Characterisation of SARS-CoV-2 genomic variation in response to molnupiravir treatment in the AGILE Phase IIa clinical trial

I’ah Donovan-Banfield; Rebekah Penrice-Randal; Hannah Goldswain; Aleksandra M. Rzeszutek; Jack Pilgrim; Katie Bullock; Geoffrey Saunders; Josh Northey; Xiaofeng Dong; Yan Ryan; Helen Reynolds; Michelle Tetlow; Lauren E. Walker; Richard FitzGerald; Colin Hale; Rebecca Lyon; Christie Woods; Shazaad Ahmad; Dennis Hadjiyiannakis; Jimstan Periselneris; Emma Knox; Calley Middleton; Lara Lavelle-Langham; Victoria Shaw; William Greenhalf; Thomas Edwards; David Lalloo; Christopher J. Edwards; Alistair C. Darby; Miles W. Carroll; Gareth Griffiths; Saye H. Khoo; Julian A. Hiscox; Tom Fletcher

doi:10.1038/s41467-022-34839-9

Characterisation of SARS-CoV-2 genomic variation in response to molnupiravir treatment in the AGILE Phase IIa clinical trial

I’ah Donovan-Banfield
, Rebekah Penrice-Randal
, Hannah Goldswain
, Aleksandra M. Rzeszutek
, Jack Pilgrim
, Katie Bullock
, Geoffrey Saunders
, Josh Northey
, Xiaofeng Dong
, Yan Ryan
, Helen Reynolds
, Michelle Tetlow
, Lauren E. Walker
, Richard FitzGerald
, Colin Hale
, Rebecca Lyon
, Christie Woods
, Shazaad Ahmad
, Dennis Hadjiyiannakis
, Jimstan Periselneris

Emma Knox, Calley Middleton, Lara Lavelle-Langham, Victoria Shaw, William Greenhalf, Thomas Edwards, David Lalloo, Christopher J. Edwards, Alistair C. Darby, Miles W. Carroll, Gareth Griffiths, Saye H. Khoo, Julian A. Hiscox, Tom Fletcher

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

30 Citations (Scopus)

Abstract

Molnupiravir is an antiviral, currently approved by the UK Medicines and Healthcare products Regulatory Agency (MHRA) for treating at-risk COVID-19 patients, that induces lethal error catastrophe in SARS-CoV-2. How this drug-induced mechanism of action might impact the emergence of resistance mutations is unclear. To investigate this, we used samples from the AGILE Candidate Specific Trial (CST)−2 (clinical trial number NCT04746183). The primary outcomes of AGILE CST-2 were to measure the drug safety and antiviral efficacy of molnupiravir in humans (180 participants randomised 1:1 with placebo). Here, we describe the pre-specified exploratory virological endpoint of CST-2, which was to determine the possible genomic changes in SARS-CoV-2 induced by molnupiravir treatment. We use high-throughput amplicon sequencing and minor variant analysis to characterise viral genomics in each participant whose longitudinal samples (days 1, 3 and 5 post-randomisation) pass the viral genomic quality criteria (n = 59 for molnupiravir and n = 65 for placebo). Over the course of treatment, no specific mutations were associated with molnupiravir treatment. We find that molnupiravir significantly increased the transition:transversion mutation ratio in SARS-CoV-2, consistent with the model of lethal error catastrophe. This study highlights the utility of examining intra-host virus populations to strengthen the prediction, and surveillance, of potential treatment-emergent adaptations.

Original language	English
Article number	7284
Pages (from-to)	e7284
Journal	Nature Communications
Volume	13
Issue number	1
DOIs	https://doi.org/10.1038/s41467-022-34839-9
Publication status	Published - 26 Nov 2022

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41467 2022 Article 34839Final published version, 12.9 MBLicence: CC BY

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Donovan-Banfield, I., Penrice-Randal, R., Goldswain, H., Rzeszutek, A. M., Pilgrim, J., Bullock, K., Saunders, G., Northey, J., Dong, X., Ryan, Y., Reynolds, H., Tetlow, M., Walker, L. E., FitzGerald, R., Hale, C., Lyon, R., Woods, C., Ahmad, S., Hadjiyiannakis, D., ... Fletcher, T. (2022). Characterisation of SARS-CoV-2 genomic variation in response to molnupiravir treatment in the AGILE Phase IIa clinical trial. Nature Communications, 13(1), e7284. Article 7284. https://doi.org/10.1038/s41467-022-34839-9

@article{b1b6eaf6c6cf4e54b02a01a9309765f6,

title = "Characterisation of SARS-CoV-2 genomic variation in response to molnupiravir treatment in the AGILE Phase IIa clinical trial",

abstract = "Molnupiravir is an antiviral, currently approved by the UK Medicines and Healthcare products Regulatory Agency (MHRA) for treating at-risk COVID-19 patients, that induces lethal error catastrophe in SARS-CoV-2. How this drug-induced mechanism of action might impact the emergence of resistance mutations is unclear. To investigate this, we used samples from the AGILE Candidate Specific Trial (CST)−2 (clinical trial number NCT04746183). The primary outcomes of AGILE CST-2 were to measure the drug safety and antiviral efficacy of molnupiravir in humans (180 participants randomised 1:1 with placebo). Here, we describe the pre-specified exploratory virological endpoint of CST-2, which was to determine the possible genomic changes in SARS-CoV-2 induced by molnupiravir treatment. We use high-throughput amplicon sequencing and minor variant analysis to characterise viral genomics in each participant whose longitudinal samples (days 1, 3 and 5 post-randomisation) pass the viral genomic quality criteria (n = 59 for molnupiravir and n = 65 for placebo). Over the course of treatment, no specific mutations were associated with molnupiravir treatment. We find that molnupiravir significantly increased the transition:transversion mutation ratio in SARS-CoV-2, consistent with the model of lethal error catastrophe. This study highlights the utility of examining intra-host virus populations to strengthen the prediction, and surveillance, of potential treatment-emergent adaptations.",

author = "I{\textquoteright}ah Donovan-Banfield and Rebekah Penrice-Randal and Hannah Goldswain and Rzeszutek, \{Aleksandra M.\} and Jack Pilgrim and Katie Bullock and Geoffrey Saunders and Josh Northey and Xiaofeng Dong and Yan Ryan and Helen Reynolds and Michelle Tetlow and Walker, \{Lauren E.\} and Richard FitzGerald and Colin Hale and Rebecca Lyon and Christie Woods and Shazaad Ahmad and Dennis Hadjiyiannakis and Jimstan Periselneris and Emma Knox and Calley Middleton and Lara Lavelle-Langham and Victoria Shaw and William Greenhalf and Thomas Edwards and David Lalloo and Edwards, \{Christopher J.\} and Darby, \{Alistair C.\} and Carroll, \{Miles W.\} and Gareth Griffiths and Khoo, \{Saye H.\} and Hiscox, \{Julian A.\} and Tom Fletcher",

year = "2022",

month = nov,

day = "26",

doi = "10.1038/s41467-022-34839-9",

language = "English",

volume = "13",

pages = "e7284",

journal = "Nature Communications",

issn = "2041-1723",

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Donovan-Banfield, I, Penrice-Randal, R, Goldswain, H, Rzeszutek, AM, Pilgrim, J, Bullock, K, Saunders, G, Northey, J, Dong, X, Ryan, Y, Reynolds, H, Tetlow, M, Walker, LE, FitzGerald, R, Hale, C, Lyon, R, Woods, C, Ahmad, S, Hadjiyiannakis, D, Periselneris, J, Knox, E, Middleton, C, Lavelle-Langham, L, Shaw, V, Greenhalf, W, Edwards, T , Lalloo, D, Edwards, CJ, Darby, AC, Carroll, MW, Griffiths, G, Khoo, SH, Hiscox, JA & Fletcher, T 2022, 'Characterisation of SARS-CoV-2 genomic variation in response to molnupiravir treatment in the AGILE Phase IIa clinical trial', Nature Communications, vol. 13, no. 1, 7284, pp. e7284. https://doi.org/10.1038/s41467-022-34839-9

TY - JOUR

T1 - Characterisation of SARS-CoV-2 genomic variation in response to molnupiravir treatment in the AGILE Phase IIa clinical trial

AU - Donovan-Banfield, I’ah

AU - Penrice-Randal, Rebekah

AU - Goldswain, Hannah

AU - Rzeszutek, Aleksandra M.

AU - Pilgrim, Jack

AU - Bullock, Katie

AU - Saunders, Geoffrey

AU - Northey, Josh

AU - Dong, Xiaofeng

AU - Ryan, Yan

AU - Reynolds, Helen

AU - Tetlow, Michelle

AU - Walker, Lauren E.

AU - FitzGerald, Richard

AU - Hale, Colin

AU - Lyon, Rebecca

AU - Woods, Christie

AU - Ahmad, Shazaad

AU - Hadjiyiannakis, Dennis

AU - Periselneris, Jimstan

AU - Knox, Emma

AU - Middleton, Calley

AU - Lavelle-Langham, Lara

AU - Shaw, Victoria

AU - Greenhalf, William

AU - Edwards, Thomas

AU - Lalloo, David

AU - Edwards, Christopher J.

AU - Darby, Alistair C.

AU - Carroll, Miles W.

AU - Griffiths, Gareth

AU - Khoo, Saye H.

AU - Hiscox, Julian A.

AU - Fletcher, Tom

PY - 2022/11/26

Y1 - 2022/11/26

N2 - Molnupiravir is an antiviral, currently approved by the UK Medicines and Healthcare products Regulatory Agency (MHRA) for treating at-risk COVID-19 patients, that induces lethal error catastrophe in SARS-CoV-2. How this drug-induced mechanism of action might impact the emergence of resistance mutations is unclear. To investigate this, we used samples from the AGILE Candidate Specific Trial (CST)−2 (clinical trial number NCT04746183). The primary outcomes of AGILE CST-2 were to measure the drug safety and antiviral efficacy of molnupiravir in humans (180 participants randomised 1:1 with placebo). Here, we describe the pre-specified exploratory virological endpoint of CST-2, which was to determine the possible genomic changes in SARS-CoV-2 induced by molnupiravir treatment. We use high-throughput amplicon sequencing and minor variant analysis to characterise viral genomics in each participant whose longitudinal samples (days 1, 3 and 5 post-randomisation) pass the viral genomic quality criteria (n = 59 for molnupiravir and n = 65 for placebo). Over the course of treatment, no specific mutations were associated with molnupiravir treatment. We find that molnupiravir significantly increased the transition:transversion mutation ratio in SARS-CoV-2, consistent with the model of lethal error catastrophe. This study highlights the utility of examining intra-host virus populations to strengthen the prediction, and surveillance, of potential treatment-emergent adaptations.

AB - Molnupiravir is an antiviral, currently approved by the UK Medicines and Healthcare products Regulatory Agency (MHRA) for treating at-risk COVID-19 patients, that induces lethal error catastrophe in SARS-CoV-2. How this drug-induced mechanism of action might impact the emergence of resistance mutations is unclear. To investigate this, we used samples from the AGILE Candidate Specific Trial (CST)−2 (clinical trial number NCT04746183). The primary outcomes of AGILE CST-2 were to measure the drug safety and antiviral efficacy of molnupiravir in humans (180 participants randomised 1:1 with placebo). Here, we describe the pre-specified exploratory virological endpoint of CST-2, which was to determine the possible genomic changes in SARS-CoV-2 induced by molnupiravir treatment. We use high-throughput amplicon sequencing and minor variant analysis to characterise viral genomics in each participant whose longitudinal samples (days 1, 3 and 5 post-randomisation) pass the viral genomic quality criteria (n = 59 for molnupiravir and n = 65 for placebo). Over the course of treatment, no specific mutations were associated with molnupiravir treatment. We find that molnupiravir significantly increased the transition:transversion mutation ratio in SARS-CoV-2, consistent with the model of lethal error catastrophe. This study highlights the utility of examining intra-host virus populations to strengthen the prediction, and surveillance, of potential treatment-emergent adaptations.

U2 - 10.1038/s41467-022-34839-9

DO - 10.1038/s41467-022-34839-9

M3 - Article

SN - 2041-1723

VL - 13

SP - e7284

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 7284

ER -

Characterisation of SARS-CoV-2 genomic variation in response to molnupiravir treatment in the AGILE Phase IIa clinical trial

Abstract

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