4.7 Article

Acid-sensing ion channels 1a (ASIC1a) inhibit neuromuscular transmission in female mice

Journal

AMERICAN JOURNAL OF PHYSIOLOGY-CELL PHYSIOLOGY
Volume 306, Issue 4, Pages C396-C406

Publisher

AMER PHYSIOLOGICAL SOC
DOI: 10.1152/ajpcell.00301.2013

Keywords

wire hanging; acid-sensing ion channels; motor nerve transmission; presynaptic modulation; extracellular acidosis

Funding

  1. FONCYT-BID [1728 OC. AR. PICT 2008-2019, 1728 OC. AR. PICT 2012-1769, 1728 OC. AR. PICT, 2667]
  2. Wellcome Trust [068941/Z/02/Z]
  3. UBACYT [20020100100427]
  4. CONICET PIP [2012-2014 11220110100768]
  5. VA Merit Review

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Acid-sensing ion channels (ASIC) open in response to extracellular acidosis. ASIC1a, a particular subtype of these channels, has been described to have a postsynaptic distribution in the brain, being involved not only in ischemia and epilepsy, but also in fear and psychiatric pathologies. High-frequency stimulation of skeletal motor nerve terminals (MNTs) can induce presynaptic pH changes in combination with an acidification of the synaptic cleft, known to contribute to muscle fatigue. Here, we studied the role of ASIC1a channels on neuromuscular transmission. We combined a behavioral wire hanging test with electrophysiology, pharmacological, and immunofluorescence techniques to compare wild-type and ASIC1a lacking mice (ASIC1a (-/-) knockout). Our results showed that 1) ASIC1a (-/-) female mice were weaker than wild type, presenting shorter times during the wire hanging test; 2) spontaneous neurotransmitter release was reduced by ASIC1a activation, suggesting a presynaptic location of these channels at individual MNTs; 3) ASIC1a-mediated effects were emulated by extracellular local application of acid saline solutions (pH = 6.0; HEPES/MES-based solution); and 4) immunofluorescence techniques revealed the presence of ASIC1a antigens on MNTs. These results suggest that ASIC1a channels might be involved in controlling neuromuscular transmission, muscle contraction and fatigue in female mice.

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