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双特异性抗体非共价复合物所载货物穿过 hCMEC/D3 血脑屏障模型的转胞吞作用。

Transcytosis of payloads that are non-covalently complexed to bispecific antibodies across the hCMEC/D3 blood-brain barrier model.

机构信息

Roche Pharma Research and Early Development (pRED), Therapeutic Modalities - Large Molecule Research, Roche Innovation Center Munich, D-82377 Penzberg, Germany.

Institute of Cell Biology and Immunology, University of Stuttgart, Allmandring 31, D-70569 Stuttgart, Germany.

出版信息

Biol Chem. 2018 Jun 27;399(7):711-721. doi: 10.1515/hsz-2017-0311.

Abstract

A transcellular shuttle system was generated for the delivery of non-covalently linked payloads across blood-brain barrier (BBB) endothelial cells. Transcytosis-enabling shuttles are composed of bispecific antibodies (bsAbs) that simultaneously bind transferrin receptor (TfR) and haptens such as digoxigenin or biocytinamide. Haptenylated payloads are attached to these vehicles via non-covalent hapten-antibody complexation. This enables targeting to and internalization into human BBB-derived microvascular endothelial hCMEC/D3 cells. In contrast to other shuttles, this system does not require special affinities or formats of their TfR-binding moieties for transcytosis and subsequent release. Non-covalent payload complexation to bsAb is flexible and robust, works for a multitude of payloads and enables separation of payloads from shuttles during transcytosis. Released payloads can enter the brain without connected bsAb entities, minimizing potential interference with distribution or functionality. Intracellular separation of shuttle and payload and recycling to cell surfaces may also enable recharging of the cell-bound BBB shuttle with payload for subsequent (merry-go-round) transport cycles.

摘要

一种跨细胞穿梭系统被构建用于将非共价连接的有效载荷递送至血脑屏障 (BBB) 内皮细胞。穿梭系统由双特异性抗体 (bsAb) 组成,该抗体同时结合转铁蛋白受体 (TfR) 和半抗原如地高辛或生物胞嘧啶酰胺。半抗原化的有效载荷通过非共价半抗原-抗体复合物连接到这些载体上。这使得能够靶向并内化到源自人 BBB 的微血管内皮 hCMEC/D3 细胞中。与其他穿梭系统不同,该系统不需要其 TfR 结合部分的特殊亲和力或格式即可进行胞吞作用和随后的释放。非共价有效载荷与 bsAb 的复合具有灵活性和稳健性,适用于多种有效载荷,并能够在胞吞作用过程中使有效载荷与穿梭系统分离。释放的有效载荷可以进入大脑而不与连接的 bsAb 实体结合,最大程度地减少了对分布或功能的潜在干扰。穿梭系统和有效载荷的细胞内分离以及向细胞表面的再循环也可能使细胞结合的 BBB 穿梭系统能够用有效载荷再充电,以进行随后的(循环)运输循环。

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