Summary of Study ST000997

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 PR000675. The data can be accessed directly via it's Project DOI: 10.21228/M8DX19 This work is supported by NIH grant, U2C- DK119886.

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Study ID	ST000997
Study Title	Acyl Carnitines Concentrations of Primary Sclerosing Cholangitis (part III)
Study Summary	To qualitatively and quantitatively analyze enterohepatically-circulated molecules using targeted acyl carnitines concentrations of peripheral blood collected from primary sclerosing cholangitis (PSC) patients compared to normal and diseased controls. There are three groups of patients. (1) Normal donor controls (ND), (2) Patients with Primary Sclerosing Cholangitis (PSC), and (3) Disease Controls (DC) which are patients with liver disease other than PSC.
Institute	Mayo Clinic
Last Name	O'Hara
First Name	Steven
Address	200 First St. SW, Rochester, Minnesota, 55905, USA
Email	ohara.steven@mayo.edu
Phone	507-284-1006
Submit Date	2017-07-05
Raw Data Available	Yes
Raw Data File Type(s)	raw(Thermo)
Analysis Type Detail	LC-MS
Release Date	2019-07-17
Release Version	1

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Project:

Project ID:	PR000675
Project DOI:	doi: 10.21228/M8DX19
Project Title:	Mayo Pilot and Feasibility: The Enterohepatic Metabolome in Primary Sclerosing Cholangitis
Project Summary:	Emerging in vitro and in vivo data, including work from our laboratory and clinical research group, suggest fundamental pathophysiologic mechanisms in primary sclerosing cholangitis (PSC) that are centered on the enterohepatic circulation of gut-derived molecules. Therefore, in this proposal, we will test the central hypothesis that increased pathologic enterohepatic circulation of enteric metabolites which trigger specific pro-fibroinflammatory hepatobiliary responses are centrally involved in the etiopathogenesis of primary sclerosing cholangitis (PSC). While these processes have been hypothesized to play a significant role in the initiation, progression, and adverse clinical sequelae of PSC, they have not been directly tested to date. In our proposal, we will experimentally address the nature and extent of the metabolomic profiles of portal and peripheral blood as well as bile in patients with PSC. We will perform qualitative and quantitative ultra-performance liquid chromatography/mass spectroscopy-based metabolomic analyses to determine metabolic changes in portal and peripheral plasma and bile. Through subsequent pathway analyses we intend to identify metabolic enzymes and known biochemical pathways that may be altered in PSC. We anticipate that patients with PSC will have distinct alterations in the portal venous and bile metabolomic profiles and associated signaling pathways compared to normal and disease controls; and these alterations may be amenable to pharmacologic manipulation and future therapies.
Institute:	Mayo Clinic
Last Name:	O'Hara
First Name:	Steven
Address:	200 First St. SW, Rochester, Minnesota, 55905, USA
Email:	ohara.steven@mayo.edu
Phone:	507-284-1006

Subject:

Subject ID:	SU001036
Subject Type:	Human
Subject Species:	Homo sapiens
Taxonomy ID:	9606
Species Group:	Mammals

Factors:

Subject type: Human; Subject species: Homo sapiens (Factor headings shown in green)

mb_sample_id	local_sample_id	Grouping
SA061711	ms6723-23	DC
SA061712	ms6723-24	DC
SA061713	ms6723-25	DC
SA061714	ms6723-22	DC
SA061715	ms6723-21	DC
SA061716	ms6723-19	DC
SA061717	ms6723-20	DC
SA061718	ms6723-26	DC
SA061719	ms6723-27	DC
SA061720	ms6723-32	DC
SA061721	ms6723-33	DC
SA061722	ms6723-31	DC
SA061723	ms6723-30	DC
SA061724	ms6723-28	DC
SA061725	ms6723-29	DC
SA061726	ms6723-18	DC
SA061727	ms6723-17	DC
SA061728	ms6723-16	DC
SA061729	ms6723-1	ND
SA061730	ms6723-9	ND
SA061731	ms6723-8	ND
SA061732	ms6723-6	ND
SA061733	ms6723-4	ND
SA061734	ms6723-2	ND
SA061735	ms6723-3	ND
SA061736	ms6723-7	ND
SA061737	ms6723-5	ND
SA061738	ms6723-10	PSC
SA061739	ms6723-15	PSC
SA061740	ms6723-14	PSC
SA061741	ms6723-13	PSC
SA061742	ms6723-12	PSC
SA061743	ms6723-11	PSC

Showing results 1 to 33 of 33

Showing results 1 to 33 of 33

Collection:

Collection ID:	CO001030
Collection Summary:	After obtaining informed consent, portal and peripheral venous blood (4 ml of each) and bile (2 mL) was collected intraoperatively in a red-top tube by a Mayo Clinic LT surgeon. Blood was placed on ice, promptly fractionated by centrifugation, divided into 100 μL aliquots, and stored at -80°C.
Sample Type:	Blood (serum)

Treatment:

Treatment ID:	TR001050
Treatment Summary:	We prospectively enrolled three groups of participants from the Mayo Clinic Liver Transplant inpatient service and outpatient clinics and have collected samples from: i) 9 patients with PSC who underwent living- donor LT, ii) 15 donors (normal controls), and iii) 20 patients with cirrhosis due to a disorder other than PSC who underwent LT (disease controls). The following inclusion and exclusion criteria were applied: Inclusion criteria 1. Adult (age>18 years). 2. PSC patient undergoing LT, healthy living donor, or other chronic liver disease patient undergoing LT. Exclusion Criteria: 1. Females who are pregnant or attempting to become pregnant. 2. Concomitant liver disease (e.g. chronic viral hepatitis in addition to PSC). 3. Acute intestinal disease (infectious enterocolitis, IBD flare) in the past 6 months. 4. Treatment with any investigational drugs within the past 6 months. 5. Use of antibiotics within the past 4 weeks. 6. Any previous organ transplant. 7. Hemodialysis.

Treatment ID:

TR001050

Treatment Summary:

We prospectively enrolled three groups of participants from the Mayo Clinic Liver Transplant inpatient service and outpatient clinics and have collected samples from: i) 9 patients with PSC who underwent living- donor LT, ii) 15 donors (normal controls), and iii) 20 patients with cirrhosis due to a disorder other than PSC who underwent LT (disease controls). The following inclusion and exclusion criteria were applied: Inclusion criteria 1. Adult (age>18 years). 2. PSC patient undergoing LT, healthy living donor, or other chronic liver disease patient undergoing LT. Exclusion Criteria: 1. Females who are pregnant or attempting to become pregnant. 2. Concomitant liver disease (e.g. chronic viral hepatitis in addition to PSC). 3. Acute intestinal disease (infectious enterocolitis, IBD flare) in the past 6 months. 4. Treatment with any investigational drugs within the past 6 months. 5. Use of antibiotics within the past 4 weeks. 6. Any previous organ transplant. 7. Hemodialysis.

Sample Preparation:

Sampleprep ID:	SP001043
Sampleprep Summary:	Acyl Carnitines Concentrations

Combined analysis:

Analysis ID	AN001626
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 Quantiva QQQ
Ion Mode	POSITIVE
Units	uM

Chromatography:

Chromatography ID:	CH001144
Instrument Name:	Waters Acquity
Column Name:	Waters Acquity BEH C8 (150 x 2mm,1.7um)
Chromatography Type:	Reversed phase

MS:

MS ID:	MS001502
Analysis ID:	AN001626
Instrument Name:	Thermo Quantiva QQQ
Instrument Type:	Triple quadrupole
MS Type:	ESI
MS Comments:	uM
Ion Mode:	POSITIVE