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激光扫描细胞术:原理与应用——最新进展

Laser scanning cytometry: principles and applications-an update.

作者信息

Pozarowski Piotr, Holden Elena, Darzynkiewicz Zbigniew

机构信息

The Brander Cancer Research Institute, New York Medical College, Valhalla, NY, USA.

出版信息

Methods Mol Biol. 2013;931:187-212. doi: 10.1007/978-1-62703-056-4_11.

Abstract

Laser scanning cytometer (LSC) is the microscope-based cytofluorometer that offers a plethora of unique analytical capabilities, not provided by flow cytometry (FCM). This review describes attributes of LSC and covers its numerous applications derived from plentitude of the parameters that can be measured. Among many LSC applications the following are emphasized: (a) assessment of chromatin condensation to identify mitotic, apoptotic cells, or senescent cells; (b) detection of nuclear or mitochondrial translocation of critical factors such as NF-κB, p53, or Bax; (c) semi-automatic scoring of micronuclei in mutagenicity assays; (d) analysis of fluorescence in situ hybridization (FISH) and use of the FISH analysis attribute to measure other punctuate fluorescence patterns such as γH2AX foci or receptor clustering; (e) enumeration and morphometry of nucleoli and other cell organelles; (f) analysis of progeny of individual cells in clonogenicity assay; (g) cell immunophenotyping; (h) imaging, visual examination, or sequential analysis using different probes of the same cells upon their relocation; (i) in situ enzyme kinetics, drug uptake, and other time-resolved processes; (j) analysis of tissue section architecture using fluorescent and chromogenic probes; (k) application for hypocellular samples (needle aspirate, spinal fluid, etc.); and (l) other clinical applications. Advantages and limitations of LSC are discussed and compared with FCM.

摘要

激光扫描细胞仪(LSC)是一种基于显微镜的细胞荧光仪,具有大量独特的分析能力,而流式细胞仪(FCM)则不具备这些能力。本综述描述了LSC的特性,并涵盖了其从众多可测量参数中衍生出的众多应用。在众多LSC应用中,以下方面得到了强调:(a)评估染色质凝聚以识别有丝分裂、凋亡或衰老细胞;(b)检测关键因子如NF-κB、p53或Bax的核转位或线粒体转位;(c)在致突变性试验中对微核进行半自动评分;(d)荧光原位杂交(FISH)分析以及利用FISH分析属性测量其他点状荧光模式,如γH2AX焦点或受体聚集;(e)对核仁及其他细胞器进行计数和形态测量;(f)在克隆形成试验中分析单个细胞的子代;(g)细胞免疫表型分析;(h)在同一细胞重新定位后使用不同探针进行成像、视觉检查或序列分析;(i)原位酶动力学、药物摄取及其他时间分辨过程;(j)使用荧光和显色探针分析组织切片结构;(k)应用于低细胞样本(针吸活检、脑脊液等);以及(l)其他临床应用。文中讨论了LSC的优点和局限性,并与FCM进行了比较。

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