Genetic or Pharmacological Ablation of Acid-Sensing Ion Channel 1a (ASIC1a) Is Not Neuroprotective in a Mouse Model of Spinal Cord Injury

Foster, Victoria S.; Saez, Natalie J.; Gillespie, Ellen R.; Jogia, Trisha; Reid, Chantelle R.; Maljevic, Snezana; Jung, Won-Cheol; Lao, Hong W.; Ruitenberg, Marc J.; King, Glen C.

doi:10.1089/neu.2022.0295

Cited by 2 publications

(4 citation statements)

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“…In addition, previous studies examining the therapeutic effects of inhibiting ASIC1a have shown promising results in different disease contexts, including myocardial infarction, stroke, spinal cord injury, and renal ischemia-reperfusion injury, in both rats and mice, with Hi1a administered i.v. in myocardial infarction, whereas ASIC1a inhibitors were given intracerebroventricularly or intrathecally when assessing CNS indications. ,,,,, However, not all studies have observed a therapeutic effect with ASIC1a inhibition, since inhibiting ASIC1a using whole PcTx1 venom resulted in decreased infarct volume following stroke when administered intracerebroventricularly but not if administered intravenously, and other studies reported worse disease outcomes with ASIC1a deletion or inhibition in spinal cord injury. , In vitro, ASIC1a KO spinal cord slices displayed greater damage compared to WT mice, and nonselective ASIC1a inhibitors worsened neuronal loss . Similarly, in vivo, ASIC1a KO mice displayed worse functional outcomes and a larger lesion after spinal cord injury, although intravenous treatment with Hi1a did not influence functional outcomes .…”

Section: Discussionmentioning

confidence: 99%

“…in myocardial infarction, whereas ASIC1a inhibitors were given intracerebroventricularly or intrathecally when assessing CNS indications. ,,,,, However, not all studies have observed a therapeutic effect with ASIC1a inhibition, since inhibiting ASIC1a using whole PcTx1 venom resulted in decreased infarct volume following stroke when administered intracerebroventricularly but not if administered intravenously, and other studies reported worse disease outcomes with ASIC1a deletion or inhibition in spinal cord injury. , In vitro, ASIC1a KO spinal cord slices displayed greater damage compared to WT mice, and nonselective ASIC1a inhibitors worsened neuronal loss . Similarly, in vivo, ASIC1a KO mice displayed worse functional outcomes and a larger lesion after spinal cord injury, although intravenous treatment with Hi1a did not influence functional outcomes . Thus, the results of the current study, where intravenous administration of Hi1a was able to improve some functional outcomes but did not consistently improve all stroke outcomes across both models may be due to a loss of drug efficacy when administered systemically compared to centrally.…”

Section: Discussionmentioning

confidence: 99%

“…For example, ASIC1a knockout (KO) mice have a marginally worse hindlimb function and marginally increased lesion size compared to wild-type (WT) mice after spinal cord injury, in contrast to the protective effects of ASIC1 KO observed in stroke . Furthermore, treatment with Hi1a intravenously 1 h postspinal cord injury resulted in no change in hindlimb function or neuronal loss . This highlights the fact that further investigation is required to elucidate the mechanistic role of ASIC1a in stroke and whether Hi1a might be a viable therapeutic.…”

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confidence: 99%

“…Furthermore, the protective effects of Hi1a were not blunted when treatment was delayed up to 8 h poststroke, which is a much longer therapeutic window than the current gold-standard treatment for stroke. , Nevertheless, there is some ambiguity in the neuroprotective effect of blunting ASIC1a signaling. For example, ASIC1a knockout (KO) mice have a marginally worse hindlimb function and marginally increased lesion size compared to wild-type (WT) mice after spinal cord injury, in contrast to the protective effects of ASIC1 KO observed in stroke . Furthermore, treatment with Hi1a intravenously 1 h postspinal cord injury resulted in no change in hindlimb function or neuronal loss .…”

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Hi1a Improves Sensorimotor Deficit following Endothelin-1-Induced Stroke in Rats but Does Not Improve Functional Outcomes following Filament-Induced Stroke in Mice

Knezic,

Budusan,

Saez

et al. 2024

ACS Pharmacol. Transl. Sci.

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Activation of acid-sensing ion channel 1a (ASIC1a) plays a major role in mediating acidosis-induced neuronal injury following a stroke. Therefore, the inhibition of ASIC1a is a potential therapeutic avenue for the treatment of stroke. Venom-peptide Hi1a, a selective and highly potent ASIC1a inhibitor, reduces the infarct size and functional deficits when injected into the brain after stroke in rodents. However, its efficacy when administered using a clinically relevant route of administration remains to be established. Therefore, the current investigation aims to examine the efficacy of systemically administered Hi1a, using two different models of stroke in different species. Mice were subjected to the filament model of middle cerebral artery occlusion (MCAO) and treated with Hi1a systemically using either a single-or multiple-dosing regimen. 24 h poststroke, mice underwent functional testing, and the brain infarct size was assessed. Rats were subjected to endothelin-1 (ET-1)-induced MCAO and treated with Hi1a intravenously 2 h poststroke. Rats underwent functional tests prior to and for 3 days poststroke, when infarct volume was assessed. Mice receiving Hi1a did not show any improvements in functional outcomes, despite a trend toward reduced infarct size. This trend for reduced infarct size in mice was consistent regardless of the dosing regimen. There was also a trend toward lower infarct size in rats treated with Hi1a. More specifically, Hi1a reduced the amount of damage occurring within the somatosensory cortex, which was associated with an improved sensorimotor function in Hi1a-treated rats. Thus, this study suggests that Hi1a or more brain-permeable ASIC1a inhibitors are a potential stroke treatment.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Hi1a Improves Sensorimotor Deficit following Endothelin-1-Induced Stroke in Rats but Does Not Improve Functional Outcomes following Filament-Induced Stroke in Mice

Knezic,

Budusan,

Saez

et al. 2024

ACS Pharmacol. Transl. Sci.

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Acid-sensing ion channel-1 contributes to the failure of myelin sheath regeneration following spinal cord injury by transcellular delivery of PGE2

Wu,

Han,

Dong

et al. 2024

Cell Mol Biol Lett

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Background Traumatic injuries to spinal cord lead to severe motor, sensory, and autonomic dysfunction. The accumulation of inhibitory compounds plays a pivotal role in the secondary damage to sparing neural tissue and the failure of axonal regeneration and remyelination. Acid-sensing ion channel-1(ASIC1A) is widely activated following neurotrauma, including spinal cord injury (SCI). However, its role in SCI remains elusive. Methods The effects of acidic environment on the differentiation and genes changes of neural stem cells (NSCs) were assessed by immunofluorescence staining and RNA-sequencing analysis, respectively. The expression of ASIC1A and prostaglandin endoperoxide synthase 2 (PTGS2) were detected by western blot and immunofluorescence staining. The concentration of prostaglandin E2 (PGE2) within NSC-derived extracellular vesicles were evaluated by ELISA. Small-interfering RNAs (siRNAs) were used to knock down Asic1a and Ptgs2 expression in NSCs. The myelin sheath regeneration and axonal remyelination in rats and Asic1a-KO mice were assessed by immunofluorescence staining. Results Following injury to the spinal cord, ASIC1A was found to be colocalized and upregulated in NSCs. ASIC1A activation prevents the differentiation of NSCs into oligodendrocytes by upregulating PTGS2, which leads to increased production and release of PGE2 within extracellular vesicles (EVs). ASIC1A or PTGS2 deficiency in NSCs counters the ASIC1A-related effects on mediating NSC differentiation by reducing PGE2 expression within NSC-derived EVs. Furthermore, intervention in ASIC1A signaling by administration of ASIC1A inhibitors or genetic deletion of ASIC1A demonstrated a pronounced advantage in enhancing myelin sheath regeneration and axonal remyelination. Conclusions The activation of ASIC1A prevents NSC differentiation into oligodendrocytes via the transcellular NSC-to-NSC delivery of PGE2, resulting in the failure of myelin sheath regeneration and axonal remyelination following SCI. The inhibition of ASIC1A presents a promising therapeutic strategy for the treatment of SCI. Graphical Abstract

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Genetic or Pharmacological Ablation of Acid-Sensing Ion Channel 1a (ASIC1a) Is Not Neuroprotective in a Mouse Model of Spinal Cord Injury

Cited by 2 publications

References 60 publications

Hi1a Improves Sensorimotor Deficit following Endothelin-1-Induced Stroke in Rats but Does Not Improve Functional Outcomes following Filament-Induced Stroke in Mice

Hi1a Improves Sensorimotor Deficit following Endothelin-1-Induced Stroke in Rats but Does Not Improve Functional Outcomes following Filament-Induced Stroke in Mice

Acid-sensing ion channel-1 contributes to the failure of myelin sheath regeneration following spinal cord injury by transcellular delivery of PGE2

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