AKAP150 Is Required for Stuttering Persistent Ca 2+ Sparklets and Angiotensin II–Induced Hypertension

Hypertension is a perplexing multiorgan disease involving renal primary pathology and enhanced angiotensin II vascular reactivity. Here, we report that a novel form of a local Ca 2+ signaling in arterial smooth muscle is linked to the development of angiotensin II–induced hypertension. Long openings and reopenings of L-type Ca 2+ channels in arterial myocytes produce stuttering persistent Ca 2+ sparklets that increase Ca 2+ influx and vascular tone. These stuttering persistent Ca 2+ sparklets arise from the molecular interactions between the L-type Ca 2+ channel and protein kinase Cα at only a few subsarcolemmal regions in resistance arteries. We have identified AKAP150 as the key protein, which targets protein kinase Cα to the L-type Ca 2+ channels and thereby enables its regulatory function. Accordingly, AKAP150 knockout mice (AKAP150 −/− ) were found to lack persistent Ca 2+ sparklets and have lower arterial wall intracellular calcium ([Ca 2+ ] i ) and decreased myogenic tone. Furthermore, AKAP150 −/− mice were hypotensive and did not develop angiotensin II–induced hypertension. We conclude that local control of L-type Ca 2+ channel function is regulated by AKAP150-targeted protein kinase Cα signaling, which controls stuttering persistent Ca 2+ influx, vascular tone, and blood pressure under physiological conditions and underlies angiotensin II–dependent hypertension.