期刊文献+
共找到2篇文章
< 1 >
每页显示 20 50 100
RMK-03^(TM)皮肤黏膜护理喷剂对上呼吸道黏膜免疫功能低下小鼠免疫调节机制的影响 被引量:2
1
作者 冒昊天 江国荣 +2 位作者 梁国强 林琳 徐俊华 《抗感染药学》 2021年第12期1738-1744,共7页
目的:通过寒冷致小鼠上呼吸道黏膜免疫功能低下(upper airway immunity dysfunction,UAID)模型的实验,基于免疫球蛋白A单克隆抗体(immunoglobulin A monoclonal antibody,IgA MAb)阻断新型冠状病毒(SARSCoV-2)的Spike-ACE 2相互作用探究... 目的:通过寒冷致小鼠上呼吸道黏膜免疫功能低下(upper airway immunity dysfunction,UAID)模型的实验,基于免疫球蛋白A单克隆抗体(immunoglobulin A monoclonal antibody,IgA MAb)阻断新型冠状病毒(SARSCoV-2)的Spike-ACE 2相互作用探究RMK-03^(TM)喷剂对上呼吸道黏膜的免疫调节机制。方法:将40只SPF级ICR小鼠分为正常组、UAID模型组、利巴韦林喷雾剂组、RMK-03;喷雾剂组4组,每组10只;利巴韦林喷剂组和RMK-03^(TM)喷剂组先给予口腔喷雾0.1 mL/只q12h,给药3 d,;第3 d,除正常组外其他各组小鼠复制UAID模型,即将小鼠放入-20℃寒冷环境中15 min,之后在室温适应1 h,经腹腔注射毛果芸香碱滴眼液(0.25 mL/只),2 min后以安乐处死小鼠,取口腔、咽喉部黏膜组织进行HE病理学切片检查,以Western blotting法考察其IgA、pIgR蛋白的表达,采用ELISA法检测细胞因子IL-4、IL-6和IFN-γ、TNF-α含量;采用免疫组化法检测ACE 2和ACE的表达情况。结果:UAID模型组小鼠唾液中SIgA含量显著低于正常组(P<0.05),提示模型复制成功;与正常组相比,UAID模型组小鼠的口腔和咽喉黏膜组织可见轻度间质水肿、小血管扩张充血,中性粒细胞伴有淋巴管轻度扩张水肿;UAID模型组小鼠口腔、咽喉部黏膜组织IgA、pIgR蛋白表达,IgA相关细胞因子IL-4、IL-6的含量及pIgR相关细胞因子IFN-γ、TNF-α的含量均显著低于正常组(P<0.05),该组的ACE、ACE 2平均光密度值(IOD/area)均显著性高于正常组(P<0.05);利巴韦林喷剂组和RMK-03;喷剂组的上述主要指标均在不同程度上优于UAID模型组,且后者的上述主要指标优于前者。结论:RMK-03^(TM)皮肤黏膜护理喷剂通过调节局部黏膜免疫屏障低下相关IgA的含量,抑制呼吸道黏膜中ACE 2活性表达,间接推测其阻断SARS-CoV-2的Spike-ACE 2相互作用以提供黏膜免疫。 展开更多
关键词 RMK-03^(TM)喷剂 呼吸道黏膜免疫功能 IgA/pIgR SARS-CoV-2 spike-ace 2
下载PDF
Evidence for a mouse origin of the SARS-CoV-2 Omicron variant 被引量:22
2
作者 Changshuo Wei Ke-Jia Shan +3 位作者 Weiguang Wang Shuya Zhang Qing Huan Wenfeng Qian 《Journal of Genetics and Genomics》 SCIE CAS CSCD 2021年第12期1111-1121,共11页
The rapid accumulation of mutations in the SARS-CoV-2 Omicron variant that enabled its outbreak raises questions as to whether its proximal origin occurred in humans or another mammalian host. Here, we identified 45 p... The rapid accumulation of mutations in the SARS-CoV-2 Omicron variant that enabled its outbreak raises questions as to whether its proximal origin occurred in humans or another mammalian host. Here, we identified 45 point mutations that Omicron acquired since divergence from the B.1.1 lineage. We found that the Omicron spike protein sequence was subjected to stronger positive selection than that of any reported SARS-CoV-2 variants known to evolve persistently in human hosts, suggesting a possibility of hostjumping. The molecular spectrum of mutations(i.e., the relative frequency of the 12 types of base substitutions) acquired by the progenitor of Omicron was significantly different from the spectrum for viruses that evolved in human patients but resembled the spectra associated with virus evolution in a mouse cellular environment. Furthermore, mutations in the Omicron spike protein significantly overlapped with SARS-CoV-2 mutations known to promote adaptation to mouse hosts, particularly through enhanced spike protein binding affinity for the mouse cell entry receptor. Collectively, our results suggest that the progenitor of Omicron jumped from humans to mice, rapidly accumulated mutations conducive to infecting that host,then jumped back into humans, indicating an inter-species evolutionary trajectory for the Omicron outbreak. 展开更多
关键词 SARS-CoV-2 Omicron Evolutionary origins Molecular spectrum of mutations spike-ace2 interaction Receptor-binding domain
原文传递
上一页 1 下一页 到第
使用帮助 返回顶部