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Autor(es)
O’Hearn, Katie; Menon, Kusum; Weiler, Hope A.; Amrein, Karin; Fergusson, Dean; Gunz, Anna; Bustos, Raul; Campos, Roberto; Catalan, Valentina; Roedl, Siegfried; Tsampalieros, Anne; Barrowman, Nick; Geier, Pavel; Henderson, Matthew; Khamessan, Ali; Lawson, Margaret L.; McIntyre, Lauralyn; Redpath, Stephanie; Jones, Glenville; Kaufmann, Martin; McNally, Dayre |
ISSN:
1471-2431 |
Idioma:
eng |
Fecha:
2023-12 |
Tipo:
Artículo |
Revista:
BMC Pediatrics |
Datos de la publicación:
vol. 23 Issue: no. 1 Pages: |
DOI:
10.1186/s12887-023-04205-9 |
Descripción:
Publisher Copyright: © 2023, BioMed Central Ltd., part of Springer Nature. |
Resumen:
Background: Vitamin D deficiency (VDD) is highly prevalent in the pediatric intensive care unit (ICU) and associated with worse clinical course. Trials in adult ICU demonstrate rapid restoration of vitamin D status using an enteral loading dose is safe and may improve outcomes. There have been no published trials of rapid normalization of VDD in the pediatric ICU. Methods: We conducted a multicenter placebo-controlled phase II pilot feasibility randomized clinical trial from 2016 to 2017. We randomized 67 critically ill children with VDD from ICUs in Canada, Chile and Austria using a 2:1 randomization ratio to receive a loading dose of enteral cholecalciferol (10,000 IU/kg, maximum of 400,000 IU) or placebo. Participants, care givers, and outcomes assessors were blinded. The primary objective was to determine whether the loading dose normalized vitamin D status (25(OH)D > 75 nmol/L). Secondary objectives were to evaluate for adverse events and assess the feasibility of a phase III trial. Results: Of 67 randomized participants, one was withdrawn and seven received more than one dose of cholecalciferol before the protocol was amended to a single loading dose, leaving 59 participants in the primary analyses (40 treatment, 19 placebo). Thirty-one/38 (81.6%) participants in the treatment arm achieved a plasma 25(OH)D concentration > 75 nmol/L versus 1/18 (5.6%) the placebo arm. The mean 25(OH)D concentration in the treatment arm was 125.9 nmol/L (SD 63.4). There was no evidence of vitamin D toxicity and no major drug or safety protocol violations. The accrual rate was 3.4 patients/month, supporting feasibility of a larger trial. A day 7 blood sample was collected for 84% of patients. A survey administered to 40 participating families showed that health-related quality of life (HRQL) was the most important outcome for families for the main trial (30, 75%). Conclusions: A single 10,000 IU/kg dose can rapidly and safely normalize plasma 25(OH)D concentrations in critically ill children with VDD, but with significant variability in 25(OH)D concentrations. We established that a phase III multicentre trial is feasible. Using an outcome collected after hospital discharge (HRQL) will require strategies to minimize loss-to-follow-up. Trial Registration. Clinicaltrials.gov NCT02452762 Registered 25/05/2015. |
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