Evaluating the impact of policies recommending PrEP to subpopulations of men and transgender women who have sex with men based on demographic and behavioral risk factors
Authors:
Holly Janes aff001; Marshall D. Brown aff001; David V. Glidden aff002; Kenneth H. Mayer aff003; Susan P. Buchbinder aff004; Vanessa M. McMahan aff005; Mauro Schechter aff006; Juan Guanira aff007; Martin Casapia aff008
Authors place of work:
Vaccine and Infectious Disease Division, Fred Hutchinson Cancer Research Center, Seattle, Washington, United States of America
aff001; Department of Epidemiology and Biostatistics, University of California School of Medicine, San Francisco, California, United States of America
aff002; Division of Infectious Diseases, Beth Israel Deaconess Medical Center, and The Fenway Institute, Fenway Health, Boston, Massachusetts, United States of America
aff003; Bridge HIV, San Francisco Department of Public Health, San Francisco, California, United States of America
aff004; Department of Medicine, University of Washington, Seattle, Washington, United States of America
aff005; Projeto Praça Onze, Universidade Federal do Rio de Janeiro, Rio de Janeiro, Brazil
aff006; Asociación Civil Impacta Salud y Educación, Lima, Peru
aff007; Asociación Civil Selva Amazónica, Iquitos, Peru
aff008
Published in the journal:
PLoS ONE 14(9)
Category:
Research Article
doi:
https://doi.org/10.1371/journal.pone.0222183
Summary
Introduction
Developing guidelines to inform the use of antiretroviral pre-exposure prophylaxis (PrEP) for HIV prevention in resource-limited settings must necessarily be informed by considering the resources and infrastructure needed for PrEP delivery. We describe an approach that identifies subpopulations of cisgender men who have sex with men (MSM) and transgender women (TGW) to prioritize for the rollout of PrEP in resource-limited settings.
Methods
We use data from the iPrEx study, a multi-national phase III study of PrEP for HIV prevention in MSM/TGW, to build statistical models that identify subpopulations at high risk of HIV acquisition without PrEP, and with high expected PrEP benefit. We then evaluate empirically the population impact of policies recommending PrEP to these subpopulations, and contrast these with existing policies.
Results
A policy recommending PrEP to a high risk subpopulation of MSM/TGW reporting condomless receptive anal intercourse over the last 3 months (estimated 3.3% 1-year HIV incidence) yields an estimated 1.95% absolute reduction in 1-year HIV incidence at the population level, and 3.83% reduction over 2 years. Importantly, such a policy requires rolling PrEP out to just 59.7% of MSM/TGW in the iPrEx population. We find that this policy is identical to that which prioritizes MSM/TGW with high expected PrEP benefit. It is estimated to achieve nearly the same reduction in HIV incidence as the PrEP guideline put forth by the US Centers for Disease Control, which relies on the measurement of more behavioral risk factors and which would recommend PrEP to a larger subset of the MSM/TGW population (86% vs. 60%).
Conclusions
These findings may be used to focus future mathematical modelling studies of PrEP in resource-limited settings on prioritizing PrEP for high-risk subpopulations of MSM/TGW. The statistical approach we took could be employed to develop PrEP policies for other at-risk populations and resource-limited settings.
Keywords:
Biology and life sciences – Organisms – People and places – Population groupings – Medicine and health sciences – Microbiology – Medical microbiology – Microbial pathogens – Pathology and laboratory medicine – Pathogens – infectious diseases – Viral pathogens – Immunodeficiency viruses – HIV – Retroviruses – Lentivirus – viruses – RNA viruses – Public and occupational health – Preventive medicine – Viral diseases – HIV infections – Sexually transmitted diseases – Epidemiology – Medical risk factors – Sexuality groupings – Men who have sex with men – HIV epidemiology – Prophylaxis – Pre-exposure prophylaxis – HIV prevention
Introduction
Pre-exposure prophylaxis (PrEP) with tenofovir disoproxil fumarate (TDF)-based oral antiretroviral regimens has been shown to be efficacious for preventing HIV acquisition in cisgender men who have sex with men (MSM), transgender women (TGW), HIV serodiscordant heterosexual couples, and people who inject drugs, with less consistent results among cisgender women [1–7]. Low adherence is likely a major factor explaining the variable efficacy across trial populations [8–10], although biological and behavioral factors may also play a role [11–18].
PrEP delivery requires considerable public health infrastructure to maximize adherence and to screen PrEP users regularly for renal safety, sexually transmitted infections (STIs), and incident HIV infection to prevent PrEP use post-infection; drug resistance is also possible [1–5]. With the licensing of oral co-formulated TDF and emtricitabine (FTC) (FTC-TDF) as PrEP [19], the World Health Organization (WHO) and the US Centers for Disease Control and Prevention (CDC) have disseminated guidelines for the use of PrEP for HIV prevention. In developing such guidelines, the population incidence of HIV, expected PrEP effectiveness, cost of medical care and infrastructure associated with PrEP delivery, and access to PrEP must be considered. Furthermore, in resource-limited settings, policies that prioritize PrEP for select subpopulations warrant consideration.
Inspired by the approaches to policy development and evaluation in other clinical contexts [20–25], we used data from iPrEx, the largest PrEP efficacy trial to date in MSM/TGW, to identify subpopulations of MSM/TGW who could be prioritized for PrEP rollout in resource-limited settings. We relied on a decision-theoretic framework, under which the optimal policy is that which maximizes population net benefit [26–32]. The optimal policy would recommend PrEP to subpopulations with the highest absolute reduction in HIV incidence due to PrEP. We call this a “PrEP-benefit-based policy”. We also considered a “risk-based” PrEP policy, similar in concept to those put forth in the WHO and CDC guidelines [33, 34], which recommends PrEP to individuals at high risk of HIV acquisition without PrEP. A risk-based policy would achieve the same population impact as a PrEP-benefit based policy if the effect of PrEP was a constant reduction in risk of HIV, i.e. if there was no modification of the PrEP effect on the relative risk scale [28, 29, 35, 36]. Under this assumption, the reduction in absolute HIV risk due to PrEP is proportional to risk of HIV without PrEP, and thus high-risk subpopulations have the largest absolute reduction in HIV incidence due to PrEP. This may be the implicit assumption underlying the risk-based policies used in existing guidelines. If, however, demographic or risk behavior characteristics modify the relative risk associated with PrEP, then subgroups at high risk of HIV without PrEP may not be those with the highest benefit from PrEP. We evaluated both risk- and benefit-based PrEP policies to explore this possibility. Specifically, we fit statistical models to the iPrEx data to identify both MSM/TGW subpopulations at high risk of HIV acquisition without PrEP, and subpopulations with high expected PrEP benefit. Next, we used these models to define risk- and PrEP-benefit-based policies, and determine the size of the MSM/TGW subpopulations who would be recommended to take PrEP and the expected HIV incidence under each policy. We compared these data-driven policies- optimized using the iPrEx data- to the existing PrEP guidelines in terms of population impact. Using the iPrEx data, we estimated the population impact of policies empirically- without reliance on modelling assumptions.
Mathematical modelling towards cost-effectiveness analysis has been the primary tool for assessing the population impact of PrEP [37–42], but the modelling has not evaluated potential prioritization based on data-driven statistical models of PrEP benefit or of HIV risk. Math-model-based population impact estimates also rely on many assumptions, such as population distributions of demographic characteristics, risk behaviours, and adherence, and on the associations between these factors and PrEP efficacy. Empirical estimates of the impact of PrEP policies, which do not rely on these assumptions, are lacking.
As for any analyses of randomized trial data, our results based on the iPrEx data pertain directly to the population enrolled in the trial, and additional data are needed to inform on the impact of PrEP policies for other populations. Of particular importance is adherence, since data suggest that adherence in iPrEx was considerably lower than in subsequent open-label and observational studies, and in settings where individuals are being provided an intervention they know to be effective [4, 5, 43–50]. Future research will be needed to determine if the impact estimates based on iPrEx generalize to populations with other distributions of adherence, as well as different demographic and risk behavior characteristics. We elaborate on this in the discussion.
Materials and methods
Ethics statement
The iPrEx study [1] was approved by the Committee on Human Research at the University of California, San Francisco, as well as local institutional review boards at each study site: Comité Institucional de Bioética, Asociación Civil Impacta Salud y Educación, Lima, Peru; Universidad San Francisco de Quito, IRB #1, Quito, Ecuador; Fenway Community Health Institutional Review Board, Boston, MA; Comissão de Ética para Análise de Projetos de Pesquisa, CAPPesq Hospital das Clínicas da Faculdade de Medicina da USP, São Paulo, Brazil; Comitê de Ética em Pesquisa, Hospital Universitario Clementino Fraga Filho/Universidade Federal de Rio de Janeiro, Rio de Janeiro, Brazil; Comitê de Ética em Pesquisa do Instituto de Pesquisa Clínica Evandro Chagas, Rio de Janeiro, Brazil; National IRB: Comissão Nacional de Ética em Pesquisa–CONEP, Ministério da Saúde, Brasília, Brazil; University of Cape Town Research Ethics Committee, Cape Town, South Africa; Human Experimentation Committee, Research Institute for Health Sciences, Chiang Mai, Thailand; Ethical Review Committee for Research in Human Subjects, Department of Medical Services, Ministry of Public Health, Nonthaburi, Thailand; Research Ethics Committee, Faculty of Medicine, Chiang Mai University, Chiang Mai, Thailand. Written informed consent was obtained from each participant prior to enrollment in the study.
The iPrEx study
The iPrEx trial was a phase III study of FTC-TDF for HIV prevention; the results of the primary analysis of safety and efficacy were published by Grant et al. [1] Enrolment began in July 2007; participants were followed until November 2010. The trial is registered at ClinicalTrials.gov and the clinical trial number is NCT00458393. The URL is https://clinicaltrials.gov/ct2/show/NCT00458393.
iPrEx enrolled 2499 HIV-uninfected MSM and TGW who were randomized to placebo or oral FTC-TDF once daily and followed for incident HIV infection. A total of 2442 participants were included in our analysis (10 were HIV-infected at enrolment and 47 did not have a follow-up HIV test). At November 21, 2010, median follow-up was 1.66 years (range: 0.07 to 3.30). The estimated efficacy of PrEP was 44% (p = 0.005). Eighty-three incident infections occurred in the placebo arm, yielding an annual HIV incidence of 4.01% (95% confidence interval [CI]: 2.89–5.08%). Forty-eight infections occurred in the FTC–TDF arm (annual HIV incidence = 1.97%, 95% CI: 1.16–2.86%). Thus, PrEP was estimated to yield a 2.04% absolute reduction in the 1-year rate of HIV infection (95% CI: 0.66%-3.55%, p = 0.003), corresponding to a number needed to treat (NNT) of 49 participants treated per HIV infection event prevented. The efficacy of PrEP on the relative risk scale was estimated to be 44% [1]. Sub-optimal adherence among trial participants likely explains the modest efficacy [51].
Interviewer-administered or computer-assisted questionnaires were used to collect demographic and behavioral risk data on all participants at trial screening. Sexual risk-taking behaviours pertain to the prior 3 months; and exchange of sex for money, drugs, or services and self-reported STIs cover the prior 6 months.
Risk and PrEP benefit modelling
We considered participants’ age, gender identity, and self-reported sexual risk behaviours at baseline to predict HIV risk and PrEP benefit. Importantly, while demographic and risk behaviour characteristics are frequently collected in clinical practice, measures of adherence are not available before PrEP is actually provided. Accordingly, measures of adherence to FTC-TDF were not included in our models of HIV risk or PrEP benefit. Categorical demographic/risk behaviour variables with less than two HIV cases per level were excluded to improve model stability.
We used Cox proportional hazards logic regression models [52, 53] to select the individual variables or combinations of variables that best predict risk of HIV infection without PrEP, given data for participants on the placebo arm. We paired the fitted Cox model with a Nelson-Aalen baseline hazard estimate [54] to estimate the cumulative HIV infection rate without PrEP, denoted by Risk0(X), where X is a vector of baseline demographic and behavioral variables. We used the same approach to predict HIV risk under PrEP using data from the FTC-TDF arm, denoted by Risk1(X). We calculated PrEP benefit as the difference in HIV risk without vs. with PrEP, Δ(X) = Risk0(X) − Risk1(X). Cross-validation was used to select the tuning parameters for the logic regression models. To assess model stability, models were re-fit in 500 bootstrap samples. Further details are summarized in supplementary materials, S1 Methods.
PrEP policies
We first considered the policy that maximizes net benefit, which recommends PrEP to individuals with a high expected benefit from PrEP as measured by Δ(X) = Risk0(X)–Risk1(X) [26–32]. The optimal threshold of PrEP benefit above which PrEP is recommended corresponds to the inverse of the threshold number needed to treat–the maximum number of individuals one is willing to treat to prevent one HIV infection [55–57]. We focused primarily on a threshold of 1.2%, after considering the null hypothesis used to design iPrEx and other PrEP efficacy trials [1, 2, 6]. The null hypothesis codifies the design assumptions about the NNT to make PrEP clinically useful. Specifically, a null of 30% PrEP efficacy and 4.0% 1-year HIV incidence in the placebo group implies that 1.2% is the smallest absolute reduction in 1-year HIV incidence due to PrEP that would justify PrEP for HIV prevention. The 1.2% threshold corresponds to an NNT of 83. We also considered the effect of different PrEP benefit thresholds.
The second type of PrEP policy we considered was motivated by current WHO guidelines, which suggest considering PrEP for sub-populations with 3 or more HIV infections per 100 person-years at risk [58]. When there is no modification of the PrEP effect on the relative risk scale, an individual’s level of PrEP benefit, Δ(X) = Risk0(X)–Risk1(X), is proportional to their risk of HIV without PrEP, Risk0(X)–and therefore high-risk individuals have the largest PrEP benefit. However, if this assumption does not hold, due to effect modification on the relative risk scale, a risk-based policy may have less population impact than a PrEP-benefit based policy. We evaluated a risk-based policy, which recommends PrEP to individuals with a 1-year HIV risk of 3% or more, consistent with the WHO guidelines. We compared this policy to the US CDC PrEP guidelines for MSM that recommends PrEP on the basis of 7 demographic and risk factors including number of male partners and condomless intercourse [33] (Table 1), and to the PrEP-benefit based policy defined above. The guidelines are based on a clinical screening index that was developed using data from VAXGEN 004, an HIV vaccine trial among MSM in the US [59, 60], and validated using data from Project Explore, an HIV behavioral intervention trial among US MSM [61].
US CDC recommended indications for use of PrEP among MSM [33] and methods used to determine associated PrEP recommendations for iPrEx trial participants, given baseline demographic and risk behaviour dataa.
Evaluating population impact
We used existing methods to assess the population impact of PrEP policies [62–65]. Each policy was first evaluated by the proportion of individuals recommended PrEP by the policy- namely, the proportion of iPrEx participants with demographic and risk behaviour characteristics that would yield a PrEP recommendation under the policy, estimated by pooling across the two treatment arms. This metric is a proxy for the resource-utilization of the policy. Second, we evaluated the expected cumulative HIV infection rate under the policy empirically: the Kaplan-Meier method [66] was used to estimate the HIV infection rate among iPrEx participants in the PrEP arm who would be recommended PrEP by the policy, and to estimate the HIV rate among iPrEx participants in the placebo arm who would not be recommended PrEP by the policy. The two estimates were combined using a weighted average, where the weights were determined by the proportion of iPrEx participants who would be recommended PrEP by the policy. Empirical estimation of policy impact is appealing in that it does not require modeling assumptions, and it is made possible by the randomized and placebo-controlled nature of the iPrEx design. Specifically, the randomized trial design ensures that the difference in HIV incidence between the PrEP and placebo groups can be attributed to PrEP itself- rather than to differences in risk taking behaviors or exposure to HIV between the groups. Point estimates and bootstrap-based confidence intervals were bias-corrected to account for having used the same data to predict risk/PrEP benefit and to evaluate population impact. See S1 Methods for details.
Results
Univariate associations with HIV infection and PrEP efficacy
Most iPrEx participants [1, 67] were cisgender male (87%) and aged 18–24 (50%) (Table 2). The most frequently reported risk behaviours were insertive or receptive condomless anal intercourse (86%) and more than 5 male sex partners (56%) over the last 3 months. The strongest univariate predictors of increased HIV risk without PrEP were cocaine use over the last month (hazard ratio (HR) 2.58 [95% CI: 1.19–5.62]) and condomless intercourse over the last 3 months (HR 1.23 [95% CI: 0.32–4.62] for insertive only; HR 4.14 [95% CI: 1.28–13.4] for receptive only; 5.11 [95% CI: 1.56–16.74] for receptive and insertive). These variables were also the strongest univariate predictors of increased PrEP efficacy, although, notably, none were statistically significant modifiers of efficacy (Table 2).
Distributions of demographic and risk behavior variables by treatment arm and their univariate associations with HIV infection risk and PrEP efficacy.
Estimated HIV incidence per 100 person-years is reported. The hazard ratio (“risk factor HR”) for each variable quantifies the association between the variable and HIV infection risk, within each treatment arm. The PrEP HR (FTC-TDF vs. Placebo) quantifies the efficacy of PrEP for each level of each variable. The ratio of PrEP HRs quantifies the association between the variable and PrEP efficacy. A Wald test of interaction is reported for each variable.
Model for risk of HIV without PrEP
The best Cox proportional hazards logic regression model for predicting HIV infection risk without PrEP is shown in Table 3. Individuals who report engaging in condomless receptive anal intercourse over the last 3 months, without insertive (HR = 3.59 [95% CI: 1.84–6.98]) or with insertive anal intercourse (HR = 4.43 [95% CI: 2.23–8.81]) were estimated to be at considerably increased risk. As shown in Fig 1A, individuals reporting either behaviour were estimated to have a 1-year HIV infection risk above 3%, and were thus recommended PrEP under the risk-based policy (59.7% of individuals); the remaining 40.3% of individuals were not recommended PrEP under this policy. The risk model itself was reasonably stable across bootstrap samples; the condomless receptive intercourse and condomless receptive and insertive intercourse variables were selected in 342 and 364 of the 500 models fit to bootstrapped datasets, respectively (S1 Fig). More importantly, the risk-based PrEP recommendations were highly stable, with 40% of individuals recommended PrEP in 70% or more bootstrap samples and the other 60% not recommended PrEP in 89% or more samples (S4 Fig).
Risk-based PrEP policy and HIV infection risk by PrEP recommendation.
Flowchart for determining PrEP recommendation for an individual MSM/TGW under the risk-based policy, which is based on a model for HIV infection risk without PrEP fit to the iPrEx data (A). Empirical estimates of the size of each subpopulation and of the 1-year HIV infection risk without PrEP in each subpopulation are also shown. The PrEP-benefit policy developed using the iPrEx data and using a PrEP benefit threshold of 1.2% is identical. Cumulative rate of HIV infection over time, by treatment arm and risk-based PrEP recommendation, with pointwise 95% confidence intervals (B).
The best Cox proportional hazards logic regression models for predicting HIV infection risk without PrEP (fit using placebo arm data) and with PrEP (fit using FTC-TDF arm data).
For each baseline demographic or risk behaviour variable entering in the model, the associated hazard ratio (HR) for HIV infection is shown.
For comparison, we developed risk models using alternative model-building and machine-learning approaches. The best stepwise Cox proportional hazards regression model was identical to that built using Cox logic regression (S1 Table) and had similar population impact; small differences appeared between models in bootstrapped datasets (S2 Table and S2 Fig). Using Cox regression model with lasso, the best-predicting model involved many more variables (S1 Table) but had a similar estimated impact (S2 Table) and was much less stable across bootstrap samples (S3 and S4 Figs).
Model for PrEP benefit
The best Cox proportional hazards logic regression model for predicting HIV infection risk with PrEP is shown in Table 3. Individuals under age 30 (HR 2.78; 95% CI: 1.25–6.21) and who reported condomless receptive and insertive anal intercourse over the last 3 months (HR 1.87; 95% CI: 1.04–3.40) were estimated to be at increased risk with PrEP. By combining this with the model for HIV risk without PrEP, a model for PrEP benefit as a function of age and condomless intercourse was obtained. However, although age predicts some variation in the level of PrEP benefit (S4 Fig), only condomless intercourse determines the PrEP recommendation under the PrEP-benefit-based policy with a benefit threshold of 1.2%: individuals reporting condomless receptive or insertive and receptive anal intercourse are predicted to have at least a 1.2% reduction in 1-year HIV infection risk due to PrEP, and are recommended PrEP under the policy (59.7% of individuals). Importantly, therefore, this PrEP-benefit-based policy recommends PrEP to the same subpopulation as does the risk-based policy.
We explored the use of an alternative PrEP benefit threshold; few thresholds could be examined given that the PrEP benefit model only predicts six levels of PrEP benefit (for three levels for type of condomless intercourse and two levels of age). Using a lower PrEP benefit threshold of 0.7%—corresponding to a 0.7% lower 1-year risk of HIV with PrEP and an NNT of 143—would result in recommending PrEP to individuals who report condomless receptive or insertive and receptive anal intercourse or who are 30 years or older (S4 Fig), an estimated 71% of the iPrEx population.
We found that the PrEP benefit model and associated PrEP-benefit-based PrEP recommendations were less stable across bootstrap samples than their risk-based counterparts (S5 Fig). Alternative modelling approaches did not yield policies with improved performance (S2 Table).
Population impact of PrEP policies
Fig 1B shows the estimated cumulative rates of HIV infection over time by treatment arm, for subpopulations of MSM/TGW who would or would not be recommended PrEP under the risk-based policy. The policy is estimated to achieve a 1.95% 1-year HIV infection rate (95% CI: 1.21%-2.73%), below the 1.97% achieved if PrEP is recommended to all MSM/TGW in the iPrEx population (95% CI: 1.16%-2.86%) (Table 4). Strikingly, the policy would require treating just 59.7% of MSM/TGW (95% CI: 24.9%-100%). The benefit of PrEP in the high-risk subgroup is an absolute 3.31% reduction in 1-year HIV incidence (95% CI: 1.20%-6.12%), corresponding to an NNT of 30 –as opposed to a policy of PrEP for all MSM/TGW which has an NNT of 49.
Estimated impact of risk-based, PrEP benefit-based, and CDC PrEP policies for the MSM/TGW population.
Policies are ordered by the associated proportion of the population that is recommended PrEP. Impact is shown over 1 and 2 years post-enrolment.
Table 4 also shows the estimated population impact of the PrEP-benefit-based policy that uses a PrEP benefit threshold of 1.2%. Since this PrEP-benefit-based policy is identical to the risk-based policy, the estimated impact of the two policies is similar; minor differences between the models occur in some bootstrap samples, with the latter model being more variable. Using a lower PrEP benefit threshold of 0.7% would result in more individuals being recommended PrEP (71.0% vs. 59.7%) and similar HIV infection rates at 1 and 2 years.
The estimated impact of the CDC guideline is shown in Table 4 as well. This guideline is estimated to recommend PrEP to a larger subpopulation of MSM/TGW than the risk-based policy (86.4% vs. 59.7%), and yet it is estimated to achieve a very similar estimated 1-year HIV infection rate (1.97% vs. 1.95%). However, it should be noted that the confidence interval for the proportion of the population to be recommended PrEP under the risk-based policy is wide, and does not rule out the possibility that the policy recommends PrEP to the same-sized subpopulation as the CDC guideline. The confidence intervals for risk- and PrEP-benefit based policies, which are derived using the iPrEx data, are wide because they account for the uncertainty in the risk- and PrEP-benefit models. In contrast, the CDC policy is fixed, having been derived using historical data, and therefore the size of the subpopulation to be recommended PrEP is estimated much more precisely. Separate data will be needed to validate the apparent difference in resource-utilization of the risk- and CDC policies.
Contrasting PrEP policies
Although a PrEP-benefit-based policy has theoretical appeal, the risk-based policy and PrEP-benefit-based policy (1.2% threshold) that we developed using the iPrEx data were found to be identical, and therefore have similar estimated population impact (Table 4). Fig 2 highlights this visually, showing the estimated 1- and 2-year HIV infection rates achieved using the policies and the estimated rate under a policy that recommends PrEP to all. The very similar performance of the risk- and PrEP-benefit-based policies reflects the fact that there are not strong interactions between PrEP and baseline demographic and risk behaviour variables, and suggests that an individual’s risk of HIV without PrEP is all that is needed to identify individuals with high absolute reduction in HIV risk due to PrEP. Coupled with the fact that the risk-based policy is more stable across bootstrap samples, we view the risk-based policy as having greater potential.
Contrasting PrEP policies with a policy that recommends PrEP to all individuals.
Policies are contrasted in terms of the proportion of individuals recommended PrEP by the policy (x-axis) and the estimated 1- and 2-year HIV infection rates under the policy (y-axis). Symbols show the estimated 1- and 2-year infection rates and lines show 95% confidence intervals.
These results do identify an important difference between the risk-based policy optimized using iPrEx data and the CDC guideline. While both policies achieve nearly the same HIV incidence as PrEP for all MSM/TGW, the CDC guideline is estimated to recommend PrEP to a larger subpopulation of MSM/TGW (Fig 2). An estimated 28.9% of individuals would be recommended PrEP by the CDC guideline but not by the risk-based policy, and another 2.2% would not be recommended PrEP by the CDC guideline but would by the risk-based policy (S3 Table). Importantly, the CDC guidelines are based on previous studies of HIV risk factors among US MSM in HIV prevention trials [59–61]. These results suggest that the CDC guidelines may be broader than they need to be to achieve a substantial reduction in HIV incidence.
It may be of interest to compare the HIV incidence achieved under policies that are constrained to use the same resources, i.e. to treat a subpopulation of the same size. However, such policies are difficult to examine with the risk and PrEP benefit models fit to the iPrEx data; the fitted risk model takes only three levels and the PrEP benefit model takes six levels and therefore the size of the subpopulations treated cannot be controlled with precision. In particular, employing anything lower than the 3% high risk threshold we used would mean PrEP is recommended to the entire MSM/TGW population. Using a lower PrEP benefit threshold of 0.7% would result in a PrEP-benefit-based policy that recommends PrEP to a similar fraction of the population as does the CDC guideline (71% vs. 86%), and the estimated HIV incidences under these two policies are highly similar (Table 3).
Point estimates suggest that all of these PrEP policies may have declining impact over time (Fig 3), especially the CDC guideline. This result is somewhat expected, given that the predictive capacity of the baseline risk behaviour variables may diminish with time.
HIV infection risk over time under risk-based, PrEP-benefit based, and CDC PrEP policies.
Cumulative rate of HIV infection over time with pointwise 95% confidence intervals. The PrEP-benefit-based policy uses a PrEP benefit threshold of 1.2%.
Population impact under higher adherence
Data suggest that adherence to PrEP may be higher in "real world" contexts, where individuals know that PrEP is effective and that they are in fact receiving it, as opposed to being blinded to PrEP vs. placebo receipt, as in the iPrEx study [4, 5, 43–50]. In addition, many analyses have shown that PrEP efficacy is strongly associated with adherence [51, 68–70]. Therefore, it is of interest to determine whether the impact of the PrEP policies we examine would differ in settings with higher adherence. We conducted a simple sensitivity analysis to address this question. Specifically, we examined scenarios where we assumed that the relative risk associated with PrEP was reduced by a factor of 1.0 to 0.1, due to improved adherence relative to that seen in the iPrEx study. This corresponds to varying the overall PrEP relative-risk from 0.56 (the observed relative risk) to 0.06. A key limitation of this sensitivity analysis is that there are no data we know of to inform on whether the same decrease in PrEP relative risk would apply equally to all subgroups of the MSM/TGW population, or whether some subgroups would have greater decreases in PrEP relative risk than others due to better adherence. Because neither study-level meta-analyses associating efficacy with adherence [69, 70] nor analyses of efficacy among adherers in individual trials [51, 68] inform on this, for simplicity we assume that the same multiplicative decrease in PrEP relative risk applies to the iPrEx population at large, as well as to the high risk subgroup identified by our risk-based PrEP policy and the high risk subgroup identified by the CDC policy.
Fig 4 shows the results of this sensitivity analysis. We make two observations. First, as expected, as the PrEP relative risk decreases, the HIV infection rate achieved under all policies decreases. Second, as the PrEP relative risk decreases, the PrEP for all policy has a more rapid decline in HIV infection rate than do the risk-based and CDC policies. This is because the latter two policies recommend PrEP to just 59.7% and 86.4% of the MSM/TGW population, respectively, and so the reduction in HIV due to PrEP only affects these subpopulations. Note that the size of the subpopulations recommended PrEP does not change across the scenarios examined here. These results suggest that risk-based policies may have less appeal in settings with higher adherence. We caution, however, that these results are a direct consequence of our assumption that the multiplicative reduction in PrEP relative risk is the same across all subpopulations. A more comprehensive modeling approach- if informed by data on how efficacy changes as a function of adherence in different subgroups of the population- could more effectively compare the impact of different PrEP policies while allowing for different patterns of adherence.
Sensitivity analysis: HIV infection rate under PrEP for all, risk-based, and CDC PrEP policies, with varying PrEP relative risk.
Cumulative 1- and 2-year HIV infection rates under each policy, as a function of the multiplicative reduction in PrEP relative risk due to increasing adherence. An 0.9 multiplicative reduction in PrEP relative risk reduces the relative risk from 0.56 to 0.50. Pointwise 95% confidence intervals are shown with shading.
Discussion
We analysed data from a landmark multi-national PrEP efficacy study in MSM/TGW to identify subpopulations predicted to be at high HIV risk without PrEP and subpopulations with high expected PrEP benefit. Based on these models, we defined risk-based and PrEP-benefit based policies for prioritizing PrEP, and evaluated and compared the policies empirically, in terms of the size of the subpopulation recommended PrEP under each policy and the expected HIV incidence under each policy. We found the risk- and PrEP-benefit-based policies to have similar estimated impact in the MSM/TGW population in iPrEx, consistent with our analyses and prior work suggesting that the PrEP effect was relatively constant on the relative risk scale, i.e. there was no strong effect modification [1, 67]. We compared the risk-based policy derived using the iPrEx data to the CDC PrEP guideline for MSM, and estimated that it would prioritize PrEP to a smaller subpopulation while achieving a similar reduction in HIV incidence. Risk-based prioritization of PrEP appears to be a resource-efficient strategy for resource-limited settings, achieving nearly the same reduction in HIV incidence as does rolling out PrEP for all MSM/TGW.
Critically, our results pertain directly only to the MSM/TGW population from which iPrEx participants were recruited. The demographic and risk behaviours that best predict HIV risk may differ in other populations. The impact of the iPrEx-derived risk-based policy may not generalize to other populations, either because the distribution of demographic and risk characteristics differs, or because the level of PrEP efficacy differs. For example, recent studies of Black American MSM and young MSM have found HIV incidence exceeding the iPrEX rates [71, 72]. In the PROUD open-label PrEP study [5], PrEP efficacy was estimated at 86%, much higher than in iPrEx. As illustrated by our sensitivity analysis, in settings where larger subpopulations are high risk and prioritized for PrEP, or where PrEP efficacy is higher, we may expect to see smaller resource savings of a risk-based PrEP policy as compared to a policy of PrEP for all.
Given that the iPrEx study was an individually-randomized trial, these results only characterise the impact of PrEP policies attributable to the direct effect of PrEP (as opposed to the total effect [73]). The duration of iPrEx follow-up also only permits estimation of impact over 1–3 years of follow-up. The reliability of the risk behaviour variables may also differ in iPrEx as opposed to more routine clinical settings [74–76].
The risk-based PrEP policy optimized using iPrEx data would recommend PrEP to MSM/TGW who report engaging in condomless receptive anal intercourse, or condomless receptive and insertive anal intercourse. However, a meaningful benefit of PrEP cannot be ruled out for MSM/TGW who engage in exclusively insertive anal intercourse. For example, there may be individual factors, such as an HIV-infected partner who is not virally suppressed, that would clearly lend themselves to a recommendation for PrEP. Providers must base their prescribing practices on individual- rather than population-level impact.
Mathematical modelling is and will continue to be essential for PrEP policy research. Using mathematical models allows researchers to study and isolate the influence of factors such PrEP uptake and adherence on population impact. Modeling can also integrate multiple sources of data, e.g. population distributions of demographic and risk behaviours, as opposed to distributions among individuals eligible for and willing to enrol in clinical trials. Modeling can capture both direct and indirect effects of PrEP, examine impact over longer time periods, and formally incorporate assumptions about the cost of providing PrEP. However, model-based estimates of PrEP impact are only as reliable as their data inputs and underlying assumptions. Mathematical models of PrEP impact typically assume the existence of subpopulations with different behaviors and levels of HIV risk, that PrEP reduces risk by a factor that is constant across risk groups, and that adherence increases PrEP efficacy by a constant amount across risk groups. We posit that PrEP efficacy trials, which have limited generalizability but which enable population impact to be estimated directly using observed data, can highlight policies for further investigation and provide preliminary estimates of population impact, thus complementing the modelling and contributing to policy discussions.
Buchbinder and colleagues [67] previously analysed the iPrEx trial data to assess the baseline demographic and risk behaviour variables individually for their ability to predict HIV infection risk without PrEP (in the placebo arm), and the population attributable fraction and NNT were calculated for risk behaviour subgroups. Two variables, condomless insertive or receptive anal intercourse, and condomless receptive anal intercourse with a partner of unknown HIV serostatus, were identified as being most important for prioritizing PrEP rollout. Our analyses went further to build multivariate models to predict not only HIV infection risk without PrEP, but also to model PrEP benefit as a function of demographic and risk behavior variables. The first variable identified by [67], but not the second, was selected into our multivariate risk- and PrEP-benefit models, and forms the basis for our associated risk-based PrEP policy. We also evaluated PrEP policies based on our multivariate risk- and PrEP-benefit models, using measures that directly characterize the population impact of the policies: the proportion of the population recommended PrEP, and the reduction in HIV incidence under the policy.
Zheng et al. [77] recently put forth statistical methods for developing PrEP policies for resource-limited settings, based on criteria for maximizing the proportion of would-be HIV-infected subjects absent PrEP who are identified and recommended PrEP (i.e. sensitivity) subject to a cost constraint (fraction of population treated), or based on minimizing cost subject to a fixed sensitivity. Policies were evaluated in terms of sensitivity and the number needed to test to detect one HIV infection, using survey data from Eastern Uganda. Instead, given randomized trial data, we evaluate policies in terms of their impact on HIV incidence. Furthermore, the risk- and benefit-based policies we consider are grounded in decision theory and are designed to maximize the net benefit of a policy.
Conclusions
We conclude that risk-based policies that prioritize PrEP for MSM/TGW subpopulations at highest risk of HIV without PrEP are worth further investigation for resource-limited settings. Risk-based policies are easy to understand and interpret and we did not find greater impact of policies that prioritize based on expected PrEP benefit. The existing CDC guideline, which requires measurement of 7 demographic and risk factors including number of male partners and condomless intercourse, or our more parsimonious risk model that is based only on condomless intercourse, could be the focus of future policy research for the MSM and TGW population. Our statistical approach could be used to explore and evaluate PrEP policies for other populations.
Supporting information
S1 Methods [docx]
Supplementary methods.
S1 Table [hr]
Cox proportional hazards regression models, selected using stepwise model selection using the Lasso penalty, for predicting HIV infection risk without PrEP (fit using placebo arm data) and with PrEP (fit using FTC-TDF arm data).
S2 Table [docx]
Estimated population impact of risk-based and PrEP-efficacy-based PrEP policies, over 1 year.
S3 Table [docx]
Comparison of PrEP recommendations for risk-based PrEP policy and US CDC PrEP guideline.
S1 Fig [docx]
Variable importance summary for Cox proportional hazards logic regression models.
S2 Fig [docx]
Variable importance summary for Cox proportional hazards regression stepwise models.
S3 Fig [docx]
Variable importance summary for Cox proportional hazards regression with lasso models.
S4 Fig [docx]
Flowchart for determining PrEP recommendation for an individual MSM/TGW under the PrEP-benefit-based policy, which is based on a model for PrEP benefit fit to the iPrEx data.
S5 Fig [docx]
Distribution of the proportion of times each individual is recommended PrEP across 500 bootstrap datasets, for policies of different types (risk- and PrEP-benefit based policies built using different modelling approaches).
Zdroje
1. Grant RM, Lama JR, Anderson PL, McMahan V, Liu AY, Vargas L, et al. Preexposure chemoprophylaxis for HIV prevention in men who have sex with men. New England Journal of Medicine. 2010;363(27):2587–99. doi: 10.1056/NEJMoa1011205 21091279
2. Baeten JM, Donnell D, Ndase P, Mugo NR, Campbell JD, Wangisi J, et al. Antiretroviral prophylaxis for HIV prevention in heterosexual men and women. N Engl J Med. 2012;367(5):399–410. doi: 10.1056/NEJMoa1108524 22784037
3. Thigpen MC, Kebaabetswe PM, Paxton LA, Smith DK, Rose CE, Segolodi TM, et al. Antiretroviral preexposure prophylaxis for heterosexual HIV transmission in Botswana. N Engl J Med. 2012;367(5):423–34. doi: 10.1056/NEJMoa1110711 22784038
4. Molina J, Capitant C, Charreau I, Meyer L, Spire B, Pialoux G, et al. On demand PrEP with oral TDF-FTC in MSM: Results of the ANRS Ipergay trial. CROI, Seattle, WA. 2015;Abstract 23LB.
5. McCormack S, Dunn DT, Desai M, Dolling DI, Gafos M, Gilson R, et al. Pre-exposure prophylaxis to prevent the acquisition of HIV-1 infection (PROUD): effectiveness results from the pilot phase of a pragmatic open-label randomised trial. Lancet. 2016;387(10013):53–60. doi: 10.1016/S0140-6736(15)00056-2 26364263
6. Van Damme L, Corneli A, Ahmed K, Agot K, Lombaard J, Kapiga S, et al. Preexposure prophylaxis for HIV infection among African women. N Engl J Med. 2012;367(5):411–22. doi: 10.1056/NEJMoa1202614 22784040
7. Marrazzo JM, Ramjee G, Richardson BA, Gomez K, Mgodi N, Nair G, et al. Tenofovir-based preexposure prophylaxis for HIV infection among African women. N Engl J Med. 2015;372(6):509–18. doi: 10.1056/NEJMoa1402269 25651245
8. Kashuba AD, Patterson KB, Dumond JB, Cohen MS. Pre-exposure prophylaxis for HIV prevention: how to predict success. Lancet. 2012;379(9835):2409–11. doi: 10.1016/S0140-6736(11)61852-7 22153566
9. van der Straten A, Van Damme L, Haberer JE, Bangsberg DR. Unraveling the divergent results of pre-exposure prophylaxis trials for HIV prevention. AIDS. 2012;26(7):F13–9. doi: 10.1097/QAD.0b013e3283522272 22333749
10. Haberer JE, Baeten JM, Campbell J, Wangisi J, Katabira E, Ronald A, et al. Adherence to antiretroviral prophylaxis for HIV prevention: a substudy cohort within a clinical trial of serodiscordant couples in East Africa. PLoS Med. 2013;10(9):e1001511. doi: 10.1371/journal.pmed.1001511 24058300
11. Burgener A, Klatt N. Uncovering the role of the vaginal microbome in undermining PrEP efficacy in women. 21st International AIDS Conference; July 18–22, 2016; Durban, South Africa2016.
12. Williams BL, Lipkin I. Role of vaginal microciota in genital inflammation and enhancing HIV acquisition in women. 21st International AIDS Conference; July 18–21, 2016; Durban, South Africa2016.
13. Naranbhai V, Abdool Karim SS, Altfeld M, Samsunder N, Durgiah R, Sibeko S, et al. Innate immune activation enhances hiv acquisition in women, diminishing the effectiveness of tenofovir microbicide gel. J Infect Dis. 2012;206(7):993–1001. doi: 10.1093/infdis/jis465 22829639
14. Thomson KA, Baeten JM, Mugo NR, Bekker LG, Celum CL, Heffron R. Tenofovir-based oral preexposure prophylaxis prevents HIV infection among women. Curr Opin HIV AIDS. 2016;11(1):18–26. doi: 10.1097/COH.0000000000000207 26417954
15. Klatt NR, Cheu R, Birse K, Zevin AS, Perner M, Noel-Romas L, et al. Vaginal bacteria modify HIV tenofovir microbicide efficacy in African women. Science 2017;356:938–45. doi: 10.1126/science.aai9383 28572388
16. Patterson KB, Prince HA, Kraft E, Jenkins AJ, Shaheen NJ, Rooney JF, et al. Penetration of tenofovir and emtricitabine in mucosal tissues: implications for prevention of HIV-1 transmission. Sci Transl Med. 2011;3(112):112re4. doi: 10.1126/scitranslmed.3003174 22158861
17. Garrett KL, Cottrell ML, Prince HM, Sykes C, Schauer A, Peery A, et al. Concentrations of TFV and TFVdp in Female Mucosal Tissues After a Single Dose of TAF. CROI 2016; Feb 22–25; Boston2016.
18. Janes H, Corey L, Ramjee G, Carpp LN, Lombard C, Cohen MS, et al. Weighing the Evidence of Efficacy of Oral PrEP for HIV Prevention in Women in Southern Africa. AIDS Res Hum Retroviruses. 2018;34(8):645–56. doi: 10.1089/AID.2018.0031 29732896
19. endinghiv.org.au. Truvada Licensed for PrEP: ACON; 2016 [updated May 10]. Available from: http://endinghiv.org.au/nsw/truvada-licensed-for-prep/.
20. Dorresteijn JAN, Visseren FLJ, Ridker PM, Wassink AMJ, Steyerberg EW, van der Graaf Y, et al. Estimating treatment effects for individual patients based on the results of randomised clinical trials. British Medical Journal. 2011;343:1–13.
21. Kovalchik SA, Tammemagi M, DBerg CD, Caporaso NE, Riley TL, Korch M, et al. Targeting of low-dose CT screening according to the risk of lung-cancer death. New England Journal of Medicine. 2013;369:245–54. doi: 10.1056/NEJMoa1301851 23863051
22. Benchikh A, Savage C, Cronin A, Salama G, Villers A, Lilja H, et al. A panel of kallikrein markers can predict outcome of prostate biopsy following clinical work-up: an independent validation study from the European Randomized Study of Prostate Cancer screening, France. BMC Cancer. 2010;10:635. doi: 10.1186/1471-2407-10-635 21092177
23. Den RB, Yousefi K, Trabulsi EJ, Abdollah F, Choeurng V, Feng FY, et al. Genomic classifier identifies men with adverse pathology after radical prostatectomy who benefit from adjuvant radiation therapy. J Clin Oncol. 2015;33(8):944–51. doi: 10.1200/JCO.2014.59.0026 25667284
24. Thanassoulis G, Williams K, Altobelli KK, Pencina MJ, Cannon CP, Sniderman AD. Individualized Statin Benefit for Determining Statin Eligibility in the Primary Prevention of Cardiovascular Disease. Circulation. 2016;133(16):1574–81. doi: 10.1161/CIRCULATIONAHA.115.018383 26945047
25. Pletcher MJ, Pignone M, Jarmul JA, Moran AE, Vittinghoff E, Newman T. Population Impact & Efficiency of Benefit-Targeted Versus Risk-Targeted Statin Prescribing for Primary Prevention of Cardiovascular Disease. J Am Heart Assoc. 2017;6(2).
26. Pauker SG, Kassirer JP. Clinical Application of Decision-Analysis—Detailed Illustration. Semin Nucl Med. 1978;8(4):324–35. 754287
27. Vickers AJ, Elkin EB. Decision curve analysis: A novel method for evaluating prediction models. Med Decis Making. 2006;26(6):565–74. doi: 10.1177/0272989X06295361 17099194
28. Janes H, Pepe MS, Huang Y. A framework for evaluating markers used to select patient treatment. Med Decis Making. 2014;34(2):159–67. doi: 10.1177/0272989X13493147 23811760
29. Vickers AJ, Kattan MW, Daniel S. Method for evaluating prediction models that apply the results of randomized trials to individual patients. Trials. 2007;8.
30. Pauker SG, Kassirer JP. Therapeutic Decision-Making—Cost-Benefit Analysis. New England Journal of Medicine. 1975;293(5):229–34. doi: 10.1056/NEJM197507312930505 1143303
31. Hunink MM, Weinstein MC, Wittenberg E, Drummond MF, Pliskin JS, Wong JB, et al. Decision making in health and medicine: integrating evidence and valuesCambridge University Press; 2014.
32. Kerr KF, Brown MD, Zhu K, Janes H. Assessing the Clinical Impact of Risk Prediction Models With Decision Curves: Guidance for Correct Interpretation and Appropriate Use. J Clin Oncol. 2016;34(21):2534–40. doi: 10.1200/JCO.2015.65.5654 27247223
33. US Public Health Service. Preexposure prophylaxis for the prevention of HIV infection in the United States: A Clinical Practice Guideline. 2014.
34. World Health Organization. Consolidated guidelines on HIV prevention, diagnosis, treatment and care for key populations 2014 [updated July]. Available from: http://www.who.int/hiv/pub/guidelines/keypopulations/en/.
35. Vickers AJ, Bennette C, Kibel AS, Black A, Izmirlian G, Stephenson AJ, et al. Who should be included in a clinical trial of screening for bladder cancer?: a decision analysis of data from the Prostate, Lung, Colorectal and Ovarian Cancer Screening Trial. Cancer. 2013;119(1):143–9. doi: 10.1002/cncr.27692 22736219
36. Vickers AJ, Kramer BS, Baker SG. Selecting patients for randomized trials: a systematic approach based on risk group. Trials. 2006;7:30. doi: 10.1186/1745-6215-7-30 17022818
37. Schackman BR, Eggman AA. Cost-effectiveness of pre-exposure prophylaxis for HIV: a review. Curr Opin HIV AIDS. 2012;7(6):587–92. doi: 10.1097/COH.0b013e3283582c8b 23076124
38. Gomez GB, Borquez A, Case KK, Wheelock A, Vassall A, Hankins C. The cost and impact of scaling up pre-exposure prophylaxis for HIV prevention: a systematic review of cost-effectiveness modelling studies. PLoS Med. 2013;10(3):e1001401. doi: 10.1371/journal.pmed.1001401 23554579
39. Carnegie NB, Goodreau SM, Liu A, Vittinghoff E, Sanchez J, Lama JR, et al. Targeting pre-exposure prophylaxis among men who have sex with men in the United States and Peru: partnership types, contact rates, and sexual role. J Acquir Immune Defic Syndr. 2015;69(1):119–25. doi: 10.1097/QAI.0000000000000555 25942463
40. Chen A, Dowdy DW. Clinical effectiveness and cost-effectiveness of HIV pre-exposure prophylaxis in men who have sex with men: risk calculators for real-world decision-making. PLoS One. 2014;9(10):e108742. doi: 10.1371/journal.pone.0108742 25285793
41. Kessler J, Myers JE, Nucifora KA, Mensah N, Toohey C, Khademi A, et al. Evaluating the impact of prioritization of antiretroviral pre-exposure prophylaxis in New York City. AIDS. 2014.
42. Nichols BE, Boucher CAB, van der Valk M, Rijnders BJA, van de Vijver D. Cost-effectiveness analysis of pre-exposure prophylaxis for HIV-1 prevention in the Netherlands: a mathematical modelling study. Lancet Infect Dis. 2016;16(12):1423–9. doi: 10.1016/S1473-3099(16)30311-5 27665989
43. Grant RM, Anderson PL, McMahan V, Liu A, Amico KR, Mehrotra M, et al. Uptake of pre-exposure prophylaxis, sexual practices, and HIV incidence in men and transgender women who have sex with men: a cohort study. Lancet Infect Dis. 2014;14(9):820–9. doi: 10.1016/S1473-3099(14)70847-3 25065857
44. Gibson S, Grant R, Hall C, Sachs M, Gagliano J, Freeborn K, et al. San Francisco AIDS Foundation Launches PrEP Health Program in Community-Based Sexual Health Center. National HIV Prevention Conference. Vancouver, Canada: US CDC; 2015. p. 229–30.
45. Liu AY, Cohen SE, Vittinghoff E, Anderson PL, Doblecki-Lewis S, Bacon O, et al. Preexposure Prophylaxis for HIV Infection Integrated With Municipal- and Community-Based Sexual Health Services. JAMA Intern Med. 2016;176(1):75–84. doi: 10.1001/jamainternmed.2015.4683 26571482
46. Glidden DV, Amico KR, Liu AY, Hosek SG, Anderson PL, Buchbinder SP, et al. Symptoms, Side Effects and Adherence in the iPrEx Open-Label Extension. Clin Infect Dis. 2016;62(9):1172–7. doi: 10.1093/cid/ciw022 26797207
47. Cohen S, Vittinghoff E, Anderson P, Doblecki-Lewis S, Bacon O, Chege W, editors. Implementation of PrEP in STD and community health clinics in the US: high uptake and drug concentrations among MSM in the demo project. Available from http://www.iapac.org/AdherenceConference/presentations/ADH9OA377.pdf. 9th International Conference on HIV Treatment and Prevention; 2014; Miami, Florida.
48. Cohen S, Vittinghoff E, Anderson P, Doblecki-Lewis S, Bacon O, Chege W, editors. Implementation of PrEP in STD clinics: high uptake and drug detection among MSM in the demonstration project. http://www.croiconference.org/sessions/implementation-prep-std-clinics-high-uptake-and-drug-detectionamong-msm-demo-project. 21st Conference on Retroviruses and Opportunistic Infections; 2014; Boston, MA.
49. Hoagland B, Moreira RI, De Boni RB, Kallas EG, Madruga JV, Vasconcelos R, et al. High pre-exposure prophylaxis uptake and early adherence among men who have sex with men and transgender women at risk for HIV Infection: the PrEP Brasil demonstration project. J Int AIDS Soc. 2017;20(1):21472. doi: 10.7448/IAS.20.1.21472 28418232
50. Hosek SG, Rudy B, Landovitz R, Kapogiannis B, Siberry G, Rutledge B, et al. An HIV Preexposure Prophylaxis Demonstration Project and Safety Study for Young MSM. J Acquir Immune Defic Syndr. 2017;74(1):21–9. doi: 10.1097/QAI.0000000000001179 27632233
51. Anderson PL, Glidden DV, Liu A, Buchbinder S, Lama JR, Guanira JV, et al. Emtricitabine-tenofovir concentrations and pre-exposure prophylaxis efficacy in men who have sex with men. Sci Transl Med. 2012;4(151):151ra25.
52. Ruczinski I, Kooperberg C, LeBlanc M. Logic Regression. Journal of Computational and Graphical Statistics. 2003;12(3):475–511.
53. Kooperberg C, Ruczinski I. Identifying interacting SNPs using Monte Carlo logic regression. Genet Epidemiol. 2005;28(2):157–70. doi: 10.1002/gepi.20042 15532037
54. Nelson W. Theory and applications of hazard plotting for censored failure data. Technometrics. 1972;14:945–65.
55. Guyatt GH, Sackett DL, Sinclair JC, Hayward R, Cook DJ, Cook RJ. Users' guides to the medical literature. IX. A method for grading health care recommendations. Evidence-Based Medicine Working Group. JAMA. 1995;274(22):1800–4. doi: 10.1001/jama.274.22.1800 7500513
56. Sinclair JC, Cook RJ, Guyatt GH, Pauker SG, Cook DJ. When should an effective treatment be used? Derivation of the threshold number needed to treat and the minimum event rate for treatment. J Clin Epidemiol. 2001;54(3):253–62. doi: 10.1016/s0895-4356(01)00347-x 11223323
57. Vickers AJ, Cronin AM, Kattan MW, Gonen M, Scardino PT, Milowsky MI, et al. Clinical benefits of a multivariate prediction model for bladder cancer: a decision analytic approach. Cancer. 2009;115(23):5460–9. doi: 10.1002/cncr.24615 19823979
58. World Health Organization. Guideline on when to start antiretroviral therapy and on pre-exposure prophylaxis for HIV 2015 [updated [updated September]; cited 2015]. Available from: http://www.who.int/hiv/pub/guidelines/earlyrelease-arv/en/.
59. Flynn NM, Forthal DN, Harro CD, Judson FN, Mayer KH, Para MF, et al. Placebo-controlled phase 3 trial of a recombinant glycoprotein 120 vaccine to prevent HIV-1 infection. J Infect Dis. 2005;191(5):654–65. doi: 10.1086/428404 15688278
60. Bartholow BN, Buchbinder S, Celum C, Goli V, Koblin B, Para M, et al. HIV sexual risk behavior over 36 months of follow-up in the world's first HIV vaccine efficacy trial. J Acquir Immune Defic Syndr. 2005;39(1):90–101. doi: 10.1097/01.qai.0000143600.41363.78 15851919
61. Koblin B, Chesney M, Coates T, Mayer K, Agredano F, Aguilu E, et al. Effects of a behavioural intervention to reduce acquisition of HIV infection among men who have sex with men: the EXPLORE randomised controlled study. Lancet. 2004;364(9428):41–50. doi: 10.1016/S0140-6736(04)16588-4 15234855
62. Song X, Pepe MS. Evaluating markers for selecting a patient's treatment. Biometrics. 2004;60(4):874–83. doi: 10.1111/j.0006-341X.2004.00242.x 15606407
63. Janes H, Pepe MS, Bossuyt PM, Barlow WE. Measuring the performance of markers for guiding treatment decisions. Ann Intern Med. 2011;154(4):253–9. doi: 10.7326/0003-4819-154-4-201102150-00006 21320940
64. Gunter L, Zhu J, Murphy S. Variable Selection for Optimal Decision Making. Artificial Intelligence in Medicine. Lecture Notes in Computer Science. 45942007. p. 149–54.
65. Janes H, Brown MD, Huang Y, Pepe MS. An approach to evaluating and comparing biomarkers for patient treatment selection. Int J Biostat. 2014;10(1):99–121. doi: 10.1515/ijb-2012-0052 24695044
66. Kaplan EL, Meier P. Nonparametric Estimation from Incomplete Observations. Journal of the American Statistical Association. 1958;53(282):457–81.
67. Buchbinder SP, Glidden DV, Liu AY, McMahan V, Guanira JV, Mayer KH, et al. HIV pre-exposure prophylaxis in men who have sex with men and transgender women: a secondary analysis of a phase 3 randomised controlled efficacy trial. Lancet Infect Dis. 2014;14(6):468–75. doi: 10.1016/S1473-3099(14)70025-8 24613084
68. Murnane PM, Brown ER, Donnell D, Coley RY, Mugo N, Mujugira A, et al. Estimating efficacy in a randomized trial with product nonadherence: application of multiple methods to a trial of preexposure prophylaxis for HIV prevention. Am J Epidemiol. 2015;182(10):848–56. doi: 10.1093/aje/kwv202 26487343
69. Hanscom B, Janes HE, Guarino PD, Huang Y, Brown ER, Chen YQ, et al. Brief Report: Preventing HIV-1 Infection in Women Using Oral Preexposure Prophylaxis: A Meta-analysis of Current Evidence. J Acquir Immune Defic Syndr. 2016;73(5):606–8. doi: 10.1097/QAI.0000000000001160 27846073
70. Fonner VA, Dalglish SL, Kennedy CE, Baggaley R, O'Reilly KR, Koechlin FM, et al. Effectiveness and safety of oral HIV preexposure prophylaxis for all populations. AIDS. 2016;30(12):1973–83. doi: 10.1097/QAD.0000000000001145 27149090
71. Hosek S, Rudy B, Landovitz R, Kapogiannis B, Siberry G, Rutledge B, et al. An HIV pre-exposure prophylaxis (PrEP) demonstration project and safety study for young MSM. J Acquir Immune Defic Syndr. 2016;74(1):21–9.
72. Koblin BA, Mayer K, Eshelman SH, Wang L, Mannheimer S, del Rio C, et al. Correlates of HIV acquisition in a cohort of black men who have sex with men in the United States: HIV Prevention Trials Network (HPTN) 061. PLoS ONE. 2013;8(7):e70413. doi: 10.1371/journal.pone.0070413 23922989
73. Halloran ME, Longini J, I. M., Struchiner CJ. Design and Analysis of Vaccine StudiesSpringer; 2010.
74. McAuliffe TL, DiFranceisco W, Reed BR. Effects of question format and collection mode on the accuracy of retrospective surveys of health risk behavior: a comparison with daily sexual activity diaries. Health Psychol. 2007;26(1):60–7. doi: 10.1037/0278-6133.26.1.60 17209698
75. Schroder KE, Carey MP, Vanable PA. Methodological challenges in research on sexual risk behavior: I. Item content, scaling, and data analytical options. Ann Behav Med. 2003;26(2):76–103. doi: 10.1207/s15324796abm2602_02 14534027
76. Mirzaei M, Ahmadi K, Saadat SH, Ramezani MA. Instruments of High Risk Sexual Behavior Assessment: A Systematic Review. Mater Sociomed. 2016;28(1):46–50. doi: 10.5455/msm.2016.28.46-50 27047267
77. Zheng W, Balzer L, van der Laan M, Petersen M, Collaboration S. Constrained binary classification using ensemble learning: an application to cost-efficient targeted PrEP strategies. Stat Med. 2018;37(2):261–79. doi: 10.1002/sim.7296 28384841
Článek vyšel v časopise
PLOS One
2019 Číslo 9
- Mohou být tuzemská klíšťata přenašeči nebezpečného syndromu alfa-gal?
- Jaká je budoucnost xenotransplantací? Prasečí játra i ledviny poprvé transplantovány lidem
- Orální lichen planus v kostce: Jak v praxi na toto multifaktoriální onemocnění s různorodými symptomy?
- Metamizol jako analgetikum první volby: kdy, pro koho, jak a proč?
- Esenciální fosfolipidy u nealkoholového postižení jater
Nejčtenější v tomto čísle
- Graviola (Annona muricata) attenuates behavioural alterations and testicular oxidative stress induced by streptozotocin in diabetic rats
- CH(II), a cerebroprotein hydrolysate, exhibits potential neuro-protective effect on Alzheimer’s disease
- Comparison between Aptima Assays (Hologic) and the Allplex STI Essential Assay (Seegene) for the diagnosis of Sexually transmitted infections
- Assessment of glucose-6-phosphate dehydrogenase activity using CareStart G6PD rapid diagnostic test and associated genetic variants in Plasmodium vivax malaria endemic setting in Mauritania