Acute cellular rejection of human renal tissue by adoptive transfer of allogeneic human peripheral blood mononuclear cells into chimeric rats: sequential gene expression of cytokines, chemokines and cytolytic effector molecules, and their regulation by CTLA-4-Ig

doi:10.1093/intimm/11.10.1673

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International Immunology, Vol. 11, No. 10, 1673-1683, October 1999
© 1999 Japanese Society for Immunology

Acute cellular rejection of human renal tissue by adoptive transfer of allogeneic human peripheral blood mononuclear cells into chimeric rats: sequential gene expression of cytokines, chemokines and cytolytic effector molecules, and their regulation by CTLA-4–Ig

Benjamin Dekel, Wulf O. Böcher, Hadar Marcus, Alex Yussim and Yair Reisner

Department of Immunology, The Weizmann Institute of Science, Rehovot 76100, Israel.

Correspondence to: Y. Reisner

T_h1- and T_h2-related cytokines (IFN- ${gamma}$ , IL-2, IL-4, IL-10), ß-chemokines(RANTES, macrophage inflammatory protein-1ß) and theirreceptor [chemotatic cytokine receptor (CCR) 5], and the cytolyticeffector molecule [Fas ligand (FasL)] play an essential rolein regulating and co-ordinating acute renal allograft rejection.A chimeric model of acute cellular rejection which involvessubcapsular grafting of human renal tissue in the kidneys ofimmunodeficient rats and subsequent i.p. infusion of allogeneichuman peripheral blood mononuclear cells (PBMC) was used tostudy cellular infiltration patterns and sequential intragraftgene expression of these key inflammatory mediators. We foundthat while all molecules are expressed within the human renalimplant at specific time points following infusion of allogeneichuman PBMC, peak mRNA expression of IFN- ${gamma}$ , IL-2, RANTES and CCR5is associated with a phase of human mononuclear infiltrationand accumulation, prior to graft destruction (induction phase).A short burst of FasL gene expression is found at the end ofinduction and at the onset of graft deterioration. IL-4 mRNA,which is hardly detectable, and IL-10 mRNA, which appears earlyand persists throughout follow-up at high levels, both peakafter the induction phase with the advent of graft destruction.Furthermore, treatment with CTLA-4–Ig, which hardly affectsmigration of human effector cells into graft tissue, is associatedwith a temporary reduction in gene transcript levels for allinflammatory mediators, especially IL-2 and IL-4, reduced apoptosisin the graft and amelioration of tissue injury. Thus, developmentof acute cellular rejection in our chimeric model involves aco-ordinated pattern of gene expression, in which CTLA-4–Igpromotes its effects by transient inactivation of infiltratinghuman cells.

Keywords: allograft rejection, animal model, apoptosis, RT-PCR, SCID, T_h1, T_h2

Transmitting editor: A. Fischer

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