脑常染色体显性动脉病伴皮质下梗死和白质脑病中的骨髓源性祖细胞。
Bone marrow-derived progenitor cells in cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy.
机构信息
Department of Neurological and Psychiatric Sciences, Thrombosis Center, University of Florence, Florence, Italy.
出版信息
Stroke. 2010 Feb;41(2):218-23. doi: 10.1161/STROKEAHA.109.563726. Epub 2009 Dec 24.
BACKGROUND AND PURPOSE
Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL) is an inherited disease due to cerebral microangiopathy presenting with variable pictures, including stroke, progressive cognitive impairment, and disability. Mechanisms leading from vessel structural changes to parenchymal damage and eventually to clinical expression are not fully understood. Among pathogenic processes, endothelial dysfunction has been hypothesized. Endothelial progenitor cells and circulating progenitor cells (CPCs) derived from bone marrow participate in endothelium structure and function maintenance and contribute to ischemic area revascularization. No data are available about these cells in CADASIL. Our objective in this study was to evaluate endothelial progenitor cells and CPCs role in CADASIL.
METHODS
Twenty-nine patients with CADASIL and 29 sex- and age-matched control subjects were enrolled. Cells were measured in peripheral blood using flow cytometry. Endothelial progenitor cells were defined as positive for CD34/KDR, CD133/KDR, and CD34/CD133/KDR; and CPCs as positive for CD34, CD133, and CD34/CD133.
RESULTS
Endothelial progenitor cells were significantly lower in patients with CADASIL than in control subjects (CD34/KDR: 0.05 versus 0.1 cells/microL, P=0.005; CD133/KDR: 0.07 versus 0.1 cells/microL, P=0.006; CD34/CD133/KDR: 0.05 versus 0.1 cells/microL, P=0.001). The difference remained significant after adjusting for age, sex, and statin use. CPCs were not significantly lower in CADASIL, but patients with stroke or dementia had significantly reduced CPC levels than patients without (CD34: 1.68 versus 2.95 cells/microL, P=0.007; CD133: 1.40 versus 2.82 cells/microL, P=0.004; CD34/CD133: 1.44 versus 2.75 cells/microL, P=0.004). CPC levels significantly correlated with cognitive and motor performance measures.
CONCLUSIONS
We have documented an association between endothelial progenitor cells and CPCs and CADASIL, extending previous data about the presence of endothelial dysfunction in this disease and its potential role in modulating phenotype.
背景与目的
伴有皮质下梗死和白质脑病的常染色体显性脑动脉病(CADASIL)是一种遗传性疾病,由脑微血管病引起,表现为多种病变,包括中风、进行性认知障碍和残疾。导致血管结构变化导致实质损伤并最终导致临床表达的机制尚未完全了解。在致病过程中,内皮功能障碍已被假设。内皮祖细胞和源自骨髓的循环祖细胞(CPCs)参与内皮结构和功能的维持,并有助于缺血区的再血管化。关于 CADASIL 中这些细胞尚无数据。我们在这项研究中的目的是评估内皮祖细胞和 CPC 在 CADASIL 中的作用。
方法
纳入 29 例 CADASIL 患者和 29 名性别和年龄匹配的对照组。使用流式细胞术在外周血中测量细胞。内皮祖细胞被定义为 CD34/KDR、CD133/KDR 和 CD34/CD133/KDR 阳性;CPCs 被定义为 CD34、CD133 和 CD34/CD133 阳性。
结果
CADASIL 患者的内皮祖细胞明显低于对照组(CD34/KDR:0.05 与 0.1 细胞/微升,P=0.005;CD133/KDR:0.07 与 0.1 细胞/微升,P=0.006;CD34/CD133/KDR:0.05 与 0.1 细胞/微升,P=0.001)。调整年龄、性别和他汀类药物使用后,差异仍然显著。CADASIL 患者的 CPC 水平无明显降低,但有中风或痴呆的患者 CPC 水平明显低于无中风或痴呆的患者(CD34:1.68 与 2.95 细胞/微升,P=0.007;CD133:1.40 与 2.82 细胞/微升,P=0.004;CD34/CD133:1.44 与 2.75 细胞/微升,P=0.004)。CPC 水平与认知和运动表现测量值显著相关。
结论
我们记录了内皮祖细胞和 CPC 与 CADASIL 之间的关联,扩展了以前关于该疾病存在内皮功能障碍及其在调节表型中的潜在作用的研究数据。
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