Hepmarc: A 96 week randomised controlled feasibility trial of add-on maraviroc in people with HIV and non-alcoholic fatty liver disease

OBJECTIVES: Maraviroc may reduce hepatic inflammation in people with HIV and non-alcoholic fatty liver disease (HIV-NAFLD) through CCR5-receptor antagonism, which warrants further exploration. METHODS: We performed an open-label 96-week randomised-controlled feasibility trial of maraviroc plus optim...

Descripción completa

Detalles Bibliográficos
Autores principales: Bradshaw, Daniel, Abramowicz, Iga, Bremner, Stephen, Verma, Sumita, Gilleece, Yvonne, Kirk, Sarah, Nelson, Mark, Housman, Rosalie, Miras, Helena, Orkin, Chloe, Fox, Ashini, Curnock, Michael, Jennings, Louise, Gompels, Mark, Clarke, Emily, Robinson, Rachel, Lambert, Pauline, Chadwick, David, Perry, Nicky
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10348519/
https://www.ncbi.nlm.nih.gov/pubmed/37450478
http://dx.doi.org/10.1371/journal.pone.0288598
_version_ 1785073682572378112
author Bradshaw, Daniel
Abramowicz, Iga
Bremner, Stephen
Verma, Sumita
Gilleece, Yvonne
Kirk, Sarah
Nelson, Mark
Housman, Rosalie
Miras, Helena
Orkin, Chloe
Fox, Ashini
Curnock, Michael
Jennings, Louise
Gompels, Mark
Clarke, Emily
Robinson, Rachel
Lambert, Pauline
Chadwick, David
Perry, Nicky
author_facet Bradshaw, Daniel
Abramowicz, Iga
Bremner, Stephen
Verma, Sumita
Gilleece, Yvonne
Kirk, Sarah
Nelson, Mark
Housman, Rosalie
Miras, Helena
Orkin, Chloe
Fox, Ashini
Curnock, Michael
Jennings, Louise
Gompels, Mark
Clarke, Emily
Robinson, Rachel
Lambert, Pauline
Chadwick, David
Perry, Nicky
author_sort Bradshaw, Daniel
collection PubMed
description OBJECTIVES: Maraviroc may reduce hepatic inflammation in people with HIV and non-alcoholic fatty liver disease (HIV-NAFLD) through CCR5-receptor antagonism, which warrants further exploration. METHODS: We performed an open-label 96-week randomised-controlled feasibility trial of maraviroc plus optimised background therapy (OBT) versus OBT alone, in a 1:1 ratio, for people with virologically-suppressed HIV-1 and NAFLD without cirrhosis. Dosing followed recommendations for HIV therapy in the Summary of Product Characteristics for maraviroc. The primary outcomes were safety, recruitment and retention rates, adherence and data completeness. Secondary outcomes included the change in Fibroscan-assessed liver stiffness measurements (LSM), controlled attenuation parameter (CAP) and Enhanced Liver Fibrosis (ELF) scores. RESULTS: Fifty-three participants (53/60, 88% of target) were recruited; 23 received maraviroc plus OBT; 89% were male; 19% had type 2 diabetes mellitus. The median baseline LSM, CAP & ELF scores were 6.2 (IQR 4.6–7.8) kPa, 325 (IQR 279–351) dB/m and 9.1 (IQR 8.6–9.6) respectively. Primary outcomes: all individuals eligible after screening were randomised; there was 92% (SD 6.6%) adherence to maraviroc [target >90%]; 83% (95%CI 70%-92%) participant retention [target >65%]; 5.5% of data were missing [target <20%]. There were noo Serious Adverse Reactions; mild-moderate intensity Adverse Reactions were reported by five participants (5/23, 22% (95%CI 5%-49%)) [target <10%]. All Adverse Reactions resolved. Secondary outcomes: no important differences were seen by treatment group for the change from baseline in LSM, CAP or ELF scores CONCLUSIONS: This feasibility study provides preliminary evidence of maraviroc safety amongst people with HIV-NAFLD, and acceptable recruitment, retention, and adherence rates. These data support a definitive randomised-controlled trial assessing maraviroc impact on hepatic steatosis and fibrosis. TRIAL REGISTRATION: Clinical trial registry: ISCRTN, registration number 31461655.
format Online
Article
Text
id pubmed-10348519
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-103485192023-07-15 Hepmarc: A 96 week randomised controlled feasibility trial of add-on maraviroc in people with HIV and non-alcoholic fatty liver disease Bradshaw, Daniel Abramowicz, Iga Bremner, Stephen Verma, Sumita Gilleece, Yvonne Kirk, Sarah Nelson, Mark Housman, Rosalie Miras, Helena Orkin, Chloe Fox, Ashini Curnock, Michael Jennings, Louise Gompels, Mark Clarke, Emily Robinson, Rachel Lambert, Pauline Chadwick, David Perry, Nicky PLoS One Research Article OBJECTIVES: Maraviroc may reduce hepatic inflammation in people with HIV and non-alcoholic fatty liver disease (HIV-NAFLD) through CCR5-receptor antagonism, which warrants further exploration. METHODS: We performed an open-label 96-week randomised-controlled feasibility trial of maraviroc plus optimised background therapy (OBT) versus OBT alone, in a 1:1 ratio, for people with virologically-suppressed HIV-1 and NAFLD without cirrhosis. Dosing followed recommendations for HIV therapy in the Summary of Product Characteristics for maraviroc. The primary outcomes were safety, recruitment and retention rates, adherence and data completeness. Secondary outcomes included the change in Fibroscan-assessed liver stiffness measurements (LSM), controlled attenuation parameter (CAP) and Enhanced Liver Fibrosis (ELF) scores. RESULTS: Fifty-three participants (53/60, 88% of target) were recruited; 23 received maraviroc plus OBT; 89% were male; 19% had type 2 diabetes mellitus. The median baseline LSM, CAP & ELF scores were 6.2 (IQR 4.6–7.8) kPa, 325 (IQR 279–351) dB/m and 9.1 (IQR 8.6–9.6) respectively. Primary outcomes: all individuals eligible after screening were randomised; there was 92% (SD 6.6%) adherence to maraviroc [target >90%]; 83% (95%CI 70%-92%) participant retention [target >65%]; 5.5% of data were missing [target <20%]. There were noo Serious Adverse Reactions; mild-moderate intensity Adverse Reactions were reported by five participants (5/23, 22% (95%CI 5%-49%)) [target <10%]. All Adverse Reactions resolved. Secondary outcomes: no important differences were seen by treatment group for the change from baseline in LSM, CAP or ELF scores CONCLUSIONS: This feasibility study provides preliminary evidence of maraviroc safety amongst people with HIV-NAFLD, and acceptable recruitment, retention, and adherence rates. These data support a definitive randomised-controlled trial assessing maraviroc impact on hepatic steatosis and fibrosis. TRIAL REGISTRATION: Clinical trial registry: ISCRTN, registration number 31461655. Public Library of Science 2023-07-14 /pmc/articles/PMC10348519/ /pubmed/37450478 http://dx.doi.org/10.1371/journal.pone.0288598 Text en © 2023 Bradshaw et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Bradshaw, Daniel
Abramowicz, Iga
Bremner, Stephen
Verma, Sumita
Gilleece, Yvonne
Kirk, Sarah
Nelson, Mark
Housman, Rosalie
Miras, Helena
Orkin, Chloe
Fox, Ashini
Curnock, Michael
Jennings, Louise
Gompels, Mark
Clarke, Emily
Robinson, Rachel
Lambert, Pauline
Chadwick, David
Perry, Nicky
Hepmarc: A 96 week randomised controlled feasibility trial of add-on maraviroc in people with HIV and non-alcoholic fatty liver disease
title Hepmarc: A 96 week randomised controlled feasibility trial of add-on maraviroc in people with HIV and non-alcoholic fatty liver disease
title_full Hepmarc: A 96 week randomised controlled feasibility trial of add-on maraviroc in people with HIV and non-alcoholic fatty liver disease
title_fullStr Hepmarc: A 96 week randomised controlled feasibility trial of add-on maraviroc in people with HIV and non-alcoholic fatty liver disease
title_full_unstemmed Hepmarc: A 96 week randomised controlled feasibility trial of add-on maraviroc in people with HIV and non-alcoholic fatty liver disease
title_short Hepmarc: A 96 week randomised controlled feasibility trial of add-on maraviroc in people with HIV and non-alcoholic fatty liver disease
title_sort hepmarc: a 96 week randomised controlled feasibility trial of add-on maraviroc in people with hiv and non-alcoholic fatty liver disease
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10348519/
https://www.ncbi.nlm.nih.gov/pubmed/37450478
http://dx.doi.org/10.1371/journal.pone.0288598
work_keys_str_mv AT bradshawdaniel hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT abramowicziga hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT bremnerstephen hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT vermasumita hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT gilleeceyvonne hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT kirksarah hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT nelsonmark hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT housmanrosalie hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT mirashelena hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT orkinchloe hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT foxashini hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT curnockmichael hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT jenningslouise hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT gompelsmark hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT clarkeemily hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT robinsonrachel hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT lambertpauline hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT chadwickdavid hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease
AT perrynicky hepmarca96weekrandomisedcontrolledfeasibilitytrialofaddonmaravirocinpeoplewithhivandnonalcoholicfattyliverdisease

Ejemplares similares