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

Patrick G.A. Oomen; Ferdinand W.N.M. Wit; Kees Brinkman; Saskia M.E. Vrouenraets; Tania Mudrikova; Berend J. van Welzen; Marc van der Valk; M. A. van Agtmael; M. Bomers; S. E. Geerlings; A. Goorhuis; V. C. Harris; J. W. Hovius; B. Lemkes; F. J.B. Nellen; E. J.G. Peters; T. van der Poll; J. M. Prins; K. C.E. Sigaloff; V. Spoorenberg; M. van Vugt; W. J. Wiersinga; C. Bruins; J. van Eden; I. J. Hylkema-van den Bout; L. M. Laan; F. J.J. Pijnappel; S. Y. Smalhout; M. E. Spelbrink; A. M. Weijsenfeld; N. K.T. Back; M. T.E. Cornelissen; R. van Houdt; M. Jonges; S. Jurriaans; C. J. Schinkel; M. R.A. Welkers; K. C. Wolthers; M. van den Berge; A. Stegeman; S. Baas; L. Hage de Looff; A. van Arkel; J. Stohr; B. Wintermans; M. J.H. Pronk; H. S.M. Ammerlaan; C. de Bree; E. S. de Munnik; Ymkje Stienstra

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: a nationwide, matched, prospective cohort study

Patrick G.A. Oomen, Ferdinand W.N.M. Wit, Kees Brinkman, Saskia M.E. Vrouenraets, Tania Mudrikova, Berend J. van Welzen, Marc van der Valk, M. A. van Agtmael, M. Bomers, S. E. Geerlings, A. Goorhuis, V. C. Harris, J. W. Hovius, B. Lemkes, F. J.B. Nellen, E. J.G. Peters, T. van der Poll, J. M. Prins, K. C.E. Sigaloff, V. SpoorenbergM. van Vugt, W. J. Wiersinga, C. Bruins, J. van Eden, I. J. Hylkema-van den Bout, L. M. Laan, F. J.J. Pijnappel, S. Y. Smalhout, M. E. Spelbrink, A. M. Weijsenfeld, N. K.T. Back, M. T.E. Cornelissen, R. van Houdt, M. Jonges, S. Jurriaans, C. J. Schinkel, M. R.A. Welkers, K. C. Wolthers, M. van den Berge, A. Stegeman, S. Baas, L. Hage de Looff, A. van Arkel, J. Stohr, B. Wintermans, M. J.H. Pronk, H. S.M. Ammerlaan, C. de Bree, E. S. de Munnik, Ymkje Stienstra

Liverpool School of Tropical Medicine

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

9 Citations (Scopus)

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 - 1 Sept 2024

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Oomen, P. G. A., Wit, F. W. N. M., Brinkman, K., Vrouenraets, S. M. E., Mudrikova, T., van Welzen, B. J., van der Valk, M., van Agtmael, M. A., Bomers, M., Geerlings, S. E., Goorhuis, A., Harris, V. C., Hovius, J. W., Lemkes, B., Nellen, F. J. B., Peters, E. J. G., van der Poll, T., Prins, J. M., Sigaloff, K. C. E., ... Stienstra, Y. (2024). Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study: a nationwide, matched, prospective cohort study. The Lancet HIV, 11(9), e576-e585. https://doi.org/10.1016/s2352-3018(24)00150-4

@article{9fa0c8d0cce245c995b76e03f27f9980,

title = "Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study: 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 = "Oomen, \{Patrick G.A.\} and Wit, \{Ferdinand W.N.M.\} and Kees Brinkman and Vrouenraets, \{Saskia M.E.\} and Tania Mudrikova and \{van Welzen\}, \{Berend J.\} and \{van der Valk\}, Marc and \{van Agtmael\}, \{M. A.\} and M. Bomers and Geerlings, \{S. E.\} and A. Goorhuis and Harris, \{V. C.\} and Hovius, \{J. W.\} and B. Lemkes and Nellen, \{F. J.B.\} and Peters, \{E. J.G.\} and \{van der Poll\}, T. and Prins, \{J. M.\} and Sigaloff, \{K. C.E.\} and V. Spoorenberg and \{van Vugt\}, M. and Wiersinga, \{W. J.\} and C. Bruins and \{van Eden\}, J. and \{Hylkema-van den Bout\}, \{I. J.\} and Laan, \{L. M.\} and Pijnappel, \{F. J.J.\} and Smalhout, \{S. Y.\} and Spelbrink, \{M. E.\} and Weijsenfeld, \{A. M.\} and Back, \{N. K.T.\} and Cornelissen, \{M. T.E.\} and \{van Houdt\}, R. and M. Jonges and S. Jurriaans and Schinkel, \{C. J.\} and Welkers, \{M. R.A.\} and Wolthers, \{K. C.\} and \{van den Berge\}, M. and A. Stegeman and S. Baas and \{Hage de Looff\}, L. and \{van Arkel\}, A. and J. Stohr and B. Wintermans and Pronk, \{M. J.H.\} and Ammerlaan, \{H. S.M.\} and \{de Bree\}, C. and \{de Munnik\}, \{E. S.\} and Ymkje Stienstra",

year = "2024",

month = sep,

day = "1",

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",

}

Oomen, PGA, Wit, FWNM, Brinkman, K, Vrouenraets, SME, Mudrikova, T, van Welzen, BJ, van der Valk, M, van Agtmael, MA, Bomers, M, Geerlings, SE, Goorhuis, A, Harris, VC, Hovius, JW, Lemkes, B, Nellen, FJB, Peters, EJG, van der Poll, T, Prins, JM, Sigaloff, KCE, Spoorenberg, V, van Vugt, M, Wiersinga, WJ, Bruins, C, van Eden, J, Hylkema-van den Bout, IJ, Laan, LM, Pijnappel, FJJ, Smalhout, SY, Spelbrink, ME, Weijsenfeld, AM, Back, NKT, Cornelissen, MTE, van Houdt, R, Jonges, M, Jurriaans, S, Schinkel, CJ, Welkers, MRA, Wolthers, KC, van den Berge, M, Stegeman, A, Baas, S, Hage de Looff, L, van Arkel, A, Stohr, J, Wintermans, B, Pronk, MJH, Ammerlaan, HSM, de Bree, C, de Munnik, ES & Stienstra, Y 2024, 'Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study: 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: a nationwide, matched, prospective cohort study. / Oomen, Patrick G.A.; Wit, Ferdinand W.N.M.; Brinkman, Kees et al.
In: The Lancet HIV, Vol. 11, No. 9, 01.09.2024, p. e576-e585.

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

TY - JOUR

T1 - Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study: a nationwide, matched, prospective cohort study

AU - Oomen, Patrick G.A.

AU - Wit, Ferdinand W.N.M.

AU - Brinkman, Kees

AU - Vrouenraets, Saskia M.E.

AU - Mudrikova, Tania

AU - van Welzen, Berend J.

AU - van der Valk, Marc

AU - van Agtmael, M. A.

AU - Bomers, M.

AU - Geerlings, S. E.

AU - Goorhuis, A.

AU - Harris, V. C.

AU - Hovius, J. W.

AU - Lemkes, B.

AU - Nellen, F. J.B.

AU - Peters, E. J.G.

AU - van der Poll, T.

AU - Prins, J. M.

AU - Sigaloff, K. C.E.

AU - Spoorenberg, V.

AU - van Vugt, M.

AU - Wiersinga, W. J.

AU - Bruins, C.

AU - van Eden, J.

AU - Hylkema-van den Bout, I. J.

AU - Laan, L. M.

AU - Pijnappel, F. J.J.

AU - Smalhout, S. Y.

AU - Spelbrink, M. E.

AU - Weijsenfeld, A. M.

AU - Back, N. K.T.

AU - Cornelissen, M. T.E.

AU - van Houdt, R.

AU - Jonges, M.

AU - Jurriaans, S.

AU - Schinkel, C. J.

AU - Welkers, M. R.A.

AU - Wolthers, K. C.

AU - van den Berge, M.

AU - Stegeman, A.

AU - Baas, S.

AU - Hage de Looff, L.

AU - van Arkel, A.

AU - Stohr, J.

AU - Wintermans, B.

AU - Pronk, M. J.H.

AU - Ammerlaan, H. S.M.

AU - de Bree, C.

AU - de Munnik, E. S.

AU - Stienstra, Ymkje

PY - 2024/9/1

Y1 - 2024/9/1

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.

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

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

M3 - Article

SN - 2352-3018

VL - 11

SP - e576-e585

JO - The Lancet HIV

JF - The Lancet HIV

IS - 9

ER -

Oomen PGA, Wit FWNM, Brinkman K, Vrouenraets SME, Mudrikova T, van Welzen BJ et al. Real-world effectiveness and tolerability of switching to doravirine-based antiretroviral therapy in people with HIV: a nationwide, matched, prospective cohort study: a nationwide, matched, prospective cohort study. The Lancet HIV. 2024 Sept 1;11(9):e576-e585. doi: 10.1016/s2352-3018(24)00150-4