Renal failure after clinical heart transplantation is associated with the TGF-β1 codon 10 gene polymorphism

Abstract

Background: To determine whether genetic factors are involved in the development of renal dysfunction due to cyclosporine nephrotoxicity, we analyzed 2 polymorphisms in the signal sequence of the transforming growth factor (TGF)–β1 gene; codon 10 (Leu 10 → Pro) and codon 25 (Arg 25 → Pro). Method Using sequence specific oligonucleotide probing, we analyzed both TGF-β1 gene polymorphisms in cardiac allograft recipients ( n = 168) who survived at least 1 year with minimal follow-up of 7 years. Patients received cyclosporine and steroids as maintenance immunosuppressive therapy. Renal dysfunction was defined as a serum creatinine ≥ 250 μmol/liter. Results Renal dysfunction was observed in 2% (3/168) of the patients at 1 year, in 7% (11/160) at 3 years, in 12% (18/152) at 5 years, and in 20% (26/131) at 7 years post-transplantation. The genotypic distributions for TGF-β1 codon 10 were 7% Pro/Pro, 61% Pro/Leu, and 32% Leu/Leu, and for codon 25 these percentages were 1% Pro/Pro, 12% Pro/Arg, and 87% Arg/Arg. We found an association between the TGF-β1 genotype encoding proline at codon 10 and renal dysfunction. At 7 years post-transplantation, 26% (23/89) of the patients with the heterozygous Pro/Leu or homozygous Pro/Pro genotype had renal dysfunction vs only 7% (3/42) of the patients with the homozygous Leu/Leu genotype ( p = 0.017). For the TGF-β1 codon 25 genotypes, we found no association between TGF-β1 genotypes and renal dysfunction. Conclusion Our data support the hypothesis that TGF-β1 is involved in the process leading to renal insufficiency in cyclosporine-treated cardiac allograft recipients. In these patients the presence of TGF-β1 Pro 10 might be a risk factor.