IRIS Institutional Research Information System - AIR Archivio Istituzionale della Ricerca

Objectives: The objective of this studywas to improve the prediction of the impact of HIV-1 protease mutations in different viral subtypes on virological response to darunavir. Methods: Darunavir-containing treatment change episodes (TCEs) in patients previously failing PIs were selected from large European databases. HIV-1 subtype B-infected patients were used as the derivation dataset and HIV- 1 non-B-infected patients were used as the validation dataset. The adjusted association of each mutation with week 8 HIV RNA change from baseline was analysed by linear regression. A prediction model was derived based on best subset least squares estimation with mutational weights corresponding to regression coefficients. Virological outcome prediction accuracy was compared with that from existing genotypic resistance interpretation systems (GISs) (ANRS 2013, Rega 9.1.0 and HIVdb 7.0). Results: TCEs were selected from 681 subtype B-infected and 199 non-B-infected adults. Accompanying drugs were NRTIs in 87%, NNRTIs in 27%and raltegravir ormaraviroc or enfuvirtide in 53%. The predictionmodel included weighted protease mutations, HIV RNA, CD4 and activity of accompanying drugs. The model's association with week 8 HIV RNA change in the subtype B (derivation) set was R2=0.47 [average squared error (ASE)=0.67, P>10-6]; in the non-B (validation) set, ASE was 0.91. Accuracy investigated by means of area under the receiver operating characteristic curves with a binary response (above the threshold value of HIV RNA reduction) showed that our finalmodel outperformed models with existing interpretation systems in both training and validation sets. Conclusions: A model with a new darunavir-weighted mutation score outperformed existing GISs in both B and non-B subtypes in predicting virological response to darunavir.

Improved darunavir genotypic mutation score predicting treatment response for patients infected with HIRaben-1 subtype B and non-subtype B receiving a salvage regimen / A. De Luca, P. Flandre, D. Dunn, M. Zazzi, A. Wensing, M.M. Santoro, H.F. Günthard, L. Wittkop, T. Kordossis, F. Garcia, A. Castagna, A. Cozzi-Lepri, D. Churchill, S. De Wit, N.H. Brockmeyer, A. Imaz, C. Mussini, N. Obel, C.F. Perno, B. Roca, P. Reiss, E. Schülter, C. Torti, A. van Sighem, R. Zangerle, D. Descamps, A. Mocroft, O. Kirk, C. Sabin, S. De Wit, J. Casabona, J.M. Miró, G. Touloumi, M. Garrido, R. Teira, F. Wit, J. Warszawski, L. Meyer, F. Dabis, M.M. Krause, J. Ghosn, C. Leport, M. Prins, H. Bucher, D. Gibb, G. Fätkenheuer, J. del Amo, C. Thorne, C. Stephan, S. Pérez-Hoyos, O. Hamouda, B. Bartmeyer, N. Chkhartishvili, A. Noguera-Julian, A. Antinori, A. d'Arminio Monforte, L. Prieto, P.R. Conejo, A. Soriano-Arandes, M. Battegay, R. Kouyos, P. Tookey, D. Konopnick, T. Goetghebuer, A. Sönnerborg, D. Haerry, S. de Wit, D. Costagliola, D. Raben, G. Chêne, F. Ceccherini-Silberstein, H. Günthard, A. Judd, D. Barger, C. Schwimmer, M. Termote, M. Campbell, C.M. Frederiksen, N. Friis-Møller, J. Kjaer, R.S. Brandt, J. Berenguer, J. Bohlius, V. Bouteloup, M. Davies, M. Dorrucci, M. Egger, H. Furrer, M. Guiguet, S. Grabar, O. Lambotte, V. Leroy, S. Lodi, S. Matheron, S. Monge, F. Nakagawa, R. Paredes, A. Phillips, M. Puoti, M. Schomaker, C. Smit, J. Sterne, R. Thiebaut, M. van der Valk, N. Wyss, V. Aubert, M. Battegay, E. Bernasconi, J. Böni, C. Burton-Jeangros, A. Calmy, M. Cavassini, G. Dollenmaier, M. Egger, L. Elzi, J. Fehr, J. Fellay, H. Furrer, C.A. Fux, M. Gorgievski, H. Günthard, D. Haerry, B. Hasse, H.H. Hirsch, M. Hoffmann, I. Hösli, C. Kahlert, L. Kaiser, O. Keiser, T. Klimkait, R. Kouyos, H. Kovari, B. Ledergerber, G. Martinetti, B. Martinez de Tejada, K. Metzner, N. Müller, D. Nadal, D. Nicca, G. Pantaleo, A. Rauch, S. Regenass, M. Rickenbach, C. Rudin, F. Schöni-Affolter, P. Schmid, J. Schüpbach, R. Speck, P. Tarr, A. Telenti, A. Trkola, P. Vernazza, R. Weber, S. Yerly. - In: JOURNAL OF ANTIMICROBIAL CHEMOTHERAPY. - ISSN 0305-7453. - 71:5(2016), pp. dkv465.1352-dkv465.1360.

Improved darunavir genotypic mutation score predicting treatment response for patients infected with HIRaben-1 subtype B and non-subtype B receiving a salvage regimen

C.F. Perno;A. d'Arminio Monforte;
2016

Abstract

Objectives: The objective of this studywas to improve the prediction of the impact of HIV-1 protease mutations in different viral subtypes on virological response to darunavir. Methods: Darunavir-containing treatment change episodes (TCEs) in patients previously failing PIs were selected from large European databases. HIV-1 subtype B-infected patients were used as the derivation dataset and HIV- 1 non-B-infected patients were used as the validation dataset. The adjusted association of each mutation with week 8 HIV RNA change from baseline was analysed by linear regression. A prediction model was derived based on best subset least squares estimation with mutational weights corresponding to regression coefficients. Virological outcome prediction accuracy was compared with that from existing genotypic resistance interpretation systems (GISs) (ANRS 2013, Rega 9.1.0 and HIVdb 7.0). Results: TCEs were selected from 681 subtype B-infected and 199 non-B-infected adults. Accompanying drugs were NRTIs in 87%, NNRTIs in 27%and raltegravir ormaraviroc or enfuvirtide in 53%. The predictionmodel included weighted protease mutations, HIV RNA, CD4 and activity of accompanying drugs. The model's association with week 8 HIV RNA change in the subtype B (derivation) set was R2=0.47 [average squared error (ASE)=0.67, P>10-6]; in the non-B (validation) set, ASE was 0.91. Accuracy investigated by means of area under the receiver operating characteristic curves with a binary response (above the threshold value of HIV RNA reduction) showed that our finalmodel outperformed models with existing interpretation systems in both training and validation sets. Conclusions: A model with a new darunavir-weighted mutation score outperformed existing GISs in both B and non-B subtypes in predicting virological response to darunavir.
English
Once-daily darunavir/ritonavir; treatment-experienced patients; virological response; HIV-1-infected patients; treatment-naive; antiretroviral treatment; resistance profile; protease; efficacy; therapy
Settore MED/07 - Microbiologia e Microbiologia Clinica
Articolo
Esperti anonimi
Pubblicazione scientifica
2016
Oxford University Press
71
5
dkv465
1352
1360
9
Pubblicato
Periodico con rilevanza internazionale
scopus
pubmed
crossref
WOS:000376291300030
2-s2.0-84965022891
26825119
Aderisco
info:eu-repo/semantics/article
Improved darunavir genotypic mutation score predicting treatment response for patients infected with HIRaben-1 subtype B and non-subtype B receiving a salvage regimen / A. De Luca, P. Flandre, D. Dunn, M. Zazzi, A. Wensing, M.M. Santoro, H.F. Günthard, L. Wittkop, T. Kordossis, F. Garcia, A. Castagna, A. Cozzi-Lepri, D. Churchill, S. De Wit, N.H. Brockmeyer, A. Imaz, C. Mussini, N. Obel, C.F. Perno, B. Roca, P. Reiss, E. Schülter, C. Torti, A. van Sighem, R. Zangerle, D. Descamps, A. Mocroft, O. Kirk, C. Sabin, S. De Wit, J. Casabona, J.M. Miró, G. Touloumi, M. Garrido, R. Teira, F. Wit, J. Warszawski, L. Meyer, F. Dabis, M.M. Krause, J. Ghosn, C. Leport, M. Prins, H. Bucher, D. Gibb, G. Fätkenheuer, J. del Amo, C. Thorne, C. Stephan, S. Pérez-Hoyos, O. Hamouda, B. Bartmeyer, N. Chkhartishvili, A. Noguera-Julian, A. Antinori, A. d'Arminio Monforte, L. Prieto, P.R. Conejo, A. Soriano-Arandes, M. Battegay, R. Kouyos, P. Tookey, D. Konopnick, T. Goetghebuer, A. Sönnerborg, D. Haerry, S. de Wit, D. Costagliola, D. Raben, G. Chêne, F. Ceccherini-Silberstein, H. Günthard, A. Judd, D. Barger, C. Schwimmer, M. Termote, M. Campbell, C.M. Frederiksen, N. Friis-Møller, J. Kjaer, R.S. Brandt, J. Berenguer, J. Bohlius, V. Bouteloup, M. Davies, M. Dorrucci, M. Egger, H. Furrer, M. Guiguet, S. Grabar, O. Lambotte, V. Leroy, S. Lodi, S. Matheron, S. Monge, F. Nakagawa, R. Paredes, A. Phillips, M. Puoti, M. Schomaker, C. Smit, J. Sterne, R. Thiebaut, M. van der Valk, N. Wyss, V. Aubert, M. Battegay, E. Bernasconi, J. Böni, C. Burton-Jeangros, A. Calmy, M. Cavassini, G. Dollenmaier, M. Egger, L. Elzi, J. Fehr, J. Fellay, H. Furrer, C.A. Fux, M. Gorgievski, H. Günthard, D. Haerry, B. Hasse, H.H. Hirsch, M. Hoffmann, I. Hösli, C. Kahlert, L. Kaiser, O. Keiser, T. Klimkait, R. Kouyos, H. Kovari, B. Ledergerber, G. Martinetti, B. Martinez de Tejada, K. Metzner, N. Müller, D. Nadal, D. Nicca, G. Pantaleo, A. Rauch, S. Regenass, M. Rickenbach, C. Rudin, F. Schöni-Affolter, P. Schmid, J. Schüpbach, R. Speck, P. Tarr, A. Telenti, A. Trkola, P. Vernazza, R. Weber, S. Yerly. - In: JOURNAL OF ANTIMICROBIAL CHEMOTHERAPY. - ISSN 0305-7453. - 71:5(2016), pp. dkv465.1352-dkv465.1360.
open
Prodotti della ricerca::01 - Articolo su periodico
154
262
Article (author)
si
A. De Luca, P. Flandre, D. Dunn, M. Zazzi, A. Wensing, M.M. Santoro, H.F. Günthard, L. Wittkop, T. Kordossis, F. Garcia, A. Castagna, A. Cozzi-Lepri, D. Churchill, S. De Wit, N.H. Brockmeyer, A. Imaz, C. Mussini, N. Obel, C.F. Perno, B. Roca, P. Reiss, E. Schülter, C. Torti, A. van Sighem, R. Zangerle, D. Descamps, A. Mocroft, O. Kirk, C. Sabin, S. De Wit, J. Casabona, J.M. Miró, G. Touloumi, M. Garrido, R. Teira, F. Wit, J. Warszawski, L. Meyer, F. Dabis, M.M. Krause, J. Ghosn, C. Leport, M. Prins, H. Bucher, D. Gibb, G. Fätkenheuer, J. del Amo, C. Thorne, C. Stephan, S. Pérez-Hoyos, O. Hamouda, B. Bartmeyer, N. Chkhartishvili, A. Noguera-Julian, A. Antinori, A. d'Arminio Monforte, L. Prieto, P.R. Conejo, A. Soriano-Arandes, M. Battegay, R. Kouyos, P. Tookey, D. Konopnick, T. Goetghebuer, A. Sönnerborg, D. Haerry, S. de Wit, D. Costagliola, D. Raben, G. Chêne, F. Ceccherini-Silberstein, H. Günthard, A. Judd, D. Barger, C. Schwimmer, M. Termote, M. Campbell, C.M. Frederiksen, N. Friis-Møller, J. Kjaer, R.S. Brandt, J. Berenguer, J. Bohlius, V. Bouteloup, M. Davies, M. Dorrucci, M. Egger, H. Furrer, M. Guiguet, S. Grabar, O. Lambotte, V. Leroy, S. Lodi, S. Matheron, S. Monge, F. Nakagawa, R. Paredes, A. Phillips, M. Puoti, M. Schomaker, C. Smit, J. Sterne, R. Thiebaut, M. van der Valk, N. Wyss, V. Aubert, M. Battegay, E. Bernasconi, J. Böni, C. Burton-Jeangros, A. Calmy, M. Cavassini, G. Dollenmaier, M. Egger, L. Elzi, J. Fehr, J. Fellay, H. Furrer, C.A. Fux, M. Gorgievski, H. Günthard, D. Haerry, B. Hasse, H.H. Hirsch, M. Hoffmann, I. Hösli, C. Kahlert, L. Kaiser, O. Keiser, T. Klimkait, R. Kouyos, H. Kovari, B. Ledergerber, G. Martinetti, B. Martinez de Tejada, K. Metzner, N. Müller, D. Nadal, D. Nicca, G. Pantaleo, A. Rauch, S. Regenass, M. Rickenbach, C. Rudin, F. Schöni-Affolter, P. Schmid, J. Schüpbach, R. Speck, P. Tarr, A. Telenti, A. Trkola, P. Vernazza, R. Weber, S. Yerly
01 - Articolo su periodico
File in questo prodotto:
File Dimensione Formato  
2016_Improved darunavir genotypic mutation score predicting treatment response for patients infected with HIV-1 subtype B_J Antimicrob Chemother.pdf

accesso aperto

Tipologia: Publisher's version/PDF
Dimensione 312.43 kB
Formato Adobe PDF
Visualizza/Apri
312.43 kB Adobe PDF Visualizza/Apri
Pubblicazioni consigliate

I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.

Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/558937
Citazioni
  • ???jsp.display-item.citation.pmc??? 1
  • Scopus 4
  • ???jsp.display-item.citation.isi??? 4
social impact