Dynamic Changes of IFN-γ-producing Cells, TGF-β and Their Predictive Value in Early Outcomes of Renal Transplantation

Background: A growing body of evidence demonstrated an immune etiology as well as nonimmune mechanismsfor episodes of clinical acute rejection and long-term allograft dysfunction.Objective: To investigate the correlation of IFN-γ-producing cells and TGF-β with incidence of clinical acuterejection in...

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Published in:International journal of organ transplantation medicine Vol. 4; no. 2; pp. 77 - 85
Main Authors: F. Mohammadi1, M. H. Niknam1, M. Nafar2, B. Einollahi3, B. Nazari1, M. Lessanpezeshki4, M. A. Amirzargar5, G. Solgi5, B. Nikbin1, A. A. Amirzargar1
Format: Journal Article
Language:English
Published: Shiraz University of Medical Sciences 01-01-2013
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Abstract Background: A growing body of evidence demonstrated an immune etiology as well as nonimmune mechanismsfor episodes of clinical acute rejection and long-term allograft dysfunction.Objective: To investigate the correlation of IFN-γ-producing cells and TGF-β with incidence of clinical acuterejection in living-related and unrelated kidney allogarft recipients during the first post-transplant year.Methods: This multi-center study was performed on 57 kidney allograft recipients from living-related(n=20) and unrelated (n=37) donors between April 2011 and September 2012 and who were followedprospectively for a mean period of one year. Peripheral blood samples were collected from all patientspre-transplantation and at days 14, 30 and 90 after transplantation; PBMCs were used as responding cellsin enzyme-linked immunosorbent spot (ELISPOT) assay to measure the frequency of IFN-γ-producingcells after stimulation with donor lymphocytes. Additionally, TGF-β levels were measured in cell culturesupernatants of ELISPOT assay.Results: During the follow-up period, 45 (79%) patients were diagnosed with stable graft function (groupA); 12 (21%) experienced clinical acute rejection episodes (group B). The frequency of IFN-γ-producingcells was significantly (p<0.001) higher in the rejection group in all three times after transplantation.Also, post-transplantation comparison for TGF-β showed a significantly (p<0.001) higher contents ingroup A vs. group B. Comparing the post-transplantation levels of TGF-β and mean numbers of IFN-γ-producing cells between groups A and B demonstrated a continuous increment in TGF-β and decreasingfrequencies of IFN-γ-producing cells in group A vs. group B.Conclusion: Serial post-transplantation monitoring of IFN-γ-producing donor reactive cells during the firstmonths is a clinically feasible approach for identification of kidney allogarft recipients at risk for ongoingimmune-mediated graft damage and later graft loss.
AbstractList Background: A growing body of evidence demonstrated an immune etiology as well as nonimmune mechanismsfor episodes of clinical acute rejection and long-term allograft dysfunction.Objective: To investigate the correlation of IFN-γ-producing cells and TGF-β with incidence of clinical acuterejection in living-related and unrelated kidney allogarft recipients during the first post-transplant year.Methods: This multi-center study was performed on 57 kidney allograft recipients from living-related(n=20) and unrelated (n=37) donors between April 2011 and September 2012 and who were followedprospectively for a mean period of one year. Peripheral blood samples were collected from all patientspre-transplantation and at days 14, 30 and 90 after transplantation; PBMCs were used as responding cellsin enzyme-linked immunosorbent spot (ELISPOT) assay to measure the frequency of IFN-γ-producingcells after stimulation with donor lymphocytes. Additionally, TGF-β levels were measured in cell culturesupernatants of ELISPOT assay.Results: During the follow-up period, 45 (79%) patients were diagnosed with stable graft function (groupA); 12 (21%) experienced clinical acute rejection episodes (group B). The frequency of IFN-γ-producingcells was significantly (p<0.001) higher in the rejection group in all three times after transplantation.Also, post-transplantation comparison for TGF-β showed a significantly (p<0.001) higher contents ingroup A vs. group B. Comparing the post-transplantation levels of TGF-β and mean numbers of IFN-γ-producing cells between groups A and B demonstrated a continuous increment in TGF-β and decreasingfrequencies of IFN-γ-producing cells in group A vs. group B.Conclusion: Serial post-transplantation monitoring of IFN-γ-producing donor reactive cells during the firstmonths is a clinically feasible approach for identification of kidney allogarft recipients at risk for ongoingimmune-mediated graft damage and later graft loss.
Author M. A. Amirzargar5
M. H. Niknam1
F. Mohammadi1
B. Nikbin1
G. Solgi5
M. Lessanpezeshki4
A. A. Amirzargar1
B. Einollahi3
B. Nazari1
M. Nafar2
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Snippet Background: A growing body of evidence demonstrated an immune etiology as well as nonimmune mechanismsfor episodes of clinical acute rejection and long-term...
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SubjectTerms Allograft
IFN-γ
Kidney
TGF-β
Title Dynamic Changes of IFN-γ-producing Cells, TGF-β and Their Predictive Value in Early Outcomes of Renal Transplantation
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