Assessment of H2S in vivo using the newly developed mitochondria-targeted mass spectrometry probe MitoA (original) (raw)
Arndt, S. et al. (2017) Assessment of H2S in vivo using the newly developed mitochondria-targeted mass spectrometry probe MitoA.Journal of Biological Chemistry, 292(19), pp. 7761-7773. (doi: 10.1074/jbc.M117.784678) (PMID:28320864) (PMCID:PMC5427258)
Abstract
Hydrogen sulfide (H2S) is produced endogenously in vivo and has multiple effects on signaling pathways and cell function. Mitochondria can be both an H2S source and sink, and many of the biological effects of H2S relate to its interactions with mitochondria. However, the significance of mitochondrial H2S is uncertain, in part due to the difficulty of assessing changes in its concentration in vivo. Although a number of fluorescent H2S probes have been developed these are best suited to cells in culture and cannot be used in vivo. To address this unmet need we have developed a mitochondria-targeted H2S probe, MitoA, which can be used to assess relative changes in mitochondrial H2S levels in vivo. MitoA comprises a lipophilic triphenylphosphonium (TPP) cation coupled to an aryl azide. The TPP cation leads to the accumulation of MitoA inside mitochondria within tissues in vivo. There, the aryl azido group reacts with H2S to form an aryl amine (MitoN). The extent of conversion of MitoA to MitoN thus gives an indication of the levels of mitochondrial H2S in vivo. Both compounds can be detected sensitively by liquid chromatography tandem mass spectrometry (LC-MS/MS) analysis of the tissues, and quantified relative to deuterated internal standards. Here we describe the synthesis and characterization of MitoA and show that it can be used to assess changes in mitochondrial H2S levels in vivo. As a proof of principle we used MitoA to show that H2S levels increase in vivo during myocardial ischemia.
| Item Type: | Articles |
|---|---|
| Status: | Published |
| Refereed: | Yes |
| Glasgow Author(s) Enlighten ID: | Hartley, Professor Richard |
| Authors: | Arndt, S., Baeza-Garza, C. D., Logan, A., Rosa, T., Wedmann, R., Prime, T. A., Martin, J. L., Saeb-Parsy, K., Krieg, T., Filipovic, M. R., Hartley, R. C., and Murphy, M. P. |
| College/School: | College of Science and Engineering > School of Chemistry |
| Journal Name: | Journal of Biological Chemistry |
| Publisher: | American Society for Biochemistry and Molecular Biology, Inc. |
| ISSN: | 0021-9258 |
| ISSN (Online): | 1083-351X |
| Published Online: | 20 March 2017 |
| Copyright Holders: | Copyright © 2017 The American Society for Biochemistry and Molecular Biology, Inc. |
| First Published: | First published in Journal of Biological Chemistry 292(19):7761-7773 |
| Publisher Policy: | Reproduced under a Creative Commons License |
University Staff: Request a correction | Enlighten Editors: Update this record
Funder and Project Information
1
'Exploring mitochondrial metabolism in health and disease using targeted biological chemistry
Richard Hartley
110158/Z/15/Z
CHEM - CHEMISTRY
1
Developing chemical mass spectrometry probes to assess the production of reactive oxygen species in vivo
Richard Hartley
BB/I012826/1
CHEM - CHEMISTRY
Deposit and Record Details
| ID Code: | 138582 |
|---|---|
| Depositing User: | Ms Mary Anne Meyering |
| Datestamp: | 21 Mar 2017 09:48 |
| Last Modified: | 28 May 2020 15:27 |
| Date of acceptance: | 20 March 2017 |
| Date of first online publication: | 20 March 2017 |
| Date Deposited: | 21 March 2017 |
| Data Availability Statement: | No |