Metabolic Syndrome Clinical Trial
Official title:
Obesity - Inflammation - Metabolic Disease: Effect of Lactobacillus Casei Shirota
Obesity and metabolic syndrome are linked by inflammation. Gut flora seems to play an
important role in the development of inflammation and metabolic syndrome in obesity.
Modulation of gut flora by probiotics has been shown in animal studies to positively
influence inflammation and metabolic disturbances.
Lactobacillus casei Shirota is able to decrease metabolic endotoxemia by altering gut flora
composition and gut permeability which leads to an improvement in neutrophil function and
insulin resistance in obesity.
The aim of the current study is to investigate the effect of Lactobacillus casei Shirota
supplementation over 12 weeks on neutrophil function (phagocytosis, oxidative burst and TLR
expression) in patients with metabolic syndrome.
Furthermore the investigators aim to investigate the effect of Lactobacillus casei Shirota
supplementation over 12 weeks on glucose tolerance, insulin resistance, inflammation, gut
flora composition, gut permeability, and endotoxemia in metabolic syndrome
Obesity and metabolic disorders (type 2 diabetes and insulin resistance) are tightly linked
to inflammation. Obesity, a pandemic affecting 30-50% of the adult population, is mediated by
a variety of genetic and environmental factors. It is well described that cytokines cause
insulin resistance which causes hyperinsulinemia and excessive fat storage in adipose tissue
and the liver. However, the triggering factor, linking inflammation to metabolic syndrome has
not been fully elucidated yet.
Recently it has been hypothesized that the gut flora is an important factor in this vicious
cycle of obesity, metabolic disease and inflammation. Firstly, metabolic activities of the
gut microbiota facilitates the extraction of calories from ingested dietary substances and
helps to store these calories in host adipose tissue for later use. Second, the gut bacterial
flora of obese mice and humans include fewer Bacteroidetes and correspondingly more
Firmicutes than that of their lean counterparts, suggesting that differences in caloric
extraction of ingested food substances may be due to the composition of the gut microbiota.
Furthermore, bacterial lipopolysaccharide derived from the intestinal microbiota may trigger
inflammation, linking it to high-fat diet-induced metabolic syndrome. High-fat diet induces
insulin resistance and oxidative stress in mice and is associated with increased gut
permeability. high fat diet induces a low-grade endotoxemia in mice ("metabolic endotoxemia)
and infusing endotoxin causes weight gain and insulin resistance. This has also been shown in
humans, where patients with fatty liver had a susceptibility to higher gut permeability,
possibly causing increased endotoxin levels.
Endotoxin and Lipopolysaccharide-binding protein (LBP) is elevated in obese patients,
patients with type 2 diabetes and patients with liver steatosis. Endotoxin causes a
significant increase in proinflammatory cytokine production in adipocytes via a TLR mediated
pathway, contribution to the proinflammatory state in obesity. Endotoxin levels correlate
with adiponectin and insulin suggesting a pathophysiological link between obesity,
inflammation and metabolic disease.
As described above, endotoxin is related to increased inflammation and oxidative stress,
causing insulin resistance. Adipocytes have been shown to play a dynamic role in regulation
of inflammation by producing cytokines via a Toll-like receptor (TLR)/Nuclear Factor kappa B
(NFkB) mediated pathway.But not only adipocytes are in a proinflammatory state - also
circulating mononuclear cells have been described to be activated. Clinical evidence suggests
immune dysfunction in obesity, since obese patients are more prone to infections after
surgery, higher incidence of lower respiratory infection which is also underlined by
impairment of cell-mediated immune responses in vivo and in vitro and a reduced intracellular
killing by neutrophils.
A similar situation has been recently described in alcoholic cirrhosis and alcoholic
hepatitis, which is also a proinflammatory condition with impaired innate immunity, leading
to infection. Endotoxin has been described as a key mediator and inadequate activation of
neutrophils leading to high oxidative burst and energy depletion of the cells with
consecutive impaired phagocytic capacity has been described.
The most effective therapy of obesity - weight loss - leads to significant improvement of
mononuclear cell activation. However, there is no data available on the effect of weight loss
on gut flora, gut permeability and endotoxin.
Since weight loss is usually very hard to achieve, other therapeutic strategies have been
tested. Since gut flora seems to be crucial in the development of the vicious cycle of
obesity, inflammation and metabolic disease, several studies tried to modify the composition
of gut microbiota. In mice treatment with antibiotics improved glucose tolerance by altering
expression of genes involved in inflammation and metabolism. A similar result was found in
mice treated with a probiotic that increases the number of Bifidobacterium spp., which leads
to improved glucose tolerance, insulin secretion and a decrease in inflammatory tone. Finally
treatment of mice with a probiotic decreased hepatic insulin resistance via a C-Jun
N-terminal Kinase (JNK) and NFkB pathway, supporting the concept that intestinal bacteria
induce endogenous signals that play a pathogenic role in hepatic insulin resistance.
Among the vast amount of bacteria described to alter gut flora and exert positive effects on
the host, we have chosen to study Lactobacillus casei Shirota several reasons: Firstly this
commercially available preparation delivers a high bacterial number in a relatively small
volume and is available as a palatable milk drink. Furthermore Lactobacillus casei Shirota
has been proven to survive the passage through the stomach and is present in the lower
intestinal tract. It has also been shown that this bacterial strain can increases the amount
of Lactobacilli and decreases the number of gram-negative organisms in the bacterial flora.
This bacterial strain has been shown to be effective in modulating natural killer cell
function and neutrophil function.
We hypothesize that Lactobacillus casei Shirota is able to decrease metabolic endotoxemia by
altering gut flora composition and gut permeability which leads to an improvement in
neutrophil function and insulin resistance in obesity
Specific Aims:
1. To investigate the effect of Lactobacillus casei Shirota supplementation over 12 weeks
on neutrophil function (phagocytosis, oxidative burst and TLR expression) in patients
with metabolic syndrome.
2. To investigate the effect of Lactobacillus casei Shirota supplementation over 12 weeks
on glucose tolerance, insulin resistance, inflammation, gut flora composition, gut
permeability, and endotoxemia in metabolic syndrome
Plan of investigations:
Patients:
30 Patients with metabolic syndrome and increased gut permeability will be randomized to
either receive food supplementation with a milk drink containing Lactobacillus casei Shirota
(3 bottles a day, 65 ml each, containing Lactobacillus casei Shirota at a concentration of
10^8 colony forming units/ml) for twelve weeks or standard medical therapy.
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