Literature DB >> 28163219

Probing the metabolic phenotype of breast cancer cells by multiple tracer stable isotope resolved metabolomics.

Andrew N Lane1, Julie Tan2, Yali Wang3, Jun Yan4, Richard M Higashi5, Teresa W-M Fan6.   

Abstract

Breast cancers vary by their origin and specific set of genetic lesions, which gives rise to distinct phenotypes and differential response to targeted and untargeted chemotherapies. To explore the functional differences of different breast cell types, we performed Stable Isotope Resolved Metabolomics (SIRM) studies of one primary breast (HMEC) and three breast cancer cells (MCF-7, MDAMB-231, and ZR75-1) having distinct genotypes and growth characteristics, using 13C6-glucose, 13C-1+2-glucose, 13C5,15N2-Gln, 13C3-glycerol, and 13C8-octanoate as tracers. These tracers were designed to probe the central energy producing and anabolic pathways (glycolysis, pentose phosphate pathway, Krebs Cycle, glutaminolysis, nucleotide synthesis and lipid turnover). We found that glycolysis was not associated with the rate of breast cancer cell proliferation, glutaminolysis did not support lipid synthesis in primary breast or breast cancer cells, but was a major contributor to pyrimidine ring synthesis in all cell types; anaplerotic pyruvate carboxylation was activated in breast cancer versus primary cells. We also found that glucose metabolism in individual breast cancer cell lines differed between in vitro cultures and tumor xenografts, but not the metabolic distinctions between cell lines, which may reflect the influence of tumor architecture/microenvironment.
Copyright © 2017 International Metabolic Engineering Society. Published by Elsevier Inc. All rights reserved.

Entities:  

Keywords:  (13)C(3)-glycerol; (13)C(3)-glycerol (PubChem CID:753); (13)C(5); (13)C(5),(15)N(2)-Glutamine (PubChem CID:5961); (13)C(6)-glucose; (13)C(6)-glucose (PubChem CID:5793); (13)C(8)-octanoate; (13)C(8)-octanoate (PubChem CID:11939); (15)N(2)-Gln; (PubChem CID:5927); 1D/2D NMR; ATP; Breast cancer metabolism; FT-ICR-MS; Mouse xenografts; Stable isotope-resolved metabolomics; UTP(PubChem CID:6133); alanine (PubChem CID:5950); aspartate (PubChem CID:5460541); glutamate (PubChem CID:5128032); lactate (PubChem CID:91435)

Mesh:

Year:  2017        PMID: 28163219      PMCID: PMC5540847          DOI: 10.1016/j.ymben.2017.01.010

Source DB:  PubMed          Journal:  Metab Eng        ISSN: 1096-7176            Impact factor:   9.783


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