Recruitment of IL-27-Producing CD4.sup.+ T Cells and Effect of IL-27 on Pleural Mesothelial Cells in Tuberculous Pleurisy

Background The numbers of IL-27-producing CD4.sup.+ T cells and the concentration of soluble IL-27 have been found to be increased in tuberculous pleural effusion (TPE). The objective of the present study was to explore the mechanism by which IL-27.sup.+CD4.sup.+ T cells are recruited into the pleural space, and to explore the impact of IL-27 on pleural mesothelial cells (PMCs). Methods The expression profiles of chemokine receptor (CCR) were determined by flow cytometry. The chemoattractant activity of chemokines CCL20 and CCL22 for IL-27.sup.+CD4.sup.+ T cells in vitro was observed. Effects of IL-27 on wound healing, proliferation and apoptosis of PMCs were also investigated. Results IL-27.sup.+CD4.sup.+ T cells in TPE expressed high level of CCR6, medium level of CCR4, and low levels of CCR2, CCR3, CCR5, CCR7, CCR10, and CXCR3. Recruitment of IL-27.sup.+CD4.sup.+ T cells into TPE could be induced by pleural CCL20 and CCL22. By activating STAT3 signaling, IL-27 significantly improved wound healing and promoted proliferation of PMCs, and completely prevented apoptosis of PMCs induced by IFN-[gamma]. Conclusions After being recruited into pleural space by CCL20 or/and CCL22, these pleural IL-27-producing CD4.sup.+ T cells may play important roles in tuberculosis immunity by affecting PMC functions.
Author(s): Zhi-Jian Ye[sup.1] [sup.2] , Li-Li Xu[sup.2] , Qiong Zhou[sup.4] , Ai Cui[sup.2] , Xiao-Juan Wang[sup.2] , Kan Zhai[sup.3] , Zhen Wang[sup.2] , Zhao-Hui Tong[sup.2] , Huan-Zhong Shi[sup.2] [sup.3] Author [...]