AI Article Synopsis

  • Researchers investigated herbal extracts for their ability to block T-type calcium channels (T-channels) linked to chronic pain, identifying sophoraflavanone G (SG) and its hop-derived analogues (2S)-6-prenylnaringenin (6-PNG) and (2S)-8-PNG as effective inhibitors.
  • The active compounds showed varying potency against T-channels, with 6-PNG and 8-PNG demonstrating reversible inhibition in certain cellular models, while SG had a stronger effect overall.
  • In animal studies, these compounds effectively reduced pain-related behaviors without significant side effects, suggesting their potential as therapeutic options for neuropathic and visceral pain.

Article Abstract

Since Ca3.2 T-type Ca channels (T-channels) expressed in the primary afferents and CNS contribute to intractable pain, we explored T-channel-blocking components in distinct herbal extracts using a whole-cell patch-clamp technique in HEK293 cells stably expressing Ca3.2 or Ca3.1, and purified and identified sophoraflavanone G (SG) as an active compound from SOPHORAE RADIX (SR). Interestingly, hop-derived SG analogues, (2S)-6-prenylnaringenin (6-PNG) and (2S)-8-PNG, but not naringenin, also blocked T-channels; IC (μM) of SG, (2S)-6-PNG and (2S)-8-PNG was 0.68-0.75 for Ca3.2 and 0.99-1.41 for Ca3.1. (2S)-6-PNG and (2S)-8-PNG, but not SG, exhibited reversible inhibition. The racemic (2R/S)-6-PNG as well as (2S)-6-PNG potently blocked Ca3.2, but exhibited minor effect on high-voltage-activated Ca channels and voltage-gated Na channels in differentiated NG108-15 cells. In mice, the mechanical allodynia following intraplantar (i.pl.) administration of an HS donor was abolished by oral or i.p. SR extract and by i.pl. SG, (2S)-6-PNG or (2S)-8-PNG, but not naringenin. Intraperitoneal (2R/S)-6-PNG strongly suppressed visceral pain and spinal ERK phosphorylation following intracolonic administration of an HS donor in mice. (2R/S)-6-PNG, administered i.pl. or i.p., suppressed the neuropathic allodynia induced by partial sciatic nerve ligation or oxaliplatin, an anti-cancer agent, in mice. (2R/S)-6-PNG had little or no effect on open-field behavior, motor performance or cardiovascular function in mice, and on the contractility of isolated rat aorta. (2R/S)-6-PNG, but not SG, was detectable in the brain after their i.p. administration in mice. Our data suggest that 6-PNG, a hop component, blocks T-channels, and alleviates neuropathic and visceral pain with little side effects.

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http://dx.doi.org/10.1016/j.neuropharm.2018.06.020DOI Listing

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