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Dzien, P., et al., Following Metabolism in Living Microorganisms by Hyperpolarized (1)H NMR. J Am Chem Soc, 2016. 138(37): p. 12278-86.
Dissolution dynamic nuclear polarization (dDNP) is used to enhance the sensitivity of nuclear magnetic resonance (NMR), enabling monitoring of metabolism and specific enzymatic reactions in vivo. dDNP involves rapid sample dissolution and transfer to a spectrometer/scanner for subsequent signal detection. So far, most biologically oriented dDNP studies have relied on hyperpolarizing long-lived nuclear spin species such as (13)C in small molecules. While advantages could also arise from observing hyperpolarized (1)H, short relaxation times limit the utility of prepolarizing this sensitive but fast relaxing nucleus. Recently, it has been reported that (1)H NMR peaks in solution-phase experiments could be hyperpolarized by spontaneous magnetization transfers from bound (13)C nuclei following dDNP. This work demonstrates the potential of this sensitivity-enhancing approach to probe the enzymatic process that could not be suitably resolved by (13)C dDNP MR. Here we measured, in microorganisms, the action of pyruvate decarboxylase (PDC) and pyruvate formate lyase (PFL)-enzymes that catalyze the decarboxylation of pyruvate to form acetaldehyde and formate, respectively. While (13)C NMR did not possess the resolution to distinguish the starting pyruvate precursor from the carbonyl resonances in the resulting products, these processes could be monitored by (1)H NMR at 500 MHz. These observations were possible in both yeast and bacteria in minute-long kinetic measurements where the hyperpolarized (13)C enhanced, via (13)C --> (1)H cross-relaxation, the signals of protons binding to the (13)C over the course of enzymatic reactions. In addition to these spontaneous heteronuclear enhancement experiments, single-shot acquisitions based on J-driven (13)C --> (1)H polarization transfers were also carried out. These resulted in higher signal enhancements of the (1)H resonances but were not suitable for multishot kinetic studies. The potential of these (1)H-based approaches for measurements in vivo is briefly discussed.
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Imaging metabolism with hyperpolarized (13)c-labeled cell substrates
From The DNP-NMR Blog:
Imaging metabolism with hyperpolarized (13)c-labeled cell substrates
Brindle, K.M., Imaging metabolism with hyperpolarized (13)c-labeled cell substrates. J Am Chem Soc, 2015. 137(20): p. 6418-27.
http://www.ncbi.nlm.nih.gov/pubmed/25950268
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06-15-2015 02:45 PM
[NMR paper] Simultaneous steady-state and dynamic 13C NMR can differentiate alternative routes of pyruvate metabolism in living cancer cells.
Simultaneous steady-state and dynamic 13C NMR can differentiate alternative routes of pyruvate metabolism in living cancer cells.
http://www.bionmr.com//www.ncbi.nlm.nih.gov/corehtml/query/egifs/http:--highwire.stanford.edu-icons-externalservices-pubmed-standard-jbc_final.gif Related Articles Simultaneous steady-state and dynamic 13C NMR can differentiate alternative routes of pyruvate metabolism in living cancer cells.
J Biol Chem. 2014 Feb 28;289(9):6212-24
Authors: Yang C, Harrison C, Jin ES, Chuang DT, Sherry AD, Malloy CR, Merritt ME,...
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04-26-2014 05:46 PM
Reproducibility study for free-breathing measurements of pyruvate metabolism using hyperpolarized 13C in the heart
From The DNP-NMR Blog:
Reproducibility study for free-breathing measurements of pyruvate metabolism using hyperpolarized 13C in the heart
Lau, A.Z., et al., Reproducibility study for free-breathing measurements of pyruvate metabolism using hyperpolarized (13) C in the heart. Magn Reson Med, 2013. 69(4): p. 1063-71.
http://www.ncbi.nlm.nih.gov/pubmed/22760647
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03-17-2014 07:23 PM
Transmit-Only/Receive-Only Radiofrequency System for Hyperpolarized 13C MRS Cardiac Metabolism Studies in Pigs
From The DNP-NMR Blog:
Transmit-Only/Receive-Only Radiofrequency System for Hyperpolarized 13C MRS Cardiac Metabolism Studies in Pigs
Giovannetti, G., et al., Transmit-Only/Receive-Only Radiofrequency System for Hyperpolarized 13C MRS Cardiac Metabolism Studies in Pigs. Appl. Magn. Reson., 2013. 44(10): p. 1125-1138.
http://dx.doi.org/10.1007/s00723-013-0477-3
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11-21-2013 01:14 AM
Hyperpolarized butyrate: A metabolic probe of short chain fatty acid metabolism in the heart
From The DNP-NMR Blog:
Hyperpolarized butyrate: A metabolic probe of short chain fatty acid metabolism in the heart
Ball, D.R., et al., Hyperpolarized butyrate: A metabolic probe of short chain fatty acid metabolism in the heart. Magn Reson Med, 2013: p. n/a-n/a.
http://www.ncbi.nlm.nih.gov/pubmed/23798473
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11-21-2013 01:14 AM
Detection of Living Anionic Species in Polymerization Reactions Using Hyperpolarized NMR
From The DNP-NMR Blog:
Detection of Living Anionic Species in Polymerization Reactions Using Hyperpolarized NMR
Lee, Y., et al., Detection of Living Anionic Species in Polymerization Reactions Using Hyperpolarized NMR. J. Am. Chem. Soc., 2013. 135(12): p. 4636-4639.
http://dx.doi.org/10.1021/ja4001008
Intermediates during the anionic polymerization of styrene were observed using hyperpolarized NMR. Dissolution dynamic nuclear polarization (DNP) of monomers provides a sufficient signal-to-noise ratio for detection of 13C NMR signals in real time as the reaction progresses. Because...
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04-29-2013 06:02 PM
Design of a quadrature surface coil for hyperpolarized 13C MRS cardiac metabolism studies in pigs
From The DNP-NMR Blog:
Design of a quadrature surface coil for hyperpolarized 13C MRS cardiac metabolism studies in pigs
Due to ENC I'm a bit behind catching up with the literature ... This article below was just published in Concepts in Magnetic Resonance and shows the diverse applications of DNP.
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04-27-2013 01:19 AM
Detection of Living Anionic Species in Polymerization Reactions Using Hyperpolarized NMR
Detection of Living Anionic Species in Polymerization Reactions Using Hyperpolarized NMR
Youngbok Lee, Gyu Seong Heo, Haifeng Zeng, Karen L. Wooley and Christian Hilty
http://pubs.acs.org/appl/literatum/publisher/achs/journals/content/jacsat/0/jacsat.ahead-of-print/ja4001008/aop/images/medium/ja-2013-001008_0005.gif
Journal of the American Chemical Society
DOI: 10.1021/ja4001008
http://feeds.feedburner.com/~ff/acs/jacsat?d=yIl2AUoC8zA
http://feeds.feedburner.com/~r/acs/jacsat/~4/mn-OxDYOupY