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癌细胞黏附与转移:选择素、整合素以及肝素的抑制潜力

Cancer cell adhesion and metastasis: selectins, integrins, and the inhibitory potential of heparins.

作者信息

Bendas Gerd, Borsig Lubor

机构信息

Department of Pharmaceutical Chemistry, University of Bonn, 53121 Bonn, Germany.

出版信息

Int J Cell Biol. 2012;2012:676731. doi: 10.1155/2012/676731. Epub 2012 Feb 12.

Abstract

Cell adhesion molecules play a significant role in cancer progression and metastasis. Cell-cell interactions of cancer cells with endothelium determine the metastatic spread. In addition, direct tumor cell interactions with platelets, leukocytes, and soluble components significantly contribute to cancer cell adhesion, extravasation, and the establishment of metastatic lesions. Clinical evidence indicates that heparin, commonly used for treatment of thromboembolic events in cancer patients, is beneficial for their survival. Preclinical studies confirm that heparin possesses antimetastatic activities that lead to attenuation of metastasis in various animal models. Heparin contains several biological activities that may affect several steps in metastatic cascade. Here we focus on the role of cellular adhesion receptors in the metastatic cascade and discuss evidence for heparin as an inhibitor of cell adhesion. While P- and L-selectin facilitation of cellular contacts during hematogenous metastasis is being accepted as a potential target of heparin, here we propose that heparin may also interfere with integrin activity and thereby affect cancer progression. This review summarizes recent findings about potential mechanisms of tumor cell interactions in the vasculature and antimetastatic activities of heparin.

摘要

细胞黏附分子在癌症进展和转移中发挥着重要作用。癌细胞与内皮细胞之间的细胞间相互作用决定了转移扩散。此外,肿瘤细胞与血小板、白细胞以及可溶性成分的直接相互作用显著促进了癌细胞的黏附、外渗以及转移病灶的形成。临床证据表明,常用于治疗癌症患者血栓栓塞事件的肝素对其生存有益。临床前研究证实,肝素具有抗转移活性,可导致多种动物模型中的转移减弱。肝素具有多种生物学活性,可能会影响转移级联反应中的多个步骤。在此,我们聚焦于细胞黏附受体在转移级联反应中的作用,并讨论肝素作为细胞黏附抑制剂的证据。虽然P-选择素和L-选择素在血行转移过程中促进细胞接触被认为是肝素的潜在靶点,但在此我们提出,肝素也可能干扰整合素活性,从而影响癌症进展。本综述总结了关于肿瘤细胞在脉管系统中相互作用的潜在机制以及肝素抗转移活性的最新研究发现。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/913b/3296185/77be849585d4/IJCB2012-676731.001.jpg

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