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首页> 外文期刊>American Journal of Physiology >Limitations of conventional approaches to identify myocyte nuclei in histologic sections of the heart.
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Limitations of conventional approaches to identify myocyte nuclei in histologic sections of the heart.

机译:常规方法鉴定心脏组织学区中肌细胞核的局限性。

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Accurate nuclear identification is crucial for distinguishing the role of cardiac myocytes in intrinsic and experimentally induced regenerative growth of the myocardium. Conventional histologic analysis of myocyte nuclei relies on the optical sectioning capabilities of confocal microscopy in conjunction with immunofluorescent labeling of cytoplasmic proteins such as troponin T, and dyes that bind to double-strand DNA to identify nuclei. Using heart sections from transgenic mice in which the cardiomyocyte-restricted alpha-cardiac myosin heavy chain promoter targeted the expression of nuclear localized beta-galactosidase reporter in >99% of myocytes, we systematically compared the fidelity of conventional myocyte nuclear identification using confocal microscopy, with and without the aid of a membrane marker. The values obtained with these assays were then compared with those obtained with anti-beta-galactosidase immune reactivity in the same samples. In addition, we also studied the accuracy of anti-GATA4 immunoreactivity for myocyte nuclear identification. Our results demonstrate that, although these strategies are capable of identifying myocyte nuclei, the level of interobserver agreement and margin of error can compromise accurate identification of rare events, such as cardiomyocyte apoptosis and proliferation. Thus these data indicate that morphometric approaches based on segmentation are justified only if the margin of error for measuring the event in question has been predetermined and deemed to be small and uniform. We also illustrate the value of a transgene-based approach to overcome these intrinsic limitations of identifying myocyte nuclei. This latter approach should prove quite useful when measuring rare events.
机译:准确的核鉴定对于区分心肌细胞在内在和实验诱导的心肌生长中的作用至关重要。肌细胞核的常规组织学分析依赖于共聚焦显微镜的光学切片能力与细胞质蛋白如肌钙蛋白T的免疫荧光标记,以及与双链DNA结合的染料中染色核。使用来自转基因小鼠的心脏切片,其中心肌细胞受限制的α-心肌肌蛋白重链启动子靶向核局部化β-半乳糖苷酶报告称为99%的肌细胞的表达,我们系统地将常规肌细胞核鉴定的保真度与共聚焦显微镜相比,没有借助膜标记。然后将通过这些测定结果获得的值与在相同样品中用抗β-半乳糖苷酶免疫反应性获得的值进行比较。此外,我们还研究了抗GATA4免疫反应性对肌细胞核鉴定的准确性。我们的结果表明,虽然这些策略能够识别肌细胞核,但杂交协议的水平和误差幅度可能会损害准确的罕见事件,例如心肌细胞凋亡和增殖。因此,这些数据表明,只有在测量所讨论的事件的误差幅度已经预先确定并被视为小而均匀,才能才能证明基于分割的变形方法。我们还说明了基于转基因的方法的价值来克服鉴定肌细胞核的这些内在限制。后一种方法应该在衡量罕见事件时证明非常有用。

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