Clinicoradiologic Criteria for the Diagnosis of Stroke-like Episodes in MELAS.

IF 3 3区医学 Q2 CLINICAL NEUROLOGY Neurology-Genetics Pub Date : 2023-08-01 DOI:10.1212/NXG.0000000000200082

Vadim Khasminsky, Eitan Auriel, Judith Luckman, Ruth Eliahou, Edna Inbar, Keshet Pardo, Yuval Landau, Rani Barnea, Maor Mermelstein, Shahar Shelly, Jonathan Naftali, Shlomi Peretz

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Abstract

Background and objectives: Stroke-like episodes (SLEs) in patients with mitochondrial encephalomyopathy, lactic acidosis, and stroke-like episodes (MELAS) syndrome are often misdiagnosed as acute ischemic stroke (AIS). We aimed to determine unique clinical and neuroimaging features for SLEs and formulate diagnostic criteria.

Methods: We retrospectively identified patients with MELAS admitted for SLEs between January 2012 and December 2021. Clinical features and imaging findings were compared with a cohort of patients who presented with AIS and similar lesion topography. A set of criteria was formulated and then tested by a blinded rater to evaluate diagnostic performance.

Results: Eleven MELAS patients with 17 SLE and 21 AISs were included. Patients with SLEs were younger (median 45 [37-60] vs 77 [68-82] years, p < 0.01) and had a lower body mass index (18 ± 2.6 vs 29 ± 4, p < 0.01), more commonly reported hearing loss (91% vs 5%, p < 0.01), and more commonly presented with headache and/or seizures (41% vs 0%, p < 0.01). The earliest neuroimaging test performed at presentation was uniformly a noncontrast CT. Two main patterns of lesion topography with a stereotypical spatiotemporal evolution were identified-an anterior pattern (7/21, 41%) starting at the temporal operculum and spreading to the peripheral frontal cortex and a posterior pattern (10/21, 59%) starting at the cuneus/precuneus and spreading to the lateral occipital and parietal cortex. Other distinguishing features for SLEs vs AIS were cerebellar atrophy (91% vs 19%, p < 0.01), previous cortical lesions with typical SLE distribution (46% vs 9%, p = 0.03), acute lesion tissue hyperemia and venous engorgement on CT angiography (CTA) (45% vs 0%, p < 0.01), and no large vessel occlusion on CTA (0% vs 100%, p < 0.01). Based on these clinicoradiologic features, a set of diagnostic criteria were constructed for possible SLE (sensitivity 100%, specificity 81%, AUC 0.905) and probable SLE (sensitivity 88%, specificity 95%, AUC 0.917).

Discussion: Clinicoradiologic criteria based on simple anamnesis and a CT scan at presentation can accurately diagnose SLE and lead to early administration of appropriate therapy.

Classification of evidence: This study provides Class III evidence that an algorithm using clinical and imaging features can differentiate stroke-like episodes due to MELAS from acute ischemic strokes.

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MELAS卒中样发作的临床放射学诊断标准。

背景和目的:线粒体脑肌病、乳酸酸中毒和卒中样发作(MELAS)综合征患者的卒中样发作(SLEs)常被误诊为急性缺血性卒中(AIS)。我们的目的是确定独特的临床和神经影像学特征的SLEs和制定诊断标准。方法:回顾性分析2012年1月至2021年12月期间因SLEs入院的MELAS患者。将临床特征和影像学结果与一组表现为AIS和类似病变地形的患者进行比较。制定了一套标准，然后由盲法评分者进行测试，以评估诊断性能。结果:11例MELAS患者合并17例SLE和21例ais。SLEs患者较年轻(中位年龄为45岁[37-60]vs 77岁[68-82]，p < 0.01)，体重指数较低(18±2.6 vs 29±4,p < 0.01)，更常见的报告听力损失(91% vs 5%， p < 0.01)，更常见的表现为头痛和/或癫痫发作(41% vs 0%， p < 0.01)。在发病时进行的最早的神经影像学检查均为非对比CT。发现两种主要的病变形态具有典型的时空演化特征:从颞盖开始向外周额叶皮层扩散的前型(7/ 21,41 %)和从楔叶/楔前叶开始向外侧枕叶和顶叶皮层扩散的后型(10/ 21,59 %)。SLE与AIS的其他区别特征是小脑萎缩(91% vs 19%， p < 0.01)，既往皮质病变具有典型SLE分布(46% vs 9%， p = 0.03)，急性病变组织充血和CT血管造影(CTA)静脉充血(45% vs 0%， p < 0.01)， CTA无大血管闭塞(0% vs 100%， p < 0.01)。基于这些临床放射学特征，构建了一套可能SLE(敏感性100%，特异性81%，AUC 0.905)和可能SLE(敏感性88%，特异性95%，AUC 0.917)的诊断标准。讨论:基于简单记忆的临床放射学标准和表现时的CT扫描可以准确诊断SLE并导致早期给予适当治疗。证据分类:本研究提供了III类证据，表明一种基于临床和影像学特征的算法可以区分MELAS引起的卒中样发作和急性缺血性卒中。

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

Neurology-Genetics Medicine-Neurology (clinical)

CiteScore

6.30

自引率

3.20%

发文量

107

审稿时长

15 weeks

期刊介绍： Neurology: Genetics is an online open access journal publishing peer-reviewed reports in the field of neurogenetics. Original articles in all areas of neurogenetics will be published including rare and common genetic variation, genotype-phenotype correlations, outlier phenotypes as a result of mutations in known disease-genes, and genetic variations with a putative link to diseases. This will include studies reporting on genetic disease risk and pharmacogenomics. In addition, Neurology: Genetics will publish results of gene-based clinical trials (viral, ASO, etc.). Genetically engineered model systems are not a primary focus of Neurology: Genetics, but studies using model systems for treatment trials are welcome, including well-powered studies reporting negative results.