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A multi-mineral intervention to improve disease-related and mechanistic biomarkers in ulcerative colitis patients: Results from a randomized trial
by
Aslam, Muhammad N
, Moraga, Gillian
, Varani, James
, Appelman, Henry D
, Sen, Ananda
, Jepsen, Karl J
, Turgeon, Danielle Kim
, McNeely, Molly M
, Allen, Ron
, Harber, Isabelle
, Stidham, Ryan
, McClintock, Shannon
, Jencks, Kara J
in
Adjuvants, Pharmaceutic
/ Adult
/ Alkaline phosphatase
/ Alkaline Phosphatase - blood
/ Analysis
/ Anti-inflammatory agents
/ Biological markers
/ Biology and Life Sciences
/ Biomarkers
/ Biomarkers - blood
/ Biomarkers - metabolism
/ Biopsy
/ Bone mineral content
/ Bone mineral density
/ Bone turnover
/ C-reactive protein
/ C-Reactive Protein - metabolism
/ Care and treatment
/ Cell surface
/ Chronic illnesses
/ Colitis, Ulcerative - blood
/ Colitis, Ulcerative - drug therapy
/ Colitis, Ulcerative - metabolism
/ Colitis, Ulcerative - pathology
/ Colon
/ Diagnosis
/ Dietary minerals
/ Dietary supplements
/ Dual energy X-ray absorptiometry
/ Enrollments
/ FDA approval
/ Feces
/ Feces - chemistry
/ Female
/ Health aspects
/ Human subjects
/ Humans
/ Inflammation
/ Inflammatory bowel disease
/ Inflammatory bowel diseases
/ Intestine
/ Laboratories
/ Leukocyte L1 Antigen Complex - metabolism
/ Male
/ Mass spectrometry
/ Mass spectroscopy
/ Medicine and Health Sciences
/ Middle Aged
/ Minerals - therapeutic use
/ Osteocalcin
/ Osteocalcin - blood
/ Placebos
/ Protein transport
/ Proteins
/ Proteomics
/ Remission
/ Remission (Medicine)
/ Research and Analysis Methods
/ Risk factors
/ Statistical analysis
/ Testing
/ Ulcerative colitis
2025
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A multi-mineral intervention to improve disease-related and mechanistic biomarkers in ulcerative colitis patients: Results from a randomized trial
by
Aslam, Muhammad N
, Moraga, Gillian
, Varani, James
, Appelman, Henry D
, Sen, Ananda
, Jepsen, Karl J
, Turgeon, Danielle Kim
, McNeely, Molly M
, Allen, Ron
, Harber, Isabelle
, Stidham, Ryan
, McClintock, Shannon
, Jencks, Kara J
in
Adjuvants, Pharmaceutic
/ Adult
/ Alkaline phosphatase
/ Alkaline Phosphatase - blood
/ Analysis
/ Anti-inflammatory agents
/ Biological markers
/ Biology and Life Sciences
/ Biomarkers
/ Biomarkers - blood
/ Biomarkers - metabolism
/ Biopsy
/ Bone mineral content
/ Bone mineral density
/ Bone turnover
/ C-reactive protein
/ C-Reactive Protein - metabolism
/ Care and treatment
/ Cell surface
/ Chronic illnesses
/ Colitis, Ulcerative - blood
/ Colitis, Ulcerative - drug therapy
/ Colitis, Ulcerative - metabolism
/ Colitis, Ulcerative - pathology
/ Colon
/ Diagnosis
/ Dietary minerals
/ Dietary supplements
/ Dual energy X-ray absorptiometry
/ Enrollments
/ FDA approval
/ Feces
/ Feces - chemistry
/ Female
/ Health aspects
/ Human subjects
/ Humans
/ Inflammation
/ Inflammatory bowel disease
/ Inflammatory bowel diseases
/ Intestine
/ Laboratories
/ Leukocyte L1 Antigen Complex - metabolism
/ Male
/ Mass spectrometry
/ Mass spectroscopy
/ Medicine and Health Sciences
/ Middle Aged
/ Minerals - therapeutic use
/ Osteocalcin
/ Osteocalcin - blood
/ Placebos
/ Protein transport
/ Proteins
/ Proteomics
/ Remission
/ Remission (Medicine)
/ Research and Analysis Methods
/ Risk factors
/ Statistical analysis
/ Testing
/ Ulcerative colitis
2025
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A multi-mineral intervention to improve disease-related and mechanistic biomarkers in ulcerative colitis patients: Results from a randomized trial
by
Aslam, Muhammad N
, Moraga, Gillian
, Varani, James
, Appelman, Henry D
, Sen, Ananda
, Jepsen, Karl J
, Turgeon, Danielle Kim
, McNeely, Molly M
, Allen, Ron
, Harber, Isabelle
, Stidham, Ryan
, McClintock, Shannon
, Jencks, Kara J
in
Adjuvants, Pharmaceutic
/ Adult
/ Alkaline phosphatase
/ Alkaline Phosphatase - blood
/ Analysis
/ Anti-inflammatory agents
/ Biological markers
/ Biology and Life Sciences
/ Biomarkers
/ Biomarkers - blood
/ Biomarkers - metabolism
/ Biopsy
/ Bone mineral content
/ Bone mineral density
/ Bone turnover
/ C-reactive protein
/ C-Reactive Protein - metabolism
/ Care and treatment
/ Cell surface
/ Chronic illnesses
/ Colitis, Ulcerative - blood
/ Colitis, Ulcerative - drug therapy
/ Colitis, Ulcerative - metabolism
/ Colitis, Ulcerative - pathology
/ Colon
/ Diagnosis
/ Dietary minerals
/ Dietary supplements
/ Dual energy X-ray absorptiometry
/ Enrollments
/ FDA approval
/ Feces
/ Feces - chemistry
/ Female
/ Health aspects
/ Human subjects
/ Humans
/ Inflammation
/ Inflammatory bowel disease
/ Inflammatory bowel diseases
/ Intestine
/ Laboratories
/ Leukocyte L1 Antigen Complex - metabolism
/ Male
/ Mass spectrometry
/ Mass spectroscopy
/ Medicine and Health Sciences
/ Middle Aged
/ Minerals - therapeutic use
/ Osteocalcin
/ Osteocalcin - blood
/ Placebos
/ Protein transport
/ Proteins
/ Proteomics
/ Remission
/ Remission (Medicine)
/ Research and Analysis Methods
/ Risk factors
/ Statistical analysis
/ Testing
/ Ulcerative colitis
2025
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A multi-mineral intervention to improve disease-related and mechanistic biomarkers in ulcerative colitis patients: Results from a randomized trial
Journal Article
A multi-mineral intervention to improve disease-related and mechanistic biomarkers in ulcerative colitis patients: Results from a randomized trial
2025
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Overview
The long-term goal of our ongoing studies is to determine if, and to what extent, a multi-mineral product (Aquamin) could benefit individuals with ulcerative colitis (UC). As a step toward achieving that goal, we carried out a pilot 180-day biomarker trial (clinicaltrials.gov ID: NCT03869905) in patients with UC in remission or with mild disease.
A total of 28 subjects participated in the study. Each subject was randomly assigned to receive either Aquamin for 180 days or placebo for 90 days. At Day-90, placebo subjects crossed over to Aquamin for the final 90 days. At Day-0, -90 and -180, serum samples were analyzed for C-reactive protein (CRP), alkaline phosphatase (ALP), intestine-specific ALP (ALPI), and for biomarkers of bone turnover (osteocalcin, TRAP5b and bone-specific ALP [BALP]). Stool specimens were assessed for fecal calprotectin (fCAL) and colon biopsies were examined histologically by Geboes scoring at the same time points. Each subject underwent DEXA scanning (at Day-0 and Day-180 only). In addition, mass spectrometry-based proteomic assessment was performed using colon biopsies obtained at each time point.
Subjects who received Aquamin for the complete 180-day period (a total of 12) demonstrated improvements in all biomarkers (CRP, fCAL, ALP, ALPI, and Geboes scoring); this was not observed in the placebo group (16 subjects). When cumulative pre-post differences were compared between the Aquamin and placebo groups, Aquamin treatment significantly decreased these differences (a 24% decrease as compared to a 38% increase with placebo, p = 0.0284). Subjects who received Aquamin for 90-days showed intermediary responses. Subjects receiving Aquamin for 180 days also demonstrated increases in bone mineral density (BMD) and bone mineral content (BMC), resulting in a statistically significant increase (7.3%, p = 0.0324) in the hip strength index over the treatment period. This was accompanied by increases in osteocalcin and TRAP5b and a decrease in BALP. The proteomic screen demonstrated upregulation of multiple gut barrier proteins, cell surface transporter molecules and certain proteins with anti-inflammatory potential in response to Aquamin. Aquamin treatment also led to downregulation of several proteins associated with the pro-inflammatory state.
The results presented here suggest that the use of a multi-mineral intervention improves disease-related biomarkers in patients with UC. These studies suggest the potential value of the mineral intervention as a low-cost, non-toxic adjuvant therapy for mild UC or for individuals with UC in remission.
Publisher
Public Library of Science,PLOS,Public Library of Science (PLoS)
Subject
/ Adult
/ Alkaline Phosphatase - blood
/ Analysis
/ Biopsy
/ C-Reactive Protein - metabolism
/ Colitis, Ulcerative - drug therapy
/ Colitis, Ulcerative - metabolism
/ Colitis, Ulcerative - pathology
/ Colon
/ Dual energy X-ray absorptiometry
/ Feces
/ Female
/ Humans
/ Leukocyte L1 Antigen Complex - metabolism
/ Male
/ Medicine and Health Sciences
/ Placebos
/ Proteins
/ Research and Analysis Methods
/ Testing
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