Elucidation of Inverse Agonist Activity of Bilastine

Mizuguchi, Hiroyuki; Wakugawa, Tomoharu; Sadakata, Hisato; Kamimura, Seiichiro; Takemoto, Masaya; Nakagawa, Tomomi; Yabumoto, Masami; Kitamura, Yoshiaki; Takeda, Noriaki; Fukui, Hirokazu

doi:10.3390/pharmaceutics12060525

Cited by 12 publications

(5 citation statements)

References 24 publications

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“…The results also show that FEX reduces the constitutive receptor activity of H1R in the absence of HIS, confirming the inverse agonist dual mode of action and its benefit when used with pre-treatment. These data are in agreement with a recent article reporting that FEX works as an inverse agonist able to inhibit the basal activity of H1R, based on a HeLa cell line system that express H1R endogenously (Mizuguchi et al, 2020). Furthermore, side-by-side comparison of the conditions showed higher anti-inflammatory activity of FEX (reduction of IL-6 and IL-8 expression) and a trend of higher downregulation of H1R expression with one-hour FEX pretreatment versus without FEX pre-treatment.…”

Section: Discussionsupporting

confidence: 93%

“…Some H1-antihistamines act as inverse agonists and reduce constitutive receptor activity by binding with and stabilizing the inactive form of H1R in the absence of HIS, thereby shifting the equilibrium of H1R toward the inactive state ( Leurs et al, 2002 ) ( Figure 1A ). As such, they may have a higher potency than neutral antagonists as they exhibit a dual mode of action: downregulation of constitutive H1R activity as well as prevention of H1R activation by HIS ( Leurs et al, 2002 ; Mizuguchi et al, 2012 ; Mizuguchi et al, 2020 ). Fexofenadine (FEX), a non-sedating antihistamine, is used to relieve AR and urticaria symptoms ( Leurs et al, 2002 ; Meltzer et al, 2021 ; Ansotegui et al, 2022 ).…”

Section: Introductionmentioning

confidence: 99%

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Establishment of a human nasal epithelium model of histamine-induced inflammation to assess the activity of fexofenadine as an inverse agonist and its link to clinical benefit

Barbot,

Lheritier-Barrand,

Murrieta-Aguttes

et al. 2024

Front. Pharmacol.

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BackgroundFexofenadine (FEX) is an antihistamine that acts as an inverse agonist against histamine (HIS) receptor 1 (H1R), which mediates the allergic reaction. Inverse agonists may be more potent than neutral antagonists, as they bind the same receptor as the agonist (HIS) but stabilize the inactive form and induce an opposite pharmacological response, suppressing the basal activity of H1R and preventing HIS from binding. This study aims to establish and validate a model of HIS-induced inflammation based on fully reconstituted human nasal epithelial tissue to assess the activity of FEX as an inverse agonist in this model and explore its link to clinical benefit.MethodsThe model was developed using nasal MucilAir™ (Epithelix) in vitro epithelium challenged by HIS. Two conditions were assessed in a side-by-side comparison: tissue was exposed to HIS + FEX with or without FEX pre-treatment (one-hour prior to HIS challenge). Tissue functionality, cytotoxicity, H1R gene expression, and inflammatory cytokines were assessed.ResultsHIS at 100 µM induced significant 3.1-fold and 2.2-fold increases for inflammatory biomarkers interleukin (IL)-8 and IL-6, respectively (p < 0.0001), as well as rapid upregulation of H1R mRNA. Inflammatory biomarkers were inhibited by FEX and H1R expression was significantly reduced (p < 0.0001). FEX alone decreased H1R expression at all doses tested. With one-hour FEX pre-treatment, there was significantly higher downregulation of IL-8 (p < 0.05) and further downregulation of H1R expression and IL-6 versus without FEX pre-treatment; the effects of FEX were improved from 22% to 40%.ConclusionA model of HIS-induced airway inflammation was established based on IL-8, IL-6 and H1R gene expression and was validated with FEX. FEX works as an inverse agonist, with a higher effect when used before+during versus only during the HIS challenge. Taking FEX before+during allergen exposure, or when symptoms first occur, may reduce basal activity and H1R gene expression, providing stronger protection against the worsening of symptoms upon allergen exposure.

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Section: Discussionsupporting

confidence: 93%

Section: Introductionmentioning

confidence: 99%

Establishment of a human nasal epithelium model of histamine-induced inflammation to assess the activity of fexofenadine as an inverse agonist and its link to clinical benefit

Barbot,

Lheritier-Barrand,

Murrieta-Aguttes

et al. 2024

Front. Pharmacol.

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“…Bilastine is an effective, well-tolerated, and safe secondgeneration, nonsedating selective inverse H1 histamine receptor agonist authorized for the treatment of allergic disorders such as ARC and urticaria in adults, adolescents, and children [15,16]. Bilastine has been extensively evaluated in pharmacokinetic, efficacy, and safety studies [17][18][19], revealing efficacy [20,21] and an excellent safety and tolerability profile [22][23][24][25][26].…”

Section: Introductionmentioning

confidence: 99%

Pharmacokinetics and Safety of Bilastine 10 mg/d in Children Aged 2 to 5 Years With Allergic Rhinoconjunctivitis or Urticaria: A Phase 3 Clinical Trial

Majorek-Olechowska,

Slomskis,

Zollerová

et al. 2024

J Investig Allergol Clin Immunol

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Background: Bilastine is a second-generation antihistamine for the symptomatic treatment of allergic rhinoconjunctivitis (ARC) and urticaria in adults, adolescents, and children. The pharmacokinetics and safety of oral bilastine 10 mg/d in children aged 2 to 5 years were evaluated. Methods: This was a multicenter, open-label clinical trial in children aged 2 to 5 years with seasonal or perennial ARC or urticaria treated once daily with bilastine 10 mg orodispersible tablets. The safety evaluation included treatment-emergent adverse events (TEAEs), vital signs, and physical examination. Pharmacokinetic data were pooled with data from a prior pediatric study, and pharmacokinetic modeling was performed to assess consistency. Results: A total of 37 children with ARC (81.1%), urticaria (8.1%), or both (10.8%) were included in the study, with a mean (SD) age of 3.7 (1.2) years. The highest plasma concentrations of bilastine were observed 1 hour after administration (634.91 ng/mL). Eight patients (21.6%) experienced 1 TEAE each, none of which was severe. Body weight and age were not covariates of variation in either systemic clearance or the volume of distribution in children aged 2 to 5 years and did not affect the pharmacokinetic parameters of bilastine. Conclusions: The pharmacokinetics of bilastine was linear and consistent with data from a previous trial, suggesting that a 10-mg dose may be used in children (2 to <12 years). No dose adjustments are deemed necessary. Oral once-daily bilastine 10 mg presented a good safety profile in children aged 2 to 5.

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“…Bilastine is a nonsedating second-generation H 1 -antihistamine characterized by a fast onset of action and a prolonged effect, 14 , 15 with inverse agonist activity. 16 To date, bilastine has been administered through the oral route in the symptomatic treatment of seasonal or perennial allergic rhinoconjunctivitis and urticaria. 17 Recently, a new ophthalmic formulation of bilastine has been developed for the treatment of allergic conjunctivitis.…”

Section: Introductionmentioning

confidence: 99%

Ocular Biodistribution of Once-Daily 0.6% Bilastine Eye Drops Reveals Highest Levels in Conjunctiva Up to 24 h Postadministration

Torrens

Ganza

Hernández

et al. 2022

Journal of Ocular Pharmacology and Therapeutics

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Purpose: Bilastine is a second-generation antihistamine that has been shown to be effective for treatment of allergic conjunctivitis. The objective of this study was to evaluate the pharmacokinetics (PKs) and biodistribution of 0.6% bilastine preservative-free eye drops. Methods: Bilastine was quantified in the conjunctiva, cornea, aqueous humor, vitreous humor, iris/ciliary body, retina/choroid, crystalline lens, and plasma, following a single topical administration to male Dutch-belted rabbits. Results: Concentrations of bilastine were highest in the conjunctiva [C max : 2,545.04 ng/g, at 6 h postadministration; area under the concentration–time curve (AUC t ): 11,382.40 ng·h/g] and cornea (C max : 609.11 ng/g, at 1 h postadministration; AUC t : 1,993.88 ng·h/g), followed by the iris/ciliary body, retina/choroid, aqueous humor, plasma, vitreous humor, and crystalline lens. Quantifiable bilastine concentrations were observed up to 24 h after instillation in the conjunctiva (388.45 ng/g), cornea (28.68 ng/g), iris/ciliary body (12.42 ng/g), retina/choroid (1.91 ng/g), and crystalline lens (0.12 ng/g). In plasma, aqueous humor, and vitreous humor, bilastine was detected up to 12 h postadministration (0.18 ng/mL, 0.40 ng/mL, and 0.32 ng/g, respectively). Conclusions: PKs and biodistribution of 0.6% bilastine eye drops in rabbits revealed a marked preferential distribution in the conjunctiva (target tissue), with sustained levels up to 24 h. These findings are consistent with clinical efficacy trials supporting once-daily administration of topical bilastine for treatment of allergic conjunctivitis.

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Elucidation of Inverse Agonist Activity of Bilastine

Cited by 12 publications

References 24 publications

Establishment of a human nasal epithelium model of histamine-induced inflammation to assess the activity of fexofenadine as an inverse agonist and its link to clinical benefit

Establishment of a human nasal epithelium model of histamine-induced inflammation to assess the activity of fexofenadine as an inverse agonist and its link to clinical benefit

Pharmacokinetics and Safety of Bilastine 10 mg/d in Children Aged 2 to 5 Years With Allergic Rhinoconjunctivitis or Urticaria: A Phase 3 Clinical Trial

Ocular Biodistribution of Once-Daily 0.6% Bilastine Eye Drops Reveals Highest Levels in Conjunctiva Up to 24 h Postadministration

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