Sepsis Clinical Trial
Official title:
Modulation of Gut Microbiota in Early Sepsis: A Pilot Study
Background Sepsis is a common disease leading to high morbidity and mortality. Gut microbiota
and/or gut permeability may play a crucial role in the development of organ dysfunction.
Hypothesis The ingestion of a multispecies probiotic in early sepsis is able to modulate gut
microbiota and/or gut permeability.
Sepsis is a systemic deleterious host response to infection causing major healthcare
problems. Sepsis affects millions of people around the world each year, with a lethality of
25%-50%. The incidence is increasing partly because of a raise in average age and occurrence
of predisposing diseases in the population, and partly because of shifts in causative
pathogens. Effectiveness of therapy administered in the initial hours of severe sepsis
critically influences the clinical outcome of the patient.
Lacking reliable biomarkers for early stages, the diagnosis of (severe) sepsis relies on a
combination of surrogate parameters indicating end organ dysfunction.
Recently, gut wall integrity has been identified as a key feature in protecting the body
against potentially harmful compounds such as bacteria, toxins and antigens. The gut barrier
consists of the mucus barrier, antimicrobial peptides, secretory IgA, the epithelial barrier,
and the gut immune system. Gut permeability is reported to increase in sepsis and to play a
key role in the development of multi-organ dysfunction. Therefore, gut permeability markers
might have the potential to predict the risk of progression from sepsis to severe sepsis. The
mechanisms leading to increased gut permeability are not completely clear, yet. Direct and
indirect interactions of pathogens, hormonal imbalances, beta-adrenergic activity,
hyperglycemia and cytokine activation as well as individual predisposition have been
proposed. It seems that increased gut permeability is the common final pathway of a multitude
of influencing factors.
Furthermore, the importance of gut microbiota composition has recently been recognized in
several diseases; however, not much is known about the role of the microbiome in sepsis to
date. Available data suggest, that disturbances in microbiome homeostasis are present in
sepsis, but it is yet unknown if these changes are cause or consequence of sepsis. Changes in
gut barrier and/or gut microbiota can lead to an increase in microbial products in
circulation, contributing to (inadequate) activation and later "paralysis" of immune cells.
It is not yet known if the gut microbiome of a patient in early stages of sepsis differs from
the healthy microbiome or from the microbiome of a patient in late stages of sepsis. Also,
the possibility to modulate the gut microbiome in early sepsis has not been studied yet.
A typical strategy to modulate the gut microbiome is the use of probiotic bacteria. In
sepsis, the use of probiotics is well established for specific indications, such as
necrotising enterocolitis in neonates, however, studies in adults are scarce. Therefore the
aim of this study is to investigate if the ingestion of a multispecies probiotic in early
sepsis is able to modulate gut microbiota and/or gut permeability and observe the clinical
outcome of treated patients.
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