Summary of Study ST001743

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 PR001116. The data can be accessed directly via it's Project DOI: 10.21228/M8FM51 This work is supported by NIH grant, U2C- DK119886.

See: https://www.metabolomicsworkbench.org/about/howtocite.php

This study contains a large results data set and is not available in the mwTab file. It is only available for download via FTP as data file(s) here.

Study ID	ST001743
Study Title	The Role of Intestinal-derived FGF15 and Vertical Sleeve Gastrectomy on Plasma Bile Acid Composition in Mice
Study Type	MS analysis
Study Summary	Bariatric surgeries such as the Vertical Sleeve Gastrectomy (VSG) are invasive but provide the most effective long-term metabolic improvements in individuals with obesity and/or Type 2 diabetes. These powerful effects of manipulating the gastrointestinal tract point to an important role of gastrointestinal signals in regulating both energy balance and metabolism. To that end, we have used mouse models of VSG to identify key gut signals that mediate these beneficial effects. Previous data from our rodent model of VSG led us to hypothesize a potential role for the hormone Fibroblast-Growth Factor15/19 (mouse/human ortholog) which pharmacologically can regulate many aspects of energy homeostasis and glucose handling. FGF15 is expressed in ileal enterocytes of the small intestine and is released postprandially. Like many other gut hormones, postprandial plasma concentrations of the human ortholog FGF19 and ileal FGF15 expression in mice increase after VSG. We generated intestinal-specific FGF15 knock out (VilCreERT2; Fgf15f/f) mice and controls, which were maintained on 60% high-fat diet. VSG resulted in increased plasma bile acid levels. However, intestinal-specific FGF15 knock out mice had considerably higher levels of circulating total and hydrophobic bile acids after VSG. Unlike what we had predicted, intestinal-specific FGF15 knock out mice lost more weight after VSG as a result of increased lean tissue loss compared to control mice. Further, the loss of bone mineral density and bone marrow adipose tissue observed after VSG in control mice was even greater in intestinal-specific FGF15 knock out mice, perhaps secondary to anemia and elevated erythropoietin/FGF23. Finally the effect of VSG to improve glucose tolerance and to reduce hepatic cholesterol was also absent in intestinal-specific FGF15 knock out mice. These data point to an important role for intestinal FGF15 to protect the organism from deleterious effects of bile acid toxicity after VSG.
Institute	University of Michigan
Department	Surgery
Laboratory	Seeley Lab
Last Name	Seeley
First Name	Randy
Address	Ann Arbor, MI, 48105, USA
Email	seeleyrj@umich.edu
Phone	734-615-2880
Submit Date	2021-04-13
Raw Data Available	Yes
Raw Data File Type(s)	d
Analysis Type Detail	LC-MS
Release Date	2021-04-29
Release Version	1

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Project:

Project ID:	PR001116
Project DOI:	doi: 10.21228/M8FM51
Project Title:	The Role of Intestinal-derived FGF15 and Vertical Sleeve Gastrectomy on Plasma Bile Acid Composition in Mice
Project Summary:	Bariatric surgeries such as the Vertical Sleeve Gastrectomy (VSG) are invasive but provide the most effective long-term metabolic improvements in individuals with obesity and/or Type 2 diabetes. These powerful effects of manipulating the gastrointestinal tract point to an important role of gastrointestinal signals in regulating both energy balance and metabolism. To that end, we have used mouse models of VSG to identify key gut signals that mediate these beneficial effects. Previous data from our rodent model of VSG led us to hypothesize a potential role for the hormone Fibroblast-Growth Factor15/19 (mouse/human ortholog) which pharmacologically can regulate many aspects of energy homeostasis and glucose handling. FGF15 is expressed in ileal enterocytes of the small intestine and is released postprandially. Like many other gut hormones, postprandial plasma concentrations of the human ortholog FGF19 and ileal FGF15 expression in mice increase after VSG. We generated intestinal-specific FGF15 knock out (VilCreERT2; Fgf15f/f) mice and controls, which were maintained on 60% high-fat diet. VSG resulted in increased plasma bile acid levels. However, intestinal-specific FGF15 knock out mice had considerably higher levels of circulating total and hydrophobic bile acids after VSG. Unlike what we had predicted, intestinal-specific FGF15 knock out mice lost more weight after VSG as a result of increased lean tissue loss compared to control mice. Further, the loss of bone mineral density and bone marrow adipose tissue observed after VSG in control mice was even greater in intestinal-specific FGF15 knock out mice, perhaps secondary to anemia and elevated erythropoietin/FGF23. Finally the effect of VSG to improve glucose tolerance and to reduce hepatic cholesterol was also absent in intestinal-specific FGF15 knock out mice. These data point to an important role for intestinal FGF15 to protect the organism from deleterious effects of bile acid toxicity after VSG.
Institute:	University of Michigan
Department:	MRC2
Laboratory:	Metabolomics core
Last Name:	Kachman
First Name:	Maureen
Address:	1000 Wall St., 5458
Email:	mkachman@med.umich.edu
Phone:	734-232-0842
Funding Source:	NIH: 1U2CDK110678-01, P30-AR069620, P30 DK089503, DK097153, 5T32DK108740, 5T32DK071212-12, UL1TR002240, DK020572, DK089503, DK107282, DK121995, RO1 DK62876 , R24 DK092759, American Diabetes Association grants 1-19-IBS-252 and 1-18-PDF-087

Subject:

Subject ID:	SU001820
Subject Type:	Mammal
Subject Species:	Mus musculus
Taxonomy ID:	10090
Gender:	Male

Factors:

Subject type: Mammal; Subject species: Mus musculus (Factor headings shown in green)

mb_sample_id	local_sample_id	Genotype	Surgery
SA163266	S00046252	CTRL	Sham
SA163267	S00046233	CTRL	Sham
SA163268	S00046245	CTRL	Sham
SA163269	S00046240	CTRL	Sham
SA163270	S00046248	CTRL	Sham
SA163271	S00046241	CTRL	VSG
SA163272	S00046242	CTRL	VSG
SA163273	S00046239	CTRL	VSG
SA163274	S00046234	CTRL	VSG
SA163275	S00046250	CTRL	VSG
SA163276	S00046237	CTRL	VSG
SA163277	S00046254	CTRL	VSG
SA163278	S00046251	FGF15INT-KO	Sham
SA163279	S00046257	FGF15INT-KO	Sham
SA163280	S00046244	FGF15INT-KO	Sham
SA163281	S00046238	FGF15INT-KO	Sham
SA163282	S00046247	FGF15INT-KO	Sham
SA163283	S00046236	FGF15INT-KO	Sham
SA163284	S00046235	FGF15INT-KO	VSG
SA163285	S00046256	FGF15INT-KO	VSG
SA163286	S00046253	FGF15INT-KO	VSG
SA163287	S00046232	FGF15INT-KO	VSG
SA163288	S00046249	FGF15INT-KO	VSG

Showing results 1 to 23 of 23

Showing results 1 to 23 of 23

Collection:

Collection ID:	CO001813
Collection Summary:	Mouse blood collection
Sample Type:	Blood (plasma)

Treatment:

Treatment ID:	TR001833
Treatment Summary:	HFD diet after sham or VSG surgery

Sample Preparation:

Sampleprep ID:	SP001826
Sampleprep Summary:	Standard bile acid analysis sample prep
Sampleprep Protocol Filename:	Bile_Acids_Assay.pdf

Combined analysis:

Analysis ID	AN002836
Analysis type	MS
Chromatography type	Reversed phase
Chromatography system	Agilent 6410
Column	Waters XBridge C18 (150mm x 2.1mm,3.5um)
MS Type	ESI
MS instrument type	Triple quadrupole
MS instrument name	Agilent 6410 QQQ
Ion Mode	NEGATIVE
Units	nM

Chromatography:

Chromatography ID:	CH002099
Instrument Name:	Agilent 6410
Column Name:	Waters XBridge C18 (150mm x 2.1mm,3.5um)
Chromatography Type:	Reversed phase

MS:

MS ID:	MS002629
Analysis ID:	AN002836
Instrument Name:	Agilent 6410 QQQ
Instrument Type:	Triple quadrupole
MS Type:	ESI
MS Comments:	Agilent Data Acquisition/Agilent Quant
Ion Mode:	NEGATIVE