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聚乙二醇化脂质体在治疗血友病的药物递送应用开发中的应用。

The use of PEGylated liposomes in the development of drug delivery applications for the treatment of hemophilia.

机构信息

Omri Laboratories Ltd., Nes Ziona, Israel.

出版信息

Int J Nanomedicine. 2010 Sep 7;5:581-91. doi: 10.2147/ijn.s8603.

Abstract

Hemophilia A is a rare X-linked bleeding disorder caused by lack or dysfunction of coagulation factor VIII (FVIII). Hemophilia A is treated with replacement therapy, but frequent injections of the missing FVIII often lead to the formation of inhibitory antibodies. Patients who develop high levels of inhibitors must be treated with bypassing agents such as activated FVII (FVIIa). Both FVIII and FVIIa have short half-lives and require multiple injections. Long-acting forms of these proteins would therefore reduce the frequency of injections, improve patient compliance and reduce complications. In this article we present a new platform technology that produces long-acting forms of FVIII and FVIIa and improves the efficacy of hemophilia treatment. This technology is based on the binding of proteins/peptides to the outer surface of PEGylated liposomes (PEGLip). Binding is dependent on an amino acid consensus sequence within the proteins and is highly specific. At the same time, binding is non-covalent and does not require any modification of the therapeutic agent or its production process. Association of proteins with PEGLip results in substantial enhancements in their pharmacodynamic properties following administration. These improvements seem to arise from the association of formulated proteins with platelets prior to induction of coagulation.

摘要

血友病 A 是一种罕见的 X 连锁出血性疾病,由凝血因子 VIII(FVIII)缺乏或功能障碍引起。血友病 A 采用替代疗法治疗,但频繁注射缺失的 FVIII 常常导致抑制性抗体的形成。产生高浓度抑制剂的患者必须使用旁路制剂如激活的凝血因子 VII(FVIIa)治疗。FVIII 和 FVIIa 的半衰期都很短,需要多次注射。这些蛋白质的长效形式将减少注射次数,提高患者依从性并减少并发症。在本文中,我们介绍了一种生产长效 FVIII 和 FVIIa 的新平台技术,可改善血友病治疗的疗效。该技术基于将蛋白质/肽结合到聚乙二醇化脂质体(PEGLip)的外表面上。结合取决于蛋白质内的氨基酸共有序列,具有高度特异性。同时,结合是非共价的,不需要对治疗剂或其生产工艺进行任何修饰。蛋白质与 PEGLip 的结合可在给药后显著增强其药效学特性。这些改善似乎源于在诱导凝血之前,与血小板形成的制剂蛋白。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/14b9/2939703/68cb75db29ae/ijn-5-581f1.jpg

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