Aortic pathology from protein kinase G activation is prevented by an antioxidant vitamin B12 analog.
Gerburg K SchwaerzerHema KalyanaramanDarren E CasteelNancy D DaltonYusu GuSeunghoe LeeShunhui ZhuangNisreen WahwahJan M SchillingHemal H PatelQian ZhangAyako MakinoDianna M MilewiczKirk L PetersonGerry R BossRenate B PilzPublished in: Nature communications (2019)
People heterozygous for an activating mutation in protein kinase G1 (PRKG1, p.Arg177Gln) develop thoracic aortic aneurysms and dissections (TAAD) as young adults. Here we report that mice heterozygous for the mutation have a three-fold increase in basal protein kinase G (PKG) activity, and develop age-dependent aortic dilation. Prkg1R177Q/+ aortas show increased smooth muscle cell apoptosis, elastin fiber breaks, and oxidative stress compared to aortas from wild type littermates. Transverse aortic constriction (TAC)-to increase wall stress in the ascending aorta-induces severe aortic pathology and mortality from aortic rupture in young mutant mice. The free radical-neutralizing vitamin B12-analog cobinamide completely prevents age-related aortic wall degeneration, and the unrelated anti-oxidant N-acetylcysteine ameliorates TAC-induced pathology. Thus, increased basal PKG activity induces oxidative stress in the aorta, raising concern about the widespread clinical use of PKG-activating drugs. Cobinamide could be a treatment for aortic aneurysms where oxidative stress contributes to the disease, including Marfan syndrome.
Keyphrases
- aortic valve
- aortic dissection
- pulmonary artery
- oxidative stress
- left ventricular
- protein kinase
- wild type
- young adults
- coronary artery
- diabetic rats
- pulmonary hypertension
- early onset
- pulmonary arterial hypertension
- heart failure
- ischemia reperfusion injury
- spinal cord
- metabolic syndrome
- adipose tissue
- cell proliferation
- cardiovascular disease
- mouse model
- induced apoptosis
- coronary artery disease
- insulin resistance
- neuropathic pain