Isolated anterior cerebral artery occlusion: an atypical form of moyamoya disease.

IF 2.6 1区 医学
Si-Meng Liu, Gan Gao, Fang-Bin Hao, Shi-Tong Liu, Ri-Miao Yang, Hou-di Zhang, Min-Jie Wang, Zheng-Xing Zou, Dan Yu, Qian Zhang, Qing-Bao Guo, Xiao-Peng Wang, He-Guan Fu, Jing-Jie Li, Cong Han, Lian Duan
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引用次数: 0

Abstract

Background: The relationship between anterior cerebral artery (ACA) occlusion and moyamoya disease (MMD) has rarely been studied. In this study, we focused on a special type of MMD: isolated ACA-occlusive MMD. We investigated clinical attributes, genotypes and progression risk factors in patients with ACA-occlusive MMD, providing initial insights into the relationship between ACA occlusion and MMD.

Methods: We retrospectively analysed digital subtraction angiography (DSA) from 2486 patients and diagnosed 139 patients with ACA-occlusive MMD. RNF213 p.R4810K (rs112735431) mutation analysis was performed. Patients were categorised into progression and non-progression groups based on whether they progressed to typical MMD. Differences in clinical characteristics, neuropsychological assessment, radiological findings and genotypes were evaluated. Logistic regression analyses identified risk factors for ACA-occlusive MMD progression.

Results: The median age of patients with ACA-occlusive MMD was 36 years, and the primary symptom was transient ischaemic attack (TIA). 72.3% of ACA-occlusive MMD patients had cognitive decline. Of 116 patients who underwent RNF213 gene mutation analysis, 90 patients (77.6%) carried the RNF213 p.R4810K GG allele and 26 (22.4%) carried the GA allele. Of 102 patients with follow-up DSA data, 40 patients (39.2%) progressed. Kaplan-Meier curve estimates indicated a higher incidence of ischaemic stroke in the progression group during follow-up (p=0.035). Younger age (p=0.041), RNF213 p.R4810K GA genotype (p=0.037) and poor collateral compensation from the middle cerebral artery (MCA) to ACA (p<0.001) were risk factors of ACA-occlusive MMD progression to typical MMD.

Conclusions: Cognitive decline and TIA might be the main manifestations of ACA-occlusive MMD. Isolated ACA occlusion may be an early signal of MMD. The initial lesion site of MMD is not strictly confined to the terminal portion of the internal carotid artery. Younger patients, patients with RNF213 p.R4810K GA genotype or those with inadequate MCA-to-ACA compensation are more likely to develop typical MMD.

孤立性大脑前动脉闭塞:一种非典型的莫亚莫亚病。
背景:大脑前动脉(ACA)闭塞与莫亚莫亚氏病(MMD)之间的关系很少被研究。在本研究中,我们重点研究了一种特殊类型的 MMD:孤立的 ACA 闭塞性 MMD。我们调查了ACA闭塞性MMD患者的临床属性、基因型和进展风险因素,为了解ACA闭塞与MMD之间的关系提供了初步见解:我们回顾性分析了 2486 例患者的数字减影血管造影(DSA),诊断出 139 例 ACA 闭塞性 MMD 患者。我们对 RNF213 p.R4810K (rs112735431) 基因突变进行了分析。根据患者是否发展为典型的MMD,将其分为进展组和非进展组。对临床特征、神经心理学评估、放射学结果和基因型的差异进行了评估。逻辑回归分析确定了ACA闭塞性多发性硬化症进展的风险因素:结果:ACA-闭塞性多发性硬化症患者的中位年龄为36岁,主要症状为短暂性脑缺血发作(TIA)。72.3%的ACA-闭塞性多发性硬化症患者认知能力下降。在接受RNF213基因突变分析的116名患者中,90名患者(77.6%)携带RNF213 p.R4810K GG等位基因,26名患者(22.4%)携带GA等位基因。在102名有随访DSA数据的患者中,有40名患者(39.2%)病情恶化。Kaplan-Meier 曲线估计结果显示,随访期间进展组缺血性中风的发生率更高(P=0.035)。年龄较小(p=0.041)、RNF213 p.R4810K GA 基因型(p=0.037)和大脑中动脉(MCA)至 ACA 的侧支补偿较差(pConclusions):认知能力下降和 TIA 可能是 ACA 闭塞性 MMD 的主要表现。孤立的 ACA 闭塞可能是 MMD 的早期信号。多发性硬化症的初始病变部位并不严格局限于颈内动脉末端。年轻患者、RNF213 p.R4810K GA 基因型患者或 MCA 对 ACA 补偿不足的患者更有可能发展为典型的 MMD。
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来源期刊
Journal of Investigative Medicine
Journal of Investigative Medicine MEDICINE, GENERAL & INTERNALMEDICINE, RESE-MEDICINE, RESEARCH & EXPERIMENTAL
自引率
0.00%
发文量
111
期刊介绍: Journal of Investigative Medicine (JIM) is the official publication of the American Federation for Medical Research. The journal is peer-reviewed and publishes high-quality original articles and reviews in the areas of basic, clinical, and translational medical research. JIM publishes on all topics and specialty areas that are critical to the conduct of the entire spectrum of biomedical research: from the translation of clinical observations at the bedside, to basic and animal research to clinical research and the implementation of innovative medical care.
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