Antibody-mediated rejection of arterialised venous allografts is inhibited by immunosuppression in rats.
OBJECTIVES AND DESIGN: We determined in a rat model (1) the presence and dynamics of alloantibodies recognizing MHC complexes on quiescent Brown-Norway (BN) splenic cells in the sera of Lewis (LEW) recipients of Brown-Norway iliolumbar vein grafts under tacrolimus immunosuppression; and (2) the pres...
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doaj-d643b2de49684973b86442e0b7c1e6262020-11-24T21:51:04ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0193e9121210.1371/journal.pone.0091212Antibody-mediated rejection of arterialised venous allografts is inhibited by immunosuppression in rats.Katrin SplithPeter FellmerIvan MatiaMartin VargaMartin OliveriusStephanie KuhnLinda FeldbrüggeFelix KrenzienHans-Michael HauGeorg WiltbergerMoritz SchmelzleSven JonasOBJECTIVES AND DESIGN: We determined in a rat model (1) the presence and dynamics of alloantibodies recognizing MHC complexes on quiescent Brown-Norway (BN) splenic cells in the sera of Lewis (LEW) recipients of Brown-Norway iliolumbar vein grafts under tacrolimus immunosuppression; and (2) the presence of immunoglobulins in the wall of acute rejected vein allografts. MATERIALS AND METHODS: Flow cytometry was used for the analysis of day 0, 14 and 30 sera obtained from Lewis recipients of isogeneic iliolumbar vein grafts (group A) or Brown-Norway grafts (group B, C) for the presence of donor specific anti-MHC class I and II antibodies. Tacrolimus 0.2 mg/kg daily was administered from day 1 to day 30 (group C). Histology was performed on day 30. RESULTS: Sera obtained preoperatively and on day 30 were compared in all groups. The statistically significant decrease of anti MHC class I and II antibody binding was observed only in allogenic non-immunosuppressed group B (splenocytes: MHC class I - day 0 (93% ± 7% ) vs day 30 (66% ± 7%), p = 0.02, MHC class II - day 0 (105% ± 3% ) vs day 30 (83% ± 5%), p = 0.003; B-cells: MHC class I - day 0 (83% ± 5%) vs day 30 (55% ± 6%), p = 0.003, MHC class II - day 0 (101% ± 1%) vs day 30 (79% ± 6%), p = 0.006; T-cells: MHC class I - day 0 (71% ± 7%) vs day 30 (49% ± 5%), p = 0.04). No free clusters of immunoglobulin G deposition were detected in any experimental group. CONCLUSION: Arterialized venous allografts induce strong donor-specific anti-MHC class I and anti-MHC class II antibody production with subsequent immune-mediated destruction of these allografts with no evidence of immunoglobulin G deposition. Low-dose tacrolimus suppress the donor-specific antibody production.http://europepmc.org/articles/PMC3949981?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Katrin Splith Peter Fellmer Ivan Matia Martin Varga Martin Oliverius Stephanie Kuhn Linda Feldbrügge Felix Krenzien Hans-Michael Hau Georg Wiltberger Moritz Schmelzle Sven Jonas |
spellingShingle |
Katrin Splith Peter Fellmer Ivan Matia Martin Varga Martin Oliverius Stephanie Kuhn Linda Feldbrügge Felix Krenzien Hans-Michael Hau Georg Wiltberger Moritz Schmelzle Sven Jonas Antibody-mediated rejection of arterialised venous allografts is inhibited by immunosuppression in rats. PLoS ONE |
author_facet |
Katrin Splith Peter Fellmer Ivan Matia Martin Varga Martin Oliverius Stephanie Kuhn Linda Feldbrügge Felix Krenzien Hans-Michael Hau Georg Wiltberger Moritz Schmelzle Sven Jonas |
author_sort |
Katrin Splith |
title |
Antibody-mediated rejection of arterialised venous allografts is inhibited by immunosuppression in rats. |
title_short |
Antibody-mediated rejection of arterialised venous allografts is inhibited by immunosuppression in rats. |
title_full |
Antibody-mediated rejection of arterialised venous allografts is inhibited by immunosuppression in rats. |
title_fullStr |
Antibody-mediated rejection of arterialised venous allografts is inhibited by immunosuppression in rats. |
title_full_unstemmed |
Antibody-mediated rejection of arterialised venous allografts is inhibited by immunosuppression in rats. |
title_sort |
antibody-mediated rejection of arterialised venous allografts is inhibited by immunosuppression in rats. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2014-01-01 |
description |
OBJECTIVES AND DESIGN: We determined in a rat model (1) the presence and dynamics of alloantibodies recognizing MHC complexes on quiescent Brown-Norway (BN) splenic cells in the sera of Lewis (LEW) recipients of Brown-Norway iliolumbar vein grafts under tacrolimus immunosuppression; and (2) the presence of immunoglobulins in the wall of acute rejected vein allografts. MATERIALS AND METHODS: Flow cytometry was used for the analysis of day 0, 14 and 30 sera obtained from Lewis recipients of isogeneic iliolumbar vein grafts (group A) or Brown-Norway grafts (group B, C) for the presence of donor specific anti-MHC class I and II antibodies. Tacrolimus 0.2 mg/kg daily was administered from day 1 to day 30 (group C). Histology was performed on day 30. RESULTS: Sera obtained preoperatively and on day 30 were compared in all groups. The statistically significant decrease of anti MHC class I and II antibody binding was observed only in allogenic non-immunosuppressed group B (splenocytes: MHC class I - day 0 (93% ± 7% ) vs day 30 (66% ± 7%), p = 0.02, MHC class II - day 0 (105% ± 3% ) vs day 30 (83% ± 5%), p = 0.003; B-cells: MHC class I - day 0 (83% ± 5%) vs day 30 (55% ± 6%), p = 0.003, MHC class II - day 0 (101% ± 1%) vs day 30 (79% ± 6%), p = 0.006; T-cells: MHC class I - day 0 (71% ± 7%) vs day 30 (49% ± 5%), p = 0.04). No free clusters of immunoglobulin G deposition were detected in any experimental group. CONCLUSION: Arterialized venous allografts induce strong donor-specific anti-MHC class I and anti-MHC class II antibody production with subsequent immune-mediated destruction of these allografts with no evidence of immunoglobulin G deposition. Low-dose tacrolimus suppress the donor-specific antibody production. |
url |
http://europepmc.org/articles/PMC3949981?pdf=render |
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