Literature DB >> 30634050

Anti-hypertensive mechanisms of cyclic depsipeptide inhibitor ligands for Gq/11 class G proteins.

Matthew M Meleka1, Alethia J Edwards2, Jingsheng Xia2, Shelby A Dahlen2, Ipsita Mohanty2, Matthew Medcalf3, Shaili Aggarwal2, Kevin D Moeller3, Ole V Mortensen2, Patrick Osei-Owusu4.   

Abstract

Augmented vasoconstriction is a hallmark of hypertension and is mediated partly by hyper-stimulation of G protein couple receptors (GPCRs) and downstream signaling components. Although GPCR blockade is a key component of current anti-hypertensive strategies, whether hypertension is better managed by directly targeting G proteins has not been thoroughly investigated. Here, we tested whether inhibiting Gq/11 proteins in vivo and ex vivo using natural cyclic depsipeptide, FR900359 (FR) from the ornamental plant, Ardisia crenata, and YM-254890 (YM) from Chromobacterium sp. QS3666, or it's synthetic analog, WU-07047 (WU), was sufficient to reverse hypertension in mice. All three inhibitors blocked G protein-dependent vasoconstriction, but to our surprise YM and WU and not FR inhibited K+-induced Ca2+ transients and vasoconstriction of intact vessels. However, each inhibitor blocked whole-cell L-type Ca2+ channel current in vascular smooth muscle cells. Subcutaneous injection of FR or YM (0.3 mg/kg, s.c.) in normotensive and hypertensive mice elicited bradycardia and marked blood pressure decrease, which was more severe and long lasting after the injection of FR relative to YM (FRt1/2 ≅ 12 h vs. YMt1/2 ≅ 4 h). In deoxycorticosterone acetate (DOCA)-salt hypertension mice, chronic injection of FR (0.3 mg/kg, s.c., daily for seven days) reversed hypertension (vehicle SBP: 149 ± 5 vs. FR SBP: 117 ± 7 mmHg), without any effect on heart rate. Our results together support the hypothesis that increased LTCC and Gq/11 activity is involved in the pathogenesis of hypertension, and that dual targeting of both proteins can reverse hypertension and associated cardiovascular disorders.
Copyright © 2019 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  Arginine vasopressin (CID: 644077); Bay K8644 (CID: 2303; Blood pressure; Calcium signaling; Cyclic depsipeptides; Endothelin-1 (CID: 16212950); FR900359 (CID: 14101198); G proteins; G(q/11) inhibitor ligands; L-type calcium channel; Nifedipine (CID: 63011); Phenylephrine (CID: 5284443); U46619 (CID: 5311493); WU-07047 (PMID: 25875152); YM-254890 (CID: 9919454)

Mesh:

Substances:

Year:  2019        PMID: 30634050      PMCID: PMC6417918          DOI: 10.1016/j.phrs.2019.01.012

Source DB:  PubMed          Journal:  Pharmacol Res        ISSN: 1043-6618            Impact factor:   7.658


  7 in total

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Authors:  Jingsheng Xia; Yannong Dou; Yixiao Mei; Frances M Munoz; Ruby Gao; Xinghua Gao; Daling Li; Patrick Osei-Owusu; James Schiffenhaus; Alex Bekker; Yuan-Xiang Tao; Huijuan Hu
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7.  Sensitive LC-MS/MS Method for the Quantification of Macrocyclic Gαq Protein Inhibitors in Biological Samples.

Authors:  Markus Kuschak; Jonathan G Schlegel; Marion Schneider; Stefan Kehraus; Jan H Voss; Alexander Seidinger; Michaela Matthey; Daniela Wenzel; Bernd K Fleischmann; Gabriele M König; Christa E Müller
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  7 in total

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