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用于跨越人血脑屏障进行药物靶向的抗人胰岛素受体抗体人源化

Humanization of anti-human insulin receptor antibody for drug targeting across the human blood-brain barrier.

作者信息

Boado Ruben J, Zhang Yufeng, Zhang Yun, Pardridge William M

机构信息

ArmaGen Technologies, Inc., Santa Monica, California 90401, USA.

出版信息

Biotechnol Bioeng. 2007 Feb 1;96(2):381-91. doi: 10.1002/bit.21120.

DOI:10.1002/bit.21120
PMID:16937408
Abstract

A murine monoclonal antibody (MAb) to the human insulin receptor (HIR) has been engineered for use as a brain drug delivery system for transport across the human blood-brain barrier (BBB). The HIRMAb was humanized by complementarity determining region (CDR) grafting on the framework regions (FR) of the human B43 IgG heavy chain and the human REI kappa light chain. A problem encountered in the humanization process was the poor secretion of the CDR-grafted HIRMAb by myeloma cells. This problem was solved by the production of human/mouse hybrids of the engineered heavy chain variable region (VH), which led to the replacement of five amino acids in the FR3 of the VH with original murine amino acids. No replacement of FR amino acids in the light chain variable region (VL) was required. The affinity of the humanized HIRMAb for the HIR was decreased 27% relative to the murine HIRMAb. The humanized HIRMAb avidly bound to the HIR of isolated human brain capillaries, which are used as an in vitro model system of the human BBB. The HIRMAb cross reacts with the HIR of Old World primates such as the Rhesus monkey. The humanized HIRMAb was radiolabeled with 125-iodine, and injected intravenously into an adult, anesthetized Rhesus monkey. Brain scanning showed the humanized HIRMAb was rapidly transported into all parts of the primate brain after intravenous administration. The humanized HIRMAb may be used as a brain drug and gene delivery system for the targeting of large molecule therapeutics across the BBB in humans.

摘要

一种针对人胰岛素受体(HIR)的鼠单克隆抗体(MAb)已被改造,用作穿越人血脑屏障(BBB)的脑药物递送系统。通过将互补决定区(CDR)嫁接到人B43 IgG重链和人REIκ轻链的框架区(FR)上,使HIRMAb人源化。人源化过程中遇到的一个问题是骨髓瘤细胞分泌CDR嫁接的HIRMAb的能力较差。通过产生工程化重链可变区(VH)的人/鼠杂种解决了这个问题,这导致VH的FR3中的五个氨基酸被原始鼠氨基酸取代。轻链可变区(VL)中的FR氨基酸无需替换。人源化HIRMAb对HIR的亲和力相对于鼠HIRMAb降低了27%。人源化HIRMAb与分离的人脑毛细血管的HIR紧密结合,人脑毛细血管用作人血脑屏障的体外模型系统。HIRMAb与旧世界灵长类动物如恒河猴的HIR发生交叉反应。将人源化HIRMAb用125碘进行放射性标记,并静脉注射到一只成年麻醉恒河猴体内。脑部扫描显示,静脉给药后人源化HIRMAb迅速转运到灵长类动物大脑的所有部位。人源化HIRMAb可作为一种脑药物和基因递送系统,用于在人类中靶向大分子治疗药物穿越血脑屏障。

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