Systematic, comprehensive, evidence-based approach to identify neuroprotective interventions for motor neuron disease: Using systematic reviews to inform expert consensus

Charis Wong; Jenna M. Gregory; Jing Liao; Kieren Egan; Hanna M. Vesterinen; Aimal Ahmad Khan; Maarij Anwar; Caitlin Beagan; Fraser S. Brown; John Cafferkey; Alessandra Cardinali; Jane Yi Chiam; Claire Chiang; Victoria Collins; Joyce Dormido; Elizabeth Elliott; Peter Foley; Yu Cheng Foo; Lily Fulton-Humble; Angus B. Gane; Stella A. Glasmacher; Áine Heffernan; Kiran Jayaprakash; Nimesh Jayasuriya; Amina Kaddouri; Jamie Kiernan; Gavin Langlands; D. Leighton; Jiaming Liu; James Lyon; Arpan R. Mehta; Alyssa Meng; Vivienne Nguyen; Na Hyun Park; Suzanne Quigley; Yousuf Rashid; Andrea Salzinger; Bethany Shiell; Ankur Singh; Tim Soane; Alexandra Thompson; Olaf Tomala; Fergal M. Waldron; Bhuvaneish T. Selvaraj; Jeremy Chataway; Robert Swingler; Peter Connick; Suvankar Pal; Siddharthan Chandran; Malcolm Macleod

doi:10.1136/bmjopen-2022-064169

Systematic, comprehensive, evidence-based approach to identify neuroprotective interventions for motor neuron disease: Using systematic reviews to inform expert consensus

Charis Wong, Jenna M. Gregory, Jing Liao, Kieren Egan, Hanna M. Vesterinen, Aimal Ahmad Khan, Maarij Anwar, Caitlin Beagan, Fraser S. Brown, John Cafferkey, Alessandra Cardinali, Jane Yi Chiam, Claire Chiang, Victoria Collins, Joyce Dormido, Elizabeth Elliott, Peter Foley, Yu Cheng Foo, Lily Fulton-Humble, Angus B. GaneStella A. Glasmacher, Áine Heffernan, Kiran Jayaprakash, Nimesh Jayasuriya, Amina Kaddouri, Jamie Kiernan, Gavin Langlands, D. Leighton, Jiaming Liu, James Lyon, Arpan R. Mehta, Alyssa Meng, Vivienne Nguyen, Na Hyun Park, Suzanne Quigley, Yousuf Rashid, Andrea Salzinger, Bethany Shiell, Ankur Singh, Tim Soane, Alexandra Thompson, Olaf Tomala, Fergal M. Waldron, Bhuvaneish T. Selvaraj, Jeremy Chataway, Robert Swingler, Peter Connick, Suvankar Pal, Siddharthan Chandran, Malcolm Macleod^*

^*Corresponding author for this work

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

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Abstract

Objectives Motor neuron disease (MND) is an incurable progressive neurodegenerative disease with limited treatment options. There is a pressing need for innovation in identifying therapies to take to clinical trial. Here, we detail a systematic and structured evidence-based approach to inform consensus decision making to select the first two drugs for evaluation in Motor Neuron Disease-Systematic Multi-arm Adaptive Randomised Trial (MND-SMART: NCT04302870), an adaptive platform trial. We aim to identify and prioritise candidate drugs which have the best available evidence for efficacy, acceptable safety profiles and are feasible for evaluation within the trial protocol. Methods We conducted a two-stage systematic review to identify potential neuroprotective interventions. First, we reviewed clinical studies in MND, Alzheimer's disease, Huntington's disease, Parkinson's disease and multiple sclerosis, identifying drugs described in at least one MND publication or publications in two or more other diseases. We scored and ranked drugs using a metric evaluating safety, efficacy, study size and study quality. In stage two, we reviewed efficacy of drugs in MND animal models, multicellular eukaryotic models and human induced pluripotent stem cell (iPSC) studies. An expert panel reviewed candidate drugs over two shortlisting rounds and a final selection round, considering the systematic review findings, late breaking evidence, mechanistic plausibility, safety, tolerability and feasibility of evaluation in MND-SMART. Results From the clinical review, we identified 595 interventions. 66 drugs met our drug/disease logic. Of these, 22 drugs with supportive clinical and preclinical evidence were shortlisted at round 1. Seven drugs proceeded to round 2. The panel reached a consensus to evaluate memantine and trazodone as the first two arms of MND-SMART. Discussion For future drug selection, we will incorporate automation tools, text-mining and machine learning techniques to the systematic reviews and consider data generated from other domains, including high-throughput phenotypic screening of human iPSCs.

Original language	English
Article number	e064169
Number of pages	14
Journal	BMJ Open
Volume	13
Issue number	2
Early online date	1 Feb 2023
DOIs	https://doi.org/10.1136/bmjopen-2022-064169
Publication status	Published - Feb 2023

Bibliographical note

Funding Information:
For the purpose of open access, the authors have applied a Creative Commons Attribution (CC BY) licence to any Author Accepted Manuscript version arising from this submission. MND-SMART is funded by grants from MND Scotland, My Name’5 Doddie Foundation (DOD/14/15) and specific donations to the Euan MacDonald Centre. The Chandran lab is supported by the UK Dementia Research Institute, which receives its funding from UK DRI Ltd, funded by the UK Medical Research Council, Alzheimer’s Society and Alzheimer’s Research UK. EE is a clinical academic fellow jointly funded by MND Scotland (MNDS) and the Chief Scientist Office (CSO) (217ARF R45951). ARM was a Lady Edith Wolfson Clinical Fellow, jointly funded by the Medical Research Council (MRC) and the Motor Neurone Disease Association (MR/R001162/1). ASalzinger is funded by Marie Sklodowska-Curie actions Innovative Training Network (ITN). BTS is funded by Rowling fellowship.

Keywords

Adult neurology
Clinical trials
Motor neurone disease
NEUROLOGY
THERAPEUTICS

UN SDGs

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

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Cite this

Wong, C., Gregory, J. M., Liao, J., Egan, K., Vesterinen, H. M., Ahmad Khan, A., Anwar, M., Beagan, C., Brown, F. S., Cafferkey, J., Cardinali, A., Chiam, J. Y., Chiang, C., Collins, V., Dormido, J., Elliott, E., Foley, P., Foo, Y. C., Fulton-Humble, L., ... Macleod, M. (2023). Systematic, comprehensive, evidence-based approach to identify neuroprotective interventions for motor neuron disease: Using systematic reviews to inform expert consensus. BMJ Open, 13(2), Article e064169. https://doi.org/10.1136/bmjopen-2022-064169

Wong, C, Gregory, JM, Liao, J, Egan, K, Vesterinen, HM, Ahmad Khan, A, Anwar, M, Beagan, C, Brown, FS, Cafferkey, J, Cardinali, A, Chiam, JY, Chiang, C, Collins, V, Dormido, J, Elliott, E, Foley, P, Foo, YC, Fulton-Humble, L, Gane, AB, Glasmacher, SA, Heffernan, Á, Jayaprakash, K, Jayasuriya, N, Kaddouri, A, Kiernan, J, Langlands, G, Leighton, D, Liu, J, Lyon, J, Mehta, AR, Meng, A, Nguyen, V, Park, NH, Quigley, S, Rashid, Y, Salzinger, A, Shiell, B, Singh, A, Soane, T, Thompson, A, Tomala, O, Waldron, FM, Selvaraj, BT, Chataway, J, Swingler, R, Connick, P, Pal, S, Chandran, S & Macleod, M 2023, 'Systematic, comprehensive, evidence-based approach to identify neuroprotective interventions for motor neuron disease: Using systematic reviews to inform expert consensus', BMJ Open, vol. 13, no. 2, e064169. https://doi.org/10.1136/bmjopen-2022-064169

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title = "Systematic, comprehensive, evidence-based approach to identify neuroprotective interventions for motor neuron disease: Using systematic reviews to inform expert consensus",

abstract = "Objectives Motor neuron disease (MND) is an incurable progressive neurodegenerative disease with limited treatment options. There is a pressing need for innovation in identifying therapies to take to clinical trial. Here, we detail a systematic and structured evidence-based approach to inform consensus decision making to select the first two drugs for evaluation in Motor Neuron Disease-Systematic Multi-arm Adaptive Randomised Trial (MND-SMART: NCT04302870), an adaptive platform trial. We aim to identify and prioritise candidate drugs which have the best available evidence for efficacy, acceptable safety profiles and are feasible for evaluation within the trial protocol. Methods We conducted a two-stage systematic review to identify potential neuroprotective interventions. First, we reviewed clinical studies in MND, Alzheimer's disease, Huntington's disease, Parkinson's disease and multiple sclerosis, identifying drugs described in at least one MND publication or publications in two or more other diseases. We scored and ranked drugs using a metric evaluating safety, efficacy, study size and study quality. In stage two, we reviewed efficacy of drugs in MND animal models, multicellular eukaryotic models and human induced pluripotent stem cell (iPSC) studies. An expert panel reviewed candidate drugs over two shortlisting rounds and a final selection round, considering the systematic review findings, late breaking evidence, mechanistic plausibility, safety, tolerability and feasibility of evaluation in MND-SMART. Results From the clinical review, we identified 595 interventions. 66 drugs met our drug/disease logic. Of these, 22 drugs with supportive clinical and preclinical evidence were shortlisted at round 1. Seven drugs proceeded to round 2. The panel reached a consensus to evaluate memantine and trazodone as the first two arms of MND-SMART. Discussion For future drug selection, we will incorporate automation tools, text-mining and machine learning techniques to the systematic reviews and consider data generated from other domains, including high-throughput phenotypic screening of human iPSCs.",

keywords = "Adult neurology, Clinical trials, Motor neurone disease, NEUROLOGY, THERAPEUTICS",

author = "Charis Wong and Gregory, {Jenna M.} and Jing Liao and Kieren Egan and Vesterinen, {Hanna M.} and {Ahmad Khan}, Aimal and Maarij Anwar and Caitlin Beagan and Brown, {Fraser S.} and John Cafferkey and Alessandra Cardinali and Chiam, {Jane Yi} and Claire Chiang and Victoria Collins and Joyce Dormido and Elizabeth Elliott and Peter Foley and Foo, {Yu Cheng} and Lily Fulton-Humble and Gane, {Angus B.} and Glasmacher, {Stella A.} and {\'A}ine Heffernan and Kiran Jayaprakash and Nimesh Jayasuriya and Amina Kaddouri and Jamie Kiernan and Gavin Langlands and D. Leighton and Jiaming Liu and James Lyon and Mehta, {Arpan R.} and Alyssa Meng and Vivienne Nguyen and Park, {Na Hyun} and Suzanne Quigley and Yousuf Rashid and Andrea Salzinger and Bethany Shiell and Ankur Singh and Tim Soane and Alexandra Thompson and Olaf Tomala and Waldron, {Fergal M.} and Selvaraj, {Bhuvaneish T.} and Jeremy Chataway and Robert Swingler and Peter Connick and Suvankar Pal and Siddharthan Chandran and Malcolm Macleod",

note = "Funding Information: For the purpose of open access, the authors have applied a Creative Commons Attribution (CC BY) licence to any Author Accepted Manuscript version arising from this submission. MND-SMART is funded by grants from MND Scotland, My Name{\textquoteright}5 Doddie Foundation (DOD/14/15) and specific donations to the Euan MacDonald Centre. The Chandran lab is supported by the UK Dementia Research Institute, which receives its funding from UK DRI Ltd, funded by the UK Medical Research Council, Alzheimer{\textquoteright}s Society and Alzheimer{\textquoteright}s Research UK. EE is a clinical academic fellow jointly funded by MND Scotland (MNDS) and the Chief Scientist Office (CSO) (217ARF R45951). ARM was a Lady Edith Wolfson Clinical Fellow, jointly funded by the Medical Research Council (MRC) and the Motor Neurone Disease Association (MR/R001162/1). ASalzinger is funded by Marie Sklodowska-Curie actions Innovative Training Network (ITN). BTS is funded by Rowling fellowship. ",

year = "2023",

month = feb,

doi = "10.1136/bmjopen-2022-064169",

language = "English",

volume = "13",

journal = "BMJ Open",

issn = "2044-6055",

publisher = "BMJ Publishing Group",

number = "2",

}

TY - JOUR

T1 - Systematic, comprehensive, evidence-based approach to identify neuroprotective interventions for motor neuron disease

T2 - Using systematic reviews to inform expert consensus

AU - Wong, Charis

AU - Gregory, Jenna M.

AU - Liao, Jing

AU - Egan, Kieren

AU - Vesterinen, Hanna M.

AU - Ahmad Khan, Aimal

AU - Anwar, Maarij

AU - Beagan, Caitlin

AU - Brown, Fraser S.

AU - Cafferkey, John

AU - Cardinali, Alessandra

AU - Chiam, Jane Yi

AU - Chiang, Claire

AU - Collins, Victoria

AU - Dormido, Joyce

AU - Elliott, Elizabeth

AU - Foley, Peter

AU - Foo, Yu Cheng

AU - Fulton-Humble, Lily

AU - Gane, Angus B.

AU - Glasmacher, Stella A.

AU - Heffernan, Áine

AU - Jayaprakash, Kiran

AU - Jayasuriya, Nimesh

AU - Kaddouri, Amina

AU - Kiernan, Jamie

AU - Langlands, Gavin

AU - Leighton, D.

AU - Liu, Jiaming

AU - Lyon, James

AU - Mehta, Arpan R.

AU - Meng, Alyssa

AU - Nguyen, Vivienne

AU - Park, Na Hyun

AU - Quigley, Suzanne

AU - Rashid, Yousuf

AU - Salzinger, Andrea

AU - Shiell, Bethany

AU - Singh, Ankur

AU - Soane, Tim

AU - Thompson, Alexandra

AU - Tomala, Olaf

AU - Waldron, Fergal M.

AU - Selvaraj, Bhuvaneish T.

AU - Chataway, Jeremy

AU - Swingler, Robert

AU - Connick, Peter

AU - Pal, Suvankar

AU - Chandran, Siddharthan

AU - Macleod, Malcolm

N1 - Funding Information: For the purpose of open access, the authors have applied a Creative Commons Attribution (CC BY) licence to any Author Accepted Manuscript version arising from this submission. MND-SMART is funded by grants from MND Scotland, My Name’5 Doddie Foundation (DOD/14/15) and specific donations to the Euan MacDonald Centre. The Chandran lab is supported by the UK Dementia Research Institute, which receives its funding from UK DRI Ltd, funded by the UK Medical Research Council, Alzheimer’s Society and Alzheimer’s Research UK. EE is a clinical academic fellow jointly funded by MND Scotland (MNDS) and the Chief Scientist Office (CSO) (217ARF R45951). ARM was a Lady Edith Wolfson Clinical Fellow, jointly funded by the Medical Research Council (MRC) and the Motor Neurone Disease Association (MR/R001162/1). ASalzinger is funded by Marie Sklodowska-Curie actions Innovative Training Network (ITN). BTS is funded by Rowling fellowship.

PY - 2023/2

Y1 - 2023/2

N2 - Objectives Motor neuron disease (MND) is an incurable progressive neurodegenerative disease with limited treatment options. There is a pressing need for innovation in identifying therapies to take to clinical trial. Here, we detail a systematic and structured evidence-based approach to inform consensus decision making to select the first two drugs for evaluation in Motor Neuron Disease-Systematic Multi-arm Adaptive Randomised Trial (MND-SMART: NCT04302870), an adaptive platform trial. We aim to identify and prioritise candidate drugs which have the best available evidence for efficacy, acceptable safety profiles and are feasible for evaluation within the trial protocol. Methods We conducted a two-stage systematic review to identify potential neuroprotective interventions. First, we reviewed clinical studies in MND, Alzheimer's disease, Huntington's disease, Parkinson's disease and multiple sclerosis, identifying drugs described in at least one MND publication or publications in two or more other diseases. We scored and ranked drugs using a metric evaluating safety, efficacy, study size and study quality. In stage two, we reviewed efficacy of drugs in MND animal models, multicellular eukaryotic models and human induced pluripotent stem cell (iPSC) studies. An expert panel reviewed candidate drugs over two shortlisting rounds and a final selection round, considering the systematic review findings, late breaking evidence, mechanistic plausibility, safety, tolerability and feasibility of evaluation in MND-SMART. Results From the clinical review, we identified 595 interventions. 66 drugs met our drug/disease logic. Of these, 22 drugs with supportive clinical and preclinical evidence were shortlisted at round 1. Seven drugs proceeded to round 2. The panel reached a consensus to evaluate memantine and trazodone as the first two arms of MND-SMART. Discussion For future drug selection, we will incorporate automation tools, text-mining and machine learning techniques to the systematic reviews and consider data generated from other domains, including high-throughput phenotypic screening of human iPSCs.

AB - Objectives Motor neuron disease (MND) is an incurable progressive neurodegenerative disease with limited treatment options. There is a pressing need for innovation in identifying therapies to take to clinical trial. Here, we detail a systematic and structured evidence-based approach to inform consensus decision making to select the first two drugs for evaluation in Motor Neuron Disease-Systematic Multi-arm Adaptive Randomised Trial (MND-SMART: NCT04302870), an adaptive platform trial. We aim to identify and prioritise candidate drugs which have the best available evidence for efficacy, acceptable safety profiles and are feasible for evaluation within the trial protocol. Methods We conducted a two-stage systematic review to identify potential neuroprotective interventions. First, we reviewed clinical studies in MND, Alzheimer's disease, Huntington's disease, Parkinson's disease and multiple sclerosis, identifying drugs described in at least one MND publication or publications in two or more other diseases. We scored and ranked drugs using a metric evaluating safety, efficacy, study size and study quality. In stage two, we reviewed efficacy of drugs in MND animal models, multicellular eukaryotic models and human induced pluripotent stem cell (iPSC) studies. An expert panel reviewed candidate drugs over two shortlisting rounds and a final selection round, considering the systematic review findings, late breaking evidence, mechanistic plausibility, safety, tolerability and feasibility of evaluation in MND-SMART. Results From the clinical review, we identified 595 interventions. 66 drugs met our drug/disease logic. Of these, 22 drugs with supportive clinical and preclinical evidence were shortlisted at round 1. Seven drugs proceeded to round 2. The panel reached a consensus to evaluate memantine and trazodone as the first two arms of MND-SMART. Discussion For future drug selection, we will incorporate automation tools, text-mining and machine learning techniques to the systematic reviews and consider data generated from other domains, including high-throughput phenotypic screening of human iPSCs.

KW - Adult neurology

KW - Clinical trials

KW - Motor neurone disease

KW - NEUROLOGY

KW - THERAPEUTICS

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DO - 10.1136/bmjopen-2022-064169

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SN - 2044-6055

VL - 13

JO - BMJ Open

JF - BMJ Open

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ER -

Systematic, comprehensive, evidence-based approach to identify neuroprotective interventions for motor neuron disease: Using systematic reviews to inform expert consensus

Abstract

Bibliographical note

Keywords

UN SDGs

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