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. 2017 Apr 18;14(4):e1002278. doi: 10.1371/journal.pmed.1002278

Clinical decision tools are needed to identify HIV-positive patients at high risk for poor outcomes after initiation of antiretroviral therapy

Margaret L McNairy 1,2,*, Elaine J Abrams 1,3, Miriam Rabkin 1,3, Wafaa M El-Sadr 1,3
PMCID: PMC5395167  PMID: 28419097

Abstract

Margaret McNairy and colleagues highlight the need for clinical decision tools to help identify HIV patients who would benefit from tailored services to avoid poor outcomes such as death and loss to follow-up.


Summary points

  • Current interest in differentiated models for HIV care has largely focused on the needs of stable patients who are doing well on antiretroviral therapy. However, tailored services are also needed for patients at the other end of the spectrum, those at high risk for poor outcomes such as death and loss to follow-up.

  • Clinical decision tools such as risk scores are needed to identify patients at high risk for poor outcomes and to provide individualized risk assessment.

  • Risk scores need to be simple to use, utilize routinely collected variables, be accurate in predicting risk, and be generalizable across contexts.

Introduction

Over the past decade, the scale-up of HIV programs in resource-limited settings has been remarkable, with over 17 million persons initiating lifesaving antiretroviral therapy (ART) by the end of 2015 [1]. However, in order to reduce HIV-related morbidity and mortality and decrease the number of new infections, it is critical to double the number of HIV-positive patients on treatment by 2020 [2]. It is equally important for health outcomes among children and adults on ART to be optimized [2,3]. To achieve these two goals—i.e., a massive increase in the number of patients on ART as well as an enhancement in the quality of care—the global health community has recognized the need for tailored HIV services to meet the unique needs of different patient groups, often referred to as differentiated models of service delivery [4].

The World Health Organization (WHO) recommends differentiating patients into four groups: those presenting with asymptomatic HIV infection at ART initiation, those initiating ART with advanced HIV disease, those who are already on ART but are unstable on treatment, and lastly those stable on ART with high adherence and a favorable clinical response [5]. However, to date, the focus has largely been on establishing differentiated service models for stable patients with the goal of maintaining adherence and retention, enhancing patient satisfaction, and increasing efficiencies in HIV programs, given the reality of overcrowded clinics that strain the capacity of the limited health workforce. Patient-managed community ART groups, one example of a differentiated service delivery model for stable patients, require fewer clinical assessments at health facilities. This in turn decompresses health facilities, relieves the workload of health care workers, and enables the patients to avoid transport costs, long wait times, and time lost from family or work [6]. Eligibility criteria for these groups and similar less intensive models of care are often based on prior performance—i.e., evidence of 6–12 months of excellent clinic attendance with high adherence to treatment and, if available, evidence of viral suppression [7,8]. Reported outcomes among such groups are impressive, with over 95% of patients retained at 1 year [7,9].

The need for a priori identification of patients at high risk for poor outcomes

Patients at high risk for poor outcomes, on the other hand, also require a service model that is tailored to their unique needs. The first group of such patients consists of those at high risk for early death after ART initiation. Adults with advanced HIV disease have been noted to have mortality rates up to 5-fold higher in the first 6 months after treatment initiation compared with after 1 year [10,11]. Mortality rates also remain high in the first year of treatment among more recent cohorts with less advanced disease [12]. In a study of 19 cohorts with advanced disease from sub-Saharan Africa, the mortality rate in the first 4 months after ART initiation was 19.1 deaths per 100 person years (PY), decreasing to 1.3 deaths/100 PY beyond 1 year of follow-up [11]. Similarly, in a multicountry study of over 37,000 HIV-infected children, the mortality rate in the first 6 months was 9.1 deaths/100 PY versus 4.5 deaths/100 PY at 24 months [13]. This high early mortality is particularly evident among patients with HIV-related tuberculosis, cryptococcal meningitis, or malnutrition [1416]. For children, poor growth, advanced disease, and young age are also predictive of early death [13,16].

The second group of patients at high risk for poor outcomes consists of those who default early from care. Rates of loss to follow-up among adults and children are highest in the first year after enrollment in care or initiation of treatment, with up to one-third of adult patients noted to be lost to follow-up within the first 6 months [12,17,18]. Outcomes among those who default from care are poor. In a meta-analysis of 28 studies conducted in sub-Saharan African countries reporting outcomes among patients who were categorized as lost to follow-up with unknown vital status and were traced in the community, the unreported mortality was 30% (95% CI 21.1%–38.9%) [19]. Moreover, patients enrolled in care but who have yet to initiate ART who experience more than a 12-month gap in their follow-up were found to re-present to clinics with more advanced disease, which could have been prevented with more consistent engagement in care [20]. Similarly, tracing studies among children who have been lost to follow-up found that 16% of HIV-positive children and 29% of children with unknown HIV status had died [21].

The evidence of poor outcomes among the two groups of patients described above demonstrates that it is critically important to identify, a priori, these patients at the time of ART initiation in order to prevent their loss to follow-up and to improve their clinical outcomes. Risk scores and clinical decision tools have been used widely in clinical medicine to simplify and standardize the identification of individuals at highest risk for a specific condition or health outcome. For example, risk scores are used to predict patients at high risk for cardiovascular disease [22] and pneumonia-related mortality [23] and to determine the need for hospitalization among patients presenting with syncope [24]. In the context of HIV, risk scores have been developed based on data from United States and European cohorts to assess short-term disease progression in HIV-positive patients on ART, 1-year mortality, and viral suppression, but none have been developed based on information from HIV-positive patients in low- and middle-income countries [2527].

Risk factors for poor outcomes in HIV are known, but individual prediction tools are lacking

While multiple studies have identified individual risk factors associated with early death and loss to follow-up among HIV-positive patients in resource-limited settings, work is needed to translate univariable and multivariable models into validated and easy-to-use risk scores to predict an individual’s risk of death and loss to follow-up after ART initiation [11,2831]. In contrast to the use of CD4+ count or WHO HIV disease staging to identify high-risk patients for disease progression, a composite risk score may provide more specific information on the magnitude of risk for each patient by integrating additional variables such as weight, history, or the presence of a specific opportunistic infection and other parameters. Risk scores also may identify patients who may not have advanced HIV disease but are at high risk of poor outcomes because of a combination of socioeconomic or demographic variables such as limited income, un- or underemployment, and a fragile social support network. For example, while most providers are likely to intuit that a patient with a CD4+ count < 50 cells/mm3 or with concurrent tuberculosis is at high risk for early mortality even after initiation of ART, there is more ambiguity in determining the risk of early mortality for a patient with a CD4+ count of 250 cells/mm3 who lives alone and is unemployed.

Similar to the assessment of risk of early mortality, it is also critical to identify those at high risk for loss to follow-up at the time of ART initiation. Among adults, factors associated with loss to follow-up include male sex, adolescence and young adulthood, low income, and low educational attainment [12,32]. For children, factors include age (<5 years as well as adolescence), stigma from peers, family and community members, transport to clinic, and lack of disclosure of HIV infection to the child [13,21,33]. There are other potential variables that may be associated with loss to follow-up to increase the precision of a risk score such as distance to clinic, prior clinic attendance, family support, and social stressors that could be incorporated in deriving precise risk scores for loss to follow-up [34].

Ideally, risk scores for both early mortality and for loss to follow-up should be based on routinely collected clinical, laboratory, and demographic information in order to enable their utilization across contexts. Fortunately, many HIV programs routinely collect common patient variables such as age, sex, marital status, pregnancy status, weight, CD4+ count, WHO disease stage, history, and current tuberculosis (TB) status among other parameters. Other potential variables that can be easily obtained include education level, income, other comorbid diseases, the presence of other household members with HIV, disclosure status, the presence of depression, and health facility characteristics such as the level of the facility (e.g., hospital versus health center) and the distance of the health facility from the patient’s home.

A useful risk score must be distinguished by its potential for easy incorporation into clinical practice, be reliable when applied by diverse cadres of health care providers, and be accurate in predicting risks across settings [35]. It is important to avoid the complexity of some existing risk scores that involve lengthy calculations and subtle clinical judgment, which is subject to variation by provider. Once a risk score is proposed for identifying patients at high risk for poor outcomes, it must then be externally validated to determine if its accuracy is preserved when applied to a new population or setting and also over time. It is also important for the proposed risk score to undergo formal impact analysis to evaluate if the score or prediction rule influences physician behavior and patient outcomes, a step that is neglected for many proposed prediction rules [36,37]. While a risk score may have excellent accuracy, it is only useful if it will be used by providers to change or direct their decisions. And finally, a fourth phase of research is to evaluate if the rule has been actually implemented in practice [37].

Differentiated HIV service delivery for high-risk patients

While the development of simple risk scores to identify patients at high risk for poor outcomes could be of substantial value, further efforts are needed to define interventions and care models to minimize the risk of these poor outcomes. Interventions to mitigate early mortality after ART initiation for patients with advanced HIV disease may include hospitalization of severely ill patients, providing prophylaxis or pre-emptive therapy for opportunistic infections, and/or more intensive clinical visit schedules. The WHO guidelines recommend for such patients the rapid initiation of ART, screening and prompt treatment for coexisting TB or cryptococcus, and provision of isoniazid preventive therapy, if indicated, as well as intensive follow-up for patients with CD4+ count < 200 cells/mm3 or WHO stage III/IV disease [5]. The Reduction of Early Mortality in HIV-Infected Adults and Children Starting Antiretroviral Therapy (REALITY) trial conducted in Zimbabwe, Kenya, Malawi, and Uganda found that enhanced prophylaxis at the time of ART initiation with ongoing cotrimoxazole prophylaxis, 12 weeks of isoniazid/pyridoxine, 5 days of azithromycin, and a single dose of albendazole was associated with a 25% reduction in early mortality among adults and children with CD4+ counts < 100 cells/mm3 [38]. The Reduction of Early Mortality among HIV-Infected Subjects Starting Antiretroviral Therapy (REMSTART) trial conducted in Tanzania and Zambia, in which patients at clinics were assigned to a combination strategy that included screening for cryptococcal disease coupled with 4 weeks of home visits for monitoring response and ART adherence support, resulted in a 28% decrease in mortality when compared to the standard of care [39]. For patients at high risk of loss to follow-up, structural and behavioral interventions such as accelerated ART initiation, phone messaging and texting for appointment reminders, tailored community support, and transport vouchers may be necessary to enhance retention in care [40].

Conclusions

Over the past decade, the scale-up of HIV services has saved millions of lives, but a substantial proportion of patients continue to suffer poor health outcomes, particularly in the first year of treatment. Clinical decision tools, including risk scores, are urgently needed to promptly identify such patients and to guide them to appropriately tailored services that offer them individual benefits while at the same time contributing to the efficient use of health system resources.

Abbreviations

ART

antiretroviral therapy

PY

person year

REALITY

Reduction of Early Mortality in HIV-Infected Adults and Children Starting Antiretroviral Therapy

REMSTART

Reduction of Early Mortality among HIV-Infected Subjects Starting Antiretroviral Therapy

TB

tuberculosis

WHO

World Health Organization

Funding Statement

The authors received no funding for this work.

Footnotes

Provenance: Not commissioned; externally peer-reviewed

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