| Literature DB >> 26512902 |
Andargachew Mulu1, Melanie Maier2, Uwe Gerd Liebert2.
Abstract
The emergence of HIV-1 drug resistance mutations has mainly been linked to the duration and composition of antiretroviral treatment (ART), as well as the level of adherence. This study reports the incidence and pattern of acquired antiretroviral drug resistance mutations and long-term outcomes of ART in a prospective cohort from Northwest Ethiopia. Two hundred and twenty HIV-1C infected treatment naïve patients were enrolled and 127 were followed-up for up to 38 months on ART. ART initiation and patients' monitoring was based on the WHO clinical and immunological parameters. HIV viral RNA measurement and drug resistance genotyping were done at baseline (N = 160) and after a median time of 30 (IQR, 27-38) months on ART (N = 127). Viral suppression rate (HIV RNA levels ≤ 400 copies/ml) after a median time of 30 months on ART was found to be 88.2% (112/127), which is in the range for HIV drug resistance prevention suggested by WHO. Of those 15 patients with viral load >400 copies/ml, six harboured one or more drug resistant associated mutations in the reverse transcriptase (RT) region. Observed NRTIs resistance associated mutations were the lamivudine-induced mutation M184V (n = 4) and tenofovir associated mutation K65R (n = 1). The NNRTIs resistance associated mutations were K103N (n = 2), V106M, Y181S, Y188L, V90I, K101E and G190A (n = 1 each). Thymidine analogue mutations and major drug resistance mutations in the protease (PR) region were not detected. Most of the patients (13/15) with virologic failure and accumulated drug resistance mutations had not met the WHO clinical and/or immunological failure criteria and continued the failing regimen. The incidence and pattern of acquired antiretroviral drug resistance mutations is lower and less complex than previous reports from sub Saharan Africa countries. Nevertheless, the data suggest the need for virological monitoring and resistance testing for early detection of failure. Moreover, adherence reinforcement will contribute to improving overall treatment outcomes.Entities:
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Year: 2015 PMID: 26512902 PMCID: PMC4626118 DOI: 10.1371/journal.pone.0141318
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Fig 1Cohort profile.
Of the 220 subjects enrolled in the study 63.6% (140/220) were on ART and blood collection for HIV DR was successful in 127 patients; Confirmed death: 12.7% (28/220); overall death including true loss: 27.3% (60/220); True loss: 14.5% (32/220).
Characteristics of the patients classified as non viremic or viremic after a median time of 30 months on ART (upper) and median CD4 T cell and RNA values (lower).
| Characteristics | Non viremic | Viremic |
|---|---|---|
| Gender | ||
| Male | 48 (42.8) | 6 (40) |
| Female | 64 (57.2) | 9 (60) |
| WHO stage at ART initiation | ||
| Stage I/II | 40 (35.7) | 4 (26.7) |
| Stage III/IV | 72 (64.3) | 11 (73.3) |
| CD4+ T cell count at baseline | ||
| <200 cells/ mm3 | 62 (55.4) | 7 (46.7) |
| ≥200 cells/ mm3 | 50 (44.6) | 8 (53.3) |
| CD4+ T cell counts at 30 months of ART | ||
| <200 cells/ mm3 | 6 (5.4) | 3 (20.0) |
| ≥200 cells/ mm3 | 106 (94.6) | 12 (80.0) |
| First line ART | ||
| 3TC + D4T + NVP | 52 (46.4) | 6 (40.0) |
| 3TC + D4T + EFV | 21 (18.8) | 2 (13.3) |
| 3TC + AZT + NVP | 27 (24.1) | 3 (20.0) |
| 3TC + AZT + EFV | 12 (10.7) | 4 (26.7) |
| Median (IQR) age [Years] | 33 (18–62) | 33.8 (23–58) |
| Median (IQR) CD4+ T cells/mm3at baseline | 204 (26–203) | 170 (75–229) |
| Median (IQR)CD4+T cells/mm3 at 30m of ART | 365 (259–434) | 387 (299–426) |
| Median (IQR) HIV RNA level at baseline | 57328 (20481–172442) | 19059 (5754–51833) |
| HIV RNA at 30 months of ART | ||
| Undetectable | 83 (74.1) | 0 |
| 1–40 | 6 (5.4) | 0 |
| 41–400 | 23 (20.5) | 0 |
| 401–5000 | 0 | 5 (33.3) |
| >5000 | 0 | 10 (66.7) |
| Median follow up time (IQR) [months] | 30.0 (26–36) | 31.0 (25–35) |
* HIV RNA < 400 copies/ml;
¶HIV RNA ≥ 400 copies/ml;
3TC (lamiduvine), D4T (stavudine), ZDV (zidovudine), TDF (tenofovir), EFV (efavirenz), NVP (nevirapine); IQR (Inter quartile range)
Acquired antiretroviral drug resistance mutations among subtype C Ethiopian patients after a median time of 30 months on ART.
| CD4+ T cells | HIV RNA | Baseline ART | Time on ART | NRTI | NNRTI | ||||||
|---|---|---|---|---|---|---|---|---|---|---|---|
| ID | Age/Gender | before | after | before | after | mutation | resistant | mutation | resistant | ||
| 5622–2 | 51/M | 250 | 391 | 26,915 | 19,952 | 3TC+D4T+EFV | 25 | M184V | 3TC, FTC | K103N | EFV, NVP |
| 5593–2 | 28/M | 401 | 449 | 14,791 | 2,511 | 3TC+D4T+EFV | 35 | M184V | 3TC, FTC | K103N | EFV, NVP |
| V106M | EFV, NVP, ETR | ||||||||||
| 5685–2 | 25/F | 229 | 393 | 26, 9153 | 91,201 | 3TC+D4T+NVP | 29 | None | - | Y181SY | NVP |
| 5524–2 | 38/M | 8 | 276 | 9,120 | 91,201 | 3TC+D4T+NVP | 33 | K65R | 3TC,DDI,FTC, TDF | Y188L | EFV, NVP |
| 5603–2 | 25/F | 32 | 270 | 158 | 4,786 | 3TC+D4T+NVP | 29 | M184V | 3TC, FTC | V90I | EFV, NVP, ETR |
| K101E | EFV, NVP, ETR | ||||||||||
| G190A | EFV, NVP, ETR | ||||||||||
| 5476–2 | 29/F | 199 | 281 | 26,302 | 53,703 | 3TC+D4T+EFV | 35 | M184V | 3TC, FTC | None | - |
| 5708–2 | 38/F | 274 | 319 | 1,071 | 26,915 | 3TC+D4T +NVP | 29 | None | - | None | - |
| 5591–2 | 30/M | 32 | 299 | 5,754 | 97,923 | 3TC+D4T+NVP | 31 | None | - | None | - |
| 5542–2 | 42/F | 75 | 474 | 33,414 | 442 | 3TC+D4T+NVP | 28 | None | - | None | - |
| 5776–2 | 40/M | 191 | 426 | 80,013 | 553 | 3TC+D4T+NVP | 32 | None | - | None | - |
| 5666–2 | 38/F | 157 | 387 | 51,833 | 889 | 3TC+D4T+NVP | 36 | None | - | None | - |
| 5684–2 | 50/F | 95 | 416 | 103,443 | 1,570 | 3TC+D4T+EFV | 34 | None | - | None | - |
| 5726–2 | 40/F | 170 | 383 | 19,059 | 1,886 | 3TC+D4T+EFV | 32 | None | - | None | - |
| 5573–2 | 51/M | 112 | 463 | 11,433 | 871 | 3TC+D4T+NVP | 30 | None | - | None | - |
| 5635–2 | 35/M | 211 | 301 | 5,635 | 1,471 | 3TC+D4T+EFV | 29 | None | - | None | - |
Age: in years; F: Female, M: Male; CD4+ T in cells/mm3; HIV RNA in copies/ml; Before: Before ART (baseline); After: After initiation of ART; Time on ART in months; NRTI (Nucleoside RT inhibitors): 3TC (lamiduvine), ddI (didanosine), d4T (stavudine), FTC (emtricitabine), TDF (tenofovir), ZDV (zidovudine); NNRTI (non-nucleoside RT inhibitors): EFV (efavirenz), ETR (etravirine), NVP (nevirapine); Amino acids: A (alanine), E (glutmatate), G (glucine), K (lysine), L (leucine), M (methionine), N (asparganine), S (serine), V (valine), Y (tyrosine)
Fig 2Immunological restoration among HIV-1C Ethiopian patients (N = 127 at each time point) during 30 months of ART.
Factors associated with virological failure by 30 months of ART.
| Variables | Crude | Adjusted | ||
|---|---|---|---|---|
| OR (95% CI) | P value | OR (95% CI) | P value | |
| Gender | ||||
| Male | Reference | |||
| Female | 1.23 (0.56–2.57) | 0.09 | 1.37 (0.65–3.17) | 0.12 |
| Age (years) | 0.91 (0.81–1.12) | 0.18 | 0.94(0.83–1.17) | 0.27 |
| Baseline WHO clinical stage | ||||
| Stage I | Reference | |||
| Stage II | 2.13(0.63–6.73) | 0.13 | 1.89(0.54–6.17) | 0.19 |
| Stage III | 1.38 (0.48–4.72) | 0.17 | 3.81 (0.81–4.12) | 0.07 |
| Stage IV | 0.88 (0.31–4.63) | 0.22 | 1.28 (1.74–9.19) | 0.8 |
| Baseline CD4+ T cell counts | ||||
| >200 | Reference | |||
| 50–200 | 1.49 (0.19–4.13) | 0.66 | 1.58(0.43–5.34) | 0.34 |
| <50 | 1.74 (0.37–4.39) | 0.69 | 1.83(0.44–5.76) | 0.39 |
| Baseline HIV RNA level | ||||
| <10, 000 | Reference | |||
| 10, 001–100, 000 | 1.31(0.59–4.79) | 0.33 | 2.18 (0.79–5.94) | 0.36 |
| >100, 000 | 0.46(0.11–6.70) | 0.13 | 0.93 (0.62–7.21) | 0.12 |
| First line ART | ||||
| NVP containing regimen | Reference | |||
| EFV containing regimen | 2.33 (0.55–3.37) | 0.4 | 1.36 (0.93–3.17) | 0.31 |
| Transmitted drug resistance | ||||
| No | Reference | |||
| Yes | 1.17 (0.29–3.88) | 0.35 | 1.77 (0.43–5.41) | 0.08 |
| Level of adherence | ||||
| Optimal | Reference | |||
| Sub-optimal | 1.48 (0.66–9.49) | 0.15 | 2.83 (0.73–9.03) | 0.6 |
| Absent | 4.78 (2.53–11.17) | 0.01 | 5.11 (2.11–21.00) | 0.02 |
*CD4+ T cells count in cells/mm3;
**HIV RNA level: copies/ml