南方科技大学知识苑(SUSTech KC): Human Kinase IGF1R/IR Inhibitor Linsitinib Controls the In Vitro and Intracellular Growth of Mycobacterium tuberculosis

题名	Human Kinase IGF1R/IR Inhibitor Linsitinib Controls the In Vitro and Intracellular Growth of Mycobacterium tuberculosis
作者	Wang, Heng 1; Bi, Jing 2; Zhang, Yuan 1; Pan, Miaomiao 1; Guo, Qinglong2 ; Xiao, Genhui 1; Cui, Yumeng 1; Hu, Song 1; Chan, Chi Kin 1; Yuan, Ying 1; Kaneko, Takushi 3; Zhang, Guoliang 2; Chen, Shawn 1
通讯作者	Bi, Jing; Chen, Shawn
发表日期	2022-09-01
DOI	10.1021/acsinfecdis.2c00278
发表期刊	ACS Infectious Diseases 影响因子和分区
ISSN	2373-8227
摘要	ATP provides energy in the biosynthesis of cellular metabolites as well as regulates protein functions through phosphorylation. Many ATP-dependent enzymes are antibacterial and anticancer targets including human kinases acted on by most of the successful drugs. In search of new chemotherapeutics for tuberculosis (TB), we screened repurposing compounds against the essential glutamine synthase (GlnA1) of Mycobacterium tuberculosis (Mtb) and identified linsitinib, a clinical-stage drug originally targeting kinase IGF1R/IR as a potent GlnA1 inhibitor. Linsitinib has direct antimycobacterial activity. Biochemical, molecular modeling, and target engagement analyses revealed the inhibition is ATP-competitive and specific in Mtb. Linsitinib also improves autophagy flux in both Mtb-infected and uninfected THP1 macrophages, as demonstrated by the decreased p-mTOR and p62 and the increased lipid-bound LC3B-II and autophagosome forming puncta. Linsitinib-mediated autophagy reduces intracellular growth of wild-type and isoniazid-resistant Mtb alone or in combination with bedaquiline. We have demonstrated that an IGF-IR/IR inhibitor can potentially be used to treat TB. Our study reinforces the concept of targeting ATP-dependent enzymes for novel anti-TB therapy.
关键词	M tuberculosis glutamine synthetase IGF1R IR inhibitor autophagy ATP-dependent enzyme
相关链接	[来源记录]
收录类别	SCI
语种	英语
学校署名	通讯
WOS研究方向	Pharmacology & Pharmacy ; Infectious Diseases
WOS类目	Chemistry, Medicinal ; Infectious Diseases
WOS记录号	WOS:000854008300001
出版者	AMER CHEMICAL SOC
来源库	Web of Science
引用统计	被引频次[WOS]：4
成果类型	期刊论文
条目标识符	http://sustech.caswiz.com/handle/2SGJ60CL/402327
专题	南方科技大学第二附属医院南方科技大学第一附属医院
作者单位	1.Global Hlth Drug Discovery Inst, Beijing 100192, Peoples R China 2.Southern Univ Sci & Technol, Shenzhen Peoples Hosp 3, Natl Clin Res Ctr Infect Dis, Guangdong Prov Clin Res Ctr TB, Shenzhen 518112, Peoples R China 3.Global Alliance TB Drug Dev, New York, NY 10005 USA
通讯作者单位	南方科技大学第二附属医院; 南方科技大学第一附属医院
推荐引用方式 GB/T 7714	Wang, Heng,Bi, Jing,Zhang, Yuan,et al. Human Kinase IGF1R/IR Inhibitor Linsitinib Controls the In Vitro and Intracellular Growth of Mycobacterium tuberculosis[J]. ACS Infectious Diseases,2022.
APA	Wang, Heng.,Bi, Jing.,Zhang, Yuan.,Pan, Miaomiao.,Guo, Qinglong.,...&Chen, Shawn.(2022).Human Kinase IGF1R/IR Inhibitor Linsitinib Controls the In Vitro and Intracellular Growth of Mycobacterium tuberculosis.ACS Infectious Diseases.
MLA	Wang, Heng,et al."Human Kinase IGF1R/IR Inhibitor Linsitinib Controls the In Vitro and Intracellular Growth of Mycobacterium tuberculosis".ACS Infectious Diseases (2022).