Baseline Resistance and Virological Outcome in Patients with Virological Failure who Start a Regimen Containing Abacavir: Eurosida Study

Author:

,Cabrera Cecilia1,Cozzi-Lepri Alessandro2,Phillips Andrew N2,Loveday Clive3,Kirk Ole4,Ait-Khaled Mounir5,Reiss Peter6,Kjær Jesper4,Ledergerber Bruno7,Lundgren Jens D4,Clotet Bonaventura1,Ruiz Lidia1,Losso M8,Duran A8,Vetter N9,Clumeck N10,Hermans P10,Sommereijns B10,Colebunders R11,Machala L12,Rozsypal H12,Nielsen J13,Lundgren J13,Benfield T13,Kirk O13,Gerstoft J14,Katzenstein T14,Røge B14,Skinhøj P14,Pedersen C15,Zilmer K16,Katlama C17,De Sa M17,Viard J-P18,Saint-Marc T19,Vanhems P20,Pradier C21,Dietrich M22,Manegold C22,van Lunzen J23,Stellbrink H-J23,Miller V24,Staszewski S24,Goebel F-D25,Salzberger Bernd26,Rockstroh J27,Kosmidis J28,Gargalianos P28,Sambatakou H28,Perdios J28,Panos G29,Karydis I29,Filandras A29,Banhegyi D30,Mulcahy F31,Yust I32,Burke M32,Pollack S33,Ben-Ishai Z33,Bentwich Z34,Maayan S35,Vella S36,Chiesi A36,Arici C37,Pristerá R38,Mazzotta F39,Gabbuti A39,Esposito R40,Bedini A40,Chirianni A41,Montesarchio E41,Vullo V42,Santopadre P42,Narciso P43,Antinori A43,Franci P43,Zaccarelli M43,Lazzarin A44,Finazzi R44,D'Arminio Monforte A45,Viksna L46,Chaplinskas S47,Hemmer R48,Staub T48,Reiss P49,Bruun J50,Maeland A50,Ormaasen V50,Knysz B51,Gasiorowski J51,Horban A52,Prokopowicz D53,Wiercinska-Drapalo A53,Boron-Kaczmarska A54,Pynka M54,Beniowski M55,Trocha H56,Antunes F57,Mansinho K58,Proenca R59,Duiculescu D60,Streinu-Cercel A61,Mikras M62,González-Lahoz J63,Diaz B63,García-Benayas T63,Martin-Carbonero L63,Soriano V63,Clotet B64,Jou A64,Conejero J64,Tural C64,Gatell JM65,Miró JM65,Blaxhult A66,Karlsson A67,Pehrson P68,Ledergerber B69,Weber R69,Francioli P70,Telenti A70,Hirschel B71,Soravia-Dunand V71,Furrer H72,Chentsova N73,Barton S74,Johnson AM75,Mercey D75,Phillips A76,Loveday C76,Johnson MA76,Mocroft A76,Pinching A77,Parkin J77,Weber J78,Scullard G78,Fisher M79,Brettle R80

Affiliation:

1. IrsiCaixa Foundation & Lluita contra la SIDA Foundation, Badalona, Spain

2. Royal Free Centre for HIV Medicine, London, UK

3. International Clinical Virology Centre (ICVC), Buckinghamshire, UK

4. EuroSIDA Coordinating Centre, Hvidovre University Hospital, Hvidovre, Denmark

5. GlaxoSmithKline, Greenford, UK

6. Academisch Medisch Centrum bij de Universiteit van Amsterdam, Amsterdam, the Netherlands

7. University Hospital, Zurich, Switzerland

8. Hospital JM Ramos Mejia, Buenos Aires. Argentina

9. Pulmologisches Zentrum der Stadt Wien, Vienna. Austria

10. Saint-Pierre Hospital, Brussels; Belgium

11. Institute of Tropical Medicine, Antwerp.

12. Faculty Hospital Bulovka, Prague. Czech Republic

13. Hvidovre Hospital, Copenhagen; Denmark

14. Rigshospitalet, Copenhagen

15. Odense University Hospital, Odense

16. Tallinn Merimetsa Hospital, Tallinn. Estonia

17. Hôpital de la Pitié-Salpêtière, Paris; France

18. Hôpital Necker-Enfants Malades, Paris

19. Hôpital Edouard Herriot, Lyon

20. University Claude Bernard, Lyon

21. Hôpital de l'Archet, Nice

22. Bernhard-Nocht-Institut for Tropical Medicine, Hamburg; Germany

23. Eppendorf Medizinische Kernklinik, Hamburg

24. JW Goethe University Hospital, Frankfurt

25. Medizinische Poliklinik, Munich

26. Universität Köln, Cologne

27. Universitäts Klinik, Bonn

28. Athens General Hospital, Athens; Greece

29. 1st IKA Hospital, Athens

30. Szent Lásló Hospital, Budapest. Hungary

31. St James's Hospital, Dublin. Ireland

32. Ichilov Hospital, Tel Aviv; Israel

33. Rambam Medical Center, Haifa

34. Kaplan Hospital, Rehovot

35. Hadassah University Hospital, Jerusalem

36. Istituto Superiore di Sanita, Rome; Italy

37. Ospedale Riuniti, Bergamo

38. Ospedale Generale Regionale, Bolzano

39. Ospedale S Maria Annunziata, Florence

40. Università di Modena, Modena

41. Presidio Ospedaliero AD Cotugno, Naples

42. Università di Roma La Sapienza, Rome

43. Ospedale Spallanzani, Rome

44. Ospedale San Raffaele, Milan

45. Osp L Sacco, Milan

46. Infectology Centre of Latvia, Riga. Latvia

47. Lithuanian AIDS Centre, Vilnius. Lithuania

48. Centre Hospitalier, Luxembourg. Luxembourg

49. Academisch Medisch Centrum bij de Universiteit van Amsterdam, Amsterdam. Netherlands

50. Ullevål Hospital, Oslo. Norway

51. Medical University, Wroclaw; Poland

52. Centrum Diagnostyki i Terapii AIDS, Warsaw

53. Medical University, Bialystok

54. Medical Univesity, Szczecin

55. Osrodek Diagnostyki i Terapii AIDS, Chorzow

56. Medical University, Gdansk

57. Hospital Santa Maria, Lisbon; Portugal

58. Hospital de Egas Moniz, Lisbon

59. Hospital Curry Cabral, Lisbon

60. Spitalul de Boli Infectioase si Tropicale Dr Victor Babes, Bucharest; Romania

61. Institute of Infectious Diseases, Bucarest

62. Derrer Hospital, Bratislava. Slovakia

63. Hospital Carlos III, Madrid; Spain

64. Hospital Germans Trias i Pujol, Barcelona

65. Hospital Clinic i Provincial, Barcelona

66. Karolinska Hospital, Stockholm; Sweden

67. Södersjukhuset, Stockholm

68. Huddinge Sjukhus, Stockholm

69. University Hospital, Zürich

70. Centre Hospitalier Universitaire Vaudois, Lausanne; Switzerland

71. Hospital Cantonal Universitaire de Geneve, Geneve

72. Inselspital Bern, Bern

73. Kiev Centre for AIDS, Kiev. Ukraine

74. St Stephen's Clinic, Chelsea and Westminster Hospital, London; United Kingdom

75. Royal Free and University College London Medical School, London University College Campus

76. Royal Free and University College Medical School, London Royal Free Campus

77. Medical College of Saint Bartholomew's Hospital, London

78. Imperial College School of Medicine at St Mary's, London

79. Royal Sussex County Hospital, Brighton

80. Western General Hospital, Edinburgh

Abstract

ObjectivesTo investigate the ability of several HIV-1 drug-resistance interpretation systems, as well as the number of pre-specified combinations of abacavir-related mutations, to predict virological response to abacavir-containing regimens in antiretroviral therapy-experienced, abacavir-naive patients starting an abacavir-containing regimen in the EuroSIDA cohort.Patients and methodsA total of 100 HIV-infected patients with viral load (VL) >500 copies/ml who had a plasma sample available at the time of starting abacavir (baseline) were included. Resistance to abacavir was interpreted by using eight different commonly used systems that consisted of rules-based algorithms or tables of mutations. Correlation between baseline abacavir-resistance mutations and month 6 virological response was performed on this population using a multivariable linear regression model accounting for censored data.ResultsThe baseline VL was 4.36 log10RNA copies/ml [interquartile range (IQR): 3.65–4.99 log10RNA copies/ml] and the median CD4 cell count was 210 cells/μl (IQR: 67–305 cells/μl). Our patients were pre-exposed to a median of seven antiretrovirals (2–12) before starting abacavir therapy. The median (range) number of abacavir mutations (according to the International AIDS Society-USA) detected at baseline was 3.5 (0–8). Overall, the Kaplan–Meier estimate of the median month 6 VL decline was 0.86 log10RNA copies/ml [95% confidence intervals (95% CI): 0.45–1.24]. The VL in those patients ( n=31) who intensified treatment by adding only abacavir decreased by a median 0.20 log10RNA copies/ml (95% CI: -0.18; +0.94). The proportion of patients who harboured viruses fully resistant to abacavir among the eight genotypic resistance interpretation algorithms ranged from 12% [Agence Nationale de Recherches sur le SIDA (ANRS)] to 79% [Stanford HIV RT and PR Sequence Database (HIVdb)]. Some interpretation systems showed statistically significant associations between the predicted resistance status and the virological response while others showed no consistent association. The number of active drugs in the regimen was associated with greater virological suppression (additional month 6 VL reduction per additional sensitive drug=0.51, 95% CI: 0.15–0.88, P=0.006); baseline VL was also weakly associated (additional month 6 VL reduction per log10higher=0.30, 95% CI: -0.02; +0.62, P=0.06). In contrast, the number of drugs previously received was associated with diminished viral reduction (additional month 6 VL reduction per additional drug=-0.14, 95% CI: -0.28; 0.00, P=0.05).ConclusionsOur results revealed a high degree of variability among several genotypic resistance interpretation algorithms currently in use for abacavir. Therefore, the interpretation of genotypic resistance for predicting response to regimens containing abacavir remains a major challenge.

Publisher

SAGE Publications

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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