MSCs from healthy volunteers could obviously block T cells in G0/

MSCs from healthy NCT-501 price volunteers could obviously block T cells in G0/G1 phase. In this study, inhibitory effects of MDS-derived MSCs on T cell proliferation were obviously impaired. Moreover, no significant cell cycle arrest was observed in PHA-stimulated T cells cocultured with CML-derived MSCs. In addition, an inhibitory effect on T cell activation is another key point of immuno-modulatory function for MSCs, although there are still disputes[21,

22]. CD25, CD69 and CD44 are candidates for T cell activation in different phases. In our study, MSCs from healthy volunteers showed significant inhibitory effects on expression of T cell activation markers, but MSCs from CML patients showed very limited inhibitory effects. These results suggested that CML-derived MSCs have GM6001 concentration immunologic abnormalities and their application in immuno-modulation might be limited. Normally, the invasion and metastasis by malignant tumor cells consists of three major steps: the receptor-mediated adhesion of tumor cells to the extracellular matrix, the degradation of the extracellular matrix by the proteinase secreted by the tumor cells, and the transfer and proliferation of tumor cells[36]. So, the loose of ECM and secreted cytokines are

important for the metastasis of the tumor cells from the primary tumor[37]. Pathological conditions will change the tumor cell fate leading to invasion and metastasis[38], Local secretion of proteases have been implicated in this tumor-stroma selleck kinase inhibitor crosstalk. Matrix Metalloproteinase-9 (MMP-9) is one of them which has the preferential ability to degrade denatured collagens (gelatin) and collagen type IV, the 2 main components of basement membranes and therefore plays a critical role in tumour progression and metastaisis[39]. Moreover, its expression increases with the increased or greater proliferation of tumor cells. We used a ds-RNA to interfere with the

expression of MMP-9 gene in CML MSC and our findings support the conclusion that MMP-9 constitutes a trigger for the switch between adhesive and invasive states in CML MSC by changing the ICAM-1 from membrane-anchored state to solvable one leading to tumor cell immune evasion and metastasis. In conclusion, the immune function of CML patient-derived MSCs showed that their immuno-modulatory Lck ability, compared to MSCs from healthy volunteers, was impaired, whichmight be a cause for an abnormal hematopoietic environment. This indicates that autologous MSCs transplantation might be futile. Instead, allogenic MSCs transplantation might be a better choice to ameliorate CML. Acknowledgements Supported by grants from the “”863 Projects”" of Ministry of Science and Technology of PR China (No. 2006AA02A109. 2006AA02A115); National Natural Science Foundation of China (No.30570771; Beijing Ministry of Science and Technology (No. D07050701350701) and Cheung Kong Scholars programme. References 1.

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