2022
DOI: 10.1139/cjpp-2021-0286
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New approaches to the design of analgesic medicinal substances

Abstract: A gamma-pyrone derivative, comenic acid, activates the opioid-like receptor-mediated signaling pathway that modulates the NaV1.8 channels in the primary sensory neuron membrane. These channels are responsible for generation of the nociceptive signal; gamma-pyrones can therefore have a great therapeutic potential as analgesics, and this effect deserves a deeper understanding. The novelty of our approach to the design of a medicinal substance is based on a combination of the data obtained on living neurons using… Show more

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Cited by 8 publications
(12 citation statements)
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“…The ability of the tripeptides to modulate voltage sensitivity of the Na V 1.8 channel is highly specific, as the concentrations of TP1 and TP2 evoking a significant decrease in Z eff are in the nanomolar range (100 nM). Experimental data strongly suggest that both molecules are promising candidates for the role of a novel analgesic medicinal substance because our prior experience with respect to the receptor-mediated effect of comenic acid demonstrates a correlation between the specific decrease in Z eff and antinociceptive effect at the organismal level [ 1 , 4 , 5 , 18 , 19 ].…”
Section: Discussionmentioning
confidence: 99%
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“…The ability of the tripeptides to modulate voltage sensitivity of the Na V 1.8 channel is highly specific, as the concentrations of TP1 and TP2 evoking a significant decrease in Z eff are in the nanomolar range (100 nM). Experimental data strongly suggest that both molecules are promising candidates for the role of a novel analgesic medicinal substance because our prior experience with respect to the receptor-mediated effect of comenic acid demonstrates a correlation between the specific decrease in Z eff and antinociceptive effect at the organismal level [ 1 , 4 , 5 , 18 , 19 ].…”
Section: Discussionmentioning
confidence: 99%
“…No effect of TP1 and TP2 on DRG neurite growth was detected. It indicates that the tripeptides, as opposed to earlier studied agents (comenic acid and ouabain applied at nanomolar concentrations), do not trigger the receptor- or transducer-mediated signaling cascades, the activation of which modulates the Na V 1.8 channel activation gating device [ 5 , 17 ]. This fact supports our suggestion that TP1 and TP2 bind directly to the Na V 1.8 channel due to intermolecular ion–ion bonding between positively charged guanidinium groups of the attacking peptide molecule and nucleophilic moieties of the Na V 1.8 channel.…”
Section: Discussionmentioning
confidence: 99%
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“…As an example, a number of short peptides were demonstrated at very low concentrations to modulate the Na V 1.8 channel activation gating system in nociceptors [19,20]. According to our data, another potentially very effective substance is EO, the Ca 2+ chelate complex of ouabain, which is also capable of modulating the Na V 1.8 channels via activation of the NKA signaling function (Kd = 1 nM) [13,21].…”
Section: Introductionmentioning
confidence: 68%