Crohn's Disease Clinical Trial
Official title:
A Prospective, Placebo Controlled, Double-Blind, Cross-over Study on the Effects of a Probiotic Preparation (VSL#3) on Metabolic Profile, Intestinal Permeability, Microbiota, Cytokines and Chemokines Expression and Other Inflammatory Markers in Pediatric Patients With Crohn's Disease
Background VSL#3 has been reported as an effective adjuvant therapy both in inducing and
maintaining remission in pediatric patients affected by Ulcerative Colitis. In addition, it
has been shown that VSL#3 is able to modulates barrier function, intestinal permeability,
and innate host functions, which if altered, could have a profound impact on the state of
colitis. However it is still unclear how VSL#3-induced changes in microbial composition
affect the status of intestinal inflammation and no study have investigated the efficacy of
VSL#3 in the maintenance of remission in pediatric patients with Crohn's disease (CD).
Objectives The purpose of this study will be to evaluate the effect of a probiotic
formulation, VSL#3, versus placebo, on metabolic profile, intestinal permeability,
microbiota, cytokines and chemokines expression in pediatric patients with CD in remission
of disease. In addition, the efficacy of VSL#3 on the maintenance of remission will be
assessed and the safety and the tolerability of the probiotic formula will be evaluated.
Methods This investigation will be a prospective, multicenter, randomized, double-blind,
placebo-controlled, cross-over trial. The study will include 50 children affected by CD in
remission of disease, as defined by a PCDAI < 10, under treatment with Azathioprine
associated or not to 5-ASA and will be articulated in 6 months as follows. All children will
be randomised to a treatment group receiving for 2 months either 1-2 packet containing 900
billion bacteria/day of VSL#3 according to their weight, and a group receiving the placebo
drug. Assignment to therapy or placebo will be determined according to a computer-generated
randomization scheme. At the completion of the 8 weeks, a "wash-out" period of 6 weeks will
be done, when no preparation will be administered. Then each patient will be switched to the
other group and followed likewise for further 8 weeks. All patients will continue regular
medications throughout the study period. A group of 10 volunteer healthy children,
comparable in age and sex, will be used as reference group for the analysis of metabolic
profile. Patients will be assessed clinically at baseline and every 8 weeks until the
completion of the study, at 24 weeks or at the time of relapse. At every visit data will be
collected including patient questionnaires regarding disease activity (stool frequency,
stool consistency, hematochezia, abdominal pain, extraintestinal manifestations of disease,
and overall patient functioning). Additional information collected at the first visit
included demographic data, family history, and symptom onset. Physical examination will be
performed at each visit by a paediatrician and included an abdominal examination and
examination for extraintestinal manifestations of CD. Routine blood tests for CD,
cellobiose/mannitol small intestinal permeability study, stool cultures, stool calprotectin,
will be performed at every visit and/or at the time of relapse. Urine will be collected for
the analysis of metabolic profile with mono and bi-dimensional high-resolution 1H NMR
spectroscopy. PCDAI and a physician's global assessment will be used to measure disease
activity. At baseline and at 24 weeks the patients will undergo ileocolonoscopy to evaluate
and endoscopic and histological activity of disease. Evaluation of microbiota on biopsies
and stool samples will be performed at the time of ileocolonoscopies using Fluorescence In
Situ Hybridization. Colon biopsies cultures will be performed in order to evaluate cytokines
and chemokines patterns by multiplex assay. Additional data will be collected during the
study regarding the safety and tolerability of therapy with VSL #3. Statistical analysis
will be performed using SPSS version 15 (SPSS Inc, Chicago, Illinois, USA). Variables will
be screened for their distribution and appropriate parametric or non parametric tests will
be adopted as required. Cross-tabulations will be evaluated by using the Fisher test and
χ2test. Statistical significance will be predetermined as P < 0.05.
Expected results The investigators expect to find profound alterations in metabolic
profiles, intestinal permeability, microbiota, cytokines and chemokine patterns of patients
affected by CD. The administration of VSL#3 is expected to ameliorate all these alterations
eventually identified. From a clinical point of view the effects of VSL#3 could be
translated in prolonged clinical remission maintenance, offering a new therapeutic tool in
the treatment of CD.
Inflammatory Bowel Disease (IBD) in childhood are chronic relapsing and remitting
inflammatory condition that have a significant impact on growth and development.
IBD involves a shift from a regulated intestinal immune response to one that is driven by
unrestrained immune cell activation and pro-inflammatory cytokine production. (1) The cause
of this increase in immune stimulation is of great interest and several studies indicate a
role for commensal bacteria in the progression of disease. (2) A recent study compared the
microbiota of patients with IBD with that of non-IBD controls and revealed a significant
difference in their composition. The microbiota of IBD patients showed abnormal microbial
composition characterized by depletion of Firmicutes and Bacteroides, which are represented
in non-IBD controls. (3)
Enhanced NF-κB activity is involved in the pathology of both forms of IBD. Crohn disease
(CD) and ulcerative colitis (UC). The mechanism of proteasome-mediated NF-κB activation in
CD and UC has been studied. Visekruna et al demonstrated that the subunit composition and
the proteolytic function of proteasomes differ between UC and CD. High expression of the
immunoproteasome subunits β1i and β2i is characteristic of the inflamed mucosa of CD (4). In
line with this, they found enhanced processing of NF-κB precursor p105 and degradation of
inhibitor of NF-κB, IκBα, by immunoproteasomes isolated from the mucosa of CD patients. In
comparison with healthy controls and CD patients, UC patients exhibited an intermediate
phenotype regarding the proteasome-mediated processing/degradation of NF-κB components (4)
.Finally, increased expression of the NF-κB family member c-Rel in the inflamed mucosa of CD
patients suggests that p50/c-Rel is important for IFN-γ-mediated induction of
immunoproteasomes via IL-12-driven Th1 responses. These findings suggest that distinct
proteasome subunits influence the intensity of NF-κB-mediated inflammation in IBD patients
(4).
In the study of Pagnini C et al., the authors report that the probiotic mixture VSL#3
prevents the onset of intestinal inflammation in the SAMP mouse model of CD-ileitis. These
effects were associated with a local effect on the intestinal epithelium (i.e., stimulation
of TNF-α production and NF-κB activation in epithelial cells, coupled with restitution of
normal intestinal epithelial barrier function).
Analysis of bacterial DNA in the stool and ileal mucosa of treated mice demonstrated a
significant increase of probiotic strains, suggesting that effective bacterial colonization
is required for the beneficial effects of probiotic treatment. This study support the
hypothesis that probiotics promote gut health through a mechanism involving stimulation of
epithelial innate responses (i.e., stimulation of TNF-α expression), rather than suppression
of inflammation. (5)
Many individual or combinations of bacterial species have been shows to ameliorate the
symptoms of IBD and to reduce intestinal inflammation in animal studies. Treatment of mice
with colitis with the probiotic formulation VSL#3 increased the production of IL-10 and the
percentage of TGFβ-expressing T-cells. Transfer of lamina propria mononuclear cells from
VSL#3-treated mice prevented colitis in recipient mice, indicating that the VSL#3 can
initiate the generation of a protective population of cells. (6)
The recent identification of symbiotic bacteria with potent anti-inflammatory properties,
and their correlative absence during disease, suggests that certain aspects of human health
may depend on the status of microbiota. (7)
In addition, the Lipopolysaccharide (LPS) is a major component of the bacterial outer
membrane that is largely responsible for mediating septic shock. Normally the body does not
react to the high concentration of LPS that is present in the intestinal lumen. Intestinal
alkaline phosphatase (IAP) seems to detoxify LPS by hydrolyzing it and maintaining
intestinal homeostasis with the commensal flora. (8)
Probiotics modulate the composition of the gut microbiota. Global microarray and
bioinformatica analysis revealed augmentation of immune response, phagocytic, and
inflammatory pathways dominated by elevation of Th1 transcription factors in IL10-KO mice.
IL10-KO mice orally administered with the probiotic VSL#3 exhibited a site-specific
downregulation of these inflammatory pathways including TLR signalling and related effector
pathways such as T-cell, B-cell receptor signaling. More important, VSL#3 triggered an
up-regulation in PPAR signaling, lipid, nitrogen, amino acid, and xenobiotic metabolism (9).
Actually it is unclear how VSL#3-induced changes in microbial composition affect the status
of intestinal inflammation. It is possible that VSL#3 promotes the presence of protective
microorganisms, likely constituents of the probiotic itself that directly influence host
innate responses. It has been reported that VSL#3 modulates barrier function, intestinal
permeability, and innate host functions, which if altered, could have a profound impact on
the state of colitis. VSL#3 has been shown to enhance barrier function through decreased
epithelial permeability in IL10_/_ mice, correlating with a reduction in intestinal
inflammation. Another recent study demonstrated that VSL#3 prevents the development of
ileitis in SAMP1/YitFc mice by enhancing epithelial barrier function and activating innate
signaling leading to NF-jB activation. These effects appear to be mediated by VSL#3 secreted
products. This is consistent with reports showing that probiotic-derived factors are capable
of modulating host responses and experimental colitis. Additionally, structural components
present in probiotic bacteria could profoundly impact immune response and favor the
production of immunosuppressive molecules such as IL-10 (10).
Purpose:
The purpose of this study is to evaluate the effect of a probiotic formulation, VSL#3,
versus placebo, on metabolic profile, intestinal permeability, microbiota, cytokines and
chemokines expression and other inflammatory markers in pediatric patients with Crohn's
Disease (CD) in remission (11).
Secondary objectives are:
- To determine the effect on Pediatric Crohn Disease Activity Index (PCDAI)
- to determine the time till flare of CD pediatric patients on VSL#3 compared to placebo
- to assess whether concurrent therapy with VSL#3 reduces the severity of a flare if it
occurs
- to assess the safety and tolerability of therapy with VSL #3 at high dosage in
pediatric patients with CD
Study design
This investigation will be a randomized, double-blind, placebo-controlled, cross-over trial.
The study will include 30 children with CD and will be articulated in 6 months as follows. A
group of 10 volunteer healthy children, comparable in age and sex, will be used as reference
group for the analysis of metabolic profile..
These children will be randomised to a treatment group receiving for 2 months either 1-2
packet containing 900 billion bacteria/day of VSL#3 according to their weight, and a group
receiving the placebo drug. Assignment to therapy or placebo will be determined according to
a computer-generated randomization scheme. The medications will be dispensed by the
investigator at each visit; compliance will be assessed by counting returned bags and
questioning the patients. Excellent compliance will be defined as no violation of the
protocol with respect to the intake of the study medication. At the completion of the 8
weeks, a "wash-out" period of 6 weeks will be done, when no preparation will be
administered. Then each patient will be switched to the other group and followed likewise
for further 8 weeks.
All patients will continue regular medications throughout the study period (azathioprine
associated or not to 5-ASA).
Patients will be assessed clinically at baseline and every 8 weeks until the completion of
the study, at 24 weeks or at the time of relapse. At every visit data will be collected
including patient questionnaires regarding disease activity (stool frequency, stool
consistency, hematochezia, abdominal pain, extraintestinal manifestations of disease, and
overall patient functioning). Additional information collected at the first visit included
demographic data, family history, and symptom onset. Physical examination will be performed
at each visit by a paediatrician and included an abdominal examination and examination for
extraintestinal manifestations of CD. Routine blood tests for CD, cellobiose/mannitol small
intestinal permeability study, stool cultures, stool calprotectin, will be performed at
every visit and/or at the time of relapse. Urine will be collected for the analysis of
metabolic profile with mono and bi-dimensional high resolution 1H NMR spectroscopy. In 10
healthy volunteer children and patients, bile acid, isoleucine, leucine, valine,
2-oxo-3methyl-valeric acid, 2-oxo-isovaleric acid, 2-methyl-3-hydroxybutyric acid,
3-hydroxybutyrate, 3-hydroxybutyrate, 3-hydroxyisovaleric acid, threonine, lactate,
3-hydroximethylglutamic acid, alanine, N-acetyl asparagine + aspartyl glutamate + glutamil
acid, acetic acid, carnitine, acetone, acetoacetate, 2-hydroxyglutarate, pyruvate, glutaric
acid, N-Acetylglutamic acid, succinate, 3-hydroxy-3-methylglucaric acid, dimethylamine,
sarcosine, N-acetyl-aspartyl-glutamate, dimethylglycine, citric acid, creatine, creatinine,
choline, betaine, malonic acid, trimethylamineoxide, sarcosine, glycine, 1-methylhistidine,
3-methylhistidine, benzoilglycine (hippuric acid) , N-methyl betaine (trigonellina),
arabinosio, uracil, guanosine, tyrosine, phenylalanine, xanthine, hypoxanthine,
3-methylhistidine will be evaluated. In addition, in children with CD, many other
metabolites signals will be expected, resulting from drugs or other compounds taken as such
or processed by the body's metabolism or intestinal microbial flora. the metabolomic
analysis will allow the evaluation of the following organ specific and systemic processes
based on low molecular weight compounds providing a profile of the metabolic system of the
subjects: intermediary metabolism of sugar, mitochondrial citric acid cycle, amino acids
metabolism, oxidative metabolism of fatty acid, break down and turnover of proteins,
metabolism of purine and pyrimidine, pathway of trans-methylation and trans-sulphide,
metabolism of intestinal bacteria; etc.
PCDAI and a physician's global assessment were used to measure disease activity. No disease
activity equals a score of 0-10, mild disease equals 11-30, moderate/severe disease equals
31 or more. (10)
At baseline and at 24 weeks the patients will undergo ileocolonoscopy to evaluate and
endoscopic and histological activity of disease. Evaluation of microbiota on biopsies and
stool samples will be performed at the time of ileocolonoscopies using FISH (Fluorescence In
Situ Hybridization). A colon culture will be performed in order to evaluate all cytokines
and chemokines by multiplex assay. In addition, the RNA analysis from biopsies will be
performed for the study of proteasome subunits or other inflammatory markers
Additional data will be collected during the study regarding the safety and tolerability of
therapy with VSL #3.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment
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