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抑制肿瘤细胞与细胞外基质的附着作为预防手术伤口肿瘤复发的一种方法。

Inhibition of tumor-cell attachment to extracellular matrix as a method for preventing tumor recurrence in a surgical wound.

作者信息

Whalen G F, Ingber D E

机构信息

Department of Surgery, Childrens Hospital, Boston, Massachusetts.

出版信息

Ann Surg. 1989 Dec;210(6):758-64. doi: 10.1097/00000658-198912000-00011.

Abstract

Studies with four different transplantable murine tumors demonstrated that surgical instruments contaminated by contact with a tumor mass could produce tumors in a surgical wound. Eighty-seven per cent of mice with wounds made by invisibly contaminated scissors developed tumors. Irrigation with water did not prevent tumor growth. Before spilled tumor cells can invade and grow into a recurrence in the wound site, they must first attach to underlying extracellular matrix. We have devised a simple in vitro assay to identify inhibitors of tumor-cell attachment to develop therapeutic compounds that can prevent tumor-cell reimplantation. Various test compounds, including proteases (trypsin and Dispase), known modulators of matrix metabolism (proline analogues, cycloheximide, heparin, cortisone, cortexolone, and heparin-steroid combinations), large molecular weight polymers (agarose, dextran, polyethylene oxide), and synthetic fibronectin peptides were tested for their ability to inhibit mouse melanoma (B16-F10) cell attachment to gelatinized dishes. Most of these compounds had little or no effect on tumor-cell adhesion when cells were plated in serum-containing medium. However we identified three compounds that inhibited tumor-cell attachment in a reversible fashion: (1) a specific inhibitor of collagen deposition (L-azetidine-2-carboxylic acid); (2) a bacterial neutral protease (Dispase); and (3) synthetic fibronectin peptides that contained the arginine-glycine-asparate (RGD) sequence that is responsible for cell binding. Dispase and the RGD-containing peptides also inhibited cell implantation and prevented tumor formation in a surgical wound. We propose that inhibitors of attachment might be used either alone or with other biologic modifiers to prohibit implantation of free tumor cells at the time of surgery and thus, to prevent local tumor recurrence.

摘要

对四种不同的可移植性小鼠肿瘤进行的研究表明,接触肿瘤块而被污染的手术器械可在手术伤口处引发肿瘤。87% 用隐形污染剪刀造成伤口的小鼠发生了肿瘤。用水冲洗并不能阻止肿瘤生长。在溢出的肿瘤细胞侵入并在伤口部位生长复发之前,它们必须首先附着于下方的细胞外基质。我们设计了一种简单的体外试验来鉴定肿瘤细胞附着的抑制剂,以开发能够防止肿瘤细胞再植入的治疗性化合物。对各种测试化合物进行了测试,包括蛋白酶(胰蛋白酶和分散酶)、已知的基质代谢调节剂(脯氨酸类似物、环己酰亚胺、肝素、可的松、皮质酮以及肝素 - 类固醇组合)、大分子聚合物(琼脂糖、葡聚糖、聚环氧乙烷)以及合成纤连蛋白肽,以检测它们抑制小鼠黑色素瘤(B16 - F10)细胞附着于明胶化培养皿的能力。当细胞接种于含血清培养基中时,这些化合物中的大多数对肿瘤细胞黏附几乎没有影响或没有影响。然而,我们鉴定出三种以可逆方式抑制肿瘤细胞附着的化合物:(1)一种胶原蛋白沉积的特异性抑制剂(L - 氮杂环丁烷 - 2 - 羧酸);(2)一种细菌中性蛋白酶(分散酶);(3)含有负责细胞结合的精氨酸 - 甘氨酸 - 天冬氨酸(RGD)序列 的合成纤连蛋白肽。分散酶和含RGD的肽也抑制细胞植入并防止手术伤口处形成肿瘤。我们提出,附着抑制剂可单独使用或与其他生物修饰剂一起使用,以在手术时阻止游离肿瘤细胞的植入,从而防止局部肿瘤复发。

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