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Expression purification and analysis of three recombinant ECD disintegrins (r-colombistatins) from P-III class snake venom metalloproteinases affecting platelet aggregation and SK-MEL-28 cell adhesion

机译:P-III类蛇毒金属蛋白酶中三种重组ECD整联蛋白(r-colombistatins)的表达纯化和分析影响血小板聚集和SK-MEL-28细胞粘附

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摘要

Crotalid venoms are rich sources of components that affect the hemostatic system. Snake venom metalloproteinases are zinc-dependent enzymes responsible for hemorrhage that also interfere with hemostasis. The disintegrin domain is a part of snake venom metalloproteinases, which involves the binding of integrin receptors. Integrins play an essential role in cancer survival and invasion, and they have been major targets for drug development and design. Both native and recombinant disintegrins have been widely investigated for their anti-cancer activities in biological systems as well as in vitro and in vivo systems. Here, three new cDNAs encoding ECD disintegrin-like domains of metalloproteinase precursor sequences obtained from a Venezuelan mapanare (Bothrops colombiensis) venom gland cDNA library have been cloned. Three different N- and C-terminal truncated ECD disintegrin-like domains of metalloproteinases named colombistatins 2, 3, and 4 were amplified by PCR, cloned into a pGEX-4T-1 vector, expressed in Escherichia coli BL21, and tested for inhibition of platelet aggregation and inhibition of adhesion of human skin melanoma (SK-Mel-28) cancer cell lines on collagen I. Purified recombinant colombistatins 2, 3, and 4 were able to inhibit ristocetin- and collagen-induced platelet aggregation. r-Colombistatins 2 showed the most potent inhibiting SK-Mel-28 cancer cells adhesion to collagen. These results suggest that colombistatins may have utility in the development of therapeutic tools in the treatment of melanoma cancers and also thrombotic diseases.
机译:响尾蛇毒液是影响止血系统的丰富成分。蛇毒金属蛋白酶是锌依赖性酶,负责出血,也干扰止血。整联蛋白结构域是蛇毒金属蛋白酶的一部分,涉及整联蛋白受体的结合。整联蛋白在癌症的存活和侵袭中起着至关重要的作用,它们已经成为药物开发和设计的主要目标。天然和重组解整合素在生物系统以及体外和体内系统中的抗癌活性已被广泛研究。在这里,已克隆了三个新的cDNA,它们编码从委内瑞拉mapanare(Bothrops colombiensis)毒腺cDNA文库中获得的金属蛋白酶前体序列的ECD整合素样结构域。通过PCR扩增了三个不同的金属蛋白酶的N和C端截短的ECD整合素样结构域,称为colombistatins 2、3和4,克隆到pGEX-4T-1载体中,在大肠杆菌BL21中表达,并测试了对BBL的抑制作用血小板聚集和抑制人皮肤黑色素瘤(SK-Mel-28)癌细胞系对胶原蛋白I的粘附。纯化的重组colombistatins 2、3和4能够抑制瑞斯托素和胶原蛋白诱导的血小板聚集。 r-Colombistatins 2显示出最有效的抑制SK-Mel-28癌细胞粘附胶原的功能。这些结果表明,结肠抑素可能在开发用于治疗黑素瘤癌症以及血栓性疾病的治疗工具中具有效用。

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