首页> 外文期刊>Cytometry, Part B. Clinical cytometry: the journal of the International Society for Analytical Cytology >'Virtual flow cytometry' of immunostained lymphocytes on microscopic tissue slides: iHCFlow (TM) tissue cytometry
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'Virtual flow cytometry' of immunostained lymphocytes on microscopic tissue slides: iHCFlow (TM) tissue cytometry

机译:显微组织切片上免疫染色的淋巴细胞的“虚拟流式细胞术”:iHCFlow(TM)组织细胞术

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Background: A method and approach is developed for fully automated measurements of immunostained lymphocytes in tissue sections by means of digital color microscopy and patent pending advanced cell analysis. The validation data for population statistic measurements of immunostained lymphocytes in tissue sections using tissue cytometry (TC) is presented. The report is the first to describe the conversion of immunohistochemistry (IHC) data to a flow cytometry-like two parameter dot-plot display, hence the technique is also a virtual flow cytometry. We believe this approach is a paradigm shift, as well as novel, and called the system iHCFlow (TM) TC. Seven issues related to technical obstacles to virtual flow cytometry (FC) are identified. Design: Segmentation of a 512 x 474 RGB image and tabular display of statistical results table took 1215 s using proprietary developed algorithms. We used a panel of seven antibodies for validation on 14 cases of mantle cell lymphoma giving percentage positive, total lymphocytes, and staining density. A total of 2,027 image frames with 810,800 cell objects (COBS) were evaluated. Antibodies to CD3, CD4, CD8, Bcl-1, Ki-67, CD20, CD5 were subjected to virtual FC on tissue. The results of TC were compared with manual counts of expert observers and with the results of flow cytometric immunophenotyping of the same specimen. Results: The correlation coefficient and 95% confidence interval by linear regression analysis yielded a high concordance between manual human results (M), FC results, and TC results per antibody, (r = 0.9365 M vs. TC, r = 0.9537 FC vs. TC). The technical issues were resolved and the solutions and results were evaluated and presented. Conclusion: These results suggest the new technology of TC by iHCFIow (TM) could be a clinically valid surrogate for both M and FC analysis when only tissue IHC is available for diagnosis and prognosis. The application for cancer diagnosis, monitoring, and prognosis is for objective, rapid, automated counting of immunostained cells in tissues with percentage results. We report a new paradigm in TC that converts IHC staining of lymphocytes to automated results and a flow cytometry-like report. The dot plot histogram display is familiar, intuitive, informative, and provides the pathologists with an automated tool to rapidly characterize the staining and size distribution of the immunoreactive as well as the negative cell population in the tissue. This systems tool is a major improvement over existing ones and satisfy fully the criteria to perform Cytomics (Ecker and Tarnok, Cytometry A 2005;65:1; Ecker and Steiner, Cytometry A 2004; 59:182-190; Ecker et al., Cytometry A 2004;59:172-181). (c) 2006 Clinical Cytometry Society.
机译:背景:开发了一种方法和方法,用于通过数字彩色显微镜和正在申请专利的高级细胞分析方法对组织切片中的免疫染色淋巴细胞进行全自动测量。提供了使用组织细胞术(TC)对组织切片中的免疫染色淋巴细胞进行人口统计测量的验证数据。该报告是第一个描述免疫组织化学(IHC)数据到流式细胞仪样两参数点图显示的转换的报告,因此该技术也是一种虚拟流式细胞仪。我们认为这种方法是一种范式转换,并且是新颖的,称为系统iHCFlow(TM)TC。确定了与虚拟流式细胞术(FC)的技术障碍相关的七个问题。设计:使用专有开发的算法对512 x 474 RGB图像进行分割并以表格形式显示统计结果表花费了1215 s。我们使用了七种抗体的组合来验证14例套细胞淋巴瘤的阳性率,总淋巴细胞和染色密度。总共评估了2,027个具有810,800个细胞对象(COBS)的图像帧。针对CD3,CD4,CD8,Bcl-1,Ki-67,CD20,CD5的抗体在组织上进行虚拟FC。将TC的结果与专家观察员的手工计数以及同一样本的流式细胞仪免疫表型结果进行比较。结果:通过线性回归分析得出的相关系数和95%置信区间在人工人为结果(M),FC结果和每种抗体的TC结果之间具有很高的一致性(r = 0.9365 M vs. TC,r = 0.9537 FC vs. TC。 TC)。解决了技术问题,并对解决方案和结果进行了评估和介绍。结论:这些结果表明,仅组织IHC可用于诊断和预后时,iHCFIow(TM)的TC新技术可能是M和FC分析的临床有效替代方法。癌症诊断,监测和预后的应用程序是对组织中免疫染色细胞进行客观,快速,自动计数的结果。我们报告了一种新的TC模式,可将淋巴细胞的IHC染色转换为自动化结果,并提供类似流式细胞术的报告。点状图直方图显示是熟悉,直观,信息丰富的,并为病理学家提供了一种自动工具,可快速表征免疫反应性以及组织中阴性细胞群体的染色和大小分布。该系统工具是对现有工具的重大改进,并且完全满足执行Cytomics的标准(Ecker和Tarnok,Cytometry A 2005; 65:1; Ecker和Steiner,Cytometry A 2004; 59:182-190; Ecker等,细胞计数法A 2004; 59:172-181)。 (c)2006临床细胞计数学会。

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