Bang Oh Young, Kim Eun Hee, Oh Mi Jeong, Yoo Jaein, Oh Gyun Sik, Chung Jong-Won, Seo Woo-Keun, Kim Gyeong-Moon, Ahn Myung-Ju, Yang Seong Wook
Department of Neurology, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea.
S&E bio Co., Ltd., Seoul, Korea.
J Stroke. 2023 May;25(2):251-265. doi: 10.5853/jos.2022.02327. Epub 2023 May 2.
This study aimed to evaluate whether extracellular-vesicle-incorporated microRNAs (miRNAs) are potential biomarkers for cancer-related stroke.
This cohort study compared patients with active cancer who had embolic stroke of unknown sources (cancer-stroke group) with patients with only cancer, patients with only stroke, and healthy individuals (control groups). The expression profiles of miRNAs encapsulated in plasma exosomes and microvesicles were evaluated using microarray and validated using quantitative real-time polymerase chain reaction. The XENO-QTM miRNA assay technology was used to determine the absolute copy numbers of individual miRNAs in an external validation cohort.
This study recruited 220 patients, of which 45 had cancer-stroke, 76 were healthy controls, 39 were cancer controls, and 60 were stroke controls. Three miRNAs (miR-205-5p, miR-645, and miR-646) were specifically incorporated into microvesicles in patients with cancer-related stroke, cancer controls, and stroke controls. The area under the receiver operating characteristic curves of these three miRNAs were 0.7692-0.8510 for the differentiation of patients with cancer-stroke from cancer-controls and 0.8077-0.8846 for the differentiation of patients with cancer-stroke from stroke controls. The levels of several miRNAs were elevated in the plasma exosomes of patients with cancer, but were lower than those in plasma microvesicles. An in vivo study showed that systemic injection of miR-205-5p promoted the development of arterial thrombosis and elevation of D-dimer levels.
Stroke due to cancer-related coagulopathy was associated with deregulated expression of miRNAs, particularly microvesicle-incorporated miR-205-5p, miR-645, and miR-646. Further prospective studies of extracellular-vesicle-incorporated miRNAs are required to confirm the diagnostic role of miRNAs in patients with stroke and to screen the roles of miRNAs in patients with cancer.
本研究旨在评估细胞外囊泡包裹的微小RNA(miRNA)是否为癌症相关性卒中的潜在生物标志物。
本队列研究将患有不明来源栓塞性卒中的活动性癌症患者(癌症-卒中组)与仅患有癌症的患者、仅患有卒中的患者以及健康个体(对照组)进行比较。使用微阵列评估血浆外泌体和微囊泡中包裹的miRNA的表达谱,并使用定量实时聚合酶链反应进行验证。采用XENO-QTM miRNA检测技术确定外部验证队列中单个miRNA的绝对拷贝数。
本研究招募了220例患者,其中45例患有癌症-卒中,76例为健康对照,39例为癌症对照,60例为卒中对照。三种miRNA(miR-205-5p、miR-645和miR-646)特异性地包裹在癌症相关性卒中患者、癌症对照和卒中对照的微囊泡中。这三种miRNA的受试者工作特征曲线下面积在区分癌症-卒中患者与癌症对照时为0.7692 - 0.8510,在区分癌症-卒中患者与卒中对照时为0.8077 - 0.8846。几种miRNA的水平在癌症患者的血浆外泌体中升高,但低于血浆微囊泡中的水平。一项体内研究表明,全身注射miR-205-5p可促进动脉血栓形成并使D-二聚体水平升高。
癌症相关性凝血病所致卒中与miRNA表达失调有关,尤其是包裹在微囊泡中的miR-205-5p、miR-645和miR-646。需要进一步对细胞外囊泡包裹的miRNA进行前瞻性研究,以确认miRNA在卒中患者中的诊断作用,并筛选miRNA在癌症患者中的作用。
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