A Gs-coupled purinergic receptor boosts Ca2+ influx and vascular contractility during diabetic hyperglycemia.
Maria Paz PradaArsalan U SyedOlivia R BuonaratiGopireddy R ReddyMatthew A NystoriakDebapriya GhoshSergi SimóDaisuke SatoKent C SasseSean M WardLuis Fernando SantanaYang K XiangJohannes W HellMadeline Nieves-CintrónManuel F NavedoPublished in: eLife (2019)
Elevated glucose increases vascular reactivity by promoting L-type CaV1.2 channel (LTCC) activity by protein kinase A (PKA). Yet, how glucose activates PKA is unknown. We hypothesized that a Gs-coupled P2Y receptor is an upstream activator of PKA mediating LTCC potentiation during diabetic hyperglycemia. Experiments in apyrase-treated cells suggested involvement of a P2Y receptor underlying the glucose effects on LTTCs. Using human tissue, expression for P2Y11, the only Gs-coupled P2Y receptor, was detected in nanometer proximity to CaV1.2 and PKA. FRET-based experiments revealed that the selective P2Y11 agonist NF546 and elevated glucose stimulate cAMP production resulting in enhanced PKA-dependent LTCC activity. These changes were blocked by the selective P2Y11 inhibitor NF340. Comparable results were observed in mouse tissue, suggesting that a P2Y11-like receptor is mediating the glucose response in these cells. These findings established a key role for P2Y11 in regulating PKA-dependent LTCC function and vascular reactivity during diabetic hyperglycemia.
Keyphrases
- blood glucose
- induced apoptosis
- protein kinase
- binding protein
- signaling pathway
- type diabetes
- endothelial cells
- oxidative stress
- wound healing
- poor prognosis
- nuclear factor
- cell cycle arrest
- lps induced
- insulin resistance
- single molecule
- adipose tissue
- cell death
- long non coding rna
- diabetic rats
- skeletal muscle
- smooth muscle