L-type Ca <sup>2+</sup> channel blockers promote vascular remodeling through activation of STIM proteins
Martin Johnson, Aparna Gudlur, Xuexin Zhang, Ping Xin, Scott M. Emrich, Ryan E. Yoast, Raphaël Courjaret, Robert M. Nwokonko, Wei Li, Nadine Hempel, Khaled Machaca, Donald L. Gill, Patrick G. Hogan, Mohamed Trebak
Abstract
Voltage-gated L-type Ca 2+ channel (Ca v 1.2) blockers (LCCBs) are major drugs for treating hypertension, the preeminent risk factor for heart failure. Vascular smooth muscle cell (VSMC) remodeling is a pathological hallmark of chronic hypertension. VSMC remodeling is characterized by molecular rewiring of the cellular Ca 2+ signaling machinery, including down-regulation of Ca v 1.2 channels and up-regulation of the endoplasmic reticulum (ER) stromal-interacting molecule (STIM) Ca 2+ sensor proteins and the plasma membrane ORAI Ca 2+ channels. STIM/ORAI proteins mediate store-operated Ca 2+ entry (SOCE) and drive fibro-proliferative gene programs during cardiovascular remodeling. SOCE is activated by agonists that induce depletion of ER Ca 2+ , causing STIM to activate ORAI. Here, we show that the three major classes of LCCBs activate STIM/ORAI-mediated Ca 2+ entry in VSMCs. LCCBs act on the STIM N terminus to cause STIM relocalization to junctions and subsequent ORAI activation in a Ca v 1.2-independent and store depletion-independent manner. LCCB-induced promotion of VSMC remodeling requires STIM1, which is up-regulated in VSMCs from hypertensive rats. Epidemiology showed that LCCBs are more associated with heart failure than other antihypertensive drugs in patients. Our findings unravel a mechanism of LCCBs action on Ca 2+ signaling and demonstrate that LCCBs promote vascular remodeling through STIM-mediated activation of ORAI. Our data indicate caution against the use of LCCBs in elderly patients or patients with advanced hypertension and/or onset of cardiovascular remodeling, where levels of STIM and ORAI are elevated.