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Low frequency of genotypic resistance in HIV-1-infected patients failing an atazanavir-containing regimen: a clinical cohort study
- Dolling, David I;
- Dunn, David T;
- Sutherland, Katherine A;
- Pillay, Deenan;
- Mbisa, Jean L;
- Parry, Chris M;
- Post, Frank A;
- Sabin, Caroline A;
- Cane, Patricia A;
- Aitken, Celia;
- Asboe, David;
- Webster, Daniel;
- Cane, Patricia;
- Castro, Hannah;
- Dunn, David;
- Dolling, David;
- Chadwick, David;
- Churchill, Duncan;
- Clark, Duncan;
- Collins, Simon;
- Delpech, Valerie;
- Geretti, Anna Maria;
- Goldberg, David;
- Hale, Antony;
- Hué, Stéphane;
- Kaye, Steve;
- Kellam, Paul;
- Lazarus, Linda;
- Leigh-Brown, Andrew;
- Mackie, Nicola;
- Orkin, Chloe;
- Rice, Philip;
- Pillay, Deenan;
- Phillips, Andrew;
- Sabin, Caroline;
- Smit, Erasmus;
- Templeton, Kate;
- Tilston, Peter;
- Tong, William;
- Williams, Ian;
- Zhang, Hongyi;
- Zuckerman, Mark;
- Greatorex, Jane;
- Wildfire, Adrian;
- O'Shea, Siobhan;
- Mullen, Jane;
- Mbisa, Tamyo;
- Cox, Alison;
- Tandy, Richard;
- Hale, Tony;
- Fawcett, Tracy;
- Hopkins, Mark;
- Ashton, Lynn;
- Booth, Claire;
- Garcia-Diaz, Ana;
- Shepherd, Jill;
- Schmid, Matthias L;
- Payne, Brendan;
- Hay, Phillip;
- Rice, Phillip;
- Paynter, Mary;
- Bibby, David;
- Kirk, Stuart;
- MacLean, Alasdair;
- Gunson, Rory;
- Coughlin, Kate;
- Fearnhill, Esther;
- Fradette, Lorraine;
- Porter, Kholoud;
- Ainsworth, Jonathan;
- Anderson, Jane;
- Babiker, Abdel;
- Fisher, Martin;
- Gazzard, Brian;
- Gilson, Richard;
- Gompels, Mark;
- Hill, Teresa;
- Johnson, Margaret;
- Kegg, Stephen;
- Leen, Clifford;
- Nelson, Mark;
- Palfreeman, Adrian;
- Post, Frank;
- Sachikonye, Memory;
- Schwenk, Achim;
- Walsh, John;
- Huntington, Susie;
- Jose, Sophie;
- Thornton, Alicia;
- Glabay, Adam;
- Orkin, C;
- Garrett, N;
- Lynch, J;
- Hand, J;
- de Souza, C;
- Fisher, M;
- Perry, N;
- Tilbury, S;
- Gazzard, B;
- Nelson, M;
- Waxman, M;
- Asboe, D;
- Mandalia, S;
- Delpech, V;
- Anderson, J;
- Munshi, S;
- Korat, H;
- Welch, J;
- Poulton, M;
- MacDonald, C;
- Gleisner, Z;
- Campbell, L;
- Gilson, R;
- Brima, N;
- Williams, I;
- Schwenk, A;
- Ainsworth, J;
- Wood, C;
- Miller, S;
- Johnson, M;
- Youle, M;
- Lampe, F;
- Smith, C;
- Grabowska, H;
- Chaloner, C;
- Puradiredja, D;
- Walsh, J;
- Weber, J;
- Ramzan, F;
- Mackie, N;
- Winston, A;
- Leen, C;
- Wilson, A;
- Allan, S;
- Palfreeman, A;
- Moore, A;
- Wakeman, K
- et al.
Published Web Location
https://doi.org/10.1093/jac/dkt199Abstract
Objectives
To determine protease mutations that develop at viral failure for protease inhibitor (PI)-naive patients on a regimen containing the PI atazanavir.Methods
Resistance tests on patients failing atazanavir, conducted as part of routine clinical care in a multicentre observational study, were randomly matched by subtype to resistance tests from PI-naive controls to account for natural polymorphisms. Mutations from the consensus B sequence across the protease region were analysed for association and defined using the IAS-USA 2011 classification list.Results
Four hundred and five of 2528 (16%) patients failed therapy containing atazanavir as a first PI over a median (IQR) follow-up of 1.76 (0.84-3.15) years and 322 resistance tests were available for analysis. Recognized major atazanavir mutations were found in six atazanavir-experienced patients (P < 0.001), including I50L and N88S. The minor mutations most strongly associated with atazanavir experience were M36I, M46I, F53L, A71V, V82T and I85V (P < 0.05). Multiple novel mutations, I15S, L19T, K43T, L63P/V, K70Q, V77I and L89I/T/V, were also associated with atazanavir experience.Conclusions
Viral failure on atazanavir-containing regimens was not common and major resistance mutations were rare, suggesting that adherence may be a major contributor to viral failure. Novel mutations were described that have not been previously documented.Many UC-authored scholarly publications are freely available on this site because of the UC's open access policies. Let us know how this access is important for you.
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