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Human chronic kidney allograft rejection is accompanied by increased intraglomerular cathepsin B and L activity
Authors:L. Paczek  J. Pazik  M. Teschner  R. M. Schaefer  W. Rowinski  J. Szmidt  K. Abgarowicz  L. Gradowska  M. Morzycka-Michalik  A. Heidland
Affiliation:Transplantation Institute, Nowogrodzka 59, 02006 Warsaw, Poland
Abstract:Abstract The major reason for late graft losses is chronic rejection. Recently, a large number of studies have indicated that proteolytic enzymes play an important role as mediators of glomerular injury. The cysteine proteinases cathepsins B and L degrade structural matrix proteins such as type I collagen and laminin. We investigated intraglomerular protease activities in 12 patients after kidney graftectomy because of end-tage renal disease following chronic rejection. A group of 12 patients undergoing nephrectomy because of cancer served as controls using only non-involved parts of the kidney. The activities of cathepsins B and L in homogenates of isolated glomeruli were measured fluorometrically methylcoumarylamidc substrates and related to DNA content. In rejected kidney allografts we observed significantly enhanced intraglomerular cathepsin B activity and cathepsin B + L activity.
Keywords:Kidney allograft    Chronic rejection    Intraglomerular    cathepsins B and L activities
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