Red Blood Cells are Appropriate Carrier for Coagulation Factor VIII

Fatemeh Sayyadipour, N. Amirizadeh, A. Oodi, Masoud Khalili, Fakhredin Saba
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引用次数: 3

Abstract

Aims Factor VIII (FVIII) replacement therapy remains a primary treatment for hemophilia A, however, the development of FVIII antibodies (inhibitors) and short half-life of the FVIII products are the major complications. Erythrocytes may prevent rapid removal of drugs from plasma. Erythrocytes are biocompatible and non-immunogenic drug delivery. In this study, in vitro activity of FVIII encapsulated by human erythrocytes was investigated. Methods FVIII was loaded into erythrocytes using the hypo-osmotic dialysis technique. FVIII activity assay has been analyzed using Activated Partial Thromboplastin Time (APTT). Presence of FVIII on erythrocytes was detected by western blotting and flowcytometry using specific monoclonal antibody (abcam, U.K) against FVIII. Moreover, the osmotic fragility and hematologic parameters of FVIII-loaded carrier erythrocytes were measured. Results Our results indicated that FVIII could not cross the membrane, where plenty of FVIII was found on the surface of the carrier erythrocyte. Flow cytometery results showed that 11% of the loaded carrier erythrocytes was positive for FVIII protein on their surface. The greatest activation of FVIII in both groups including lysate and non-lysate FVIII-loaded RBCs was observed on the first day, and the coagulant activity of this factor was gradually reduced on days 3 and 5. In 1:50 dilution of both groups, significant differences in FVIII activity were observed in 1:50 dilution of both groups, especially on the 5th day. Conclusion This study aims to introduce erythrocytes as appropriate carriers for FVIII to prolong the dosing intervals in the effective and safe levels for a relatively longer time.
红细胞是凝血因子VIII的适宜载体
因子VIII (FVIII)替代疗法仍然是a型血友病的主要治疗方法,然而,FVIII抗体(抑制剂)的产生和FVIII产物半衰期短是主要并发症。红细胞可能妨碍药物从血浆中迅速清除。红细胞具有生物相容性和非免疫原性。本研究考察了人红细胞包膜FVIII的体外活性。方法采用低渗透透析技术将FVIII注入红细胞。FVIII活性测定采用活化部分凝血活素时间(APTT)进行分析。使用特异性单克隆抗体(abcam, uk),通过western blotting和流式细胞术检测FVIII在红细胞中的存在。此外,还测量了fviii载体红细胞的渗透脆性和血液学参数。结果FVIII不能穿过细胞膜,在载体红细胞表面发现大量的FVIII。流式细胞术结果显示,11%的载红细胞表面FVIII蛋白阳性。在两组(包括裂解物和非裂解物装载FVIII的红细胞)中,第一天观察到FVIII的最大激活,并且在第3天和第5天该因子的凝血活性逐渐降低。在1:50稀释时,两组FVIII活性在1:50稀释时差异显著,特别是在第5天。结论本研究旨在引入红细胞作为FVIII的合适载体,延长FVIII在有效和安全水平上的给药间隔时间。
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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