Oxidative stress-dependent contribution of HMGB1 to the interplay between apoptosis and autophagy in diabetic rat liver

Petrović, Anja; Bogojević, Desanka; Korać, Aleksandra; Golić, Igor; Jovanović-Stojanov, Sofija; Martinović, Vesna; Ivanović-Matić, Svetlana; Stevanović, Jelena; Poznanović, Goran; Grigorov, Ilijana

Please use this identifier to cite or link to this item: https://biore.bio.bg.ac.rs/handle/123456789/272

Title:	Oxidative stress-dependent contribution of HMGB1 to the interplay between apoptosis and autophagy in diabetic rat liver
Authors:	Petrović, Anja Bogojević, Desanka Korać, Aleksandra Golić, Igor Jovanović-Stojanov, Sofija Martinović, Vesna Ivanović-Matić, Svetlana Stevanović, Jelena Poznanović, Goran Grigorov, Ilijana
Keywords:	Apoptosis/autophagy interplay;Diabetes;HMGB1;Liver damage;Melatonin;Oxidative stress
Issue Date:	1-Nov-2017
Rank:	M22
Project:	Signaling molecules in diabetes: search for potential targets in intrinsic pathways for prediction and intervention in diabetes
Journal:	Journal of Physiology and Biochemistry
Abstract:	© 2017, University of Navarra. The progression of oxidative stress, resulting cell damage, and cell death underlies the etiology of liver damage/dysfunction as a complication of diabetes. High-mobility group box 1 (HMGB1) protein, a chromatin-binding nuclear protein and damage-associated molecular pattern molecule, is integral to oxidative stress and signaling pathways regulating cell death and ce... © 2017, University of Navarra. The progression of oxidative stress, resulting cell damage, and cell death underlies the etiology of liver damage/dysfunction as a complication of diabetes. High-mobility group box 1 (HMGB1) protein, a chromatin-binding nuclear protein and damage-associated molecular pattern molecule, is integral to oxidative stress and signaling pathways regulating cell death and cell survival. We previously found that in streptozotocin (STZ)-induced diabetic rats, reduction of oxidative stress after melatonin administration lowered necrotic cell death and increased expression of HMGB1 and hepatocellular damage. In the present study, we examined whether alleviation of diabetes-attendant oxidative stress and ensuing change in HMGB1 expression influence the dynamic equilibrium between apoptosis/autophagy and liver damage. We observed that elevated HMGB1 protein levels in diabetic rat liver accompanied increased interactions of HMGB1 with TLR4 and RAGE, and activation of the intrinsic apoptotic pathway and Beclin 1-dependent autophagy. The absence of p62 degradation in diabetic rat liver pointed to defective autophagy which was responsible for lower autophagosome/autophagolysosome formation and an increased apoptosis/autophagy ratio. Compared to diabetic rats, in melatonin-treated diabetic rats, the structure of liver cells was preserved, HMGB1/TLR4 interaction and downstream apoptotic signaling were significantly reduced, HMGB1/Beclin 1 colocalization and interactions were augmented and Beclin 1-mediated autophagy, mithophagy in particular, were increased. We concluded that in mild oxidative stress, HMGB1 is cytoprotective, whereas in intense oxidative stress, HMGB1 actions promote cell death and liver damage. Since reduced HMGB1 binds to RAGE but not to TLR4, redox modification of HMGB1 as a mechanism regulating the cross-talk between apoptosis and autophagy in diabetes is discussed.
URI:	https://biore.bio.bg.ac.rs/handle/123456789/272
ISSN:	1138-7548
DOI:	10.1007/s13105-017-0574-0
Appears in Collections:	Journal Article

Show full item record

SCOPUS^TM
Citations

50

checked on Mar 27, 2025

Page view(s)

7

checked on Apr 2, 2025

Google Scholar^TM

Check

SCOPUS^TM
Citations

Page view(s)

Google Scholar^TM

Altmetric

Altmetric

SCOPUSTM Citations

Page view(s)

Google ScholarTM

Altmetric

Altmetric

SCOPUS^TM
Citations

Google Scholar^TM