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  • On the shuttling across the blood-brain barrier via tubule formation: Mechanism and cargo avidity bias.

On the shuttling across the blood-brain barrier via tubule formation: Mechanism and cargo avidity bias.

Science advances (2020-11-29)
Xiaohe Tian, Diana M Leite, Edoardo Scarpa, Sophie Nyberg, Gavin Fullstone, Joe Forth, Diana Matias, Azzurra Apriceno, Alessandro Poma, Aroa Duro-Castano, Manish Vuyyuru, Lena Harker-Kirschneck, Anđela Šarić, Zhongping Zhang, Pan Xiang, Bin Fang, Yupeng Tian, Lei Luo, Loris Rizzello, Giuseppe Battaglia
摘要

The blood-brain barrier is made of polarized brain endothelial cells (BECs) phenotypically conditioned by the central nervous system (CNS). Although transport across BECs is of paramount importance for nutrient uptake as well as ridding the brain of waste products, the intracellular sorting mechanisms that regulate successful receptor-mediated transcytosis in BECs remain to be elucidated. Here, we used a synthetic multivalent system with tunable avidity to the low-density lipoprotein receptor-related protein 1 (LRP1) to investigate the mechanisms of transport across BECs. We used a combination of conventional and super-resolution microscopy, both in vivo and in vitro, accompanied with biophysical modeling of transport kinetics and membrane-bound interactions to elucidate the role of membrane-sculpting protein syndapin-2 on fast transport via tubule formation. We show that high-avidity cargo biases the LRP1 toward internalization associated with fast degradation, while mid-avidity augments the formation of syndapin-2 tubular carriers promoting a fast shuttling across.

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Triton X-100, laboratory grade
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MISSION® esiRNA, targeting human PACSIN2