Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study

the AIDS Therapy Evaluation in the Netherlands (ATHENA) Observational HIV Cohort; Patrick G A Oomen; Ferdinand Wit; Kees Brinkman; Saskia M E Vrouenraets; T Mudrikova; Marc van der Valk

doi:10.1016/s2352-3018(24)00150-4

Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study

the AIDS Therapy Evaluation in the Netherlands (ATHENA) Observational HIV Cohort, Patrick G A Oomen, Ferdinand Wit, Kees Brinkman, Saskia M E Vrouenraets, T Mudrikova, Marc van der Valk

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

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Abstract

Background: Currently, real-world data on doravirine are scarce. In a national prospective cohort, we assessed the effectiveness and tolerability of switching to doravirine-based antiretroviral therapy (ART) in people with HIV. Methods: We did a nationwide, matched, prospective cohort study of people with HIV without previous virological failure and stable for at least 12 months on non-doravirine-containing triple or dual ART switching to doravirine before Sept 1, 2020 (exposed group). Participants in the exposed group were matched 1:2 to individuals continuing stable non-doravirine-containing ART, on age, sex, HIV acquisition category, time since ART initiation, calendar time, pre-ART CD4-count, pre-ART plasma viral load (PVL) and anchor drug class before switching. The primary outcome was protocol-defined virological failure (PDVF; PVL of ≥200 copies per mL) in the intention-to-treat (ITT) population at week 104, with participants modifying their regimen or becoming lost to follow-up considered as PDVF (non-inferiority margin +5%). In contrast, in the on-treatment population, those who modified their regimen or became lost to follow-up were censored from that moment onwards. Tolerability was a secondary outcome. Findings: In total, 590 participants in the exposed group and 1180 participants in the unexposed group (of whom 55·3% used integrase strand transfer inhibitor-based regimens) were included. In the ITT analysis, PDVF occurred in 135 (22·9%) exposed participants and in 295 (25·0%) unexposed participants (risk difference –2·12%, upper limit of the one-sided 95% CI +1·40%). In the on-treatment analysis, 10 (2·2%) of 455 non-censored exposed participants and 26 (2·9%) of 885 non-censored unexposed participants had PDVF (risk difference –0·70%, upper limit of the one-sided 95% CI +0·73%). All exposed participants with a PVL of 200 copies or more per mL resuppressed without regimen modification: no confirmed virological failure (two consecutive PVLs of ≥200 copies per mL) was observed. 104 (17·6%) exposed participants and 211 (17·9%) unexposed participants modified their regimen. 73 (12.4%) exposed participants discontinued doravirine due to adverse events: abnormal dreams (1·7%) and insomnia (1·5%) were most common. Interpretation: Switching to doravirine in well suppressed people with HIV without previous virological failure was non-inferior compared with continuing non-doravirine-containing regimens after 2 years in a real-world setting. Funding: None.

Original language	English
Pages (from-to)	e576-e585
Journal	The Lancet HIV
Volume	11
Issue number	9
DOIs	https://doi.org/10.1016/s2352-3018(24)00150-4
Publication status	Published - Sept 2024

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the AIDS Therapy Evaluation in the Netherlands (ATHENA) Observational HIV Cohort, Oomen, P. G. A., Wit, F., Brinkman, K., Vrouenraets, S. M. E., Mudrikova, T., & van der Valk, M. (2024). Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study. The Lancet HIV, 11(9), e576-e585. https://doi.org/10.1016/s2352-3018(24)00150-4

@article{18884f4b35354001aea601c28c71d9de,

title = "Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study",

abstract = "Background: Currently, real-world data on doravirine are scarce. In a national prospective cohort, we assessed the effectiveness and tolerability of switching to doravirine-based antiretroviral therapy (ART) in people with HIV. Methods: We did a nationwide, matched, prospective cohort study of people with HIV without previous virological failure and stable for at least 12 months on non-doravirine-containing triple or dual ART switching to doravirine before Sept 1, 2020 (exposed group). Participants in the exposed group were matched 1:2 to individuals continuing stable non-doravirine-containing ART, on age, sex, HIV acquisition category, time since ART initiation, calendar time, pre-ART CD4-count, pre-ART plasma viral load (PVL) and anchor drug class before switching. The primary outcome was protocol-defined virological failure (PDVF; PVL of ≥200 copies per mL) in the intention-to-treat (ITT) population at week 104, with participants modifying their regimen or becoming lost to follow-up considered as PDVF (non-inferiority margin +5\%). In contrast, in the on-treatment population, those who modified their regimen or became lost to follow-up were censored from that moment onwards. Tolerability was a secondary outcome. Findings: In total, 590 participants in the exposed group and 1180 participants in the unexposed group (of whom 55·3\% used integrase strand transfer inhibitor-based regimens) were included. In the ITT analysis, PDVF occurred in 135 (22·9\%) exposed participants and in 295 (25·0\%) unexposed participants (risk difference –2·12\%, upper limit of the one-sided 95\% CI +1·40\%). In the on-treatment analysis, 10 (2·2\%) of 455 non-censored exposed participants and 26 (2·9\%) of 885 non-censored unexposed participants had PDVF (risk difference –0·70\%, upper limit of the one-sided 95\% CI +0·73\%). All exposed participants with a PVL of 200 copies or more per mL resuppressed without regimen modification: no confirmed virological failure (two consecutive PVLs of ≥200 copies per mL) was observed. 104 (17·6\%) exposed participants and 211 (17·9\%) unexposed participants modified their regimen. 73 (12.4\%) exposed participants discontinued doravirine due to adverse events: abnormal dreams (1·7\%) and insomnia (1·5\%) were most common. Interpretation: Switching to doravirine in well suppressed people with HIV without previous virological failure was non-inferior compared with continuing non-doravirine-containing regimens after 2 years in a real-world setting. Funding: None.",

author = "\{van Agtmael\}, \{M. A.\} and A. Goorhuis and Peters, \{E. J.G.\} and \{the AIDS Therapy Evaluation in the Netherlands (ATHENA) Observational HIV Cohort\} and Prins, \{J. M.\} and \{van Vugt\}, M. and Laan, \{L. M.\} and Cornelissen, \{M. T.E.\} and M. Jonges and Wolthers, \{K. C.\} and \{van den Berge\}, M. and S. Baas and \{van Arkel\}, A. and Pronk, \{M. J. H.\} and \{de Bree\}, C. and W. Alers and Nobel, \{H. E.\} and Berrevoets, \{M. A.H.\} and Brouwer, \{A. E.\} and C. Rokx and Anas, \{A. A.\} and Bax, \{H. I.\} and \{van Gorp\}, \{E. C.M.\} and \{de Mendon{\c c}a Melo\}, M. and \{van Nood\}, E. and Nouwen, \{J. L.\} and Rijnders, \{B. J.A.\} and Schurink, \{C. A.M.\} and L. Slobbe and \{de Vries-Sluijs\}, \{T. E.M.S.\} and N. Bassant and M. Vriesde and \{van Zonneveld\}, \{L. M.\} and \{de Groot\}, J. and \{van Kampen\}, \{J. J.A.\} and Koopmans, \{M. P.G.\} and J. Rahamat-Langendoen and Douma, \{R. A.\} and Mulder, \{M. A.\} and Schippers, \{E. F.\} and Gelinck, \{L. B.S.\} and F. Mollema and T. Nguyen and Groeneveld, \{P. H.P.\} and Lammers, \{A. J.J.\} and \{de Boer\}, \{M. G.J.\} and \{van der Sluis\}, D. and Claas, \{E. C.J.\} and \{den Hollander\}, \{J. G.\} and Brouwer, \{C. J.\} and E. Mulder and Smit, \{J. V.\} and \{van Niekerk\}, T. and O. Pontesilli and \{van Tienen\}, C. and A. Stoop and \{van Wolfswinkel\}, \{M. E.\} and J. Schippers and Kampschreur, \{L. M.\} and C. Timmer and S. Faber and J. Wagenaar and \{de Regt\}, M. and Schouten, \{W. E.M.\} and H. Blaauw and M. Knapen and M. Kok and M. Albers and \{de Haan\}, M. and M. McCall and J. Rahamat-Langendoen and D. Burger and M. Claassen and Hassing, \{R. J.\} and Verhagen, \{D. W.M.\} and \{van Wijk\}, M. and M. Bakker and Postma, \{D. F.\} and Schenk, \{H. M.\} and A. Boonstra and Niesters, \{H. G.M.\} and Bruns, \{A. H.W.\} and Hensgens, \{M. P.M.\} and Oosterheert, \{J. J.\} and A. Verbon and \{van der Valk\}, M. and Bezemer, \{D. O.\} and C. Smit and Wit, \{F. W.M.N.\} and D. Bergsma and Koster, \{L. E.\} and Lelivelt, \{K. J.\} and \{van de Sande\}, L. and Schoorl, \{M. J.C.\} and Visser, \{K. M.\} and \{van der Vliet\}, \{S. T.\} and \{van den Akker\}, M. and Bakker, \{Y. M.\} and M. Bezemer-Goedhart and \{El Hammoud\}, I. and Lucas, \{E. G.A.\} and Mulder, \{H. W.\} and \{van Veen\}, R. and Witte, \{E. C.M.\} and Oomen, \{Patrick G A\} and Ferdinand Wit and Kees Brinkman and Vrouenraets, \{Saskia M E\} and T Mudrikova and \{van der Valk\}, Marc",

year = "2024",

month = sep,

doi = "10.1016/s2352-3018(24)00150-4",

language = "English",

volume = "11",

pages = "e576--e585",

journal = "The Lancet HIV",

issn = "2352-3018",

publisher = "Elsevier Ltd.",

number = "9",

}

the AIDS Therapy Evaluation in the Netherlands (ATHENA) Observational HIV Cohort, Oomen, PGA, Wit, F, Brinkman, K, Vrouenraets, SME, Mudrikova, T & van der Valk, M 2024, 'Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study', The Lancet HIV, vol. 11, no. 9, pp. e576-e585. https://doi.org/10.1016/s2352-3018(24)00150-4

Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study. / the AIDS Therapy Evaluation in the Netherlands (ATHENA) Observational HIV Cohort; Oomen, Patrick G A; Wit, Ferdinand et al.
In: The Lancet HIV, Vol. 11, No. 9, 09.2024, p. e576-e585.

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

TY - JOUR

T1 - Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV

T2 - a nationwide, matched, prospective cohort study

AU - van Agtmael, M. A.

AU - Goorhuis, A.

AU - Peters, E. J.G.

AU - the AIDS Therapy Evaluation in the Netherlands (ATHENA) Observational HIV Cohort

AU - Prins, J. M.

AU - van Vugt, M.

AU - Laan, L. M.

AU - Cornelissen, M. T.E.

AU - Jonges, M.

AU - Wolthers, K. C.

AU - van den Berge, M.

AU - Baas, S.

AU - van Arkel, A.

AU - Pronk, M. J. H.

AU - de Bree, C.

AU - Alers, W.

AU - Nobel, H. E.

AU - Berrevoets, M. A.H.

AU - Brouwer, A. E.

AU - Rokx, C.

AU - Anas, A. A.

AU - Bax, H. I.

AU - van Gorp, E. C.M.

AU - de Mendonça Melo, M.

AU - van Nood, E.

AU - Nouwen, J. L.

AU - Rijnders, B. J.A.

AU - Schurink, C. A.M.

AU - Slobbe, L.

AU - de Vries-Sluijs, T. E.M.S.

AU - Bassant, N.

AU - Vriesde, M.

AU - van Zonneveld, L. M.

AU - de Groot, J.

AU - van Kampen, J. J.A.

AU - Koopmans, M. P.G.

AU - Rahamat-Langendoen, J.

AU - Douma, R. A.

AU - Mulder, M. A.

AU - Schippers, E. F.

AU - Gelinck, L. B.S.

AU - Mollema, F.

AU - Nguyen, T.

AU - Groeneveld, P. H.P.

AU - Lammers, A. J.J.

AU - de Boer, M. G.J.

AU - van der Sluis, D.

AU - Claas, E. C.J.

AU - den Hollander, J. G.

AU - Brouwer, C. J.

AU - Mulder, E.

AU - Smit, J. V.

AU - van Niekerk, T.

AU - Pontesilli, O.

AU - van Tienen, C.

AU - Stoop, A.

AU - van Wolfswinkel, M. E.

AU - Schippers, J.

AU - Kampschreur, L. M.

AU - Timmer, C.

AU - Faber, S.

AU - Wagenaar, J.

AU - de Regt, M.

AU - Schouten, W. E.M.

AU - Blaauw, H.

AU - Knapen, M.

AU - Kok, M.

AU - Albers, M.

AU - de Haan, M.

AU - McCall, M.

AU - Rahamat-Langendoen, J.

AU - Burger, D.

AU - Claassen, M.

AU - Hassing, R. J.

AU - Verhagen, D. W.M.

AU - van Wijk, M.

AU - Bakker, M.

AU - Postma, D. F.

AU - Schenk, H. M.

AU - Boonstra, A.

AU - Niesters, H. G.M.

AU - Bruns, A. H.W.

AU - Hensgens, M. P.M.

AU - Oosterheert, J. J.

AU - Verbon, A.

AU - van der Valk, M.

AU - Bezemer, D. O.

AU - Smit, C.

AU - Wit, F. W.M.N.

AU - Bergsma, D.

AU - Koster, L. E.

AU - Lelivelt, K. J.

AU - van de Sande, L.

AU - Schoorl, M. J.C.

AU - Visser, K. M.

AU - van der Vliet, S. T.

AU - van den Akker, M.

AU - Bakker, Y. M.

AU - Bezemer-Goedhart, M.

AU - El Hammoud, I.

AU - Lucas, E. G.A.

AU - Mulder, H. W.

AU - van Veen, R.

AU - Witte, E. C.M.

AU - Oomen, Patrick G A

AU - Wit, Ferdinand

AU - Brinkman, Kees

AU - Vrouenraets, Saskia M E

AU - Mudrikova, T

AU - van der Valk, Marc

PY - 2024/9

Y1 - 2024/9

N2 - Background: Currently, real-world data on doravirine are scarce. In a national prospective cohort, we assessed the effectiveness and tolerability of switching to doravirine-based antiretroviral therapy (ART) in people with HIV. Methods: We did a nationwide, matched, prospective cohort study of people with HIV without previous virological failure and stable for at least 12 months on non-doravirine-containing triple or dual ART switching to doravirine before Sept 1, 2020 (exposed group). Participants in the exposed group were matched 1:2 to individuals continuing stable non-doravirine-containing ART, on age, sex, HIV acquisition category, time since ART initiation, calendar time, pre-ART CD4-count, pre-ART plasma viral load (PVL) and anchor drug class before switching. The primary outcome was protocol-defined virological failure (PDVF; PVL of ≥200 copies per mL) in the intention-to-treat (ITT) population at week 104, with participants modifying their regimen or becoming lost to follow-up considered as PDVF (non-inferiority margin +5%). In contrast, in the on-treatment population, those who modified their regimen or became lost to follow-up were censored from that moment onwards. Tolerability was a secondary outcome. Findings: In total, 590 participants in the exposed group and 1180 participants in the unexposed group (of whom 55·3% used integrase strand transfer inhibitor-based regimens) were included. In the ITT analysis, PDVF occurred in 135 (22·9%) exposed participants and in 295 (25·0%) unexposed participants (risk difference –2·12%, upper limit of the one-sided 95% CI +1·40%). In the on-treatment analysis, 10 (2·2%) of 455 non-censored exposed participants and 26 (2·9%) of 885 non-censored unexposed participants had PDVF (risk difference –0·70%, upper limit of the one-sided 95% CI +0·73%). All exposed participants with a PVL of 200 copies or more per mL resuppressed without regimen modification: no confirmed virological failure (two consecutive PVLs of ≥200 copies per mL) was observed. 104 (17·6%) exposed participants and 211 (17·9%) unexposed participants modified their regimen. 73 (12.4%) exposed participants discontinued doravirine due to adverse events: abnormal dreams (1·7%) and insomnia (1·5%) were most common. Interpretation: Switching to doravirine in well suppressed people with HIV without previous virological failure was non-inferior compared with continuing non-doravirine-containing regimens after 2 years in a real-world setting. Funding: None.

AB - Background: Currently, real-world data on doravirine are scarce. In a national prospective cohort, we assessed the effectiveness and tolerability of switching to doravirine-based antiretroviral therapy (ART) in people with HIV. Methods: We did a nationwide, matched, prospective cohort study of people with HIV without previous virological failure and stable for at least 12 months on non-doravirine-containing triple or dual ART switching to doravirine before Sept 1, 2020 (exposed group). Participants in the exposed group were matched 1:2 to individuals continuing stable non-doravirine-containing ART, on age, sex, HIV acquisition category, time since ART initiation, calendar time, pre-ART CD4-count, pre-ART plasma viral load (PVL) and anchor drug class before switching. The primary outcome was protocol-defined virological failure (PDVF; PVL of ≥200 copies per mL) in the intention-to-treat (ITT) population at week 104, with participants modifying their regimen or becoming lost to follow-up considered as PDVF (non-inferiority margin +5%). In contrast, in the on-treatment population, those who modified their regimen or became lost to follow-up were censored from that moment onwards. Tolerability was a secondary outcome. Findings: In total, 590 participants in the exposed group and 1180 participants in the unexposed group (of whom 55·3% used integrase strand transfer inhibitor-based regimens) were included. In the ITT analysis, PDVF occurred in 135 (22·9%) exposed participants and in 295 (25·0%) unexposed participants (risk difference –2·12%, upper limit of the one-sided 95% CI +1·40%). In the on-treatment analysis, 10 (2·2%) of 455 non-censored exposed participants and 26 (2·9%) of 885 non-censored unexposed participants had PDVF (risk difference –0·70%, upper limit of the one-sided 95% CI +0·73%). All exposed participants with a PVL of 200 copies or more per mL resuppressed without regimen modification: no confirmed virological failure (two consecutive PVLs of ≥200 copies per mL) was observed. 104 (17·6%) exposed participants and 211 (17·9%) unexposed participants modified their regimen. 73 (12.4%) exposed participants discontinued doravirine due to adverse events: abnormal dreams (1·7%) and insomnia (1·5%) were most common. Interpretation: Switching to doravirine in well suppressed people with HIV without previous virological failure was non-inferior compared with continuing non-doravirine-containing regimens after 2 years in a real-world setting. Funding: None.

UR - http://www.scopus.com/inward/record.url?scp=85202145629&partnerID=8YFLogxK

U2 - 10.1016/s2352-3018(24)00150-4

DO - 10.1016/s2352-3018(24)00150-4

M3 - Article

C2 - 39209387

AN - SCOPUS:85202145629

SN - 2352-3018

VL - 11

SP - e576-e585

JO - The Lancet HIV

JF - The Lancet HIV

IS - 9

ER -

the AIDS Therapy Evaluation in the Netherlands (ATHENA) Observational HIV Cohort, Oomen PGA, Wit F, Brinkman K, Vrouenraets SME, Mudrikova T et al. Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study. The Lancet HIV. 2024 Sept;11(9):e576-e585. doi: 10.1016/s2352-3018(24)00150-4

Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study

Abstract

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