RNF213 Mutation Associated with the Progression from Middle Cerebral Artery Steno-Occlusive Disease to Moyamoya Disease.

IF 3.8 2区 医学 Q1 CLINICAL NEUROLOGY
Tomoki Sasagasako, Yohei Mineharu, Takeshi Funaki, Yasutaka Fushimi, Hideo Chihara, Silsu Park, Kota Nakajima, Yasuzumi Matsui, Masakazu Okawa, Takayuki Kikuchi, Yoshiki Arakawa
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Abstract

Middle cerebral artery steno-occlusive disease (MCAD) has been recognized as a different clinical entity from moyamoya disease (MMD). Although MCAD can progress to MMD, the extent to which patients actually progress and the risk factors for this progression have not been fully elucidated. We retrospectively reviewed patients with MCAD who underwent RNF213 genotyping. Demographic features, RNF213 p.R4810K mutation, medical history, and longitudinal changes in angiography were analyzed. Sixty patients with 81 affected hemispheres were enrolled. During the follow-up period, 17 patients developed MMD, and the RNF213 p.R4810K mutation was the only factor significantly associated with progression to MMD (odds ratio, 16.1; 95% CI, 2.13-731; P = 0.001). The log-rank test demonstrated that patients with the mutation had a higher risk of progression to MMD (P = 0.007), stenosis progression (P = 0.010), and symptomatic cerebral infarction or hemorrhage (P = 0.026). In Cox regression analysis the p.R4810K mutation remained a significant factor after adjusting for age group (childhood or adult onset) at diagnosis (hazard ratio, 8.42; 95% CI, 1.10-64.4). Hemisphere-based analysis also showed that the mutation was associated with a higher risk of progression to the MMD hemisphere (P = 0.002), stenosis progression (P = 0.005), and cerebral infarction or hemorrhage (P = 0.012). The RNF213 p.R4810K mutation was identified as a risk factor for progression from MCAD to MMD. Genotyping for this mutation may contribute to risk stratification in MCAD.

Abstract Image

RNF213 基因突变与大脑中动脉狭窄性闭塞症发展为莫亚莫亚病有关
大脑中动脉狭窄闭塞症(MCAD)已被认为是一种不同于莫亚莫亚病(MMD)的临床实体。虽然 MCAD 可发展为 MMD,但患者实际发展的程度以及发展的风险因素尚未完全阐明。我们对接受了 RNF213 基因分型的 MCAD 患者进行了回顾性研究。我们分析了人口学特征、RNF213 p.R4810K突变、病史和血管造影的纵向变化。共纳入了 60 名患者,81 个受影响的半球。在随访期间,17 名患者发展为 MMD,而 RNF213 p.R4810K 突变是唯一与发展为 MMD 显著相关的因素(几率比,16.1;95% CI,2.13-731;P = 0.001)。对数秩检验表明,突变患者进展为 MMD(P = 0.007)、血管狭窄进展(P = 0.010)和无症状脑梗死或出血(P = 0.026)的风险较高。在Cox回归分析中,p.R4810K突变在调整诊断时的年龄组(儿童或成人发病)后仍是一个重要因素(危险比,8.42;95% CI,1.10-64.4)。基于半球的分析还显示,突变与MMD半球进展(P = 0.002)、狭窄进展(P = 0.005)、脑梗塞或出血(P = 0.012)的风险较高有关。RNF213 p.R4810K突变被确定为从MCAD发展为MMD的风险因素。对该基因突变进行基因分型可能有助于对MCAD进行风险分层。
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来源期刊
Translational Stroke Research
Translational Stroke Research CLINICAL NEUROLOGY-NEUROSCIENCES
CiteScore
13.80
自引率
4.30%
发文量
130
审稿时长
6-12 weeks
期刊介绍: Translational Stroke Research covers basic, translational, and clinical studies. The Journal emphasizes novel approaches to help both to understand clinical phenomenon through basic science tools, and to translate basic science discoveries into the development of new strategies for the prevention, assessment, treatment, and enhancement of central nervous system repair after stroke and other forms of neurotrauma. Translational Stroke Research focuses on translational research and is relevant to both basic scientists and physicians, including but not restricted to neuroscientists, vascular biologists, neurologists, neuroimagers, and neurosurgeons.
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