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液体活检在实体瘤预测性基因突变分析中的应用:病理医师的视角。

Liquid biopsy for predictive mutational profiling of solid cancer: The pathologist's perspective.

机构信息

Department of Pathology, Faculty of Medicine, University of Debrecen, Nagyerdei krt 98, H-4032, Debrecen, Hungary.

出版信息

J Biotechnol. 2019 May 20;297:66-70. doi: 10.1016/j.jbiotec.2019.04.002. Epub 2019 Apr 3.

Abstract

The pathological diagnostics of cancer - based on the histological features - is today increasingly completed by molecular profiling at variable depth in an almost evident fashion. Predictive information should cover potential therapeutic targets and/or major resistance mechanisms the nature of which is subject of alteration during the course of the treatment. Mutational profiling recently became technically available by the analysis of circulating free DNA obtained following non-invasive peripheral blood or body fluid sampling. This "liquid biopsy" approach reflects the general status considering the actual tumor burden, irrespective of the intratumoral distribution and anatomical site. However, the dynamics of the liquid compartment relies on tissue-related processes reflected by histological variables. The amount and composition of free DNA seems to be influenced by many factors, including the stage and anatomical localization of the cancer, the relative mass of neoplastic subclones, the growth rate, the stromal and inflammatory component, the extent of tumor cell death and necrosis. The histopathological context should be considered also when analysis of cfDNA is about to replace repeated tumor sampling for molecular follow-up.

摘要

癌症的病理诊断——基于组织学特征——如今在很大程度上通过分子分析得到了补充,这种分析的深度因变量而异。预测信息应该涵盖潜在的治疗靶点和/或主要的耐药机制,这些机制的性质在治疗过程中会发生改变。最近,通过分析非侵入性外周血或体液采样获得的循环游离 DNA,使突变分析在技术上成为可能。这种“液体活检”方法反映了一般状态,考虑到实际的肿瘤负担,而不考虑肿瘤内的分布和解剖部位。然而,液体隔室的动态依赖于组织相关过程,这些过程由组织学变量反映。游离 DNA 的数量和组成似乎受到许多因素的影响,包括癌症的阶段和解剖定位、肿瘤亚克隆的相对质量、生长速度、基质和炎症成分、肿瘤细胞死亡和坏死的程度。当 cfDNA 分析即将取代重复的肿瘤取样进行分子随访时,也应该考虑组织病理学背景。

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