Aryl Hydrocarbon Receptor Nuclear Translocator in Vascular Smooth Muscle Cells Is Required for Optimal Peripheral Perfusion Recovery

Borton, Anna H; Benson, Bryan L.; Neilson, Lee E.; Saunders, Ashley B.; Alaiti, Mohamad Amer; Huang, Alex Yee-Chen; Jain, Mukesh K.; Proweller, Aaron; Ramírez-Bergeron, Diana L.

doi:10.1161/jaha.118.009205

Cited by 1 publication

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References 73 publications

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“…28 Although our data did not demonstrate any variation in HIF-1α and FGF2 mRNA expression, previous studies indicated that the loss of hypoxic signals in vascular SMC impaired the ability of mice to recover from ischemia following femoral artery ligation. Borton et al 29 have reported that the deletion of the HIF-β subunit in SMC altered SMC proliferation and migration as well as compromised limb reperfusion. Others have shown that FGF2 is an important element in the arteriogenic response of SMC.…”

Section: Discussionmentioning

confidence: 99%

Diabetes Impaired Ischemia-Induced PDGF (Platelet-Derived Growth Factor) Signaling Actions and Vessel Formation Through the Activation of Scr Homology 2-Containing Phosphatase-1

Mercier

Brazeau

Lamoureux

et al. 2021

ATVB

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Objective: Critical limb ischemia is a major complication of diabetes characterized by insufficient collateral vessel development and proper growth factor signaling unresponsiveness. Although mainly deactivated by hypoxia, phosphatases are important players in the deregulation of proangiogenetic pathways. Previously, SHP-1 (Scr homology 2-containing phosphatase-1) was found to be associated with the downregulation of growth factor actions in the diabetic muscle. Thus, we aimed to gain further understanding of the impact of SHP-1 on smooth muscle cell (SMC) function under hypoxic and diabetic conditions. Approach and Results: Despite being inactivated under hypoxic conditions, high glucose level exposure sustained SHP-1 phosphatase activity in SMC and increased its interaction with PDGFR (platelet-derived growth factor receptor)-β, thus reducing PDGF proangiogenic actions. Overexpression of an inactive form of SHP-1 fully restored PDGF-induced proliferation, migration, and signaling pathways in SMC exposed to high glucose and hypoxia. Nondiabetic and diabetic mice with deletion of SHP-1 specifically in SMC were generated. Ligation of the femoral artery was performed, and blood flow was measured for 4 weeks. Blood flow reperfusion, vascular density and maturation, and limb survival were all improved while vascular apoptosis was attenuated in diabetic SMC-specific SHP-1 null mice as compared to diabetic mice. Conclusions: Diabetes and high glucose level exposure maintained SHP-1 activity preventing hypoxia-induced PDGF actions in SMC. Specific deletion of SHP-1 in SMC partially restored blood flow reperfusion in the diabetic ischemic limb. Therefore, local modulation of SHP-1 activity in SMC could represent a potential therapeutic avenue to improve the proangiogenic properties of SMC under ischemia and diabetes.

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Section: Discussionmentioning

confidence: 99%