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循环肿瘤标志物的多样性:多模态液体活检的视角

Diversity of the Circulating Tumor Markers: Perspectives of a Multimodal Liquid Biopsy.

作者信息

Kuligina Ekaterina S, Yanus Grigoriy A, Imyanitov Evgeny N

机构信息

N. N. Petrov National Medical Research Center of Oncology, St. Petersburg, 197758, Russia.

St. Petersburg State Pediatric Medical University, St. Petersburg, 194100, Russia.

出版信息

Biochemistry (Mosc). 2024 Nov;89(11):1985-1997. doi: 10.1134/S0006297924110129.

Abstract

Over the past decade, liquid biopsy (LB) has become a routine diagnostic test essential for the treatment of malignant tumors of various localizations. Its capabilities include early diagnosis, molecular genotyping, prognosis, prediction, and monitoring of tumor response. Typically, liquid biopsy involves the extraction of a single type of tumor-derived molecules or cellular elements from blood and subsequent molecular analysis. These elements may include circulating tumor DNA (ctDNA), circulating tumor cells (CTCs), circulating tumor RNA (ctRNA), or contents of extracellular vesicles (exosomes). Despite the technical sophistication of molecular analysis methods for circulating biomarkers, this diagnostic approach has limited relevance. In a significant proportion of cancer patients (ranging from 10 to 50%, depending on the tumor type), none of these analytes can be detected and analyzed, even in the presence of large, progressing neoplastic foci in the body. It seems reasonable to suggest that heterogeneous fractions of the circulating tumor-specific biomarkers complement each other, thus simultaneous analysis of several fractions will not only increase sensitivity of the method but also more accurately characterize and predict the clinical situation. This review examines the possibilities and advantages of applying a combined multiparametric approach to liquid biopsy, which involves testing multiple circulating analytes in a single blood sample.

摘要

在过去十年中,液体活检(LB)已成为各种部位恶性肿瘤治疗必不可少的常规诊断测试。其功能包括早期诊断、分子基因分型、预后评估、预测以及监测肿瘤反应。通常,液体活检涉及从血液中提取单一类型的肿瘤衍生分子或细胞成分,随后进行分子分析。这些成分可能包括循环肿瘤DNA(ctDNA)、循环肿瘤细胞(CTC)、循环肿瘤RNA(ctRNA)或细胞外囊泡(外泌体)的内容物。尽管用于循环生物标志物的分子分析方法技术复杂,但这种诊断方法的相关性有限。在相当一部分癌症患者中(根据肿瘤类型,比例在10%至50%之间),即使体内存在大且进展性的肿瘤病灶,这些分析物也均无法被检测和分析到。合理的推测是,循环肿瘤特异性生物标志物的异质部分相互补充,因此同时分析多个部分不仅会提高该方法的灵敏度,还能更准确地表征和预测临床情况。本综述探讨了在液体活检中应用联合多参数方法(即在单个血样中检测多种循环分析物)的可能性和优势。

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