Induction of chronic renal allograft injury by injection of a monoclonal antibody against a donor MHC Ib molecule in a nude rat model.

Martina Koch; Verena Broecker; Annice Heratizadeh; Corinna Doege; Juergen Strehlau; Michael Mengel; Björn Nashan

Induction of chronic renal allograft injury by injection of a monoclonal antibody against a donor MHC Ib molecule in a nude rat model.

Standard

Induction of chronic renal allograft injury by injection of a monoclonal antibody against a donor MHC Ib molecule in a nude rat model. / Koch, Martina; Broecker, Verena; Heratizadeh, Annice; Doege, Corinna; Strehlau, Juergen; Mengel, Michael; Nashan, Björn.

In: TRANSPL IMMUNOL, Vol. 19, No. 3-4, 3-4, 2008, p. 187-191.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Koch, M, Broecker, V, Heratizadeh, A, Doege, C, Strehlau, J, Mengel, M & Nashan, B 2008, 'Induction of chronic renal allograft injury by injection of a monoclonal antibody against a donor MHC Ib molecule in a nude rat model.', TRANSPL IMMUNOL, vol. 19, no. 3-4, 3-4, pp. 187-191. <http://www.ncbi.nlm.nih.gov/pubmed/18595711?dopt=Citation>

APA

Koch, M., Broecker, V., Heratizadeh, A., Doege, C., Strehlau, J., Mengel, M., & Nashan, B. (2008). Induction of chronic renal allograft injury by injection of a monoclonal antibody against a donor MHC Ib molecule in a nude rat model. TRANSPL IMMUNOL, 19(3-4), 187-191. [3-4]. http://www.ncbi.nlm.nih.gov/pubmed/18595711?dopt=Citation

Vancouver

Koch M, Broecker V, Heratizadeh A, Doege C, Strehlau J, Mengel M et al. Induction of chronic renal allograft injury by injection of a monoclonal antibody against a donor MHC Ib molecule in a nude rat model. TRANSPL IMMUNOL. 2008;19(3-4):187-191. 3-4.

Bibtex

@article{418e1f65e4c54e3497aaee809408d8e4,

title = "Induction of chronic renal allograft injury by injection of a monoclonal antibody against a donor MHC Ib molecule in a nude rat model.",

abstract = "BACKGROUND: Chronic allograft injury induced by immunological as well as non-immunological mechanisms is still a major cause of long-term graft loss after renal transplantation. Major histocompatibility complex (MHC) incompatibilities as well as donor-specific alloantibodies are known risk factors, but the interaction of cellular and humoral mechanisms leading to allograft damage remains to be defined. The aim of this study was to analyze the impact of donor-specific post-transplant antibodies against a non-classical MHC Ib antigen apart from T-cell-dependent immune response. Therefore, we utilized a transplant rat model injecting a moAb directed against a donor MHC Ib molecule into athymic nude recipients lacking an immunocompetent T-cell system. METHODS: F344 kidneys were transplanted into LEW.RNU rats. Donor and recipient differ in the RT1.C locus (MHC Ib) but are phenotypically identical for the RT1.A (MHC I) and RT1.B/D (MHC II) loci. A moAb directed against the donors RT1.C(lv1) was injected into recipients with stable graft function. A control group remained untreated after transplantation. The rats were monitored for renal function and grafts were analyzed for morphological changes, infiltrating cells and C4d deposition. RESULTS: Antibody-infused rats developed renal impairment with massive urine albumin excretion. Histological changes consistent with antibody-mediated injury were interstitial fibrosis, tubular atrophy and severe glomerulopathy accompanied by an infiltrate of numerous macrophages. At time of death, grafts were negative for C4d at the peritubular capillaries and arterial endothelium. CONCLUSION: Antibodies directed against a MHC Ib antigen are able to induce allograft injury in T-cell-deficient rats. This model underlines the role of non-classical MHC disparities for long-term allograft survival and demonstrates the long-term results of antibody-induced allograft damage.",

author = "Martina Koch and Verena Broecker and Annice Heratizadeh and Corinna Doege and Juergen Strehlau and Michael Mengel and Bj{\"o}rn Nashan",

year = "2008",

language = "Deutsch",

volume = "19",

pages = "187--191",

journal = "TRANSPL IMMUNOL",

issn = "0966-3274",

publisher = "Elsevier",

number = "3-4",

}

RIS

TY - JOUR

T1 - Induction of chronic renal allograft injury by injection of a monoclonal antibody against a donor MHC Ib molecule in a nude rat model.

AU - Koch, Martina

AU - Broecker, Verena

AU - Heratizadeh, Annice

AU - Doege, Corinna

AU - Strehlau, Juergen

AU - Mengel, Michael

AU - Nashan, Björn

PY - 2008

Y1 - 2008

N2 - BACKGROUND: Chronic allograft injury induced by immunological as well as non-immunological mechanisms is still a major cause of long-term graft loss after renal transplantation. Major histocompatibility complex (MHC) incompatibilities as well as donor-specific alloantibodies are known risk factors, but the interaction of cellular and humoral mechanisms leading to allograft damage remains to be defined. The aim of this study was to analyze the impact of donor-specific post-transplant antibodies against a non-classical MHC Ib antigen apart from T-cell-dependent immune response. Therefore, we utilized a transplant rat model injecting a moAb directed against a donor MHC Ib molecule into athymic nude recipients lacking an immunocompetent T-cell system. METHODS: F344 kidneys were transplanted into LEW.RNU rats. Donor and recipient differ in the RT1.C locus (MHC Ib) but are phenotypically identical for the RT1.A (MHC I) and RT1.B/D (MHC II) loci. A moAb directed against the donors RT1.C(lv1) was injected into recipients with stable graft function. A control group remained untreated after transplantation. The rats were monitored for renal function and grafts were analyzed for morphological changes, infiltrating cells and C4d deposition. RESULTS: Antibody-infused rats developed renal impairment with massive urine albumin excretion. Histological changes consistent with antibody-mediated injury were interstitial fibrosis, tubular atrophy and severe glomerulopathy accompanied by an infiltrate of numerous macrophages. At time of death, grafts were negative for C4d at the peritubular capillaries and arterial endothelium. CONCLUSION: Antibodies directed against a MHC Ib antigen are able to induce allograft injury in T-cell-deficient rats. This model underlines the role of non-classical MHC disparities for long-term allograft survival and demonstrates the long-term results of antibody-induced allograft damage.

AB - BACKGROUND: Chronic allograft injury induced by immunological as well as non-immunological mechanisms is still a major cause of long-term graft loss after renal transplantation. Major histocompatibility complex (MHC) incompatibilities as well as donor-specific alloantibodies are known risk factors, but the interaction of cellular and humoral mechanisms leading to allograft damage remains to be defined. The aim of this study was to analyze the impact of donor-specific post-transplant antibodies against a non-classical MHC Ib antigen apart from T-cell-dependent immune response. Therefore, we utilized a transplant rat model injecting a moAb directed against a donor MHC Ib molecule into athymic nude recipients lacking an immunocompetent T-cell system. METHODS: F344 kidneys were transplanted into LEW.RNU rats. Donor and recipient differ in the RT1.C locus (MHC Ib) but are phenotypically identical for the RT1.A (MHC I) and RT1.B/D (MHC II) loci. A moAb directed against the donors RT1.C(lv1) was injected into recipients with stable graft function. A control group remained untreated after transplantation. The rats were monitored for renal function and grafts were analyzed for morphological changes, infiltrating cells and C4d deposition. RESULTS: Antibody-infused rats developed renal impairment with massive urine albumin excretion. Histological changes consistent with antibody-mediated injury were interstitial fibrosis, tubular atrophy and severe glomerulopathy accompanied by an infiltrate of numerous macrophages. At time of death, grafts were negative for C4d at the peritubular capillaries and arterial endothelium. CONCLUSION: Antibodies directed against a MHC Ib antigen are able to induce allograft injury in T-cell-deficient rats. This model underlines the role of non-classical MHC disparities for long-term allograft survival and demonstrates the long-term results of antibody-induced allograft damage.

M3 - SCORING: Zeitschriftenaufsatz

VL - 19

SP - 187

EP - 191

JO - TRANSPL IMMUNOL

JF - TRANSPL IMMUNOL

SN - 0966-3274

IS - 3-4

M1 - 3-4

ER -