Non-occupational HIV post-exposure prophylaxis at a Sydney metropolitan sexual health clinic
Trine Gulholm A , Salina Jamani A , I. Mary Poynten B and David J. Templeton A B C DA RPA Sexual Health, Royal Prince Alfred Hospital, Sydney, NSW 2050, Australia.
B The Kirby Institute, University of New South Wales, Sydney, NSW 2052, Australia.
C Central Clinical School, University of Sydney, Sydney, NSW 2006, Australia.
D Corresponding author. Email: david.templeton@email.cs.nsw.gov.au
Sexual Health 10(5) 438-441 https://doi.org/10.1071/SH13018
Submitted: 1 February 2013 Accepted: 20 June 2013 Published: 21 August 2013
Abstract
Background: Non-occupational HIV post-exposure prophylaxis (NPEP) is prescribed following a risk exposure in an effort to reduce the risk of HIV seroconversion. We aimed to describe the prescribing practices of NPEP at RPA Sexual Health in Sydney, the prevalence and correlates of adverse events (AEs), and factors associated with completing the 28-day course. Methods: The study population included individuals prescribed NPEP during January 2008–December 2011. Correlates of AEs and course completion were assessed by logistic regression. Results: On 319 occasions during the study period, 282 individuals presented for NPEP. Over 90% of presentations followed unprotected anal intercourse between men, mostly receptive (63.6%). Tenofovir–emtricitabine–stavudine (n = 149; 46.7%) and tenofovir–emtricitabine (n = 136; 42.6%) were most commonly prescribed. AEs were reported at 101 presentations (31.7%, 95% confidence interval (CI): 26.6–37.1%), with nausea and lethargy/malaise being the most common. Younger age (P for trend = 0.032), earlier year of NPEP prescription (P for trend = 0.011), being prescribed a regimen other than tenofovir–emtricitabine (P = 0.026), changing the NPEP regimen (P < 0.001) and known completion of the course (P = 0.005) were independently associated with AEs. The course was completed in 228 presentations (71.5%, 95% CI: 66.2–76.4%). Completion was associated with reporting AEs (P = 0.007) and changing regimen (P = 0.001). No documented NPEP failures were identified, although two recipients subsequently seroconverted to HIV due to ongoing high-risk behaviour. Conclusions: NPEP is appropriately targeted to the highest risk HIV exposures at our clinic. Active recall may improve follow-up rates in NPEP recipients.
Additional keywords: adverse effects, homosexuality, male, medication adherence.
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