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Evaluating the population impact of hepatitis C direct acting antiviral treatment as prevention for people who inject drugs (EPIToPe) – a natural experiment (protocol)

INTRODUCTION: Hepatitis C virus (HCV) is the second largest contributor to liver disease in the UK, with injecting drug use as the main risk factor among the estimated 200 000 people currently infected. Despite effective prevention interventions, chronic HCV prevalence remains around 40% among peopl...

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Autores principales: Hickman, Matthew, Dillon, John F, Elliott, Lawrie, De Angelis, Daniela, Vickerman, Peter, Foster, Graham, Donnan, Peter, Eriksen, Ann, Flowers, Paul, Goldberg, David, Hollingworth, William, Ijaz, Samreen, Liddell, David, Mandal, Sema, Martin, Natasha, Beer, Lewis J Z, Drysdale, Kate, Fraser, Hannah, Glass, Rachel, Graham, Lesley, Gunson, Rory N, Hamilton, Emma, Harris, Helen, Harris, Magdalena, Harris, Ross, Heinsbroek, Ellen, Hope, Vivian, Horwood, Jeremy, Inglis, Sarah Karen, Innes, Hamish, Lane, Athene, Meadows, Jade, McAuley, Andrew, Metcalfe, Chris, Migchelsen, Stephanie, Murray, Alex, Myring, Gareth, Palmateer, Norah E, Presanis, Anne, Radley, Andrew, Ramsay, Mary, Samartsidis, Pantelis, Simmons, Ruth, Sinka, Katy, Vojt, Gabriele, Ward, Zoe, Whiteley, David, Yeung, Alan, Hutchinson, Sharon J
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BMJ Publishing Group 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6773339/
https://www.ncbi.nlm.nih.gov/pubmed/31551376
http://dx.doi.org/10.1136/bmjopen-2019-029538
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author Hickman, Matthew
Dillon, John F
Elliott, Lawrie
De Angelis, Daniela
Vickerman, Peter
Foster, Graham
Donnan, Peter
Eriksen, Ann
Flowers, Paul
Goldberg, David
Hollingworth, William
Ijaz, Samreen
Liddell, David
Mandal, Sema
Martin, Natasha
Beer, Lewis J Z
Drysdale, Kate
Fraser, Hannah
Glass, Rachel
Graham, Lesley
Gunson, Rory N
Hamilton, Emma
Harris, Helen
Harris, Magdalena
Harris, Ross
Heinsbroek, Ellen
Hope, Vivian
Horwood, Jeremy
Inglis, Sarah Karen
Innes, Hamish
Lane, Athene
Meadows, Jade
McAuley, Andrew
Metcalfe, Chris
Migchelsen, Stephanie
Murray, Alex
Myring, Gareth
Palmateer, Norah E
Presanis, Anne
Radley, Andrew
Ramsay, Mary
Samartsidis, Pantelis
Simmons, Ruth
Sinka, Katy
Vojt, Gabriele
Ward, Zoe
Whiteley, David
Yeung, Alan
Hutchinson, Sharon J
author_facet Hickman, Matthew
Dillon, John F
Elliott, Lawrie
De Angelis, Daniela
Vickerman, Peter
Foster, Graham
Donnan, Peter
Eriksen, Ann
Flowers, Paul
Goldberg, David
Hollingworth, William
Ijaz, Samreen
Liddell, David
Mandal, Sema
Martin, Natasha
Beer, Lewis J Z
Drysdale, Kate
Fraser, Hannah
Glass, Rachel
Graham, Lesley
Gunson, Rory N
Hamilton, Emma
Harris, Helen
Harris, Magdalena
Harris, Ross
Heinsbroek, Ellen
Hope, Vivian
Horwood, Jeremy
Inglis, Sarah Karen
Innes, Hamish
Lane, Athene
Meadows, Jade
McAuley, Andrew
Metcalfe, Chris
Migchelsen, Stephanie
Murray, Alex
Myring, Gareth
Palmateer, Norah E
Presanis, Anne
Radley, Andrew
Ramsay, Mary
Samartsidis, Pantelis
Simmons, Ruth
Sinka, Katy
Vojt, Gabriele
Ward, Zoe
Whiteley, David
Yeung, Alan
Hutchinson, Sharon J
author_sort Hickman, Matthew
collection PubMed
description INTRODUCTION: Hepatitis C virus (HCV) is the second largest contributor to liver disease in the UK, with injecting drug use as the main risk factor among the estimated 200 000 people currently infected. Despite effective prevention interventions, chronic HCV prevalence remains around 40% among people who inject drugs (PWID). New direct-acting antiviral (DAA) HCV therapies combine high cure rates (>90%) and short treatment duration (8 to 12 weeks). Theoretical mathematical modelling evidence suggests HCV treatment scale-up can prevent transmission and substantially reduce HCV prevalence/incidence among PWID. Our primary aim is to generate empirical evidence on the effectiveness of HCV ‘Treatment as Prevention’ (TasP) in PWID. METHODS AND ANALYSIS: We plan to establish a natural experiment with Tayside, Scotland, as a single intervention site where HCV care pathways are being expanded (including specialist drug treatment clinics, needle and syringe programmes (NSPs), pharmacies and prison) and HCV treatment for PWID is being rapidly scaled-up. Other sites in Scotland and England will act as potential controls. Over 2 years from 2017/2018, at least 500 PWID will be treated in Tayside, which simulation studies project will reduce chronic HCV prevalence among PWID by 62% (from 26% to 10%) and HCV incidence will fall by approximately 2/3 (from 4.2 per 100 person-years (p100py) to 1.4 p100py). Treatment response and re-infection rates will be monitored. We will conduct focus groups and interviews with service providers and patients that accept and decline treatment to identify barriers and facilitators in implementing TasP. We will conduct longitudinal interviews with up to 40 PWID to assess whether successful HCV treatment alters their perspectives on and engagement with drug treatment and recovery. Trained peer researchers will be involved in data collection and dissemination. The primary outcome – chronic HCV prevalence in PWID – is measured using information from the Needle Exchange Surveillance Initiative survey in Scotland and the Unlinked Anonymous Monitoring Programme in England, conducted at least four times before and three times during and after the intervention. We will adapt Bayesian synthetic control methods (specifically the Causal Impact Method) to generate the cumulative impact of the intervention on chronic HCV prevalence and incidence. We will use a dynamic HCV transmission and economic model to evaluate the cost-effectiveness of the HCV TasP intervention, and to estimate the contribution of the scale-up in HCV treatment to observe changes in HCV prevalence. Through the qualitative data we will systematically explore key mechanisms of TasP real world implementation from provider and patient perspectives to develop a manual for scaling up HCV treatment in other settings. We will compare qualitative accounts of drug treatment and recovery with a ‘virtual cohort’ of PWID linking information on HCV treatment with Scottish Drug treatment databases to test whether DAA treatment improves drug treatment outcomes. ETHICS AND DISSEMINATION: Extending HCV community care pathways is covered by ethics (ERADICATE C, ISRCTN27564683, Super DOT C Trial clinicaltrials.gov: NCT02706223). Ethical approval for extra data collection from patients including health utilities and qualitative interviews has been granted (REC ref: 18/ES/0128) and ISCRCTN registration has been completed (ISRCTN72038467). Our findings will have direct National Health Service and patient relevance; informing prioritisation given to early HCV treatment for PWID. We will present findings to practitioners and policymakers, and support design of an evaluation of HCV TasP in England.
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spelling pubmed-67733392019-10-21 Evaluating the population impact of hepatitis C direct acting antiviral treatment as prevention for people who inject drugs (EPIToPe) – a natural experiment (protocol) Hickman, Matthew Dillon, John F Elliott, Lawrie De Angelis, Daniela Vickerman, Peter Foster, Graham Donnan, Peter Eriksen, Ann Flowers, Paul Goldberg, David Hollingworth, William Ijaz, Samreen Liddell, David Mandal, Sema Martin, Natasha Beer, Lewis J Z Drysdale, Kate Fraser, Hannah Glass, Rachel Graham, Lesley Gunson, Rory N Hamilton, Emma Harris, Helen Harris, Magdalena Harris, Ross Heinsbroek, Ellen Hope, Vivian Horwood, Jeremy Inglis, Sarah Karen Innes, Hamish Lane, Athene Meadows, Jade McAuley, Andrew Metcalfe, Chris Migchelsen, Stephanie Murray, Alex Myring, Gareth Palmateer, Norah E Presanis, Anne Radley, Andrew Ramsay, Mary Samartsidis, Pantelis Simmons, Ruth Sinka, Katy Vojt, Gabriele Ward, Zoe Whiteley, David Yeung, Alan Hutchinson, Sharon J BMJ Open Public Health INTRODUCTION: Hepatitis C virus (HCV) is the second largest contributor to liver disease in the UK, with injecting drug use as the main risk factor among the estimated 200 000 people currently infected. Despite effective prevention interventions, chronic HCV prevalence remains around 40% among people who inject drugs (PWID). New direct-acting antiviral (DAA) HCV therapies combine high cure rates (>90%) and short treatment duration (8 to 12 weeks). Theoretical mathematical modelling evidence suggests HCV treatment scale-up can prevent transmission and substantially reduce HCV prevalence/incidence among PWID. Our primary aim is to generate empirical evidence on the effectiveness of HCV ‘Treatment as Prevention’ (TasP) in PWID. METHODS AND ANALYSIS: We plan to establish a natural experiment with Tayside, Scotland, as a single intervention site where HCV care pathways are being expanded (including specialist drug treatment clinics, needle and syringe programmes (NSPs), pharmacies and prison) and HCV treatment for PWID is being rapidly scaled-up. Other sites in Scotland and England will act as potential controls. Over 2 years from 2017/2018, at least 500 PWID will be treated in Tayside, which simulation studies project will reduce chronic HCV prevalence among PWID by 62% (from 26% to 10%) and HCV incidence will fall by approximately 2/3 (from 4.2 per 100 person-years (p100py) to 1.4 p100py). Treatment response and re-infection rates will be monitored. We will conduct focus groups and interviews with service providers and patients that accept and decline treatment to identify barriers and facilitators in implementing TasP. We will conduct longitudinal interviews with up to 40 PWID to assess whether successful HCV treatment alters their perspectives on and engagement with drug treatment and recovery. Trained peer researchers will be involved in data collection and dissemination. The primary outcome – chronic HCV prevalence in PWID – is measured using information from the Needle Exchange Surveillance Initiative survey in Scotland and the Unlinked Anonymous Monitoring Programme in England, conducted at least four times before and three times during and after the intervention. We will adapt Bayesian synthetic control methods (specifically the Causal Impact Method) to generate the cumulative impact of the intervention on chronic HCV prevalence and incidence. We will use a dynamic HCV transmission and economic model to evaluate the cost-effectiveness of the HCV TasP intervention, and to estimate the contribution of the scale-up in HCV treatment to observe changes in HCV prevalence. Through the qualitative data we will systematically explore key mechanisms of TasP real world implementation from provider and patient perspectives to develop a manual for scaling up HCV treatment in other settings. We will compare qualitative accounts of drug treatment and recovery with a ‘virtual cohort’ of PWID linking information on HCV treatment with Scottish Drug treatment databases to test whether DAA treatment improves drug treatment outcomes. ETHICS AND DISSEMINATION: Extending HCV community care pathways is covered by ethics (ERADICATE C, ISRCTN27564683, Super DOT C Trial clinicaltrials.gov: NCT02706223). Ethical approval for extra data collection from patients including health utilities and qualitative interviews has been granted (REC ref: 18/ES/0128) and ISCRCTN registration has been completed (ISRCTN72038467). Our findings will have direct National Health Service and patient relevance; informing prioritisation given to early HCV treatment for PWID. We will present findings to practitioners and policymakers, and support design of an evaluation of HCV TasP in England. BMJ Publishing Group 2019-09-24 /pmc/articles/PMC6773339/ /pubmed/31551376 http://dx.doi.org/10.1136/bmjopen-2019-029538 Text en © Author(s) (or their employer(s)) 2019. Re-use permitted under CC BY. Published by BMJ. This is an open access article distributed in accordance with the Creative Commons Attribution 4.0 Unported (CC BY 4.0) license, which permits others to copy, redistribute, remix, transform and build upon this work for any purpose, provided the original work is properly cited, a link to the licence is given, and indication of whether changes were made. See: https://creativecommons.org/licenses/by/4.0/.
spellingShingle Public Health
Hickman, Matthew
Dillon, John F
Elliott, Lawrie
De Angelis, Daniela
Vickerman, Peter
Foster, Graham
Donnan, Peter
Eriksen, Ann
Flowers, Paul
Goldberg, David
Hollingworth, William
Ijaz, Samreen
Liddell, David
Mandal, Sema
Martin, Natasha
Beer, Lewis J Z
Drysdale, Kate
Fraser, Hannah
Glass, Rachel
Graham, Lesley
Gunson, Rory N
Hamilton, Emma
Harris, Helen
Harris, Magdalena
Harris, Ross
Heinsbroek, Ellen
Hope, Vivian
Horwood, Jeremy
Inglis, Sarah Karen
Innes, Hamish
Lane, Athene
Meadows, Jade
McAuley, Andrew
Metcalfe, Chris
Migchelsen, Stephanie
Murray, Alex
Myring, Gareth
Palmateer, Norah E
Presanis, Anne
Radley, Andrew
Ramsay, Mary
Samartsidis, Pantelis
Simmons, Ruth
Sinka, Katy
Vojt, Gabriele
Ward, Zoe
Whiteley, David
Yeung, Alan
Hutchinson, Sharon J
Evaluating the population impact of hepatitis C direct acting antiviral treatment as prevention for people who inject drugs (EPIToPe) – a natural experiment (protocol)
title Evaluating the population impact of hepatitis C direct acting antiviral treatment as prevention for people who inject drugs (EPIToPe) – a natural experiment (protocol)
title_full Evaluating the population impact of hepatitis C direct acting antiviral treatment as prevention for people who inject drugs (EPIToPe) – a natural experiment (protocol)
title_fullStr Evaluating the population impact of hepatitis C direct acting antiviral treatment as prevention for people who inject drugs (EPIToPe) – a natural experiment (protocol)
title_full_unstemmed Evaluating the population impact of hepatitis C direct acting antiviral treatment as prevention for people who inject drugs (EPIToPe) – a natural experiment (protocol)
title_short Evaluating the population impact of hepatitis C direct acting antiviral treatment as prevention for people who inject drugs (EPIToPe) – a natural experiment (protocol)
title_sort evaluating the population impact of hepatitis c direct acting antiviral treatment as prevention for people who inject drugs (epitope) – a natural experiment (protocol)
topic Public Health
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6773339/
https://www.ncbi.nlm.nih.gov/pubmed/31551376
http://dx.doi.org/10.1136/bmjopen-2019-029538
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