Acute Infectious Diarrhoea in Children Clinical Trial
Official title:
Exploratory Study to Evaluate the Effect of L-isoleucine Supplemented Oral Rehydration Solution in the Treatment of Acute Diarrhoea in Children and in Inducing Innate Immunity
Efforts are continuing to improve the efficacy of oral rehydration solution in terms of reducing the severity (stool volume) and duration of diarrhoea (enhancement of recovery). Antimicrobial peptides, produced by the epithelial cells, represent an important component of the innate immunity of all epithelial surfaces of the body including intestine. Induction of expression of antimicrobial peptides on epithelial cell surface, may thus hasten recovery from infectious diarrhoea. Isoleucine is an essential amino acid that is easily available and not very expensive, and its addition to oral rehydration solution might help early clearance of diarrhoeal pathogen by inducing secretion of antimicrobial peptide by the small intestinal epithelial cells. Additionally, it is expected to hasten recovery from diarrhoea by reestablishing the commensal bacteria. The aim of this pilot study is to assess if addition of isoleucine to oral rehydration solution induces secretion of antimicrobial peptide, help establish normal bacterial populations in the intestine, and favourably impacts the severity and duration of diarrhoea in young children. If the results are found encouraging, a therapeutic trial with adequate sample size would be justified.
Globally, diarrhoea still accounts for 1.6 to 2.5 million deaths annually, and children in
the developing world experience an average of 3 episodes of diarrhoea each year. Despite the
decline in diarrhoeal mortality, it remains a leading cause of childhood morbidity and
deaths [1]. Prevention of dehydration using appropriate home-made fluids or ORS solution,
and correction of dehydration using ORS solution or intravenous fluid as indicated followed
by maintenance of hydration using ORS solution, along with continuation of usual food
including breastfeeding are most important elements of management of acute diarrhea.
Antimicrobial therapy is recommended in the management of a few specific etiologic
diarrhoeas such as severe cholera, shigellosis, invasive intestinal amoebiasis, and
symptomatic giardiasis. The cost of therapy and more importantly the emergence of resistance
pathogens are the major concerns for antimicrobial therapy for diarrhoea as for other
bacterial infections.
ORS plays a major role in the treatment diarrhoeal diseases; however, it does neither reduce
the severity nor the duration of diarrhoea, its major limitations. Efforts are continuing to
overcome these limitations by developing newer formulations and delivery mechanisms e.g.
1. Changing/replacing the substrates (e.g. addition of alanine or glycine to glucose or
replacing glucose by multodextrin and rice powder)
2. Reducing the concentration of glucose and sodium and thus osmolarity of ORS solution.
Alanine/glycine and rice powder containing ORS demonstrated some reduction in the stool
output [2-5]. However, none of the formulations developed and tested till date demonstrated
any beneficial effect on the duration of diarrhoea. Similarly, reduced osmolarity ORS has
some beneficial effect on reducing the stool output and vomiting, and reducing failure of
ORT mainly in children with non-cholera diarrhea, but did not have any effect on the
diarrhoea duration [6]. The World Health Organization (WHO) and the United Nations Children
Fund (UNICEF) have recently recommended routine use of the reduced-osmolarity ORS in the
management of diarrhoeal diseases [7]; however, there are scopes to further improve its
efficacy.
Antimicrobial peptides and innate immunity
Antimicrobial peptides represent an important component of the innate immune defenses of
organisms ranging from plants to insects to humans. They are broad-spectrum, surface-active
agents that kill microbes by forming pores in their membranes. Most have broad spectrum of
activities against bacteria, viruses and fungi. In mammals, two major classes of
antimicrobial peptides have been described- defensins and cathelicidins (LL-37). The
defensins are a subclass of antimicrobial peptides, and in mammals, they are present in
neutrophil granules where they are necessary for the non-oxidative killing of phagocytised
microbes [8]. It is now well established that defensins are also produced at virtually all
epithelial surfaces of mammals, including those of the skin, airways, gut, and urogenital
tracts [9, 10]. Expression of some epithelial defensins is constitutive and contributes to a
non-inflammatory antimicrobial barrier at the epithelial surface. Other defensins are
inducible and highly expressed at sites of inflammation or infection [9, 11, 12]. Impairment
of defensin functions increases susceptibility to infection of the airway in cystic fibrosis
[13] and to enhanced Salmonella infection in the mouse intestinal tract [14]. In addition to
their direct antimicrobial activities, Beta-defensins are chemotactic for memory T cells and
dendritic cells, suggesting that they play an important role in the integration of the
innate and acquired immune responses [15].
The molecular mechanisms underlying induction of epithelial defensins remain largely
unexplored. Pattern-recognition receptors [16] likely play a critical role in this process,
as has been shown in CD-14-mediated induction of Beta-defensins by bacterial
lipopolysaccharide [17]. Whole heat-killed bacteria and fungi induce human Beta-defensins-2
in human keratinocytes, but the molecular basis of this response is not understood [11].
Inflammatory cytokines such as tumor necrosis factor Alpha (TNF) and IL-10 also induces
Beta-defensins [18, 19]. Because pharmacological induction of defensins at epithelial
barriers may have therapeutic utility, a search for novel molecules that could induce
production of epithelial defensin, assessed by using cell-based assays, have long been
underway. It has recently been observed that L-isoleucine and its analogues are highly
specific Beta-defensin inducers in epithelial cells [20]. It has also been observed that
when isoleucine is administered to animals (chicken), the gut flora shifts to the probiotic
species, it stimulates paneth cells to secrete antimicrobial peptides in human intestinal
tissue, and it causes a shift in gut flora leading to an increased numbers of Lactobacilli.
(Manuscript, Ashida T & M Zasloff et al) in treatment of patients with Crohn's disease.
The above observations suggest a potential role of L-isoleucine in the management of
infections of mucosal tissues including those in the gastrointestinal tract.
Antimicrobial peptides in Shigella infections
In 2001, researchers from ICDDRB and Karolinska Institute (BA) reported in Nature Medicine a
down regulation of LL-37 and human Beta-defensin-1 (HBD-1) in the epithelial cells in
diarrhoea caused by Shigella dysenteriae type I and other enteric bacteria [21]. This down
regulation could be reproduced in vitro by using the cell lines U937 of monocyte origin and
HT-29 of colonic epithelial origin, when infected with Shigella or plasmid DNA derived from
Shigella. The down regulation can be an important immune escape mechanism for pathogens to
avoid potent mucosal effector molecules such as antimicrobial peptides. Since antimicrobial
factors drench the mucosal surfaces, it is conceivable that pathogenic bacteria
down-regulate the front line defenses of humans as a part of their invasive process.
Therefore, a novel approach will be to block this down-regulation or to take a therapeutic
approach to up-regulate the production of endogenous antimicrobials. Recent studies have
shown that short chain fatty acids (SCFA) can up-regulate expression of LL-37 in colonic
epithelial cells, and among them sodium butyrate was the best inducer [22, 23]. Moreover,
butyrate induces colonic cell differentiation that has been reported to be a key determinant
of LL-37 expression in human colon epithelium [22]. However, it was shown that pathways
other than those involved in cell differentiation are involved in the up-regulation of LL-37
with butyrate [23]. Butyrate is produced in the colon by fermentation of dietary fibre.
Thus, there is a link between the normal gut flora and the expression of endogenous
antibiotics. Additionally, SCFAs including butyrate has been shown to reduce clinical
symptoms, and alter microbiological and pathological features in experimental Shigella
infections in rabbit models [24]. Thus, a relationship between the severity of Shigella
infections and mucosal levels of antimicrobial peptides is conceivable. Oral administration
of sodium butyrate to rabbits infected with Shigella showed up-regulation of CAP-18 (rabbit
homologue of LL-37) in the colonic epithelial cells with a concomitant reduction in shigella
load in stool and clinical recovery (Raqib et al, manuscript accepted). Preventing
down-regulation or enhancing antimicrobial peptide expression could provide an alternative
treatment in protecting humans and animal livestock against bacterial pathogens. These
studies may provide a basis for therapeutic manipulation of endogenous antimicrobial
peptides including LL-37 expression in vivo using dietary substances or butyrate to
strengthen the epithelial defense barrier. Therefore, we have initiated a clinical study in
ICDDRB to evaluate the efficacy of butyrate enema in the treatment of shigellosis.
Butyrate has been shown to induce antimicrobial peptides in the colon; however; it can't be
administered orally as such. Moreover, most of the acute diarrhoeal diseases are caused by
infection of the small intestine. Isoleucine, an essential amino acid, might be a reasonable
alternative for enhancing secretion of antimicrobial peptides from the paneth cells and
other defense molecules from the upper small intestine (Manuscript, Ashida T & M Zasloff et
al). This may help clear the pathogens, shift gut flora to a more "normal" commensal species
distribution, and enhance recovery from infectious diarrhoea. Therefore, we hypothesize that
use of L-isoleucine supplemented ORS solution will induce antimicrobial peptides and enhance
clinical recovery of children with acute watery diarrhoea.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment