通过计算机辅助图像分析测量上皮癌前病变(上皮内瘤变)的特性,得出化学预防药物临床试验的终点标记。

Cancer surveys Pub Date : 1998-01-01
C W Boone, G J Kelloff
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引用次数: 0

摘要

NCI化学预防处正在支持80多个化学预防药物的临床试验,并有数十种药物正在开发中。CAQIA测量的上皮癌前病变(也称为浸润前或IEN)的结构和功能特性,如细胞核大小、形状和细胞增殖和凋亡率的日益异常,构成了化学预防药物短期临床试验中特异性和定量终点标志物的基础。IEN通常(如果不是一成不变的话)之前有两种情况弥漫性地影响上皮:基因组不稳定和慢性增生。慢性上皮下炎症也很常见。单个病变的多中心性和多路径遗传进展是设计终点标记和在化学预防药物的临床试验中规划足够的活检取样时必须考虑的重要特征。CAQIA在测量IEN的细胞变化时提供了更高的灵敏度和特异性,例如越来越异常的核大小、核形状、核DNA的综合光密度和核染色质纹理特征。一个名为“深谷探测器”的软件程序,可以测量染色DNA的组织学切片细胞核中染色质团块边缘的光密度梯度,这是许多核染色质质地特征测量的一个例子。在宫颈高级别IEN肿瘤细胞的细胞核图像中,有111个深谷区,而非肿瘤增生细胞的细胞核仅显示16个。化学预防剂对IEN的调节作用可以通过它们在每个细胞核中产生的深谷位点的平均数量的变化来量化。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Endpoint markers for clinical trials of chemopreventive agents derived from the properties of epithelial precancer (intraepithelial neoplasia) measured by computer-assisted image analysis.

The Chemoprevention Branch, NCI, is supporting over 80 clinical trials of chemopreventive agents and has dozens of drugs under development. The structural and functional properties of epithelial precancer (also called preinvasive or IEN), such as increasingly aberrant nuclear size, shape and rates of cellular proliferation and apoptosis, measured by CAQIA, form the basis for specific and quantitative end markers in short term clinical trials of chemopreventive agents. IEN very frequently, if not invariably, is preceded by two conditions diffusely affecting the epithelium: genomic instability and chronic hyperplasia. Chronic subepithelial inflammation is also commonly present. Multicentricity and multipath genetic progression of individual lesions are important characteristics that must be considered when designing endpoint markers and planning for adequate biopsy sampling in clinical trials of chemopreventive agents. Use of CAQIA provides increased sensitivity and specificity when measuring the cellular changes of IEN, such as increasingly aberrant nuclear size, nuclear shape, integrated optical density of nuclear DNA and nuclear chromatin texture features. A software program called the Deep Valley Detector, which measures the optical density gradient at the margins of chromatin clumps in cell nuclei of histological sections stained for DNA, is one example of many nuclear chromatin texture features measured. In the image of the nucleus of a neoplastic cell from high grade IEN of the cervix, 111 deep valley sites were counted, whereas the nucleus of a non-neoplastic hyperplastic cell showed only 16 sites. The modulating effects of chemopreventive agents on IEN may be quantitated by the change they produce in the average number of deep valley sites per nucleus.

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