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通过与重组白蛋白融合来延长凝血因子的药代动力学半衰期。

Extending the pharmacokinetic half-life of coagulation factors by fusion to recombinant albumin.

机构信息

Hubert J. Metzner, CSL Behring GmbH, Emil-von-Behring-Str. 76, 35041 Marburg, Germany, Tel.: +49 6421 394417, Fax: +49 6421 394663, E-mail:

出版信息

Thromb Haemost. 2013 Nov;110(5):931-9. doi: 10.1160/TH13-03-0213. Epub 2013 Aug 29.

Abstract

The prophylactic treatment of haemophilia B and the management of haemophilia A or B with inhibitors demand frequent administrations of coagulation factors due to the suboptimal half-lives of the products commercially available and currently in use, e.g. recombinant factor IX (rFIX) and recombinant factor VIIa (rFVIIa), respectively. The extension of the half-lives of rFIX and rFVIIa could allow for longer intervals between infusions and could thereby improve adherence and clinical outcomes and may improve quality of life. Albumin fusion is one of a number of different techniques currently being examined to prolong the half-life of rFIX and rFVIIa. Results from a phase I clinical trial demonstrated that the recombinant fusion protein linking FIX to albumin (rIX-FP) has a five-times longer half-life than rFIX, and preclinical studies with the recombinant fusion protein linking FVIIa to albumin (rVIIa-FP) suggest that rVIIa-FP possesses a significantly extended half-life versus rFVIIa. In this review, we describe albumin fusion technology and examine the recent progress in the development of rIX-FP and rVIIa-FP.

摘要

预防性治疗乙型血友病和抑制物的甲型或乙型血友病的管理,由于商业上可及和目前正在使用的产品的半衰期不理想,例如重组因子 IX(rFIX)和重组因子 VIIa(rFVIIa),需要频繁给予凝血因子。延长 rFIX 和 rFVIIa 的半衰期可以允许更长的输注间隔,从而改善依从性和临床结果,并可能改善生活质量。白蛋白融合是目前正在研究的延长 rFIX 和 rFVIIa 半衰期的多种不同技术之一。一项 I 期临床试验的结果表明,将 FIX 与白蛋白连接的重组融合蛋白(rIX-FP)的半衰期是 rFIX 的五倍,而将 FVIIa 与白蛋白连接的重组融合蛋白(rVIIa-FP)的临床前研究表明,rVIIa-FP 的半衰期明显长于 rFVIIa。在这篇综述中,我们描述了白蛋白融合技术,并考察了 rIX-FP 和 rVIIa-FP 的最新研发进展。

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