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Spider Venom Peptide Pn3a Inhibition of Primary Afferent High Voltage-Activated Calcium Channels

Front Pharmacol. 2021-01; 
Jeffrey R McArthur, Nehan R Munasinghe, Rocio K Finol-Urdaneta, David J Adams, Macdonald J Christie
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Catalog Antibody … rCa v 2.2 (a gift from Dr. D. Lipscombe), hCa v 2.2 (a gift from Dr. D. Yue), hCa v 2.3 (purchased from GenScript United States Inc.) were co-transfected with β 3 , α 2 δ 1 and GFP?… Get A Quote

摘要

Despite potently inhibiting the nociceptive voltage-gated sodium (Na) channel, Na1.7, -theraphotoxin Pn3a is antinociceptive only upon co-administration with sub-therapeutic opioid agonists, or by itself at doses >3,000-fold greater than its Na1.7 by a yet undefined mechanism. Na channels are structurally related to voltage-gated calcium (Ca) channels, Ca1 and Ca2. These channels mediate the high voltage-activated (HVA) calcium currents ( ) that orchestrate synaptic transmission in nociceptive dorsal root ganglion (DRG) neurons and are fine-tuned by opioid receptor (OR) activity. Using whole-cell patch clamp recording, we found that Pn3a (10?μM) inhibits ~55% of rat DRG neuron HVA- and 60-80% of Ca1.2, ... More

關鍵詞

antinociceptive, calcium channel, dorsal root ganglion, high-voltage activated, opioids, pain, spider venom-derived peptide
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