Sequential steps in hematogenous metastasis of cancer cells studied by in vivo videomicroscopy.

Invasion & metastasis Pub Date : 1997-01-01
V L Morris, E E Schmidt, I C MacDonald, A C Groom, A F Chambers
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Abstract

Understanding metastatic spread of cancer is of upmost importance to developing successful strategies to treat this disease. In this review, we present a picture of the process of hematogenous metastasis from the initial arrest of cancer cells, their extravasation, postextravasation migration, and their replication to form tumors, based on experimental results using in vivo videomicroscopy. The cancer cells are initially arrested by size constraints within minutes of entering the circulation and with little hemodynamic destruction. Within 24-48 h >80% of these cancer cells extravasate as single cells by adhesion to and spreading along the vessel wall, often using pseudopodial projections to move into the surrounding tissue without disrupting the microcirculation. Some of the extravasated cells also use pseudopodial projections to migrate to specific structures in the tissue where they can replicate. Many cancer cells can persist as dormant cells, neither dividing nor undergoing apoptosis. Only a small fraction of extravasated cells begin to divide to form micrometastases, and only a very small fraction of these micrometastases continue to grow to form tumors. Possible clinical implications are that (1) initial arrest and extravasation may be difficult to prevent and thus may be poor therapeutic targets; (2) dormant single cells will not be affected by conventional cancer therapies which are designed to treat actively growing cells; and (3) regulation of growth of cells after extravasation is key to determining whether clinically evident metastases form - this stage of metastasis thus offers promising targets for new antimetastasis drugs.

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活体视频显微镜研究癌细胞血行转移的顺序步骤。
了解癌症的转移性扩散对于制定治疗这种疾病的成功策略至关重要。在这篇综述中,我们介绍了血液转移的过程,从最初的癌细胞被阻止,它们的外渗,外渗后的迁移,以及它们的复制形成肿瘤的过程,基于体内视频显微镜的实验结果。癌细胞最初在进入血液循环的几分钟内就被大小限制所抑制,几乎没有血液动力学破坏。在24-48小时内,80%以上的癌细胞以单细胞形式附着在血管壁上并沿血管壁扩散,通常利用假足突向周围组织移动而不破坏微循环。一些外渗的细胞也利用假足突迁移到组织中的特定结构,在那里它们可以复制。许多癌细胞可以作为休眠细胞持续存在,既不分裂也不凋亡。只有一小部分外渗细胞开始分裂形成微转移瘤,而这些微转移瘤中只有极少数继续生长形成肿瘤。可能的临床意义是:(1)初始骤停和外渗可能难以预防,因此可能是较差的治疗靶点;(2)休眠的单细胞不会受到传统癌症疗法的影响,这些疗法旨在治疗活跃生长的细胞;(3)外渗后细胞的生长调节是决定是否形成临床明显转移的关键,这一阶段的转移为新的抗转移药物提供了有希望的靶点。
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