The Mechanism of Inhibitory Actions of S-Petasin, a Sesquiterpene of<i>Petasites formosanus</i>, on L-Type Calcium Current in NG108-15 Neuronal Cells

Wu, Sheng‐Nan; Chen, Hsinyo; Lin, Yun

doi:10.1055/s-2003-37711

Cited by 16 publications

(10 citation statements)

References 12 publications

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“…The negative chronotropic and inotropic properties of S-petasin also can be attributed mainly to inhibition of voltage-dependent Ca 2+ channels but not to blockade of dihydropyridine binding sites of L-type Ca 2+ channel or to muscarinic receptor activation [29]. Direct affection of L-type Ca 2+ channels by S-petasin was also found in NG108 ± 15 neuronal cells [30]. S-Isopetasin allosterically antagonizes carbachol in isolated guinea pig atria [31].…”

Section: Resultsmentioning

confidence: 87%

Petasites hybridusExtractsin vitroInhibit COX-2 and PGE₂Release by Direct Interaction with the Enzyme and by Preventing p42/44 MAP Kinase Activation in Rat Primary Microglial Cells

et al. 2005

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Rhizomes of butterbur, Petasites hybridus L. (Asteraceae), have been used since ancient times for the treatment of inflammatory diseases. In the present study, the effects of lipophilic extracts from rhizomes of Petasites hybridus on the formation and release of prostaglandin E2 were investigated. The extracts had different contents of petasin and isopetasin: A: 2.1 % and 0.4 %, B: 0.2 % and 0.1 %, C: 12.1 % and 6.1 % and D: 21.9 % and 9.4 %, respectively. Direct inhibition of cyclooxygenase (COX) -1 and -2 isoenzymes and inhibition of the expression of COX-2 and p42/44 MAP kinase in rat primary microglial cells were tested. All extracts were found to be only weak direct inhibitors of COX-1 (IC50> 400 microg/mL). However, most extracts revealed a strong inhibitory activity against the inducible isoform COX-2 ( A: IC50=30.4 microg/mL; B: IC50=60.6 microg/mL; C: IC50=22.6 microg/mL; D: IC50=20.0 microg/mL). This activity was not correlated to the content of petasin and isopetasin. Pure petasin and isopetasin neither inhibited COX-1 nor COX-2 (IC50 > 400 microM for both compounds and enzymes). Petasites extracts dose-dependently inhibited LPS-induced and thus COX-2-mediated PGE2 release in primary rat microglial cells (A: IC50= 2.4 microg/mL; C: IC50=5.8 microg/mL and D: IC50=4.6 microg/mL). Also this effect was independent from the petasin and isopetasin content. COX-2 synthesis in microglia was totally blocked with 5 microg/mL of C whereas COX-1 synthesis was not influenced. C and D did not affect the LPS-induced activation of p38 MAPK and IkappaBalpha, but they prevented the LPS-induced activation of p42/44 MAPK. Therefore, these Petasites hybridus extracts can be regarded as natural selective inhibitors of COX-2 and its expression, an effect which is independent from the petasin content.

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Section: Resultsmentioning

confidence: 87%

Petasites hybridusExtractsin vitroInhibit COX-2 and PGE₂Release by Direct Interaction with the Enzyme and by Preventing p42/44 MAP Kinase Activation in Rat Primary Microglial Cells

et al. 2005

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“…In the present in vitro results, S -petasin (30–100 μ M), but not at 300 μ M which is beyond a physiological condition, did not inhibit cumulative OVA-induced contractions of isolated sensitized guinea pig trachealis, which were unaffected by 1 μ M nifedipine, suggesting that S -petasin does not inhibit degranulation or activation of mast cells [57]. Indeed, S -petasin was reported to be an L-type voltage-dependent Ca 2+ channel blocker in rat aortic smooth muscle cells [58, 59] and in mouse NG 108-15 neuronal cells [60]. In these neuronal cells, a higher concentration (100 μ M) of S -petasin was also reported to inhibit the delayed rectifier K + current in a time-dependent manner, suggesting that such a blockage does not seem to be instantaneous, but develops with time after the channels are opened [60].…”

Section: Discussionmentioning

confidence: 99%

“…Indeed, S -petasin was reported to be an L-type voltage-dependent Ca 2+ channel blocker in rat aortic smooth muscle cells [58, 59] and in mouse NG 108-15 neuronal cells [60]. In these neuronal cells, a higher concentration (100 μ M) of S -petasin was also reported to inhibit the delayed rectifier K + current in a time-dependent manner, suggesting that such a blockage does not seem to be instantaneous, but develops with time after the channels are opened [60]. The blockage by S -petasin may contribute to the regulation of neuronal activity, but not to relaxation of the trachea-bronchial tree.…”

Section: Discussionmentioning

confidence: 99%

S‐Petasin, the Main Sesquiterpene of Petasites formosanus, Inhibits Phosphodiesterase Activity and Suppresses Ovalbumin‐Induced Airway Hyperresponsiveness

Shih

Huang

Chen

et al. 2011

Evidence-Based Complementary and Alternative Medicine

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S-Petasin is the main sesquiterpene of Petasites formosanus, a traditional folk medicine used to treat hypertension, tumors and asthma in Taiwan. The aim of the present study was to investigate its inhibitory effects on phosphodiesterase (PDE) 1–5, and on ovalbumin (OVA)-induced airway hyperresponsiveness (AHR) in a murine model of allergic asthma. S-Petasin concentration-dependently inhibited PDE3 and PDE4 activities with 50% inhibitory concentrations (IC50) of 25.5, and 17.5 μM, respectively. According to the Lineweaver-Burk analysis, S-petasin competitively inhibited PDE3 and PDE4 activities with respective dissociation constants for inhibitor binding (K i) of 25.3 and 18.1 μM, respectively. Both IC50 and K i values for PDE3 were significantly greater than those for PDE4. S-Petasin (10–30 μmol/kg, administered subcutaneously (s.c.)) dose-dependently and significantly attenuated the enhanced pause (P enh) value induced by methacholine (MCh) in sensitized and challenged mice. It also significantly suppressed the increases in total inflammatory cells, lymphocytes, neutrophils, eosinophils and levels of cytokines, including interleukin (IL)-2, IL-4 and IL-5, tumor necrosis factor (TNF)-α and interferon (IFN)-γ in bronchoalveolar lavage fluid (BALF) of these mice. In addition, S-petasin (10–30 μmol/kg, s.c.) dose-dependently and significantly attenuated total and OVA-specific immunoglobulin E (IgE) levels in the serum and BALF, and enhanced the IgG2a level in serum of these mice. The PDE4H value of S-petasin was >300 μM; therefore, its PDE4H/PDE4L value was calculated to be >17. In conclusion, the present results for S-petasin at least partially explain why Petasites formosanus is used as a folk medicine to treat asthma in Taiwan.

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“…They both inhibit the synthesis of peptide-leukotriene, whilst petasin also blocks the release of the eosinophil cationic protein [35]. Additionally, petasin inhibits contractions induced by histamine, carbachol, and the accumulation of calcium ions [19,41,44]. It follows that non-specific antispasmodic and antimuscarinic effects are responsible for the myorelaxant activity of petasin [2].…”

Section: Active Substances From Petasites and Their Mechanism Of Actionmentioning

confidence: 99%

A botanical and pharmacological description of petasites species

Tys

Szopa

Lalak

et al. 2015

Current Issues in Pharmacy and Medical Sciences

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The objective of this review was to evaluate the botanical and pharmacological description of Petasites species. Petasides (butterbur) as a perennial shrub which was found in Europe and also in a parts of Asia and North America, has been widely used medicinally for centuries. At present, the main phytopharmacology uses for Petasides extracts are for prophylactic treatment of migraines, as well as an antispasmodic agent for bronchial asthma and pertussis. Furthermore, it has been used effectively in preventing gastric ulcers, and in urinary tract spasms and treating patients with irritable bladder. But still, there is a need for more studies on the potential applications of butterbur extract in medicine.

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The Mechanism of Inhibitory Actions of S-Petasin, a Sesquiterpene ofPetasites formosanus, on L-Type Calcium Current in NG108-15 Neuronal Cells

Cited by 16 publications

References 12 publications

Petasites hybridusExtractsin vitroInhibit COX-2 and PGE₂Release by Direct Interaction with the Enzyme and by Preventing p42/44 MAP Kinase Activation in Rat Primary Microglial Cells

Petasites hybridusExtractsin vitroInhibit COX-2 and PGE₂Release by Direct Interaction with the Enzyme and by Preventing p42/44 MAP Kinase Activation in Rat Primary Microglial Cells

S‐Petasin, the Main Sesquiterpene of Petasites formosanus, Inhibits Phosphodiesterase Activity and Suppresses Ovalbumin‐Induced Airway Hyperresponsiveness

A botanical and pharmacological description of petasites species

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The Mechanism of Inhibitory Actions of S-Petasin, a Sesquiterpene ofPetasites formosanus, on L-Type Calcium Current in NG108-15 Neuronal Cells

Cited by 16 publications

References 12 publications

Petasites hybridusExtractsin vitroInhibit COX-2 and PGE2Release by Direct Interaction with the Enzyme and by Preventing p42/44 MAP Kinase Activation in Rat Primary Microglial Cells

Petasites hybridusExtractsin vitroInhibit COX-2 and PGE2Release by Direct Interaction with the Enzyme and by Preventing p42/44 MAP Kinase Activation in Rat Primary Microglial Cells

S‐Petasin, the Main Sesquiterpene of Petasites formosanus, Inhibits Phosphodiesterase Activity and Suppresses Ovalbumin‐Induced Airway Hyperresponsiveness

A botanical and pharmacological description of petasites species

Contact Info

Product

Resources

About

Petasites hybridusExtractsin vitroInhibit COX-2 and PGE₂Release by Direct Interaction with the Enzyme and by Preventing p42/44 MAP Kinase Activation in Rat Primary Microglial Cells

Petasites hybridusExtractsin vitroInhibit COX-2 and PGE₂Release by Direct Interaction with the Enzyme and by Preventing p42/44 MAP Kinase Activation in Rat Primary Microglial Cells