Acute inhibition of acid sensing ion channel 1a after spinal cord injury selectively affects excitatory synaptic transmission, but not intrinsic membrane properties, in deep dorsal horn interneurons

Following a spinal cord injury (SCI), secondary damage mechanisms are triggered that cause inflammation and cell death. A key component of this secondary damage is a reduction in local blood flow that initiates a well-characterised ischemic cascade. Downstream hypoxia and acidosis activate acid sens...

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Published in:PloS one 2023-11, Vol.18 (11), p.e0289053-e0289053
Main Authors: Foster, Victoria S, Saez, Natalie, King, Glenn F, Rank, Michelle M
Format: Article
Language:English
Subjects:
Acidification
Acidosis
Analysis
Animals
Blood flow
Brain research
Care and treatment
Cell death
Damage
Diagnosis
Dorsal horn
Electrophysiology
Excitatory postsynaptic potentials
Experiments
Fentanyl
Hypoxia
Interneurons
Ion channels
Ischemia
Kinases
Kinetics
Membranes
Motor neurons
Neurons
Paralysis
Receptor channels
Recovery of function
Spinal cord injuries
Surgery
Synaptic transmission
Venom
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Saez, Natalie
King, Glenn F
Rank, Michelle M
description Following a spinal cord injury (SCI), secondary damage mechanisms are triggered that cause inflammation and cell death. A key component of this secondary damage is a reduction in local blood flow that initiates a well-characterised ischemic cascade. Downstream hypoxia and acidosis activate acid sensing ion channel 1a (ASIC1a) to trigger cell death. We recently showed that administration of a potent venom-derived inhibitor of ASIC1a, Hi1a, leads to tissue sparing and improved functional recovery when delivered up to 8 h after ischemic stroke. Here, we use whole-cell patch-clamp electrophysiology in a spinal cord slice preparation to assess the effect of acute ASIC1a inhibition, via a single dose of Hi1a, on intrinsic membrane properties and excitatory synaptic transmission long-term after a spinal cord hemisection injury. We focus on a population of interneurons (INs) in the deep dorsal horn (DDH) that play a key role in relaying sensory information to downstream motoneurons. DDH INs in mice treated with Hi1a 1 h after a spinal cord hemisection showed no change in active or passive intrinsic membrane properties measured 4 weeks after SCI. DDH INs, however, exhibit significant changes in the kinetics of spontaneous excitatory postsynaptic currents after a single dose of Hi1a, when compared to naive animals (unlike SCI mice). Our data suggest that acute ASIC1a inhibition exerts selective effects on excitatory synaptic transmission in DDH INs after SCI via specific ligand-gated receptor channels, and has no effect on other voltage-activated channels long-term after SCI.
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DDH INs in mice treated with Hi1a 1 h after a spinal cord hemisection showed no change in active or passive intrinsic membrane properties measured 4 weeks after SCI. DDH INs, however, exhibit significant changes in the kinetics of spontaneous excitatory postsynaptic currents after a single dose of Hi1a, when compared to naive animals (unlike SCI mice). 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subjects Acidification
Acidosis
Analysis
Animals
Blood flow
Brain research
Care and treatment
Cell death
Damage
Diagnosis
Dorsal horn
Electrophysiology
Excitatory postsynaptic potentials
Experiments
Fentanyl
Hypoxia
Interneurons
Ion channels
Ischemia
Kinases
Kinetics
Membranes
Motor neurons
Neurons
Paralysis
Receptor channels
Recovery of function
Spinal cord injuries
Surgery
Synaptic transmission
Venom
title Acute inhibition of acid sensing ion channel 1a after spinal cord injury selectively affects excitatory synaptic transmission, but not intrinsic membrane properties, in deep dorsal horn interneurons
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