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UOOC平台与腾讯课堂相结合的“在线异步教学” 被引量:21
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作者 陈彦涛 胡惠媛 +3 位作者 杨波 任祥忠 李翠华 王国成 《大学化学》 CAS 2020年第5期115-120,共6页
新冠病毒大规模爆发,在线教学成为教师首选。而避免网络拥堵和保证学习效果是在线教学面临的两难问题。我们借助于UOOC平台和腾讯课堂,以“聚合物结构与性能”课程为样本,实践了新型“线上异步教学”模式。其中,SPOC课程便于学生自主安... 新冠病毒大规模爆发,在线教学成为教师首选。而避免网络拥堵和保证学习效果是在线教学面临的两难问题。我们借助于UOOC平台和腾讯课堂,以“聚合物结构与性能”课程为样本,实践了新型“线上异步教学”模式。其中,SPOC课程便于学生自主安排时间;“章节测验”和“生生互评”则有利于学生获得多角度反馈;小课题侧重于案例分析,引导学生开展探究式学习。总体而言,“在线异步教学”模式打破了教与学的时空限制,保证了疫情期间的教学质量,也为打造“金课”奠定了基础。 展开更多
关键词 在线教学 异步教学 翻转课堂 UOOC平台 腾讯课堂
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聚合物链状分子的构象统计——推荐一个高分子实验 被引量:1
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作者 陈彦涛 胡惠媛 +1 位作者 杨波 石玉磊 《大学化学》 CAS 2022年第7期115-120,共6页
介绍了利用分子模拟对链状分子进行构象统计的实验设计。选取常见且结构简单的聚乙烯作为研究对象,利用软件Materials Studio对聚乙烯进行建模,模拟其运动过程,在微观层面重现了链状分子构象,验证了构象尺寸的标度理论,有利于学生对链... 介绍了利用分子模拟对链状分子进行构象统计的实验设计。选取常见且结构简单的聚乙烯作为研究对象,利用软件Materials Studio对聚乙烯进行建模,模拟其运动过程,在微观层面重现了链状分子构象,验证了构象尺寸的标度理论,有利于学生对链构象建立形象化认知。该实验设计便于学生在个人电脑上操作,满足有限的实验课时要求。 展开更多
关键词 高分子实验 聚合物链 构象统计 分子模拟
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Gefitinib and fostamatinib target EGFR and SYK to attenuate silicosis:a multi-omics study with drug exploration 被引量:8
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作者 Mingyao Wang Zhe Zhang +15 位作者 Jiangfeng Liu Meiyue Song Tiantian Zhang Yiling Chen huiyuan hu Peiran Yang Bolun Li Xiaomin Song Junling Pang Yanjiang Xing Zhujie Cao Wenjun Guo Hao Yang Jing Wang Juntao Yang Chen Wang 《Signal Transduction and Targeted Therapy》 SCIE CSCD 2022年第6期2066-2078,共13页
Silicosis is the most prevalent and fatal occupational disease with no effective therapeutics,and currently used drugs cannot reverse the disease progress.Worse still,there are still challenges to be addressed to full... Silicosis is the most prevalent and fatal occupational disease with no effective therapeutics,and currently used drugs cannot reverse the disease progress.Worse still,there are still challenges to be addressed to fully decipher the intricated pathogenesis.Thus,specifying the essential mechanisms and targets in silicosis progression then exploring anti-silicosis pharmacuticals are desperately needed.In this work,multi-omics atlas was constructed to depict the pivotal abnormalities of silicosis and develop targeted agents.By utilizing an unbiased and time-resolved analysis of the transcriptome,proteome and phosphoproteome of a silicosis mouse model,we have verified the significant differences in transcript,protein,kinase activity and signaling pathway level during silicosis progression,in which the importance of essential biological processes such as macrophage activation,chemotaxis,immune cell recruitment and chronic inflammation were emphasized.Notably,the phosphorylation of EGFR(p-EGFR)and SYK(pSYK)were identified as potential therapeutic targets in the progression of silicosis.To inhibit and validate these targets,we tested fostamatinib(targeting SYK)and Gefitinib(targeting EGFR),and both drugs effectively ameliorated pulmonary dysfunction and inhibited the progression of inflammation and fibrosis.Overall,our drug discovery with multi-omics approach provides novel and viable therapeutic strategies for the treatment of silicosis. 展开更多
关键词 SILICOSIS SYK DRUGS
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