Sickle Cell Disease Clinical Trial
Official title:
Development of a Ready-to-use Nutraceutical Food for Patients With Sickle Cell Disease (SCD): Testing of Vascular Support Components
Sickle cell disease (SCD) is the most common inherited disorder worldwide affecting 300,000 births annually, most occuring in sub-Saharan Africa (SSA) where poor detection and care result in high childhood mortality, malnutrition, illness and disability in survivors. SCD is caused by abnormal haemoglobin, the compound in red blood cells(RBC) that carries oxygen. Much of the disability in SCD may be caused by vascular damage from the breakdown of damaged RBC. Research in high-income countries has led to some effective therapies but these are currently costly and complex. The investigators will test two different formulations of an affordable, ready-to-use supplementary food (RUSF) specifically tailored for children with SCD. As well as containing energy, protein, essential fats, vitamins and minerals, the vascular RUSF (RUSFv) will be fortified with the amino-acids arginine and citrulline and be delivered with a daily chloroquine dose to create a novel "nutraceutical" intervention. Arginine is converted to nitric oxide which is essential for vascular health. Arginine levels are low in SCD because the arginine-degrading enzyme, arginase, is released from RBCs. The investigators propose that by supplying additional arginine (and citrulline which converts to arginine) and suppressing arginase activity (an action of chloroquine) the investigators can improve vascular function. Our study will test this theory, and if provision of RUSF improves growth in children with SCD.
Arginine is the substrate of endothelial nitric oxide (NO) synthase. Citrulline converts to
arginine and has a greater bioavailability than arginine. Chloroquine is a competitive
inhibitor of arginase which is released from lysed red cells and possibly through liver
damage. Raised arginase predicts low plasma arginine levels and may predict clinical disease
severity.
The interventions being tested are designed to target:
(i) the moderate to severe growth retardation commonly observed in children with SCD
especially in low income countries; (ii) endothelial dysregulation secondary to low NO
bioavailability, inflammation and oxidant stress, hypothesised to underlie much of the
clinical pathology in SCD.
This study will test the following hypotheses:
1. That the provision of energy, protein and micronutrients within a ready to use
supplementary food will increase linear growth, weight gain and proportion of fat-free
mass in children with SCD.
2. That the provision of supplementary L-arginine and L-citrulline within the matrix of a
twice-daily RUSF plus daily chloroquine (CQ) for 4 months, compared to a standard RUSF
and weekly anti-malarial prophylaxis CQ to children with SCD will:
- Increase plasma arginine concentrations and the ratio of plasma arginine:
ornithine.
- Decrease or not alter plasma asymmetric dimethylarginine (ADMA) concentrations
- Improve NO-dependent vascular function as detected by an increase in maximum flow
mediated dilatation (FMDmax)
3. That the provision of daily CQ at a dosage of 2-3mg base/kg/day for 4 months to
children with SCD will:
- Decrease the activity of plasma arginase through competitive inhibition
- Decrease levels of plasma inflammatory markers
If successful then larger studies of efficacy and effectiveness would be needed to assess
long-term endpoints of hospitalization, stroke, and mortality. Existing evidence suggests
that the proposed intervention also has the potential to increase the efficacy of
hydroxyurea (HU) therapy. The successful development of an affordable ready-to-use
'nutraceutical' food with proven efficacy in growth promotion and vascular health could
represent a major step forward for SCD patients in low-income countries.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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