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HIV co-receptor tropism in treatment-naïve patients: impact on CD4 decline and subsequent response to HAART Laura Waters, Sundhiya Mandalia, Adrian Wildfire, Paul Randell, Brian Gazzard & Graeme Moyle. St Stephen’s Centre, Chelsea & Westminster Hospital, London, UK
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R5 viruses (M-tropic, NSI) Transmitted variants Prevalent in early disease X4 viruses (T-tropic, SI) Late disease; associated with CD4 decline, HIV RNA increase and clinical progression Dual-tropic viruses use CCR5 or CXCR4 (in vitro) CCR5 Q L S D T F F L R A P I A L H Y V L V W L F I L S T V L A L I V I V V Y A S L Y N H S Y V P I F L A G V I D T F L V V W P L I A I C I I V G H Y I L G L I I C I S L P M V I L T F Y G W I I V F I P S C L T A Y L I A G V I T Y P I I G L G L T S F F N V I V I I L L M G Y L N F C A I F W P Y C L T L I F I A L G G A S H A K D L K K M T RS D F L C K N Y F G D R Y L A I V NS R P R K L L A K E H T Q V S E A D D R Y I C D N DL W V V V F Q F Q F P Y R S K L S K L A K R K Q HG K S H D S F I L L E I I KQ G C E F E N T H K V L K K L F K T S A Q H V S R G S S A T S G I L S K G K R T E S E SS S F G H S S V S H S S V A A N W K N F N A N E E R F C P E K M S D Y D G S G M E E T Y N D S T Y I S I GE M - NH 2 * * * N 39- -6575- -97 110- -133154- -176-202 224--239 -262 -282 308- -352 F A CXCR4 352 C L A D T F F H L L S P L A F N Y I V L W L L F I G F G F L I L I L I L F I T F Y G T S S T V L I F T I T V G S F V V V W P A I A G C M V L L I Y I V G L V L S L I L P I V T I L F Y V W L M F Y I P L F I I V N A L L M V I F Y P V G L G L S L F N V F I L L I L I N I N F C T V M A P Y C V T L M T I A I G E G Q H E I D L K R M T K S Y T M C Q N F G R Y L A V V A FA K A R T V T F V G H VL S Q K EG L H Y T C S Y S QY Q F W K N F Q H P F S K T L L V H R K KE N R C R N T F Q E F F G L N N C S S S N R D Q L C K K F F RN Y L L V H I AK R F F Q K A C C S I F QQ S V Y TR S T G E P E R A S E Q E A A A Q A A I Q K V N I K Q C P E S T YY N I D Y I P S S V Q YDM - NH 2 - COOH R 31- -57 67- -89 102- -125146- -168-197 219- -235 -258 303- T L R A I S VG L R P L D K R 277- D W CCR5- & CXCR4-tropic HIV
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Prevalence of Co-receptor Usage Study/SourcePopulationR5X4X4/R5 Maraviroc Phase 2 a Naive9406 Homer cohort b (n=979) Naive83<117 C & W cohort c (n=563) Naïve/ Experienced 85<115 GSK d (n=299) Naive88012 TORO 1/2 e Experienced62434 ViroLogic f Experienced50248 a Data on filed Demarest et al. ICAAC 2004. Abstract H-1136 b Brumme ZL et al. JID 2005;192(3):466-74.e Whitcomb et al. CROI 2003. Abstract 557 c Moyle GJ et al. JID 2005;191(6):866-72 f Huang et al. ICAAC 2002. Abstract 2040
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Prevalence and Predictive Factors for R5 and X4 Coreceptor Usage Prevalence (%) CD4 (cells/mm 3 ) 84.3% 59.3% 300 300 (n=81) (n=185) (n=248) (n=81) (n=185) (n=248) 83.5% R5 Prevalence 563 HIV patients –85% male –66% Caucasian –Mean age: 44 years –Clade B: 76% –R5 tropic: 85% –R5/X4 dual tropic: 15% Moyle GJ, et al. JID 2005 Mean R5 Tropic R5/ X4 Tropic CD4 (cells/mm 3 ) 307*231 HIV RNA (copies/mL) 35,800 † 66,228 *P=0.007; † P<0.001.
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Prevalence of R5 Use by Baseline CD4 and HIV RNA Levels Prevalence of R5 Use (%) 100806040200 300 300 Baseline CD4 (cells/mm 3 ) >100K >100K Baseline HIV RNA (copies/mL) >5-50K >5-50K >50-100K >50-100K <5K <5K n=563. Moyle GJ, et al. JID 2005
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Clinical Progression & Response to HAART Swiss HIV Cohort 96 progressors vs. 84 matched non-progressors R5 at baseline (n=84) X4/R5 at baseline (n=84) Significance CD4 rise at 6 months 8240p = 0.012 HIV RNA < 500 at 6 months 57 (68%)27 (32%)p = 0.33 Hazard ratio for clinical progression 1.004.0095% CI 1.83 – 8.72 Phillpott et al. IAS 2006. Abstract THAA0201
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Determination of R5/X4 Tropism Two potential roles for tropism testing: Guiding therapy decisions Predicting disease progression
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Aim To study the impact of R5/X4 tropism as determined by the ViroLogic Phenosense Assay on: The rate of CD4 decline prior to commencing therapy Response to therapy: - CD4 rise - Time to HIV RNA < 50 c/mL - Proportion with HIV RNA < 50 c/mL
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Methods Study Design Subjects from epidemiology study: R5 tropic vs. X4/mixed/dual tropic Prospective cohort database used to record: - Sequential CD4 counts from tropism test to HAART initiation (censored if < 3 months) - Sequential CD4 counts and HIV RNA after HAART - HAART regimen prescribed
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Methods Response to HAART HAART defined as: - ≥ 2NRTI + NNRTI - ≥ 2NRTI + PI (unboosted) - ≥ 2NRTI + PI/r (boosted) Exclusions: - Non-HAART regimens - < 6 months follow-up Data censored at: - 96 weeks - End of follow-up - Therapy switch for virological failure
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Methods Statistics CD4 decline: DAVG using MIXED model adjusted for baseline HIV RNA CD4 response to HAART: univariate + multivariate linear MIXED model (adj. for baseline HIV RNA and HAART) Proportion with HIV RNA < 50 c/mL: 2 test Time to HIV RNA < 50 c/mL: survival analysis; Cox’s proportional hazards regression to adj. for baseline HIV RNA and HAART
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Results 402 naïve subjects tropism tested: - 326 R5 - 73 X4/R5 (mixed/dual) - 3 X4 340 commenced HAART by August 2006 - 51 excluded from analysis* - 229 R5 - 60 X4/mixed/dual 62 remained off therapy *< 6/12 follow-up (n=28); non-HAART (n=23)
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Baseline Demographics R5-tropic (n=326) X4/R5 (n=76) p-value Male288 (88.3%)72 (94.7%)0.101 White Black Other 236 (72.4%) 44 (13.5%) 46 (14.1%) 50 (65.8%) 9 (11.8%) 17 (22.4%) 0.203 CD4 (IQR)325 (207-458)203 (58-375)<0.001 HIV RNA (IQR)39385 (13358-120818)142568 (47186-275726)<0.001 Mutations NRTI NNRTI PI ------ ------ 0.826 0.893 0.550 Clade B Clade Other Untested 252 (77.3%) 57 (17.5%) 17 (5.2%) 64 (84.2%) 11 (14.5%) 1 (1.3%) 0.242
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Baseline Genotypic Resistance R5-tropic (n=326)X4-tropic (n=76)p-value NRTI mutations: 0 1 2 3 ≥4 untested 286 (87.7%) 19 (5.8%) 4 (1.2%) 2 (0.6%) 1 (0.4%) 14 (4.3%) 66 (86.8%) 5 (6.6%) 1 (1.3%) 2 (2.7%) 0.826 PI mutations: 0 1 2 3 ≥4 untested 304 (93.3%) 3 (0.8%) 2 (0.6%) 1 (0.4%) 2 (0.6%) 14 (4.3%) 69 (90.8%) 2 (2.7%) 1 (1.3%) 2 (2.7%) 0.550 NNRTI mutations 0 1 ≥2 untested 302 (92.6%) 6 (1.8%) 4 (1.2%) 14 (4.3%) 71 (93.4%) 1 (1.3%) 2 (2.7%) 0.893
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-600 -500 -400 -300 -200 -100 0 100 200 300 400 3691215182124 Duration since sample result (months) CD4 count from time when sample taken Naïve : R5Naïve : X4/R5 DAVG analysis (time weighted differences in average. Censored at HAART; Error bars are 95% CI p = 0.562 p = 0.026 R5 n= 187 119 127 100 107 76 74 72 93 X4 n= 23 18 13 9 11 6 5 2 2 CD4 decline before HAART
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R5 n= 229 197 190 188 194 172 161 151 182 X4 n= 60 51 2650 56 44 47 50 50 CD4 rise on HAART -600 -500 -400 -300 -200 -100 0 100 200 300 400 03691215182124 Duration since sample result (months) CD4 count from time when sample taken Naïve: R5Naïve: X4/R5 Time weighted differences in averages (DAVG) from baseline estimated using linear MIXED model
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CD4 rise on HAART R5X4/R5p-value 12 months mean (95% CI) 185 (166-204) 182 (145-219) 0.812 24 months mean (95% CI) 247 (227-267) 292 (254-330) 0.482
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Rates of Viral Suppression 289 subjects (229 R5, 60 X4/R5) started HAART R5 tropic (n=229) X4/R5 tropic (n=60) p-value N (%) with HIV RNA < 50 at 6 months 163 (71.2%) 45 (75.0%) 0.637 N (%) with HIV RNA < 50 at 12 months 168 (73.4%) 47 (78.3%) 0.509 N (%) with HIV RNA < 50 at 24 months 166 (72.5%) 41 (68.3%) 0.670
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Time to Viral Suppression 0 0.1 0.2 0.3 0.4 0.5 0.6 0.7 0.8 0.9 1 069151821 Duration since sample result (months) Proportion achieving VL<50 copies/ml R5X4/R5 R5 n= 229 197 190 188 194 172 161 151 X4 n= 60 51 2650 56 44 47 50 312 Survival analysis; Cox’s proportional hazards regression to adjust for baseline HIV RNA and HAART
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Conclusions Subjects with X4 HIV-1 experience more rapid CD4 decline than those with R5 patients (adjusted for baseline viral load) Similar proportions achieve viral suppression at 1 year and 2 years CD4 rise similar over 96 weeks of HAART Time to viral suppression same for R5 and X4 virus when adjusted for baseline viral load
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Acknowledgements Dr Marta Boffito All the St Stephen’s Centre patients Pfizer for funding of tropism testing Monogram Biosciences
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