Mutation of the 5'-untranslated region stem-loop mRNA structure reduces type i collagen deposition and arterial stiffness in male obese mice

Francisco I., Ramirez-Perez, Makenzie L., Woodford, Mariana, Morales-Quinones, Zachary I., Grunewald, Francisco J., Cabral-Amador, Tadashi, Yoshida, David A., Brenner, Camila, Manrique-Acevedo, Luis A., Martinez-Lemus, Bysani, Chandrasekar, Jaume, Padilla

American Journal of Physiology - Heart and Circulatory Physiology |

Arterial stiffening, a characteristic feature of obesity and type 2 diabetes, contributes to the development and progression of cardiovascular diseases (CVD). Currently, no effective prophylaxis or therapeutics is available to prevent or treat arterial stiffening. A better understanding of the molecular mechanisms underlying arterial stiffening is vital to identify newer targets and strategies to reduce CVD burden. A major contributor to arterial stiffening is increased collagen deposition. In the 50-untranslated regions of mRNAs encoding for type I collagen, an evolutionally conserved stem-loop (SL) structure plays an essential role in its stability and post-transcriptional regulation. Here, we show that feeding a high-fat/high-sucrose (HFHS) diet for 28 wk increases adiposity, insulin resistance, and blood pressure in male wild-type littermates. Moreover, arterial stiffness, assessed in vivo via aortic pulse wave velocity, and ex vivo using atomic force microscopy in aortic explants or pressure myography in isolated femoral and mesenteric arteries, was also increased in those mice. Notably, all these indices of arterial stiffness, along with collagen type I levels in the vasculature, were reduced in HFHS-fed mice harboring a mutation in the 50SL structure, relative to wild-type littermates. This protective vascular phenotype in 50SL-mutant mice did not associate with a reduction in insulin resistance or blood pressure. These findings implicate the 50SL structure as a putative therapeutic target to prevent or reverse arterial stiffening and CVD associated with obesity and type 2 diabetes. NEW & NOTEWORTHY In the 5'-untranslated (UTR) regions of mRNAs encoding for type I collagen, an evolutionally conserved SL structure plays an essential role in its stability and posttranscriptional regulation. We demonstrate that a mutation of the SL mRNA structure in the 5'-UTR decreases collagen type I deposition and arterial stiffness in obese mice. Targeting this evolutionarily conserved SL structure may hold promise in the management of arterial stiffening and CVD associated with obesity and type 2 diabetes.