TRANSFORMING GROWTH FACTOR-?? LEVELS IN HUMAN ALLOGRAFT CHRONIC FIBROSIS CORRELATE WITH RATE OF DECLINE IN RENAL FUNCTION1

Autor: Roy D. Bloom, D.A. Laskow, Moona Alidoost, Oleh Pankewycz, Gail Haussman, Carolyn E. Grotkowski, Bulent Cuhaci, Lavjay Butani, M. S. A. Kumar, Bruce Pratt, Benjamin C. Sturgill, Kathy Cahill
Rok vydání: 1999
Předmět:
Zdroj: Transplantation. 68:785-790
ISSN: 0041-1337
DOI: 10.1097/00007890-199909270-00010
Popis: BACKGROUND Long-term renal transplant function is limited primarily by a progressive scarring process loosely termed "chronic rejection, chronic allograft nephropathy, or allograft fibrosis." Although the etiology of transplant fibrosis is uncertain, several possible factors including chronic cyclosporin A (CsA) exposure may contribute to its pathogenesis. CsA stimulates renal fibrosis perhaps through the induction of the potent pro-sclerotic growth factor, transforming growth factor beta (TGFbeta). Previously, we demonstrated that, in human transplant biopsies, acute CsA toxicity but not acute tubular necrosis is associated with elevated levels of renal TGFbeta protein. We now examine whether long-term CsA treatment (>1 year) is associated with elevated levels of intra-allograft TGFbeta and whether heightened expression of TGFbeta is clinically significant. METHODS Using immunohistochemical techniques, we determined the relative level of expression of intrarenal TGFbeta protein in transplant biopsies. We studied biopsies obtained from 40 CsA-treated patients that were diagnosed as having chronic allograft fibrosis. Biopsies were scored as having minimal or high levels of TGFbeta. RESULTS Seventy-two percent of patients expressed high levels of intra-allograft TGFbeta. This group of patients lost renal function at an average rate of -19.5+/-17.3 ml/min/year. In contrast, patients with minimal or no TGFbeta expression experienced a decline of only -6.2+/-4.1 ml/min/year (P=0.01). CONCLUSIONS These results suggest that the majority of CsA-treated patients with biopsy proven chronic fibrosis have elevated levels of intra-graft TGFbeta that correlates with an increased rate of decline in renal function.
Databáze: OpenAIRE