Antibacterial optimization of 4-aminothiazolyl analogues of the natural product GE2270 A: identification of the cycloalkylcarboxylic acids.-论文-万方医学网

第一作者： Matthew J,LaMarche

第一单位： Global Discovery Chemistry, Novartis Institutes for Biomedical Research, Cambridge, Massachusetts 02139, United States. matthew.lamarche@novartis.com

作者： Matthew J,LaMarche ^[1] ; Jennifer A,Leeds ; Kerri,Amaral ; Jason T,Brewer ; Simon M,Bushell ; Janetta M,Dewhurst ; JoAnne,Dzink-Fox ; Eric,Gangl ; Julie,Goldovitz ; Akash,Jain ; Steve,Mullin ; Georg,Neckermann ; Colin,Osborne ; Deborah,Palestrant ; Michael A,Patane ; Elin M,Rann ; Meena,Sachdeva ; Jian,Shao ; Stacey,Tiamfook ; Lewis,Whitehead ; Donghui,Yu

作者单位： Global Discovery Chemistry, Novartis Institutes for Biomedical Research, Cambridge, Massachusetts 02139, United States. matthew.lamarche@novartis.com ^[1]

医学主题词动物(Animals);抗菌药(Anti-Bacterial Agents);曲线下面积(Area Under Curve);羧酸类(Carboxylic Acids);结晶学, X线(Crystallography, X-Ray);抗药性, 细菌(Drug Resistance, Bacterial);女(雌)性(Female);革兰氏阳性菌(Gram-Positive Bacteria);革兰氏阳性菌感染(Gram-Positive Bacterial Infections);男(雄)性(Male);小鼠(Mice);微生物敏感性试验(Microbial Sensitivity Tests);模型, 分子(Models, Molecular);分子构象(Molecular Conformation);突变(Mutation);肽类, 环(Peptides, Cyclic);大鼠(Rats);大鼠, Sprague-Dawley(Rats, Sprague-Dawley);脓毒症(Sepsis);溶解度(Solubility);立体异构现象(Stereoisomerism);构效关系(Structure-Activity Relationship);噻唑类(Thiazoles)

DOI 10.1021/jm200938f

PMID 21999529

发布时间 2017-11-16

检索历史清除

Antibacterial optimization of 4-aminothiazolyl analogues of the natural product GE2270 A: identification of the cycloalkylcarboxylic acids.

Journal of medicinal chemistry

相似文献

同项目论文

Journal of medicinal chemistry

相关期刊

参考文献：
指定格式：	NoteExpress EndNote RefWorks NoteFirst

检索历史 清除

Antibacterial optimization of 4-aminothiazolyl analogues of the natural product GE2270 A: identification of the cycloalkylcarboxylic acids.

Journal of medicinal chemistry

相似文献

同项目论文

Journal of medicinal chemistry

相关期刊

检索历史清除