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Inhibition of the carnitine acylcarnitine carrier by carbon monoxide reveals a novel mechanism of action with non-metal-containing proteins

Academic Article
Publication Date:
2022
abstract:
Both toxic and physiological effects of CO are mostly caused by well described interactions with heme-groups of proteins. Interactions of CO with non-heme proteins have also been unveiled. Besides interaction of CO with mitochondrial heme containing respiratory complexes, a BK channel and the phosphate carrier which do not contain metal cofactors, have been identified as CO targets. However, the molecular mechanisms of interaction with non-metal-containing proteins are not understood. We show in this work the effect of CO on the mitochondrial carnitine carrier (SLC25A20) using CORM-3, a widely recognized CO releasing compound. CO exerts an inhibitory effect at the micromolar concentration on the transport function of the transporter extracted from treated mitochondria. The effect is due to a single Cys residue, C136 as revealed by mass spectrometry analysis. A computational approach predicted the need for vicinal Asp and Lys residues for the C136 carbonylation to occur. These data demonstrate a novel mechanism of interaction of CO with a protein not containing metal atoms and will enable the prediction of CO targets.
Iris type:
01.01 Articolo in rivista
Keywords:
mitochondria; SLC25A20; CORM-3; Carbon monoxide
List of contributors:
Tonazzi, Annamaria; Giangregorio, Nicola
Authors of the University:
GIANGREGORIO NICOLA
TONAZZI ANNAMARIA
Handle:
https://iris.cnr.it/handle/20.500.14243/417434
Published in:
FREE RADICAL BIOLOGY & MEDICINE
Journal
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http://www.scopus.com/record/display.url?eid=2-s2.0-85133621735&origin=inward
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