Objectives Pre-exposure prophylaxis (PrEP) is a highly effective method of HIV prevention for men who have sex with men (MSM). However, uncertainty remains around the optimal eligibility criteria for PrEP, specifically whether there are subgroups at low risk of HIV for whom PrEP might not be warranted.
Methods PROUD was an open-label waitlist trial design that randomised MSM attending participating sexual health centres in England to receive PrEP immediately (IMM) or after a deferral period of 1 year (DEF). This analysis is based on participants who were randomised to the deferred arm, when they did not have access to PrEP. HIV incidence was compared between subgroups defined by baseline characteristics.
Results Overall, 21 participants acquired HIV infection over 239.3 person-years (PY) follow-up, yielding an incidence rate of 8.8/100 PY (95% CI 5.4 to 13.4). Two highly significant predictors for HIV acquisition were identified. Men with a self-reported diagnosis of syphilis, rectal chlamydia (CT) or rectal gonorrhoea (GC) in the previous 12 months had an incidence of 17.2/100 PY (95% CI 9.7 to 28.5); those reporting receptive anal intercourse without a condom (ncRAI) with two or more partners in the previous 3 months had an incidence of 13.6/100 PY (95% CI 7.9 to 21.7). The incidence rate among participants lacking both of these risk factors was 1.1/100 PY (1/87.6, 95% CI 0.03 to 6.4).
Conclusions The high HIV incidence in PROUD suggests that most participants appropriately judged their need for PrEP. Eligibility criteria for a PrEP programme can therefore be broad, as in the current guidelines. However, a recent history of syphilis or rectal CT/GC, or multiple ncRAI partners indicates a high imminent risk of HIV infection. MSM with any of these characteristics should be offered PrEP as a matter of urgency.
- eligibility criteria
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Oral pre-exposure prophylaxis (PrEP) has been shown to be a highly effective method of HIV prevention for men who have sex with men (MSM).1–3 At a population level, this effect is mediated both through the direct avoidance of infections among individuals who take PrEP and the indirect prevention of infections that would have occurred subsequently in the transmission chain.4 In the UK, new HIV diagnoses among MSM remained stable for over a decade but have declined in the last 2 years, likely mainly as a result of the combination of PrEP, an increase in HIV testing and routine rapid treatment after diagnosis.5 6
An important issue in PrEP roll-out programmes is participant eligibility since cost-effectiveness is critically dependent on the HIV incidence in the target population. From a clinical perspective the risk:benefit ratio of PrEP may be disadvantageous in individuals at negligible risk of HIV infection, for example, those in a monogamous serodifferent relationship whose partner is virologically suppressed on treatment. WHO guidelines recommend PrEP in populations with an annual incidence greater than 3%.7 However, individual risk of acquiring HIV infection is highly heterogeneous and implementation of this recommendation is not straightforward. Several organisations have issued PrEP guidelines, which include eligibility criteria for MSM.8–10 The central criterion in all guidelines is reported anal intercourse without a condom, although with no explicit reference to the number of partners. Other criteria include the use of postexposure prophylaxis (PEP), a recent diagnosis with a bacterial STI and a history of sexualised drug use.
PROUD was an open-label trial that randomised MSM attending participating sexual health centres in the England to receive PrEP immediately or after a deferral period of 1 year (waitlist design).2 11 A key finding from the trial was the unexpectedly high HIV incidence during the deferral period (9 per 100 person-years [PY]). Here we present an analysis of baseline risk factors for the acquisition of HIV among men randomised to the deferred group before they had access to PrEP. The objective of this analysis was to examine the relative importance of the recommended eligibility criteria for a future PrEP programme, identify any other risk factors and explore whether there are subgroups at low risk of HIV for whom PrEP might not be warranted. The results should inform eligibility criteria for MSM in the UK and similar populations elsewhere in Europe.
Participants were enrolled into the PROUD trial between November 2012 and April 2014, and were randomly assigned to start PrEP immediately at enrolment (IMM) or after a 1-year deferral period (DEF). Eligible participants were HIV negative; tested by a routinely used assay in the previous 4 weeks or on the day of enrolment, male at birth, aged 18 years or older, had attended the enrolling clinic previously, and reported anal sex without a condom in the previous 90 days and stated it likely that this behaviour would recur again in the next 90 days. At enrolment, participants’ self-completed a questionnaire on: demographic characteristics, including age, education, country of birth, whether they had been circumcised and relationship status; self-reported history of number of HIV/STI screens, STIs and the use of post-exposure prophylaxis (PEP) in the previous 12 months; and sexual behaviour in the previous 90 days. Sexual behaviour included the use of poppers and drugs most commonly associated with chemsex (defined in the footnote to table 1), and the number of different anal sex partners (total, receptive sex, insertive sex, receptive/insertive sex without a condom, receptive/insertive sex without a condom and partner known to be HIV positive). Follow-up visits, including a full STI screen, were scheduled every 3 months.
This analysis is based on participants who were randomised to the DEF arm during the period when they did not have access to PrEP. An incident HIV infection was defined as a reactive HIV antigen-antibody test result, confirmed by the detection of HIV RNA, in participants who were HIV negative at enrolment. Originally, PrEP was planned to be offered at the 12-month scheduled visit. However, in October 2014, based on an interim analysis, the Independent Data Monitoring Committee recommended that all participants should be offered PrEP. Loss to follow-up in the trial was low, with HIV status known in 89% of participants at the end of the deferred phase.2 We additionally sought to identify participants who may have been diagnosed with HIV in a non-study clinic by linking (based on pseudoanonymised identifiers) to the Public Health England (PHE) national database of new HIV diagnoses.12
HIV incidence was compared between different subgroups according to baseline data. For participants who acquired HIV, date of infection was taken to be the date of the first reactive test. Follow-up was censored at the first visit either when a participant was actually offered PrEP (if they remained in follow-up) or when a participant would have been offered PrEP within the trial (if they experienced early loss to follow-up). This differs from the censoring rules in the main analysis, which were based on the timing of HIV tests in study clinics and did not consider PHE linkage data. In addition, two participants enrolled twice in the trial (first to DEF and then to IMM). In the main analysis, their entire follow-up was assigned according to their original randomisation allocation (intention to treat); in the present analysis, their follow-up is censored at the date of their second randomisation (when they were offered PrEP).2Online supplementary appendix table 1 summarises the censoring rules described above.
Due to the small number of events, we used exact Poisson methods (ci command for incidence rates [IR] and expoisson for rate ratios [RR] with the midp option). For categorical variables, the most frequent category was used as the reference group. To examine whether incidence changed over the period of follow-up, a Weibull model was compared against an exponential model. Statistical analyses were conducted in Stata V.14.0.
A total of 268 participants from the DEF arm were included in the analysis after excluding one individual due to a reactive HIV antigen-antibody test at enrolment, despite a non-reactive point-of-care test. Baseline questionnaires were not completed by two individuals and responses were occasionally missing for some questions for others (maximum 6.3% missing, table 1, footnote). At enrolment, median age was 35 years (IQR: 28–41), 40.2% were born outside the UK, 69.8% were recruited through a London clinic and 55.1% were single (table 1). In the previous 12 months, 39.5% reported they had been diagnosed with rectal chlamydia (CT), rectal gonorrhoea (GC) or syphilis (referred to subsequently as a key STI), and 36.7% had received at least one PEP prescription. There was wide variability in the reported number of anal sex partners in the 90 days prior to enrolment. 9.2% reported a single partner while 27.5% reported 20 or more with a median of 10 (IQR: 4–20). A high proportion reported receptive anal intercourse without a condom (ncRAI); 87.5% at least once and 11.7% reported 10 or more such partners.
Overall, 21 participants acquired HIV infection over 239.3 PY follow-up, yielding an IR of 8.8 per 100 PY (95% CI 5.4 to 13.4 per 100 PY). Matching with the national HIV new diagnoses database yielded an additional 19.4 years of follow-up (from 31 participants), and one further HIV infection in addition to the 20 infections originally reported.2 During the relatively short period of follow-up, there was a non-significant (p=0.13) increase in HIV incidence (Weibull shape parameter=1.4).
Reporting a diagnosis of a key STI in the previous 12 months was a highly significant predictor for HIV acquisition. The IR in this subgroup was 17.2 per 100 PY (15/87.0, 95% CI 9.7 to 28.5), 4.8-fold higher (95% CI 1.8 to 14.9) than the rate for men who did not report such a diagnosis. Incidence did not vary substantially according to the specific key STI that was reported (table 2). Table 2 also shows that HIV incidence was relatively low among participants reporting a pharyngeal or urethral STI (without a rectal STI).
The other strong predictive factor was the number of self-reported anal sex partners in the previous 90 days, whether this was expressed overall, just for receptive sex or further limited to condomless sex (online supplementary appendix table 2). These variables are highly correlated and therefore difficult to distinguish, although the clearest gradient in risk was seen for the number of ncRAI partners. A threshold effect was evident, with HIV risk sharply elevated for men reporting two or more partners; HIV incidence in this subgroup was 13.6 per 100 PY (17/125.3, 95% CI 7.9 to 21.7), with an RR of 4.6 (95% CI 1.5 to 19.8). Thirty-one participants (12.2%) reported that the only condomless sex they had was insertive, none of whom acquired HIV during follow-up (95% CI 0 to 12.3 per 100 PY); 16 (51.6%) of these participants were circumcised.
The diagnosis of a key STI in the year prior to enrolment was closely related to the number of ncRAI partners in the previous 3 months. For those with 0, 1, 2–4, 5–9 and 10+partners, 22.6%, 30.7%, 40.0%, 54.5% and 66.7% reported an STI in the previous year, respectively (p value for trend <0.001). In a bivariate model that included both ncRAI and key STI, the relative risk estimates for two or more ncRAI partners were attenuated (RR 4.6 to 2.9) but the estimate for the diagnosis of a key STI was largely unchanged (RR 4.8 to 4.7). All but one (20/21, 95.2%) of the HIV infections occurred among the 177 participants who reported either a key STI or ncRAI with two or more partners; the PY observed in the group reporting either of these characteristics comprised 63.4% (151.6/239.3) of the overall follow-up. The IR of the participants lacking both of these risk factors was 1.1 per 100 PY (1/87.6, 95% CI 0.03 to 6.4 per 100 PY).
Non-significant trends in the expected direction were seen for other variables, including PEP use, use of chemsex-associated drugs, the number of HIV tests age (younger men at higher risk) (table 1). Participants in full-time employment were at higher risk of HIV compared to those not in full-time employment. There was no effect of location of clinic (London vs non-London) or whether the participant was born in the UK. Participants in a relationship but who were not cohabiting were at a lower risk of HIV infection than either single men or men in a cohabiting relationship.
The most powerful individual predictor of HIV infection in PROUD was the diagnosis of syphilis or a bacterial rectal infection (CT/GC) in the previous year; HIV incidence was 17.2 per 100 PY in this subpopulation. A recent analysis of MSM who were repeat attenders at genitourinary medicine (GUM) clinics in England identified similar factors but the strength of the association was weaker and the proportion of infections associated with this risk factor was much smaller.13 This is likely explained by the lower HIV incidence and smaller proportion of attenders with a history of an STI in the national study. A secondary analysis of the iPrEx trial examined predictors of HIV infection in the placebo arm.14 The only STI variable reported in this trial was whether an infection had been reported in the previous 6 months, irrespective of the type or site of infection. This lack of specificity may explain the small difference in HIV incidence between participants with (4.9 per 100 PY) and without (3.6 per 100 PY) an STI report. The strong effect in PROUD may be partly due to the regularity of STI screening in sexual health clinics in the UK, with participants receiving a median of three screens in the year prior to enrolment.11 Pharyngeal and urethral STIs were not associated with an increased HIV risk, suggesting that the selection for variables to include in risk algorithms should focus on rectal infections and early syphilis.
The other important predictive variable was the number of sexual partners in the previous 3 months, particularly the number of ncRAI partners. Participants with fewer than two ncRAI partners were at a comparatively lower risk of HIV infection (2.9 per 100 PY), falling just below the WHO threshold of ‘substantial’ risk. The risk fell further below this threshold when combined with the absence of a key STI diagnosis, suggesting that this subgroup should be a lower priority to receive PrEP (ie, one or fewer ncRAI partners in previous 3 months and no key STI diagnosed in previous 12 months). In the extreme case where PrEP confers 100% protection, 95% of incident HIV infections would have been prevented by providing PrEP only to individuals reporting either a key STI or ncRAI with two or more partners (63% of the PY of follow-up). While the very high HIV incidence in PROUD raises the question of generalisability to other lower risk settings, we believe this concern applies more to our quantitative estimates than to the findings in general, which should be broadly applicable. Another clinically relevant finding was the low risk for men who engage exclusively in condomless insertive anal intercourse, mirroring findings in the iPrEx study.14 However, individual clinical decisions clearly should take into account current risk behaviours as well as historical and anticipated ones. The definition of ‘historical’ is also not standardised across guidelines, some referring to the previous 6 months and some not specifying a time frame at all.8 9
HIV incidence among PROUD participants without access to PrEP was fourfold higher than that of the MSM population attending GUM clinics in the UK.2 13 This is likely to represent an enrichment phenomenon where self-awareness of a high risk of acquiring HIV infection motivates individuals to seek PrEP.15 If genuine, this phenomenon is favourable for the cost-effectiveness of PrEP, which is highly dependent on HIV incidence in the group to whom it is offered.16 17 Analyses of risk factors for the acquisition of HIV infection have been conducted in cohort studies of MSM in several countries,13 18 19 often with a motivation to inform eligibility criteria for PrEP or to identify individuals at particularly high risk who could potentially be targeted.14 18 A limitation of these studies was an inability to identify those participants who would have been interested in taking PrEP had it been available. The key strength of this secondary analysis of PROUD is the restriction to MSM who were either actively seeking PrEP or had accepted a clinical recommendation from their clinician.
The main limitation of our analysis is the low number of incident HIV infections, but this was unavoidable due to the size of the trial. The consequences are twofold: imprecise estimates of HIV incidence and an inability to undertake multivariate analyses to develop a risk algorithm. Although PrEP was not available through the National Health Service during the study period, some participants in the deferred arm may have accessed it through other means. PEP use was also common with 174 courses prescribed to 85 participants during the study period,2 which could have further reduced the estimated incidence. Finally, our results are sensitive to the specific recall periods that were used in the questionnaires.
In conclusion, the high HIV incidence in PROUD suggests that participants appropriately judged their risk of acquiring HIV and the benefits of PrEP. Eligibility criteria for a PrEP programme following PROUD can therefore be broad for MSM, as in the current guidelines. However, the risk of acquiring HIV is declining in some settings due to increased PrEP coverage, an increase in HIV testing and rapid treatment after an HIV diagnosis.6 20 This complicates this judgement and may change the predictive value of individual risk factors. In particular, we note a possible further reduction in the already low risk for those reporting only one partner with whom they had not used a condom for receptive anal sex and it will be important to continue to review the need for PrEP in this group. However, a recent history of syphilis, rectal CT/GC or two or more ncRAI partners indicates a high imminent risk of HIV infection, and HIV-negative MSM with any of these characteristics should be offered PrEP as a matter of urgency.
An important unresolved question in pre-exposure prophylaxis (PrEP) programmes is patient eligibility.
As the amount of PrEP is generally limited, it is important that it is offered to those at the highest risk of acquiring HIV.
Highest HIV risk was among men who have sex with men (MSM) reporting a recent rectal STI or syphilis diagnosis, or reporting condomless receptive anal intercourse with two or more partners.
HIV-negative MSM with either of these characteristics should be offered PrEP as a matter of urgency.
Handling editor Henry John Christiaan de Vries
Collaborators PROUD study group: David I Dolling, Monica Desai, Alan McOwan, Richard Gilson, Amanda Clarke, Martin Fisher, Gabriel Schembri, Ann K Sullivan, Nicola Mackie, Iain Reeves, Mags Portman, John Saunders, Julie Fox, Jake Bayley, Michael Brady, Christine Bowman, Charles J Lacey, Stephen Taylor, David White, Simone Antonucci, Mitzy Gafos, Sheena McCormack, Owen N Gill, David T Dunn and Anthony Nardone. PROUD clinic teams: Vanessa Apea, Drew Clark, Paul Davis, James Hand, Machel Hunt, Rebecca Neale, Jackie O’Connell, Margaret Portman, Liat Sarner, John Saunders, Louise Terry, Angelina Twumasi, Salina Tsui, Dayan Vijeratnam, Ryan Whyte, Andy Williams (Barts), Sian Gately, Gerry Gilleran, Jill Lyons, Chris McCormack, Katy Moore, Cathy Stretton, Stephen Taylor, David White (Birmingham), Alex Acheampong, Michael Bramley, Marion Campbell, Ruby Chowdhry, Amanda Clarke, Stewart Eastwood, Babs Fennell, Martin Fisher, Wendy Hadley, Kerry Hobbs, Sarah Kirk, Nicky Perry, Charlotte Rawlinson, Celia Richardson, Claire Richardson, Mark Roche, Emma Simpkin, Simon Shaw, Elisa Souto, Julia Williams, Elaney Youssef (Brighton), Simone Antonucci, Tristan Barber, Cindy Eliot, Serge Fedele, Chris Higgs, Kathryn McCormick, Sheena McCormack, Alan McOwan, Alexandra Meijer, Sam Pepper, Jane Rowlands, Gurmit Singh, Alfredo SolerCarracedo, Sonali Sonecha, Ann Sullivan, David Taylor, Lervina Thomas (Chelsea and Westminster), Frederick Attakora, Marina Bourke, Richard Castles, Rebecca Clark, Anke De-Masi, Veronica Espa, Rumbidzai Hungwe, Martin Lincoln, Sifiso Mguni, Rhianon Nevin-Dolan, Iain Reeves (Homerton), Hannah Alexander, Jake Bayley, Michael Brady, Lucy Campbell, Sophie Candfield, Shema Doshi, Olivia Liddle, Larissa Mulka, Priyanka Saigal, James Stevenson (King’s), James Boateng, Brynn Chappell, Susanna Currie, Carolyn Davies, Dornubari Lebari, Matthew Phillips, Gabriel Schembri, Lisa Southon, Sarah Thorpe, Anna Vas, Chris Ward, Claire Warren, Stephanie Yau (Manchester), Alejandro Arenas-Pinto, Asma Ashraf, Matthew Bolton, Richard Gilson, Lewis Haddow, Sara McNamara, Ana Milinkovic, June Minton, Dianne Morris, Clare Oakland, Steve O’Farrell, Pierre Pellegrino, Sarah Pett, Nina Vora, Carmel Young, Taris Zarko-Flynn (Mortimer Market), Wilbert Ayap, Ling Jun Chen, Adam Croucher, Sarah Fidler, Kristin Kuldanek, Ken Legg, Agathe Leon, Nicola Mackie, Nadia Naous, Killian Quinn, Severine Rey, Judith Zhou (St Marys), Margaret-Anne Bevan, Julie Fox, Nina Francia, Eleanor Hamlyn, Lisa Hurley, Helen Iveson, Isabelle Jendrulek, Tammy Murray, Alice Sharp, Andrew Skingsley, Chi Kai Tam, Al Teague, Caroline Thomas, Juan-Manuel Tiraboschi (St Thomas’), Christine Brewer, Richard Evans, Jan Gravely, Charles Lacey, Gary Lamont, Fabiola Martin, Georgina Morris, Sarah Russell-Sharpe, John Wightman (York), Anthony Bains, Gill Bell, Christine Bowman, Terry Cox, Claire Dewsnap, Charlie Hughes, Hannah Loftus, Naomi Sutton, Debbie Talbot, Vince Tucker (Sheffield). MRC CTU at UCL: Sarah Banbury, Elizabeth Brodnicki, Christina Chung, David I Dolling, David T Dunn, Keith Fairbrother, Michelle Gabriel, Mitzy Gafos, Sajad Khan, Shabana Khan, Sheena McCormack, Brendan Mauger, Gemma Sancha, Annabelle South, Yinka Sowunmi, Susan Spencer and Ellen White. Social Science team: Gill Bell, Caroline Rae, Michael Rayment, Will Nutland and Sonali Wayal. Public Health England: Monica Desai, Sarika Desai, Nigel Field, Noel Gill, Kate Hyland, Peter Kirwan, Anthony Nardone and Parnam Seyan. Gilead Sciences: Rich Clarke and Jim Rooney.
Contributors SM led the study. DTD, MD, MG and SM conceived and designed the study. AKS, AC and SM recruited participants and collected data. EW conducted the analyses and led the writing on this paper. PK conducted the participant matching. All authors read and approved the final manuscript. EW had full access to all the data in the study and had final responsibility for the decision to submit for publication.
Funding The PROUD trial was supported by ad hoc funding from the Medical Research Council (MRC) Clinical Trials Unit at University College London and an innovations grant from Public Health England, and most clinics received support through the UK NIHR Clinical Research Network. Gilead Sciences provided Truvada, distributed drug to clinics and awarded a grant for the additional diagnostic tests including drug concentrations in plasma. EW, DTD and SM were supported by the UK Medical Research Council (MRC_UU_12023/23) during preparation of and outside the submitted work.
Competing interests The PROUD study was provided drug free of charge by Gilead Sciences which also distributed it to participating clinics and provided funds for additional diagnostic tests for HCV and drug levels. EW's university fees and stipend were funded by Gilead Sciences. DTD has received fees for participation on advisory boards and educational workshops from ViiV Healthcare and Gilead Sciences. PK was part funded by Gilead Sciences during 2017/2018. AC received advisory board fees from Gilead Sciences and GSK/ViiV; speaker fees from Gilead and conferences bursaries from Gilead & Janssen. SM reports grants from the European Union H2020 scheme, EDCTP 2, the National Institute of Health Research and Gilead Sciences; other support from Gilead Sciences, and the Population Council Microbicide Advisory Board; and is Chair of the Project Advisory Committee for USAID grant awarded to CONRAD to develop tenofovir-based products for use by women (non-financial).
Patient consent for publication Not required.
Ethics approval The study was reviewed and approved by the London Bridge Research Ethics Committee (REC number: 12/LO/1289). The study protocol is available online (http://www.proud.mrc.ac.uk/about/study-protocol/).
Provenance and peer review Not commissioned; externally peer reviewed.
Data sharing statement The PROUD data are held at MRC CTU at UCL, which encourages optimal use of data by employing a controlled access approach to data sharing, incorporating a transparent and robust system to review requests and provide secure data access consistent with the relevant ethics committee approvals. All requests for data are considered and can be initiated by contacting firstname.lastname@example.org.
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