Protease inhibitor monotherapy for long-term management of HIV infection: A randomised, controlled, open-label, non-inferiority trial: A randomised, controlled, open-label, non-inferiority trial

Nicholas I. Paton; Wolfgang Stöhr; Alejandro Arenas-Pinto; Martin Fisher; Ian Williams; Margaret Johnson; Chloe Orkin; Fabian Chen; Vincent Lee; Alan Winston; Mark Gompels; Julie Fox; Karen Scott; David T. Dunn; M. Fisher; A. Clarke; W. Hadley; D. Stacey; M. Johnson; P. Byrne; I. Williams; N. De Esteban; P. Pellegrino; L. Haddow; A. Arenas-Pinto; C. Orkin; J. Hand; C. De Souza; L. Murthen; A. Crawford-Jones; F. Chen; R. Wilson; E. Green; J. Masterson; V. Lee; K. Patel; R. Howe; A. Winston; S. Mullaney; M. Gompels; L. Jennings; Nicholas Beeching; R. Tamaklo; J. Fox; A. Teague; I. Jendrulek; J. Tiraboschi; E. Wilkins; Y. Clowes; A. Thompson; G. Brook; M. Trivedi; K. Aderogba; M. Jones; A. DeBurgh-Thomas; L. Jones; I. Reeves; S. Mguni; D. Chadwick; P. Spence; N. Nkhoma; Z. Warwick; S. Price; S. Read; E. Herieka; J. Walker; R. Woodward; J. Day; L. Hilton; V. Harinda; H. Blackman; P. Hay; W. Mejewska; O. Okolo; E. Ong; K. Martin; L. Munro; D. Dockrell; L. Smart; J. Ainsworth; A. Waters; S. Kegg; S. McNamara; S. Taylor; G. Gilleran; B. Gazzard; J. Rowlands; S. Allan; R. Sandhu; N. O'Farrell; S. Quaid; F. Martin; C. Bennett; M. Kapembwa; J. Minton; J. Calderwood; F. Post; L. Campbell; E. Wandolo; A. Palfreeman; L. Mashonganyika; T. Balachandran; M. Kakowa; R. O'Connell; C. Tanawa; S. Jebakumar; L. Hagger; S. Quah; S. McKernan; C. Lacey; S. Douglas; S. Russell-Sharpe; C. Brewer; C. Leen; S. Morris; S. Obeyesekera; S. Williams; N. David; M. Roberts; J. Wollaston; N. Paton; W. Stöhr; K. Scott; D. Dunn; E. Beaumont; S. Fleck; M. Hall; S. Hennings; I. Kummeling; S. Martins; E. Owen-Powell; F. van Hooff Sanders; L. Vivas; E. White

doi:10.1016/s2352-3018(15)00176-9

Protease inhibitor monotherapy for long-term management of HIV infection: A randomised, controlled, open-label, non-inferiority trial: A randomised, controlled, open-label, non-inferiority trial

Nicholas I. Paton
, Wolfgang Stöhr
, Alejandro Arenas-Pinto
, Martin Fisher
, Ian Williams
, Margaret Johnson
, Chloe Orkin
, Fabian Chen
, Vincent Lee
, Alan Winston
, Mark Gompels
, Julie Fox
, Karen Scott
, David T. Dunn
, M. Fisher
, A. Clarke
, W. Hadley
, D. Stacey
, M. Johnson
, P. Byrne

I. Williams, N. De Esteban, P. Pellegrino, L. Haddow, A. Arenas-Pinto, C. Orkin, J. Hand, C. De Souza, L. Murthen, A. Crawford-Jones, F. Chen, R. Wilson, E. Green, J. Masterson, V. Lee, K. Patel, R. Howe, A. Winston, S. Mullaney, M. Gompels, L. Jennings, Nicholas Beeching, R. Tamaklo, J. Fox, A. Teague, I. Jendrulek, J. Tiraboschi, E. Wilkins, Y. Clowes, A. Thompson, G. Brook, M. Trivedi, K. Aderogba, M. Jones, A. DeBurgh-Thomas, L. Jones, I. Reeves, S. Mguni, D. Chadwick, P. Spence, N. Nkhoma, Z. Warwick, S. Price, S. Read, E. Herieka, J. Walker, R. Woodward, J. Day, L. Hilton, V. Harinda, H. Blackman, P. Hay, W. Mejewska, O. Okolo, E. Ong, K. Martin, L. Munro, D. Dockrell, L. Smart, J. Ainsworth, A. Waters, S. Kegg, S. McNamara, S. Taylor, G. Gilleran, B. Gazzard, J. Rowlands, S. Allan, R. Sandhu, N. O'Farrell, S. Quaid, F. Martin, C. Bennett, M. Kapembwa, J. Minton, J. Calderwood, F. Post, L. Campbell, E. Wandolo, A. Palfreeman, L. Mashonganyika, T. Balachandran, M. Kakowa, R. O'Connell, C. Tanawa, S. Jebakumar, L. Hagger, S. Quah, S. McKernan, C. Lacey, S. Douglas, S. Russell-Sharpe, C. Brewer, C. Leen, S. Morris, S. Obeyesekera, S. Williams, N. David, M. Roberts, J. Wollaston, N. Paton, W. Stöhr, K. Scott, D. Dunn, E. Beaumont, S. Fleck, M. Hall, S. Hennings, I. Kummeling, S. Martins, E. Owen-Powell, F. van Hooff Sanders, L. Vivas, E. White

University of London
National University of Singapore
University Hospitals Sussex NHS Foundation Trust
University College London
Royal Free London NHS Foundation Trust
Barts Health NHS Trust
Royal Berkshire NHS Foundation Trust
Manchester University NHS Foundation Trust
Imperial College Healthcare NHS Trust
North Bristol NHS Trust
Guy's and St Thomas' NHS Foundation Trust
Elton John Centre
Queen Mary University of London
Liverpool University Hospitals NHS Foundation Trust
Northern Care Alliance NHS Group
London North West University Healthcare NHS Trust
Gloucestershire Hospitals NHS Foundation Trust
Homerton University Hospital NHS Foundation Trust
South Tees Hospitals NHS Foundation Trust
University Hospitals Plymouth NHS Trust
University Hospitals Dorset NHS Foundation Trust
Mid and South Essex NHS Foundation Trust
Solent NHS Trust
St Georges Hospital
Royal Victoria Infi rmary
Sheffield Teaching Hospitals NHS Foundation Trust
North Middlesex University Hospital NHS Trust
Queen Elizabeth Hospital
University Hospitals Birmingham NHS Foundation Trust
Chelsea and Westminster Hospital NHS Foundation Trust
University Hospitals Coventry and Warwickshire NHS Trust
Harrogate and District NHS Foundation Trust
Leeds Teaching Hospitals NHS Trust
King’s College Hospital
University Hospitals of Leicester NHS Trust
Bedfordshire Hospitals NHS Foundation Trust
North West Anglia NHS Foundation Trust
Royal Victoria Hospital Belfast
York Teaching Hospital
NHS Lothian
Barking Hospital
Norfolk and Norwich University Hospitals NHS Foundation Trust
Worcestershire Acute Hospitals NHS Trust

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

80 Citations (Scopus)

Abstract

Background: Standard-of-care antiretroviral therapy (ART) uses a combination of drugs deemed essential to minimise treatment failure and drug resistance. Protease inhibitors are potent, with a high genetic barrier to resistance, and have potential use as monotherapy after viral load suppression is achieved with combination treatment. We aimed to assess clinical risks and benefi ts of protease inhibitor monotherapy in long-term clinical use: in particular, the eff ect on drug resistance and future treatment options. Methods In this pragmatic, parallel-group, randomised, controlled, open-label, non-inferiority trial, we enrolled adults (=18 years of age) positive for HIV attending 43 public sector treatment centres in the UK who had suppressed viral load (<50 copies per mL) for at least 24 weeks on combination ART with no change in the previous 12 weeks and a CD4 count of more than 100 cells per μL. Participants were randomly allocated (1:1) to maintain ongoing triple therapy (OT) or to switch to a strategy of physician-selected ritonavir-boosted protease inhibitor monotherapy (PI-mono); we recommended ritonavir (100 mg)-boosted darunavir (800 mg) once daily or ritonavir (100 mg)-boosted lopinavir (400 mg) twice daily, with prompt return to combination treatment if viral load rebounded. All treatments were oral. Randomisation was with permuted blocks of varying size and stratifi ed by centre and baseline ART; we used a computer-generated, sequentially numbered randomisation list. The primary outcome was loss of future drug options, defi ned as new intermediate-level or high-level resistance to one or more drugs to which the patient's virus was deemed sensitive at trial entry (assessed at 3 years; non-inferiority margin of 10%). We estimated probability of rebound and resistance with Kaplan-Meier analysis. Analyses were by intention to treat. This trial is registered with the International Standard Randomised Controlled Trial Number registry, number ISRCTN04857074. Findings Between Nov 4, 2008, and July 28, 2010, we randomly allocated 587 participants to OT (291) or PI-mono (296). At 3 years, one or more future drug options had been lost in two participants (Kaplan-Meier estimate 0.7%) in the OT group and six (2.1%) in the PI-mono group: diff erence 1.4% (-0.4 to 3.4); non-inferiority shown. 49 (16.8%) participants in the OT group and 65 (22.0%) in the PI-mono group had grade 3 or 4 clinical adverse events (diff erence 5.1% [95% CI -1.3 to 11.5]; p=0.12); 45 (six treatment related) and 56 (three treatment related) had serious adverse events. Interpretation Protease inhibitor monotherapy, with regular viral load monitoring and prompt reintroduction of combination treatment for rebound, preserved future treatment options and did not change overall clinical outcomes or frequency of toxic eff ects. Protease inhibitor monotherapy is an acceptable alternative for long-term clinical management of HIV infection.

Original language	English
Pages (from-to)	e417-e426
Journal	The Lancet HIV
Volume	2
Issue number	10
DOIs	https://doi.org/10.1016/s2352-3018(15)00176-9
Publication status	Published - 1 Oct 2015
Externally published	Yes

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SDG 3 Good Health and Well-being

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10.1016/s2352-3018(15)00176-9Licence: CC BY

Cite this

Paton, N. I., Stöhr, W., Arenas-Pinto, A., Fisher, M., Williams, I., Johnson, M., Orkin, C., Chen, F., Lee, V., Winston, A., Gompels, M., Fox, J., Scott, K., Dunn, D. T., Fisher, M., Clarke, A., Hadley, W., Stacey, D., Johnson, M., ... White, E. (2015). Protease inhibitor monotherapy for long-term management of HIV infection: A randomised, controlled, open-label, non-inferiority trial: A randomised, controlled, open-label, non-inferiority trial. The Lancet HIV, 2(10), e417-e426. https://doi.org/10.1016/s2352-3018(15)00176-9

@article{84fd88e4b06e4917bccc4005e5bdeaf8,

title = "Protease inhibitor monotherapy for long-term management of HIV infection: A randomised, controlled, open-label, non-inferiority trial: A randomised, controlled, open-label, non-inferiority trial",

abstract = "Background: Standard-of-care antiretroviral therapy (ART) uses a combination of drugs deemed essential to minimise treatment failure and drug resistance. Protease inhibitors are potent, with a high genetic barrier to resistance, and have potential use as monotherapy after viral load suppression is achieved with combination treatment. We aimed to assess clinical risks and benefi ts of protease inhibitor monotherapy in long-term clinical use: in particular, the eff ect on drug resistance and future treatment options. Methods In this pragmatic, parallel-group, randomised, controlled, open-label, non-inferiority trial, we enrolled adults (=18 years of age) positive for HIV attending 43 public sector treatment centres in the UK who had suppressed viral load (<50 copies per mL) for at least 24 weeks on combination ART with no change in the previous 12 weeks and a CD4 count of more than 100 cells per μL. Participants were randomly allocated (1:1) to maintain ongoing triple therapy (OT) or to switch to a strategy of physician-selected ritonavir-boosted protease inhibitor monotherapy (PI-mono); we recommended ritonavir (100 mg)-boosted darunavir (800 mg) once daily or ritonavir (100 mg)-boosted lopinavir (400 mg) twice daily, with prompt return to combination treatment if viral load rebounded. All treatments were oral. Randomisation was with permuted blocks of varying size and stratifi ed by centre and baseline ART; we used a computer-generated, sequentially numbered randomisation list. The primary outcome was loss of future drug options, defi ned as new intermediate-level or high-level resistance to one or more drugs to which the patient's virus was deemed sensitive at trial entry (assessed at 3 years; non-inferiority margin of 10\%). We estimated probability of rebound and resistance with Kaplan-Meier analysis. Analyses were by intention to treat. This trial is registered with the International Standard Randomised Controlled Trial Number registry, number ISRCTN04857074. Findings Between Nov 4, 2008, and July 28, 2010, we randomly allocated 587 participants to OT (291) or PI-mono (296). At 3 years, one or more future drug options had been lost in two participants (Kaplan-Meier estimate 0.7\%) in the OT group and six (2.1\%) in the PI-mono group: diff erence 1.4\% (-0.4 to 3.4); non-inferiority shown. 49 (16.8\%) participants in the OT group and 65 (22.0\%) in the PI-mono group had grade 3 or 4 clinical adverse events (diff erence 5.1\% [95\% CI -1.3 to 11.5]; p=0.12); 45 (six treatment related) and 56 (three treatment related) had serious adverse events. Interpretation Protease inhibitor monotherapy, with regular viral load monitoring and prompt reintroduction of combination treatment for rebound, preserved future treatment options and did not change overall clinical outcomes or frequency of toxic eff ects. Protease inhibitor monotherapy is an acceptable alternative for long-term clinical management of HIV infection.",

author = "Paton, \{Nicholas I.\} and Wolfgang St{\"o}hr and Alejandro Arenas-Pinto and Martin Fisher and Ian Williams and Margaret Johnson and Chloe Orkin and Fabian Chen and Vincent Lee and Alan Winston and Mark Gompels and Julie Fox and Karen Scott and Dunn, \{David T.\} and M. Fisher and A. Clarke and W. Hadley and D. Stacey and M. Johnson and P. Byrne and I. Williams and \{De Esteban\}, N. and P. Pellegrino and L. Haddow and A. Arenas-Pinto and C. Orkin and J. Hand and \{De Souza\}, C. and L. Murthen and A. Crawford-Jones and F. Chen and R. Wilson and E. Green and J. Masterson and V. Lee and K. Patel and R. Howe and A. Winston and S. Mullaney and M. Gompels and L. Jennings and Nicholas Beeching and R. Tamaklo and J. Fox and A. Teague and I. Jendrulek and J. Tiraboschi and E. Wilkins and Y. Clowes and A. Thompson and G. Brook and M. Trivedi and K. Aderogba and M. Jones and A. DeBurgh-Thomas and L. Jones and I. Reeves and S. Mguni and D. Chadwick and P. Spence and N. Nkhoma and Z. Warwick and S. Price and S. Read and E. Herieka and J. Walker and R. Woodward and J. Day and L. Hilton and V. Harinda and H. Blackman and P. Hay and W. Mejewska and O. Okolo and E. Ong and K. Martin and L. Munro and D. Dockrell and L. Smart and J. Ainsworth and A. Waters and S. Kegg and S. McNamara and S. Taylor and G. Gilleran and B. Gazzard and J. Rowlands and S. Allan and R. Sandhu and N. O'Farrell and S. Quaid and F. Martin and C. Bennett and M. Kapembwa and J. Minton and J. Calderwood and F. Post and L. Campbell and E. Wandolo and A. Palfreeman and L. Mashonganyika and T. Balachandran and M. Kakowa and R. O'Connell and C. Tanawa and S. Jebakumar and L. Hagger and S. Quah and S. McKernan and C. Lacey and S. Douglas and S. Russell-Sharpe and C. Brewer and C. Leen and S. Morris and S. Obeyesekera and S. Williams and N. David and M. Roberts and J. Wollaston and N. Paton and W. St{\"o}hr and K. Scott and D. Dunn and E. Beaumont and S. Fleck and M. Hall and S. Hennings and I. Kummeling and S. Martins and E. Owen-Powell and Sanders, \{F. van Hooff\} and L. Vivas and E. White",

year = "2015",

month = oct,

day = "1",

doi = "10.1016/s2352-3018(15)00176-9",

language = "English",

volume = "2",

pages = "e417--e426",

journal = "The Lancet HIV",

issn = "2352-3018",

publisher = "Elsevier Ltd",

number = "10",

}

Paton, NI, Stöhr, W, Arenas-Pinto, A, Fisher, M, Williams, I, Johnson, M, Orkin, C, Chen, F, Lee, V, Winston, A, Gompels, M, Fox, J, Scott, K, Dunn, DT, Fisher, M, Clarke, A, Hadley, W, Stacey, D, Johnson, M, Byrne, P, Williams, I, De Esteban, N, Pellegrino, P, Haddow, L, Arenas-Pinto, A, Orkin, C, Hand, J, De Souza, C, Murthen, L, Crawford-Jones, A, Chen, F, Wilson, R, Green, E, Masterson, J, Lee, V, Patel, K, Howe, R, Winston, A, Mullaney, S, Gompels, M, Jennings, L, Beeching, N, Tamaklo, R, Fox, J, Teague, A, Jendrulek, I, Tiraboschi, J, Wilkins, E, Clowes, Y, Thompson, A, Brook, G, Trivedi, M, Aderogba, K, Jones, M, DeBurgh-Thomas, A, Jones, L, Reeves, I, Mguni, S, Chadwick, D, Spence, P, Nkhoma, N, Warwick, Z, Price, S, Read, S, Herieka, E, Walker, J, Woodward, R, Day, J, Hilton, L, Harinda, V, Blackman, H, Hay, P, Mejewska, W, Okolo, O, Ong, E, Martin, K, Munro, L, Dockrell, D, Smart, L, Ainsworth, J, Waters, A, Kegg, S, McNamara, S, Taylor, S, Gilleran, G, Gazzard, B, Rowlands, J, Allan, S, Sandhu, R, O'Farrell, N, Quaid, S, Martin, F, Bennett, C, Kapembwa, M, Minton, J, Calderwood, J, Post, F, Campbell, L, Wandolo, E, Palfreeman, A, Mashonganyika, L, Balachandran, T, Kakowa, M, O'Connell, R, Tanawa, C, Jebakumar, S, Hagger, L, Quah, S, McKernan, S, Lacey, C, Douglas, S, Russell-Sharpe, S, Brewer, C, Leen, C, Morris, S, Obeyesekera, S, Williams, S, David, N, Roberts, M, Wollaston, J, Paton, N, Stöhr, W, Scott, K, Dunn, D, Beaumont, E, Fleck, S, Hall, M, Hennings, S, Kummeling, I, Martins, S, Owen-Powell, E, Sanders, FVH, Vivas, L & White, E 2015, 'Protease inhibitor monotherapy for long-term management of HIV infection: A randomised, controlled, open-label, non-inferiority trial: A randomised, controlled, open-label, non-inferiority trial', The Lancet HIV, vol. 2, no. 10, pp. e417-e426. https://doi.org/10.1016/s2352-3018(15)00176-9

Protease inhibitor monotherapy for long-term management of HIV infection: A randomised, controlled, open-label, non-inferiority trial: A randomised, controlled, open-label, non-inferiority trial. / Paton, Nicholas I.; Stöhr, Wolfgang; Arenas-Pinto, Alejandro et al.
In: The Lancet HIV, Vol. 2, No. 10, 01.10.2015, p. e417-e426.

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

TY - JOUR

T1 - Protease inhibitor monotherapy for long-term management of HIV infection: A randomised, controlled, open-label, non-inferiority trial: A randomised, controlled, open-label, non-inferiority trial

AU - Paton, Nicholas I.

AU - Stöhr, Wolfgang

AU - Arenas-Pinto, Alejandro

AU - Fisher, Martin

AU - Williams, Ian

AU - Johnson, Margaret

AU - Orkin, Chloe

AU - Chen, Fabian

AU - Lee, Vincent

AU - Winston, Alan

AU - Gompels, Mark

AU - Fox, Julie

AU - Scott, Karen

AU - Dunn, David T.

AU - Fisher, M.

AU - Clarke, A.

AU - Hadley, W.

AU - Stacey, D.

AU - Johnson, M.

AU - Byrne, P.

AU - Williams, I.

AU - De Esteban, N.

AU - Pellegrino, P.

AU - Haddow, L.

AU - Arenas-Pinto, A.

AU - Orkin, C.

AU - Hand, J.

AU - De Souza, C.

AU - Murthen, L.

AU - Crawford-Jones, A.

AU - Chen, F.

AU - Wilson, R.

AU - Green, E.

AU - Masterson, J.

AU - Lee, V.

AU - Patel, K.

AU - Howe, R.

AU - Winston, A.

AU - Mullaney, S.

AU - Gompels, M.

AU - Jennings, L.

AU - Beeching, Nicholas

AU - Tamaklo, R.

AU - Fox, J.

AU - Teague, A.

AU - Jendrulek, I.

AU - Tiraboschi, J.

AU - Wilkins, E.

AU - Clowes, Y.

AU - Thompson, A.

AU - Brook, G.

AU - Trivedi, M.

AU - Aderogba, K.

AU - Jones, M.

AU - DeBurgh-Thomas, A.

AU - Jones, L.

AU - Reeves, I.

AU - Mguni, S.

AU - Chadwick, D.

AU - Spence, P.

AU - Nkhoma, N.

AU - Warwick, Z.

AU - Price, S.

AU - Read, S.

AU - Herieka, E.

AU - Walker, J.

AU - Woodward, R.

AU - Day, J.

AU - Hilton, L.

AU - Harinda, V.

AU - Blackman, H.

AU - Hay, P.

AU - Mejewska, W.

AU - Okolo, O.

AU - Ong, E.

AU - Martin, K.

AU - Munro, L.

AU - Dockrell, D.

AU - Smart, L.

AU - Ainsworth, J.

AU - Waters, A.

AU - Kegg, S.

AU - McNamara, S.

AU - Taylor, S.

AU - Gilleran, G.

AU - Gazzard, B.

AU - Rowlands, J.

AU - Allan, S.

AU - Sandhu, R.

AU - O'Farrell, N.

AU - Quaid, S.

AU - Martin, F.

AU - Bennett, C.

AU - Kapembwa, M.

AU - Minton, J.

AU - Calderwood, J.

AU - Post, F.

AU - Campbell, L.

AU - Wandolo, E.

AU - Palfreeman, A.

AU - Mashonganyika, L.

AU - Balachandran, T.

AU - Kakowa, M.

AU - O'Connell, R.

AU - Tanawa, C.

AU - Jebakumar, S.

AU - Hagger, L.

AU - Quah, S.

AU - McKernan, S.

AU - Lacey, C.

AU - Douglas, S.

AU - Russell-Sharpe, S.

AU - Brewer, C.

AU - Leen, C.

AU - Morris, S.

AU - Obeyesekera, S.

AU - Williams, S.

AU - David, N.

AU - Roberts, M.

AU - Wollaston, J.

AU - Paton, N.

AU - Stöhr, W.

AU - Scott, K.

AU - Dunn, D.

AU - Beaumont, E.

AU - Fleck, S.

AU - Hall, M.

AU - Hennings, S.

AU - Kummeling, I.

AU - Martins, S.

AU - Owen-Powell, E.

AU - Sanders, F. van Hooff

AU - Vivas, L.

AU - White, E.

PY - 2015/10/1

Y1 - 2015/10/1

N2 - Background: Standard-of-care antiretroviral therapy (ART) uses a combination of drugs deemed essential to minimise treatment failure and drug resistance. Protease inhibitors are potent, with a high genetic barrier to resistance, and have potential use as monotherapy after viral load suppression is achieved with combination treatment. We aimed to assess clinical risks and benefi ts of protease inhibitor monotherapy in long-term clinical use: in particular, the eff ect on drug resistance and future treatment options. Methods In this pragmatic, parallel-group, randomised, controlled, open-label, non-inferiority trial, we enrolled adults (=18 years of age) positive for HIV attending 43 public sector treatment centres in the UK who had suppressed viral load (<50 copies per mL) for at least 24 weeks on combination ART with no change in the previous 12 weeks and a CD4 count of more than 100 cells per μL. Participants were randomly allocated (1:1) to maintain ongoing triple therapy (OT) or to switch to a strategy of physician-selected ritonavir-boosted protease inhibitor monotherapy (PI-mono); we recommended ritonavir (100 mg)-boosted darunavir (800 mg) once daily or ritonavir (100 mg)-boosted lopinavir (400 mg) twice daily, with prompt return to combination treatment if viral load rebounded. All treatments were oral. Randomisation was with permuted blocks of varying size and stratifi ed by centre and baseline ART; we used a computer-generated, sequentially numbered randomisation list. The primary outcome was loss of future drug options, defi ned as new intermediate-level or high-level resistance to one or more drugs to which the patient's virus was deemed sensitive at trial entry (assessed at 3 years; non-inferiority margin of 10%). We estimated probability of rebound and resistance with Kaplan-Meier analysis. Analyses were by intention to treat. This trial is registered with the International Standard Randomised Controlled Trial Number registry, number ISRCTN04857074. Findings Between Nov 4, 2008, and July 28, 2010, we randomly allocated 587 participants to OT (291) or PI-mono (296). At 3 years, one or more future drug options had been lost in two participants (Kaplan-Meier estimate 0.7%) in the OT group and six (2.1%) in the PI-mono group: diff erence 1.4% (-0.4 to 3.4); non-inferiority shown. 49 (16.8%) participants in the OT group and 65 (22.0%) in the PI-mono group had grade 3 or 4 clinical adverse events (diff erence 5.1% [95% CI -1.3 to 11.5]; p=0.12); 45 (six treatment related) and 56 (three treatment related) had serious adverse events. Interpretation Protease inhibitor monotherapy, with regular viral load monitoring and prompt reintroduction of combination treatment for rebound, preserved future treatment options and did not change overall clinical outcomes or frequency of toxic eff ects. Protease inhibitor monotherapy is an acceptable alternative for long-term clinical management of HIV infection.

AB - Background: Standard-of-care antiretroviral therapy (ART) uses a combination of drugs deemed essential to minimise treatment failure and drug resistance. Protease inhibitors are potent, with a high genetic barrier to resistance, and have potential use as monotherapy after viral load suppression is achieved with combination treatment. We aimed to assess clinical risks and benefi ts of protease inhibitor monotherapy in long-term clinical use: in particular, the eff ect on drug resistance and future treatment options. Methods In this pragmatic, parallel-group, randomised, controlled, open-label, non-inferiority trial, we enrolled adults (=18 years of age) positive for HIV attending 43 public sector treatment centres in the UK who had suppressed viral load (<50 copies per mL) for at least 24 weeks on combination ART with no change in the previous 12 weeks and a CD4 count of more than 100 cells per μL. Participants were randomly allocated (1:1) to maintain ongoing triple therapy (OT) or to switch to a strategy of physician-selected ritonavir-boosted protease inhibitor monotherapy (PI-mono); we recommended ritonavir (100 mg)-boosted darunavir (800 mg) once daily or ritonavir (100 mg)-boosted lopinavir (400 mg) twice daily, with prompt return to combination treatment if viral load rebounded. All treatments were oral. Randomisation was with permuted blocks of varying size and stratifi ed by centre and baseline ART; we used a computer-generated, sequentially numbered randomisation list. The primary outcome was loss of future drug options, defi ned as new intermediate-level or high-level resistance to one or more drugs to which the patient's virus was deemed sensitive at trial entry (assessed at 3 years; non-inferiority margin of 10%). We estimated probability of rebound and resistance with Kaplan-Meier analysis. Analyses were by intention to treat. This trial is registered with the International Standard Randomised Controlled Trial Number registry, number ISRCTN04857074. Findings Between Nov 4, 2008, and July 28, 2010, we randomly allocated 587 participants to OT (291) or PI-mono (296). At 3 years, one or more future drug options had been lost in two participants (Kaplan-Meier estimate 0.7%) in the OT group and six (2.1%) in the PI-mono group: diff erence 1.4% (-0.4 to 3.4); non-inferiority shown. 49 (16.8%) participants in the OT group and 65 (22.0%) in the PI-mono group had grade 3 or 4 clinical adverse events (diff erence 5.1% [95% CI -1.3 to 11.5]; p=0.12); 45 (six treatment related) and 56 (three treatment related) had serious adverse events. Interpretation Protease inhibitor monotherapy, with regular viral load monitoring and prompt reintroduction of combination treatment for rebound, preserved future treatment options and did not change overall clinical outcomes or frequency of toxic eff ects. Protease inhibitor monotherapy is an acceptable alternative for long-term clinical management of HIV infection.

U2 - 10.1016/s2352-3018(15)00176-9

DO - 10.1016/s2352-3018(15)00176-9

M3 - Article

SN - 2352-3018

VL - 2

SP - e417-e426

JO - The Lancet HIV

JF - The Lancet HIV

IS - 10

ER -

Protease inhibitor monotherapy for long-term management of HIV infection: A randomised, controlled, open-label, non-inferiority trial: A randomised, controlled, open-label, non-inferiority trial

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