Recombinant disintegrin (r-Cam-dis) from Crotalus adamanteus inhibits adhesion of human pancreatic cancer cell lines to laminin-1 and vitronectin.

Journal of Venom Research Pub Date : 2015-04-26 eCollection Date: 2015-01-01
Montamas Suntravat, Henriquez S Barret, Cameron A Jurica, Sara E Lucena, John C Perez, Elda E Sánchez
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Abstract

Pancreatic cancer is a malignant cancer common worldwide having poor prognosis, even when diagnosed at its early stage. Cell adhesion plays a critical role in cancer invasion and metastasis. Integrins are major mediators of cell adhesion and play an important role in invasion and metastatic growth of human pancreatic cancer cells. Snake disintegrins are the most potent ligands of several integrins and have potential therapeutic applications for cancers. We have previously cloned and expressed a new recombinant RGD-disintegrin from Crotalus adamanteus (r-Cam-dis). This recently published r-Cam-dis has an extra nine amino acids derived from the vector (SPGARGSEF) at the N-terminus end and has strong anti-platelet activity. However, this r-Cam-dis contains the contamination of the cleavage of the N-terminal end of the pET-43.1a cloning vector. In this study, we have cloned r-Cam-dis in a different cloning vector (pGEX-4T-1) showing five different amino acids (GSPEF) at the N-terminal part. This new r-Cam-dis was expressed and tested for inhibition of platelet aggregation, specific binding activity with seven different integrins, and inhibition of adhesion of three different pancreatic cancer cell lines on laminin-1 and vitronectin. The r-Cam-dis showed potent binding to αvβ3 integrin, but was moderate to weak with αvβ5, αvβ6, α2β1, and α6β1. Interestingly, the inhibition of r-Cam-dis on pancreatic cancer cell lines adhesion to laminin-1 was more effective than that to vitronectin. Based on our binding results to integrin receptors and previous adhesion studies using function-blocking monoclonal antibodies, it is suggested that r-Cam-dis could be inhibiting adhesion of pancreatic cancer cell lines through integrins α2β1, α6β1, αvβ5, and αvβ6.

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重组金刚蟾崩解素(r-Cam-dis)抑制人胰腺癌细胞系对层粘连蛋白-1和玻璃体粘连蛋白的粘附。
胰腺癌是一种世界范围内常见的恶性癌症,即使在早期诊断,预后也很差。细胞粘附在肿瘤的侵袭和转移中起着至关重要的作用。整合素是细胞粘附的主要介质,在人胰腺癌细胞的侵袭和转移生长中起重要作用。蛇崩解素是几种整合素中最有效的配体,具有潜在的癌症治疗应用。我们已经从Crotalus adamanteus (r-Cam-dis)中克隆并表达了一种新的重组rgd -崩解素。这个最近发表的r-Cam-dis在n端有额外的9个氨基酸来源于载体(SPGARGSEF),具有很强的抗血小板活性。然而,这种r-Cam-dis含有pet -43.1克隆载体n端切割的污染。在这项研究中,我们在不同的克隆载体(pGEX-4T-1)上克隆了r-Cam-dis,在n端部分显示了五种不同的氨基酸(GSPEF)。我们表达了这种新的r-Cam-dis,并测试了它对血小板聚集的抑制作用,与7种不同整合素的特异性结合活性,以及对三种不同胰腺癌细胞系对层粘连蛋白-1和玻璃体连接蛋白的粘附抑制作用。r-Cam-dis与αvβ3整合素结合较强,与αvβ5、αvβ6、α2β1、α6β1结合较弱。有趣的是,r-Cam-dis对胰腺癌细胞株粘附laminin-1的抑制作用比对玻璃板连接蛋白的抑制作用更有效。根据我们与整合素受体的结合结果和先前使用功能阻断单克隆抗体进行的粘附研究,我们认为r-Cam-dis可能通过整合素α2β1、α6β1、αvβ5和αvβ6抑制胰腺癌细胞株的粘附。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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