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Nanowire array chips for molecular typing of rare trafficking leukocytes with application to neurodegenerative pathology

机译:纳米线阵列芯片的分子类型罕见贩卖白细胞与应用程序退行性神经病理学

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Despite the presence of the blood-brain barrier (BBB) that restricts the entry of immune cells and mediators into the central nervous system (CNS), a small number of peripheral leukocytes can traverse the BBB and infiltrate into the CNS. The cerebrospinal fluid (CSF) is one of the major routes through which trafficking leukocytes migrate into the CNS. Therefore, the number of leukocytes and their phenotypic compositions in the CSF may represent important sources to investigate immune-to-brain interactions or diagnose and monitor neurodegenerative diseases. Due to the paucity of trafficking leucocytes in the CSF, a technology capable of efficient isolation, enumeration, and molecular typing of these cells in the clinical settings has not been achieved. In this study, we report on a biofunctionalized silicon nanowire array chip for highly efficient capture and multiplexed phenotyping of rare trafficking leukocytes in small quantities (50 microliters) of clinical CSF specimens collected from neurodegenerative disease patients. The antibody coated 3D nanostructured materials exhibited vastly improved rare cell capture efficiency due to high-affinity binding and enhanced cell-substrate interactions. Moreover, our platform creates multiple cell capture interfaces, each of which can selectively isolate specific leukocyte phenotypes. A comparison with the traditional immunophenotyping using flow cytometry demonstrated that our novel silicon nanowire-based rare cell analysis platform can perform rapid detection and simultaneous molecular characterization of heterogeneous immune cells. Multiplexed molecular typing of rare leukocytes in CSF samples collected from Alzheimer's disease patients revealed the elevation of white blood cell counts and significant alterations in the distribution of major leukocyte phenotypes. Our technology represents a practical tool for potentially diagnosing and monitoring the pathogenesis of neurodegenerative diseases by allowing an effective hematological analysis of the CSF from patients.
机译:尽管血脑屏障的存在(BBB)限制了免疫细胞的条目和介质进入中枢神经系统(中枢神经系统),少量的外围白细胞可以遍历BBB和渗透到中枢神经系统。脑脊液(CSF)是主要的贩卖白细胞路线迁移到中枢神经系统。白细胞及其表型成分CSF可能代表的重要来源调查immune-to-brain交互或诊断和监测神经退行性疾病。由于缺乏贩卖白细胞CSF,技术效率的能力隔离、枚举和分子类型的没有这些细胞在临床设置实现。biofunctionalized硅纳米线阵列芯片高效的捕获和多路复用表型出现罕见的贩卖白细胞少量临床脑脊液(50毫升)标本收集的神经退行性疾病的病人。纳米材料表现出极大的由于提高稀有细胞捕获效率高亲和性结合和增强的细胞基质交互。多个细胞捕获接口,每个可以选择性地分离特定的白细胞吗表型。immunophenotyping使用流式细胞仪证明我们的小说硅nanowire-based稀有细胞分析平台执行快速检测和同步分子特性的异构免疫细胞。罕见的白细胞的脑脊液样本收集阿尔茨海默氏症病人了白细胞计数和海拔发生重大变化的分布主要的白细胞表型。代表了一种潜在的实用工具诊断和监测的发病机制通过允许一个神经退行性疾病有效的CSF的血液分析病人。

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