NOTE: Please ensure that a correct amount of stool sample is provided in EACH vial. If this cannot be the case, please click on the <Practical> tab for further information.
The GI360 Profile is an innovative, comprehensive and clinically-applicable stool profile, utilizing multiplex PCR molecular technology coupled with growth-based culture and ID by MALDI-TOF, sensitive biochemical assays and microscopy to detect and assess the status of pathogens, viruses, parasites and bacteria that may be contributing to acute or chronic gastrointestinal symptoms and disease.
Microbiome Abundance and Diversity The GI360 Profile is a gut microbiota DNA analysis tool that identifies and characterizes the abundance and diversity of more than 45 targeted analytes that peer-reviewed research has shown to contribute to dysbiosis and other chronic disease states.
The GI360 can identify the presence of pathogenic viruses, bacteria, and parasites using multiplexed, real-time PCR. Viruses are the primary cause of acute diarrhea, and the least commonly tested. The identification of pathogenic bacteria, viruses and parasites improves treatment strategies and patient outcomes.
The Dysbiosis Index (DI) is a calculation with scores from 1 to 5 based on the overall bacterial abundance and profile within the patient's sample as compared to a reference population. Values above 2 indicate a microbiota profile that differs from the defined normobiotic reference population (i.e., dysbiosis). The higher the DI above 2, the more the sample is considered to deviate from normobiosis.
x1 indicates a one day collection. Available also as 2 and 3 day collection.
Indications
• Gastrointestinal Symptoms
• Inflammation
• Joint Pain
• Mucosal Barrier Dysfunction
• Autoimmune Disease
• Food Sensitivities
• Chronic or Acute Diarrhea
• Abdominal Pain
• IBD/IBS
• Nutritional Deficiencies
• Bloody Stool
• Fever and Vomiting
Overview
What does the GI360 cover?
ABUNDANCE & DIVERSITY AMONG 6 KEY BACTERIAL PHYLA
- Actinobacteria
- Verrucomicrobia
- Tenericutes
- Proteobacteria
- Firmicutes
- Bacteroidetes
PATHOGENIC BACTERIA with Multiplex PCR, including
- Campylobacter (C. jejuni, C. coli and C. lari)
- C. difficile Toxin A
- C. difficile Toxin B
- E. coli O157
- Enterotoxigenic E. coli LT/ST
- Shiga-like Toxin E. coli stx1
- Shiga-like Toxin E. coli stx2
- Salmonella
- Vibro cholerae
- Shigella (S. boydii, S. sonnei, S. flexneri & S. dysenteriae)
PATHOGENIC, IMBALANCED & DYSBIOTIC BACTERIA with culture
PARASITIC PATHOGENS
- Cryptosporidium
- Entamoeba histolytica
- Giardia
VIRUSES
- Adrenovirus 40/41
- Norovirus GI/GII
- Rotavirus A
YEAST
INTESTINAL DIGESTION & HEALTH MARKERS
- Elastase
- Fat Stain
- Carbohydrates
- Lactoferrin
- Lysozyme
- Calprotectin
- Secretory IgA
- Total SCFA's
- % Acetate
- % Propionate
- % Butyrate
- % Valerate
- Butyrate
- pH
- Beta-glucuronidase
- Occult Blood
PARASITES & WORMS
- Protozoa
- Cestodes - Tapeworms
- Trematodes - Flukes
- Dematodes - Round Worms
NATURAL & PRESCRIPTIVE AGENT SENSITIVITIES
OTHER MARKERS
- Red blood cells
- White blood cells
- Muscle & vegetable fibers
- Charcot-Leyden Crystals
- Pollen
- Color & consistency
- Mucus
AVAILABLE ADD-ONS
Practical
Practical (add-ons available)
Specimen requirements: STOOL
1 day collection
Also available as 2 and 3 day collection
QUANTITY: Each vial must be filled until the indicated fill line, and must not be filled to the top.
STORAGE:
Black & Orange capped vials: REFRIGERATE (DO NOT freeze)
White capped vial: FREEZE for at least 6 hours
PLEASE NOTE:
If there are any missing or improperly produced samples, the following options are available:
1. SEND A NEW (COMPLETE) SAMPLE, where the patient/practitioner will be liable for the added shipment costs.
2. REQUEST a downgraded version of the test. The downgraded report will only contain the analytes measured from each vile:
- BLACK capped vial: parasitology
- YELLOW/ORANGE capped vial: Bacteria/Yeast Culture & PCR
- WHITE capped vial: all stool chemistries (acetate, butyrate, calprotectin, elastase, fat stain, lactoferrin, lysozyme, mucus, muscle fibres, occult blood, pH, propionate, RBC, SIgA, valerate, vegetable fibres, WBC and beta-glucuronidase.
Once the downgraded version of the test has been requested based on the delivered vials, the invoice price will be adjusted to accommodate the new report. A new order will have to be submitted to receive a full report, as results cannot be transferred between past orders.
Average processing time:
21 days
Available add-ons:
Zonulin add-on for GI360
Age Considerations:
The PCR Microbiome section (only) may best be served for those ages 2 and above due to variations in the microbiome in ages 0-2. For infants and new-borns, collect from the middle of the stool, not touching the diaper as this will contaminate the sample. The stool needs to be free of urine.
Research
Research
• Aasbrenn M, Valeur J, Farup PG. Evaluation of a faecal dysbiosis test for irritable bowel syndrome in subjects with and without obesity. Scandinavian Journal of Clinical and Laboratory Investigation. 2017;78(1-2):109-113. DOI: 10.1080/00365513.2017.1419372
• Andréasson K, Alrawi Z, Persson A, Jönsson G, Marsal J. Intestinal dysbiosis is common in systemic sclerosis and associated with gastrointestinal and extraintestinal features of disease. Arthritis Research & Therapy. 2016;18(1). DOI: 10.1186/s13075-016-1182-z
• Bennet SMP, Böhn L, Störsrud S, et al. Multivariate modelling of faecal bacterial profiles of patients with IBS predicts responsiveness to a diet low in FODMAPs. Gut. 2017;67(5):872-881. DOI: 10.1136/gutjnl-2016-313128
• Casén C, Vebø HC, Sekelja M, et al. Deviations in human gut microbiota: a novel diagnostic test for determining dysbiosis in patients with IBS or IBD. Alimentary Pharmacology & Therapeutics. 2015;42(1):71-83. DOI: 10.1111/apt.13236
• Farup PG, Aasbrenn M, Valeur J. Separating “good” from “bad” faecal dysbiosis – evidence from two cross-sectional studies. BMC Obesity. 2018;5(1). DOI: 10.1186/s40608-018-0207-3
• Farup P, Valeur J. Faecal Microbial Markers and Psychobiological Disorders in Subjects with Morbid Obesity. A Cross-Sectional Study. Behavioral Sciences. 2018;8(10):89. DOI: 10.3390/bs8100089
• Magnusson MK, Strid H, Sapnara M, et al. Anti-TNF Therapy Response in Patients with Ulcerative Colitis Is Associated with Colonic Antimicrobial Peptide Expression and Microbiota Composition. Journal of Crohns and Colitis. 2016;10(8):943-952. DOI: 10.1093/ecco-jcc/jjw051
• Magnusson MK, Strid H, Isaksson S, Simrén M, Öhman L. The Mucosal Antibacterial Response Profile and Fecal Microbiota Composition Are Linked to the Disease Course in Patients with Newly Diagnosed Ulcerative Colitis. Inflammatory Bowel Diseases. 2017;23(6):956-966. DOI: 10.1097/mib.0000000000001130
• Mazzawi T, Lied GA, Sangnes DA, et al. The kinetics of gut microbial community composition in patients with irritable bowel syndrome following fecal microbiota transplantation. Plos One. 2018;13(11). DOI: 10.1371/journal.pone.0194904
• Olbjørn C, Småstuen MC, Thiis-Evensen E, et al. Fecal microbiota profiles in treatment-naïve pediatric inflammatory bowel disease – associations with disease phenotype, treatment, and outcome. Clinical and Experimental Gastroenterology. 2019;Volume 12:37-49. DOI: 10.2147/ceg.s186235
• Thorkildsen LT, Nwosu FC, Avershina E, et al. Dominant Fecal Microbiota in Newly Diagnosed Untreated Inflammatory Bowel Disease Patients. Gastroenterology Research and Practice. 2013;2013:1-13. DOI: 10.1155/2013/636785
• Valeur J, Småstuen MC, Knudsen T, Lied GA, Røseth AG. Exploring Gut Microbiota Composition as an Indicator of Clinical Response to Dietary FODMAP Restriction in Patients with Irritable Bowel Syndrome. Digestive Diseases and Sciences. 2018;63(2):429-436. DOI: 10.1007/s10620-017-4893-3
• Vebø HC, Sekelja M, Nestestog R, et al. Temporal Development of the Infant Gut Microbiota in Immunoglobulin E-Sensitized and Nonsensitized Children Determined by the GA-Map Infant Array. Clinical and Vaccine Immunology. 2011;18(8):1326-1335. DOI: 10.1128/cvi.00062-11
• Vebø HC, Karlsson MK, Avershina E, Finnby L, Rudi K. Bead-beating artefacts in the Bacteroidetes to Firmicutes ratio of the human stool metagenome. Journal of Microbiological Methods. 2016;129:78-80. DOI: 10.1016/j.mimet.2016.08.005