Targeting macrophagic SHP2 for ameliorating osteoarthritis via TLR signaling  被引量：4

作　　者：Ziying Sun Qianqian Liu Zhongyang Lv Jiawei Li Xingquan Xu Heng Sun Maochun Wang Kuoyang Sun Tianshu Shi Zizheng Liu Guihua Tan Wenqiang Yan Rui Wu Yannick Xiaofan Yang Shiro Ikegawa Qing Jiang Yang Sun Dongquan Shi 

机构地区：[1]State Key Laboratory of Pharmaceutical Biotechnology,Department of Sports Medicine and Adult Reconstructive Surgery,Nanjing Drum Tower Hospital,the Affiliated Hospital of Nanjing University Medical School,Nanjing 210008,China [2]Laboratory for Bone and Joint Disease,Model Animal Research Center(MARC),Nanjing University,Nanjing 210093,China [3]State Key Laboratory of Pharmaceutical Biotechnology,Department of Biotechnology and Pharmaceutical Sciences,School of Life Science,Nanjing University,Nanjing 210023,China [4]Drum Tower of Clinical Medicine,Nanjing Medical University,Nanjing 210008,China [5]Laboratory for Bone and Joint Diseases,RIKEN Center for Integrative Medical Science(IMS,RIKEN),Tokyo 108-8639,Japan

出　　处：《Acta Pharmaceutica Sinica B》2022年第7期3073-3084,共12页药学学报（英文版）

基　　金：supported by the National Science Foundation of China(NSFC 81802196,81572129,81872877,91853109,and 81772335);Key Program of NSFC(81730067,China);Special Program of Chinese Academy of Science(XDA16020805,China);Jiangsu Provincial Key Medical Center Foundation(China);Jiangsu Provincial Medical Outstanding Talent Foundation(China);Jiangsu Provincial Key Medical Talent Foundation(China)。

摘　　要：Osteoarthritis(OA),in which M1 macrophage polarization in the synovium exacerbates disease progression,is a major cause of cartilage degeneration and functional disabilities.Therapeutic strategies of OA designed to interfere with the polarization of macrophages have rarely been reported.Here,we report that SHP099,as an allosteric inhibitor of src-homology 2-containing protein tyrosine phosphatase 2(SHP2),attenuated osteoarthritis progression by inhibiting M1 macrophage polarization.We demonstrated that M1 macrophage polarization was accompanied by the overexpression of SHP2 in the synovial tissues of OA patients and OA model mice.Compared to wild-type(WT)mice,myeloid lineage conditional Shp2 knockout(c KO)mice showed decreased M1 macrophage polarization and attenuated severity of synovitis,an elevated expression of cartilage phenotype protein collagen II(COL2),and a decreased expression of cartilage degradation markers collagen X(COL10)and matrix metalloproteinase3(MMP3)in OA cartilage.Further mechanistic analysis showed that SHP099 inhibited lipopolysaccharide(LPS)-induced Toll-like receptor(TLR)signaling mediated by nuclear factor kappa B(NF-κB)and PI3K—AKT signaling.Moreover,intra-articular injection of SHP099 also significantly attenuated OA progression,including joint synovitis and cartilage damage.These results indicated that allosteric inhibition of SHP2 might be a promising therapeutic strategy for the treatment of OA.

关 键 词：SHP2 SHP099 OSTEOARTHRITIS SYNOVITIS Toll-like receptor signaling MACROPHAGE Cartilage degradation M1 macrophage polarization 

分 类 号：R684.3[医药卫生—骨科学]