C. Fernández Camblor scite author profile

Objective: Studies evaluating renal transplant (RT) outcome in children who underwent an augmentation cystoplasty (AC) are contradictory and the current knowledge is based on studies with a limited number of patients. The aim of this study is to compare RT outcome between children who underwent AC and those without augmentation.Patients and methods: A total of 20p who underwent an AC prior to the RT (12 with ureter and 8 with intestine) were enrolled in the study and were compared to a control group of 24p without AC, transplanted in the same time period (1991–2011). Data including; age at transplant, allograft source, urological complications, urinary tract infections (UTI) incidence, the presence of VUR, and patient and graft survival were compared between the groups.Results: Mean age at RT and mean follow-up were 9.7 vs. 7.9 years and 6.9 vs. 7.9 years in the AC group and control group, respectively (NS). The graft originated in living donors for 60% of AC patients and 41.6% of the control RT patients. The rate of UTI were 0.01 UTI/patient/year and 0.004 UTI/patient/year in the augmented group and controls, respectively (p = 0.0001). In the AC group of 14p with UTIs, 10 (71%) had VUR and 5p out of 8 (62.5%) in the control group had VUR. In the AC group, of the 7p with ≥3 UTIs, 3 (43%) were non-compliant with CIC and the incidence of UTIs was not related with the type of AC or if the patient did CIC through a Mitrofanoff conduit or through the urethra. Graft function at the end of study was 92.9 ± 36.85 ml/min/m2 in the AC group and 88.17 ± 28.2 ml/min/m2 in the control group (NS). Graft survival at 10 years was also similar 88% in the AC group and 84.8% in controls. In the AC group 3p lost their grafts and 5 in the control group with respective mean follow-up of 10.6 ± 4.3 and 7.1 + 4.7 years.Conclusion: There are no significant differences in the RT outcome between children transplanted with AC or without. However, recurrent UTIs are more frequent in the former group and these UTIs are related with non-compliance with CIC or the presence of VUR but, even so, UTIs will not lead to impaired graft function in most of the patients.

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BK Virus Infection in Pediatric Renal Transplantation

Santoveña

Meseguer

Mejía

et al. 2015

Transplantation Proceedings

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Limited sampling strategies for tacrolimus exposure (AUC_0-24) prediction after Prograf^®and Advagraf^®administration in children and adolescents with liver or kidney transplants

et al. 2014

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SummaryTo develop limited sampling strategies (LSSs) to predict total tacrolimus exposure (AUC 0-24 ) after the administration of Advagraf â and Prograf â (Astellas Pharma S.A, Madrid, Spain) to pediatric patients with stable liver or kidney transplants. Forty-one pharmacokinetic profiles were obtained after Prograf â and Advagraf â administration. LSSs predicting AUC 0-24 were developed by linear regression using three extraction time points. Selection of the most accurate LSS was made based on the r 2 , mean error, and mean absolute error. All selected LSSs had higher correlation with AUC 0-24 than the correlation found between C 0 and AUC 0-24 . Best LSS for Prograf â in liver transplants was C 0_1.5_4 (r 2 = 0.939) and for kidney transplants C 0_1_3 (r 2 = 0.925). For Advagraf â , the best LSS in liver transplants was C 0_1_2.5 (r 2 = 0.938) and for kidney transplants was C 0_0.5_4 (r 2 = 0.931). Excluding transplant type variable, the best LSS for Prograf â is C 0-1-3 (r 2 = 0.920) and the best LSS for Advagraf â was C 0_0.5_4 (r 2 = 0.926). Considering transplant type irrespective of the formulation used, the best LSS for liver transplants was C 0_2_3 (r 2 = 0.913) and for kidney transplants was C 0_0.5_4 (r 2 = 0.898). Best LSS, considering all data together, was C 0_1_4 (r 2 = 0.898). We developed several LSSs to predict AUC 0-24 for tacrolimus in children and adolescents with kidney or liver transplants after Prograf â and/or Advagraf â treatment.

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Respiratory Disease in Aggregate Quarry Workers Related to Risk Factors and Pi Phenotype

Montes

Rego²,

Camblor³

et al. 2004

Journal of Occupational and Environmental Medicine

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Anti-GBM and anti-MPO antibodies coexist in a case of pulmonary renal syndrome

et al. 2005

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