In mice, 3,3-dimethyl-1-butanol (DMB) supplementation initiated at midlife prevented age-related endothelial dysfunction and attenuated in vivo aortic stiffening by ~70%.
Does 3,3-dimethyl-1-butanol supplementation prevent age-related vascular dysfunction in mice?
Long-term DMB supplementation initiated at midlife prevents age-related endothelial dysfunction and attenuates aortic stiffening in mice, suggesting potential for reducing cardiovascular risk with aging.
Vascular dysfunction: develops progressively with ageing; increases the risk of cardiovascular diseases (CVD); and is characterized by endothelial dysfunction and arterial stiffening, which are primarily mediated by superoxide-driven oxidative stress and consequently reduced nitric oxide (NO) bioavailability and arterial structural changes. Interventions initiated before vascular dysfunction manifests may have more promise for reducing CVD risk than interventions targeting established dysfunction. Gut microbiome-derived trimethylamine N-oxide (TMAO) induces vascular dysfunction, is associated with higher CV risk, and can be suppressed by 3,3-dimethyl-1-butanol (DMB). We investigated whether DMB supplementation could prevent age-related vascular dysfunction in C57BL/6N mice when initiated prior to development of dysfunction. Mice received drinking water with 1% DMB or normal drinking water (control) from midlife (18 months) until being studied at 21, 24 or 27 months of age, and were compared to young adult (5 month) mice. Endothelial function carotid artery endothelium-dependent dilatation (EDD) to acetylcholine; pressure myography progressively declined with age in control mice, which was fully prevented by DMB via higher NO-mediated EDD and lower superoxide-related suppression of EDD (normalization of EDD with the superoxide dismutase mimetic TEMPOL). In vivo aortic stiffness (pulse wave velocity) increased progressively with age in controls, but DMB attenuated stiffening by ∼ 70%, probably due to preservation of endothelial function, as DMB did not affect aortic intrinsic mechanical (structural) stiffness (stress-strain testing) nor adventitial abundance of the arterial structural protein collagen. Our findings indicate that long-term DMB supplementation prevents/attenuates age-related vascular dysfunction, and therefore has potential for translation to humans for reducing CV risk with ageing. KEY POINTS: Vascular dysfunction, characterized by endothelial dysfunction and arterial stiffening, develops progressively with ageing and increases the risk of cardiovascular diseases (CVD). Interventions aimed at preventing the development of CV risk factors have more potential for preventing CVD relative to those aimed at reversing established dysfunction. The gut microbiome-derived metabolite trimethylamine N-oxide (TMAO) induces vascular dysfunction, is associated with higher CV risk and can be suppressed by supplementation with 3,3-dimethyl-1-butanol (DMB). In mice, DMB prevented the development of endothelial dysfunction and delayed and attenuated in vivo arterial stiffening with ageing when supplementation was initiated in midlife, prior to the development of dysfunction. DMB supplementation or other TMAO-suppressing interventions have potential for translation to humans for reducing CV risk with ageing.
Casso et al. (금요일)은 노화 관련 혈관 기능 장애에 대한 연구를 수행했습니다. 3,3-디메틸-1-부탄올(DMB)과 일반 식수를 비교하여 내피 기능(경동맥 내피 의존성 이완)과 생체 내 대동맥 경직성(맥파 속도)을 평가했습니다. 생쥐에서 중년기에 시작된 3,3-디메틸-1-부탄올(DMB) 보충은 노화 관련 내피 기능 장애를 예방하고 생체 내 대동맥 경직을 약 70% 완화했습니다.
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