Rates of switching to second-line antiretroviral therapy and impact of delayed switching on immunologic, virologic, and mortality outcomes among HIV-infected adults with virologic failure in Rakai, Uganda

We conducted a retrospective study of HIV-infected adults initiated on ART between June 2004 and June 2011 in the RHSP clinical cohort, in south-central Uganda. Since 2004, RHSP, with funding from the President’s Emergency Plan for AIDS Relief (PEPFAR), has provided free ART using a community-based decentralized service-delivery model. First-line ART regimens consisted of two nucleoside/nucleotide reverse transcriptase inhibitors (NRTIs; zidovudine or stavudine and lamivudine) and one non-nucleoside reverse transcriptase inhibitor (NNRTI; nevirapine or efavirenz), while second-line consisted of ritonavir-boosted lopinavir with 2 NRTIs. After ART initiation, participants were seen weekly for the first month, then biweekly for 2 months and monthly thereafter, with adherence and HIV risk reduction promotion at all visits, and CD4 and VL monitoring every 6 months. In 2005, RHSP initiated bi-annual routine VL monitoring to identify patients experiencing virologic failure. Interventions to address virologic failure included intensified adherence counseling, peer support, and switching to second-line ART [13]. Decisions about and timing of the switch to second-line ART were made on a case-by-case basis at the clinician’s discretion, and were based on the suspected cause of virologic failure (poor adherence or suspected drug resistance).

We included all HIV-infected adults aged 18 years or older who had been on ART for at least 6 months. Operational definitions of virologic failure changed over time so we defined virologic failure based on the current WHO guidelines [8] as two consecutive VLs > 1000 copies/ml detected within 12 months while on ART. Viral suppression was defined as having a VL < 400 copies/ml.

The primary analysis explored the risk factors of switching to second-line ART among patients confirmed to have VF. The primary outcome was a switch to second-line ART after first occurrence of VF defined as the change from an NNRTI-based regimen to a ritonavir-boosted, lopinavir-based regimen, and the primary exposure was time from VF to switching to second-line ART. The secondary analysis focused on patients that switched to second-line ART during the study to evaluate the risk of immunologic decline, virologic increase or death associated with delay in switching to second line ART. We defined an event of immunologic decline as decrease in CD4 count up 50 cells/ul from the CD4 at the time of virologic failure, and event of virologic increase as an increase of viral load count ≥0.5 log10 copies/ml from the VL at the time of virologic failure. We considered deaths that occurred in patients switched to second-line ART. In this analysis, the exposure of interest was time from VF to immunologic decline or virologic increase or death, compared among patients switched 0–6 months, 7–12 months, 13–24 months, ≥25 months.. Other exposure variables of interest included characteristics at ART initiation; age in years (18–24, 25–34, 35+), gender, type of ART treatment clinic defined as central if care was received at the large, fixed-location referral clinic/laboratory at the RHSP main facility in Kalisizo, or peripheral if care was received at one of 16 HIV treatment clinics conducted by visiting RHSP staff once every two weeks at local government health center facilities, year of ART initiation categorized as 2004–2007 or 2008–2011 to indicate scale-up and stabilized implementation phases of the ART program, WHO stage at ART initiation (I, II, III/IV), CD4 count at ART initiation (<100 or ≥100 cells/ul); characteristics at time of VF: CD4 count (<100 or ≥100 cells/ul), viral load (≤5000, 5001–10,000 or >10,000 copies/ml), year of VF and status of virologic failure prior to VF.

For the primary analysis, person time of observation was computed from the date that the second consecutive (confirmatory) VL of VF was >1000 copies/ml to the time of switching to second-line ART if switched or censored at the last available clinic visit if lost to follow-up or at time of death or administratively censored on April 01, 2014 if not switched, whichever occurred first. Then we used competing risk models to estimate the cumulative incidence and adjusted hazard ratios (aHRs) with 95% confidence intervals (CIs) of switching to the second-line ART regimen following VF, treating death as a competing risk [14]. In the secondary analysis, person time of observation was computed from the date of the second consecutive (confirmatory) VL of VF was >1000 copies/ml to the time of immunologic decline, virologic increase or death for patients that reached the respective end points, or censored at the last available clinic visit if lost to follow-up or at time of death or administratively censored on April 01, 2014 if they didn’t reach the endpoint, whichever came first. We aimed to achieve a hypothetical randomized trial in which patients were enrolled after confirmed VF and randomly assigned to either switch to second-line ART in 0–6, 7–12 months, 13–24 months, 25+ months or delay switching to longer than two years. Given that the VL profile of a patient influences switching to second-line ART (exposure of interest) and also influences the risk of death, future immunologic and virologic outcomes, there is likelihood of confounding by indication. Therefore we used the cox proportional marginal structured models (MSMs) to estimate the association between the exposure and outcomes. VL was considered a time-varying confounder and used to compute inverse probability weights (IPWs) of time to switching and the IPWs of censoring using pooled logistic regression models with robust standard error estimates to account for repeated measures. We adjusted for VL at each visit, duration on first-line ART until VF, year of VF failure, CD4 at ART initiation and VL at time of VF to compute the weights and thereafter stabilized them. Cox proportional hazard MSM adjusted hazard ratios (aHRs) with 95% confidence intervals were estimated separately for the endpoints of immunologic decline and virologic increase, and for a composite endpoint defined as a CD4 decrease of at least 50 cells/ul compared to CD4 at virologic failure, or a virologic increase of at least 0.5 log 10 copies/ml compared to VL at virologic failure or death. Incidence rates of exposure variable were computed using exact poisson regression models and exposure variables with a wald test p-value ≤0.15 in the univariate analysis were included in multivariate analyses. In addition, age and gender were maintained in the multivariate analysis irrespective of their statistical significance to ensure adjustment for any age or gender related confounding. Analysis was performed using STATA 14.0 (STATA, Inc., Texas, USA).

A total of 82 (66.1%) patients with virologic failure were switched to second-line ART at a rate of 49/100 pys (95% CI = 39.1–60.4). The median timing of switching to second-line ART was 8.1 months (IQR = 3.7–17.0) after virologic failure detection. The cumulative incidences of switching at 6, 12, and 24 months after virologic failure were 30.2% (95% CI = 22.8–39.3), 44.6% (95% CI = 36.1–54.1), and 65.0% (95% CI = 55.7–74.2), respectively.

In univariate analyses, significant predictors of more rapid switching to second-line ART were younger age, lower CD4 at ART initiation, and higher VL at the time of virologic failure diagnosis (Table 2). In the adjusted analysis, the adjusted hazard ratio of switching with CD4 < 100 cells/ul at ART initiation relative to patients with ≥100 cells/ul was 2.30, with a 95% CI of 1.5–3.6. Cumulative incidence curves generated from the adjusted competing risk models show a steep increase in the rate of switching in the first 3 years and consistent differences in the rates of switching by the level of CD4 at ART initiation the cumulative incidences of switching at 2 years were ~80% and 40%, respectively (Fig. 1).

The rate of switching was also increased with higher VL at the time of virologic failure; compared to patients with VLs ≤ 5000 copies/ml, patients with VLs of 5001–10,000 copies/ml had an aHR of 1.81 and a 95% CI of 0.9–3.6, and patients with VLs > 10,000 copies/ml had an aHR of 3.38 and a 95% CI of 1.9–6.2. Cumulative incidence curves generated from the adjusted competing risk models show a steep increase in the rate of switching in the first three years and consistent differences in the rates of switching by the level of viral load at virologic failure. Corresponding cumulative incidence at 2 years was 40%, 60%, and 80%, respectively (Fig. 2). No other factors were associated with rates of switching (Table 2).

During the follow-up, 30 patients reached the end point of immunologic decline in 259 person years of observation. The overall incidence rate of developing immunologic decline was 11.6/100 pys (95% CI = 8.1–16.6). Patients switched in 0–6 months had an incidence rate of 5.5/100 pys (95% CI = 2.5–12.3), while the incidence rate was 13.6/100 pys (95% CI = 6.5–28.5) among patients switched in 7–12 months, 16.0/100 pys (95% CI = 8.6–29.7) among patients switched in 13–24 months and 19.4/100 pys (95% CI = 9.2–40.7) among patients switched after 24 months since virologic failure. In the adjusted analysis, compared to patients who were switched within 6 months of confirmed virologic failure, patients who switched within 7–12 months and 13–24 months had a non-significantly different hazard ratio of 2.21 (95% CI = 0.4–13.7) and 2.76(95% CI = 0.6–13.7 respectively, while those switched in 25 months or more, experienced significantly higher hazard rate of developing immunologic decline (aHR = 5.11, 95% CI = 1.0–25.2) [Table 3]. Of the candidate confounding variables, age was significantly associated with immunologic decline. Patients aged 18–24 years at ART initiation, those aged 25–34 years had non-significantly different hazards of immunologic decline, while those 35 years or older had a significantly higher hazard rate of immunologic decline (aHRs = 11.14, 95% CI = 1.5–84.2). Other potential confounders found non-significant included; type of ART treatment clinic, WHO stage at ART initiation, CD4 count at ART initiation, first line ART regimen, viral load at first line ART failure, CD4 at first line ART failure, year of virologic failure and virologic suppression prior to virologic failure (Additional files 1, 2 and 3: Tables S1–S3).

When the end point was virologic increase defined as an increase of 0.5 log 10 copies/ml above VL at time of virologic failure, 24 patients reached the end point in 270.1 person years of observation (incidence = 8.9 cases/100 pys, 95% CI = 6.0–13.3) . Patients switched in 0–6 months had an incidence rate of 3.7/100 pys (95% CI = 1.4–9.9), those switched in 7–12 months had an incidence rate of 1.3/100 pys (95% CI = 0.2–9.4) while those switched in 13–24 months and 25 or more months had incidence of 15.2/100 pys (95% CI = 7.9–29.3) and 36.4(95% CI = 19.6–67.8) respectively. In the adjusted analysis, compared to patients who were switched within 6 months of confirmed virologic failure, patients who switched within 7–12 months had a non-significantly different hazard ratio of 0.32 (95% CI = 0.0–3.6), while those switched in 13–34 and 25 months or more experienced significantly higher hazard rate of developing virologic increase (aHR = 10.16, 95% CI = 1.9–53.0) and aHR = 10.13, 95% CI = 1.7–59.3 respectively) [Table 3]. All potential confounders evaluated had non-significant association with incidence of virologic increase (Additional files 1, 2 and 3: Tables S1–S3).

Lastly, we evaluated the risk of the composite endpoint associated with timing to switch to second-line ART. The Two deaths occurred in patients that switched to second line, the overall incidence rate was 20.2/100 pys (95% CI = 15.0–27.2). Patients switched in 0–6 months had an incidence rate of 10.4/100 pys (95% CI = 5.6–19.3), while the incidence rate was 13.7/100 pys (95% CI = 6.5–28.7) among patients switched in 7–12 months, 36.4/100 pys (95% CI = 21.9–60.3) among patients switched in 13–24 months and 45.8/100 pys (95% CI = 25.3–82.6) among patients switched after 24 months since virologic failure. In the adjusted analysis, compared to patients who were switched within 6 months of confirmed virologic failure, patients who switched within 7–12 months had a non-significantly different hazard ratio of 1.06 (95% CI = 0.3–3.9), while those switched with 13–24 months experienced significantly higher hazard rate of dying or developing immunologic or virologic decline (aHR = 5.05, 95% CI = 1.5–16.9), as did those who switched after 24 months (aHR = 5.58, 95% CI = 1.9–16.7) [Table 3]. All potential confounders evaluated had non-significant association with the composite endpoint (Additional files 1, 2 and 3: Tables S1–S3).