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与中性抗生物素蛋白和阳离子化人白蛋白偶联物结合的生物素向脑内的递送。

Brain delivery of biotin bound to a conjugate of neutral avidin and cationized human albumin.

作者信息

Kang Y S, Pardridge W M

机构信息

Department of Medicine, UCLA School of Medicine 90024.

出版信息

Pharm Res. 1994 Sep;11(9):1257-64. doi: 10.1023/a:1018982125649.

DOI:10.1023/a:1018982125649
PMID:7816753
Abstract

The delivery of pharmaceuticals through the brain capillary endothelial wall, which makes up the blood-brain barrier (BBB) in vivo, may be facilitated by conjugation of therapeutics to brain drug delivery vectors. Since cationized albumin has been shown to undergo absorptive-mediated transcytosis through the BBB in vivo, cationized human serum albumin (cHSA) is a potential brain drug delivery vector in humans. Conjugation of biotinylated therapeutics to brain drug delivery vectors is facilitated by the preparation of vector/avidin conjugates. Therefore, the present studies describe the preparation of a cHSA-avidin conjugate and the delivery of 3H-biotin bound to this conjugate through the BBB in vivo in anesthetized rats. Since the cationic nature of avidin (AV) accelerates the removal of avidin-based conjugates from blood in vivo, the present studies also describe the preparation and the pharmacokinetics of 3H-biotin bound to a conjugate of cHSA and neutral avidin (NLA). The bifunctional nature of the conjugate was retained: the cHSA/NLA conjugate contained 2.8 to 6.8 biotin binding sites per conjugate, and the BBB permeability-surface area (PS) product for 3H-biotin bound to cHSA/NLA was at least 7-fold greater than the BBB PS product for 3H-biotin bound to a conjugate of NLA and native HSA (nHSA). The systemic clearance of the cHSA conjugate was reduced 10-fold by the use of NLA as opposed to AV. The increased area under the plasma concentration curve (AUC) of the cHSA-NLA conjugate correlated with an increase in brain delivery of 3H-biotin as compared to the brain delivery achieved with the cHSA/AV conjugate.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

通过构成体内血脑屏障(BBB)的脑毛细血管内皮壁递送药物,可通过将治疗药物与脑药物递送载体偶联来促进。由于已证明阳离子化白蛋白在体内可通过BBB进行吸附介导的转胞吞作用,因此阳离子化人血清白蛋白(cHSA)是人类潜在的脑药物递送载体。通过制备载体/抗生物素蛋白偶联物,可促进生物素化治疗药物与脑药物递送载体的偶联。因此,本研究描述了cHSA-抗生物素蛋白偶联物的制备,以及与该偶联物结合的3H-生物素在麻醉大鼠体内通过BBB的递送。由于抗生物素蛋白(AV)的阳离子性质会加速基于抗生物素蛋白的偶联物在体内从血液中的清除,本研究还描述了与cHSA和中性抗生物素蛋白(NLA)的偶联物结合的3H-生物素的制备及其药代动力学。偶联物的双功能性质得以保留:cHSA/NLA偶联物每个偶联物含有2.8至6.8个生物素结合位点,与NLA和天然HSA(nHSA)的偶联物结合的3H-生物素的BBB通透性-表面积(PS)乘积相比,与cHSA/NLA结合的3H-生物素的BBB PS乘积至少大7倍。与使用AV相比,使用NLA可使cHSA偶联物的全身清除率降低10倍。与cHSA/AV偶联物实现的脑递送相比,cHSA-NLA偶联物体内血浆浓度曲线下面积(AUC)的增加与3H-生物素脑递送的增加相关。(摘要截短于250字)

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