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分子病理学的下一步:细胞学中的下一代测序

Next step of molecular pathology: next-generation sequencing in cytology.

作者信息

Silva Ricella Souza da, Schmitt Fernando

机构信息

IPATIMUP Diagnostics, IPATIMUP - Institute of Molecular Pathology and Immunology of Porto University, Porto, Portugal.

RISE (Health Research Network), Porto, Portugal.

出版信息

J Pathol Transl Med. 2024 Nov;58(6):291-298. doi: 10.4132/jptm.2024.10.22. Epub 2024 Nov 7.

Abstract

The evolving landscape of precision oncology underscores the pivotal shift from morphological diagnosis to treatment decisions driven by molecular profiling. Recent guidelines from the European Society for Medical Oncology recomend the use of next-generation sequencing (NGS) across a broader range of cancers, reflecting its superior efficiency and clinical value. NGS not only updates oncology testing by offering quicker, sample-friendly, and sensitive analysis but also reduces the need for multiple individual tests. Cytology samples, often obtained through less invasive methods, can yield high-quality genetic material suitable for molecular analysis. This article focuses on optimizing the use of cytology samples in NGS, and outlines their potential benefits in identifying actionable molecular alterations for targeted therapies across various solid tumors. It also addresses the need for validation studies and the strategies to incorporate or combine different types of samples into routine clinical practice. Integrating cytological and liquid biopsies into routine clinical practice, alongside conventional tissue biopsies, offers a comprehensive approach to tumor genotyping, early disease detection, and monitoring of therapeutic responses across various solid tumor types. For comprehensive biomarker characterization, all patient specimens, although limited, is always valuable.

摘要

精准肿瘤学不断演变的格局凸显了从形态学诊断到由分子谱分析驱动治疗决策的关键转变。欧洲医学肿瘤学会最近的指南建议在更广泛的癌症类型中使用下一代测序(NGS),这反映了其卓越的效率和临床价值。NGS不仅通过提供更快、对样本友好且灵敏的分析更新了肿瘤学检测,还减少了对多个单独检测的需求。细胞学样本通常通过侵入性较小的方法获取,能够产生适用于分子分析的高质量遗传物质。本文着重于优化NGS中细胞学样本的使用,并概述其在识别各种实体瘤靶向治疗的可操作分子改变方面的潜在益处。它还讨论了验证研究的必要性以及将不同类型样本纳入或组合到常规临床实践中的策略。将细胞学和液体活检与传统组织活检一起纳入常规临床实践,为各种实体瘤类型的肿瘤基因分型、疾病早期检测和治疗反应监测提供了一种全面的方法。对于全面的生物标志物表征,所有患者标本尽管有限,但始终具有价值。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7752/11573480/a5c95da6f3a5/jptm-2024-10-22f1.jpg

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