TY - JOUR
T1 - Rat renal allograft tolerance is associated with local TGF-β and absence of IL-2r expression within chimeric immunocytic foci
AU - Hewitt, C. W.
AU - Strande, L.
AU - Santos, M.
AU - Goodman, M.
AU - Tarnoff, M.
AU - Zaontz, M. R.
AU - DelRossi, A. J.
AU - Doolin, E. J.
N1 - Funding Information:
This work was supported in part by grants from the American Heart Association, the International Association of Fire Fighters Burn Foundation, the Foundation of UMDNJ, and faculty practice grants from RWJMS/Cooper Hospital.
PY - 1997
Y1 - 1997
N2 - Tolerance was induced in Lewis (LEW) rat renal allograft recipients of Brown Norway kidneys by multiple pretransplant donor-blood transfusions and prior limited cyclosporine A. Rat renal allograft tolerance was associated with the induction of systemic donor T cells (10%), an early phase of nonspecific suppressor-cell generation, followed by maturation of systemic antigen-specific suppressor cells, and renal cellular infiltrates that develop long-term in situ in the kidney graft model. It was hypothesized that these traits represent chimeric immunocytic foci that are locally regulated via a TGF-β-dependent mechanism. Both immunohistochemical staining and digital image analysis for cellular and extracellular TGF-β, IL-2 receptor (CD25), and the BN Class I-MHC marker (OX-27) were performed. Control rejecting (REJ) kidneys did not demonstrate any differences with respect to levels of infiltrating immunocyte area vs long-term surviving (TOL) kidneys (3.9% vs 4.5%, P = .303). Immunostaining with the BN Class I MHC marker (OX- 27) demonstrated high levels of chimerism within immunocyte foci of the tolerant grafts (OX-27 BN+ immunocytes 49.0% ± 5.1%). In situ cellular IL-2 receptor (CD25) expression was demonstrated in REJ kidney infiltrates but not within TOL immunocytic infiltrating foci, when measured as percent of total lymphocytes (REJ = 5.0% vs TOL = 0.4%, P = .031). Conversely, TGF-β expression was significantly higher in immunocytes of TOL kidneys when measured as the number of DAB chromogen-staining pixels per total immunocyte area (TOL = .076 vs REJ = .047, P = .003). In conclusion, these results suggested that stable mixed immune chimerism (SMIC) plays an important role in DST-CyA-induced tolerance in situ. SMIC-induced tolerance may involve a local TGF-β-dependent mechanism that is associated with in situ TGF-β (+) and IL-2r (-) immunocytes.
AB - Tolerance was induced in Lewis (LEW) rat renal allograft recipients of Brown Norway kidneys by multiple pretransplant donor-blood transfusions and prior limited cyclosporine A. Rat renal allograft tolerance was associated with the induction of systemic donor T cells (10%), an early phase of nonspecific suppressor-cell generation, followed by maturation of systemic antigen-specific suppressor cells, and renal cellular infiltrates that develop long-term in situ in the kidney graft model. It was hypothesized that these traits represent chimeric immunocytic foci that are locally regulated via a TGF-β-dependent mechanism. Both immunohistochemical staining and digital image analysis for cellular and extracellular TGF-β, IL-2 receptor (CD25), and the BN Class I-MHC marker (OX-27) were performed. Control rejecting (REJ) kidneys did not demonstrate any differences with respect to levels of infiltrating immunocyte area vs long-term surviving (TOL) kidneys (3.9% vs 4.5%, P = .303). Immunostaining with the BN Class I MHC marker (OX- 27) demonstrated high levels of chimerism within immunocyte foci of the tolerant grafts (OX-27 BN+ immunocytes 49.0% ± 5.1%). In situ cellular IL-2 receptor (CD25) expression was demonstrated in REJ kidney infiltrates but not within TOL immunocytic infiltrating foci, when measured as percent of total lymphocytes (REJ = 5.0% vs TOL = 0.4%, P = .031). Conversely, TGF-β expression was significantly higher in immunocytes of TOL kidneys when measured as the number of DAB chromogen-staining pixels per total immunocyte area (TOL = .076 vs REJ = .047, P = .003). In conclusion, these results suggested that stable mixed immune chimerism (SMIC) plays an important role in DST-CyA-induced tolerance in situ. SMIC-induced tolerance may involve a local TGF-β-dependent mechanism that is associated with in situ TGF-β (+) and IL-2r (-) immunocytes.
UR - http://www.scopus.com/inward/record.url?scp=0030904706&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=0030904706&partnerID=8YFLogxK
U2 - 10.1016/S0041-1345(97)00284-4
DO - 10.1016/S0041-1345(97)00284-4
M3 - Article
C2 - 9193580
AN - SCOPUS:0030904706
SN - 0041-1345
VL - 29
SP - 2183
EP - 2184
JO - Transplantation proceedings
JF - Transplantation proceedings
IS - 4
ER -