| Literature DB >> 26839984 |
Veronika Svachova1, Alena Sekerkova1, Petra Hruba2, Irena Tycova2, Marketa Rodova1, Eva Cecrdlova1, Janka Slatinska3, Eva Honsova4, Ilja Striz1, Ondrej Viklicky2,3.
Abstract
B cells play an important role in the immune responses which affect the outcomes of kidney allografts. Dynamic changes of B-cell compartments in clinical kidney transplantation are still poorly understood. B-cell subsets were prospectively monitored using flow cytometry for 1 year in 98 kidney transplant recipients. Data were correlated with immunosuppression and clinical outcomes. An increase in the total population of B lymphocytes was observed during the first week after transplantation. The level of IgM(high) CD38(high) CD24(high) transitional B cells reduced significantly up until the third month, with partial repopulation in the first year. Lower numbers of transitional B cells in the third month were associated with higher risk of graft rejection. IgM(+) IgD(+) CD27(-) naive B cells did not change within follow-up. IgM(+) CD27(+) nonswitched memory B cells and IgM(-) CD27(+) switched memory B cells increased on post-operative day 7. IgM(-) CD38(high) CD27(high) plasmablasts showed similar kinetics during the first post-transplant year, similar to transitional B cells. In conclusion, sensitized kidney transplant recipients as well as those with either acute or chronic rejection within the first post-transplant year exhibited lower levels of transitional B cells. Therefore, these data further support the hypothesis that transitional B cells have a protective role in kidney transplantation.Entities:
Keywords: B cells; kidney transplantation; rejection; transitional B cells
Mesh:
Substances:
Year: 2016 PMID: 26839984 DOI: 10.1111/tri.12751
Source DB: PubMed Journal: Transpl Int ISSN: 0934-0874 Impact factor: 3.782