Summary of Study ST000549

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 PR000383. The data can be accessed directly via it's Project DOI: 10.21228/M8JG7B This work is supported by NIH grant, U2C- DK119886.

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Study ID	ST000549
Study Title	Investigating large scale metabolomics in mice serum lacking insulin receptors and IGF-1 receptors
Study Summary	Large scale metabolomics from control, M-IR-/-, M-IGF1R-/- , and MIGIRKO mice serum. Also compare mice on a chow diet to mice on a high fat diet (HFD).
Institute	Mayo Clinic
Last Name	O'Neill
First Name	Brian
Address	One Joslin Place, Boston, MA 02215
Email	brian.o'neill@joslin.harvard.edu
Phone	617-309-2400
Submit Date	2017-02-03
Analysis Type Detail	LC-MS
Release Date	2019-03-06
Release Version	1

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Project:

Project ID:	PR000383
Project DOI:	doi: 10.21228/M8JG7B
Project Title:	Mayo Metabolomics Pilot and Feasibility Award: Role of muscle insulin and IGF-1 signaling on serum and muscle metabolite profiles
Project Summary:	Skeletal muscle insulin resistance is a cardinal feature of the pathogenesis of type 2 diabetes. Insulin and IGF-1 signal through their highly related receptors to impact on many aspects of muscle physiology including glucose homeostasis, protein metabolism, and mitochondrial function. Early physiological studies, as well as recent large scale metabolomic studies, have shown that changes in specific pools of circulating amino acid metabolites, such as branched chain amino acids (BCAAs), are associated with insulin resistance and can predict future diabetes, but the source and impact of these changes in amino acids are not fully understood. We have recently generated mice which lack insulin receptors (IR) or IGF-1 receptors (IGF1R) or both in muscle using Cre lox recombination. We find that mice which lack only IR or only IGF1R in muscle show minimal changes in muscle mass, but do display increases in proteasomal activity and autophagy in muscle. On the other hand, mice with combined loss of both IR and IGF1R display markedly decreased muscle mass and enhanced degradation pathways, associated with increased protein synthesis, and display changes in mitochondrial gene regulation, indicating that both receptors can compensate to some extent for loss of the other. We hypothesize that IR and IGF1R signaling in muscle coordinate amino acid metabolite turnover and fuel substrate/mitochondrial metabolism, and that in insulin resistant states, changes in protein metabolism and mitochondrial function disrupt relative proportions of amino acid metabolites, which in turn contribute to diabetes risk and/or muscle pathology. We propose to test this hypothesis by performing large scale metabolomics on serum and muscle from mice lacking IR, IGF1R or both in muscle, and we will compare these changes to both insulin deficient streptozotocin-treated and insulin resistant diet-induced obese mouse models. To gain insight into which pathways are critical for metabolite changes, we will also treat mice with specific inhibitors of mTOR, a common protein synthesis pathway, as well as inhibitors of autophagy or proteasomal degradation and determine metabolite concentrations in muscle and serum. These studies will identify specific pathways that impact amino acid and mitochondrial metabolite flux which are perturbed in insulin resistant states, and potentially provide insights into how changes in amino acid metabolites contribute to diabetes risk.
Institute:	Mayo Clinic
Last Name:	O'Neill
First Name:	Brian
Address:	One Joslin Place, Boston, MA 02215
Email:	brian.o'neill@joslin.harvard.edu
Phone:	617-309-2400

Subject:

Subject ID:	SU000571
Subject Type:	Mouse
Subject Species:	Mus musculus
Taxonomy ID:	10090
Species Group:	Mammal

Factors:

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

mb_sample_id	local_sample_id	Group	Genotype
SA028326	19jan15_08	CD	Irlox
SA028327	05jan15_35-r001	CD	Irlox
SA028328	05jan15_35-r002	CD	Irlox
SA028329	05jan15_25-r001	CD	Irlox
SA028330	19jan15_06	CD	Irlox
SA028331	19jan15_25	CD	Irlox
SA028332	19jan15_65	CD	Irlox
SA028333	05jan15_08-r002	CD	Irlox
SA028334	19jan15_75	CD	Irlox
SA028335	05jan15_25-r002	CD	Irlox
SA028336	19jan15_48	CD	Irlox
SA028337	05jan15_06-r001	CD	Irlox
SA028338	19jan15_46	CD	Irlox
SA028339	05jan15_06-r002	CD	Irlox
SA028340	05jan15_08-r001	CD	Irlox
SA028341	19jan15_35	CD	Irlox
SA028342	19jan15_09	Control	IGFR lox
SA028343	05jan15_13-r001	Control	IGFR lox
SA028344	05jan15_13-r002	Control	IGFR lox
SA028345	19jan15_71	Control	IGFR lox
SA028346	19jan15_13	Control	IGFR lox
SA028347	05jan15_31-r002	Control	IGFR lox
SA028348	19jan15_31	Control	IGFR lox
SA028349	19jan15_53	Control	IGFR lox
SA028350	19jan15_49	Control	IGFR lox
SA028351	05jan15_09-r001	Control	IGFR lox
SA028352	05jan15_31-r001	Control	IGFR lox
SA028353	05jan15_09-r002	Control	IGFR lox
SA028370	19jan15_58	Control	Irlox
SA028371	19jan15_21	Control	Irlox
SA028372	19jan15_61	Control	Irlox
SA028373	19jan15_28	Control	Irlox
SA028374	05jan15_28-r001	Control	Irlox
SA028375	19jan15_60	Control	Irlox
SA028376	19jan15_20	Control	Irlox
SA028377	05jan15_20-r001	Control	Irlox
SA028378	05jan15_18-r002	Control	Irlox
SA028379	05jan15_20-r002	Control	Irlox
SA028380	05jan15_21-r002	Control	Irlox
SA028381	05jan15_28-r002	Control	Irlox
SA028382	05jan15_18-r001	Control	Irlox
SA028383	05jan15_21-r001	Control	Irlox
SA028384	19jan15_68	Control	Irlox
SA028385	19jan15_18	Control	Irlox
SA028354	19jan15_30	Control	IRlox IGFR lox
SA028355	19jan15_32	Control	IRlox IGFR lox
SA028356	05jan15_27-r002	Control	IRlox IGFR lox
SA028357	19jan15_29	Control	IRlox IGFR lox
SA028358	19jan15_27	Control	IRlox IGFR lox
SA028359	05jan15_27-r001	Control	IRlox IGFR lox
SA028360	19jan15_70	Control	IRlox IGFR lox
SA028361	05jan15_32-r001	Control	IRlox IGFR lox
SA028362	05jan15_30-r002	Control	IRlox IGFR lox
SA028363	19jan15_67	Control	IRlox IGFR lox
SA028364	19jan15_69	Control	IRlox IGFR lox
SA028365	05jan15_30-r001	Control	IRlox IGFR lox
SA028366	19jan15_72	Control	IRlox IGFR lox
SA028367	05jan15_32-r002	Control	IRlox IGFR lox
SA028368	05jan15_29-r001	Control	IRlox IGFR lox
SA028369	05jan15_29-r002	Control	IRlox IGFR lox
SA028386	05jan15_39-r001	HFD	Irlox
SA028387	05jan15_39-r002	HFD	Irlox
SA028388	05jan15_40-r001	HFD	Irlox
SA028389	05jan15_04-r002	HFD	Irlox
SA028390	05jan15_40-r002	HFD	Irlox
SA028391	05jan15_38-r002	HFD	Irlox
SA028392	19jan15_44	HFD	Irlox
SA028393	05jan15_10-r002	HFD	Irlox
SA028394	05jan15_11-r001	HFD	Irlox
SA028395	05jan15_11-r002	HFD	Irlox
SA028396	05jan15_10-r001	HFD	Irlox
SA028397	05jan15_38-r001	HFD	Irlox
SA028398	05jan15_04-r001	HFD	Irlox
SA028399	19jan15_51	HFD	Irlox
SA028400	19jan15_11	HFD	Irlox
SA028401	19jan15_10	HFD	Irlox
SA028402	19jan15_04-r001	HFD	Irlox
SA028403	19jan15_50	HFD	Irlox
SA028404	19jan15_78	HFD	Irlox
SA028405	19jan15_79	HFD	Irlox
SA028406	19jan15_38	HFD	Irlox
SA028407	19jan15_39	HFD	Irlox
SA028408	05jan15_23-r002	IGFRKO	IGFR -/-
SA028409	05jan15_14-r002	IGFRKO	IGFR -/-
SA028410	05jan15_14-r001	IGFRKO	IGFR -/-
SA028411	19jan15_12	IGFRKO	IGFR -/-
SA028412	05jan15_34-r001	IGFRKO	IGFR -/-
SA028413	19jan15_14	IGFRKO	IGFR -/-
SA028414	19jan15_74	IGFRKO	IGFR -/-
SA028415	19jan15_63	IGFRKO	IGFR -/-
SA028416	05jan15_34-r002	IGFRKO	IGFR -/-
SA028417	19jan15_52	IGFRKO	IGFR -/-
SA028418	19jan15_34	IGFRKO	IGFR -/-
SA028419	19jan15_45	IGFRKO	IGFR -/-
SA028420	05jan15_05-r002	IGFRKO	IGFR -/-
SA028421	05jan15_05-r001	IGFRKO	IGFR -/-
SA028422	19jan15_54	IGFRKO	IGFR -/-
SA028423	05jan15_23-r001	IGFRKO	IGFR -/-
SA028424	19jan15_23	IGFRKO	IGFR -/-
SA028425	05jan15_12-r002	IGFRKO	IGFR -/-

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Collection:

Collection ID:	CO000565
Collection Summary:	mouse serum
Sample Type:	Blood

Treatment:

Treatment ID:	TR000585
Treatment Summary:	Mice lacking insulin receptors (IR -/- genotype, IRKO group), or IGF-1 receptors (ICF-1 -/- genotype, IGFRKO group), or both (MIGIRKO group) were generated using Cre lox recombination. Controls (group control and CD) were IR lox/lox, IGF-1 lox/lox, or both genotypes. Additional, 10 mice were included that were fed different diets for 8 weeks, chow or high fat diet (group HFD).

Sample Preparation:

Sampleprep ID:	SP000578
Sampleprep Summary:	large scale metabolomics in mouse serum

Combined analysis:

Analysis ID	AN000837	AN000838	AN000839
Analysis type	MS	MS	MS
Chromatography type	HILIC	HILIC	Reversed phase
Chromatography system	Agilent 1290 Infinity	Agilent 1290 Infinity	Agilent 1290 Infinity
Column	Waters Acquity BEH Amide (150 x 2.1mm,1.7um)	Waters Acquity BEH Amide (150 x 2.1mm,1.7um)	Waters Acquity HSS C18 (150 x 2.1mm,1.8um)
MS Type	ESI	ESI	ESI
MS instrument type	QTOF	QTOF	QTOF
MS instrument name	Agilent 6550 QTOF	Agilent 6550 QTOF	Agilent 6550 QTOF
Ion Mode	POSITIVE	NEGATIVE	POSITIVE
Units	intensity	intensity	intensity

Chromatography:

Chromatography ID:	CH000598
Instrument Name:	Agilent 1290 Infinity
Column Name:	Waters Acquity BEH Amide (150 x 2.1mm,1.7um)
Chromatography Type:	HILIC

Chromatography ID:	CH000599
Instrument Name:	Agilent 1290 Infinity
Column Name:	Waters Acquity HSS C18 (150 x 2.1mm,1.8um)
Chromatography Type:	Reversed phase

MS:

MS ID:	MS000738
Analysis ID:	AN000837
Instrument Name:	Agilent 6550 QTOF
Instrument Type:	QTOF
MS Type:	ESI
Ion Mode:	POSITIVE

MS ID:	MS000739
Analysis ID:	AN000838
Instrument Name:	Agilent 6550 QTOF
Instrument Type:	QTOF
MS Type:	ESI
Ion Mode:	NEGATIVE

MS ID:	MS000740
Analysis ID:	AN000839
Instrument Name:	Agilent 6550 QTOF
Instrument Type:	QTOF
MS Type:	ESI
Ion Mode:	POSITIVE