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Low risk of attrition among adults on antiretroviral therapy in the Rwandan national program: a retrospective cohort analysis of 6, 12, and 18 month outcomes
© Nuwagaba-Biribonwoha et al.; licensee BioMed Central Ltd. 2014
Received: 29 March 2014
Accepted: 29 July 2014
Published: 29 August 2014
We report levels and determinants of attrition in Rwanda, one of the few African countries with universal ART access.
We analyzed data abstracted from health facility records of a nationally representative sample of adults [≥18 years] who initiated ART 6, 12, and 18 months prior to data collection; and collected facility characteristics with a health facility assessment questionnaire. Weighted proportions and rates of attrition [loss to follow-up or death] were calculated, and patient- and health facility-level factors associated with attrition examined using Cox proportional hazard models.
1678 adults initiated ART 6, 12 and 18 months prior to data collection, with 1508 person-years [PY] on ART. Attrition was 6.8% [95% confidence interval [CI] 6.0-7.8]: 2.9% [2.4-3.5] recorded deaths and 3.9% [3.4-4.5] lost to follow-up. Population attrition rate was 7.5/100PY [6.1-9.3]. Adjusted hazard ratio [aHR] for attrition was 4.2 [3.0-5.7] among adults enrolled from in-patient wards [vs 2.2 [1.6-3.0] from PMTCT, ref: VCT]. Compared to adults who initiated ART 18 months earlier, aHR for adults who initiated ART 12 and 6 months earlier was 1.8 [1.3-2.5] and 1.3 [0.9-1.9] respectively. Male aHR was 1.4 [1.0-1.8]. AHR of adults enrolled at urban health facilities was 1.4 [1.1-1.8, ref: rural health facilities]. AHR for adults with CD4+ ≥200 cells/μL vs <200 cells/μL was 0.8 [0.6-1.0]; and adults attending facilities with performance-based financing since 2004–2006 [vs. 2007–2008] had aHR 0.8 [0.6-0.9].
Attrition was low in the Rwandan national program. The above patient and facility correlates of attrition can be the focus of interventions to sustain high retention.
Millions of HIV-infected adults have initiated antiretroviral therapy [ART] in the past decade, but the overall impact of these programs can be compromised by patient attrition, including death and loss to follow-up [1–8]. Rwanda is one of a handful of African countries to have achieved universal ART access, with at least 80% of the people eligible for ART receiving it [9, 10]. ART services in Rwanda were established in 2002, and by 2012, over 100,000 HIV-infected patients had initiated ART at more than 400 health facilities [11, 12]. High levels of retention on ART were reported for the first few years of the national program [13, 14]; indeed, in a nationally representative study conducted in 2004–2005, 92% and 86% of patients who initiated ART 6 and 12 months earlier, respectively, were alive and on ART at the health facility of ART initiation . Over time, the national program expanded significantly, with over a five-fold increase in the number of facilities providing ART and the number of patients initiating ART . As Rwanda, continues to build sustainable ART programs, it is important to continually assess whether these high levels of retention can be sustained with program scale-up and universal ART access. We use data from a nationally representative study of adults initiating ART to report on levels and correlates of attrition.
Study design and data collected
During the study period the national adult ART initiation criteria in Rwanda were CD4 < 200 cells/μL or WHO stage IV, with stavudine and zidovudine as the main nucleoside reverse-transcriptase inhibitors used in first line ART regimens . Patients sampled for the study described above were eligible for this analysis if they were 18 years or older, and had initiated first-line ART at one of the study facilities 6, 12, and 18 months [+/− 2 months] prior to data collection or transferred into one of the study facilities within 30 days of ART initiation. We aimed to determine the population estimate of attrition by conducting secondary analysis of an existing dataset, using the entire sample. Basing on Lowrance et al’s estimates of death and lost to follow-up, we determined that a dataset of 1798 would allow detection of attrition between 5% and 7% with >90% power and 5% precision. Of the 1798 adults originally sampled, 120 were excluded as they started ART outside of the above-specified timeframe [n = 24], were missing information on the date of ART initiation [n = 90], ART regimen [n = 1], and age [n = 1], or transferred to another health facility on the same day as starting ART [n = 4], resulting in a final analytic sample of 1678 adults (Figure 1).
The outcome for this analysis was attrition, which included patients who were known to have died and those who were lost to follow-up [LTF]. Adults were considered LTF if they were not known to have died or transferred to another health facility and had not made a clinical or pharmacy visit in the 90 days before data abstraction. Adults were considered retained on ART if they picked up ART in the 90 days preceding data abstraction. Adults who were recorded as transferring out to another health facility were reported in a separate category, and not included in the retained or attrition outcomes.
Statistical analysis was conducted using Stata software version 12.1 [StataCorp. 2011. Stata Statistical Software: Release 12. College Station, TX: StataCorp LP]. Survey procedures, including finite population correction, were used to adjust estimates for the complex survey design. We applied sampling weights that took into account the probability of a health facility being selected from the 113 health facilities providing ART at the time of sampling and the probability of a participant being selected from all adults who initiated ART at 6, 12 and 18 months previously, and thus results presented in this paper represent population-wide estimates of attrition. Descriptive statistics were computed for patient- and health facility-level characteristics. We calculated the proportion and rates per 100 person years [PY] of attrition for the entire population and by time on ART [i.e. 6, 12 and 18 months], and the 95% confidence interval around these estimates. Adults who transferred to another health facility were censored at the date of transfer.
Patient- and health facility-level factors associated with attrition were modeled using weighted data in bivariate and multivariable Cox proportional hazard models to calculate crude and adjusted hazard ratios and 95% confidence intervals. Variables included in the model were pre-selected according to hypothesised relevance and data availability, excluding variables that were collinear or lacked heterogeneity. We aggregated adults who had initiated ART 6, 12, and 18 months prior to data collection to increase statistical power, and controlled for time since ART initiation in the multivariable model.
The study protocol was approved by the Rwanda National Ethics Committee and the Institutional Review Board at Columbia University. This study was funded through the President’s Emergency Plan for AIDS Relief [PEPFAR] through the Centers for Disease Control and Prevention [CDC] and received Associate Director of Science [ADS] clearance. This analysis was based on data collected by abstraction from existing medical records; individual-level patient consent was waived by all approving ethical boards, and not sought.
A total of 1678 adults were included in this analysis, 644 [37.4%], 578 [33.3%], and 456 [29.3%] who had initiated ART 6, 12 and 18 months prior to data collection, respectively. The total amount of follow-up time was 1508 person years, while the average follow-up time was 11.3 months. The weighted population was 8,373, 3123 [37.3%], 2762 [33.0%], and 2488 [29.7%] patients who had initiated ART 6, 12 and 18 months prior to data collection respectively, and represented 86.4% of the sampling frame population of 9,693.
Patient characteristics: overall distribution and by time on ART
Time on ART prior to data collection
Overall (all adults)
6 months on ART
12 months on ART
18 months on ART
n = 1,678
n = 644
n = 578
n = 456
Source of referral to ART clinic
WHO stage at ART initiation d
Stage I and II
CD4+ count (cells/μL) at ART initiation
0 – 199
Initial ART regimen containing…
Characteristics of clinic attended
Start of performance based financing
Home visits support for PLWHA e
Half the population attended health facilities located in rural areas [50.0%], and the majority attended health centers [64.2%, vs 35.8% at hospitals]; and public government facilities [74.7%, vs 25.3% at faith based health facilities]. All health facilities had performance based financing Nearly half [44.9%] of the population attended health facilities where performance based financing had been introduced more recently [2007–2008 vs. 2004–2006] and half attended health facilities where home visit support services for patients who miss health facility visits were available [50.9%].
When comparing the population by time of ART initiation, the population who initiated ART 6 and 12 months prior to data collection had a higher proportion of older adults [36 years and older], adults with WHO Stage I and II at ART initiation, and adults with CD4+ count above 200 cells/μL at ART initiation, than the population who initiated ART 18 months prior to data collection. Stavudine use in the initial ART regimen declined from 83.3% to 65.3% and 34.1% for adults who had initiated ART 18, 12 and 6 months previously, while zidovudine use increased from 16.6% to 34.1% and to 65.8% respectively.
Proportion and rate of attrition and transfers per 100 person years: overall and by time on ART
Time on ART prior to data collection
Overall (all adults)
6 months on ART
12 months on ART
18 months on ART
1509 person years
330 person years
559 person years
619 person years
[6.0 – 7.8]
[2.7 – 4.5]
[7.1 – 10.9]
[7.9 – 11.4]
[2.4 – 3.5]
[1.1 – 2.3]
[3.5 – 6.0]
Lost to follow-up
[3.4 – 4.5]
[1.3 – 2.7]
[5.0 – 7.0]
[3.2 – 5.6]
[4.5 – 6.8]
[4.5 – 8.2]
[2.5 – 5.3]
[4.8 – 9.8]
Retained on ART
[86.0 – 89.2]
[88.4 – 92.2]
[84.7 – 90.0]
[80.4 – 87.5]
[6.1 – 9.3]
[4.3 – 11.9]
[6.6 – 12.7]
[4.6 – 9.2]
[2.3 – 4.5]
[1.7 – 6.9]
[1.6 – 5.6]
[2.0 – 5.9]
Lost to follow-up
[3.3 – 5.6]
[1.8 – 8.8]
[4.2 – 9.2]
[2.0 – 4.9]
[4.7 – 7.8]
[7.9 – 19.4]
[2.4 – 6.3]
[3.4 – 7.5]
Retained on ART
[92.8 – 98.7]
[174.5 – 184.6]
[88.1 – 92.6]
[59.5 – 62.7]
Crude and adjusted Cox proportional models for the hazard of attrition (death or loss to follow-up)
Multi-variable model n = 1,678
HR of attrition
aHR of attrition
Time on ART prior to data collection
18 months on ART
6 months on ART
[0.8 – 1.7]
[0.9 - 1.9]
12 months on ART
[1.2 - 2.4]
[1.3 - 2.5]
[0.5 - 1.2]
[0.5 - 1.3]
[0.6 - 1.2]
[0.7 - 1.4]
[0.4 - 0.9]
[0.5 - 1.3]
[1.0 - 1.6]
[1.0 - 1.8]
Source of referral to ART clinic
Voluntary Counseling and Testing
[1.6 - 2.7]
[1.6 - 3.0]
[3.0 - 5.6]
[3.0 - 5.7]
[1.2 - 2.2]
[1.1 - 2.0]
CD4+ count at ART initiation (cells/μL)
0 – 199
[0.5 - 0.9]
[0.6 - 1.0]
[0.7 - 1.3]
[0.8 - 1.3]
Initial ART regimen
[0.9 - 1.3]
[0.8 - 1.2]
[0.7 - 3.6]
[0.8 - 3.9]
[1.1 - 2.0]
[1.1 - 1.8]
[0.7 - 1.2]
[0.6 - 1.1]
Start of performance based financing
[0.6 - 1.2]
[0.6 - 0.9]
Home support visits for PLWHA available
[0.9 - 1.6]
[1.0 - 1.6]
The hazard of attrition was lower among adults whose CD4+ count at ART initiation was 200 cells/μL or greater, aHR 0.8 [95% CI: 0.6-1.0], compared to those who initiated ART with CD4+ counts below 200 cells/μL. Lower attrition hazard was also observed among adults who attended health facilities that had longer-standing performance-based financing [since 2004–2006], aHR 0.8 [95% CI: 0.6-0.9], compared to patients attending health facilities where performance based financing had began more recently [2007–2008]. Age, initial ART regimen, level of health facility and availability of home visit services were not significantly associated with attrition in adjusted analyses.
We assessed levels of attrition 6, 12 and 18 months following ART initiation among a nationally representative sample of adults receiving HIV services in Rwanda. We estimated overall population attrition to be 6.8% and the attrition rate as 7.5/100 PY. Lowrance et al., who explored this question in the early phase of the Rwanda ART program [2004–2005], reported attrition of 6.7% of patients at 6 months and 9.5% at 12 months on ART . We found much lower attrition at 6 months, 3.5%, and approximately the same attrition at 12 months, 8.8%, in 2007–2008, suggesting a significant reduction in attrition at the 6 months following ART initiation. Our results tally with more recent findings using a significantly larger sample in two regions of Rwanda . This is an important finding because the risk of attrition tends to be highest immediately after ART initiation, and is usually due to high mortality within this time period [18–20]. These findings may reflect the benefits of initiating ART earlier in HIV disease, as the median CD4+ count at ART initiation in our sample was 65 cells/μL, higher than that observed by Lowrance et al.
While Lowrance et al. observed that death and LTF contributed equally to attrition in the early phase of ART scale-up in Rwanda, our data indicate that LTF increasingly accounts for the majority of attrition. This may reflect deteriorating ascertainment and documentation of deaths as the ART program expands, and an increase in undocumented transfers as ART services are decentralized [20–22]. Stronger linkages and feedback between communities and health facilities [to report deaths] and between health facilities [to report transfers] could result in more accurate estimations of true loss to follow-up, mortality, and transfers and thus more complete assessment of the ART program impact.
While the level of attrition observed in our sample was in-line with other findings from Rwanda [13, 14, 23, 17], it is substantially lower than that observed in other programs within the East African region, which report attrition in the range of 18% to 40% 12 months after ART initiation [24–28]. Multiple factors may be contributing to the low attrition in ART programs in Rwanda. First, the median CD4+ count at ART initiation in our population was significantly higher than has been observed in other countries [18, 25, 29, 30], and could account for this association. Our results also showed that CD4+ counts >200/μL were associated with a 20% reduction in attrition. Notably, patients whose CD4+ counts at ART initiation were missing had similar hazard of attrition to the patients with the lowest CD4+ counts. This finding suggests that patients whose CD4+ counts are not assessed and recorded at ART initiation may be as vulnerable to attrition as the sickest patients. Secondly, adults in the Rwanda ART program tend to have high adherence to ART [31, 32] which in turn can reduce mortality, and thus attrition. This is further evidenced by adherence and viral load assessments conducted on a subset of participants in this analysis which revealed that overall [combining adults on ART 6, 12 and 18 months], 94% and 78% took 100% of their medication in the 3 and 30 days preceding the interview, and 83% had viral load under 40 copies/mL at the time of interview .
The most significant factor associated with increased hazard of attrition in our study was starting ART while admitted within an in-patient ward. This finding has been observed by others , and is likely due to high mortality in this severely ill group and LTF due to undocumented deaths [20, 34]. Indeed, the median CD4 count at ART initiation among in-patients was about a third of observed among other study participants. Recent recommendations by WHO and the Rwanda Ministry of Health [35–37], which endorse ART initiation at higher CD4 counts [350 cells/μ/L and more recently 500 cells/μ/L], could result in adults initiating ART earlier in HIV disease, and thus lower attrition. Enrolling from PMTCT services was also associated with high attrition. This has been observed in a number of African programs [38, 39], and is a challenge worth addressing as countries begin to implement for life-long ART for all pregnant and breastfeeding women. The finding that men had higher attrition than women is not uncommon in African HIV treatment programs [40–44]; this is a high risk group that requires targeted interventions to minimize attrition.
Adults who attended health facilities with a longer duration of performance based financing had a lower hazard attrition in our analysis. Although our analysis lacked data to comparatively examine attrition at facilitates without performance based financing, implementation of performance based financing is perceived as a strong motivator for provision of better health care services [45–47], and may have contributed to improvements in patient outcomes at these health facilities clinics. It is possible that sites that initiated performance based financing earlier had other unmeasured characteristics that influenced attrition outcomes, and further research should examine the specific impact of this strategy on lowering attrition in African ART programs.
Our study did not find a correlation between home visits and attrition, a finding in line with results of a multi-country ecological study examining the impact of site-level factors on attrition . Whereas it has been observed that home-visits can be associated with better retention , it is likely that in our setting of high retention, the impact of home visits was minimal, particularly if targeted to patients with high risk of attrition that may have insurmountable barriers to returning to care.
Our study had a number of strengths. We had a large sample of adults drawn from a nationally representative sample of adults on ART, and there was representation from different types of health facilities in various settings. The study was conducted in one of the first few African countries to achieve universal ART access. In multivariate analyses, we explored associations between both patient- and health facility- level factors and attrition. A limitation to note, however, is that the study lacked sufficient power to examine factors associated with death and LTF in separate models or present results stratified by time on ART. Despite this, the results effectively demonstrate the low attrition rates and some key factors associated with the risk of attrition for the overall population.
Our results suggest sustained low attrition in the Rwanda national ART program in the context of significant expansion in the number of clinics providing HIV care and treatment services and the number of patients on ART. Loss to follow-up was the more significant contributor to attrition suggesting that better ascertainment and documentation of deaths and patient transfers may be necessary. In this context of universal ART access, specific groups remain at risk of high attrition [including in-patients, men, PMTCT clients and adults attending urban facilities] and require targeted interventions to further reduce attrition. Performance-based financing could be a useful tool in minimizing attrition in this context.
We thank the participants and staff at the facilities included in the study for their participation; study co-investigators, collaborators and the field team. The work in this publication was supported by the United States President’s Emergency Plan for AIDS Relief [PEPFAR] through the United States Centers for Disease Control and Prevention [CDC] under the terms of Cooperative Agreement Number U62/CCU222407 in partnership with the Global Fund to Fight AIDS, Tuberculosis and Malaria. The contents of this publication are solely the responsibility of the authors and do not necessarily represent the official views of PEPFAR, CDC or Global Fund.
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