Malnutrition Clinical Trial
Official title:
Randomized Controlled Trial of a Reduced Carbohydrate Formulation of F75 Therapeutic Milk Among Children With Severe Acute Malnutrition
Inpatient treatment for complicated severe acute malnutrition (SAM) continues to have a high
mortality in Africa. This is partly because children are commonly brought for admission
because they are seriously ill, rather than being brought to hospital because of
malnutrition alone. Mortality rates are especially high where SAM is complicated by HIV or
TB. The early phase of inpatient nutritional treatment for severe acute malnutrition is
based on a low-protein milk known as F75, which is given to improve metabolic homeostasis
prior to the re-feeding to achieve catch-up growth. F75 provides a high proportion of energy
from carbohydrates, including sucrose, lactose and maltodextrin. However, malabsorption of
different types of carbohydrates, but lactose in particular, is known to occur in SAM and
may lead to osmotic diarrhoea. Diarrhoea is common in children with SAM and is associated
with increased mortality. Furthermore, switching from a catabolic state to a high energy
diet that consists of predominantly carbohydrates can lead to 're-feeding syndrome' that may
lead to severe electrolyte abnormalities and multiple organ dysfunction.
The aim of this trial is to determine whether reducing the carbohydrate content of F75, and
removing lactose, improves the stabilisation of severely malnourished children. The trial
will involve randomising children who are eligible to receive F75 milk to either the current
formulation or a revised formulation. Both formulations will be given according to current
recommendations regarding frequency of feeding and caloric value. Since the purpose of F75
is to stabilise the child metabolically and biochemically, the primary endpoint of the trial
will be time to stabilisation (the end of the first phase of treatment for severe acute
malnutrition). Blood and stool samples at admission and after three days will be used to
determine the effects on carbohydrate and fat malabsorption and evidence of the re-feeding
syndrome. Children will be followed up until discharge from hospital. The project has been
planned in consultation with the World Health Organisation (WHO) and, if the revised
formulation of F75 results in improved outcomes, will lead to a global change in
recommendations for its formulation.
Admission to hospital with complicated severe acute malnutrition (SAM) in Africa commonly
has a case fatality of 10-30%. Importantly, children are usually admitted to hospital
because they are severely ill rather than for malnutrition alone. Mortality may be improved
to some extent by adherence to WHO recommended management, but the direct application of
these guidelines to all contexts is controversial. The WHO guidelines were designed on the
basis of historical data on nutrient requirements and medical treatments and almost none of
the recommendations are supported by evidence from clinical trials.
For the treatment of complicated inpatient SAM, the guidelines consist of three distinct
phases of treatment: phase 1 or stabilization phase where a low protein, liquid diet (F75)
is introduced with a reduced energy intake (80-100 kcal/kg/day). Once a child has
stabilised, there is a 'transition phase' consisting of either ready to use therapeutic
foods (RUTF) with supplemental F75 or alternatively another milk formula known as F100. RUTF
is a peanut based, energy dense supplement used to obtain catch-up growth. F100 is a liquid
formula with a higher energy density and protein content than F75. The caloric intake is
increased daily to a maximum of 130 kcal/kg/day. Finally, 'Phase 3' is the recovery phase
during which the aim is to achieve catch-up growth with either RUTF or F100.
Typically, the highest mortality rate is found in the early phases of treatment. Children
who fail treatment early often have profuse diarrhoea, signs of circulatory insufficiency
which is hard to treat. The most recent reports from Zambia and Kenya note a prevalence of
diarrhoea of more than 60% amongst children with SAM and it is associated with increased
mortality. Currently at Kilifi County Hospital and Coast Provincial General Hospital, ~20%
of children are given either a diluted or lactose-free milk feed during rehabilitation of
SAM, although there are no specific guidelines for this. Diarrhoea may be caused by a viral
or bacterial gastroenteritis, sepsis, or may be nutritionally induced (osmotic). There are
no routinely available tests to distinguish osmotic from infective or other causes of
diarrhoea in hospitals in sub-Saharan Africa.
The proportion of energy derived from carbohydrates in F75 is high. The carbohydrates in F75
milk (as well as F100 and RUTF) consist of a mixture of maltodextrin, sucrose and lactose.
Disaccharides such as maltose, lactose or sucrose are normally hydrolysed into
monosaccharides by disaccharidases localized at the tip of small intestinal villi. The
monosaccharides such as glucose and galactose can then be transported across the apical
membrane through Na+ dependent glucose transporter, whilst fructose makes use of a
facilitative fructose transporter. There is limited information on the intestinal function
and intestinal carbohydrate absorption in malnourished children. However, data from Jamaica
and South Africa suggest that there is impaired absorption of disaccharides (lactose and
sucrose), regardless of the presence or suspicion of gastroenteritis. Limited histological
evidence has shown intestinal atrophy in children with SAM. These data are consistent with
clinical signs of lactose malabsorption found in children with severe malnutrition.
Recently, evidence of impaired absorption of monosaccharide glucose in children with SAM was
reported in Malawi.
Apart from diarrhoea, early deterioration may also be related to severe metabolic
derangements due to a sudden change from a catabolic to an anabolic state, resulting in
refeeding syndrome. Refeeding syndrome is characterized by hypophosphataemia, hypokalaemia,
hypomagnesaemia and sodium retention. These severe electrolyte disturbances can lead to
impaired cardiac, pulmonary and neurological function and are often hard to treat. By
receiving energy predominantly from sugars, pancreatic insulin secretion is increased which
induces uptake of electrolytes including phosphate and potassium, into cells. Furthermore,
as protein synthesis is stimulated, increased production of adenosine tri-phosphate (ATP)
leads to a higher cellular demand for phosphate. Although insulin secretion appears to be
partially impaired in the early stages of refeeding, hypophosphatemia is a common feature
during refeeding of malnourished children, and is associated with mortality.
In this trial, the investigators aim to evaluate the outcome of using a revised formulation
of F75 milk with reduced carbohydrate composition and without lactose, compared to the
current formulation of F75 during the initial stabilisation period amongst children with
severe acute malnutrition. In the new formulation, more will be provided by lipids and the
total energy provided will be unchanged. The trial will be undertaken in two hospitals in
Kenya and one hospital in Malawi.
Enrolment and follow up was completed in December 2015, laboratory analysis of plasma and
faecal samples in ongoing.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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