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利用靶向低密度脂蛋白受体的肽载体实现货物跨血脑屏障运输。

Use of LDL receptor-targeting peptide vectors for and cargo transport across the blood-brain barrier.

作者信息

Molino Yves, David Marion, Varini Karine, Jabès Françoise, Gaudin Nicolas, Fortoul Aude, Bakloul Karima, Masse Maxime, Bernard Anne, Drobecq Lucile, Lécorché Pascaline, Temsamani Jamal, Jacquot Guillaume, Khrestchatisky Michel

机构信息

Vect-Horus S.A.S., Faculté de Médecine, Marseille, France; and.

Aix Marseille Université, Centre National de la Recherche Scientifique, Neurobiologie des Interactions Cellulaires et Neurophysiopathologie, Marseille, France.

出版信息

FASEB J. 2017 May;31(5):1807-1827. doi: 10.1096/fj.201600827R. Epub 2017 Jan 20.

Abstract

The blood-brain barrier (BBB) prevents the entry of many drugs into the brain and, thus, is a major obstacle in the treatment of CNS diseases. There is some evidence that the LDL receptor (LDLR) is expressed at the BBB and may participate in the transport of endogenous ligands from blood to brain, a process referred to as receptor-mediated transcytosis. We previously described a family of peptide vectors that were developed to target the LDLR. In the present study, BBB models that were derived from wild-type and LDLR-knockout animals ( ) were used to validate the specific LDLR-dependent transcytosis of LDL a nondegradative route. We next showed that LDLR-targeting peptide vectors, whether in fusion or chemically conjugated to an Ab Fc fragment, promote binding to apical LDLR and transendothelial transfer of the Fc fragment across BBB monolayers the same route as LDL. Finally, we demonstrated that LDLR significantly contributes to the brain uptake of vectorized Fc. We thus provide further evidence that LDLR is a relevant receptor for CNS drug delivery receptor-mediated transcytosis and that the peptide vectors we developed have the potential to transport drugs, including proteins or Ab based, across the BBB.-Molino, Y., David, M., Varini, K., Jabès, F., Gaudin, N., Fortoul, A., Bakloul, K., Masse, M., Bernard, A., Drobecq, L., Lécorché, P., Temsamani, J., Jacquot, G., Khrestchatisky, M. Use of LDL receptor-targeting peptide vectors for and cargo transport across the blood-brain barrier.

摘要

血脑屏障(BBB)会阻止许多药物进入大脑,因此是中枢神经系统疾病治疗中的一个主要障碍。有证据表明,低密度脂蛋白受体(LDLR)在血脑屏障处表达,可能参与内源性配体从血液到大脑的转运,这一过程称为受体介导的转胞吞作用。我们之前描述了一类为靶向LDLR而开发的肽载体。在本研究中,使用源自野生型和LDLR基因敲除动物的血脑屏障模型来验证LDL通过非降解途径进行的特定LDLR依赖性转胞吞作用。接下来我们表明,靶向LDLR的肽载体,无论是与抗体Fc片段融合还是化学偶联,都能促进与顶端LDLR的结合以及Fc片段通过血脑屏障单层的跨内皮转运,其途径与LDL相同。最后,我们证明LDLR对载体化Fc的脑摄取有显著贡献。因此,我们进一步证明LDLR是中枢神经系统药物递送中通过受体介导的转胞吞作用的相关受体,并且我们开发的肽载体有潜力转运包括蛋白质或基于抗体的药物穿过血脑屏障。——莫利诺,Y.,大卫,M.,瓦里尼,K.,雅贝斯,F.,高丹,N.,福尔图尔,A.,巴克洛,K.,马斯,M.,伯纳德,A.,德罗贝克,L.,勒科尔谢,P.,泰萨马尼,J.,雅库,G.,克雷斯查蒂斯基,M. 利用靶向低密度脂蛋白受体的肽载体实现血脑屏障的药物递送和货物转运

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