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In vivo measurement of epidermal thickness changes associated with tumor promotion in murine models

机译:在小鼠模型中体内测量与肿瘤促进相关的表皮厚度变化

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摘要

The characterization of tissue morphology in murine models of pathogenesis has traditionally been carried out by excision of affected tissues with subsequent immunohistological examination. Excision-based histology provides a limited two-dimensional presentation of tissue morphology at the cost of halting disease progression at a single time point and sacrifice of the animal. We investigate the use of noninvasive reflectance mode confocal scanning laser microscopy (rCSLM) as an alternative tool to biopsy in documenting epidermal hyperplasia in murine models exposed to the tumor promoter 12-O-tetradecanoylphorbol-13-acetate (TPA). An automated technique utilizing average axial rCSLM reflectance profiles is used to extract epidermal thickness values from rCSLM data cubes. In comparisons to epidermal thicknesses determined from hematoxylin and eosin (H&E) stained tissue sections, we find no significant correlation to rCSLM-derived thickness values. This results from method-specific artifacts: physical alterations of tissue during H&E preparation in standard histology and specimen-induced abberations in rCSLM imaging. Despite their disagreement, both histology and rCSLM methods reliably measure statistically significant thickness changes in response to TPA exposure. Our results demonstrate that in vivo rCSLM imaging provides epithelial biologists an accurate noninvasive means to monitor cutaneous pathogenesis.
机译:传统上,通过切除受影响的组织并随后进行免疫组织学检查,可以在鼠的发病机理模型中对组织形态进行表征。基于切除的组织学提供了组织形态学的有限的二维表示,其代价是在单个时间点停止疾病的进展并牺牲了动物。我们调查使用无创反射模式共聚焦扫描激光显微镜(rCSLM)作为活检的替代工具,用于在暴露于肿瘤启动子12-O-十四烷酰佛波醇13-乙酸盐(TPA)的小鼠模型中记录表皮增生。利用平均rCSLM轴向平均反射率轮廓的自动技术从rCSLM数据立方体中提取表皮厚度值。与由苏木精和曙红(H&E)染色的组织切片确定的表皮厚度相比,我们发现与rCSLM衍生的厚度值无显着相关性。这是由特定于方法的伪像导致的:在标准组织学中进行H&E准备期间组织的物理变化以及rCSLM成像中标本引起的像变。尽管存在分歧,但组织学和rCSLM方法均能可靠地测量TPA暴露引起的统计学上显着的厚度变化。我们的结果表明,体内rCSLM成像为上皮生物学家提供了一种准确的无创手段来监测皮肤发病机理。

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