Literature DB >> 3925760

Impact of cyclosporine on renal transplant practice at the University of Texas Medical School at Houston.

B D Kahan, R H Kerman, C A Wideman, S M Flechner, M Jarowenko, C T Van Buren.   

Abstract

CsA has improved the outcome of renal allotransplantation with CAD and LRD kidneys. CsA mitigates risk factors heretofore presenting substantial obstacles to CAD transplantation: HLA matching, pretransplant splenectomy, extensive numbers of conditioning blood transfusions, and old age. In LRD transplantation, CsA obviates the need for donor-specific transfusions in the haploidentical situation, and for prednisone in the HLA-identical setting. The incidence of drug-induced nephrotoxicity beyond six months is 30% with the degree of dysfunction proportionate to the degree of histo-incompatibility, suggesting that subclinical allograft rejection due to overzealous dose reduction may compromise allograft function. At present, total conversion from CsA to Aza appears ill-advised; even patients who never suffered allograft rejection under CsA therapy frequently lose their allograft when the inferior level of Aza suppression is substituted. Drug-induced hypertension, a modestly significant factor, diminishes further by two years posttransplant. The benefit of CsA therapy is a reduced incidence of 19% initial and 10% recurrent rejection episodes. Of great importance is the observation that 17% of rejection episodes followed patient noncompliance. Further, the incidence of bacterial infections was greatly reduced, and viral infections modestly lessened. Only the occurrence of pneumocystis carinii was increased, but 92% of patients survived in spite of serious pulmonary infection. Development of a consistent CsA regimen has reduced the median initial hospitalization to 12.5 days for LRD and 14 days for CAD, a level well within the range stipulated for the Disease-Related Guidelines of the Medicare Program. Furthermore, readmission is less frequent; one-third of patients never reenter the hospital.(ABSTRACT TRUNCATED AT 250 WORDS)

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Year:  1985        PMID: 3925760     DOI: 10.1016/s0272-6386(85)80157-8

Source DB:  PubMed          Journal:  Am J Kidney Dis        ISSN: 0272-6386            Impact factor:   8.860


  7 in total

1.  Renal function following kidney transplantation in children treated with cyclosporine.

Authors:  U B Berg; A B Bohlin
Journal:  Pediatr Nephrol       Date:  1992-07       Impact factor: 3.714

Review 2.  Complications of cyclosporin therapy.

Authors:  B D Kahan; S M Flechner; M I Lorber; C Jensen; D Golden; C T Van Buren
Journal:  World J Surg       Date:  1986-06       Impact factor: 3.352

Review 3.  Renal transplantation in patients 65 years old or older.

Authors:  C A Vivas; D P Hickey; M L Jordan; R M O'Donovan; J Lutins; R Shapiro; T E Starzl; T R Hakala
Journal:  J Urol       Date:  1992-04       Impact factor: 7.450

4.  Sirolimus pharmacokinetics in pediatric renal transplant recipients receiving calcineurin inhibitor co-therapy.

Authors:  Asher D Schachter; Mark R Benfield; Robert J Wyatt; Paul C Grimm; Robert S Fennell; John T Herrin; David S Lirenman; Ruth A McDonald; Ricardo Munoz-Arizpe; William E Harmon
Journal:  Pediatr Transplant       Date:  2006-12

5.  Causes of renal allograft loss. Progress in the 1980s, challenges for the 1990s.

Authors:  E J Schweitzer; A J Matas; K J Gillingham; W D Payne; P F Gores; D L Dunn; D E Sutherland; J S Najarian
Journal:  Ann Surg       Date:  1991-12       Impact factor: 12.969

6.  Short sirolimus half-life in pediatric renal transplant recipients on a calcineurin inhibitor-free protocol.

Authors:  Asher D Schachter; K E Meyers; L D Spaneas; J A Palmer; M Salmanullah; J Baluarte; K L Brayman; W E Harmon
Journal:  Pediatr Transplant       Date:  2004-04

7.  Clinical experience in 200 renal transplants at Catholic Medical Center.

Authors:  Y S Yoon; B K Bang; Y B Koh; Y K Lee; T G Whang; M S Yoon; Y H Park; K S Shin; S N Kim
Journal:  Korean J Intern Med       Date:  1987-01       Impact factor: 2.884

  7 in total

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