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肿瘤细胞黏附与迁移在器官特异性转移形成中的作用。

Role of tumor cell adhesion and migration in organ-specific metastasis formation.

作者信息

Gassmann P, Enns A, Haier J

机构信息

Department of General Surgery, University Hospital Münster, Germany.

出版信息

Onkologie. 2004 Dec;27(6):577-82. doi: 10.1159/000081343.

Abstract

To form clinically evident metastases--the main cause of death in cancer patients--, tumor cells (TC) must complete a highly complex series of steps called the metastatic cascade, including local invasiveness, intravasation, circulation, adhesion and extravasation, survival, proliferation and angiogenesis. Since failure of any one of these steps results in metastatic failure, understanding the metastatic cascade may guide us to new therapeutic concepts. Here we review the role of specific TC adhesion and migration processes for organ-selective metastasis formation. TC adhesion in the microvasculature of host organs is a specific and highly regulated process mainly mediated by selectins for TC/endothelial cell binding and by integrins for TC/extracellular matrix interactions. Defined expression of the adhesion molecules and their corresponding ligands in the host organs and on the TC governs organ-selective non-random TC arrest. TC motility and subsequent chemotactically guided extravasation of adherent cells is the second rate-limiting step in organ-specific metastasis formation. Only if cells have completed adhesion and extravasation the growth of micrometastases and finally clinically evident metastases can occur.

摘要

要形成临床上明显的转移灶(癌症患者死亡的主要原因),肿瘤细胞(TC)必须完成一系列高度复杂的步骤,即所谓的转移级联反应,包括局部侵袭、血管内渗、循环、黏附、血管外渗、存活、增殖和血管生成。由于这些步骤中的任何一个失败都会导致转移失败,因此了解转移级联反应可能会引导我们形成新的治疗理念。在此,我们综述特定肿瘤细胞黏附和迁移过程在器官选择性转移形成中的作用。肿瘤细胞在宿主器官微血管中的黏附是一个特定且高度受调控的过程,主要由选择素介导肿瘤细胞与内皮细胞的结合,由整合素介导肿瘤细胞与细胞外基质的相互作用。宿主器官和肿瘤细胞上黏附分子及其相应配体的特定表达决定了器官选择性非随机肿瘤细胞停滞。肿瘤细胞的运动性以及随后黏附细胞在趋化作用引导下的血管外渗是器官特异性转移形成中的第二个限速步骤。只有当细胞完成黏附和血管外渗后,微转移灶的生长以及最终临床上明显的转移灶才会出现。

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