Alternative antiretroviral monitoring strategies for HIV-infected patients in east Africa: opportunities to save more lives?

We sought to identify "efficient frontiers", defined as those strategies delivering the greatest health benefit given a plausible budget scenario [16, 17]. Strategies within an efficient frontier confer the greatest benefit for a specified budget. Strategies outside this frontier are unable to deliver the greatest benefit regardless of budget, and therefore are not preferred choices regardless of available resources.

We identified efficient frontiers by calculating the incremental cost-effectiveness ratio (ICER) of each monitoring strategy. ICERs measure the additive benefit of each strategy compared with its next best alternative, and interpret this benefit together with its additive cost. The ICER compares different choices in a systematic, quantitative manner, placing them "on a level playing field", and providing a widely used quantitative measure of value. Higher ICERs (meaning a greater cost per additional benefit) are less favourable, corresponding to lower value. Lower ICERs (meaning a lower cost per additional benefit) are more favourable, corresponding to higher value. ICERs are useful for informing resource allocation decisions because reallocating resources from a numerically higher (less favourable) ICER towards a numerically lower (more favourable) ICER can increase health benefits without requiring additional resources. We performed all analyses from a societal perspective using a lifetime time horizon. All costs and benefits were measured in US dollar (USD) values for 2008 and were discounted at an annual rate of 3%. In all cases, we followed recommendations of the US Panel on Cost-Effectiveness in Health [18]. We simulated cohorts of 1,000,000, with a one-day cycle time (the minimum time interval over which patient characteristics could change).

Considerable debate exists over acceptable value "thresholds" and their appropriate variation with resource constraints [19]. To aid interpretation of our ICER results for different monitoring strategies, we used our simulation to estimate ICER results for other common, resource-constrained decisions (e.g., initiation of cART at CD4 counts of 350 cells/mm³ versus 200 cells/mm³, and whether to make second- and third-line cART regimens routinely available).

We compared the downstream effects of alternative monitoring strategies on HIV-positive patients newly started on cART. In accord with the USAID-AMPATH experience, we assumed that the first cART regimen was nevirapine in combination with two nucleoside reverse transcriptase inhibitors. Distributions of age, sex and CD4 count at cART initiation were based on characteristics of patients enrolled in USAID-AMPATH (Table 1). We did not perform distinct analyses for women who were exposed to single-agent prophylaxis for mother to child transmission; however, the impact of nevirapine resistance was explored in a sensitivity analysis.

We evaluated a matrix of different monitoring strategies: type of monitoring (clinical versus CD4 versus virologic versus combinations and conditional strategies); viral load threshold for switching (500, 1000, 5000, and 10,000 copies/ml); and frequency of monitoring (three, six and 12 months). Clinical monitoring was defined as evaluation by a health professional for signs and symptoms of AIDS [20]. We deliberately constructed a broad matrix of options that included some strategies that are not guideline recommended at the current time, but which might seem like plausible alternatives (for example, obtaining routine viral load without routine CD4 counts).

Because space limitations preclude the presentation of the numerous strategies that we evaluated, we focus on results from the subset of strategies on the efficient frontier. We first identified efficient frontiers for scenarios with two and three available cART regimens. We then identified the efficient frontier for a scenario that does not specify a fixed number of cART regimens, but rather allows the number of available cART regimens to vary.

We estimated outcomes of life years, quality-adjusted life years (QALY), and costs (USD). QALYs are a preference-weighted metric that incorporate both quantity and quality of life, and reflect the idea that a year of poor-quality life is valued less than a year of high-quality life [18].

Because some strategies may be sufficiently close to an efficient frontier that their exclusion is solely due to statistical uncertainty (from random variation in the model), we performed sensitivity analyses in which the cost and effectiveness estimates for each strategy were varied over their 95% interpercentile range. In separate sensitivity analyses, to assess the impact of biased inputs, we varied all inputs to the model across their plausible ranges, seeking to identify whether changes in model input assumptions would lead to different strategies on the efficient frontier.

When we explored a scenario in which two cART regimens were available (Table 2, Figure 2), no laboratory monitoring strategies employing routine CD4 monitoring alone (e.g., CD4 count every six months) were on the efficient frontier. Overall, these strategies did not offer a good use of healthcare resources, because greater benefit would be conferred by alternative strategies, regardless of a programme's budget or willingness to pay for health benefits.

When willingness to pay remained limited to initiating cART at a CD4 count of 200 cells/mm³ rather than 350 cells/mm³, the efficient frontier was mostly comprised of monitoring strategies that were structured conditionally, in which CD4 was obtained routinely and a follow-up viral load was only obtained if the CD4 count met WHO criteria for immunologic failure. Conservative monitoring frequencies (12 or six months rather than three months) and switching thresholds (10,000 copies/mL rather than 500 copies/mL) were preferred. In sensitivity analyses, only one strategy employing routine CD4 monitoring alone (every 12 months) was close to the efficient frontier.

As willingness to pay rose beyond initiating cART at a CD4 count of 350 cells/mm³ rather than 200 cells/mm³, the efficient frontier continued to be mostly comprised of monitoring strategies that were structured conditionally; however, these strategies now employed less conservative monitoring frequencies and switching thresholds. Only one strategy employing routine CD4 monitoring alone (every six months) was close to the efficient frontier.

As willingness to pay greatly exceeded the value of earlier cART initiation, the efficient frontier became comprised of monitoring strategies that used routine viral load monitoring, with progressively greater frequencies and less conservative switching thresholds.

When we explored a scenario in which three cART regimens were available (Table 3, Figure 3), strategies with routine CD4 monitoring alone continued to be excluded from the efficient frontier, and therefore never offered a good use of healthcare resources. As willingness to pay approached the value of cART initiation at a CD4 count of 350 cells/mm³ rather than 200 cells/mm³ (ICER $2600/QALY), the efficient frontier was comprised of monitoring strategies that were structured conditionally, where CD4 was obtained routinely and a follow-up viral load was only obtained if the CD4 count met WHO immunologic criteria. As willingness to pay greatly exceeded the value of earlier cART initiation, the efficient frontier was comprised of monitoring strategies that used routine viral load monitoring. In sensitivity analyses, no strategy employing routine CD4 monitoring alone was close to the efficient frontier.

When we considered a scenario that does not specify a fixed number of cART regimens, but rather allows the number of available cART regimens to vary (Table 4, Figure 4), strategies for routine CD4 monitoring alone continued to be excluded from the efficient frontier. At willingness-to-pay levels below that of earlier cART initiation, the efficient frontier was limited to a sole strategy (one cART regimen and using clinical rather than laboratory monitoring). As willingness-to-pay levels rose above that of early cART initiation, the greatest benefit was delivered by incorporating multiple regimens with routine viral load monitoring. In sensitivity analyses, only two strategies employing routine CD4 monitoring alone were close to the efficient frontier.

Conditional strategies were no longer on the efficient frontier because the ICER of routinely offering multiple cART regimens (compared with providing one cART regimen only) was fairly high (ICER > $5000/QALY), and because the ICER of any laboratory testing strategy would only be favourable if multiple cART regimens were routinely offered. As willingness to pay exceeded the ICER of offering multiple cART regimens, they were also high enough to support the ICER of routine use of viral load testing.

Sensitivity analyses suggested that efficient frontiers were robust to alternative assumptions (Additional file 1, Figure S2), with monitoring strategies based on CD4 counts alone almost never falling on the efficient frontier. A notable exception to this stability occurred when assumptions were varied regarding the pricing of second- and third-line cART regimens relative to first-line cART. When later cART regimens were assumed to be no more expensive than first-line cART regimens, the value of monitoring strategies that involved routine viral load testing became more favourable.