INTRODUCTION
Following its launch in 2003, South Africa's antiretroviral therapy (ART) programme has been successful, with over five million people living with HIV (PWH) initiated on treatment by 2022, resulting in a decline in HIV-related deaths and an improved quality of life [1, 2]. Timely identification of individuals with advanced HIV disease (AHD) is crucial for optimizing care and treatment outcomes [3]. AHD, defined as HIV with a CD4 count less than 200 cells/mm3, has significant implications for patient prognosis, susceptibility to coinfections, and the need for additional screening and prophylaxis, in addition to ART [3].
Upon entry or re-entry into HIV care, around 30% of individuals are found to have AHD, highlighting the importance of CD4 testing for persons not taking ART as a standard of care [4]. PWH who are not on ART are at a higher risk for tuberculosis (TB) disease due to compromised immune function [5]. TB screening is also crucial in HIV care, particularly during ART initiation/re-initiation to mitigate the risk of immune reconstitution inflammatory syndrome, and is recommended annually for PWH who are stable on ART [6]. However, for PWH stable on ART, continued CD4 monitoring offers little benefit and is not cost-effective [7].
In South Africa, the prevalence of undiagnosed TB among PWH not on ART is estimated to be between 5% and 10% [8, 9]. An interim analysis of our cohort study conducting intensive TB screening among PWH-initiating ART revealed an unexpectedly low prevalence of undiagnosed TB. Only one of the first 100 enrolled PWH reporting no ART use had TB, prompting further investigation to explain this striking finding.
Undisclosed ART use, where PWH may access and ingest ART without reporting this to healthcare providers, has been identified in public health clinic settings in South Africa [10, 11] and is linked with administrative challenges faced by migrants when changing health facilities, as well as individuals who change clinics due to stigma or fear of reprimand for missed visits [12, 13]. Undisclosed ART use may lead to unnecessary HIV counselling and testing, inappropriate laboratory testing and inefficient use of healthcare resources. Detecting ART use in PWH who self-report not taking ART is challenging, especially in settings where frequent viral load monitoring is restricted due to cost and the electronic data systems between health facilities are not linked, allowing for people to attend multiple clinics without detection.
Our group recently developed a point-of-care (POC) urine-based tenofovir (TFV) immunoassay which detects TFV ingested in the last 4 days [14–17]. We employed this test to estimate the prevalence of undisclosed ART use in a cohort of PWH in South Africa recruited for a TB prevalence study.
METHODS
Study design
We conducted a cross-sectional study assessing undisclosed ART use nested within the DROP-TB study, a cohort study evaluating TB prevalence and a novel urine lipoarabinomannan (LAM) TB diagnostic test [18] in South Africa. The DROP-TB study enrolled PWH not taking ART from two public health clinics (rural and peri-urban) in the uMkhanyakude district in KwaZulu-Natal, South Africa. These are Department of Health primary healthcare clinics, where professional nurses provide basic primary care services, including HIV and TB testing, at no cost to the user [19]. DROP-TB eligibility criteria included: (1) age ≥18 years; (2) a confirmed positive HIV test; (3) ART-naïve or self-reporting not taking ART in the prior 90 days; (4) presented to clinic for HIV testing to initiate or re-initiate ART; and (4) did not receive TB treatment in the prior 90 days. ART use was initially assessed by the patient self-report to the counsellor conducting the HIV test. Persons presenting to clinics for HIV testing were informed of the opportunity to participate in DROP-TB only after initial eligibility was established, to minimize social desirability bias in self-reporting of ART use to participate in the study.
Study procedures
Participants enrolling in DROP-TB between December 2021 and May 2024 underwent a baseline clinical examination, answered standardized questions about TB and HIV history, and provided samples for routine laboratory investigations including TB diagnostic testing (performed through the National Health Laboratory Service), and research-related testing including TB reference testing with TB culture and investigational TB assays (performed in the clinical laboratory at AHRI [20]). At the baseline visit, participants provided blood for CD4 testing, sputum for Xpert MTB/RIF Ultra (Cepheid, Sunnyvale, CA), MGIT liquid TB culture (Becton-Dickinson, Franklin Lakes, NJ) and urine for both lateral flow LAM (LF-LAM, Abbott) testing and the novel urine-based LAM test. Urine remaining after DROP-TB testing was frozen and stored at −80°C. Participants received reimbursement of ZAR 150 (USD 8.50) for participation. A positive (prevalent) TB result was defined as a positive sputum Xpert Ultra or TB culture, or initiation of TB treatment by a Department of Health clinician within 3 months of enrolment.
We tested thawed urine samples with the urine-based lateral flow assay (LFA) for TFV. Urine samples were tested retrospectively as a research procedure by study laboratory personnel; results were not provided to participants or their providers. The urine TFV LFA is a low-cost POC test that can identify the presence of TFV in urine within a timeframe of 4–7 days of ingestion. The test is 96% sensitive and 100% specific for TFV detection at concentrations >1500 ng/ml compared to the gold standard of liquid chromatography/tandem mass spectrometry (LC-MS/MS) and can be easily implemented by healthcare personnel in real-time [16]. The LFA has comparable accuracy in testing fresh versus frozen urine samples [16]. All urine samples were tested after being thawed to room temperature, consistent with laboratory protocol. We defined undisclosed ART use as a positive urine TFV LFA result in a DROP-TB participant, since all participants reported no ART use within the past 90 days.
Statistical analysis
We assessed the proportion of individuals with undisclosed ART use according to the TFV LFA test. Descriptive statistics compared demographics and characteristics in those with a positive urine TFV assay to those without. We compared the proportions of categorical data with Chi-squared tests and medians of continuous data with t-tests. We employed logistic regression models to evaluate predictors of ART non-disclosure and the association between ART non-disclosure and TB. We fitted a multivariable logistic regression model including variables of a priori interest (age, sex) and included potential explanatory variables found to be significant in bivariate analyses with a p-value < 0.25. Statistically significant p-values in the final model were defined as less than 0.05.
Ethics
The study was approved by UKZN BREC/00001174/2020 and UW IRB STUDY00000124. All participants provided written informed consent to participate and for future testing of stored samples.
RESULTS
We tested stored frozen urine samples from 404 PWH enrolled in the DROP-TB study who presented for ART initiation or re-initiation. All participants had a positive HIV rapid test, confirmed using the standard testing algorithm, from one of two study recruitment clinics in KwaZulu-Natal between December 2021 and May 2024. Among PWH with urine tested for TFV, 242 (60%) were women, the median age was 32 (IQR 26–39) years, and the median CD4 count was 345 cells/mm3 (IQR 181–510) (Table 1). Fourteen (3%) participants tested positive for TB (10 men), of whom all had at least one TB symptom. Most participants (N = 341, 84%) had a secondary level of education or higher, were financially dependent on social grants (N = 249, 61%) and were in a relationship (N = 288, 71%). More people attended the urban clinic (67% vs. 33%) and most (75%) did not smoke tobacco.
Table 1 Characteristics of PWH reporting no ART use, presenting for ART initiation, at two clinics in South Africa
| Total cohort | ART present on LFA | ART not present on LFA | ||
| Characteristics | N=404 | N=79 (20%) | N=325 (80%) | p-value |
| Gender, N (%) | ||||
| Female | 241/404 (60%) | 45 (57%) | 196 (60%) | |
| Male | 163/404 (40%) | 34 (43%) | 129 (40%) | 0.57 |
| Age, N (%): median (IQR) | 32 (25−38) | 37 (27−39) | 31 (24−36) | <0.001 |
| 18−29 | 148/404 (37%) | 16 (20%) | 132 (41%) | |
| 30−49 | 235/404 (58%) | 53 (67%) | 182 (56%) | |
| >50 | 21/404 (5%) | 10 (13%) | 11 (3%) | <0.001 |
| Facility location, N (%) | ||||
| Peri-urban clinic | 271/404 (67%) | 36 (46%) | 235 (72%) | |
| Rural clinic | 133/404 (33%) | 43 (54%) | 90 (28%) | <0.001 |
| CD4 count, N (%): median (IQR) | 345 (181−510) | 466 (277−625) | 322 (175−490) | <0.001 |
| 0−200 | 113/398 (28%) | 14/78 (18%) | 99/320 (31%) | |
| 200−350 | 90/398 (23%) | 11/78 (14%) | 79/320 (25%) | |
| 350−500 | 84/398 (21%) | 16/78 (21%) | 68/320 (21%) | |
| >=500 | 111/398 (28%) | 37/78 (47%) | 74/320 (23%) | <0.001 |
| Highest education, N (%) | ||||
| Primary | 48/404 (12%) | 18 (23%) | 30 (9%) | |
| Secondary | 341/404 (84%) | 57 (72%) | 284 (87%) | |
| Tertiary | 3/404 (1%) | 0 (0%) | 3 (1%) | |
| Unknown | 12/404 (3%) | 4 (5%) | 8 (3%) | 0.003 |
| Source of income, N (%) | ||||
| Employed, formal sector | 86/404 (21%) | 13 (16%) | 73 (22%) | |
| Employed, informal sector | 52/404 (13%) | 11 (14%) | 41 (13%) | |
| Student | 16/404 (4%) | 2 (3%) | 14 (4%) | |
| Unemployed, receives social grant | 90/404 (22%) | 22 (28%) | 68 (28%) | |
| Unemployed, dependent on others’ grants | 158/404 (39%) | 31 (39%) | 127 (39%) | |
| Other | 2/404 (1%) | 0 (0%) | 2 (1%) | 0.61 |
| Smoking status, n/N (%) | ||||
| Current | 98/404 (24%) | 27 (34%) | 71 (22%) | |
| Declined to answer | 1/404 (0%) | 0 (0%) | 1 (0%) | |
| Former | 3/404 (1%) | 0 (0%) | 3 (1%) | |
| Never | 302/404 (75%) | 52 (66%) | 250 (77%) | 0.11 |
| Marital status, N (%) | ||||
| In relationship | 287/404 (71%) | 50 (63%) | 237 (73%) | |
| Living with a partner | 33/404 (9%) | 8 (10%) | 25 (8%) | |
| Married, one spouse | 22/404 (5%) | 3 (4%) | 19 (6%) | |
| Single | 62/404 (15%) | 18 (23%) | 44 (13%) | 0.15 |
| TB positive, N (%) | 14/404 (3%) | 6 (8%) | 8 (2%) | 0.02 |
| Ever taken ART, N (%) | ||||
| No | 353/404 (87%) | 57 (72%) | 296 (91%) | |
| Yes, but not in 90 days | 51/404 (13%) | 22 (23%) | 29 (9%) | <0.001 |
Undisclosed ART use was identified through urine TFV in 79 (20%) of participants, with 57/79 (72%) reporting to be ART-naïve. PWH with undisclosed ART use were older (median age: 37 vs. 31 years) and had higher CD4 counts (median: 466 vs. 322 cells/µl). Among people with TB, 40% had recent TFV use (Table 1). In multivariable models, odds of undisclosed ART use increased with increasing age (aOR 2.4 [95% CI 1.31−4.38, p = 0.004] for ages 30–49; aOR 7.2 [95% CI 2.75−20.4, p = 0.001] for ages >50 vs. age <30), increasing CD4 count (aOR 3.61 [95% CI 1.78−7.01, p = 0.001] for CD4 ≥500 vs. CD4 <200), attendance at the rural clinic versus urban (aOR 3.13 [95% CI 1.89−5.18, p = 0.001]) and having TB (aOR 3.26 [95% CI 1.09–9.70, p = 0.03]) (Table 2).
Table 2 Predictors of undisclosed ART use in PWH
| n/N (%) | Adjusted odds ratio (95% CI) | p-value | |
| Gender | |||
| Female | 242/404 (60) | ref | 0.57 |
| Male | 163/404 (40) | 1.15 (0.70−1.89) | |
| Age | |||
| 18−29 | 148/404 (37) | ref | |
| 30−49 | 235/404 (58) | 2.40 (1.31−4.38) | 0.004 |
| >50 | 21/404 (5) | 7.5 (2.75−20.41) | <0.001 |
| CD4 count (cells/mm3) | |||
| 0−200 | 113/398 (28) | ref | |
| 200−350 | 91/398 (23) | 0.97 (0.41−2.25) | 0.94 |
|
350−500 > = 500 |
84/398 (21) 111/398 (28) |
1.66 (0.76−3.63) 3.61 (1.78−7.01) |
0.20 <0.001 |
| Clinic location: | |||
| Peri-urban | 272/404 (67) | ref | |
| Rural | 133/404 (33) | 3.13 (1.89−5.18) | <0.001 |
| TB status | |||
| Negative | 391/404 (97) | ref | |
| Positive | 14/404 (3) | 3.26 (1.09–9.70) | 0.03 |
DISCUSSION
Using a novel urine TFV LFA, we found that 20% of PWH presenting to two clinics for ART initiation and re-initiation had undisclosed ART use. This is consistent with previous studies which suggest that a substantial number of PWH may not report ART use at public health clinics in South Africa [10, 11]. Interestingly, 72% (57/79) of those with undisclosed ART use reported to be ART-naïve, highlighting the importance of targeting this population for TFV urine testing during HIV screening. However, the urine test should not be limited to this group, as it may miss a substantial proportion of individuals who are using ART but not disclosing.
Undisclosed ART use was associated with older age, higher CD4 counts, attending the rural clinic and having active TB. One possible explanation for these associations is that individuals who do not disclose their ART use may be presenting to clinics while virally suppressed and stable on treatment. Older age and higher CD4 counts may reflect a longer duration of ART use [21]. The association with rural sites may be driven by limited job opportunities in rural areas: In public health clinics, where clients do not have portable electronic medical records, health workers may request a physical transfer letter from the previous clinic. PWH presenting to a clinic to continue stable ART previously received elsewhere may be declined enrolment without a transfer letter from the previous clinic [22]. In contrast, no documentation is required to initiate ART. Individuals from rural areas may migrate for employment and establish ART care locally, but upon returning home, may not disclose their ART use to avoid the cost and inconvenience of obtaining transfer letters from their ART site, preferring to present as ART-naïve [11–13, 22]. Contrary to our initial hypothesis, we found a significant positive association between active TB and undisclosed ART use. Since most of those with TB were men (70%), the association may reflect employment-related migration of men. This unexpected finding underscores the importance of routine TB screening at every clinic visit, regardless of ART status.
South Africa has the world's largest ART programme and non-disclosure of ART to clinics will result in higher costs from unnecessary testing, treatment and personnel time spent on counselling. Reducing non-disclosures could optimize the use of resources for testing and clinical care. The high frequency of non-disclosure highlights the need for person-friendly differentiated service delivery (DSD) approaches that cater to the unique needs of individuals who may be accessing ART without disclosing to healthcare providers, particularly those who are highly mobile and need to change clinics frequently [12, 13]. By addressing the root causes of non-disclosure, DSD models can provide tailored support and monitoring strategies to improve patient outcomes and optimize healthcare resource usage [23], as the current clinic transfer practice is not person-centred. People who conceal ART are mobile populations who relocate for work, family obligations and stigma linked with experiences at prior clinics [12]. The need for flexible and compassionate approaches that consider unique circumstances should be encouraged in healthcare.
Resources utilized at initiation visits are more intensive compared to those at continuation visits. During initiation, comprehensive diagnostic tests, extensive counselling, and education on HIV and ART are provided, along with initial treatment planning and close monitoring for potential drug interactions and side effects. In contrast, continuation visits focus on viral load monitoring, adherence support and less frequent medication refills (Table 3). Therefore, accurately identifying true ART initiators versus those re-entering care after undocumented transfers is crucial [24]. At present, there are greater administrative challenges in confirming the continuation of care than in initiating or re-initiating it [12]. Our proposal is to use the test as a tool to identify individuals who need continuation care, while an integrated system with unique identifiers is implemented. The introduction of this test must be accompanied by extensive training, and removal of burdensome administrative requirements of transfer letters, to ensure it does not become another tool for stigmatization. The goal is not to make this test a permanent fixture in care, but to use it as an interim solution to address non-disclosure until an integrated system is in place.
Table 3 Difference between resources used and client follow-up burden/frequency during ART initiation versus ART continuation visit at clinics in South Africa
| Resources | ART initiation | ART continuation |
| HIV diagnostics | HIV rapid testing | No testing |
| Laboratory tests |
CD4, CrCl, TB lcNAAT, Hb, HBsAg and CrAg if CD4 < 100 cells/µl No VL testing |
VL at M3, M10, M22 and yearly TB lcNAAT yearly |
| Counselling | HIV, ART and adherence | Support |
| Medication | Initial treatment education and planning, 1M supply dispensed |
Medication refills 3−6M supply dispensed |
| Screening | TB, STIs, pregnancy, NCDs, cervical cancer, mental health issues and meningitis | TB symptoms |
| Additional support | Social work, mental health and so on | Less intensive support services |
| Monitoring | Close monitoring for potential drug interactions and toxicity | Ongoing care and maintenance |
| Examination | Full physical examination to determine clinical stage | No physical examination |
| Return frequency | 1 week follow-up, 1M follow-up, 3M follow-up | 6M follow-up |
There were several limitations to this study. Only two health facilities were included in the analysis, which limits the generalizability of the results. The urine LFA detects TFV only and not other antiretrovirals. However, TFV is part of the first-line fixed-dose ART regimen used in South Africa and much of the world—tenofovir-lamivudine-dolutegravir—so it is a robust indicator of ART use. Although TFV is also a component of oral Pre-Exposure Prophylaxis (PrEP) for HIV prevention, PrEP use is uncommon in the study area [25, 26] and this study limited eligibility to those with a positive HIV test. This indicates that a positive urine TFV represented ART use, not PrEP.
Our study is unique in reporting on undisclosed ART use at public health clinics in South Africa in using an objective metric of ART exposure, verifying use with an LFA designed to be used in clinic settings. Other studies investigating ART non-disclosure used laboratory-based testing to verify ART exposure, which is expensive and requires laboratory-based personnel [10, 11, 16]. A POC urine LFA costs less than USD 2 per test and can be performed by healthcare personnel in the clinic. Urine TFV LFAs are highly sensitive, easy to use and can be used as an immediate solution to identify undisclosed ART use at clinics in South Africa, since PWH may be disincentivized to disclose ART use with current clinic practices. Given the high proportion of undisclosed ART use detected in our study, we recommend using urine TFV LFAs during clinic-based HIV testing in South Africa. PWH found to have TFV in urine can be asked, in a non-judgemental manner, about ART use and reasons for non-disclosure. Clinicians can then determine whether ART continuation procedures may be appropriate (instead of initiation) and facilitate a formal transfer from the previous clinic, streamlining care and avoiding redundant testing. To effectively integrate POC urine LFA into routine HIV testing, healthcare workers would require training, not only about the challenges faced by individuals with undisclosed ART, but also how to respond in a welcoming way when identifying ART use through a test result, ultimately enabling patient-centred care and support.
CONCLUSIONS
By utilizing POC urine LFA testing for TFV, individuals with HIV on ART can be identified, allowing for appropriate DSD referrals as or until clinic practices are transformed to incentivize disclosure. This approach may improve the accuracy of national HIV treatment retention metrics and optimize resource allocation, leading to a more robust South African ART programme.
COMPETING INTERESTS
AES receives grant funding from Merck as a clinical trial investigator.
AUTHORS’ CONTRIBUTIONS
NS, MG and AES designed the study. NS and NP collected the data. TS, SC and MZ tested the samples. NS and AES analysed the data. NS and AES drafted the manuscript. All authors contributed to the revisions and content of the final manuscript.
ACKNOWLEDGEMENTS
We are grateful to the people of uMkhanyakude for participating in our study. We are also grateful to the uMkhanyakude District Department of Health and clinic staff.
FUNDING
The study was funded by the National Institutes of Health (NIH)/National Institute of Allergy and Infectious Diseases (NIAID) (K23 AI140918), with additional support from K23 MH122286 (MAS) and 2R01AI143340 (MAS, MG). MJS acknowledges additional support from K24 HL166024.
DATA AVAILABILITY STATEMENT
The data that support the findings of this study are available on request from the corresponding author. The data are not publicly available due to privacy or ethical restrictions.
Nattrass N. South Africa's “rollout” of highly active antiretroviral therapy: a critical assessment. J Acquire Immune Defic Syndr. 2006;43(5):618–23.
UNAIDS. unaids.org/en/regionscountries/countries/southafrica. 2022. Accessed May 27, 2025
Prabhu S, Harwell JI, Kumarasamy N. Advanced HIV: diagnosis, treatment, and prevention. Lancet HIV. 2019;6(8):e540–e51.
Meya DB, Tugume L, Nabitaka V, Namuwenge P, Phiri S, Oladele R, et al. Establishing targets for advanced HIV disease: a call to action. South Afr J HIV Med. 2021;22(1):1266.
Ellis PK, Martin WJ, Dodd PJ. CD4 count and tuberculosis risk in HIV‐positive adults not on ART: a systematic review and meta‐analysis. PeerJ. 2017;5:e4165.
Sueki H, Mizukawa Y, Aoyama Y. Immune reconstitution inflammatory syndrome in non‐HIV immunosuppressed patients. J Dermatol. 2018;45(1):3–9.
Ford N, Meintjes G, Pozniak A, Bygrave H, Hill A, Peter T, et al. The future role of CD4 cell count for monitoring antiretroviral therapy. Lancet Infect Dis. 2015;15(2):241–7.
Yanes‐Lane M, Ortiz‐Brizuela E, Campbell JR, Benedetti A, Churchyard G, Oxlade O, et al. Tuberculosis preventive therapy for people living with HIV: a systematic review and network meta‐analysis. PLoS Med. 2021;18(9):e1003738.
Osman M, Karat AS, Khan M, Meehan SA, von Delft A, Brey Z, et al. Health system determinants of tuberculosis mortality in South Africa: a causal loop model. BMC Health Serv Res. 2021;21(1):388.
Mavhandu‐Ramarumo LG, Tambe LAM, Matume ND, Katerere D, Bessong PO. Undisclosed exposure to antiretrovirals prior to treatment initiation: an exploratory analysis. South Afr J HIV Med. 2021;22(1):1200.
Sithole N, Gunda R, Koole O, Krows M, Schaafsma T, Moshabela M, et al. Undisclosed antiretroviral therapy use at primary health care clinics in rural KwaZulu Natal South Africa: a DO‐ART trial sub‐study. AIDS Behav. 2021;25(11):3695–703.
Sithole N, Nkosi B, Seeley J, Barnabas RV, Siedner MJ, Moshabela M. “I didn't reveal my ART status because I didn't have money to fetch the transfer letter”‐ understanding lack of treatment disclosure at presentation to care in South Africa: a qualitative study. AIDS Behav. 2024;29(2):715–724.
Sithole N, Nkosi B, Seeley J, Barnabas RV, Seidner MJS, Moshabela M. AIDS 2024 Abstract Book. WEPED339. “I truly don't know how to handle my relationship with getting this treatment”‐ Negotiating life on antiretroviral therapy. A mix methods study on patient journeys to obtain ART in South Africa. IAS AIDS; 2024. Munich, Germany. https://www.iasociety.org/sites/default/files/AIDS2024/abstract‐book/AIDS‐2024_Abstracts.pdf
Spinelli MA, Glidden DV, Anderson PL, Gandhi M, Cohen S, Vittinghoff E, et al. Brief Report: Short‐term adherence marker to PrEP predicts future nonretention in a large PrEP demo project: implications for point‐of‐care adherence testing. J Acquir Immune Defic Syndr. 2019;81(2):158–62.
Spinelli MA, Rodrigues WC, Wang G, Vincent M, Glidden DV, Okochi H, et al. Brief Report: High accuracy of a real‐time urine antibody‐based tenofovir point‐of‐care test compared with laboratory‐based ELISA in diverse populations. J Acquir Immune Defic Syndr. 2020;84(2):149–52.
Gandhi M, Wang G, King R, Rodrigues WC, Vincent M, Glidden DV, et al. Development and validation of the first point‐of‐care assay to objectively monitor adherence to HIV treatment and prevention in real‐time in routine settings. AIDS. 2020;34(2):255–60.
Gandhi M, Bacchetti P, Spinelli MA, Okochi H, Baeten JM, Siriprakaisil O, et al. Brief Report: Validation of a urine tenofovir immunoassay for adherence monitoring to PrEP and ART and establishing the cutoff for a point‐of‐care test. J Acquir Immune Defic Syndr. 2019;81(1):72–7.
Abstract Supplement Oral Abstracts from the 23rd International AIDS Conference, 6–10 July 2020. J Int AIDS Soc. 2020;23 Suppl 4(Suppl 4):e25547.
Health KDo. Umkhanyakude District Health Plan 2018/19–2020/21. 2018/19. https://www.spotlightnsp.co.za/wp‐content/uploads/2020/12/Umkhanyakude_DHP_2018.19.pdf. Accessed May 27, 2025
AHRI. Africa Heath Research Institute web page. https://www.ahri.org/about/2025. Accessed May 27, 2025
Wong EB, Olivier S, Gunda R, Koole O, Surujdeen A, Gareta D, et al. Convergence of infectious and non‐communicable disease epidemics in rural South Africa: a cross‐sectional, population‐based multimorbidity study. Lancet Glob Health. 2021;9(7):e967–e76.
Melanie Bisnauth KR, Chinyandura C. HIV treatment in South Africa: how to help people stay on ARVs when life gets in the way. 2022. https://theconversation.com/hiv‐treatment‐in‐south‐africa‐how‐to‐help‐people‐stay‐on‐arvs‐when‐life‐gets‐in‐the‐way‐190684. Accessed May 27, 2025
UNAIDS. Joint United Nations Program on HIV/AIDS (UNAIDS). UNAIDS Data 2017. Geneva: UNAIDS; 2017.
Etoori D, Wringe A, Kabudula CW, Renju J, Rice B, Gomez‐Olive FX, et al. Misreporting of patient outcomes in the South African National HIV Treatment Database: consequences for programme planning, monitoring, and evaluation. Front Public Health. 2020;8:100.
Shahmanesh M, Chimbindi N, Busang J, Chidumwa G, Mthiyani N, Herbst C, et al. Effectiveness of integrating HIV prevention within sexual reproductive health services with or without peer support among adolescents and young adults in rural KwaZulu‐Natal, South Africa (Isisekelo Sempilo): 2 × 2 factorial, open‐label, randomised controlled trial. Lancet HIV. 2024;11(7):e449–e60.
HSRC. The Sixth South African National HIV Prevalence, Incidence, and Behaviour Survey (SABSSM VI). 2024. https://hsrc.ac.za/wp‐content/uploads/2024/09/SABSSM‐KZN‐dialogue‐23‐September‐2024_FINAL.pdf. Accessed May 27, 2025
You have requested "on-the-fly" machine translation of selected content from our databases. This functionality is provided solely for your convenience and is in no way intended to replace human translation. Show full disclaimer
Neither ProQuest nor its licensors make any representations or warranties with respect to the translations. The translations are automatically generated "AS IS" and "AS AVAILABLE" and are not retained in our systems. PROQUEST AND ITS LICENSORS SPECIFICALLY DISCLAIM ANY AND ALL EXPRESS OR IMPLIED WARRANTIES, INCLUDING WITHOUT LIMITATION, ANY WARRANTIES FOR AVAILABILITY, ACCURACY, TIMELINESS, COMPLETENESS, NON-INFRINGMENT, MERCHANTABILITY OR FITNESS FOR A PARTICULAR PURPOSE. Your use of the translations is subject to all use restrictions contained in your Electronic Products License Agreement and by using the translation functionality you agree to forgo any and all claims against ProQuest or its licensors for your use of the translation functionality and any output derived there from. Hide full disclaimer
© 2025. This work is published under http://creativecommons.org/licenses/by/4.0/ (the "License"). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.
Abstract
Introduction
Differentiated service delivery (DSD) models for HIV and tuberculosis (TB) care prioritize efficient resource allocation and targeted interventions, and benefit from accurate assessment of patients’ antiretroviral therapy (ART) pill‐taking status. Accurate ART use identification is essential for ensuring proper care transition services rather than unnecessary initiation. A point‐of‐care urine tenofovir (TFV) assay may identify undisclosed ART use in settings with high rates of TB and HIV coinfection.
Methods
A cohort of people living with HIV (PWH) presenting for routine care, including newly diagnosed and those returning to care, and reporting no ART use within 90 days, was enrolled in a clinic‐based cross‐sectional study of TB prevalence which tested for TB using sputum and urine‐based TB tests in two clinics in KwaZulu‐Natal, South Africa. CD4 counts were determined at the time of ART initiation, per national guidelines. A novel urine‐based lateral flow assay (LFA) which detects TFV ingested within the past 4–7 days was used to assess ART use from thawed urine samples, which were collected concurrently with the self‐report assessment. Conditional logistic regression models assessed predictors of ART non‐disclosure.
Results
Between 12/2021 and 5/2024, 404 PWH (40% male) reporting no recent ART use presented for ART initiation. TB testing identified 14 (3%) PWH with undiagnosed TB. Seventy‐nine (20%) had detectable TFV in urine indicating undisclosed ART use, with a median CD4 count of 466 cells/mm3 (IQR 277–625) compared to 322 cells/mm3 (IQR 175–490, p = 0.001) in those without undisclosed ART use. In a multivariable model, undisclosed ART use was associated with older age, rural clinic site, higher CD4 count and having active TB, but not with gender, education or employment.
Conclusions
Among people presenting for HIV treatment initiation, 20% had evidence of ART use within 4–7 days by TFV urine LFA testing. Integration of point‐of‐care urine TFV assays into DSD models of HIV care may support providers to engage PWH about treatment challenges, address potential barriers to disclosure and facilitate seamless transfers between clinics. If successful, this strategy may reduce duplicative care entries and promote more efficient use of resources.
You have requested "on-the-fly" machine translation of selected content from our databases. This functionality is provided solely for your convenience and is in no way intended to replace human translation. Show full disclaimer
Neither ProQuest nor its licensors make any representations or warranties with respect to the translations. The translations are automatically generated "AS IS" and "AS AVAILABLE" and are not retained in our systems. PROQUEST AND ITS LICENSORS SPECIFICALLY DISCLAIM ANY AND ALL EXPRESS OR IMPLIED WARRANTIES, INCLUDING WITHOUT LIMITATION, ANY WARRANTIES FOR AVAILABILITY, ACCURACY, TIMELINESS, COMPLETENESS, NON-INFRINGMENT, MERCHANTABILITY OR FITNESS FOR A PARTICULAR PURPOSE. Your use of the translations is subject to all use restrictions contained in your Electronic Products License Agreement and by using the translation functionality you agree to forgo any and all claims against ProQuest or its licensors for your use of the translation functionality and any output derived there from. Hide full disclaimer
Details
; Govender, Indira 2 ; Spinelli, Matthew 3
; Smit, Theresa 1
; Cibane, Siyabonga 1 ; Zwane, Mlungisi 1 ; Phakathi, Njabulo 1 ; Krows, Meighan 4 ; Nkosi, Busisiwe 5 ; Seeley, Janet 6
; Barnabas, Ruanne V. 7 ; Siedner, Mark J. 8 ; Moshabela, Mosa 9 ; Celum, Connie 10
; Grant, Alison 2 ; Gandhi, Monica 3
; Shapiro, Adrienne E. 10
1 Africa Health Research Institute, Somkhele, South Africa
2 Africa Health Research Institute, Somkhele, South Africa, London School of Hygiene & Tropical Medicine, London, UK
3 Division of HIV, Infectious Diseases, and Global Medicine, University of California San Francisco, San Francisco, California, USA
4 Department of Global Health, University of Washington, Seattle, Washington, USA
5 University of Toledo, Toledo, Ohio, USA
6 Africa Health Research Institute, Somkhele, South Africa, London School of Hygiene & Tropical Medicine, London, UK, University of KwaZulu‐Natal, Durban, South Africa
7 Division of Infectious Diseases, Massachusetts General Hospital, Boston, Massachusetts, USA, Harvard Medical School, Boston, Massachusetts, USA
8 Africa Health Research Institute, Somkhele, South Africa, University of KwaZulu‐Natal, Durban, South Africa, Division of Infectious Diseases, Massachusetts General Hospital, Boston, Massachusetts, USA, Harvard Medical School, Boston, Massachusetts, USA
9 University of KwaZulu‐Natal, Durban, South Africa
10 Department of Global Health, University of Washington, Seattle, Washington, USA, Division of Allergy & Infectious Diseases, Department of Medicine, University of Washington, Seattle, Washington, USA