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Endothelium-dependent vasodilation in myogenically active mouse skeletal muscle arterioles: Role of EDH and K+ channels

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posted on 2024-11-01, 05:50 authored by Simon Potocnik, Iain McSherry, Hong Ding, T Murphy, Neelakumari Kotecha, Kim Dora, Kathryn Yuill, Chris Triggle, Michael Hill
As smooth muscle cell (SMC) membrane potential (Em) is critical for vascular responsiveness, and arteriolar SMCs are depolarized at physiological intraluminal pressures, we hypothesized that myogenic tone impacts on dilation mediated by endothelium-derived hyperpolarization (EDH). Studies were performed on cannulated mouse cremaster arterioles [diameter, 33 ± 2 ?m (n = 23) at 60 mmHg; SMC Em -34.6 ± 1.2 mV (n = 7)]. Myogenic activity was assessed as tone developed in response to intraluminal pressure. Functional observations were related to mRNA, protein expression, and anatomy. Acetylcholine concentration-response curves showed a modest shift following indomethacin (10 ?M) and L-NAME (100 ?M), although maximal vasodilation was achieved. Residual dilation was removed by apamin (1 ?M) in combination with TRAM-34 (1 ?M) or charybotoxin (0.1 ?M), indicating the requirement of small (S) and intermediate (I) calcium-activated potassium channels (KCa). Charybdotoxin, but not TRAM-34, caused vasoconstriction, presumably through the inhibition of SMC BKCa. Expression of SK3 and IK1 was confirmed by immunohistochemistry and polymerase chain reaction, while myoendothelial junctions were common, suggesting a high degree of cell coupling. Also consistent with a role for endothelial KCa channels, acetylcholine increased endothelium [Ca2+]i. Apamin and TRAM-34 similarly blocked EDH-mediated dilation at intraluminal pressures of 30 and 90 mmHg, suggesting that in mouse arterioles, SKCa- and IKCa- mediated mechanisms predominate and operate independently of physiological levels of myogenic activation.

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Related Materials

  1. 1.
    DOI - Is published in 10.1080/10739680902804042
  2. 2.
    ISSN - Is published in 10739688

Journal

Microcirculation

Volume

16

Issue

5

Start page

377

End page

390

Total pages

14

Publisher

Informa Healthcare

Place published

United Kingdom

Language

English

Former Identifier

2006011862

Esploro creation date

2020-06-22

Fedora creation date

2010-11-19

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