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Merck
CN
  • Deliver anti-PD-L1 into brain by p-hydroxybenzoic acid to enhance immunotherapeutic effect for glioblastoma.

Deliver anti-PD-L1 into brain by p-hydroxybenzoic acid to enhance immunotherapeutic effect for glioblastoma.

Journal of controlled release : official journal of the Controlled Release Society (2020-01-10)
Haiyan Guo, Ruifeng Wang, Dongli Wang, Songli Wang, Jianfen Zhou, Zhilan Chai, Shengyu Yao, Jinyang Li, Linwei Lu, Yu Liu, Cao Xie, Weiyue Lu
摘要

In glioblastoma with typical immunosuppressive characteristics, immune checkpoint inhibitors treatment showed unsatisfactory clinical effects, attributable to the exclusion of antibodies by blood-brain barrier (BBB) to a large extent. Herein, a conjugate of anti-programmed death ligand 1 antibody (αPDL1) and the targeting moiety p-hydroxybenzoic acid (pHA) was designed to realize crossing BBB of antibody based on the dopamine receptor mediated transcytosis. Conjugation with pHA did not influence the binding affinity of αPDL1 with PD-L1 protein, thus maintaining the capability of PD pathway blockade. Importantly, pHA-αPDL1 crossed BBB, demonstrated by the increased distribution in both the brain and the glioma after intravenous administration of pHA-αPDL1. Compared with the unmodified αPDL1, pHA-αPDL1 prolonged the survival time and suppressed tumor growth more effectively in an orthotopic glioblastoma model by activating glioma-infiltrating T cells. Our results suggested the potential of the antibody-pHA conjugate to improve efficacy for cerebral diseases by providing a potential platform for macromolecules to play therapeutics role in the brain.

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Sigma-Aldrich
4-(N-马来酰亚胺甲基)环己烷-1-羧酸3-磺基-N-羟基琥珀酰亚胺酯 钠盐, powder