The cardioprotective effect persisting during recovery from cold acclimation is mediated by the beta(2)-adrenoceptor pathway and Akt activation

Tibenská, V.; Marvanová, A.; Elsnicová, B.; Hejnová, L.; Vebr, P.; Novotný, J.; Kolář, František; Nováková, Olga; Žurmanová, J.M.

doi:https://dx.doi.org/10.1152/japplphysiol.00756.2020

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The cardioprotective effect persisting during recovery from cold acclimation is mediated by the beta(2)-adrenoceptor pathway and Akt activation

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SYSNO ASEP	0542131
Document Type	J - Journal Article
R&D Document Type	Journal Article
Subsidiary J	Článek ve WOS
Title	The cardioprotective effect persisting during recovery from cold acclimation is mediated by the beta(2)-adrenoceptor pathway and Akt activation
Author(s)	Tibenská, V. (CZ) Marvanová, A. (CZ) Elsnicová, B. (CZ) Hejnová, L. (CZ) Vebr, P. (CZ) Novotný, J. (CZ) Kolář, František (FGU-C)_{RID, ORCID, SAI} Nováková, Olga (FGU-C) Žurmanová, J.M. (CZ)
Source Title	Journal of Applied Physiology. - : American Physiological Society - ISSN 8750-7587 Roč. 130, č. 3 (2021), s. 746-755
Number of pages	10 s.
Language	eng - English
Country	US - United States
Keywords	beta2-adrenergic signaling ; cardioprotection ; cold acclimation ; glycogen synthase kinase-3beta ; protein kinase B/Akt
Subject RIV	ED - Physiology
OECD category	Physiology (including cytology)
R&D Projects	GA17-07748S GA ČR - Czech Science Foundation (CSF)
Method of publishing	Open access
Institutional support	FGU-C - RVO:67985823
UT WOS	000630429900019
EID SCOPUS	85103227946
DOI	https://doi.org/10.1152/japplphysiol.00756.2020
Annotation	The infarct size-limiting effect elicited by cold acclimation (CA) is accompanied by increased mitochondrial resistance and unaltered beta(1)-adrenergic receptor (AR) signaling persisting for 2 wk at room temperature. As the mechanism of CA-elicited cardioprotection is not fully understood, we examined the role of the salvage beta(2)-AR/G(i)/Akt pathway. Male Wistar rats were exposed to CA (8 degrees C, 5 wk), whereas the recovery group (CAR) was kept at 24 degrees C for additional 2 wk. We show that the total number of myocardial beta-ARs in the left ventricular myocardium did not change after CA but decreased after CAR. We confirmed the infarct size-limiting effect in both CA and CAR groups. Acute administration of beta(2)-AR inhibitor ICI-118551 abolished the protective effect in the CAR group but had no effect in the control and CA groups. The inhibitory G(i)alpha(1/2) and G(i)alpha(3) proteins increased in the membrane fraction of the CAR group, and the phospho-Akt (Ser(473))-to-Akt ratio also increased. Expression, phosphorylation, and mitochondrial location of the Akt target glycogen synthase kinase (GSK-3 beta) were affected neither by CA nor by CAR. However, GSK-3 beta translocated from the Z-disk to the H-zone after CA, and acquired its original location after CAR. Our data indicate that the cardioprotection observed after CAR is mediated by the beta 2-AR/G(i) pathway and Akt activation. Further studies are needed to unravel downstream targets of the central regulators of the CA process and the downstream targets of the Akt protein after CAR.
Workplace	Institute of Physiology
Contact	Lucie Trajhanová, lucie.trajhanova@fgu.cas.cz, Tel.: 241 062 400
Year of Publishing	2022
Electronic address	https://doi.org/10.1152/japplphysiol.00756.2020

Number of the records: 1