Irritable Bowel Syndrome Clinical Trial
Official title:
Kynurenine Pathway Metabolites as Novel Translational Biological Markers of Irritable Bowel Syndrome: Relationship to Gastrointestinal Function, Cognition and Co-morbid Depression
Irritable bowel syndrome (IBS) is a common disorder affecting up to 20% of the general
population. Despite the prevalence of the disorder, it remains poorly understood. This is
reflected in a symptom based diagnostic scheme, the lack of a suitable biological marker and
inadequate treatment options. Current knowledge suggests the disorder is as a result of a
dysregulated brain-gut axis, a complex construct describing the bidirectional communication
systems underpinning normal gastrointestinal functioning.
The investigators hypothesize here that the disruption of this brain-gut axis is facilitated
by an increased degradation of tryptophan along the kynurenine pathway. This metabolic
abnormality has the potential to impact on both GI and CNS signaling through its effects on
serotonergic signaling and the impact of metabolites like kynurenic acid and quinolinic acid
on cognitive processes respectively.
Previous data from our laboratory indicated increased tryptophan degradation in IBS patients
and suggested the metabolites produced as putative biological markers of the condition. In
this study the investigators aim to reconcile cognitive impairment in IBS with GI and CNS
symptom severity and kynurenine pathway metabolites.
The investigators will establish these baseline measures in IBS compared to control
subjects. A battery of cognitive assessments will be carried out using a computerized
testing system. Standardized rating scales will be used to assess GI and CNS symptom
severity. GC-MS/MS, a recently acquired technology platform in our laboratory, will be used
to quantify plasma quinolinic acid levels.
This study is based on the hypothesis that the disruption of this brain-gut axis in
irritable bowel syndrome (IBS) is a consequence of increased degradation of tryptophan along
the kynurenine pathway. The investigators aim to fully characterize this putative metabolic
abnormality and determine its impact on both gastrointestinal (GI) and central nervous
system (CNS) signaling by examining the relationship between individual pathway metabolites,
GI symptoms and cognitive processing in IBS patients
An increased degradation of tryptophan along the kynurenine pathway has been reported in
both depression and IBS (Clarke et al 2009a; Fitzgerald et al 2008; Myint et al 2007).
Although such studies have suggested an alteration in the production of quinolinic acid as a
consequence of this disruption, actual levels of this NMDA receptor agonist remain to be
measured and are essential to the full characterization of pathway disruption. The relevance
of this strategy is confirmed by studies that have implicated peripheral quinolinic acid
measures as surrogate marker of disease activity in juvenile idiopathic inflammatory
myopathies (Rider et al 2002). Moreover it has been demonstrated that increasing plasma
levels of this neurotoxic metabolite can influence CNS processes (Yan et al 2005) and that
an increased peripheral production of kynurenine can increase central quinolinic acid
concentrations (Raison et al 2009a). A correlation between alterations in the kynurenine
pathway, GI disturbances and cognitive outcomes remains to be fully defined. In this study,
the investigators propose to obtain a complete profile of plasma kynurenine pathway
metabolites in IBS patients with and without comorbid depression. Temporal instability in
symptom profile is a hallmark of IBS and represents a considerable obstacle to biomarker
discovery (Clarke et al 2009b). The preliminary data generated here will potentially be used
as the basis for future grant applications that will propose a longitudinal study of these
putative biomarker candidates.
BACKGROUND/SIGNIFICANCE
Irritable bowel syndrome (IBS) is a functional gastrointestinal disorder accounting for up
to 20% of cases presenting at gastroenterologist clinics in the western world with an
unexplained female predominance (Ersryd et al 2007). Although the typical symptoms are
commonly experienced in the general population, the abdominal pain and disturbances in
defecatory function experienced by IBS sufferers are on a scale that positions the disorder
as one of the leading causes of work absenteeism and presenteeism in western societies.
Clearly the burden it places on the individual sufferer and society as a whole is
substantial and is further compounded by its draining of healthcare resources (Clarke et al
2009b).
Despite the widespread prevalence of the disorder is it still poorly understood and is
largely characterized by the lack of a reliable validated biological marker. This is
reflected in the reliance on symptom based diagnostic criteria in conjunction with the
exclusion of other gastrointestinal disorders (Drossman 2006). Further complications arise
in the form of the psychiatric comorbidity so frequently observed among the IBS population
(Spiller 2004). It is perhaps unsurprising then that treatment options are inadequate and
advances in our understanding of the disorder are urgently required to address the unmet
medical needs of its sufferers.
Tryptophan is an essential amino acid and its role as a precursor to many biologically
active agents ensures its importance in the consideration of a variety of disease states
including schizophrenia (Barry et al 2009; Schwarcz and Pellicciari 2002), depression (Myint
et al 2007) and inflammatory bowel disease (Forrest et al 2003). Although much of the
attention to date has focused on the production of serotonin from tryptophan, the
often-overlooked kynurenine metabolic pathway (Appendix figure 1) consumes over 95% of the
available peripheral tryptophan in mammals (Clarke et al 2009a). The first step in this
cascade involves the conversion of tryptophan to kynurenine with reports suggesting that the
majority of CNS concentrations of the metabolite are drawn from the periphery (Myint et al
2007). This is an important consideration and validates the use of plasma tryptophan
metabolites in biomarker studies. This first rate limiting step in the metabolic cascade is
catalysed by either the ubiquitous indoleamine-2,3-dioxygenase (IDO) or the largely hepatic
based tryptophan 2,3-dioxygenase (TDO). Crucially in the context of stress related disorders
like IBS and depression, the activity of both enzymes can be induced by agents which are
stress responsive-IDO by inflammatory mediators and TDO by corticosteroids (Ruddick et al
2006).
Once formed, kynurenine essentially participates in two important but alternate metabolic
scenarios-one leading to the formation of the neuroprotective kynurenic acid and the other
leading to the production of the neurotoxic quinolinic acid (Ruddick et al 2006). The
neuroprotective effects of kynurenic acid are attributed to its competitive blockade of the
NMDA receptor at the glycine co-agonist site. Conversely quinolinic acid has excititoxic
properties due to its potent activation of the NR2A and NR2B NMDA receptor subunits
(Schwarcz and Pellicciari 2002). Clearly any imbalance in the production of these bioactive
ligands could lead to profound disturbances in CNS glutamatergic signaling and thus affect
glutamate-driven behaviours such as learning and memory.
Recent progress in the study of IBS has largely been brought about by a theoretical view of
the condition as a disorder of the brain-gut axis (Ohman and Simren 2007). Within this
construct, stressful insults are now thought to be integral to the destabilization of normal
brain-gut axis signaling. Higher brain centres are involved both in the processing of
afferent GI signals and the communication of changes in an individuals emotional state to
the gastrointestinal tract (Mayer 2000a; Mayer 2000b). The emotional motor system,
consisting of the limbic system and paralimbic structures such as the medial prefrontal
cortex, amygdala and hypothalamus, is one such centre. The importance of these structures in
the maintenance of normal cognitive function implies that brain-gut axis perturbations could
manifest as cognitive impairment across a number of domains.
Other lines of evidence also support an altered neuropsychological state in IBS. An emerging
body of research points to the presence of a low grade inflammation in this disorder
(Barbara and Stanghellini 2009; Clarke et al 2009b). It has recently been reported that
baseline interleukin-6 levels, the cytokine that is most consistently reported to be
elevated in IBS (Clarke et al 2009b), is predictive of cognitive symptoms of depression at
follow up in a longitudinal study (Gimeno et al 2009). It has also been demonstrated that
patients with chronic fatigue syndrome, a disorder that has also been linked with increased
inflammatory mediators (Raison et al 2009b), have associated cognitive deficits (Thomas and
Smith 2009). Previous studies from our laboratory have highlighted the relationship between
the inflammatory profile in IBS and an increased degradation of tryptophan along the
kynurenine pathway (Clarke et al 2009a; Fitzgerald et al 2008). Moreover, cancer patients
treated by cytokine immunotherapy experience related and persistent cognitive alterations
(Capuron et al 2001) and the cognitive alterations accompanying infection are also present
in apyretic sick subjects (Capuron et al 1999). The increased tryptophan degradation
observed following this immunotherapy is considered to be a key mediator of the resulting
neuropsychological alterations (Capuron et al 2002; Raison et al 2009a). Cumulatively, these
studies suggest that IBS is a disorder possessing a molecular signature (increased,
inflammation and disturbed tryptophan metabolism) indicative of cognitive deficits.
However, despite the uncovering of this molecular signature in IBS, the widespread
acceptance of the brain-gut axis model and the high psychiatric comorbidity, a comprehensive
cognitive profiling of the IBS patient population has not been performed. The cognitive
assessments that have been reported support a cognitive phenotype in the disorder but to
date have focused on singular aspects of affective memory performance (Kilkens et al 2005;
Kilkens et al 2004) or verbal IQ deficits (Dancey et al 2009). Moreover, there has been, to
our knowledge no study correlating cognitive function with mechanistically-oriented
biomarkers.
Before the benefits of such a correlation can be accrued however, a more complete assessment
of cognitive dysfunction in IBS is urgently required. The Cambridge Neuropsychological Test
Automated Battery (CANTAB) is a computerized cognitive assessment program that covers within
its remit a broad section of cognitive domains (Fray and Robbins 1996). The battery has been
validated in the assessment of cognitive dysfunction across a wide range of disease states
including psychiatric disorders such as anxiety (Kaplan et al 2006) and both unipolar and
bipolar mood disorders (Elliott et al 1996; Sweeney et al 2000). Insights gained from
neuroimaging studies in IBS which highlight the higher brain centres functioning abnormally
in the syndrome (Mayer et al., 2008) can be used to inform the initial choice of tests to be
applied to IBS subjects. Investigations in other disorders that are reported to have an
inflammatory component such as chronic fatigue disorder where assessments of free recall,
reaction time and vigilance in conjunction with the Stroop colour-word interference task to
measure distraction from irrelevant stimuli have yielded interesting results (Thomas and
Smith 2009). The specific executive function assessments which can be applied include the
Stocking of Cambridge Task (SOC) which assesses a subject's ability to rearrange a set of
balls in a specified minimum number of moves and minimum time and the
intradimensional/extradimensional (ID/ED) attentional set shifting task (adapted from the
Wisconcin Card Sorting Test (WCST)) used to assess a subjects ability to maintain attention.
CANTAB visual memory tasks such as the spatial recognition memory task (SRM) and the paired
associates learning task (PAL) can be used to assess deficits in memory (Michopoulos et al
2008). Taken together, these tests are sensitive to dysfunction across a number of different
brain regions (Sweeney et al 2000). Recently the cognitive assessments available in the
CANTAB battery have been used in conjunction with measures of clinical insight to assess the
association between poor insight and cognitive impairment in schizophrenia (Donohoe et al
2009). This may also be relevant to IBS where an increased awareness of and concern about
bodily sensations and GI functioning is well established (Posserud et al 2009). It will also
be important to rule out alternative explanations for any alterations that are observed
included task irrelevant thoughts related to the disease. Few attempts have been made to
link such findings to GI symptoms and putative biological marker candidates.
;
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