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Literature DB >> 29360991

Elevated plasma catecholamines functionally compensate for the reduced myogenic tone in smooth muscle STIM1 knockout mice but with deleterious cardiac effects.

Prahalathan Pichavaram¹, Wen Yin^1,2, Kirk W Evanson¹, Jonathan H Jaggar¹, Salvatore Mancarella¹.

Abstract

Aims: Stromal interaction molecule 1 (STIM1) has emerged as an important player in the regulation of growth and proliferation of smooth muscle cells. Therefore, we hypothesized that STIM1 plays a crucial role in the maintenance of vascular integrity. The objective of this study was to evaluate whether reduced expression of STIM1 could modify the structure and function of the vasculature, leading to changes in blood pressure (BP). Methods and results: Smooth muscle-specific STIM1 knockout (sm-STIM1 KO) in mice resulted in arteries with ∼80% reduced STIM1 protein expression as compared with control mice. Mesenteric vessels exposed to increasing transmural pressure revealed attenuated myogenic reactivity and reduced vasoconstrictor response to phenylephrine in sm-STIM1 KO arteries. BP monitored via telemetry in sm-STIM1 KO and matched controls did not reveal differences. However, heart rate was significantly increased in sm-STIM1 KO mice. Consistent with these findings, plasma catecholamine levels were higher in sm-STIM1 KO than in control mice. Increased sympathetic activity in sm-STIM1 KO mice was unmasked by apha1-adrenergic receptor inhibitor (prazosin) and by treatment with the ganglion-blocking agent, hexamethonium. Both treatments resulted in a greater reduction of BP in sm-STIM1 KO mice. Cytoskeleton of cultured smooth muscle cells was studied by immunocytochemistry using specific antibodies. Staining for actin and vinculin revealed significant alterations in the cytoskeletal architecture of cells isolated from sm-STIM1 KO arteries. Finally, although sm-STIM1 KO mice were protected from Ang II-induced hypertension, such treatment resulted in significant fibrosis and a rapid deterioration of cardiac function. Conclusions: STIM1 deletion in smooth muscle results in attenuated myogenic tone and cytoskeletal defects with detrimental effects on the mechanical properties of arterial tissue. Although BP is maintained by elevated circulating catecholamine, this compensatory stimulation has a deleterious long-term effect on the myocardium.

Entities: Chemical Disease Gene Species

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Year: 2018 PMID： 29360991 PMCID： PMC6279083 DOI： 10.1093/cvr/cvy015

Source DB: PubMed Journal: Cardiovasc Res ISSN： 0008-6363 Impact factor: 10.787

43 in total

1. Orai1 and STIM reconstitute store-operated calcium channel function.

Authors: Jonathan Soboloff; Maria A Spassova; Xiang D Tang; Thamara Hewavitharana; Wen Xu; Donald L Gill
Journal: J Biol Chem Date: 2006-06-09 Impact factor: 5.157

2. Sympathectomy or doxazosin, but not propranolol, blunt myocardial interstitial fibrosis in pressure-overload hypertrophy.

Authors: Stefano Perlini; Giuseppina Palladini; Ivana Ferrero; Rossana Tozzi; Silvia Fallarini; Angelica Facoetti; Rosanna Nano; Francesca Clari; Giuseppe Busca; Roberto Fogari; Alberto U Ferrari
Journal: Hypertension Date: 2005-10-10 Impact factor: 10.190

3. Increased activation of stromal interaction molecule-1/Orai-1 in aorta from hypertensive rats: a novel insight into vascular dysfunction.

Authors: Fernanda R C Giachini; Chin-Wei Chiao; Fernando S Carneiro; Victor V Lima; Zidonia N Carneiro; Anne M Dorrance; Rita C Tostes; R Clinton Webb
Journal: Hypertension Date: 2008-12-15 Impact factor: 10.190

4. Effect of acute administration of prazosin on blood pressure, heart rate and plasma renin level in the conscious normotensive rat.

Authors: J Atkinson; P Luthi; M Sonnay; N Boillat
Journal: Clin Exp Pharmacol Physiol Date: 1986-07 Impact factor: 2.557

5. RNA interference targeting STIM1 suppresses vascular smooth muscle cell proliferation and neointima formation in the rat.

Authors: Fleur C Aubart; Yassine Sassi; Alain Coulombe; Nathalie Mougenot; Cédric Vrignaud; Pascal Leprince; Philippe Lechat; Anne-Marie Lompré; Jean-Sébastien Hulot
Journal: Mol Ther Date: 2008-12-23 Impact factor: 11.454

6. Evidence for STIM1- and Orai1-dependent store-operated calcium influx through ICRAC in vascular smooth muscle cells: role in proliferation and migration.

Authors: Marie Potier; José C Gonzalez; Rajender K Motiani; Iskandar F Abdullaev; Jonathan M Bisaillon; Harold A Singer; Mohamed Trebak
Journal: FASEB J Date: 2009-04-13 Impact factor: 5.191

7. Sympathetic augmentation in hypertension: role of nerve firing, norepinephrine reuptake, and Angiotensin neuromodulation.

Authors: Markus P Schlaich; Elisabeth Lambert; David M Kaye; Zygmunt Krozowski; Duncan J Campbell; Gavin Lambert; Jacqui Hastings; Anuradha Aggarwal; Murray D Esler
Journal: Hypertension Date: 2003-11-10 Impact factor: 10.190

8. Essential role for STIM1/Orai1-mediated calcium influx in PDGF-induced smooth muscle migration.

Authors: Jonathan M Bisaillon; Rajender K Motiani; José C Gonzalez-Cobos; Marie Potier; Katharine E Halligan; Wael F Alzawahra; Margarida Barroso; Harold A Singer; David Jourd'heuil; Mohamed Trebak
Journal: Am J Physiol Cell Physiol Date: 2010-01-27 Impact factor: 4.249

9. STIM1, an essential and conserved component of store-operated Ca2+ channel function.

Authors: Jack Roos; Paul J DiGregorio; Andriy V Yeromin; Kari Ohlsen; Maria Lioudyno; Shenyuan Zhang; Olga Safrina; J Ashot Kozak; Steven L Wagner; Michael D Cahalan; Gönül Veliçelebi; Kenneth A Stauderman
Journal: J Cell Biol Date: 2005-05-02 Impact factor: 10.539

Elevated plasma catecholamines functionally compensate for the reduced myogenic tone in smooth muscle STIM1 knockout mice but with deleterious cardiac effects.

1. Orai1 and STIM reconstitute store-operated calcium channel function.

2. Sympathectomy or doxazosin, but not propranolol, blunt myocardial interstitial fibrosis in pressure-overload hypertrophy.

3. Increased activation of stromal interaction molecule-1/Orai-1 in aorta from hypertensive rats: a novel insight into vascular dysfunction.

4. Effect of acute administration of prazosin on blood pressure, heart rate and plasma renin level in the conscious normotensive rat.

5. RNA interference targeting STIM1 suppresses vascular smooth muscle cell proliferation and neointima formation in the rat.

6. Evidence for STIM1- and Orai1-dependent store-operated calcium influx through ICRAC in vascular smooth muscle cells: role in proliferation and migration.

7. Sympathetic augmentation in hypertension: role of nerve firing, norepinephrine reuptake, and Angiotensin neuromodulation.

8. Essential role for STIM1/Orai1-mediated calcium influx in PDGF-induced smooth muscle migration.

9. STIM1, an essential and conserved component of store-operated Ca2+ channel function.

10. STIM1-dependent Ca(2+) microdomains are required for myofilament remodeling and signaling in the heart.

Review 1. STIM and Orai Mediated Regulation of Calcium Signaling in Age-Related Diseases.

2. STIM1-dependent peripheral coupling governs the contractility of vascular smooth muscle cells.

3. Rad-GTPase contributes to heart rate via L-type calcium channel regulation.

4. Mapping the Proximity Interaction Network of STIM1 Reveals New Mechanisms of Cytoskeletal Regulation.