Summary of Study ST001836

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 PR001157. The data can be accessed directly via it's Project DOI: 10.21228/M8510S 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	ST001836
Study Title	Quantitative lipids study on blood serum and ceacal content of rat models
Study Type	blood serum and caecum content
Study Summary	Lipids were analyzed in blood serum and cecal content in rat models
Institute	Helmholtz Centre for Environmental Research
Department	Department of Molecular Systems biology
Laboratory	Functional Metabolomics
Last Name	Rolle-Kampczyk
First Name	Ulrike
Address	Permoserstrasse 15, 04318 Leipzig, Germany
Email	ulrike.rolle-kampczyk@ufz.de
Phone	0049 341 235 1537
Submit Date	2021-06-21
Raw Data Available	Yes
Raw Data File Type(s)	wiff
Analysis Type Detail	LC-MS
Release Date	2021-07-02
Release Version	1

Select appropriate tab below to view additional metadata details:

Project:

Project ID:	PR001157
Project DOI:	doi: 10.21228/M8510S
Project Title:	Fecal Transplant from Roux-Y-Gastric-Bypass rat model into a diet induced obesity rat model
Project Summary:	Investigating alterations in the intestinal microbiome metabolome and host blood metabolome in a diet induced obesity (DIO) rat model after fecal transplant from rats, which underwent Roux-Y-Gastric-Bypass surgery (RYGB). Experimental groups for rat experiments. 1)Rats in the ‘RYGB_Donor group’ underwent RYGB surgery. Postoperatively, animals received a two-choice diet, consisting of a SC and HFD. Once the animals recovered and achieved a stabilized weight reduction at 4 weeks postoperatively, body weight and food intake were recorded daily. 2)Rats allocated into the ‘RYGB_AB group’ were handled the same as animals in the ‘RYGB_donor group’. From postoperative week 4 onwards, animals received an antibiotic treatment (AB) consisting of ampicillin (1 g/l; Ratiopharm), vancomycin (0.5 g/l; Ratiopharm), neomycin (1 g/l; Bela-pharm), and metronidazole (1 g/l; CP-Pharma), provided freshly every day via drinking water.[19, 20] All antibiotics were given for the time period indicated in each figure.[21] 3)Rats in the ‘Lean group’ served as healthy, age-matched controls, constantly kept under SC. 4)Rats in the ‘Lean_AB group’ received the same antibiotic treatment as animals in the RYGB_AB group, serving as a control for antibiotic-specific side effects. All antibiotics were given for the time periods indicated in each figure. 5)Rats in the ‘DIO group’ received no surgery, but were otherwise handled like RYGB litter mates. 6)Rats in the ‘DIO_FMT_RYGB group’ received fecal RYGB_Donor microbiota transplantation once per week, but were otherwise handled like DIO litter mates. For fecal transplantation experiments, 100 mg of fresh stool from body weight-stabilized RYGB donors were re-suspended in 1 ml of PBS, homogenized carefully and administered via oral gavage with 200 μl of the suspension. 7)Rats in the ‘FMT_Lean group’ were handled like DIO litter mates, but were orally gavaged with 200 μl of filtrate received from lean donors, and served as a control for fecal transplantation and specificity of effect size(s) as a function of the donor microbiota. 8)Rats in the ‘DIO_PF_FMT group’ were handled like DIO litter mates, but pair-fed to the SC/HFD food intake of ‘FMT_Lean littermates, serving as a control for effects secondary to reduced caloric intake.
Institute:	Helmholtz Centre for Environmental Research - UFZ
Last Name:	Haange
First Name:	Sven
Address:	Permoserstrasse 1, Leipzig, Saxony, 04318, Germany
Email:	sven.haange@ufz.de
Phone:	0049 341 2351099

Subject:

Subject ID:	SU001913
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	Tissue	Sample treatment
SA170686	1024038893	Caecum	DIO
SA170687	1024038904	Caecum	DIO
SA170688	1024041219	Caecum	DIO
SA170689	1024038919	Caecum	DIO
SA170690	1024038651	Caecum	DIO
SA170691	1024038923	Caecum	DIO
SA170692	1024041363	Caecum	DIO
SA170693	1024041378	Caecum	DIO
SA170694	1024041295	Caecum	DIO
SA170695	1024041276	Caecum	DIO
SA170696	1024035756	Caecum	DIO_AB
SA170697	1024035775	Caecum	DIO_AB
SA170698	1024041223	Caecum	DIO_AB
SA170699	1024041261	Caecum	DIO_AB
SA170700	1024041238	Caecum	DIO_AB
SA170701	1024041242	Caecum	DIO_AB
SA170702	1024041382	Caecum	DIO_FMT_RYGB
SA170703	1024041325	Caecum	DIO_FMT_RYGB
SA170704	1024038671	Caecum	DIO_FMT_RYGB
SA170705	1024038860	Caecum	DIO_FMT_RYGB
SA170706	1024038841	Caecum	DIO_FMT_RYGB
SA170707	1024038666	Caecum	DIO_FMT_RYGB
SA170708	1024041257	Caecum	DIO_FMT_RYGB
SA170709	1024038874	Caecum	DIO_FMT_RYGB
SA170710	1024041281	Caecum	DIO_FMT_RYGB
SA170711	1024038889	Caecum	DIO_FMT_RYGB
SA170712	1024038938	Caecum	DIO_PF_FMT
SA170713	1024038942	Caecum	DIO_PF_FMT
SA170714	1024038981	Caecum	DIO_PF_FMT
SA170715	1024038957	Caecum	DIO_PF_FMT
SA170716	1024038961	Caecum	DIO_PF_FMT
SA170717	1024038976	Caecum	DIO_PF_FMT
SA170718	1024041408	Caecum	FMT_lean
SA170719	1024041397	Caecum	FMT_lean
SA170720	1024041330	Caecum	FMT_lean
SA170721	1024041359	Caecum	FMT_lean
SA170722	1024035761	Caecum	FMT_lean
SA170723	1024041344	Caecum	FMT_lean
SA170724	1024041311	Caecum	Lean
SA170725	1024038995	Caecum	Lean
SA170726	1024039011	Caecum	Lean
SA170727	1024039007	Caecum	Lean
SA170728	1024041306	Caecum	Lean
SA170729	1024038753	Caecum	Lean
SA170730	1024038802	Caecum	Lean
SA170731	1024039026	Caecum	Lean
SA170732	1024038768	Caecum	Lean
SA170733	1024038791	Caecum	Lean
SA170734	1024032782	Caecum	Lean_AB
SA170735	1024032797	Caecum	Lean_AB
SA170736	1024038787	Caecum	Lean_AB
SA170737	1024038772	Caecum	Lean_AB
SA170738	1024038734	Caecum	Lean_AB
SA170739	1024038749	Caecum	Lean_AB
SA170740	1024041465	Caecum	RYGB_AB
SA170741	1024041446	Caecum	RYGB_AB
SA170742	1024041484	Caecum	RYGB_AB
SA170743	1024032778	Caecum	RYGB_AB
SA170744	1024038690	Caecum	RYGB_AB
SA170745	1024032763	Caecum	RYGB_AB
SA170746	1024038685	Caecum	RYGB_AB
SA170747	1024038720	Caecum	RYGB_AB
SA170748	1024032759	Caecum	RYGB_AB
SA170749	1024041427	Caecum	RYGB_Donor
SA170750	1024041431	Caecum	RYGB_Donor
SA170751	1024038836	Caecum	RYGB_Donor
SA170752	1024041412	Caecum	RYGB_Donor
SA170753	1024032744	Caecum	RYGB_Donor
SA170754	1024041451	Caecum	RYGB_Donor
SA170755	1024038701	Caecum	RYGB_Donor
SA170756	1024038715	Caecum	RYGB_Donor
SA170757	1024038821	Caecum	RYGB_Donor
SA170758	1024033074	Plasma	DIO
SA170759	1024033093	Plasma	DIO
SA170760	1024033060	Plasma	DIO
SA170761	1024033089	Plasma	DIO
SA170762	1024033036	Plasma	DIO_FMT_RYGB
SA170763	1024033041	Plasma	DIO_FMT_RYGB
SA170764	1024033055	Plasma	DIO_FMT_RYGB
SA170765	1024033021	Plasma	DIO_FMT_RYGB
SA170766	1024033104	Plasma	DIO_PF_FMT
SA170767	1024033119	Plasma	DIO_PF_FMT
SA170768	1024035794	Plasma	DIO_PF_FMT
SA170769	1024035780	Plasma	DIO_PF_FMT
SA170770	1024035805	Plasma	DIO_PF_FMT
SA170771	1024035810	Plasma	DIO_PF_FMT
SA170772	1024035843	Plasma	Lean
SA170773	1024035858	Plasma	Lean
SA170774	1024035824	Plasma	Lean
SA170775	1024035839	Plasma	Lean
SA170776	1024032971	Plasma	RYGB_AB
SA170777	1024033017	Plasma	RYGB_AB
SA170778	1024032991	Plasma	RYGB_AB
SA170779	1024032952	Plasma	RYGB_Donor
SA170780	1024032933	Plasma	RYGB_Donor
SA170781	1024032948	Plasma	RYGB_Donor
SA170782	1024032986	Plasma	RYGB_Donor
SA170783	1024032638	Serum	DIO
SA170784	1024032623	Serum	DIO
SA170785	1024041174	Serum	DIO

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Collection:

Collection ID:	CO001906
Collection Summary:	Animals were sacrificed, blood and cecum tissue were removed, snap frozen in liquid nitrogen and stored at -80°C until further analysis
Sample Type:	Cecum

Treatment:

Treatment ID:	TR001926
Treatment Summary:	RYGB surgery was performed on age-matched (8-10-weeks old) male Wistar IGS rats. After four weeks of recovery, animals were put on an antibiotic cocktail consisting of ampicillin (1 g/l; Ratiopharm), vancomycin (0.5 g/l; Ratiopharm), neomycin (1 g/l; Bela-pharm), and metronidazole (1 g/l; CP-Pharma), provided freshly every day via drinking water. The parallel FMT group received fecal RYGB microbiota transplantation once per week, but were otherwise handled like DIO littermates. For fecal transplantation experiments, 100 mg of fresh stool from bodyweight-stabilized RYGB donors was re-suspended in 1 ml of PBS, homogenized carefully and administered via oral gavage with 200 μl of the suspension.

Treatment ID:

TR001926

Treatment Summary:

RYGB surgery was performed on age-matched (8-10-weeks old) male Wistar IGS rats. After four weeks of recovery, animals were put on an antibiotic cocktail consisting of ampicillin (1 g/l; Ratiopharm), vancomycin (0.5 g/l; Ratiopharm), neomycin (1 g/l; Bela-pharm), and metronidazole (1 g/l; CP-Pharma), provided freshly every day via drinking water. The parallel FMT group received fecal RYGB microbiota transplantation once per week, but were otherwise handled like DIO littermates. For fecal transplantation experiments, 100 mg of fresh stool from bodyweight-stabilized RYGB donors was re-suspended in 1 ml of PBS, homogenized carefully and administered via oral gavage with 200 μl of the suspension.

Sample Preparation:

Sampleprep ID:	SP001919
Sampleprep Summary:	Sample preparation for MetIDQ p180 Kit measurement Solvents: Acetonitril (Merck KGaA, Darmstadt, Germany hypergrade for LC-MS) Water MiliQ, Extracting agent - ACN / H2O (1:1) Equipment 4 steel balls size M Eppendorf Tubes 2mL Tissue slicer (Rettberg, Germany) Centrifuge (Sigma) Work steps Approximately 100mg of caecum sample and 4 steel balls of size M into each tube. Per mg of sample 5µL of extracting agent was added. Shake the samples for 10 minutes at 30 Hz in the tissue slicer and centrifuge for 2 minutes at 14000 rpm. 10 µL supernatant was used for the targeted analytics. Blood serum samples 10 µL were used for analysis Kit reparation The analysis was performed using the validated MetIDQ p180 Kit and described in Siskos et al. [1]. Data processing was carried out with the provided quantitation method Kit (Biocrates Life Sciences AG, Innsbruck, Austria). 1 Siskos AP, Jain P, Römisch-Margl W, Bennett M, Achaintre D, Asad Y, et al. Interlaboratory Reproducibility of a Targeted Metabolomics Platform for Analysis of Human Serum and Plasma. Anal Chem 2017;89:656-65.

Sampleprep ID:

SP001919

Sampleprep Summary:

Sample preparation for MetIDQ p180 Kit measurement Solvents: Acetonitril (Merck KGaA, Darmstadt, Germany hypergrade for LC-MS) Water MiliQ, Extracting agent - ACN / H2O (1:1) Equipment 4 steel balls size M Eppendorf Tubes 2mL Tissue slicer (Rettberg, Germany) Centrifuge (Sigma) Work steps Approximately 100mg of caecum sample and 4 steel balls of size M into each tube. Per mg of sample 5µL of extracting agent was added. Shake the samples for 10 minutes at 30 Hz in the tissue slicer and centrifuge for 2 minutes at 14000 rpm. 10 µL supernatant was used for the targeted analytics. Blood serum samples 10 µL were used for analysis Kit reparation The analysis was performed using the validated MetIDQ p180 Kit and described in Siskos et al. [1]. Data processing was carried out with the provided quantitation method Kit (Biocrates Life Sciences AG, Innsbruck, Austria). 1 Siskos AP, Jain P, Römisch-Margl W, Bennett M, Achaintre D, Asad Y, et al. Interlaboratory Reproducibility of a Targeted Metabolomics Platform for Analysis of Human Serum and Plasma. Anal Chem 2017;89:656-65.

Combined analysis:

Analysis ID	AN002978
Analysis type	MS
Chromatography type	Reversed phase
Chromatography system	UPLC (Waters Acquity, Waters Corporation, Milford, USA)
Column	Agilent Zorbax Eclipse XDB C18 (100 x 3.0mm,3.5um)
MS Type	ESI
MS instrument type	Triple quadrupole
MS instrument name	ABI Sciex 5500 QTrap
Ion Mode	POSITIVE
Units	µM

Chromatography:

Chromatography ID:	CH002207
Chromatography Summary:	LC - Instrument Parameters AbsoluteIDQ® p180 Kit (Biocrates Life Science AG, Innsbruck, Austria) System: UPLC (Waters Acquity, Waters Corporation, Milford, USA) Column: Agilent, Zorbax Eclipse XDB C18, 3.0 x 100 mm, 3.5 μM, Agilent Waldbronn, Germany Precolumn: Security Guard, Phenomenex, C18, 4 x 3 mm; Phenomenex, Aschaffenburg, Germany Materials: Water MiliQ, Methanol (Merck KGaA, Darmstadt, Germany, hypergrade for LC-MS) Acetonitril (Merck KGaA, Darmstadt, Germany hypergrade for LC-MS) Ammonium Acetate (Honeywell - Fluka, Seelze, Germany) Formic Acid (Honeywell, Fluka, Seelze, Germany) Running Solvent: 5mM ammonium acetat in methanol LC: A: 2mL Formic acid in MilliQ water B: 1mL Formic Acid in Acetonitrile Gradient Table LC Time (min) Flow Rate (mL/min) %A %B Curve Initial 0.500 100.0 0.0 Initial 0.50 0.500 100.0 0.0 6 4.00 0.500 30.0 70.0 6 5.30 0.500 30.0 70.0 6 5.40 0.500 100.0 0.0 6 7.30 0.500 100.0 0.0 6
Methods Filename:	LC_parameters-metabolites.pdf
Instrument Name:	UPLC (Waters Acquity, Waters Corporation, Milford, USA)
Column Name:	Agilent Zorbax Eclipse XDB C18 (100 x 3.0mm,3.5um)
Flow Gradient:	FIA Time (min) Flow Rate (mL/min) %A %B Curve Initial 0.030 0.0 100.0 Initial 1.60 0.030 0.0 100.0 6 2.40 0.200 0.0 100.0 6 2.80 0.200 0.0 100.0 6 3.00 0.030 0.0 100.0 6
Flow Rate:	0.03ml/min
Solvent A:	100% methanol; 5mM ammonium acetate
Solvent B:	50% methanol/50% water; 5mM ammonium acetate
Chromatography Type:	Reversed phase

MS:

MS ID:	MS002768
Analysis ID:	AN002978
Instrument Name:	ABI Sciex 5500 QTrap
Instrument Type:	Triple quadrupole
MS Type:	ESI
MS Comments:	Analyst version 1.6 Software from SCIEX. For Validation METIDQ Software version Boron from Biocrates
Ion Mode:	POSITIVE
Analysis Protocol File:	MS_parameters_1.pdf