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Molecular basis for rational construction of RVGP modified liposomal delivery system targeting to brain
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作者 Bo Deng Wei Cui +5 位作者 Shuang Ma Xiaona Liu Zhan Zhang baiyi yan Kun Chen Ying Xie 《Journal of Chinese Pharmaceutical Sciences》 CAS CSCD 2019年第7期484-501,共18页
The rational construction of active targeting liposomes will provide an important structural support for its effective brain targeting.However,there is no clear understanding of the structure-activity relationship of ... The rational construction of active targeting liposomes will provide an important structural support for its effective brain targeting.However,there is no clear understanding of the structure-activity relationship of active targeting liposomes.Combining multiscale computational simulation and experimental verification,we established a computational model of RVGP modified PEGylated liposomes(RVGP-PEG-L)and investigated the role of PEG and molecular interaction mechanism of carrier-ligand-receptor.The result indicated that the complex network conformation formed by PEG with 42 monomers(42 PEG)above the density of 8%was the molecular basis for PEG-L to achieve long-circulation function.The lowest monomer number of PEG linker to ensure the targeting ability of RVGP was 42.However,the pose of RVGP binding to nAChR changed after it was linked with PEG-L due to the restraint of PEG chain,leading to a decrease of binding free energy.Increasing the monomer number of PEG linker or improving the non-polarity of polymers was a potential strategy to enhance the combination of RVGP-PEG-L with nAChR on the targeting cell. 展开更多
关键词 Multiscale dynamic simulation Liposomes Molecular interaction mechanism Rational construction
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