4.4 Article

Influence of severity of anemia on clinical findings in infants with sickle cell anemia: Analyses from the BABY HUG study

Journal

PEDIATRIC BLOOD & CANCER
Volume 59, Issue 4, Pages 675-678

Publisher

WILEY
DOI: 10.1002/pbc.24037

Keywords

acute chest syndrome; hydroxyurea; pain; renal; sickle cell anemia; spleen; transcranial doppler

Funding

  1. National Heart, Lung, and Blood Institute/National Institutes of Health [N01-HB-07150, N01-HB-07160]
  2. Best Pharmaceuticals for Children Act
  3. National Institute of Child Health and Human Development

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Background Clinical complications of sickle cell anemia begin in infancy. BABY HUG (ClinicalTrials.gov, NCT00006400) was a NHLBI-NICHD supported randomized phase III placebo-controlled trial of hydroxyurea (HU) in infants (recruited at 918 months) unselected for clinical severity with sickle cell anemia. This secondary analysis of data from BABY HUG examines the influence of anemia on the incidence of sickle cell related complications, and the impact of hydroxyurea therapy in altering these events by comparing children with lower (<25th percentile) and higher (>75th percentile) hemoglobin concentrations at study entry. Procedure Infants were categorized by: (1) age-adjusted hemoglobin quartiles as determined by higher (Hi) and lower (Lo) hemoglobin concentrations at study entry (912 months old: <8.0 and >10.0?gm/dL; 1218 months old: <8.1 and >9.9?gm/dL) and (2) treatment arm (hydroxyurea or placebo). Four subgroups were created: placebo (PL) LoHb (n?=?25), PL HiHb (n?=?27), hydroxyurea (HU) LoHb (n?=?21), and HU HiHb (n?=?18). The primary and secondary endpoints of BABY HUG were analyzed by subgroup. Results Infants with lower hemoglobin at baseline were more likely to have a higher incidence of clinical events (acute chest syndrome, pain crisis, fever) as well as higher TCD velocities and lower neuropsychological scores at study exit. Hydroxyurea reduced the incidence of these findings. Conclusion Infants with more severe anemia are at risk for increased clinical events that may be prevented by early initiation of hydroxyurea. Pediatr Blood Cancer 2012;59:675678. (c) 2011 Wiley Periodicals, Inc.

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