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作 者:Hong Wu Hongyan Li Yiqiang Liu Jingchen Liang Qianshi Liu Zhigang Xu Zhongzhu Chen Xia Zhang Kun Zhang Chuan Xu
机构地区:[1]Integrative Cancer Center&Cancer Clinical Research Center,Sichuan Cancer Hospital&Institute,Sichuan Cancer Center School of Medicine,University of Electronic Science and Technology of China,No.55,Section 4,South Ren-min Road,Chengdu,610042,Sichuan,PR China [2]Department of Medical Ultrasound and Central Laboratory,Shanghai Tenth People’s Hospital,Ultrasound Research and Education Institute,Tongji University School of Medicine,No.301 Yan-chang-zhong Road,Shanghai,200072,PR China [3]International Academy of Targeted Therapeutics and Innovation,Chongqing University of Arts and Sciences,NO.319,Red River Avenue,Yong-chuan,402160,Chongqing,PR China [4]Institute of Pathology and Southwest Cancer Center,Southwest Hospital,Third Military Medical University(Army Medical University),NO.30,Gao-tan-yan-zheng Street,Chongqing,400038,PR China
出 处:《Bioactive Materials》2022年第7期223-238,共16页生物活性材料(英文)
基 金:This work was supported by the National Natural Science Foundation of China(82022033,81873048,81771836 and 82004006);Sichuan Provincial Science Fund for applied basic research of China(2020YJ0108);Sichuan Provincial Science Fund for Distinguished Young Scholars of China(2020JDJQ0065).
摘 要:The presence of multiple immunosuppressive targets and insufficient activation and infiltration of cytotoxic T lymphocytes(CTLs)allow tumor cells to escape immune surveillance and disable anti-PD-1/PD-L1 immunotherapy.Nanobiotechnology-engineered autologous tumor vaccines(ATVs)that were camouflaged by tumor cell membrane(TCM)were designed to activate and facilitate CTLs infiltration for killing the unprotected lung tumor cells,consequently realizing the sequential immunotherapy.PDE5 was firstly screened out as a new immunosuppressive target of lung cancer in clinical practice.Immediately afterwards,phosphodiesterase-5(PDE5)and programmed cell death 1 ligand 1(PD-L1)dual-target co-inhibition was proposed to unfreeze the immunosuppressive microenvironment of NSCLC.Systematic studies validated that this ATVs-unlocked sequential immunotherapy after co-encapsulating PDE5 inhibitor and NO donor(i.e.,L-arginine)exerted robust anti-tumor effects through increasing inducible nitric oxide synthase(iNOS)expression,blockading PDE5 pathway and activating systematic immune responses,which synergistically eradicated local and abscopal lung cancers in either orthotopic or subcutaneous models.The pluripotent ATVs that enable PDE5 inhibition and sequential immunotherapy provide a new avenue to mitigate immunosuppressive microenvironment and magnify anti-PD-1/PD-L1 immunotherapy.
关 键 词:Autologous tumor vaccines(ATVs) Sequential immunotherapy Immunosuppressive microenvironment Tumor tropism Immune escape target
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