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Effects of Site-directed Mutagenesis of L469 in Helix-5 of Human Papillomavirus 16 L1 on Pentamer Formation
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作者 PAN Dong WANG Lincong +5 位作者 LIU Meiyi JIN Shi WANG Liyan YU Xianghui ZHA Xiao WU Yuqing 《Chemical Research in Chinese Universities》 SCIE CAS CSCD 2017年第3期392-399,共8页
Located at the carboxyl terminal of the human papillomavirus major capsid protein L1, helix-5(h5) is cru-cial to L1 folding and pentamer formation. Site-directed mutagenesis of the leucine residue on site 469 into l... Located at the carboxyl terminal of the human papillomavirus major capsid protein L1, helix-5(h5) is cru-cial to L1 folding and pentamer formation. Site-directed mutagenesis of the leucine residue on site 469 into lysine, alanine, serine and glycine was performed to explore the effect of the resultant mutations on L 1 pentamer formation. The soluble yields of the L1 pentamers of the L469A and L469K mutants were nearly two fold higher than that of the wild type. Molecular dynamics simulation was then performed to reveal the intrinsic mechanisms involved in the improvement of L 1 pentamer yield. Accordingly, the secondary structures of h5, β-G2, β-B1, β-C, β-D, and β-F were altered. The altered structures improved the hydrophobic interaction between h5 and fl-core "jelly" and the stability of h5. The hydrophobic surface area of residue 469 was reduced by 50% relative to that of the wild type. The C--O group of residue 469 and C--N group of L470 were both exposed to the solvent in the L469A mutant. These modifications may account for the increased solubility and stability and the promotion of pentamer formation induced by the point mutation. Therefore, the changes in the hydrophobic properties of h5 and the core structure determined the pentamer formation and solubility. This study may assist the development of a cost-effective platform for the production of prophylactic virus-like particle vaccines. 展开更多
关键词 Human papillomavirus Capsid protein helix-5 L1 pentamer
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孕晚期胎膜早破孕妇阴道内菌群变化、外周血单个核细胞FoxP3、STAT5表达及妊娠结局 被引量:4
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作者 王贝贝 马丽丽 曹宇新 《中国计划生育学杂志》 2022年第12期2816-2820,共5页
目的:孕晚期胎膜早破(PROM)孕妇阴道内菌群变化、外周血单个核细胞叉头翼状螺旋转录因子3(FoxP3)、信号转导与转录激活因子5(STAT5)表达及其妊娠结局分析。方法:收集2020年6月-2021年12月本院收治的PROM孕妇(PROM组)123例和正常妊娠晚... 目的:孕晚期胎膜早破(PROM)孕妇阴道内菌群变化、外周血单个核细胞叉头翼状螺旋转录因子3(FoxP3)、信号转导与转录激活因子5(STAT5)表达及其妊娠结局分析。方法:收集2020年6月-2021年12月本院收治的PROM孕妇(PROM组)123例和正常妊娠晚期孕妇(对照组)120例临床资料,检测分娩前阴道分泌物微生物分布,外周血单个核细胞FoxP3、STAT5 mRNA表达水平及血清IFN-γ、IL-12、IL-4、IL-10水平,分析两组阴道菌群分布与FoxP3、STAT5 mRNA表达水平的差异。结果:PROM组乳酸杆菌患者占比(51.2%)低于对照组(75.0%),革兰阳性杆菌(15.5%)、革兰阳性球菌(13.0%)、溶血性葡萄球菌(21.1%)、粪肠球菌(25.2%)、阴沟肠杆菌(17.9%)占比高于对照组(6.7%、5.0%、8.3%、10.0%、7.5%),外周血单个核细胞FoxP3(0.78±0.12)、STAT5 mRNA(1.04±0.22)表达水平均低于对照组(1.26±0.34、1.75±0.42)(均P<0.05);与对照组比较,PROM组血清IFN-γ、IL-12水平升高,IL-4、IL-10水平降低,且PROM组阴道微生态失调孕妇外周血单个核细胞FoxP3、STAT5 mRNA表达水平低于阴道微生态正常孕妇,妊娠结局不良者外周血单个核细胞FoxP3、STAT5 mRNA表达水平低于妊娠结局良好者(均P<0.05)。结论:PROM患者外周血单个核细胞FoxP3、STAT5 mRNA表达水平降低,与患者阴道内菌群变化和妊娠结局有关,可能是PROM发生的相关机制。 展开更多
关键词 孕晚期胎膜早破 阴道微生态失调 不良妊娠结局 叉头翼状螺旋转录因子3 信号转导与转录激活因子5
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