Defining the Risk of Elective Cyclosporine Withdrawal in Stable Kidney Transplant Recipients

Anjum, Shakeel; Andany, Magdalena Adeva; McClean, Jeffrey C.; Danielson, Barbara; Kasiske, Bertram L.

doi:10.1034/j.1600-6143.2002.020210.x

Cited by 15 publications

(7 citation statements)

References 31 publications

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“…Future clinical trials are needed to study the impact of interventions that reduce the risk of CHD, NODAT, and also metabolic syndrome. Such trials could study the impact of steroid avoidance [35], CNI withdrawal [36], switching from CNIs to mTOR inhibitors [37], and higher doses of mycophenolate mofetil along with lower levels of CNIs, on modifying the risks of CHD, NODAT, and metabolic syndrome. Trials studying new agents that increase HDL cholesterol could test whether or not these agents modify the risks of CHD and metabolic syndrome [38].…”

Section: Discussionmentioning

confidence: 99%

Clinical diagnosis of metabolic syndrome: predicting new-onset diabetes, coronary heart disease, and allograft failure late after kidney transplant

Israni¹,

Snyder²,

Skeans³

et al. 2012

Transplant International

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Summary Metabolic syndrome is associated with coronary heart disease (CHD) and new‐onset diabetes after kidney transplant (NODAT). Using data collected from transplant centers worldwide for the Patient Outcomes in Renal Transplantation study, we examined associations of metabolic syndrome (n = 2253 excluding recipients with diabetes pretransplant), CHD (n = 2253), and NODAT (n = 1840 further excluding recipients with diabetes in the first year post‐transplant), with the primary outcome of allograft failure. We assessed risk factors associated with secondary outcomes of metabolic syndrome, NODAT, and CHD after adjusting for type of baseline immunosuppression and transplant center effects. Metabolic syndrome prevalence was 39.8% at 12–24 months post‐transplant and 35.4% at 36–48 months. Metabolic syndrome was independently associated with NODAT (hazard ratio 3.46, 95% confidence interval 2.40–4.98, P < 0.0001), CHD (2.03, 1.16–3.52, P = 0.013), and allograft failure (1.36, 1.03–1.79, P = 0.028). Allograft failure occurred in 218 patients (14.6%). After adjustment for metabolic syndrome, NODAT (1.63, 1.18–2.24, P = 0.003) and CHD (5.48, 3.27–9.20, P < 0.0001) remained strongly associated with increased risk of allograft failure. Metabolic syndrome, NODAT, and CHD are risk factors for allograft failure. NODAT and CHD are risk factors for allograft failure, independent of metabolic syndrome.

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Section: Discussionmentioning

confidence: 99%

Clinical diagnosis of metabolic syndrome: predicting new-onset diabetes, coronary heart disease, and allograft failure late after kidney transplant

Israni¹,

Snyder²,

Skeans³

et al. 2012

Transplant International

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“…Anjum et al (17) reported an increased risk for patients with both two HLA-B and two HLA-DR mismatches. The measurement of the frequency of precursor cytotoxic T lymphocytes in the peripheral blood could allow identification of patients in whom minimization of immunosuppression can be achieved safely (9,18).…”

Section: Discussionmentioning

confidence: 99%

Predictive Factors of Acute Rejection after Early Cyclosporine Withdrawal in Renal Transplant Recipients Who Receive Mycophenolate Mofetil

Hazzan¹,

Labalette²,

Copin³

et al. 2005

Journal of the American Society of Nephrology

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The aim of this randomized, open-labeled trial was to compare the incidence of acute rejection after an early (3 mo posttransplantation) withdrawal of cyclosporine (CsA) or mycophenolate mofetil (MMF) in renal transplantation. Among 218 eligible recipients, 108 nonsensitized, rejection-free patients who were under a triple drug regimen (CsA-MMF-prednisone) and had received a first kidney from a deceased donor were enrolled. At 3 mo after graft, they were gradually withdrawn from CsA (MMF group, n ‫؍‬ 54) or MMF (CsA group, n ‫؍‬ 54). A graft biopsy and a pharmacokinetic study of CsA and mycophenolic acid were systematically performed before the randomization. At 1 yr, graft and patient survival rates were 100% in each group. Renal function was improved in the MMF group compared with the CsA group (Cockcroft calculated clearance 64.7 ؎ 18.7 versus 56.5 ؎ 18.0 ml/min; P ‫؍‬ 0.023). However, the probability of acute rejection was higher in the MMF group (18.5 versus 5.6%; P ‫؍‬ 0.045). The 10 patients who developed acute rejection after CsA withdrawal had a significantly higher incidence of borderline changes on the randomization biopsy than the 44 rejection-free patients (five of 10 versus eight of 44; P ‫؍‬ 0.034), and they displayed a lower area under the curve of mycophenolic acid (43 ؎ 9 versus 58 ؎ 22 mg/h per L; P ‫؍‬ 0.045). Multivariate analysis confirmed that borderline changes and area under the curve of mycophenolic acid were significant risk factors of acute rejection after CsA discontinuation. It is concluded that a systematic graft biopsy and a pharmacokinetic study of mycophenolic acid are needed to reduce the risk for acute rejection after CsA withdrawal.

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“…Although acute rejection occurred more frequently in patients electing CsA withdrawal, there was no difference in graft survival over nearly 6 years of follow-up compared with patients electing to remain on CsA. The risk of acute rejection was similar in patients treated with MMF, and those treated with AZA (4/67; 6% versus 26/314; 8%), although the small number of patients receiving MMF precludes drawing firm conclusions regarding the impact of these agents on acute rejection (41).…”

Section: Cni Withdrawal Regimensmentioning

confidence: 70%

“…Anjum et al (41) evaluated risk factors for acute rejection in a large cohort of stable renal transplant patients (nϭ464) undergoing voluntary CsA withdrawal. CsA withdrawal was begun 1 year after transplant/last rejection episode.…”

Section: Cni Withdrawal Regimensmentioning

confidence: 99%

Toxicity-Sparing Protocols Using Mycophenolate Mofetil in Renal Transplantation

Land

Vincenti²

2005

Transplantation

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The introduction of triple-therapy regimens that include a calcineurin inhibitor (CNI), steroids, and azathioprine greatly reduced the risk of acute rejection in renal transplantation. However, the long-term use of both CNIs and steroids is associated with serious toxicities that ultimately can impact patient/graft survival. Mycophenolate mofetil (MMF), a highly effective immunosuppressant with no known nephrotoxicity, has been shown to provide benefits in preserving long-term renal allograft function relative to azathioprine. For these reasons, MMF has become an integral component of toxicity-sparing maintenance regimens that seek to minimize patient exposure to CNIs and steroids. This paper provides an overview of current strategies for reducing the toxicities associated with these agents, which include both withdrawal and avoidance regimens with or without induction therapy. Data are accumulating that toxicity-sparing regimens involving MMF are safe and decrease the risk of side effects that accompany the use of CNIs and steroids. Future studies will determine how to best implement these regimens in the renal transplant population.

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Defining the Risk of Elective Cyclosporine Withdrawal in Stable Kidney Transplant Recipients

Cited by 15 publications

References 31 publications

Clinical diagnosis of metabolic syndrome: predicting new-onset diabetes, coronary heart disease, and allograft failure late after kidney transplant

Clinical diagnosis of metabolic syndrome: predicting new-onset diabetes, coronary heart disease, and allograft failure late after kidney transplant

Predictive Factors of Acute Rejection after Early Cyclosporine Withdrawal in Renal Transplant Recipients Who Receive Mycophenolate Mofetil

Toxicity-Sparing Protocols Using Mycophenolate Mofetil in Renal Transplantation

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