Systematic Genetic Assessment in Young Patients With Cryptogenic Stroke: The ES-EASY project.

IF 8.9 1区医学 Q1 CLINICAL NEUROLOGY

Stroke Pub Date : 2025-09-19 DOI:10.1161/STROKEAHA.125.051020

Loraine Mania-Pâris, Antonio Vitobello, Hana Safraou, Frédéric Tran Mau-Them, Yannis Duffourd, Sophie Nambot, Ange-Line Bruel, Anne-Sophie Denommé-Pichon, Gauthier Duloquin, Yannick Béjot, Laurence Faivre, Christel Thauvin-Robinet, Quentin Thomas

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引用次数: 0

Abstract

Background: Up to 15% of strokes occur in young adults, with more cryptogenic cases, raising the possibility of rare causes, such as genetic diseases. Although available in everyday practice, genetic analyses are usually reserved for patients with evocative personal or family history. We aimed to assess the interest of systematic genetic analyses in young adults with cryptogenic stroke and estimate the true frequency of genetic disorders in such patients.

Methods: We conducted a retrospective observational cohort study with additional prospective genetic testing. We screened all patients under 50 admitted to Dijon University Hospital stroke unit between 2018 and 2021. Those already genetically tested during etiological work-up were included in a first cohort (cohort 1). Among the remaining patients, those with unexplained intracerebral hemorrhage or stroke (ie, cryptogenic stroke), or a stroke subtype known to have monogenic forms, were offered exome sequencing to form cohort 2. Monogenic diagnoses were defined by likely pathogenic/pathogenic variants according to American College of Medical Genetics and Genomics criteria.

Results: Among 305 patients with stroke screened, 24 had prior genetic testing (cohort 1) with exome sequencing, genome sequencing, gene panels or targeted gene analyses, leading to a molecular diagnosis in 8 (33%). Of the remaining 281 patients, 71 met eligibility criteria and 35 consented to the study (cohort 2). Exome sequencing identified pathogenic variants in 4 of them (11%). The overall diagnostic yield of genetic tests was 20.3% (12/59 patients tested across both cohorts). In total, monogenic causes explained 3.9% (12/305) of all young stroke cases. Notably, most diagnosed patients (66%) had no family history of stroke. Genetic cardiopathies and conditions conferring increased cardiovascular risk factors accounted for 50% of diagnoses.

Conclusions: Genetic analyses should be considered in all unexplained strokes or in stroke subtypes with known genetic forms (eg, Moya Moya syndrome, cardiopathy, small vessel disease), even without an evocative family history.

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年轻隐源性脑卒中患者的系统遗传评估：ES-EASY项目。

背景：高达15%的中风发生在年轻人中，有更多的隐源性病例，增加了罕见原因的可能性，如遗传疾病。虽然在日常实践中可用，遗传分析通常保留给有唤起个人或家族史的患者。我们的目的是评估系统遗传分析对年轻成人隐源性卒中的兴趣，并估计遗传疾病在这些患者中的真实频率。方法：我们进行了一项回顾性观察队列研究，并进行了额外的前瞻性基因检测。我们筛选了2018年至2021年间第戎大学医院卒中病房收治的所有50岁以下患者。在病因检查期间已进行基因检测的患者被纳入第一组（队列1）。在剩余的患者中，那些不明原因的脑出血或中风（即隐源性中风），或已知有单基因形式的中风亚型，进行外显子组测序，形成队列2。单基因诊断是根据美国医学遗传学和基因组学学院的标准，通过可能的致病/致病变异来定义的。结果：在305例卒中筛查患者中，24例进行了基因检测（队列1），包括外显子组测序、基因组测序、基因面板或靶向基因分析，其中8例（33%）进行了分子诊断。在剩余的281例患者中，71例符合资格标准，35例同意研究（队列2）。外显子组测序发现其中4例（11%）存在致病性变异。基因检测的总体诊断率为20.3%（在两个队列中检测的59例患者中有12例）。在所有青少年脑卒中病例中，单基因原因占3.9%（12/305）。值得注意的是，大多数确诊患者（66%）没有中风家族史。遗传性心脏病和导致心血管危险因素增加的疾病占诊断的50%。结论：对于所有不明原因的中风或已知遗传形式的中风亚型（如Moya Moya综合征、心脏病、小血管疾病），即使没有令人联想的家族史，也应考虑进行遗传分析。

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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来源期刊

Stroke 医学-临床神经学

CiteScore

13.40

自引率

6.00%

发文量

2021

审稿时长

3 months

期刊介绍： Stroke is a monthly publication that collates reports of clinical and basic investigation of any aspect of the cerebral circulation and its diseases. The publication covers a wide range of disciplines including anesthesiology, critical care medicine, epidemiology, internal medicine, neurology, neuro-ophthalmology, neuropathology, neuropsychology, neurosurgery, nuclear medicine, nursing, radiology, rehabilitation, speech pathology, vascular physiology, and vascular surgery. The audience of Stroke includes neurologists, basic scientists, cardiologists, vascular surgeons, internists, interventionalists, neurosurgeons, nurses, and physiatrists. Stroke is indexed in Biological Abstracts, BIOSIS, CAB Abstracts, Chemical Abstracts, CINAHL, Current Contents, Embase, MEDLINE, and Science Citation Index Expanded.