Invited Review: Arteriolar smooth muscle mechanotransduction: Ca<sup>2+</sup>signaling pathways underlying myogenic reactivity

Hill, Michael A.; Zou, Hui; Potocnik, Simon; Meininger, Gerald A.; Davis, Michael J.

doi:10.1152/jappl.2001.91.2.973

Cited by 249 publications

(247 citation statements)

References 112 publications

Supporting

Mentioning

243

Contrasting

Order By: Relevance

“…Consistent with this notion is evidence that in ovine fetal cerebral arteries norepinephrineinduced contractions occur primarily due to Ca 2ϩ influx, whereas in adults Ca 2ϩ released from intracellular stores also contributes (35). Whether, in addition to depolarization, mechanosensitive elements directly signal pressure-induced voltagedependent Ca 2ϩ channel activation in the newborn cerebrovasculature cannot be concluded from our study (21,36). In newborn cerebral arteries, pressure-induced constriction is Ca 2ϩ dependent.…”

Section: Pressure-induced Constriction Occurs Via Voltage-dependent Csupporting

confidence: 45%

“…Another potential mechanism is that integrins, a family of membrane-spanning glycoproteins, mechanotransduce changes in intravascular pressure to voltagedependent Ca 2ϩ channel activity (21,36). In addition, intravascular pressure may also activate Ca 2ϩ influx via alternative pathways, including store-operated or capacitative Ca 2ϩ entry (45,59).…”

Section: Pressure-induced Constriction Occurs Via Voltage-dependent Cmentioning

confidence: 99%

See 1 more Smart Citation

Ionic mechanisms mediating the myogenic response in newborn porcine cerebral arteries

Ahmed¹,

Waters²,

Leffler³

et al. 2004

American Journal of Physiology-Heart and Circulatory Physiology

View full text Add to dashboard Cite

Ionic mechanisms mediating the myogenic response in newborn porcine cerebral arteries. Am J Physiol Heart Circ Physiol 287: H2061-H2069, 2004. First published July 29, 2004 doi:10.1152/ajpheart.00660.2004.-Mechanisms that underlie autoregulation in the newborn vasculature are unclear. Here we tested the hypothesis that in newborn porcine cerebral arteries intravascular pressure elevates wall tension, leading to an increase in intracellular calcium concentration ([Ca 2ϩ ]i) and a constriction that is opposed by pressure-induced K ϩ channel activation. Incremental step (20 mmHg) elevations in intravascular pressure between 10 and 90 mmHg induced an immediate transient elevation in arterial wall [Ca 2ϩ ]i and a short-lived constriction that was followed by a smaller steady-state [Ca 2ϩ ]i elevation and sustained constriction. Pressures between 10 and 90 mmHg increased steady-state arterial wall [Ca 2ϩ ]i between ϳ142 and 299 nM and myogenic (defined as passive-active) tension between 25 and 437 dyn/cm. The relationship between pressure and myogenic tension was strongly Ca 2ϩ dependent until forced dilation. At low pressure, 60 mM K ϩ induced a steady-state elevation in arterial wall [Ca 2ϩ ]i and a constriction. Nimodipine, a voltage-dependent Ca 2ϩ channel blocker, and removal of extracellular Ca 2ϩ similarly dilated arteries at low or high pressures. 4-Aminopyridine, a voltage-dependent K ϩ (Kv) channel blocker, induced significantly larger constrictions at high pressure, when compared with those at low pressure. Although selective Ca 2ϩ -activated K ϩ (KCa) channel blockers and intracellular Ca 2ϩ release inhibitors induced only small constrictions at low and high pressures, a low concentration of caffeine (1 M), a ryanodine-sensitive Ca 2ϩ release (RyR) channel activator, increased K Ca channel activity and induced dilation. These data suggest that in newborn cerebral arteries, intravascular pressure elevates wall tension, leading to voltage-dependent Ca 2ϩ channel activation, an increase in wall [Ca 2ϩ ]i and Ca 2ϩ -dependent constriction. In addition, pressure strongly activates K v channels that opposes constriction but only weakly activates K Ca channels. wall tension; intravascular pressure; intracellular calcium; voltagedependent potassium channel; calcium-activated potassium channel

show abstract

Section: Pressure-induced Constriction Occurs Via Voltage-dependent Csupporting

confidence: 45%

Section: Pressure-induced Constriction Occurs Via Voltage-dependent Cmentioning

confidence: 99%

Ionic mechanisms mediating the myogenic response in newborn porcine cerebral arteries

Ahmed¹,

Waters²,

Leffler³

et al. 2004

American Journal of Physiology-Heart and Circulatory Physiology

View full text Add to dashboard Cite

show abstract

“…These findings raise an interesting possibility that some Ca v 1.2 channel isoforms are less sensitive to Ca 2ϩ -induced inactivation that controls both the slow inactivation (33) and run-down of the channel (34). Because ␣ 1C,125 and ␣ 1C,127 are able to maintain a more sustained Ca 2ϩ flux, they may have a specific role in VSMC functions that require prolonged Ca 2ϩ influx, such as the maintenance of vascular tone and elasticity of arterial walls (35).…”

Section: Molecular Remodeling Of Cav12␣1 Associated With Atherosclermentioning

confidence: 99%

Atherosclerosis-related molecular alteration of the human Ca _V 1.2 calcium channel α _1C subunit

Tiwari

Zhang

Heller

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Atherosclerosis is an inflammatory process characterized by proliferation and dedifferentiation of vascular smooth muscle cells (VSMC). Cav1.2 calcium channels may have a role in atherosclerosis because they are essential for Ca 2؉ -signal transduction in VSMC. The pore-forming Cav1.2␣1 subunit of the channel is subject to alternative splicing. Here, we investigated whether the Cav1.2␣1 splice variants are affected by atherosclerosis. VSMC were isolated by laser-capture microdissection from frozen sections of adjacent regions of arteries affected and not affected by atherosclerosis. In VSMC from nonatherosclerotic regions, RT-PCR analysis revealed an extended repertoire of Cav1.2␣1 transcripts characterized by the presence of exons 21 and 41A. In VSMC affected by atherosclerosis, expression of the Cav1.2␣1 transcript was reduced and the Cav1.2␣1 splice variants were replaced with the unique exon-22 isoform lacking exon 41A. Molecular remodeling of the Cav1.2␣1 subunits associated with atherosclerosis caused changes in electrophysiological properties of the channels, including the kinetics and voltage-dependence of inactivation, recovery from inactivation, and rundown of the Ca 2؉ current. Consistent with the pathophysiological state of VSMC in atherosclerosis, cell culture data pointed to a potentially important association of the exon-22 isoform of Cav1.2␣1 with proliferation of VSMC. Our findings are consistent with a hypothesis that localized changes in cytokine expression generated by inflammation in atherosclerosis affect alternative splicing of the Cav1.2␣1 gene in the human artery that causes molecular and electrophysiological remodeling of Cav1.2 calcium channels and possibly affects VSMC proliferation.alternative splicing ͉ cell proliferation ͉ vascular smooth muscle cells

show abstract

“…In some small arteries, a different type of contractile Ca 2ϩ signal also may be generated, particularly when levels of receptor activation are high: Ca 2ϩ oscillations that are spatially uniform and synchronized among the different cells (6,23 ] (15, 27) but also, importantly, involves increased activity of certain protein kinases, possible transactivation of extracellular growth factor receptor, activity of the local renin-angiotensin system (RAS), and other enzymes (for review on mechanisms of MT, see Ref. 7). Surprisingly, however, it was not known previously whether ␣ 1 -adrenoceptor-induced Ca 2ϩ signals in such arteries were of the type described above or whether they might be different, due to the markedly different state of the cell once MT has developed.…”

mentioning

confidence: 99%

Ca²⁺ signaling in mouse mesenteric small arteries: myogenic tone and adrenergic vasoconstriction

Zacharia

Zhang²,

Wier³

2007

American Journal of Physiology-Heart and Circulatory Physiology

View full text Add to dashboard Cite

show abstract

Invited Review: Arteriolar smooth muscle mechanotransduction: Ca²⁺signaling pathways underlying myogenic reactivity

Cited by 249 publications

References 112 publications

Ionic mechanisms mediating the myogenic response in newborn porcine cerebral arteries

Ionic mechanisms mediating the myogenic response in newborn porcine cerebral arteries

Atherosclerosis-related molecular alteration of the human Ca _V 1.2 calcium channel α _1C subunit

Ca²⁺ signaling in mouse mesenteric small arteries: myogenic tone and adrenergic vasoconstriction

Contact Info

Product

Resources

About

Invited Review: Arteriolar smooth muscle mechanotransduction: Ca2+signaling pathways underlying myogenic reactivity

Cited by 249 publications

References 112 publications

Ionic mechanisms mediating the myogenic response in newborn porcine cerebral arteries

Ionic mechanisms mediating the myogenic response in newborn porcine cerebral arteries

Atherosclerosis-related molecular alteration of the human Ca V 1.2 calcium channel α 1C subunit

Ca2+ signaling in mouse mesenteric small arteries: myogenic tone and adrenergic vasoconstriction

Contact Info

Product

Resources

About

Invited Review: Arteriolar smooth muscle mechanotransduction: Ca²⁺signaling pathways underlying myogenic reactivity

Atherosclerosis-related molecular alteration of the human Ca _V 1.2 calcium channel α _1C subunit

Ca²⁺ signaling in mouse mesenteric small arteries: myogenic tone and adrenergic vasoconstriction