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Development of a peptidomimetic ligand for efficient isolation and purification of factor VIII via affinity chromatography

机译:拟肽配体的开发,可通过亲和色谱法有效分离和纯化因子VIII

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摘要

Hemophilia A, one of the most severe bleeding disorders, results from an inherited deficiency of factor VIII (FVIII) function. Treatment by injection of FVIII has been a common procedure for decades. Nevertheless, the production and purification of FVIII remains a challenging task. Current procedures using immunoaffinity chromatography are expensive and suffer from the instability of the applied antibody ligands, which elute along with the product and contaminate it. Recently, FVIII was purified by use of octapeptide ligands, but their low protease-resistance limits their application. We here report the systematic rational and combinatorial optimization procedure that allowed us to transfer the octapeptide ligands into a small peptidomimetic. This compound is the smallest ligand known for separation of such a large protein (330 kDa). It not only binds and purifies FVIII with high efficiency but also is stable, protease-resistant, and cheap to produce in preparative scale. Hence it offers a valuable alternative to antibody-based purification procedures.
机译:A型血友病是最严重的出血性疾病之一,是由于遗传性VIII因子(FVIII)功能缺陷所致。数十年来,通过注射FVIII进行治疗已成为一种常见方法。尽管如此,FVIII的生产和纯化仍然是一项艰巨的任务。当前使用免疫亲和层析的方法昂贵且遭受所施加的抗体配体的不稳定性,所述抗体配体随产物一起洗脱并污染其。最近,通过使用八肽配体纯化了FVIII,但是它们的低蛋白酶抗性限制了它们的应用。我们在这里报告了系统的合理和组合优化程序,使我们能够将八肽配体转移到小的拟肽中。该化合物是已知的可分离如此大蛋白质(330 kDa)的最小配体。它不仅可以高效地结合和纯化FVIII,而且稳定,耐蛋白酶,并且可廉价制备。因此,它为基于抗体的纯化程序提供了有价值的替代方法。

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