Ween peripheral Th22 frequency and the levels of three kinds of blood cells in MDS patients, no significant differences were found.Correlation between Th22, Th17, and Th1 Cells in MDS PATIENTSIn E-MDS patients, a significantly positive correlation was found between peripheral Th22 cells and Th17 cells (r = 0.675, P = 0.004, Pearson correlation analysis) while no statistical correlation was obtained in L-MDS patients (r = 0.138, P = 0.610, Spearman correlation analysis). Peripheral Th22 cells showed no significant correlation with peripheral Th1 (P = 0.053).DiscussionThe presence of immune reactions against hematopoietic cells in MDS patients has crystallized as specific cell subsets and cytokines turmoil have been found as indispensable components of MDS pathophysiology. Th17, a new CD4+ T cell lineage thatFigure 2. Circulating percentages of Th17 cells, Th1 cells, and Th22 cells in MDS. (A) Circulating percentages of Th17 (CD4+ IL-17+) cells from 56-59-7 supplier healthy controls, E-MDS and L-MDS. Significantly increased 58-49-1 manufacturer percentage of Th17 cells was found in E-MDS patients (median, 1.90 ; range, 0.58?6.01 ) compared to L-MDS (median, 1.16 ; range, 0.15?.86 ) (*P = 0.002) or healthy controls (median, 1.01 ; range, 0.55?.69 ) (*P = 0.002). (B) Circulating percentages of Th1 (CD4+IFNc+) cells from healthy controls, E-MDS and L-MDS. There was no significant difference between E-MDS (median, 9.65 ; range, 6.16?1.08 ) patients and L-MDS (median, 8.41 ; range, 2.59?5.23 ) or healthy controls (median, 9.06 ; range, 6.01?14.02 ). (C) Circulating percentages of Th22 (CD4+ IL-22+ IL-172IFNc2 ) cells from healthy controls, E-MDS and L-MDS. Significantly elevated percentage of Th22 cells was found in L-MDS patients (1.7760.84 ) compared to E-MDS (1.2760.50 ) (*P = 0.03) and healthy controls (0.7160.17 ) (*P,0.0001). Obviously increased percentage of Th22 cells was shown between E-MDS and healthy controls (*P = 0.002). (D) Circulating percentages of Th17 cells from healthy controls, bone marrow (BM) blasts ,5 and blasts 5 patients. The circulating percentages of Th17 cells remained significantly higher in blasts ,5 compared with healthy donors. (*P = 0.003). 23727046 doi:10.1371/journal.pone.0051339.gTh22 and Th17 Cells in Different Stages of MDSFigure 3. Concentrations of IL-22 and IL-17 in PB and BM from healthy controls and MDS patients. (A) Concentrations of IL-22 in PB plasma from healthy controls, E-MDS and L-MDS patients. There was no significant difference between E-MDS (median, 21.66 pg/ml; range, 16.02?36.00 pg/ml, P.0.05) or L-MDS patients (median, 23.37 pg/ml; range, 17.00?4.66 pg/ml, P.0.05) and healthy controls (median, 23.86 pg/ml; range, 14.04?6.49 pg/ml, P.0.05). (B) Concentrations of IL-17 in PB plasma from healthy controls, E-MDS and L-MDS patients. No significant difference was found between E-MDS (median, 22.32 pg/ml; range, 19.13?0.11 pg/ml, P.0.05) 15755315 or L-MDS (median, 25.39 pg/ml; range, 17.86?6.31 pg/ml, P.0.05) patients and healthy controls (median, 25.11 pg/ml; range, 16.87?7.00 pg/ml, P.0.05).(C)Concentrations of IL-22 in BM plasm from healthy controls, E-MDS and L-MDS patients. There was no significant difference between E-MDS (median, 40.34 pg/ml; range, 11.08?01.33 pg/ml, P.0.05) or L-MDS patients (median, 30.68 pg/ml; range, 23.86?9.43 pg/ml, P.0.05) and healthy controls (median, 33.59 pg/ml; range, 20.93?1.74 pg/ml, P.0.05). (D) Concentrations of IL-17 in BM plasm from healthy controls, E-MDS and L-MDS patients. No significant difference was.Ween peripheral Th22 frequency and the levels of three kinds of blood cells in MDS patients, no significant differences were found.Correlation between Th22, Th17, and Th1 Cells in MDS PATIENTSIn E-MDS patients, a significantly positive correlation was found between peripheral Th22 cells and Th17 cells (r = 0.675, P = 0.004, Pearson correlation analysis) while no statistical correlation was obtained in L-MDS patients (r = 0.138, P = 0.610, Spearman correlation analysis). Peripheral Th22 cells showed no significant correlation with peripheral Th1 (P = 0.053).DiscussionThe presence of immune reactions against hematopoietic cells in MDS patients has crystallized as specific cell subsets and cytokines turmoil have been found as indispensable components of MDS pathophysiology. Th17, a new CD4+ T cell lineage thatFigure 2. Circulating percentages of Th17 cells, Th1 cells, and Th22 cells in MDS. (A) Circulating percentages of Th17 (CD4+ IL-17+) cells from healthy controls, E-MDS and L-MDS. Significantly increased percentage of Th17 cells was found in E-MDS patients (median, 1.90 ; range, 0.58?6.01 ) compared to L-MDS (median, 1.16 ; range, 0.15?.86 ) (*P = 0.002) or healthy controls (median, 1.01 ; range, 0.55?.69 ) (*P = 0.002). (B) Circulating percentages of Th1 (CD4+IFNc+) cells from healthy controls, E-MDS and L-MDS. There was no significant difference between E-MDS (median, 9.65 ; range, 6.16?1.08 ) patients and L-MDS (median, 8.41 ; range, 2.59?5.23 ) or healthy controls (median, 9.06 ; range, 6.01?14.02 ). (C) Circulating percentages of Th22 (CD4+ IL-22+ IL-172IFNc2 ) cells from healthy controls, E-MDS and L-MDS. Significantly elevated percentage of Th22 cells was found in L-MDS patients (1.7760.84 ) compared to E-MDS (1.2760.50 ) (*P = 0.03) and healthy controls (0.7160.17 ) (*P,0.0001). Obviously increased percentage of Th22 cells was shown between E-MDS and healthy controls (*P = 0.002). (D) Circulating percentages of Th17 cells from healthy controls, bone marrow (BM) blasts ,5 and blasts 5 patients. The circulating percentages of Th17 cells remained significantly higher in blasts ,5 compared with healthy donors. (*P = 0.003). 23727046 doi:10.1371/journal.pone.0051339.gTh22 and Th17 Cells in Different Stages of MDSFigure 3. Concentrations of IL-22 and IL-17 in PB and BM from healthy controls and MDS patients. (A) Concentrations of IL-22 in PB plasma from healthy controls, E-MDS and L-MDS patients. There was no significant difference between E-MDS (median, 21.66 pg/ml; range, 16.02?36.00 pg/ml, P.0.05) or L-MDS patients (median, 23.37 pg/ml; range, 17.00?4.66 pg/ml, P.0.05) and healthy controls (median, 23.86 pg/ml; range, 14.04?6.49 pg/ml, P.0.05). (B) Concentrations of IL-17 in PB plasma from healthy controls, E-MDS and L-MDS patients. No significant difference was found between E-MDS (median, 22.32 pg/ml; range, 19.13?0.11 pg/ml, P.0.05) 15755315 or L-MDS (median, 25.39 pg/ml; range, 17.86?6.31 pg/ml, P.0.05) patients and healthy controls (median, 25.11 pg/ml; range, 16.87?7.00 pg/ml, P.0.05).(C)Concentrations of IL-22 in BM plasm from healthy controls, E-MDS and L-MDS patients. There was no significant difference between E-MDS (median, 40.34 pg/ml; range, 11.08?01.33 pg/ml, P.0.05) or L-MDS patients (median, 30.68 pg/ml; range, 23.86?9.43 pg/ml, P.0.05) and healthy controls (median, 33.59 pg/ml; range, 20.93?1.74 pg/ml, P.0.05). (D) Concentrations of IL-17 in BM plasm from healthy controls, E-MDS and L-MDS patients. No significant difference was.