CRISP - Computer Retrieval of Information on Scientific Projects, Abstract Display

Version 2.5.2.0

Abstract

Grant Number: 1R33DK070291-01

Project Title: Dynamic Metabolomics via Isotopomer Analysis (RMI)

PI Information: Name Email Title

BRUNENGRABER, HENRI hxb8@case.edu PROFESSOR AND CHAIR

Abstract: DESCRIPTION (provided by applicant): The general aim of metabolomics is to identify, measure and interpret the complex time-related concentration, activity and flux of endogenous metabolites in cells, tissues, and other biosamples. We propose a three-pronged approach to metabolomics: (i) upgrading metabolite measurements by focusing on instrumentation to increase sensitivity, (ii) employing C-labeled substrates and 2H2O to generate data enabling estimates of fluxes in metabolic networks via mass isotopomer analysis, and (iii) utilizing state of the art models and multivariate statistics to test the hypothesis that specific tracers add information to metabolomics. The three aims of the study are: 1. To expand analytical procedures for the concentration and mass isotopomer distribution of metabolites (acyl-CoAs, acylcarnitines, aminoacids, carboxylic acids, as well as intermediates of glycolysis, the pentosephosphate pathway, and the citric acid cycle) extracted from perfused rat livers, as well as from the plasma and urine of control, and insulin resistant rats. A matrix isotopomer balance method will be used to fit isotopomer labeling patterns to fluxes. 2. To study the temporal patterns of concentration and mass isotopomer distribution of both known and unknown metabolites extracted from perfused liver, plasma, urine and organs of mice. Changes in the profiles following an intervention will identify discriminating intermediates and isotopomers, which may play a role in metabolic regulation. We will apply multivariate statistical methods to reduce the dimensions of the data set of unknown peaks, detecting those that discriminate between treatments. 3. To investigate the temporal pattern of concentration and mass isotopomer distribution of metabolites labeled from 2H-enriched water in perfused organs and in vivo. 2H2O, which is non-toxic at low enrichment, distributes evenly in all body compartments, and is an ideal as a metabolomics probe for human studies. Multivariate statistical tests will determine if 2H2O enhances concentration-based metabolomics. The significance of our study is two-fold. First, we provide a bridge in developing metabolomics, moving from a solid foundation in hypothesis-based research to a new data-driven "omics" approach. Second, we provide a rigorous test of the hypothesis that the mathematical analysis of mass isotopomer data enhances concentration-based metabolomics to provide new avenues for understanding metabolic diseases.
Public Health Relevance:
This Public Health Relevance is not available.
Thesaurus Terms:
analytical method, metabolomics, stable isotope, technology /technique development
carbon, deuterium
biotechnology, laboratory mouse, laboratory rat

Institution: CASE WESTERN RESERVE UNIVERSITY

10900 EUCLID AVE

CLEVELAND, OH 44106

Fiscal Year: 2004

Department: NUTRITION

Project Start: 30-SEP-2004

Project End: 31-JUL-2007

ICD: NATIONAL INSTITUTE OF DIABETES AND DIGESTIVE AND KIDNEY DISEASES

IRG: ZRG1

Grant Number:	1R33DK070291-01
Project Title:	Dynamic Metabolomics via Isotopomer Analysis (RMI)

PI Information:	Name	Email	Title
	BRUNENGRABER, HENRI	hxb8@case.edu	PROFESSOR AND CHAIR

Institution:	CASE WESTERN RESERVE UNIVERSITY
	10900 EUCLID AVE
	CLEVELAND, OH 44106
Fiscal Year:	2004
Department:	NUTRITION
Project Start:	30-SEP-2004
Project End:	31-JUL-2007
ICD:	NATIONAL INSTITUTE OF DIABETES AND DIGESTIVE AND KIDNEY DISEASES
IRG:	ZRG1