Investigating the Role of Cannabinoid Type 1 Receptors in Vascular Function and Remodeling in a Hypercholesterolemic Mouse Model with Low-Density Lipoprotein-Cannabinoid Type 1 Receptor Double Knockout Animals

Zsolt Vass; Kinga Shenker-Horváth; Bálint Bányai; Kinga Nóra Vető; Viktória Török; Janka Borbála Gém; György L Nádasy; Kinga Bernadett Kovács; Eszter Mária Horváth; Zoltán Jakus; László Hunyady; Mária Szekeres; Gabriella Dörnyei

doi:10.3390/ijms25179537

Investigating the Role of Cannabinoid Type 1 Receptors in Vascular Function and Remodeling in a Hypercholesterolemic Mouse Model with Low-Density Lipoprotein-Cannabinoid Type 1 Receptor Double Knockout Animals

Int J Mol Sci. 2024 Sep 2;25(17):9537. doi: 10.3390/ijms25179537.

Authors

Affiliations

¹ Department of Morphology and Physiology, Faculty of Health Sciences, Semmelweis University, 17 Vas Street, 1088 Budapest, Hungary.
² Center for Sports Nutrition Science, Hungarian University of Sports Science, 42-48 Alkotás Street, 1123 Budapest, Hungary.
³ Department of Physiology, Faculty of Medicine, Semmelweis University, 37-47 Tűzoltó Street, 1094 Budapest, Hungary.
⁴ Institute of Molecular Life Sciences, HUN-REN Research Centre for Natural Sciences, 2 Magyar Tudósok Körútja, 1117 Budapest, Hungary.

Abstract

Hypercholesterolemia forms the background of several cardiovascular pathologies. LDL receptor-knockout (LDLR-KO) mice kept on a high-fat diet (HFD) develop high cholesterol levels and atherosclerosis (AS). Cannabinoid type 1 receptors (CB₁Rs) induce vasodilation, although their role in cardiovascular pathologies is still controversial. We aimed to reveal the effects of CB₁Rs on vascular function and remodeling in hypercholesterolemic AS-prone LDLR-KO mice. Experiments were performed on a newly established LDLR and CB₁R double-knockout (KO) mouse model, in which KO and wild-type (WT) mice were kept on an HFD or a control diet (CD) for 5 months. The vascular functions of abdominal aorta rings were tested with wire myography. The vasorelaxation effects of acetylcholine (Ach, 1 nM-1 µM) were obtained after phenylephrine precontraction, which was repeated with inhibitors of nitric oxide synthase (NOS) and cyclooxygenase (COX), Nω-nitro-L-arginine (LNA), and indomethacin (INDO), respectively. Blood pressure was measured with the tail-cuff method. Immunostaining of endothelial NOS (eNOS) was carried out. An HFD significantly elevated the cholesterol levels in the LDLR-KO mice more than in the corresponding WT mice (mean values: 1039 ± 162 mg/dL vs. 91 ± 18 mg/dL), and they were not influenced by the presence of the CB₁R gene. However, with the defect of the CB₁R gene, damage to the Ach relaxation ability was moderated. The blood pressure was higher in the LDLR-KO mice compared to their WT counterparts (systolic/diastolic values: 110/84 ± 5.8/6.8 vs. 102/80 ± 3.3/2.5 mmHg), which was significantly elevated with an HFD (118/96 ± 1.9/2 vs. 100/77 ± 3.4/3.1 mmHg, p < 0.05) but attenuated in the CB₁R-KO HFD mice. The expression of eNOS was depressed in the HFD WT mice compared to those on the CD, but it was augmented if CB₁R was knocked out. This newly established double-knockout mouse model provides a tool for studying the involvement of CB₁Rs in the development of hypercholesterolemia and atherosclerosis. Our results indicate that knocking out the CB₁R gene significantly attenuates vascular damage in hypercholesterolemic mice.

Keywords: CB1 receptor; LDL receptor; atherosclerosis; cholesterol; endocannabinoid; high-fat diet; hypercholesterolemia; vascular remodeling.

MeSH terms

Acetylcholine / pharmacology
Animals
Atherosclerosis / etiology
Atherosclerosis / genetics
Atherosclerosis / metabolism
Atherosclerosis / pathology
Diet, High-Fat / adverse effects
Disease Models, Animal*
Hypercholesterolemia* / genetics
Hypercholesterolemia* / metabolism
Hypercholesterolemia* / pathology
Male
Mice
Mice, Inbred C57BL
Mice, Knockout*
Nitric Oxide Synthase Type III / metabolism
Receptor, Cannabinoid, CB1* / genetics
Receptor, Cannabinoid, CB1* / metabolism
Receptors, LDL* / deficiency
Receptors, LDL* / genetics
Receptors, LDL* / metabolism
Vascular Remodeling / drug effects
Vasodilation* / drug effects

Substances

Acetylcholine
Nitric Oxide Synthase Type III
Receptor, Cannabinoid, CB1
Receptors, LDL
CNR1 protein, mouse
Ldlr protein, mouse

Grants and funding

This work was supported by the grants ÚNKP-22-3-II-SE-6 (to Z.V.), ÚNKP-20-1-SE-12 (K.N.V.), and ÚNKP-23-3-II-SE-15 (K.B.K.) of the New National Excellence Program of the Ministry for Culture and Innovation from the Source of National Research and Semmelweis University; by PhD grants PhDKUT0561 (to Z.V.) and PhDKUT0776 (to K.S.-H.) of the Semmelweis University, Faculty of Health Sciences; by the Hungarian National Grants NKFIH K139231 (to L.H.), K139165 (to Z.J.), and K132596 (to Ákos Koller); and by the Hungarian Society of Hypertension, Research Grant 2023 (M.S.). Z.J. is a recipient of the János Bolyai Research Scholarship of the Hungarian Academy of Sciences (BO/00898/22).