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帕比纳夫斯帕 Alfa 的转铁蛋白受体靶向特性促进了它被各种类型的人脑衍生细胞摄取。

Transferrin receptor-targeting property of pabinafusp alfa facilitates its uptake by various types of human brain-derived cells .

作者信息

Fukatsu Tomoki, Morio Hanae, Furihata Tomomi, Sonoda Hiroyuki

机构信息

JCR Pharmaceuticals, Research Division, Kobe, Japan.

Laboratory of Clinical Pharmacy and Experimental Therapeutics, School of Pharmacy, Tokyo University of Pharmacy and Life Sciences, Tokyo, Japan.

出版信息

Front Drug Deliv. 2023 Jul 3;3:1082672. doi: 10.3389/fddev.2023.1082672. eCollection 2023.

Abstract

Pabinafusp alfa, which is an anti-mucopolysaccharidosis II drug, consists of iduronate-2-sulfatase (IDS) genetically fused with an anti-transferrin receptor (TfR) antibody. While IDS is known to enter cells via mannose-6-phosphate receptor (M6PR)-mediated endocytosis, the anti-TfR antibody moiety of pabinafusp alfa is supposed to trigger the TfR-mediated transcytosis involved in its blood-brain barrier (BBB) penetration to deliver IDS into the brain, which thus makes it effective for treatment of brain symptoms of the disease. However, since these uptake processes remain unexamined , this study aims at elucidating how human brain cells manipulate these receptors to facilitate pabinafusp alfa uptake. The results of pabinafusp alfa uptake assays showed that the TfR played an primary role in its uptake by brain microvascular endothelial cells. The TfR contribution was also found in neuronal cells at levels comparable to M6PR. Interestingly, the predominant roles of TfR over M6PR in pabinafusp alfa uptake were also observed in astrocytes and pericytes. To summarize, our results support the TfR-targeting strategy of pabinafusp alfa for facilitating its BBB penetration while simultaneously identifying previously unnoticed TfR roles in its uptake into human neuronal and non-neuronal brain cells. These findings are certain to provide important insights into the mechanisms behind clinical actions of pabinafusp alfa.

摘要

帕比纳夫斯帕 Alfa 是一种抗黏多糖贮积症 II 药物,由与抗转铁蛋白受体 (TfR) 抗体基因融合的艾杜糖醛酸 -2- 硫酸酯酶 (IDS) 组成。虽然已知 IDS 通过甘露糖 -6- 磷酸受体 (M6PR) 介导的内吞作用进入细胞,但帕比纳夫斯帕 Alfa 的抗 TfR 抗体部分应该触发参与其血脑屏障 (BBB) 穿透的 TfR 介导的转胞吞作用,从而将 IDS 输送到大脑中,这使其对治疗该疾病的脑部症状有效。然而,由于这些摄取过程尚未得到研究,本研究旨在阐明人类脑细胞如何操纵这些受体以促进帕比纳夫斯帕 Alfa 的摄取。帕比纳夫斯帕 Alfa 摄取试验的结果表明,TfR 在脑微血管内皮细胞摄取它的过程中起主要作用。在神经元细胞中也发现了 TfR 的作用,其水平与 M6PR 相当。有趣的是,在星形胶质细胞和周细胞中也观察到 TfR 在帕比纳夫斯帕 Alfa 摄取中比 M6PR 起更主要的作用。总之,我们的结果支持帕比纳夫斯帕 Alfa 靶向 TfR 的策略以促进其血脑屏障穿透,同时确定了以前未被注意到的 TfR 在其摄取到人类神经元和非神经元脑细胞中的作用。这些发现肯定会为帕比纳夫斯帕 Alfa 临床作用背后的机制提供重要见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3260/12363330/323ce7db4993/fddev-03-1082672-g001.jpg

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