- 作者:Ting Liua ; b ; 1 ; Yuncheng Lia ; 1 ; Kexiong Lina ; 1 ; Hongjin Yina ; Binfeng Hea ; Michael Zhengc ; Guansong Wanga ; wanggs2003@hotmail.com
- 关键词:JAKs ; Janus kinases ; STATs ; signal transducers and activators of transcription ; HIF-1 ; hypoxia induced factor 1 ; PASMCs ; pulmonary arterial smooth muscle cells ; VSMCs ; vascular smooth muscle cells ; R-SMCs ; rhomboid VSMCs ; S-SMCs ; spindle-shaped SMCs ; PAH
- 刊名:The International Journal of Biochemistry and Cell Biology
- 出版年:2012
- 期刊代码:127_13572725
- 类别:med
- 出版时间:August, 2012
- 卷:44
- 期:8
- 页码:1337-1345
- 文件大小:1111 K
The results showed that S100A4 immunostaining was localized in the cytoplasm and nuclei of PASMCs exposure to hypoxia and it was predominantly expressed in rhomboid cells (R-SMCs). The mRNA and protein levels of S100A4 expression increased in PASMCs after hypoxic stimulus for 4, 8, 16 h. The immunofluorescence intensity and protein levels of S100A4 were suppressed, and the number of R-SMCs was reduced, when pretreatment with HIF-1伪 siRNA, STAT3 siRNA, S100A4 siRNA, and S100A4 inhibitor NSC 95397. Pretreatment with HIF-1伪 siRNA and anti-IL-6 antibodies, the levels of phospho-JAK2, -STAT3, and S100A4 were decreased, while HIF-1伪 kept stable in hypoxic cells. Importantly, pretreatment with HIF-1伪 siRNA, anti-IL-6 antibodies, STAT3 siRNA, and S100A4 siRNA, significantly attenuated the proliferation of PASMCs exposure to hypoxia. These data demonstrate that S100A4 is predominantly expressed in hypoxic R-SMCs, and regulated by the activation of JAK2-STAT3 signal pathway, which is dependent on hypoxia-induced HIF-1伪 expression. These results suggest that JAK2-STAT3 and HIF-1伪 could serve as targets for the regulation of phenotype modulation of PASMCs during the process of pulmonary vessel lesions.