Differential proteomic and oxidative profiles unveil dysfunctional protein import to adipocyte mitochondria in obesity-associated aging and diabetes

Gomez-Serrano, Maria; Camafeita, Emilio; Lopez, Juan Antonio; Rubio, Miguel A.; Breton, Irene; Garcia-Consuegra, Ines; Garcia-Santos, Eva; Lago, Jesus; Sanchez-Pernaute, Andres; Torres, Antonio; Vazquez, Jesus; Peral, Belen

Publication:
Differential proteomic and oxidative profiles unveil dysfunctional protein import to adipocyte mitochondria in obesity-associated aging and diabetes

dc.contributor.author	Gomez-Serrano, Maria
dc.contributor.author	Camafeita, Emilio
dc.contributor.author	Lopez, Juan Antonio
dc.contributor.author	Rubio, Miguel A.
dc.contributor.author	Breton, Irene
dc.contributor.author	Garcia-Consuegra, Ines
dc.contributor.author	Garcia-Santos, Eva
dc.contributor.author	Lago, Jesus
dc.contributor.author	Sanchez-Pernaute, Andres
dc.contributor.author	Torres, Antonio
dc.contributor.author	Vazquez, Jesus
dc.contributor.author	Peral, Belen
dc.contributor.funder	Ministerio de Economía, Industria y Competitividad (España)
dc.contributor.funder	Unión Europea. Fondo Europeo de Desarrollo Regional (FEDER/ERDF)
dc.contributor.funder	Autonomous University of Madrid (España)
dc.contributor.funder	Instituto de Salud Carlos III
dc.contributor.funder	Fundación ProCNIC
dc.date.accessioned	2017-10-20T10:23:13Z
dc.date.available	2017-10-20T10:23:13Z
dc.date.issued	2017
dc.description.abstract	Human age-related diseases, including obesity and type 2 diabetes (T2DM), have long been associated to mitochondrial dysfunction; however, the role for adipose tissue mitochondria in these conditions remains unknown. We have tackled the impact of aging and T2DM on adipocyte mitochondria from obese patients by quantitating not only the corresponding abundance changes of proteins, but also the redox alterations undergone by Cys residues thereof. For that, we have resorted to a high-throughput proteomic approach based on isobaric labeling, liquid chromatography and mass spectrometry. The alterations undergone by the mitochondrial proteome revealed aging-and T2DM-specific hallmarks. Thus, while a global decrease of oxidative phosphorylation (OXPHOS) subunits was found in aging, the diabetic patients exhibited a reduction of specific OXPHOS complexes as well as an up-regulation of the anti-oxidant response. Under both conditions, evidence is shown for the first time of a link between increased thiol protein oxidation and decreased protein abundance in adipose tissue mitochondria. This association was stronger in T2DM, where OXPHOS mitochondrial-vs. nuclear-encoded protein modules were found altered, suggesting impaired mitochondrial protein translocation and complex assembly. The marked down-regulation of OXPHOS oxidized proteins and the alteration of oxidized Cys residues related to protein import through the redox-active MIA (Mitochondrial Intermembrane space Assembly) pathway support that defects in protein translocation to the mitochondria may be an important underlying mechanism for mitochondrial dysfunction in T2DM and physiological aging. The present draft of redox targets together with the quantification of protein and oxidative changes may help to better understand the role of oxidative stress in both a physiological process like aging and a pathological condition like T2DM.
dc.description.peerreviewed	Sí
dc.description.sponsorship	This work was supported by grant SAF2012-33014 from MINECO, Spain (B.P.) and partially financed with FEDER funds, FPI-UAM Program (M.G.S.), PI15/01199 from ISCIII, Spain (A.T.) and Pro CNIC Foundation (E.C., J.A.L. and J.V). All data and materials are available.
dc.format.page	415-428
dc.format.volume	11
dc.identifier	ISI:000398212000042
dc.identifier.citation	Redox Biol. 2017; 11:415-428
dc.identifier.doi	10.1016/j.redox.2016.12.013
dc.identifier.issn	2213-2317
dc.identifier.journal	Redox Biology
dc.identifier.pubmedID	28064117
dc.identifier.uri	http://hdl.handle.net/20.500.12105/5125
dc.language.iso	eng
dc.publisher	Elsevier
dc.relation.projectFECYT	info:eu-repo/grantAgreement/ES/SAF2012-33014
dc.relation.projectFIS	info:fis/Instituto de Salud Carlos III/null/null/Subprograma de proyectos de investigacion en salud (AES 2015). Modalidad proyectos en salud. (2015)/PI15/01199
dc.relation.publisherversion	https://doi.org/10.1016/j.redox.2016.12.013
dc.repisalud.institucion	CNIC
dc.repisalud.orgCNIC	CNIC::Grupos de investigación::Proteómica cardiovascular
dc.repisalud.orgCNIC	CNIC::Unidades técnicas::Proteómica / Metabolómica
dc.rights.accessRights	open access	es_ES
dc.rights.license	Attribution-NonCommercial-NoDerivatives 4.0 Internacional	*
dc.rights.uri	http://creativecommons.org/licenses/by-nc-nd/4.0/	*
dc.subject	Adipose tissue
dc.subject	Mitochondria
dc.subject	OXPHOS
dc.subject	Redox proteomics
dc.subject	Thiol oxidation
dc.subject	Type 2 diabetes
dc.subject	CYTOCHROME-C-OXIDASE
dc.subject	WHITE ADIPOSE-TISSUE
dc.subject	COMPLEX-I
dc.subject	INSULIN-RESISTANCE
dc.subject	QUANTITATIVE PROTEOMICS
dc.subject	TRANSCRIPTION FACTOR
dc.subject	MASS-SPECTROMETRY
dc.subject	REDOX PROTEOMICS
dc.subject	EXPRESSION
dc.subject	DISEASE
dc.title	Differential proteomic and oxidative profiles unveil dysfunctional protein import to adipocyte mitochondria in obesity-associated aging and diabetes
dc.type	journal article
dc.type.hasVersion	VoR
dspace.entity.type	Publication
relation.isAuthorOfPublication	9cc180a8-cdfc-409f-bf52-c4a72421fb37
relation.isAuthorOfPublication	620c7d10-2b0e-45a4-a556-9f84b9d6df64
relation.isAuthorOfPublication	d79f2bf1-6f13-4b5f-9ae3-4c0ea06e9dcb
relation.isAuthorOfPublication	9743763b-919c-4fa9-a53c-57c41be5e0ac
relation.isAuthorOfPublication.latestForDiscovery	9cc180a8-cdfc-409f-bf52-c4a72421fb37