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首页> 外文期刊>Journal of Clinical Pathology >Dynamic behavioural interpretation of cervical intraepithelial neoplasia with molecular biomarkers
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Dynamic behavioural interpretation of cervical intraepithelial neoplasia with molecular biomarkers

机译:分子生物学标志物对宫颈上皮内瘤变的动态行为解释

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摘要

The microscopic phenoiype of cervical intraepithelial neoplasia (CIN) reflects a fine balance between factors that promote or reduce CIN development. A shortcoming of the current grading system is its reliance on static morphology and microscopic haematoxylin-eosin features of the epithelium alone. In reality, CIN is a dynamic process, and the epithelium may exhibit differing results over time. Functional biomarkers p16, Ki-67, p53, retinoblastoma protein cytokeratin (CK)14 and CK13, help in the assessment of an individual CIN's lesion's potential for progression and regression. The aggregate information provided by these biomarkers exceeds the value of the classic grading system. Consequently, many more CINs that will either regress or progress can be accurately identified. These findings agree with known molecular interactions between HPV and the host. For accurate interpretation of a CIN, it is essential that these biomarkers be determined quantitatively and separately in the superficial, middle and deep layers of the epithelium. Such geography-specific epithelial evaluations of quantitative biomarkers emphasise the dynamic nature of a particular CIN lesion, thereby changing the art of static morphology grading into dynamic interpretation of the diseased tissue, with a strong prognostic effect.
机译:宫颈上皮内瘤变(CIN)的微观表型反映了促进或减少CIN发生的因素之间的良好平衡。当前分级系统的缺点在于其仅依赖于上皮的静态形态和苏木精-曙红的微观特征。实际上,CIN是一个动态过程,随着时间的流逝,上皮可能显示出不同的结果。功能性生物标志物p16,Ki-67,p53,成视网膜细胞瘤蛋白细胞角蛋白(CK)14和CK13,有助于评估单个CIN病变的进展和消退潜力。这些生物标志物提供的汇总信息超过了经典分级系统的价值。因此,可以准确地识别出将消退或进展的更多CIN。这些发现与HPV和宿主之间已知的分子相互作用一致。为了准确解释CIN,必须在上皮的浅层,中层和深层分别定量和单独测定这些生物标志物。定量生物标记物的此类特定于地理的上皮评估强调了特定CIN病变的动态性质,从而将静态形态学的技术转变为对患病组织的动态解释,具有很强的预后效果。

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