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Identification of anti-Mycobacterium tuberculosis agents targeting the interaction of bacterial division proteins FtsZ and SepFe
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作者 Hongjuan Zhang Ying Chen +6 位作者 Yu Zhang Luyao Qiao Xiangyin Chi Yanxing Han Yuan Lin Shuyi Si Jiandong Jiang 《Acta Pharmaceutica Sinica B》 SCIE CAS CSCD 2023年第5期2056-2070,共15页
Tuberculosis(TB)is one of the deadly diseases caused by Mycobacterium tuberculosis(Mtb),which presents a significant public health challenge.Treatment of TB relies on the combination of several anti-TB drugs to create... Tuberculosis(TB)is one of the deadly diseases caused by Mycobacterium tuberculosis(Mtb),which presents a significant public health challenge.Treatment of TB relies on the combination of several anti-TB drugs to create shorter and safer regimens.Therefore,new anti-TB agents working by different mechanisms are urgently needed.FtsZ,a tubulin-like protein with GTPase activity,forms a dynamic Z-ring in cell division.Most of FtsZ inhibitors are designed to inhibit GTPase activity.In Mtb,the function of Z-ring is modulated by SepF,a FtsZ binding protein.The FtsZ/SepF interaction is essential for FtsZ bundling and localization at the site of division.Here,we established a yeast twohybrid based screening system to identify inhibitors of FtsZ/SepF interaction in M.tuberculosis.Using this system,we found compound T0349 showing strong anti-Mtb activity but with low toxicity to other bacteria strains and mice.Moreover,we have demonstrated that T0349 binds specifically to SepF to block FtsZ/SepF interaction by GST pull-down,fluorescence polarization(FP),surface plasmon resonance(SPR)and CRISPRi knockdown assays.Furthermore,T0349 can inhibit bacterial cell division by inducing filamentation and abnormal septum.Our data demonstrated that FtsZ/SepF interaction is a promising anti-TB drug target for identifying agents with novel mechanisms. 展开更多
关键词 Anti-Mycobacterium tuberculosis FTSZ sepf Bacterial division Yeast two-hybrid CRISPRi Protein—protein interaction Inhibitor
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结核分枝杆菌SepF蛋白的生物信息学分析
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作者 宋娜娜 李永明 《医学理论与实践》 2024年第6期1016-1019,共4页
目的:采用生物信息学方法分析结核分枝杆菌的Rv2147c基因及其编码的SepF蛋白结构和功能。方法:自NCBI网站获取Rv2147c基因及SepF蛋白的基本信息;使用Protparam和ProtScale预测SepF蛋白的理化性质和亲疏水性;使用SignaIP6.0 Server、DEEP... 目的:采用生物信息学方法分析结核分枝杆菌的Rv2147c基因及其编码的SepF蛋白结构和功能。方法:自NCBI网站获取Rv2147c基因及SepF蛋白的基本信息;使用Protparam和ProtScale预测SepF蛋白的理化性质和亲疏水性;使用SignaIP6.0 Server、DEEP TMHMM和NetPhos3.1软件预测SepF蛋白的信号肽、跨膜结构及磷酸化位点;使用SOPMA预测SepF蛋白的二级结构,通过SWISS MODEL软件构建该蛋白的三级结构模型;分别使用IEDB和SYFPEITHI预测SepF蛋白的B和T细胞表位;通过STRING数据库预测SepF的相互作用蛋白。结果:Rv2147c基因全长657bp,编码的SepF蛋白氨基酸数为218,分子式为C_(1095)H_(1668)N_(320)O_(337)S_(10)。SepF蛋白含有磷酸化位点和抗原表位。结论:生物信息学方法分析SepF蛋白含有一个保守的结构域,其结构域与结核分枝杆菌耐药性的产生密切相关,为抗结核药物靶点的选择提供了新方向。预测SepF蛋白含有大量抗原表位,可能成为结核病疫苗的候选蛋白。 展开更多
关键词 结核分枝杆菌 Rv1963 sepf蛋白 生物信息学分析
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投入-产出系统生产要素动态匹配状况评判初探 被引量:1
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作者 向刚 《云南工业大学学报》 1996年第2期62-67,共6页
探讨了生产要素系统组合效应概念和基本特性,进而建立一种投入-产出系统生产要素动态匹配状况的实证评价判据和方法,最后给出对实际系统的评判分析案例.
关键词 生产要素 动态匹配 评判 投入-产出系统
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