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HIV treatment eligibility expansion and timely antiretroviral treatment initiation following enrollment in HIV care: A metaregression analysis of programmatic data from 22 countries


In a large-scale analysis, Olga Tymejczyk and colleagues study antiretroviral therapy initiation in people with HIV infection accompanying secular changes in treatment eligibility.


Published in the journal: HIV treatment eligibility expansion and timely antiretroviral treatment initiation following enrollment in HIV care: A metaregression analysis of programmatic data from 22 countries. PLoS Med 15(3): e32767. doi:10.1371/journal.pmed.1002534
Category: Research Article
doi: https://doi.org/10.1371/journal.pmed.1002534

Summary

In a large-scale analysis, Olga Tymejczyk and colleagues study antiretroviral therapy initiation in people with HIV infection accompanying secular changes in treatment eligibility.

Introduction

Individual and population-level benefits of antiretroviral treatment (ART) are maximized when treatment is initiated soon after HIV infection occurs [15]. ART slows the progression of HIV to AIDS and reduces infections and mortality among those living with HIV [6,7]. In addition, ART lowers viral load in HIV-infected individuals, thereby reducing the risk of onward HIV transmission [2,711]. Recent studies have shown that immediate versus delayed initiation of ART reduces risks of AIDS and severe opportunistic illnesses [12]. Some studies suggest that earlier initiation of ART may also improve rates of retention in care and medication adherence, and promote more rapid achievement of viral load suppression [1315]. As a result of this evidence, the World Health Organization (WHO) now recommends immediate initiation of ART for all people diagnosed with HIV, regardless of CD4 count [16].

A systematic review of retention in HIV care between testing and treatment among patients who were ineligible to initiate ART at the time of diagnosis estimated that less than one-third of patients remained continuously engaged in HIV care until the point of ART eligibility [17]. Other reviews of losses along the HIV care continuum in sub-Saharan Africa have estimated that 54%–69% of those ineligible for ART at the time of HIV care enrollment are lost to care prior to ART initiation, with the poorest retention rates among adolescents, young adults, and those enrolling in care at earlier stages of infection [18,19]. In contrast, among patients eligible for ART at the time of enrollment into care, the proportions lost to care prior to ART initiation were 25%–36% [18,19]. In a recent analysis from South Africa, which compared outcomes among patients just below and just above the ART eligibility cutoff, patient eligibility for immediate treatment was associated with a 25 percentage point (pp) increase in ART initiation and an 18 pp increase in 12-month retention [20].

Using longitudinal data on patients enrolling in HIV care from the International Epidemiology Databases to Evaluate AIDS (IeDEA) network, we sought to assess changes in timely ART initiation at the original site of care enrollment following major expansions in HIV treatment guidelines across multiple countries and regions and to identify factors associated with these changes.

Methods

Data sources and management

Patient data

IeDEA (www.iedea.org) contains sociodemographic and clinical data for over 1.7 million patients enrolled in HIV care in 46 countries across 7 regional cohort collaborations [21]. The vast majority (87%) of IeDEA sites are public sector health facilities, including both primary-level sites (42%) and secondary/tertiary-level sites (58%) [22], thus representing a diverse population of HIV patients. Almost all IeDEA sites offer HIV counseling and testing on-site, and common entry points into HIV care at these sites are internal referrals from other units (i.e., HIV counseling and testing), antenatal care, outpatient departments, and referrals from other health facilities, as well as community-based testing programs in their catchment areas [22,23]. In this analysis, we used prospectively and retrospectively collected data from 2006–2017 for 6 regional cohorts with pre-ART data available (Asia-Pacific, Central and South America, Central Africa, East Africa, North America, and Southern Africa). Prior to data merge and analysis, each region’s data were harmonized by regional data managers in accordance with IeDEA data exchange standards regarding variable definitions, data cleaning, and formatting.

ART guidelines

We conducted a systematic search for current and historical ART eligibility guidelines of countries participating in IeDEA, including sources such as the Joint United Nations Programme on HIV/AIDS (UNAIDS) Database of National HIV Guidelines [24], the International Association of Providers of AIDS Care (IAPAC) Global HIV Watch [25], the HIV Treatment Guideline Database, health ministry websites, search engines, and published literature, including ART guideline reviews [2628]. For countries with no publicly available ART guidelines, we obtained information from in-country HIV clinicians, researchers, and ministry of health officials. We identified the time points when each country expanded ART eligibility to include asymptomatic people living with HIV (PLWH) with CD4 counts ≤350 cells/μL and ≤500 cells/μL. We also identified concurrent expansions of guidelines related to expanded treatment for pregnant women and patients coinfected with tuberculosis, regardless of other eligibility criteria (i.e., CD4 counts or clinical staging). If the exact month of ART eligibility expansion was unknown, a midyear value was used.

This cohort study utilized deidentified data approved for use by local ethical committees in each of the IeDEA regions included in the analysis.

Eligibility criteria

Sites eligible for inclusion had to have HIV care data available on patients for the period after care enrollment but preceding ART initiation (pre-ART data), as well as data on both ART initiators and noninitiators. Patients had to be at least 16 years old at enrollment (18 in North America) and have at least 12 months of possible follow-up between enrollment and database closure. Patients were excluded if they transferred to an IeDEA site from another clinic, lacked a clinic visit and lab record, or were known not to be ART naïve at enrollment (with ART defined as any regimen of at least 3 antiretroviral drugs, excluding treatment taken for prevention of maternal-to-child transmission).

To ensure that there was no differential selection into the sample by ART eligibility, distributions of CD4 counts at enrollment were assessed with respect to possible discontinuities at the point of ART eligibility (CD4 = 350 and CD4 = 500 for the 2 analyses), which would indicate potential exclusion of non-ART-eligible patients from contributing sites’ cohorts (S1 Text).

Outcome

The outcome of interest was site-level absolute pp change in cumulative incidence of ART initiation (CI-ART) within 6 months of enrollment at each site—namely, the difference in CI-ART between those enrolling in HIV care 6–18 months prior to national ART eligibility expansion (“pre” or baseline period) and those enrolling 6–18 months thereafter (“post” period). Pp changes were computed separately for ART eligibility expansions to CD4 counts ≤350 cells/μL and ≤500 cells/μL. Patients enrolling in the 6 months immediately preceding and following guideline introduction were excluded to allow for early or lagged implementation of national guidelines at the site level and to ensure that the 6-month CI-ART outcome for the “pre” period occurred before the guideline change. Additionally, to ensure sufficient data for reliable outcome estimation, sites that had fewer than 30 study eligible patients who enrolled in either of the “pre” and “post” periods bracketing ART eligibility expansion were excluded.

To derive the outcome measure, we estimated overall 6-month CI-ART separately for the “pre” and “post” ART eligibility expansion periods via competing risks regression with the Aalen-Johansen estimator, treating death and pre-ART loss to clinic as competing events. To minimize the risk of misclassifying temporarily disengaged patients as lost, pre-ART loss to clinic was defined as not returning to clinic for at least 12 months, with no evidence of subsequent return.

Statistical and analytic methods

The CI-ART was estimated via competing risk methods, with the Aalen-Johansen estimator, and treating death and loss to clinic as competing risks, as outlined in a July 2016 concept proposal to the IeDEA Executive Committee (S2 Text), which also prespecified inclusion and exclusion criteria, outcome definitions, and key stratification variables. As discussed in the appendix (S2 Text), other analytic approaches, including the use of site-level metaregression and the pre-post within-site comparisons to derive the outcome, were selected after data became available.

To assess variability of change in 6-month CI-ART across sites, forest plots were used to visualize site-level outcomes, and between-site variances (tau-squared) and p-values from chi-squared tests of between-site heterogeneity were calculated.

Pooled estimates and stratification

We calculated pooled summary estimates of the pp change in 6-month CI-ART across all sites for each major expansion in treatment eligibility criteria, along with corresponding 95% confidence intervals (CIs). We stratified all estimates across several site and patient characteristics. Site characteristics included IeDEA region (see “Data Sources”), site setting (urban versus rural), and site-level summary measures of the patient population enrolling at the site, including overall proportion of female clients (≤45%, 45%–65%, >65%); baseline 6-month CI-ART (grouped in quartiles) among all patients and among those previously eligible for treatment as a site-level measure of the preexisting service level and capacity to expand; and proportion of patients eligible for treatment in the “post” period, under expanded guidelines, as a measure of unmet need for treatment. Patient characteristics included sex, age at enrollment (dichotomized into 16–24 years and ≥25 years, to align with the 15–24 age category that is commonly used by WHO [29]), and CD4 count at enrollment. CD4 count at enrollment was categorized to reflect patients’ ART eligibility status vis-à-vis each guideline change: newly eligible (CD4 count 201–350) and previously eligible (CD4 ≤ 200) for the ART eligibility expansion to CD4 ≤ 350 cells/μL and newly eligible (CD4 351–500) and previously eligible (CD4 ≤ 350), in analyses of ART eligibility expansion to CD4 ≤ 500 cells/μL.

Metaregression models

Linear random effects metaregression models were used to examine factors associated with changes in 6-month CI-ART while controlling for concurrent expansions of other ART eligibility criteria and to assess the predicted magnitude of change in 6-month CI-ART following ART eligibility expansions. Bivariate and multivariable associations between the pp change in 6-month CI-ART and site and patient population characteristics were examined through linear random effects metaregression, adjusted for concurrent expansions of ART eligibility criteria for pregnant women and tuberculosis patients. To meet the assumption of linearity in the association between continuous independent variables and the outcome, cohort size was log transformed.

Covariates used in metaregression models included variables related to site characteristics (i.e., baseline 6-month CI-ART, baseline median enrollment CD4, median age at enrollment, and proportion of female patients at a site), as well as binary variables related to concurrent guideline changes extending HIV treatment to all pregnant women and tuberculosis patients. Site-level covariates were derived separately for each of the 2 ART eligibility expansions (to CD4 ≤ 350 cells/μL and to CD4 ≤ 500 cells/μL), based on each site’s patient population in the periods bracketing each ART eligibility expansion.

Analyses were completed in Stata 14.

Results

Overall, 260 IeDEA sites had provided longitudinal data on at least 60 patients—the minimum for potential inclusion in the analysis. Thirty sites were further excluded because of lack of data on pre-ART patients. Among the remaining 230 sites, 225 were in countries where eligibility expansions of interest occurred during the period under study. Among these sites, 171 had sufficiently large cohorts for inclusion in this analysis (i.e., at least 30 patients meeting the eligibility criteria described above in each 12-month period bracketing guideline expansion).

ART eligibility expansions and site characteristics

The analysis of ART eligibility expansion to treat asymptomatic PLWH with CD4 count ≤350 cells/μL included 145 sites (with 169,717 patients) in 22 countries where guidelines changed between 2007 and 2012. Six of these countries revised national treatment eligibility guidelines before WHO’s November 2009 recommendation [30] to initiate treatment at CD4 ≤ 350, by a mean of 15 months (range 5–27 months). Among the 16 countries that adopted expanded guidelines after WHO’s recommendation, the mean time elapsed was 20 months (range 6–31 months).

The analysis of ART eligibility expansion for asymptomatic PLWH with CD4 count ≤500 cells/μL included 152 sites (with 128,552 patients) in 15 countries where guidelines changed between 2009 and 2015. Three of these countries introduced new guidelines prior to WHO’s June 2013 recommendation [31] on treatment eligibility (mean of 28 months; range 11–42 months). Among the remaining 12 countries, national guideline change followed WHO recommendations by a mean of 9 months (range 1–24 months).

For both analyses, half of the sites were from Southern Africa (50% and 51%, respectively; Table 1).

Tab. 1. Characteristics of 171 sites and 284,740 patients included in the analyses.
Characteristics of 171 sites and 284,740 patients included in the analyses.
Abbreviations: ART, antiretroviral treatment; DRC, Democratic Republic of the Congo.

During the periods preceding ART eligibility expansions to CD4 ≤ 350 and CD4 ≤ 500, the median proportion of patients initiating ART within 6 months of enrollment was 53.3% and 57.5% of patients, respectively (Table 2).

Tab. 2. Overall and pooled change in 6-month cumulative incidence of antiretroviral treatment initiation (CI-ART) after ART eligibility guideline expansion to CD4 ≤ 350 and CD4 ≤ 500.
Overall and pooled change in 6-month cumulative incidence of antiretroviral treatment initiation (CI-ART) after ART eligibility guideline expansion to CD4 ≤ 350 and CD4 ≤ 500.
a Includes only sites with ≥30 patients in each “pre” and “post” period in the given stratum

Patient demographics were similar across sites, with a median age of 34 years and female patients comprising more than 60% of patients on average. Baseline median CD4 counts at enrollment into HIV care were higher among sites included in the analysis of CD4≤500 ART eligibility expansion than among the CD4≤350 ART eligibility expansion sites (273 cells/μL versus 223 cells/μL). However, a larger proportion of patients were missing data for CD4 count at enrollment during both the “pre” and “post” periods in the analysis of the second ART eligibility expansion (median 33% versus 14% and 39% versus 20%, respectively; Table 1).

Pooled estimates of change in 6-month CI-ART following ART eligibility expansions

Marked changes in CI-ART were observed after each expansion in treatment eligibility: 4.3 pp (95% CI 2.6–6.1 pp) after the expansion to CD4 ≤ 350 cells/μL and 15.9 pp (95% CI 14.3–17.4 pp) after the expansion to CD4 ≤ 500 cells/μL (Table 2). There was considerable heterogeneity in site-level changes in CI-ART for both guideline expansions, and heterogeneity chi-squared tests were statistically significant (both p <0.001). However, a much larger proportion of sites experienced positive changes in 6-month CI-ART following the latter ART eligibility expansion to CD4 ≤ 500 cells/μL (Fig 1A and 1B). Overall, 33% of sites (48/145) had statistically significant increases in 6-month CI-ART after the expansion to CD4 ≤ 350 cells/μL, 57% of sites (83/145) had no statistically discernible change, and 10% (14/145) had statistically significant decreases. After expansion to CD4 ≤ 500 cells/μL, 74% of sites (112/152) had statistically significant increases, 26% of sites (39/152) had no statistically discernible change, and <1% (1/152) had a statistically significant decrease.

Fig. 1. Site-level changes in 6-month cumulative incidence of antiretroviral treatment initiation (CI-ART) after guideline expansions to (A) CD4 ≤ 350 and (B) CD4 ≤ 500.
Site-level changes in 6-month cumulative incidence of antiretroviral treatment initiation (CI-ART) after guideline expansions to (A) CD4 ≤ 350 and (B) CD4 ≤ 500.
Pooled estimates and confidence intervals are in gray.

In stratified analyses of the guideline expansion to treat patients with CD4 ≤ 350 cells/μL, changes in 6-month CI-ART were most pronounced at sites in Asia-Pacific, East Africa, and Central Africa (12.0, 7.6 and 7.3 pp, respectively), at sites with higher proportions of newly eligible patients in the “post” period (4.9 pp and 7.9 pp for clinics in the top 2 quartiles of the proportion of patients newly eligible for treatment, respectively), and sites in the lowest quartile of “pre” period 6-month CI-ART (11.8 pp). There was also a trend in the association between lower “pre” period 6-month CI-ART among previously eligible patients specifically and greater site-level change in CI-ART after guideline expansion (Table 2).

Following the CD4 ≤ 500 expansion, the largest changes in CI-ART were observed in Southern and East Africa (17.6 pp and 15.8 pp, respectively). As observed in the CD4 ≤ 350 analysis, there was a trend of greater change in 6-month CI-ART with lower “pre” period 6-month CI-ART (overall and among previously eligible patients specifically); sites in the lowest quartile of “pre” period 6-month CI-ART had the largest changes in CI-ART following ART eligibility expansion (26.2 pp). However, in contrast to trends observed following expansion to CD4 ≤ 350, there was no trend in CI-ART across quartiles of proportion of newly eligible patients in the “post” period (Table 2).

In analyses stratified by patient characteristics, no significant differences in the pp change in CI-ART were observed by sex or age after expansion to CD4 ≤ 350 cells/μL. However, after expansion to CD4 ≤ 500 cells/μL, appreciably larger increases were observed among women when compared to men (16.8 versus 13.7 pp) and among patients aged 16–24 years at enrollment, compared to those 25 years or older (21.5 versus 15.5 pp). Striking differences were also observed in pooled estimates of change in CI-ART by CD4 count at enrollment. Specifically, while no or minimal improvement was observed among patients who were already ART eligible before guideline expansion, a large increase was noted among those newly eligible for treatment under the expanded ART criteria (18.2 pp among newly eligible patients after expansion to CD4 ≤ 350 cells/μL and 47.4 pp among newly eligible patients after expansion to CD4 ≤ 500 cells/μL; Table 2, Fig 2).

Fig. 2. Distribution of site-level changes in 6-month cumulative incidence of antiretroviral treatment initiation (CI-ART) after expansions to CD4 ≤ 350 and CD4 ≤ 500, by patient ART eligibility status at enrollment.
Distribution of site-level changes in 6-month cumulative incidence of antiretroviral treatment initiation (CI-ART) after expansions to CD4 ≤ 350 and CD4 ≤ 500, by patient ART eligibility status at enrollment.
a Defined as those enrolling at CD4 ≤ 200 (in the expansion to CD4 ≤ 350 analysis) and those enrolling at CD4 between 201 and 350 (in the expansion to CD4 ≤ 500 analysis). b Defined as those enrolling at CD4 ≤ 350 (in the expansion to CD4 ≤ 350 analysis) and those enrolling at CD4 between 351 and 500 (in the expansion to CD4 ≤ 500 analysis).

Metaregression: Predicted and adjusted effects

Six-month CI-ART during the period before ART eligibility expansion was the strongest correlate of change in CI-ART following eligibility expansion. In bivariate analyses, the predicted change in 6-month CI-ART after expansion to CD4 ≤ 350 was 9.1 pp for a site with “pre”-period CI-ART of 40% and 1.4 pp for a site with “pre”-period CI-ART of 60%. After expansion to CD4 ≤ 500, the predicted changes in CI-ART were 24.1 pp and 14.6 pp, respectively. In adjusted metaregression models, “pre”-period 6-month CI-ART was the strongest correlate of pp change in 6-month CI-ART after ART eligibility expansion (Table 3). Adjusted changes in CI-ART following both ART eligibility expansions were greatest among those sites with lower pre-expansion levels of CI-ART; each 10-unit decrease in the “pre”-period 6-month CI-ART was associated with an average 3.9 and 5.3 pp change in CI-ART after CD4 ≤ 350 and CD4 ≤ 500 cells/μL eligibility expansions, respectively. Increasing cohort size was also positively associated with change in CI-ART (Table 3).

Tab. 3. Crude and adjusted metaregression analyses of change in 6-month cumulative incidence of antiretroviral treatment initiation (CI-ART) after ART eligibility guideline expansion to CD4 ≤ 350 and CD4 ≤ 500.
Crude and adjusted metaregression analyses of change in 6-month cumulative incidence of antiretroviral treatment initiation (CI-ART) after ART eligibility guideline expansion to CD4 ≤ 350 and CD4 ≤ 500.
a The model was also adjusted for ART eligibility concurrently expanded to encompass all individuals with tuberculosis or pregnancy.

Metaregression models adjusting for site, patient population, and guideline characteristics explained 24.1% and 38.1% of between-site variability, with tau-squared reduced from 126.1 to 95.7 and from 110.4 to 68.3 in the CD4 ≤ 350 and CD4 ≤ 500 analyses, respectively.

Discussion

Our study found that expansions in ART eligibility criteria for people with HIV infection were followed by substantial increases in rates of timely ART initiation at the original clinic of enrollment, with much larger increases among those newly eligible under the expanded guidelines compared with those eligible under prior guidelines. Importantly, with expansion to CD4 ≤ 500, increases were most pronounced for persons aged 16–24 years, a critical population that has historically been particularly difficult to engage in care. For both ART eligibility expansions examined (i.e., to CD4 ≤ 350 and CD4 ≤ 500), changes in 6-month CI-ART were greatest at sites that had lower rates of ART initiation prior to ART eligibility expansion and, in metaregression analyses, “pre”-period rates of ART initiation were significantly and inversely associated with changes in CI-ART following guideline change. Larger increases in CI-ART overall were observed following the adoption of CD4 count ≤500 cells/μL treatment eligibility guidelines, with statistically significant increases in CI-ART observed at 74% of sites and a dramatic shift in the pooled estimate of CI-ART across all sites included in the analysis.

Concern has been expressed that expanding ART eligibility may result in sick patients being “crowded out” by asymptomatic patients [32]. Importantly, and consistent with research from South Africa [33,34], increases in ART initiation among newly eligible patients on average were not offset by decreases in ART initiation rates among previously eligible patients, meaning that access to treatment by sicker patients with lower CD4 counts did not decrease when patients with higher CD4 counts became eligible and started treatment. In fact, sites with the lowest baseline ART initiation rates among previously eligible patients saw the greatest overall increases in ART initiation after guideline expansion, which also suggests that broadened treatment eligibility did not compromise access for sicker patients.

Another major finding of our study is that increases in timely ART initiation were largest among young adults—a group that has been consistently shown to have lower rates of retention in care both prior to and after ART initiation, as well as lower rates of ART initiation at early stages of infection [3538]. Improving timely ART initiation among young adults is particularly important, given that this age group accounts for almost half of new HIV infections among adults [39].

To our knowledge, no analyses to date have assessed differences in ART initiation following major changes in HIV treatment eligibility criteria across multiple countries and regions. While the results of this analysis are promising, further research is needed to assess how increases in ART initiation at higher CD4 counts and among asymptomatic patients affect retention in the HIV care continuum over the longer term, including ART adherence, and sustained HIV virologic suppression. While some studies have suggested increased loss to follow-up on ART among patients with higher CD4 counts [40,41], evidence increasingly supports improved retention among patients initiating with higher CD4 counts [15], including those immediately eligible for ART versus those just under the eligibility threshold [20], and same-day (or “rapid”) ART initiators [42], with any increases in loss to follow-up more than offset by eliminating opportunity for pre-ART attrition [43].

The results of this study are important, given a recent systematic review of national HIV treatment cascades, which indicated that the most common “break point” in the HIV care cascade is between diagnosis and initiation of ART [10], which is critical for achieving optimal HIV care outcomes at the individual and population level [44]. In conjunction with efforts to improve HIV testing and linkage to care [45,46], in part via point-of-care CD4 testing to assess patients’ ART eligibility [47], accelerating the adoption of expanded treatment eligibility criteria, including WHO’s current “Treat All” recommendation, could help reduce rates of pre-ART loss to clinic and increase rates of timely ART initiation. Mathematical models suggest that improving rates of HIV testing, linkage, and immediate ART initiation, combined with other prevention interventions, could nearly stop HIV transmission [48].

At the country level, however, treatment guidelines often lag behind WHO guidance, creating missed opportunities to realize the preventive potential of ART [26,27]. A recent analysis of HIV treatment policy changes in sub-Saharan Africa found that the average time for the adoption of the 2013 guidelines was 10 months (range 0 to 36 months) [26]. Compounding delays in the national adoption of global guidance are lags in the practical implementation of new treatment policies at the service delivery level, where outdated practices among frontline health workers, treatment readiness requirements, and resource constraints lead to further delays in ART initiation among eligible HIV patients [49]. Confirming the importance of service delivery factors in promoting more timely ART initiation, a large intervention study in Uganda recently demonstrated a substantial increase in the proportion of eligible patients initiating ART within 14 days of eligibility determination from 38% to 80% (a 42 pp increase) through relatively simple and low-cost changes at the health facility level [50]. Our study results highlight the importance of promoting ART eligibility expansions, including universal test-and-treat guideline scenarios, with complementary strategies at the facility level to maximize timely diagnosis and ART initiation rates among ART-eligible persons.

Major strengths of this study include the analysis of data from a large number of patients and sites across several world regions. Patient- and site-level characteristics were used to provide setting-specific estimates and to adjust for some differences in patient mix across sites. Where known, concurrent expansions of ART eligibility criteria regarding pregnancy and tuberculosis status were also controlled for, to account for varied scopes and foci of guideline changes. Findings from this large and heterogeneous sample of real-world service delivery settings may be generalizable to many contexts, especially where substantial room remains to expand ART eligibility guidelines. Additionally, the use of a 12-month buffer period around the national guideline change date helped both to reduce exposure misclassification and to control for differences in patient mix and seasonal patterns of ART initiation in within-site pre-post comparisons.

However, even with the use of a buffer period, the lack of data on the exact timing of site-level implementation of expanded ART eligibility guidelines likely contributed to imprecision of the site-level CI-ART estimates, as implementation of expanded guidelines may have preceded national adoption at some sites and lagged at other sites. Furthermore, the inclusion of 171 sites from 22 countries necessarily means considerable heterogeneity of ART referral and record-keeping practices, which may have also affected the precision of the estimates. With half of all sites and over 60% of patients in this analysis being from Southern Africa, overall estimates are strongly influenced by this region. However, changes in CI-ART were similar across regions, especially in the expansion to CD4≤500 analysis, albeit with some regions having lower volumes of data (Asia-Pacific and South and Central America) and therefore less precise CI-ART estimates.

While many sites experienced increases in timely ART initiation, particularly after treatment eligibility was expanded to CD4 ≤ 500 cells/μL, no change in CI-ART and occasional decreases in CI-ART were also observed, possibly as a result of unmeasured site-level factors (e.g., medication or reagent shortages, staffing changes, and other resource constraints). We did not have data on many facility- and patient population-related factors that could help illuminate the reasons behind observed decreases in ART initiation at selected sites after country-level guideline expansion. In addition, random fluctuation or regression to the mean may help explain some decreases and increases (for example, changes observed among sites with lowest “pre”-period ART initiation rates).

Nuanced expansions in national ART eligibility criteria related to clinical stage and pregnancy and tuberculosis status, as well as special populations, such as sex workers and serodiscordant couples, could not be reflected in this analysis. Furthermore, assumptions of a midyear policy change for countries where the exact month of ART eligibility expansion was unknown, in combination with possible early or delayed site-level implementation of national guidelines, may have obscured the effects of guideline change at the site level.

The increases in CI-ART that we observed may also overestimate the true impact of ART eligibility expansions, given our inability to directly account for secular trends in CI-ART and lack of a counterfactual within countries during the periods bracketing ART eligibility expansions. However, the change in timely ART initiation among those previously eligible after the guideline expansion is likely a good proxy for what would have happened to those newly eligible under the guideline expansion had the guideline not changed. The larger increase in timely ART initiation among those newly eligible (18.2 pp for CD4 ≤ 350 and 47.4 pp for CD4 ≤ 500) versus those previously eligible (no change for CD4 ≤ 350 and a small increase of 4.9 pp for CD4 ≤ 500) is more consistent with a guideline effect than a secular trend.

While our study design precludes causal attribution, recent research in South Africa, including studies that used regression discontinuity analysis to account for secular trends prior to and following eligibility expansions [33,45], as well as to examine ART initiation rates just above and just under eligibility threshold [20], lend support for a causal association between ART eligibility expansions and increases in ART initiation.

Conclusions

Our study of a global sample of HIV clinics indicates that ART eligibility expansion was followed by substantial increases in timely ART initiation at the original site of enrollment, including among young adults aged 16–24 years, as well as at clinics with lower rates of timely ART initiation prior to treatment eligibility expansions. That many clinics can support the initiation of ART among newly eligible patients with less advanced disease without an adverse impact on ART initiation rates among those with more advanced disease may reflect a transition away from the emergency treatment era in some locations. While we did not have sufficient data available to assess the changes in CI-ART following the implementation of the currently recommended Treat All approach, these findings underscore the utility of ART eligibility expansion as an essential strategy in support of the UNAIDS 90-90-90 targets globally. As countries increasingly adopt WHO’s Treat All recommendation, future research should explore its impact on timely ART initiation, as well as other longer-term HIV care outcomes, including retention, ART adherence, and sustained virologic suppression.

Disclaimer

The content of this publication is solely the responsibility of the authors and does not necessarily represent the official views of any of the governments or institutions mentioned above.

Supporting Information

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Zdroje

1. Eholie SP, Vella S, Anglaret X. Commentary: Antiretroviral therapy initiation criteria in low resource settings—from ‘when to start’ to ‘when not to start’. AIDS. 2014;28 Suppl 2:S101–4. doi: 10.1097/QAD.0000000000000237 24849468

2. Bock NN, Emerson RC, Reed JB, Nkambule R, Donnell DJ, Bicego GT, et al. Changing Antiretroviral Eligibility Criteria: Impact on the Number and Proportion of Adults Requiring Treatment in Swaziland. J Acquir Immune Defic Syndr. 2016;71(3):338–44. doi: 10.1097/QAI.0000000000000846 26361174

3. Siegfried N, Uthman OA, Rutherford GW. Optimal time for initiation of antiretroviral therapy in asymptomatic, HIV-infected, treatment-naive adults. Cochrane Database Syst Rev. 2010;(3):Cd008272. doi: 10.1002/14651858.CD008272.pub2 20238364

4. The TEMPRANO ANRS Study Group. A Trial of Early Antiretrovirals and Isoniazid Preventive Therapy in Africa. N Engl J Med. 2015;373(9):808–22. doi: 10.1056/NEJMoa1507198 26193126.

5. Lundgren JD, Babiker AG, Gordin F, Emery S, Grund B, Sharma S, et al. Initiation of Antiretroviral Therapy in Early Asymptomatic HIV Infection. N Engl J Med. 2015;373(9):795–807. doi: 10.1056/NEJMoa1506816 26192873

6. Ray M, Logan R, Sterne JA, Hernandez-Diaz S, Robins JM, Sabin C, et al. The effect of combined antiretroviral therapy on the overall mortality of HIV-infected individuals. AIDS. 2010;24(1):123–37. doi: 10.1097/QAD.0b013e3283324283 19770621

7. Montaner JS, Hogg R, Wood E, Kerr T, Tyndall M, Levy AR, et al. The case for expanding access to highly active antiretroviral therapy to curb the growth of the HIV epidemic. Lancet. 2006;368(9534):531–6. doi: 10.1016/S0140-6736(06)69162-9 16890841

8. Loutfy MR, Wu W, Letchumanan M, Bondy L, Antoniou T, Margolese S, et al. Systematic review of HIV transmission between heterosexual serodiscordant couples where the HIV-positive partner is fully suppressed on antiretroviral therapy. PLoS ONE. 2013;8(2):e55747. doi: 10.1371/journal.pone.0055747 23418455. Erratum in: PLoS ONE. 2013;8(12)

9. Attia S, Egger M, Muller M, Zwahlen M, Low N. Sexual transmission of HIV according to viral load and antiretroviral therapy: systematic review and meta-analysis. AIDS. 2009;23(11):1397–404. doi: 10.1097/QAD.0b013e32832b7dca 19381076

10. Levi J, Raymond A, Pozniak A, Vernazza P, Kohler P, Hill A. Can the UNAIDS 90-90-90 target be achieved? A systematic analysis of national HIV treatment cascades. BMJ Glob Health. 2016; Sep 15;1(2):e000010. doi: 10.1136/bmjgh-2015-000010 28588933

11. Cohen MS, Chen YQ, McCauley M, Gamble T, Hosseinipour MC, Kumarasamy N. Prevention of HIV-1 infection with early antiretroviral therapy. N Engl J Med. 2011;365. doi: 10.1056/NEJMoa1105243 21767103

12. Eholié SP, Badje A, Kouame GM, N’takpe J-B, Moh R, Danel C, et al. Antiretroviral treatment regardless of CD4 count: the universal answer to a contextual question. AIDS Res Ther. 2016;13(1):27. doi: 10.1186/s12981-016-0111-1 27462361

13. Jain V, Byonanebye DM, Amanyire G, Kwarisiima D, Black D, Kabami J, et al. Successful Antiretroviral Therapy Delivery and Retention in Care Among Asymptomatic Individuals with High CD4+ T Cell Counts ≥350 cells/uL in Rural Uganda. AIDS. 2014;28(15):2241–9. doi: 10.1097/QAD.0000000000000401 25022596

14. Hall HI, Tang T, Westfall AO, Mugavero MJ. HIV care visits and time to viral suppression, 19 U.S. jurisdictions, and implications for treatment, prevention and the national HIV/AIDS strategy. PLoS ONE. 2013;8(12):e84318. doi: 10.1371/journal.pone.0084318 24391937

15. Clouse K, Pettifor A, Maskew M, Bassett J, Van Rie A, Gay C, et al. Initiating antiretroviral therapy when presenting with higher CD4 cell counts results in reduced loss to follow-up in a resource-limited setting. AIDS. 2013;27(4):645–50. doi: 10.1097/QAD.0b013e32835c12f9 23169326

16. World Health Organization. Guideline on when to start antiretroviral therapy and on pre-exposure prophylaxis for HIV. Geneva: World Health Organization; 2015.

17. Rosen S, Fox MP. Retention in HIV care between testing and treatment in sub-Saharan Africa: a systematic review. PLoS Med. 2011;8(7):e1001056. doi: 10.1371/journal.pmed.1001056 21811403

18. Mugglin C, Estill J, Wandeler G, Bender N, Egger M, Gsponer T, et al. Loss to programme between HIV diagnosis and initiation of antiretroviral therapy in sub-Saharan Africa: systematic review and meta-analysis. Trop Med Int Health. 2012;17(12):1509–20. doi: 10.1111/j.1365-3156.2012.03089.x 22994151

19. Kranzer K, Govindasamy D, Ford N, Johnston V, Lawn SD. Quantifying and addressing losses along the continuum of care for people living with HIV infection in sub-Saharan Africa: a systematic review. J Int AIDS Soc. 2012;15(2):17383. doi: 10.7448/IAS.15.2.17383 23199799

20. Bor J, Fox MP, Rosen S, Venkataramani A, Tanser F, Pillay D, et al. Treatment eligibility and retention in clinical HIV care: A regression discontinuity study in South Africa. PLoS Med. 2017;14(11):e1002463. doi: 10.1371/journal.pmed.1002463 29182641

21. IeDEA. The International Epidemiology Databases to Evaluate AIDS (IeDEA) [cited 2016 Dec 2]. Available from: http://iedea.org/.

22. Fritz CQ, Blevins M, Lindegren ML, Wools-Kaloutsian K, Musick BS, Cornell M, et al. Comprehensiveness of HIV care provided at global HIV treatment sites in the IeDEA consortium: 2009 and 2014. J Int AIDS Soc. 2017;20(1):20933. doi: 10.7448/IAS.20.1.20933 28364561

23. Duda SN, Farr AM, Lindegren ML, Blevins M, Wester CW, Wools-Kaloustian K, et al. Characteristics and comprehensiveness of adult HIV care and treatment programmes in Asia-Pacific, sub-Saharan Africa and the Americas: results of a site assessment conducted by the International epidemiologic Databases to Evaluate AIDS (IeDEA) Collaboration. J Int AIDS Soc. 2014;17(1):19045. doi: 10.7448/IAS.17.1.19045 25516092

24. Joint United Nations Programme on HIV/AIDS. UNAIDS Database of National HIV Guidelines [cited 2016 Dec 2]. Available from: http://www.who.int/hiv/pub/national_guidelines/en

25. IAPAC. Global HIV Policy Watch: International Association of Providers of AIDS Care; [cited 2016 Dec 2]. Available from: http://www.hivpolicywatch.org/.

26. Gupta S, Granich R. When will sub-Saharan Africa adopt HIV treatment for all? South Afr J HIV Med. 2016;17(1):1–6.

27. Gupta S, Williams B, Montaner J. Realizing the potential of treatment as prevention: global ART policy and treatment coverage. Curr HIV/AIDS Rep. 2014;11(4):479–86. doi: 10.1007/s11904-014-0230-z 25266850

28. Ying R, Granich RM, Gupta S, Williams BG. CD4 Cell Count: Declining Value for Antiretroviral Therapy Eligibility. Clin Infect Dis. 2016;62(8):1022–8. doi: 10.1093/cid/civ1224 26826372

29. Joint United Nations Programme on HIV/AIDS. Global AIDS Update 2016. Geneva: Joint United Nations Programme on HIV/AIDS; 2016

30. World Health Organization. Rapid advice: antiretroviral therapy for HIV infection in adults and adolescents. Geneva: World Health Organization: 2009.

31. World Health Organization. Consolidated Guidelines on the use of Antiretroviral Drugs for Treating and Preventing HIV Infection: Recommendations for a Public Health Approach. Geneva: World Health Organization; 2013.

32. Ford N, Calmy A, Hurst S. When to start antiretroviral therapy in resource-limited settings: a human rights analysis. BMC Int Health Hum Rights. 2010 Mar 31;10:6. doi: 10.1186/1472-698X-10-6 20356356

33. Kluberg SA, Fox MP, LaValley M, Barnighausen T, Pillay D, Bor J. Do ART Eligibility Expansions Crowd Out the Sickest? Evidence From South Africa. Conference on Retroviruses and Opportunistic Infections; 2016 Feb 22–25; Boston, MA, USA.

34. Plazy M, Dabis F, Naidu K, Orne-Gliemann J, Barnighausen T, Dray-Spira R. Change of treatment guidelines and evolution of ART initiation in rural South Africa: data of a large HIV care and treatment programme. BMC Infect Dis. 2015;15:452. doi: 10.1186/s12879-015-1207-2 26497054

35. Lahuerta M, Ue F, Hoffman S, Elul B, Kulkarni SG, Wu Y, et al. The Problem of Late ART initiation in Sub-Saharan Africa: A Transient Aspect of Scale-up or a Long-term Phenomenon? J Health Care Poor Underserved. 2013;24(1):359–83. doi: 10.1353/hpu.2013.0014 23377739

36. Lessells RJ, Mutevedzi PC, Cooke GS, Newell M-L. Retention in HIV care for individuals not yet eligible for antiretroviral therapy: rural KwaZulu-Natal, South Africa. J Acquir Immune Defic Syndr. 2011;56(3):e79–e86. doi: 10.1097/QAI.0b013e3182075ae2 21157360

37. Kranzer K, Bradley J, Musaazi J, Nyathi M, Gunguwo H, Ndebele W, et al. Loss to follow-up among children and adolescents growing up with HIV infection: age really matters. J Int AIDS Soc. 2017;20(1):21737. doi: 10.7448/IAS.20.1.21737 28715158

38. Wong VJ, Murray KR, Phelps BR, Vermund SH, McCarraher DR. Adolescents, young people, and the 90-90-90 goals: a call to improve HIV testing and linkage to treatment. AIDS. 2017;31 Suppl 3:S191–s4. doi: 10.1097/QAD.0000000000001539 28665876

39. Joint United Nations Programme on HIV/AIDS. Young People and HIV. Geneva: Joint United Nations Programme on HIV/AIDS; 2012.

40. Mberi MN, Kuonza LR, Dube NM, Nattey C, Manda S, Summers R. Determinants of loss to follow-up in patients on antiretroviral treatment, South Africa, 2004–2012: a cohort study. BMC Health Serv Res. 2015;15:259. doi: 10.1186/s12913-015-0912-2 26141729

41. Van Cutsem G, Ford N, Hildebrand K, Goemaere E, Mathee S, Abrahams M, et al. Correcting for Mortality Among Patients Lost to Follow Up on Antiretroviral Therapy in South Africa: A Cohort Analysis. PLoS ONE. 2011;6(2):e14684. doi: 10.1371/journal.pone.0014684 21379378

42. Ford N, Migone C, Calmy A, Kerschberger B, Kanters S, Nsanzimana S, et al. Benefits and risks of rapid initiation of antiretroviral therapy: a systematic review and meta-analysis. AIDS. 2017; 32(1):17. doi: 10.1097/QAD.0000000000001671 29112073

43. Rosen S, Maskew M, Fox MP, Nyoni C, Mongwenyana C, Malete G, et al. Initiating Antiretroviral Therapy for HIV at a Patient's First Clinic Visit: The RapIT Randomized Controlled Trial. PLoS Med. 2016;13(5):e1002015. doi: 10.1371/journal.pmed.1002015 27163694. Erratum in: PLoS Med. 2016 Jun;13(6):e1002050.

44. Kay ES, Batey DS, Mugavero MJ. The HIV treatment cascade and care continuum: updates, goals, and recommendations for the future. AIDS Res Ther. 2016;13:35. doi: 10.1186/s12981-016-0120-0 27826353

45. Bor J, Ahmed S, Fox MP, Rosen S, Meyer-Rath G, Katz IT, et al. Effect of eliminating CD4-count thresholds on HIV treatment initiation in South Africa: An empirical modeling study. PLoS ONE. 2017;12(6):e0178249. doi: 10.1371/journal.pone.0178249 28617805

46. Hayes R, Floyd S, Schaap A, Shanaube K, Bock P, Sabapathy K, et al. A universal testing and treatment intervention to improve HIV control: One-year results from intervention communities in Zambia in the HPTN 071 (PopART) cluster-randomised trial. PLoS Med. 2017;14(5):e1002292. doi: 10.1371/journal.pmed.1002292 28464041

47. Desai MA, Okal DO, Rose CE, Ndivo R, Oyaro B, Otieno FO, et al. Effect of point-of-care CD4 cell count results on linkage to care and antiretroviral initiation during a home-based HIV testing campaign: a non-blinded, cluster-randomised trial. Lancet HIV. 2017;4(9):e393–e401. doi: 10.1016/S2352-3018(17)30091-7 28579225

48. Granich RM, Gilks CF, Dye C, De Cock KM, Williams BG. Universal voluntary HIV testing with immediate antiretroviral therapy as a strategy for elimination of HIV transmission: a mathematical model. Lancet. 2009;373(9657):48–57. doi: 10.1016/S0140-6736(08)61697-9 19038438

49. Ford N, Nsanzimana S. Accelerating initiation of antiretroviral therapy. Lancet HIV. 3(11):e504–e5. doi: 10.1016/S2352-3018(16)30152-7 27658872

50. Amanyire G, Semitala FC, Namusobya J, Katuramu R, Kampiire L, Wallenta J, et al. Effects of a multicomponent intervention to streamline initiation of antiretroviral therapy in Africa: a stepped-wedge cluster-randomised trial. Lancet HIV. 2016;3(11):e539–e48. doi: 10.1016/S2352-3018(16)30090-X 27658873

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