Effect of CRTH2 antagonism on the response to experimental rhinovirus infection in asthma: a pilot randomised controlled trial

Hugo Farne; Nicholas Glanville; Nicholas  Johnson; Tata Kebadze; Julia Aniscenko; Eteri Regis; Jie Zhu; Maria-Belen Trujillo-Torralbo; Onn Min  Kon; Patrick Mallia; Toby Prevost; Michael R. Rose; Michael Edwards; Sebastian Johnston; Aran Singanayagam; David J. Jackson

doi:DOI: 10.1136/thoraxjnl-2021-217429

Effect of CRTH2 antagonism on the response to experimental rhinovirus infection in asthma: a pilot randomised controlled trial

Hugo Farne, Nicholas Glanville, Nicholas Johnson, Tata Kebadze, Julia Aniscenko, Eteri Regis, Jie Zhu, Maria-Belen Trujillo-Torralbo, Onn Min Kon, Patrick Mallia, Toby Prevost, Michael R. Rose, Michael Edwards, Sebastian Johnston, Aran Singanayagam, David J. Jackson

Cicely Saunders Institute of Palliative Care, Policy & Rehabilitation

Research output: Contribution to journal › Article › peer-review

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Abstract

Abstract

Background and aims: The chemoattractant receptor-homologous molecule expressed on T helper type 2 cells (CRTH2) antagonist timapiprant improved lung function and asthma control in a phase 2 study, with evidence suggesting reduced exacerbations. We aimed to assess whether timapiprant attenuated or prevented asthma exacerbations induced by experimental rhinovirus (RV) infection. We furthermore hypothesised that timapiprant would dampen RV-induced type 2 inflammation and consequently improve antiviral immune responses.

Methods: Atopic patients with partially controlled asthma on maintenance inhaled corticosteroids were randomised to timapiprant (n=22) or placebo (n=22) and challenged with RV-A16 3 weeks later. The primary endpoint was the cumulative lower respiratory symptom score over the 14 days post infection. Upper respiratory symptoms, spirometry, airway hyperresponsiveness, exhaled nitric oxide, RV-A16 virus load and soluble mediators in upper and lower airways samples, and CRTH2 staining in bronchial biopsies were additionally assessed before and during RV-A16 infection.

Results: Six subjects discontinued the study and eight were not infected; outcomes were assessed in 16 timapiprant-treated and 14 placebo-treated, successfully infected subjects. There were no differences between treatment groups in clinical exacerbation severity including cumulative lower respiratory symptom score day 0-14 (difference 3.0 (95% CI -29.0 to 17.0), p=0.78), virus load, antiviral immune responses, or RV-A16-induced airway inflammation other than in the bronchial biopsies, where CRTH2 staining was increased during RV-A16 infection in the placebo-treated but not the timapiprant-treated group. Timapiprant had a favourable safety profile, with no deaths, serious adverse events or drug-related withdrawals.

Conclusion: Timapiprant treatment had little impact on the clinicopathological changes induced by RV-A16 infection in partially controlled asthma.

Keywords: asthma; viral infection.

Original language	English
Article number	thoraxjnl-2021-217429
Number of pages	10
Journal	Thorax
DOIs	https://doi.org/DOI: 10.1136/thoraxjnl-2021-217429
Publication status	E-pub ahead of print - 29 Oct 2021

Keywords

Asthma
Viral infection

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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DOI: 10.1136/thoraxjnl-2021-217429Licence: CC BY

2021.08.31 Timapiprant in RV challenge in asthma_Thorax_main text_CLEANAccepted author manuscript, 227 KBLicence: Other

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Farne, H., Glanville, N., Johnson, N., Kebadze, T., Aniscenko, J., Regis, E., Zhu, J., Trujillo-Torralbo, M.-B., Kon, O. M., Mallia, P., Prevost, T., Rose, M. R., Edwards, M., Johnston, S., Singanayagam, A., & Jackson, D. J. (2021). Effect of CRTH2 antagonism on the response to experimental rhinovirus infection in asthma: a pilot randomised controlled trial. Thorax, Article thoraxjnl-2021-217429. Advance online publication. https://doi.org/DOI: 10.1136/thoraxjnl-2021-217429

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title = "Effect of CRTH2 antagonism on the response to experimental rhinovirus infection in asthma: a pilot randomised controlled trial",

abstract = "AbstractBackground and aims: The chemoattractant receptor-homologous molecule expressed on T helper type 2 cells (CRTH2) antagonist timapiprant improved lung function and asthma control in a phase 2 study, with evidence suggesting reduced exacerbations. We aimed to assess whether timapiprant attenuated or prevented asthma exacerbations induced by experimental rhinovirus (RV) infection. We furthermore hypothesised that timapiprant would dampen RV-induced type 2 inflammation and consequently improve antiviral immune responses.Methods: Atopic patients with partially controlled asthma on maintenance inhaled corticosteroids were randomised to timapiprant (n=22) or placebo (n=22) and challenged with RV-A16 3 weeks later. The primary endpoint was the cumulative lower respiratory symptom score over the 14 days post infection. Upper respiratory symptoms, spirometry, airway hyperresponsiveness, exhaled nitric oxide, RV-A16 virus load and soluble mediators in upper and lower airways samples, and CRTH2 staining in bronchial biopsies were additionally assessed before and during RV-A16 infection.Results: Six subjects discontinued the study and eight were not infected; outcomes were assessed in 16 timapiprant-treated and 14 placebo-treated, successfully infected subjects. There were no differences between treatment groups in clinical exacerbation severity including cumulative lower respiratory symptom score day 0-14 (difference 3.0 (95% CI -29.0 to 17.0), p=0.78), virus load, antiviral immune responses, or RV-A16-induced airway inflammation other than in the bronchial biopsies, where CRTH2 staining was increased during RV-A16 infection in the placebo-treated but not the timapiprant-treated group. Timapiprant had a favourable safety profile, with no deaths, serious adverse events or drug-related withdrawals.Conclusion: Timapiprant treatment had little impact on the clinicopathological changes induced by RV-A16 infection in partially controlled asthma.Keywords: asthma; viral infection.",

keywords = "Asthma, Viral infection",

author = "Hugo Farne and Nicholas Glanville and Nicholas Johnson and Tata Kebadze and Julia Aniscenko and Eteri Regis and Jie Zhu and Maria-Belen Trujillo-Torralbo and Kon, {Onn Min} and Patrick Mallia and Toby Prevost and Rose, {Michael R.} and Michael Edwards and Sebastian Johnston and Aran Singanayagam and Jackson, {David J.}",

year = "2021",

month = oct,

day = "29",

doi = "DOI: 10.1136/thoraxjnl-2021-217429",

language = "English",

journal = "Thorax",

issn = "0040-6376",

publisher = "BRITISH MED JOURNAL PUBL GROUP",

}

Farne, H, Glanville, N, Johnson, N, Kebadze, T, Aniscenko, J, Regis, E, Zhu, J, Trujillo-Torralbo, M-B, Kon, OM, Mallia, P, Prevost, T, Rose, MR, Edwards, M, Johnston, S, Singanayagam, A & Jackson, DJ 2021, 'Effect of CRTH2 antagonism on the response to experimental rhinovirus infection in asthma: a pilot randomised controlled trial', Thorax. https://doi.org/DOI: 10.1136/thoraxjnl-2021-217429

TY - JOUR

T1 - Effect of CRTH2 antagonism on the response to experimental rhinovirus infection in asthma: a pilot randomised controlled trial

AU - Farne, Hugo

AU - Glanville, Nicholas

AU - Johnson, Nicholas

AU - Kebadze, Tata

AU - Aniscenko, Julia

AU - Regis, Eteri

AU - Zhu, Jie

AU - Trujillo-Torralbo, Maria-Belen

AU - Kon, Onn Min

AU - Mallia, Patrick

AU - Prevost, Toby

AU - Rose, Michael R.

AU - Edwards, Michael

AU - Johnston, Sebastian

AU - Singanayagam, Aran

AU - Jackson, David J.

PY - 2021/10/29

Y1 - 2021/10/29

N2 - AbstractBackground and aims: The chemoattractant receptor-homologous molecule expressed on T helper type 2 cells (CRTH2) antagonist timapiprant improved lung function and asthma control in a phase 2 study, with evidence suggesting reduced exacerbations. We aimed to assess whether timapiprant attenuated or prevented asthma exacerbations induced by experimental rhinovirus (RV) infection. We furthermore hypothesised that timapiprant would dampen RV-induced type 2 inflammation and consequently improve antiviral immune responses.Methods: Atopic patients with partially controlled asthma on maintenance inhaled corticosteroids were randomised to timapiprant (n=22) or placebo (n=22) and challenged with RV-A16 3 weeks later. The primary endpoint was the cumulative lower respiratory symptom score over the 14 days post infection. Upper respiratory symptoms, spirometry, airway hyperresponsiveness, exhaled nitric oxide, RV-A16 virus load and soluble mediators in upper and lower airways samples, and CRTH2 staining in bronchial biopsies were additionally assessed before and during RV-A16 infection.Results: Six subjects discontinued the study and eight were not infected; outcomes were assessed in 16 timapiprant-treated and 14 placebo-treated, successfully infected subjects. There were no differences between treatment groups in clinical exacerbation severity including cumulative lower respiratory symptom score day 0-14 (difference 3.0 (95% CI -29.0 to 17.0), p=0.78), virus load, antiviral immune responses, or RV-A16-induced airway inflammation other than in the bronchial biopsies, where CRTH2 staining was increased during RV-A16 infection in the placebo-treated but not the timapiprant-treated group. Timapiprant had a favourable safety profile, with no deaths, serious adverse events or drug-related withdrawals.Conclusion: Timapiprant treatment had little impact on the clinicopathological changes induced by RV-A16 infection in partially controlled asthma.Keywords: asthma; viral infection.

AB - AbstractBackground and aims: The chemoattractant receptor-homologous molecule expressed on T helper type 2 cells (CRTH2) antagonist timapiprant improved lung function and asthma control in a phase 2 study, with evidence suggesting reduced exacerbations. We aimed to assess whether timapiprant attenuated or prevented asthma exacerbations induced by experimental rhinovirus (RV) infection. We furthermore hypothesised that timapiprant would dampen RV-induced type 2 inflammation and consequently improve antiviral immune responses.Methods: Atopic patients with partially controlled asthma on maintenance inhaled corticosteroids were randomised to timapiprant (n=22) or placebo (n=22) and challenged with RV-A16 3 weeks later. The primary endpoint was the cumulative lower respiratory symptom score over the 14 days post infection. Upper respiratory symptoms, spirometry, airway hyperresponsiveness, exhaled nitric oxide, RV-A16 virus load and soluble mediators in upper and lower airways samples, and CRTH2 staining in bronchial biopsies were additionally assessed before and during RV-A16 infection.Results: Six subjects discontinued the study and eight were not infected; outcomes were assessed in 16 timapiprant-treated and 14 placebo-treated, successfully infected subjects. There were no differences between treatment groups in clinical exacerbation severity including cumulative lower respiratory symptom score day 0-14 (difference 3.0 (95% CI -29.0 to 17.0), p=0.78), virus load, antiviral immune responses, or RV-A16-induced airway inflammation other than in the bronchial biopsies, where CRTH2 staining was increased during RV-A16 infection in the placebo-treated but not the timapiprant-treated group. Timapiprant had a favourable safety profile, with no deaths, serious adverse events or drug-related withdrawals.Conclusion: Timapiprant treatment had little impact on the clinicopathological changes induced by RV-A16 infection in partially controlled asthma.Keywords: asthma; viral infection.

KW - Asthma

KW - Viral infection

U2 - DOI: 10.1136/thoraxjnl-2021-217429

DO - DOI: 10.1136/thoraxjnl-2021-217429

M3 - Article

SN - 0040-6376

JO - Thorax

JF - Thorax

M1 - thoraxjnl-2021-217429

ER -

Effect of CRTH2 antagonism on the response to experimental rhinovirus infection in asthma: a pilot randomised controlled trial

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Keywords

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