Summary of Study ST000960

This data is available at the NIH Common Fund's National Metabolomics Data Repository (NMDR) website, the Metabolomics Workbench, https://www.metabolomicsworkbench.org, where it has been assigned Project ID PR000659. The data can be accessed directly via it's Project DOI: 10.21228/M8GX0J This work is supported by NIH grant, U2C- DK119886.

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Study ID	ST000960
Study Title	The Influence of Sugar, Artificial Sweeteners, and the Microbiome on Rodent Triglyceride Composition (part III)
Study Summary	Targeted triglyceride concentration panel of rodents treated with diets rich in commonly used artifically sweeteners will be assessed in this study. We hypothesized that a specific subset of plasma metabolites are generated as a result from a diet rich in commonly used artificial sweeteners and their subsequent processing by the gut microbiome, which could ultimately lead to impaired glycemic control and negative physiological health outcomes. To test this hypothesis we administered normal, high glucose, fructose, aspartame, and acesulfame potassium diets to rats for 3 weeks, followed by a plasma collection through cardiac puncture and metabolic analysis. We also treated the gut microbiota with in rats with the same diets plus bacitracin/streptomycin to observe how alterations of the microbiome influence the plasma metabolic profile in these animals. The resulting data will give us insights into the influence of high sugar and artificial sweetener diets on homeostatic metabolic processes and dive into the symbiotic relationship of the gut microbiome with this process.
Institute	Mayo Clinic
Last Name	Hoffmann
First Name	Brian
Address	8701 Watertown Plank Road Milwaukee, WI 53226
Email	bhoffmann@mcw.edu
Phone	414-955-8671
Submit Date	2018-04-14
Analysis Type Detail	LC-MS
Release Date	2020-04-15
Release Version	1

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Project:

Project ID:	PR000659
Project DOI:	doi: 10.21228/M8GX0J
Project Title:	Mayo Pilot and Feasibility: The Influence of Sugar, Artificial Sweeteners, and the Microbiome on Metabolism
Project Summary:	As diabetes becomes a growing heath concern, afflicting nearly 25.8 million people in the United States and nearly 220 million people worldwide, there has been an increased awareness of environmental factors like diet that are contributing to the disease. In diabetic patients, a major causal factor contributing to progression of the disease is hyperglycemia, although the underlying mechanisms by which hyperglycemia impairs homeostatic processes are not well understood. While we know that early intensive glycemic control reduces the risk of cardiovascular complications in humans and rodent models, there is a large gap in studies of the etiology of hyperglycemia-induced alterations in the disease. To combat high sugar diets that could contribute to diabetes and subsequent hyperglycemia, non-caloric artificial sweeteners have become one of the most utilized food additives worldwide due to their consideration as a low caloric substitute. However, supporting scientific data as to the safety of these non-caloric artificial sweeteners is limited and controversial. The negative implications of consuming a high sugar diet on overall health have long been linked to diabetes, obesity, and resulting systemic health problems; however, it was not until recently that the negative impact of consuming artificial sweeteners in the place of sugar had been increasingly recognized. Recent evidence also suggests that a diet rich in artificial sweeteners can induce glucose intolerance through the alteration of the gut microbiome. We hypothesize that a specific subset of plasma metabolites are generated as a result from a diet rich in commonly used artificial sweeteners and their subsequent processing by the gut microbiome, which could ultimately lead to impaired glycemic control and negative physiological health outcomes. To test this hypothesis this study will 1) administer a diet high in glucose, fructose, and 4 common artificial sweeteners separately to rats followed by a plasma metabolic analysis (AIM 1) and 2) treat the gut microbiota with antibiotics in these animals to observe how alterations of the microbiome influence the plasma metabolic profile in animals receiving the altered diets (AIM 2). The resulting data will give us insights into the influence of high sugar and artificial sweetener diets on homeostatic metabolic processes and dive into the symbiotic relationship of the gut microbiome with this process. This data will provide crucial insights into the dietary use of artificial sweeteners in the replacement of sugars and how it alters metabolic pathways that could potentially lead to altered states of obesity, diabetes, and cardiovascular disease.
Institute:	Mayo Clinic
Last Name:	Hoffmann
First Name:	Brian
Address:	8701 Watertown Plank Road Milwaukee, WI 53226
Email:	bhoffmann@mcw.edu
Phone:	414-955-8671

Subject:

Subject ID:	SU000999
Subject Type:	Mammal
Subject Species:	Rattus norvegicus
Taxonomy ID:	10116

Factors:

Subject type: Mammal; Subject species: Rattus norvegicus (Factor headings shown in green)

mb_sample_id	local_sample_id	Grouping
SA057423	ms6706-12	Group 1
SA057424	ms6706-38	Group 1
SA057425	ms6706-39	Group 1
SA057426	ms6706-7	Group 1
SA057427	ms6706-31	Group 1
SA057428	ms6706-6	Group 1
SA057429	ms6706-53	Group 10
SA057430	ms6706-51	Group 10
SA057431	ms6706-54	Group 10
SA057432	ms6706-50	Group 10
SA057433	ms6706-59	Group 10
SA057434	ms6706-60	Group 10
SA057435	ms6706-57	Group 10
SA057436	ms6706-20	Group 2
SA057437	ms6706-21	Group 2
SA057438	ms6706-42	Group 2
SA057439	ms6706-30	Group 2
SA057440	ms6706-10	Group 2
SA057441	ms6706-32	Group 2
SA057442	ms6706-4	Group 3
SA057443	ms6706-28	Group 3
SA057444	ms6706-19	Group 3
SA057445	ms6706-27	Group 3
SA057446	ms6706-5	Group 3
SA057447	ms6706-3	Group 3
SA057448	ms6706-47	Group 4
SA057449	ms6706-33	Group 4
SA057450	ms6706-34	Group 4
SA057451	ms6706-29	Group 4
SA057452	ms6706-14	Group 4
SA057453	ms6706-9	Group 4
SA057454	ms6706-15	Group 5
SA057455	ms6706-26	Group 5
SA057456	ms6706-43	Group 5
SA057457	ms6706-17	Group 5
SA057458	ms6706-23	Group 5
SA057459	ms6706-16	Group 5
SA057460	ms6706-2	Group 6
SA057461	ms6706-44	Group 6
SA057462	ms6706-18	Group 6
SA057463	ms6706-41	Group 6
SA057464	ms6706-25	Group 6
SA057465	ms6706-13	Group 6
SA057466	ms6706-48	Group 7
SA057467	ms6706-11	Group 7
SA057468	ms6706-35	Group 7
SA057469	ms6706-46	Group 7
SA057470	ms6706-22	Group 7
SA057471	ms6706-1	Group 7
SA057472	ms6706-8	Group 8
SA057473	ms6706-45	Group 8
SA057474	ms6706-36	Group 8
SA057475	ms6706-24	Group 8
SA057476	ms6706-37	Group 8
SA057477	ms6706-40	Group 8
SA057478	ms6706-49	Group 9
SA057479	ms6706-55	Group 9
SA057480	ms6706-56	Group 9
SA057481	ms6706-58	Group 9
SA057482	ms6706-52	Group 9

Showing results 1 to 60 of 60

Showing results 1 to 60 of 60

Collection:

Collection ID:	CO000993
Collection Summary:	Samples were collected by cardiac puncture and plasma was collected following standard centrifugation steps. Immediately following the samples were separated into 500 uL aliquots in 600 uL tubes and frozen in liquid nitrogen.
Sample Type:	Blood (plasma)

Treatment:

Treatment ID:	TR001013
Treatment Summary:	We administered normal, high glucose, aspartame, and acesulfame potassium diets to rats for 3 weeks, followed by a plasma collection through cardiac puncture and metabolic analysis (Group 1-4 samples). We also treated the gut microbiota with in rats with the same diets plus bacitracin/streptomycin to observe how alterations of the microbiome influence the plasma metabolic profile in these animals (Groups 5-8). The samples here contain the fructose diet group (Group 9). We also treated the gut microbiota with in rats with the same diets plus bacitracin/streptomycin to observe how alterations of the microbiome influence the plasma metabolic profile in these animals (Groups 5-8). The samples here contain the fructose diet group with antibiotic (Group 10). For the gut microbiota experiment, during the last 10 days of the diet subsets of all groups will have bacitracin and streptomycin (B/S) provided in their drinking water (0.5g/250 mL). The resulting data will give us insights into the influence of high sugar and artificial sweetener diets on homeostatic metabolic processes and dive into the symbiotic relationship of the gut microbiome with this process. Group1 = normal diet Group2 = high glucose diet Group3 = aspartame diet Group4 = acesulfame potassium diet Group5 = rat gut microbiota normal diet + antibotics Group6 = rat gut microbiota high glucose diet + antibotics Group7 = rat gut microbiota aspartame diet + antibotics Group8 = rat gut acesulfame potassium diet + antibotics Group9 = fructose diet Group10 = rat gut fructose diet + antibotics

Treatment ID:

TR001013

Treatment Summary:

We administered normal, high glucose, aspartame, and acesulfame potassium diets to rats for 3 weeks, followed by a plasma collection through cardiac puncture and metabolic analysis (Group 1-4 samples). We also treated the gut microbiota with in rats with the same diets plus bacitracin/streptomycin to observe how alterations of the microbiome influence the plasma metabolic profile in these animals (Groups 5-8). The samples here contain the fructose diet group (Group 9). We also treated the gut microbiota with in rats with the same diets plus bacitracin/streptomycin to observe how alterations of the microbiome influence the plasma metabolic profile in these animals (Groups 5-8). The samples here contain the fructose diet group with antibiotic (Group 10). For the gut microbiota experiment, during the last 10 days of the diet subsets of all groups will have bacitracin and streptomycin (B/S) provided in their drinking water (0.5g/250 mL). The resulting data will give us insights into the influence of high sugar and artificial sweetener diets on homeostatic metabolic processes and dive into the symbiotic relationship of the gut microbiome with this process. Group1 = normal diet Group2 = high glucose diet Group3 = aspartame diet Group4 = acesulfame potassium diet Group5 = rat gut microbiota normal diet + antibotics Group6 = rat gut microbiota high glucose diet + antibotics Group7 = rat gut microbiota aspartame diet + antibotics Group8 = rat gut acesulfame potassium diet + antibotics Group9 = fructose diet Group10 = rat gut fructose diet + antibotics

Sample Preparation:

Sampleprep ID:	SP001006
Sampleprep Summary:	plasma triglyceride (TG) composition

Combined analysis:

Analysis ID	AN001574
Analysis type	MS
Chromatography type	Reversed phase
Chromatography system	Waters Acquity
Column	Waters Acquity BEH C8 (150 x 2mm,1.7um)
MS Type	ESI
MS instrument type	Triple quadrupole
MS instrument name	Thermo Quantum Ultra
Ion Mode	NEGATIVE
Units	% composition by nmol

Chromatography:

Chromatography ID:	CH001103
Instrument Name:	Waters Acquity
Column Name:	Waters Acquity BEH C8 (150 x 2mm,1.7um)
Chromatography Type:	Reversed phase

MS:

MS ID:	MS001452
Analysis ID:	AN001574
Instrument Name:	Thermo Quantum Ultra
Instrument Type:	Triple quadrupole
MS Type:	ESI
Ion Mode:	NEGATIVE