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黏附受体作为循环肿瘤细胞的治疗靶点。

Adhesion receptors as therapeutic targets for circulating tumor cells.

机构信息

Department of Biomedical Engineering, Cornell University Ithaca, NY, USA.

出版信息

Front Oncol. 2012 Jul 24;2:79. doi: 10.3389/fonc.2012.00079. eCollection 2012.

Abstract

Metastasis contributes to >90% of cancer-associated mortality. Though primary tumors can be removed by surgical resection or chemo/radiotherapy, metastatic disease is a great challenge to treatment due to its systemic nature. As metastatic "seeds," circulating tumor cells (CTCs) are believed to be responsible for dissemination from a primary tumor to anatomically distant organs. Despite the possibility of physical trapping of CTCs in microvessels, recent advances have provided insights into the involvement of a variety of adhesion molecules on CTCs. Such adhesion molecules facilitate direct interaction with the endothelium in specific tissues or indirectly through leukocytes. Importantly, significant progress has been made in understanding how these receptors confer enhanced invasion and survival advantage during hematogenous circulation of CTCs through recruitment of macrophages, neutrophils, platelets, and other cells. This review highlights the identification of novel adhesion molecules and how blocking their function can compromise successful seeding and colonization of CTCs in new microenvironment. Encouraged by existing diagnostic tools to identify and isolate CTCs, strategic targeting of these adhesion molecules to deliver conventional chemotherapeutics or novel apoptotic signals is discussed for the neutralization of CTCs in the circulation.

摘要

转移是导致 90%以上癌症相关死亡的原因。虽然原发性肿瘤可以通过手术切除、化疗或放疗来治疗,但转移性疾病是一个巨大的治疗挑战,因为它具有系统性。循环肿瘤细胞(CTCs)被认为是从原发性肿瘤扩散到解剖学上远处器官的“种子”。尽管 CTC 可能会被微血管物理捕获,但最近的进展提供了对 CTC 上各种粘附分子参与的深入了解。这些粘附分子通过与特定组织中的内皮细胞直接相互作用或通过白细胞间接相互作用来促进转移。重要的是,在了解这些受体如何通过招募巨噬细胞、中性粒细胞、血小板和其他细胞在 CTC 的血液传播过程中赋予增强的侵袭和生存优势方面取得了重大进展。这篇综述强调了鉴定新型粘附分子的重要性,以及阻断其功能如何损害 CTC 在新微环境中成功播种和定植。受现有诊断工具识别和分离 CTC 的鼓舞,讨论了针对这些粘附分子的策略性靶向,以输送常规化疗药物或新型凋亡信号,从而中和循环中的 CTC。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b62b/3402858/779d30c38176/fonc-02-00079-g0001.jpg

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