Glycyrrhizic Acid Inhibits High-Mobility Group Box-1 and Homocysteine-Induced Vascular Dysfunction

Laura Kate Gadanec; Ulf Andersson; Vasso Apostolopoulos; Anthony Zulli

doi:10.3390/nu15143186

Glycyrrhizic Acid Inhibits High-Mobility Group Box-1 and Homocysteine-Induced Vascular Dysfunction

Nutrients. 2023 Jul 18;15(14):3186. doi: 10.3390/nu15143186.

Authors

Laura Kate Gadanec¹, Ulf Andersson², Vasso Apostolopoulos^{1

3}, Anthony Zulli¹

Affiliations

¹ Institute of Health and Sport, Victoria University, Melbourne, VIC 3030, Australia.
² Department of Women's and Children's Health, Karolinska Institute, 17177 Stockholm, Sweden.
³ Immunology Program, Australian Institute for Musculoskeletal Science, Melbourne, VIC 3021, Australia.

Abstract

Hyperhomocysteinemia (HHcy) worsens cardiovascular outcomes by impairing vascular function and promoting chronic inflammation via release of danger-associated molecular patterns, such as high-mobility group box-1 (HMGB-1). Elevated levels of HMGB-1 have recently been reported in patients with HHcy. Therefore, targeting HMGB-1 may be a potential therapy to improve HHcy-induced cardiovascular pathologies. This study aimed to further elucidate HMGB-1's role during acute HHcy and HHcy-induced atherogenesis and to determine if inhibiting HMGB-1 with glycyrrhizic acid (Glyz) improved vascular function. Male New Zealand White rabbits (n = 25) were placed on either a standard control chow (CD; n = 15) or atherogenic diet (AD; n = 10) for 4 weeks. Rabbit serum and Krebs taken from organ bath studies were collected to quantify HMGB-1 levels. Isometric tension analysis was performed on abdominal aorta (AA) rings from CD and AD rabbits. Rings were incubated with homocysteine (Hcy) [3 mM] for 60 min to induce acute HHcy or rhHMGB-1 [100 nM]. Vascular function was assessed by relaxation to cumulative doses of acetylcholine. Markers of vascular dysfunction and inflammation were quantified in the endothelium, media, and adventitia of AA rings. HMGB-1 was significantly upregulated in serum (p < 0.0001) and Krebs (p < 0.0001) after Hcy exposure or an AD. Incubation with Hcy (p < 0.0001) or rhHMGB-1 (p < 0.0001) and an AD (p < 0.0001) significantly reduced relaxation to acetylcholine, which was markedly improved by Glyz. HMGB-1 expression was elevated (p < 0.0001) after Hcy exposure and AD (p < 0.0001) and was normalized after Glyz treatment. Moreover, markers of vascular function, cell stress and inflammation were also reduced after Glyz. These results demonstrate that HMGB-1 has a central role during HHcy-induced vascular dysfunction and inhibiting it with Glyz could be a potential treatment option for cardiovascular diseases.

Keywords: atherogenesis; cardiovascular diseases; glycyrrhizic acid; high-mobility group box-1; homocysteine; hyperhomocysteinemia.

MeSH terms

Acetylcholine / pharmacology
Animals
Atherosclerosis*
Glycyrrhizic Acid / pharmacology
HMGB Proteins
Homocysteine
Hyperhomocysteinemia* / complications
Hyperhomocysteinemia* / drug therapy
Inflammation / metabolism
Male
Rabbits

Substances

Acetylcholine
Glycyrrhizic Acid
HMGB Proteins
Homocysteine

Grants and funding

This research received no external funding.