TY - JOUR
T1 - Hydroxyurea to prevent brain injury in children with sickle cell disease (HU Prevent)—A randomized, placebo-controlled phase II feasibility/pilot study
AU - Casella, James F.
AU - Furstenau, Dana K.
AU - Adams, Robert J.
AU - Brambilla, Donald J.
AU - Lebensburger, Jeffrey D.
AU - Fehr, James J.
AU - Jordan, Lori C.
AU - King, Allison A.
AU - Ichord, Rebecca N.
AU - McKinstry, Robert C.
AU - Kraut, Michael A.
AU - Shaw, Dennis W.
AU - White, Desiree A.
AU - Whyte-Stewart, Donna A.
AU - Avadhani, Radhika
AU - Barron-Casella, Emily A.
AU - Cannon, Alicia D.
AU - Eaton, Cyd K.
AU - Riekert, Kristin A.
AU - Shay, Joanne E.
AU - Smith-Seidel, Cynthia A.
AU - Weiss, Diane C.
AU - Ostapkovich, Noeleen D.
AU - Vermillion, Krista
AU - Treine, Kevin E.
AU - Kingsbury, Claire E.
AU - Strouse, John J.
AU - Thompson, Richard E.
AU - Hanley, Daniel F.
N1 - Publisher Copyright:
© 2024 Wiley Periodicals LLC.
PY - 2024/10
Y1 - 2024/10
N2 - Central nervous system (CNS) injury is common in sickle cell disease (SCD) and occurs early in life. Hydroxyurea is safe and efficacious for treatment of SCD, but high-quality evidence from randomized trials to estimate its neuroprotective effect is scant. HU Prevent was a randomized (1:1), double-blind, phase II feasibility/pilot trial of dose-escalated hydroxyurea vs. placebo for the primary prevention of CNS injury in children with HbSS or HbS-β0-thalassemia subtypes of SCD age 12–48 months with normal neurological examination, MRI of the brain, and cerebral blood flow velocity. We hypothesized that hydroxyurea would reduce by 50% the incidence of CNS injury. Two outcomes were compared: primary—a composite of silent cerebral infarction, elevated cerebral blood flow velocity, transient ischemic attack, or stroke; secondary—a weighted score estimating the risk of suffering the consequences of stroke (the Stroke Consequences Risk Score—SCRS), based on the same outcome events. Six participants were randomized to each group. One participant in the hydroxyurea group had a primary outcome vs. four in the placebo group (incidence rate ratio [90% CI] 0.216 [0.009, 1.66], p =.2914) (~80% reduction in the hydroxyurea group). The mean SCRS score was 0.078 (SD 0.174) in the hydroxyurea group, 0.312 (SD 0.174) in the placebo group, p =.072, below the p-value of.10 often used to justify subsequent phase III investigations. Serious adverse events related to study procedures occurred in 3/41 MRIs performed, all related to sedation. These results suggest that hydroxyurea may have profound neuroprotective effect in children with SCD and support a definitive phase III study to encourage the early use of hydroxyurea in all infants with SCD.
AB - Central nervous system (CNS) injury is common in sickle cell disease (SCD) and occurs early in life. Hydroxyurea is safe and efficacious for treatment of SCD, but high-quality evidence from randomized trials to estimate its neuroprotective effect is scant. HU Prevent was a randomized (1:1), double-blind, phase II feasibility/pilot trial of dose-escalated hydroxyurea vs. placebo for the primary prevention of CNS injury in children with HbSS or HbS-β0-thalassemia subtypes of SCD age 12–48 months with normal neurological examination, MRI of the brain, and cerebral blood flow velocity. We hypothesized that hydroxyurea would reduce by 50% the incidence of CNS injury. Two outcomes were compared: primary—a composite of silent cerebral infarction, elevated cerebral blood flow velocity, transient ischemic attack, or stroke; secondary—a weighted score estimating the risk of suffering the consequences of stroke (the Stroke Consequences Risk Score—SCRS), based on the same outcome events. Six participants were randomized to each group. One participant in the hydroxyurea group had a primary outcome vs. four in the placebo group (incidence rate ratio [90% CI] 0.216 [0.009, 1.66], p =.2914) (~80% reduction in the hydroxyurea group). The mean SCRS score was 0.078 (SD 0.174) in the hydroxyurea group, 0.312 (SD 0.174) in the placebo group, p =.072, below the p-value of.10 often used to justify subsequent phase III investigations. Serious adverse events related to study procedures occurred in 3/41 MRIs performed, all related to sedation. These results suggest that hydroxyurea may have profound neuroprotective effect in children with SCD and support a definitive phase III study to encourage the early use of hydroxyurea in all infants with SCD.
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U2 - 10.1002/ajh.27423
DO - 10.1002/ajh.27423
M3 - Article
C2 - 38953438
AN - SCOPUS:85197279391
SN - 0361-8609
VL - 99
SP - 1906
EP - 1916
JO - American journal of hematology
JF - American journal of hematology
IS - 10
ER -