Malaria Clinical Trial
Official title:
Optimizing Hydroxyurea Therapy in Children With Sickle Cell Anemia In Malaria Endemic Areas: The NOHARM Maximum Tolerated Dose (MTD) Study
The Novel use Of Hydroxyurea in an African Region with Malaria (NOHARM) study is the first
placebo-controlled randomized clinical trial of hydroxyurea treatment in a malaria endemic
region. NOHARM has now achieved full enrollment; all children have completed the blinded
portion of the protocol and are in the open-label study treatment portion.
This extension study of maximum tolerated dose (MTD), addresses the next critical set of
questions about the optimal dosing and monitoring of hydroxyurea treatment for children with
SCA in low-resource settings. By providing guidance about optimal hydroxyurea treatment, the
NOHARM MTD Study will directly inform policies that can transform the health of African
children living with SCA.
All children enrolled in NOHARM received hydroxyurea treatment at a fixed daily dose of 20
mg/kg/day. This dose was selected as a likely safe dose, but does not escalate hydroxyurea to
MTD as is commonly done in the US. Without this information, we cannot know whether
hydroxyurea treatment at the MTD would be feasible (since it requires closer monitoring to
avoid hematological toxicities), safe (since adverse events may be greater with MTD, risk of
malaria may be altered by MTD, and risk of infections as a result of neutropenia could also
be greater with MTD) or beneficial (MTD is associated with higher hemoglobin and fetal
hemoglobin concentration).
In this extension MTD study of open-label hydroxyurea for children in NOHARM who complete the
initial study, consented children will be randomized to either fixed-dose or MTD hydroxyurea
treatment for a minimum of 24 months. If hydroxyurea treatment continues to prove safe and
effective in this low-resource malaria endemic area, and an optimal dosing scheme is
determined, then the long-term goal is for all study children to transition to hydroxyurea
treatment provided through the Ugandan Ministry of Health. To provide for a smooth
transition, we will continue all children at either MTD or fixed dose hydroxyurea until a
common end date (November 2019), at which time all study participants will have received a
minimum of 24 months of additional hydroxyurea (either MTD or fixed dose). Addmedica, the
Paris-based pharmaceutical company that provides the current active drug and placebo for the
NOHARM trial, has agreed to provide additional hydroxyurea for this MTD study at no cost to
the study or the participants.
The Specific Aims of the NOHARM MTD proposal include two initiatives for participants who are
currently enrolled in NOHARM:
Aim 1. To determine the safety and efficacy of maximum tolerated dose (MTD) vs. fixed dose
(20 mg/kg/day) hydroxyurea treatment in children with SCA in a low-resource, malaria endemic
setting. For safety, we will compare adverse events and severe adverse events, including
hematologic toxicities. For efficacy, we will assess hemoglobin level, fetal hemoglobin
percentage (% HbF), and incidence of vaso-occlusive events such as pain crisis and acute
chest syndrome.
Aim 2. To compare the clinical outcomes of MTD vs. fixed dose hydroxyurea treatment in
children with SCA in a low-resource, malaria endemic setting. Clinical outcomes assessed will
include growth and malaria incidence over a 24-month follow-up period, and differences in
renal, splenic, and cerebrovascular function between study entry and 24-month follow-up.
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