10-4). Conversely, no evidence was found for the causal impact of grey matter imaging-derived phenotypes on disease risk in the opposite direction. We provide suggestive evidence that genetically predicted multiple sclerosis and neuromyelitis optica spectrum disorder are associated with increased cortical surface area and decreased subcortical volume in specific regions. Our findings shed light on the associations of grey matter alterations with the risk of multiple sclerosis and neuromyelitis optica spectrum disorder.

多发性硬化症和神经性脊髓炎视谱系障碍中灰质结构的因果关系:孟德尔随机化的启示。
多发性硬化症和神经脊髓炎视谱系障碍是中枢神经系统的两种致残性炎症性脱髓鞘疾病。尽管在观察性研究中,灰质改变与多发性硬化症和神经脊髓炎视谱系障碍都有关联,但这些关联是否表明这些疾病与灰质改变之间存在因果关系,目前尚不清楚。因此,我们进行了双向双样本孟德尔随机分析,研究 202 种灰质成像衍生表型(33 224 人)与多发性硬化症(47 429 例和 68 374 例对照)以及神经脊髓炎视光学频谱障碍(215 例和 1244 例对照)之间的因果关系。我们的结果表明,遗传预测的多发性硬化与左侧海马旁回的表面积呈正相关(β = 0.018,P = 2.383 × 10-4),而与双侧尾状核(左侧:β = -0.020,P = 7.203 × 10-5;右侧:β = -0.021,P = 3.274 × 10-5)和普鲁门核(左侧:β = -0.030,P = 2.175 × 10-8;右侧:β = -0.024,P = 1.047 × 10-5)的体积呈负相关。此外,神经脊髓炎视谱系障碍风险的增加与左侧中央旁回表面积的增加有关(β = 0.023,P = 1.025 × 10-4)。相反,没有证据表明灰质成像表型对疾病风险有相反方向的因果影响。我们提供的提示性证据表明,基因预测的多发性硬化症和神经脊髓炎视网膜频谱障碍与特定区域皮质表面积增加和皮质下体积减少有关。我们的研究结果揭示了灰质改变与多发性硬化症和神经脊髓炎视神经频谱障碍风险之间的关联。
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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CiteScore
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