The blood-brain barrier transmigrating single domain antibody: mechanisms of transport and antigenic epitopes in human brain endothelial cells.

Abulrob A; Sprong H; Van Bergen en Henegouwen P; Stanimirovic D

首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >The blood-brain barrier transmigrating single domain antibody: mechanisms of transport and antigenic epitopes in human brain endothelial cells.

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The blood-brain barrier transmigrating single domain antibody: mechanisms of transport and antigenic epitopes in human brain endothelial cells.

机译：血脑屏障迁移单结构域抗体：人脑内皮细胞中的运输机制和抗原表位。

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Antibodies against receptors that undergo transcytosis across the blood-brain barrier (BBB) have been used as vectors to target drugs or therapeutic peptides into the brain. We have recently discovered a novel single domain antibody, FC5, which transmigrates across human cerebral endothelial cells in vitro and the BBB in vivo. The purpose of this study was to characterize mechanisms of FC5 endocytosis and transcytosis across the BBB and its putative receptor on human brain endothelial cells. The transport of FC5 across human brain endothelial cells was polarized, charge independent and temperature dependent, suggesting a receptor-mediated process. FC5 taken up by human brain endothelial cells co-localized with clathrin but not with caveolin-1 by immunochemistry and was detected in clathrin-enriched subcellular fractions by western blot. The transendothelial migration of FC5 was reduced by inhibitors of clathrin-mediated endocytosis, K+ depletion and chlorpromazine, but was insensitive to caveolae inhibitors, filipin, nystatin or methyl-beta-cyclodextrin. Following internalization, FC5 was targeted to early endosomes, bypassed late endosomes/lysosomes and remained intact after transcytosis. The transcytosis process was inhibited by agents that affect actin cytoskeleton or intracellular signaling through PI3-kinase. Pretreatment of human brain endothelial cells with wheatgerm agglutinin, sialic acid, alpha(2,3)-neuraminidase or Maackia amurensis agglutinin that recognizes alpha(2,3)-, but not with Sambucus nigra agglutinin that recognizes alpha(2,6) sialylgalactosyl residues, significantly reduced FC5 transcytosis. FC5 failed to recognize brain endothelial cells-derived lipids, suggesting that it binds luminal alpha(2,3)-sialoglycoprotein receptor which triggers clathrin-mediated endocytosis. This putative receptor may be a new target for developing brain-targeting drug delivery vectors.

机译：针对通过血脑屏障（BBB）进行胞吞作用的受体的抗体已用作将药物或治疗性肽靶向大脑的载体。我们最近发现了一种新颖的单结构域抗体FC5，该抗体在体外和人体内的BBB跨人脑内皮细胞迁移。这项研究的目的是表征FC5内吞和跨BBB的转运作用及其在人脑内皮细胞上的推定受体的机制。 FC5在人脑内皮细胞中的转运是极化的，不依赖电荷且依赖温度，表明受体介导的过程。通过免疫化学方法，人脑内皮细胞摄取的FC5与网格蛋白共定位，而与小窝蛋白1共定位，并通过Western blot在富含网格蛋白的亚细胞级分中检测到。网格蛋白介导的内吞作用，K +耗竭和氯丙嗪的抑制剂可减少FC5的跨内皮迁移，但对小窝抑制剂，菲律宾磷脂，制霉菌素或甲基β-环糊精不敏感。内化后，FC5靶向早期内体，绕过晚期内体/溶酶体，并在转胞吞作用后保持完整。通过PI3-激酶影响肌动蛋白细胞骨架或细胞内信号转导的药物抑制了转胞吞作用。用小麦胚芽凝集素，唾液酸，α（2,3）-神经氨酸酶或Maackia amurensis凝集素预处理可识别α（2,3）-的人脑内皮细胞，但不使用识别α（2,6）唾液酸半乳糖基的黑接骨凝集素进行预处理残基，显着减少FC5的胞吞作用。 FC5无法识别脑内皮细胞来源的脂质，表明它结合了腔内α（2,3）-唾液糖蛋白受体，从而触发网格蛋白介导的内吞作用。该推定的受体可能是开发靶向脑的药物递送载体的新靶标。

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《Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry》 |2005年第4期|共14页
作者
Abulrob A; Sprong H; Van Bergen en Henegouwen P; Stanimirovic D;
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正文语种 eng
中图分类神经病学与精神病学;
关键词
Brain; Endothelial cell; Human; Blood-Brain Barrier; 脑; 血脑屏障;

机译：Brain;Endothelial cell;Human;Blood-Brain Barrier;脑;血脑屏障;

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专利

1. The blood-brain barrier transmigrating single domain antibody: mechanisms of transport and antigenic epitopes in human brain endothelial cells. [J] . Abulrob A, Sprong H, Van Bergen en Henegouwen P, Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry . 2005,第4期

机译：血脑屏障迁移单结构域抗体：人脑内皮细胞中的运输机制和抗原表位。
2. Comparison of ABC transporter modulation by atazanavir in lymphocytes and human brain endothelial cells: ABC transporters are involved in the atazanavir-limited passage across an in vitro human model of the blood-brain barrier. [J] . Bousquet L, Roucairol C, Hembury A, AIDS Research and Human Retroviruses . 2008,第9期

机译：Atazanavir在淋巴细胞和人脑内皮细胞中对ABC转运蛋白调节的比较：ABC转运蛋白参与了atazanavir限制的跨血脑屏障体外人类模型的传代。
3. Developing brain cells produce factors capable of inducing the HT7 antigen, a blood-brain barrier-specific molecule, in chick endothelial cells. [J] . Ikeda E, Flamme I, Risau W Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences . 1996,第3期

机译：发育中的脑细胞产生能够在鸡内皮细胞中诱导HT7抗原（一种血脑屏障特异性分子）的因子。
4. Single-Domain Antibody-Mediated Delivery of Therapeutics across the Blood-Brain Barrier [C] . D. Stanimirovic, A. Abulrob U. Iqbal, A. Haqqani, Annual meeting exposition of the Controlled Release Society . 2011

机译：跨血脑屏障的单域抗体介导的药物治疗
5. Positional and functional epitope mapping of endoglin, a proliferation-associated antigen of human endothelial cells. [D] . She, Xinwei. 2003

机译：内皮糖蛋白的位置和功能表位作图，内皮糖蛋白是人内皮细胞的一种增殖相关抗原。
6. Functional Expression of P-glycoprotein and Organic Anion Transporting Polypeptides at the Blood-Brain Barrier: Understanding Transport Mechanisms for Improved CNS Drug Delivery? [O] . Wazir Abdullahi, Thomas P. Davis, Patrick T. Ronaldson -1

机译：P-糖蛋白和有机阴离子转运多肽在血脑屏障中的功能表达：了解改善中枢神经系统药物递送的转运机制？
7. The blood-brain barrier transmigrating single domain antibody: mechanisms of transport and antigenic epitopes in human brain endothelial cells. [O] . Abulrob, Abedelnasser, Sprong, Hein, Van Bergen En Henegouwen, Paul, 2005

机译：血脑屏障迁移单结构域抗体：人脑内皮细胞中的运输机制和抗原表位。

The blood-brain barrier transmigrating single domain antibody: mechanisms of transport and antigenic epitopes in human brain endothelial cells.

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