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Icaritin inhibits the progression of urothelial cancer by suppressing PADI2-mediated neutrophil infiltration and neutrophil extracellular trap formation
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作者 Zezhong Mou Yiling chen +10 位作者 Jinzhong Hu Yun Hu Lujia Zou xinan chen Shenghua Liu Qiuping Yin Jian Gong Shuchen Li Shanhua Mao chenyang Xu Haowen Jiang 《Acta Pharmaceutica Sinica B》 SCIE CAS CSCD 2024年第9期3916-3930,共15页
Tumor relapse and metastasis are the major causes of mortality associated with urothelial cancer.In the tumor microenvironment,negative regulatory molecules and various immune cell subtypes suppress antitumor immunity... Tumor relapse and metastasis are the major causes of mortality associated with urothelial cancer.In the tumor microenvironment,negative regulatory molecules and various immune cell subtypes suppress antitumor immunity.The inflammatory microenvironment,associated with neutrophils and neutrophil extracellular traps(NETs),promotes tumor metastasis.However,no drugs are currently available to specifically inhibit neutrophils and NETs.In this study,we first demonstrated that icaritin(ICT),a Chinese herbal remedy that is a first-line treatment for advanced and incurable hepatocellular carcinoma,reduces NETs caused by suicidal NETosis and prevents neutrophil infiltration in the tumor microenvironment.Mechanistically,ICT binds to and inhibits the expression of PADI2 in neutrophils,thereby suppressing PADI2-mediated histone citrullination.Moreover,ICT inhibits ROS generation,suppresses the MAPK signaling pathway,and inhibits NET-induced tumor metastasis.Simultaneously,ICT inhibits tumoral PADI2-mediated histone citrullination,which consequently suppresses the transcription of neutrophil-recruiting genes such as GM-CSF and IL-6.The downregulation of IL-6 expression,in turn,forms a regulatory feedback loop through the JAK2/STAT3/IL-6 axis.Through a retrospective study of clinical samples,we found a correlation between neutrophils,NETs,UCa prognosis,and immune evasion.Combining ICT with immune checkpoint inhibitors may have synergistic effects.In summary,our study demonstrated that ICT could be a novel inhibitor of NETs and a novel UCa treatment. 展开更多
关键词 ICARITIN NEUTROPHIL Neutrophil extracellular trap PADI2 Urothelial cancer
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弓形虫优势表位融合于HPV16L1“N端”的融合体可显著提高表位免疫反应性
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作者 谭晓淳 林中民 +3 位作者 吕金辉 谢自新 陈薪安 李文姝 《生物工程学报》 CAS CSCD 北大核心 2021年第1期290-300,共11页
弓形虫和人乳头瘤病毒(HPV)具有共同的免疫保护人群,选择HPV16型晚期结构蛋白1(HPV16L1)为载体,携带弓形虫多表位(RSepitope)以期提高表位免疫原性同时可实现共免疫效应。文中分别以构建的融合体RSepitope-HPV16L1(RSepitope融合于HPV16... 弓形虫和人乳头瘤病毒(HPV)具有共同的免疫保护人群,选择HPV16型晚期结构蛋白1(HPV16L1)为载体,携带弓形虫多表位(RSepitope)以期提高表位免疫原性同时可实现共免疫效应。文中分别以构建的融合体RSepitope-HPV16L1(RSepitope融合于HPV16L1"N"端)以及HPV16L1-RSepitope(RSepitope融合于HPV16L1"C"端),脂质体转染COS-7细胞后,RSepitope-HPV16L1融合体形式可以在转染细胞中得到有效转录和翻译,分别可检测到相应的RSepitope和HPV16L1的mRNA和蛋白,但HPV16L1-RSepitope融合体形式在转染细胞中检测不到目标抗原的mRNA和蛋白。融合体采用"DNA初免-蛋白质加强免疫"的方案免疫BALB/c小鼠,酶联免疫吸附试验(ELISA)和酶联免疫斑点试验(ELISPOT)分别检测到RSepitope-HPV16L1免疫鼠血清中显著升高的体液和细胞免疫反应(即最高水平的RSepitope特异性抗体IgG和IFN-γ),且比较单独RSepitope免疫组(不与HPV16L1融合),产生的是显著升高的Th1和Th2免疫反应类型,提示HPV16L1作为表位载体的优势效应。而HPV16L1-RSepitope融合体形式体内也未能诱导有效的免疫反应。以上研究提示,HPV16L1"N"端可能是较为合适的表位融合位置,融合体表位特异性免疫学效应显著提高,研究结果为提高表位疫苗的免疫原性提供了一个合理的载体融合策略。 展开更多
关键词 弓形虫 HPV16L1 融合体 免疫效应
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