Your search keyword '"Peeling RW"' showing total 293 results

1. Point-of-care testing and treatment of sexually transmitted and genital infections to improve birth outcomes in high-burden, low-resource settings (WANTAIM): a pragmatic cluster randomised crossover trial in Papua New Guinea

Author

Riddell, MA, Vallely, LM, Mengi, A, Badman, SG, Low, N, Wand, H, Bolnga, JW, Babona, D, Mola, GDL, Wiseman, V, Kelly-Hanku, A, Homer, CSE, Morgan, C, Luchters, S, Whiley, DM, Robinson, LJ, Au, L, Pukai-Gani, I, Laman, M, Kariwiga, G, Toliman, PJ, Batura, N, Tabrizi, SN, Rogerson, SJ, Garland, SM, Guy, RJ, Peeling, RW, Pomat, WS, Kaldor, JM, Vallely, AJB, Riddell, MA, Vallely, LM, Mengi, A, Badman, SG, Low, N, Wand, H, Bolnga, JW, Babona, D, Mola, GDL, Wiseman, V, Kelly-Hanku, A, Homer, CSE, Morgan, C, Luchters, S, Whiley, DM, Robinson, LJ, Au, L, Pukai-Gani, I, Laman, M, Kariwiga, G, Toliman, PJ, Batura, N, Tabrizi, SN, Rogerson, SJ, Garland, SM, Guy, RJ, Peeling, RW, Pomat, WS, Kaldor, JM, and Vallely, AJB

Abstract

BACKGROUND: Chlamydia trachomatis, Neisseria gonorrhoeae, Trichomonas vaginalis, and bacterial vaginosis have been associated with adverse maternal and perinatal outcomes, but there is conflicting evidence on the benefits of antenatal screening and treatment for these conditions. We aimed to determine the effect of antenatal point-of-care testing and immediate treatment of C trachomatis, N gonorrhoeae, T vaginalis, and bacterial vaginosis on preterm birth, low birthweight, and other adverse maternal and perinatal outcomes compared with current standard of care, which included symptom-based treatment without laboratory confirmation. METHODS: In this pragmatic cluster randomised crossover trial, we enrolled women (aged ≥16 years) attending an antenatal clinic at 26 weeks' gestation or earlier (confirmed by obstetric ultrasound), living within approximately 1 h drive of a study clinic, and able to provide reliable contact details at ten primary health facilities and their catchment communities (clusters) in Papua New Guinea. Clusters were randomly allocated 1:1 to receive either the intervention or control (standard care) in the first phase of the trial. Following an interval (washout period) of 2-3 months at the end of the first phase, each cluster crossed over to the other group. Randomisation was stratified by province. Individual participants were informed about trial group allocation only after completing informed consent procedures. The primary outcome was a composite of preterm birth (livebirth before 37 weeks' gestation), low birthweight (<2500 g), or both, analysed according to the intention-to-treat population. This study is registered with ISRCTN Registry, ISRCTN37134032, and is completed. FINDINGS: Between July 26, 2017, and Aug 30, 2021, 4526 women were enrolled (2210 [63·3%] of 3492 women in the intervention group and 2316 [62·8%] of 3687 in the control group). Primary outcome data were available for 4297 (94·9%) newborn babies of 4526 women. The proporti

Published

2024

2. Lateral flow test engineering and lessons learned from COVID-19

Author

Budd J, Miller BS, Weckman NE, Cherkaoui D, Huang D, Decruz AT, Fongwen N, Han G, Broto M, Estcourt CS, Gibbs J, Pillay D, Sonnenberg P, Meurant R, Thomas MR, Keegan N, Stevens MM, Nastouli E, Topol EJ, Johnson AM, Shahmanesh M, Ozcan A, Collins JJ, Suarez MF, Rodriguez B, Peeling RW, McKendry RA

Published

2023

3. Impact of a Group-Based Video and Interactive Group Session Addressing Diarrheal Disease, Helminthic and Schistosomiasis Infections, Hypertension and Diabetes on Short and Long-Term Improvement in Knowledge and Healthy Behaviors in Seroconcordant HIV-Negative Zambian Couples

Author

Sharkey T, Parker R, Wall KM, Malama K, Kilembe W, Inambao M, Tichacek A, Kwok C, Ahmed N, Burke R, Peeling RW, and Allen S

Published

2022

4. Point-of-care testing and treatment of sexually transmitted and genital infections during pregnancy in Papua New Guinea (WANTAIM trial): protocol for an economic evaluation alongside a cluster-randomised trial

Author

Batura, N, Saweri, OPM, Vallely, A, Pomat, W, Homer, C, Guy, R, Luchters, S, Mola, G, Vallely, LM, Morgan, C, Kariwiga, G, Wand, H, Rogerson, S, Tabrizi, SN, Whiley, DM, Low, N, Peeling, RW, Siba, PM, Riddell, M, Laman, M, Bolnga, J, Robinson, LJ, Morewaya, J, Badman, S, Kelly-Hanku, A, Toliman, PJ, Peter, W, Peach, E, Garland, S, Kaldor, J, Wiseman, V, Batura, N, Saweri, OPM, Vallely, A, Pomat, W, Homer, C, Guy, R, Luchters, S, Mola, G, Vallely, LM, Morgan, C, Kariwiga, G, Wand, H, Rogerson, S, Tabrizi, SN, Whiley, DM, Low, N, Peeling, RW, Siba, PM, Riddell, M, Laman, M, Bolnga, J, Robinson, LJ, Morewaya, J, Badman, S, Kelly-Hanku, A, Toliman, PJ, Peter, W, Peach, E, Garland, S, Kaldor, J, and Wiseman, V

Abstract

INTRODUCTION: Left untreated, sexually transmitted and genital infections (henceforth STIs) in pregnancy can lead to serious adverse outcomes for mother and child. Papua New Guinea (PNG) has among the highest prevalence of curable STIs including syphilis, chlamydia, gonorrhoea, trichomoniasis and bacterial vaginosis, and high neonatal mortality rates. Diagnosis and treatment of these STIs in PNG rely on syndromic management. Advances in STI diagnostics through point-of-care (PoC) testing using GeneXpert technology hold promise for resource-constrained countries such as PNG. This paper describes the planned economic evaluation of a cluster-randomised cross-over trial comparing antenatal PoC testing and immediate treatment of curable STIs with standard antenatal care in two provinces in PNG. METHODS AND ANALYSIS: Cost-effectiveness of the PoC intervention compared with standard antenatal care will be assessed prospectively over the trial period (2017-2021) from societal and provider perspectives. Incremental cost-effectiveness ratios will be calculated for the primary health outcome, a composite measure of the proportion of either preterm birth and/or low birth weight; for life years saved; for disability-adjusted life years averted; and for non-health benefits (financial risk protection and improved health equity). Scenario analyses will be conducted to identify scale-up options, and budget impact analysis will be undertaken to understand short-term financial impacts of intervention adoption on the national budget. Deterministic and probabilistic sensitivity analysis will be conducted to account for uncertainty in key model inputs. ETHICS AND DISSEMINATION: This study has ethical approval from the Institutional Review Board of the PNG Institute of Medical Research; the Medical Research Advisory Committee of the PNG National Department of Health; the Human Research Ethics Committee of the University of New South Wales; and the Research Ethics Committee of the London S

Published

2021

5. The potential for quality assurance systems to save costs and lives: the case of early infant diagnosis of HIV

Author

Terris-Prestholt, F, Boeras, D, Ong, JJ, Torres-Rueda, S, Cassim, N, Mbengue, MAS, Mboup, S, Mwau, M, Munemo, E, Nyegenye, W, Odhiambo, CO, Dabula, P, Sandstrom, P, Sarr, M, Simbi, R, Stevens, W, Tucker, JD, Vickerman, P, Ciaranello, A, Peeling, RW, Terris-Prestholt, F, Boeras, D, Ong, JJ, Torres-Rueda, S, Cassim, N, Mbengue, MAS, Mboup, S, Mwau, M, Munemo, E, Nyegenye, W, Odhiambo, CO, Dabula, P, Sandstrom, P, Sarr, M, Simbi, R, Stevens, W, Tucker, JD, Vickerman, P, Ciaranello, A, and Peeling, RW

Abstract

OBJECTIVES: Scaling up of point-of-care testing (POCT) for early infant diagnosis of HIV (EID) could reduce the large gap in infant testing. However, suboptimal POCT EID could have limited impact and potentially high avoidable costs. This study models the cost-effectiveness of a quality assurance system to address testing performance and screening interruptions, due to, for example, supply stockouts, in Kenya, Senegal, South Africa, Uganda and Zimbabwe, with varying HIV epidemics and different health systems. METHODS: We modelled a quality assurance system-raised EID quality from suboptimal levels: that is, from misdiagnosis rates of 5%, 10% and 20% and EID testing interruptions in months, to uninterrupted optimal performance (98.5% sensitivity, 99.9% specificity). For each country, we estimated the 1-year impact and cost-effectiveness (US$/DALY averted) of improved scenarios in averting missed HIV infections and unneeded HIV treatment costs for false-positive diagnoses. RESULTS: The modelled 1-year costs of a national POCT quality assurance system range from US$ 69 359 in South Africa to US$ 334 341 in Zimbabwe. At the country level, quality assurance systems could potentially avert between 36 and 711 missed infections (i.e. false negatives) per year and unneeded treatment costs between US$ 5808 and US$ 739 030. CONCLUSIONS: The model estimates adding effective quality assurance systems are cost-saving in four of the five countries within the first year. Starting EQA requires an initial investment but will provide a positive return on investment within five years by averting the costs of misdiagnoses and would be even more efficient if implemented across multiple applications of POCT.

Published

2020

6. Sensitivity requirements for the point of care diagnosis of Chlamydia trachomatis and Neisseria gonorrhoeae in women

Author

Vickerman, P, Watts, C, Alary, M, Mabey, D, and Peeling, RW

Subjects

Neisseria gonorrhoeae -- Diagnosis -- Models -- Methods, Sexually transmitted diseases -- Diagnosis, Chlamydia trachomatis -- Diagnosis -- Models -- Methods, Health, Diagnosis, Evaluation, Models, Methods

Abstract

Background/objectives: Most current tests for Neisseria gonorrhoeae and Chlamydia trachomatis require the support of a laboratory, and results are not usually available before the patient has left the clinic. This [...]

Published

2003

7. Chlamydia trachomatis and invasive cervical cancer: a pooled analysis of the IARC multicentric case-control study

Author

Smith, J.S., Bosetti, C, Munoz, N., Herrero, R, Bosch, F.X., Eluf-Neto, J, Meijer, C.J.L.M., van den Brule, AJ, Franceschi, S, Peeling, RW, and VU University medical center

Published

2004

8. Dengue: a continuing global threat

Author

Guzman, MG, Halstead, SB, Artsob, H, Buchy, P, Farrar, J, Gubler, DJ, Hunsperger, E, Kroeger, A, Margolis, HS, Martínez, E, Nathan, MB, Pelegrino, JL, Simmons, C, Yoksan, S, Peeling, RW, Guzman, MG, Halstead, SB, Artsob, H, Buchy, P, Farrar, J, Gubler, DJ, Hunsperger, E, Kroeger, A, Margolis, HS, Martínez, E, Nathan, MB, Pelegrino, JL, Simmons, C, Yoksan, S, and Peeling, RW

Abstract

Dengue fever and dengue haemorrhagic fever are important arthropod-borne viral diseases. Each year, there are ∼50 million dengue infections and ∼500,000 individuals are hospitalized with dengue haemorrhagic fever, mainly in Southeast Asia, the Pacific and the Americas. Illness is produced by any of the four dengue virus serotypes. A global strategy aimed at increasing the capacity for surveillance and outbreak response, changing behaviours and reducing the disease burden using integrated vector management in conjunction with early and accurate diagnosis has been advocated. Antiviral drugs and vaccines that are currently under development could also make an important contribution to dengue control in the future.

Published

2010

9. Chlamydia pneumoniae serology: interlaboratory variation in microimmunofluorescence assay results.

Author

Peeling, RW, Wang, SP, Grayston, JT, Blasi, F, Boman, J, Clad, A, Freidank, H, Gaydos, CA, Gnarpe, J, Hagiwara, T, Jones, RB, Orfila, J, Persson, K, Puolakkainen, M, Saikku, P, Schachter, J, Peeling, RW, Wang, SP, Grayston, JT, Blasi, F, Boman, J, Clad, A, Freidank, H, Gaydos, CA, Gnarpe, J, Hagiwara, T, Jones, RB, Orfila, J, Persson, K, Puolakkainen, M, Saikku, P, and Schachter, J

Published

2000

10. Screening for Sexually Transmitted Infection Pathogens in Semen Samples

Author

Peeling, RW, primary and Embree, J, additional

Published

2005

11. Point-of-care testing for sexually transmitted infections: recent advances and implications for disease control.

Author

Tucker JD, Bien CH, Peeling RW, Tucker, Joseph D, Bien, Cedric H, and Peeling, Rosanna W

Published

2013

12. Performance of serological tests for syphilis in sexually transmitted diseases clinics in Guangxi Autonomous Region, China: implications for syphilis surveillance and control.

Author

Yin YP, Wei WH, Wang HC, Zhu BY, Yu YH, Chen XS, Peeling RW, Cohen MS, Yin, Yue-Ping, Wei, Wan-Hui, Wang, Hong-Chun, Zhu, Bang-Yong, Yu, Yan-Hua, Chen, Xiang-Sheng, Peeling, Rosanna W, and Cohen, Myron S

Abstract

Background: China is experiencing a growing syphilis epidemic. Individuals are currently screened and cases are confirmed using traditional serological testing methods.Methods: A total of 11 558 serum specimens from patients at 14 sexually transmitted diseases (STD) clinics at provincial, prefecture and county levels in Guangxi Autonomous Region were tested at local clinics using the toluidine red unheated serum test (TRUST) and the SD Bioline Syphilis 3.0 Treponema Pallidum (SD-TP) test and then transported to the National STD Reference Laboratory for TRUST and confirmatory Treponema pallidum particle assay (TPPA) testing.Results: In local clinics, 13.2% of specimens were TRUST positive and 12.8% were TRUST and SD-TP positive. At the Reference Laboratory, 15.4% of specimens were TRUST positive and 11.8% were TRUST and TPPA positive. Local clinics showed a significantly higher prevalence of active syphilis compared with results from the Reference Laboratory (12.8 v. 11.8%, chi(2) = 4.59, P = 0.03). The local TRUST tests had consistent results with Reference Laboratory tests qualitatively among 96.2% of the specimens and quantitatively among 95.5% of the specimens. The algorithm of TRUST screening and then SD-TP confirmation among positive TRUST specimens at local STD clinics had 96.6% sensitivity and 99.3% specificity in diagnosing active syphilis compared with the 'gold standard' based on TRUST and TPPA positivity at the Reference Laboratory (positive predictive value 95.1% and negative predictive value 99.5%).Conclusion: The TRUST screening and SD-TP confirmation in combination can be used at local STD clinics for the efficient diagnosis of serologically active syphilis. However, continuing capacity building and quality assurance remain critical in ensuring the quality of syphilis diagnosis at local clinics. [ABSTRACT FROM AUTHOR]

Published

2009

13. Airflow limitation, asthma, and Chlamydia pneumoniae-specific heat shock protein 60.

Author

Hahn DL and Peeling RW

Published

2008

14. Diagnostic tools for preventing and managing maternal and congenital syphilis: an overview.

Author

Peeling RW and Ye H

Abstract

Syphilis is a major cause of adverse outcomes in pregnancy in developing countries. Fetal death and morbidity due to congenital syphilis are preventable if infected mothers are identified and treated appropriately by the middle of the second trimester. Most pregnant women with syphilis are asymptomatic and can only be identified through serological screening. Non-treponemal tests, such as the rapid plasma reagin (RPR) test, are sensitive, simple to perform, and inexpensive. However, they have often not been available at primary health-care settings because they required cold storage for reagents and electricity to operate a rotator. Additionally, as many as 28% of positive RPR results in pregnant women are biological false positives. Confirmatory assays are usually available only in reference laboratories. Technological advances have resulted in improved serodiagnostic tools for syphilis. New enzyme immunoassays are available for surveillance and for large-scale screening programmes. Decentralized antenatal screening with on-site confirmation is now possible since new RPR reagents that are stable at room temperature have become commercially available, as have solar-powered rotators and simple, rapid point-of-care treponemal tests that use whole blood and do not require electricity or equipment. These will be valuable tools for preventing or eliminating congenital syphilis. The development of a non-invasive rapid treponemal test that distinguishes between active and past infections remains a high priority in areas where syphilis is endemic. Copyright © 2004 World Health Organization [ABSTRACT FROM AUTHOR]

Published

2004

15. Surveillance for outbreaks of respiratory tract infections in nursing homes.

Author

Loeb M, McGeer A, McArthur M, Peeling RW, Petric M, and Simor AE

Published

2000

16. Avoiding HIV and dying of syphilis.

Author

Peeling RW, Mabey D, Fitzgerald DW, and Watson-Jones D

Published

2004

17. Global health: syphilis control -- a continuing challenge.

Author

Hook EW III and Peeling RW

Published

2004

18. Point-of-care tests to strengthen health systems and save newborn lives: the case of syphilis.

Author

Mabey DC, Sollis KA, Kelly HA, Benzaken AS, Bitarakwate E, Changalucha J, Chen XS, Yin YP, Garcia PJ, Strasser S, Chintu N, Pang T, Terris-Prestholt F, Sweeney S, Peeling RW, Mabey, David C, Sollis, Kimberly A, Kelly, Helen A, Benzaken, Adele S, and Bitarakwate, Edward

Published

2012

19. Chlamydia pneumoniae serology: interlaboratory variation in microimmunofluorescence assay results.

Author

Peeling RW, Wang S, Grayston JT, Blasi F, Boman J, Clad A, Freidank H, Gaydos CA, Gnarpe J, Hagiwara T, Jones RB, Orfila J, Persson K, Puolakkainen M, Saikku P, and Schachter J

Abstract

The lack of standardization in chlamydia serology has made interpretation of published data difficult. This study was initiated to determine the extent of interlaboratory variation of microimmunofluorescence (MIF) test results for the serodiagnosis of Chlamydia pneumoniae infections. Identical panels of 22 sera were sent to 14 laboratories in eight countries for the determination of IgG and IgM antibodies by MIF. Although there was extensive variation in the numeric titer values, the overall percentage agreement with the reference standard titers from the University of Washington was 80%. For results by serodiagnostic category, the best agreement was for four-fold rise in IgG titers, while the lowest agreement was for negative or low IgG titers. Agreement for IgM titers was 50%-95%. Four laboratories failed to discern false-positive IgM titers possibly because of the presence of rheumatoid factor. Further studies are underway to determine the source of interlaboratory variation for the MIF test. [ABSTRACT FROM AUTHOR]

Published

2000

20. Head-to-head comparison of accuracy of a rapid point-of-care HIV test with oral versus whole-blood specimens: a systematic review and meta-analysis.

Author

Pai NP, Balram B, Shivkumar S, Martinez-Cajas JL, Claessens C, Lambert G, Peeling RW, and Joseph L

Published

2012

21. Mass treatment with single-dose azithromycin for trachoma.

Author

Solomon AW, Holland MJ, Alexander NDE, Massae PA, Aguirre A, Natividad-Sancho A, Molina S, Safari S, Shao JF, Courtright P, Peeling RW, West SK, Bailey RL, Foster A, Mabey DCW, Solomon, Anthony W, Holland, Martin J, Alexander, Neal D E, Massae, Patrick A, and Aguirre, Aura

Abstract

Background: Trachoma, caused by repeated ocular infection with Chlamydia trachomatis, is an important cause of blindness. Current recommended dosing intervals for mass azithromycin treatment for trachoma are based on a mathematical model.Methods: We collected conjunctival swabs for quantitative polymerase-chain-reaction assay of C. trachomatis before and 2, 6, 12, 18, and 24 months after mass treatment with azithromycin in a Tanzanian community in which trachoma was endemic. For ethical reasons, at 6, 12, and 18 months, we gave tetracycline eye ointment to residents who had clinically active trachoma.Results: At baseline, 956 of 978 residents (97.8 percent) received either one oral dose of azithromycin or (if azithromycin was contraindicated) a course of tetracycline eye ointment. The prevalence of infection fell from 9.5 percent before mass treatment to 2.1 percent at 2 months and 0.1 percent at 24 months. The quantitative burden of ocular C. trachomatis infection in the community was 13.9 percent of the pretreatment level at 2 months and 0.8 percent at 24 months. At each time point after baseline, over 90 percent of the total community burden of C. trachomatis infection was found among subjects who had been positive the previous time they were tested.Conclusions: The prevalence and intensity of infection fell dramatically and remained low for two years after treatment. One round of very-high-coverage mass treatment with azithromycin, perhaps aided by subsequent periodic use of tetracycline eye ointment for persons with active disease, can interrupt the transmission of ocular C. trachomatis infection. [ABSTRACT FROM AUTHOR]

Published

2004

22. Strategies for control of trachoma: observational study with quantitative PCR.

Author

Solomon AW, Holland MJ, Burton MJ, West SK, Alexander NDE, Aguirre A, Massae PA, Mkocha H, Muñoz B, Johnson GJ, Peeling RW, Bailey RL, Foster A, and Mabey DCW

Published

2003

23. Reproductive-tract infections in women in low-income, low-prevalence situations: assessment of syndromic management in Matlab, Bangladesh.

Author

Hawkes S, Morison L, Foster S, Gausia K, Chakraborty J, Peeling RW, Mabey D, Hawkes, S, Morison, L, Foster, S, Gausia, K, Chakraborty, J, Peeling, R W, and Mabey, D

Abstract

Background: In the control of reproductive-tract infections, including sexually transmitted infections (STIs), in low-income and middle-income countries, WHO recommends syndromic management for individuals with symptoms. This intervention was initially developed in areas where prevalence of such infections is high. We investigated the clinical effectiveness and cost of this approach among a group of women with a low prevalence of infection.Methods: During a 5-month period, we investigated all women complaining of abnormal vaginal discharge and seeking care at maternal and child health/family-planning centres in Matlab, Bangladesh, for the presence of laboratory-diagnosed reproductive-tract infections and STIs. Syndromic diagnoses made by trained health-care workers were compared with laboratory diagnosis of infection. We then calculated the costs of treating women by means of the recommended WHO algorithm and an adapted algorithm incorporating use of a speculum and simple diagnostic tests.Findings: The prevalence of endogenous infections among 320 women seen was 30%. Cervical infections (Neisseria gonorrhoeae and Chlamydia trachomatis) were found in only three women. The WHO algorithm had a high sensitivity (100%) but a low specificity (zero for bacterial vaginosis, candida, and Trichomonas vaginalis). The speculum-based algorithm had a low sensitivity (between zero and 59%) but a higher specificity (79-97%). Between 36% and 87% of costs would have been spent on uninfected women.Interpretation: The high rate of overtreatment in the population studied carries both financial and social costs--the latter in potentially exposing women misdiagnosed as having an STI to threats of domestic disruption or even violence. We make recommendations for management programmes in areas of low STI prevalence and low income. [ABSTRACT FROM AUTHOR]

Published

1999

24. The Pathogenesis and Clinical Management of Dengue

Author

Whitehorn, J, Peeling, RW, Simmons, C, and Wills, B

Subjects

3. Good health

Abstract

Dengue is an arboviral disease that exerts a significant public health burden on the tropical\ud world. Currently there is no available vaccine or specific therapeutic. My reviews show that\ud our understanding of dengue pathogenesis, transmission dynamics and optimal case\ud management is incomplete. The work presented in this thesis is a compilation of expert\ud reviews/perspectives and primary research that addresses some of these knowledge gaps.\ud Understanding dengue pathogenesis and in particular, risk factors for progression to severe\ud dengue, is an important priority to reduce morbidity and mortality, especially in young\ud children. Genetic variants of the MICB and PLCE genes have been shown to be associated\ud with severe dengue. I tested the hypothesis that these variants are also associated with less\ud severe dengue infection and with higher early viraemia levels in two studies involving the\ud genotyping of 3961 and 2742 dengue cases respectively. My studies showed that these\ud genetic variants are associated with less severe but clinically apparent dengue infection but\ud showed no evidence of an association with higher viraemia levels. The functional basis of\ud these susceptibility mutations remains unclear.\ud Dengue transmission dynamics are shaped by the prevalence of the permissive vectors,\ud Aedes aegypti and Aedes albopictus. My research hypothesis was that susceptibility and\ud transmission of dengue might differ between the two species. I conducted a clinical study that\ud compared the susceptibility of Ae. aegypti and Ae. albopictus to both initial and disseminated\ud dengue after direct blood feeding experiments on viraemic patients. This work showed that\ud both mosquito types were equally susceptible to initial infection with dengue but that Ae.\ud albopictus was less likely to develop salivary infection, and, thus, an infectious phenotype.\ud These results have important implications for the development of dengue transmission\ud models, especially in areas of dengue emergence where the influence of Ae. albopictus is\ud thought to be greatest. In addition, the results confirm the central importance of patient\ud plasma viraemia in causing successful DENV transmission, suggesting that reducing this\ud through the use of antivirals could potentially reduce transmission.\ud Clinical management of dengue patients remains an enormous challenge. Statins are rational\ud candidate drugs for dengue because of their previously identified positive influence on\ud vascular endothelial function. I conducted a clinical trial of lovastatin therapy in adult dengue\ud patients. The trial showed that lovastatin was safe and well tolerated in dengue patients but it\ud did not show any positive effects on the kinetics of viraemia or on any of the pre-specified\ud clinical or laboratory features. I conducted a survey of platelet management in 20 countries\ud and found a wide variety of approaches to the use of platelets in dengue underscoring the\ud need for prospective clinical trials to inform evidence in this area. To reduce the large sample\ud size normally required for the development of dengue therapeutics, I considered the use of a\ud human dengue infection model in dengue drug development. This model has the potential to\ud a game-changer in drug development and in the design of future trials.

Published

2015

25. Dried blood spots to improve patient management in remote settings

Author

Smit, Pw, Peeling, Rw, and Mabey, D

Abstract

The overall aim of the thesis was to assess the feasibility and utility of using blood collected on filter paper, dried blood spots (DBS), to improve patient management in remote settings. The use of DBS was evaluated for patient monitoring, quality assurance of point of care testing, and for surveillance to improve syndromic management.\ud Systematic literature reviews, laboratory studies, and implementation of DBS based diagnostics were performed to answer these objectives. DBS is a feasible alternative to plasma in monitoring viral load in HIV patients on treatment. The type of filter paper, collection, storage and processing methods are critically important to obtain valid results for monitoring HIV. A DBS protocol was evaluated for syphilis serology, giving an adjusted sensitivity and specificity of 97.7% and 99.4% compared to plasma. DBS was implemented as quality assurance for Point-of-care test (PaCT), which showed that health worker proficiency varied significantly between clinics, stressing the importance of quality assurance.\ud Laboratory evaluations revealed the possibility of obtaining adequate sensitivities to detect febrile illnesses; malaria, dengue, leptospira, B.bacilliformis, and chikungunya, but not for R. typhi and O.tsutsugamushi by DBS. When implemented in Peru, a local B.bacilliformis outbreak was identified which proved that DBS was more sensitive than the current surveillance method. The goal of this research was to determine whether DBS can improve patient management in remote settings. As new technologies are being developed rapidly, the use of simple and robust tools such as filter paper has continued to provide an affordable and reliable solution for clinical sample collection. While DBS is not the best sampling method, it is the simplicity and robustness that makes it useful in remote settings. This research showed that DBS can be used for monitoring HIV patient on antiretroviral therapy, the quality of syphilis diagnosis, and determining the major causes of fever in children to improve recommendations for syndromic management.

Published

2013

26. Diagnostic yield as an important metric for the evaluation of novel tuberculosis tests: rationale and guidance for future research.

Author

Broger T, Marx FM, Theron G, Marais BJ, Nicol MP, Kerkhoff AD, Nathavitharana R, Huerga H, Gupta-Wright A, Kohli M, Nichols BE, Muyoyeta M, Meintjes G, Ruhwald M, Peeling RW, Pai NP, Pollock NR, Pai M, Cattamanchi A, Dowdy DW, Dewan P, and Denkinger CM

Subjects

Humans, Diagnostic Tests, Routine, Sputum microbiology, Tuberculosis diagnosis

Abstract

Better access to tuberculosis testing is a key priority for fighting tuberculosis, the leading cause of infectious disease deaths in people. Despite the roll-out of molecular WHO-recommended rapid diagnostics to replace sputum smear microscopy over the past decade, a large diagnostic gap remains. Of the estimated 10·6 million people who developed tuberculosis globally in 2022, more than 3·1 million were not diagnosed. An exclusive focus on improving tuberculosis test accuracy alone will not be sufficient to close the diagnostic gap for tuberculosis. Diagnostic yield, which we define as the proportion of people in whom a diagnostic test identifies tuberculosis among all people we attempt to test for tuberculosis, is an important metric not adequately explored. Diagnostic yield is particularly relevant for subpopulations unable to produce sputum such as young children, people living with HIV, and people with subclinical tuberculosis. As more accessible non-sputum specimens (eg, urine, oral swabs, saliva, capillary blood, and breath) are being explored for point-of-care tuberculosis testing, the concept of yield will be of growing importance. Using the example of urine lipoarabinomannan testing, we illustrate how even tests with limited sensitivity can diagnose more people with tuberculosis if they enable increased diagnostic yield. Using tongue swab-based molecular tuberculosis testing as another example, we provide definitions and guidance for the design and conduct of pragmatic studies that assess diagnostic yield. Lastly, we show how diagnostic yield and other important test characteristics, such as cost and implementation feasibility, are essential for increased effective population coverage, which is required for optimal clinical care and transmission impact. We are calling for diagnostic yield to be incorporated into tuberculosis test evaluation processes, including the WHO Grading of Recommendations, Assessment, Development, and Evaluations process, providing a crucial real-life implementation metric that complements traditional accuracy measures., Competing Interests: Declaration of interests TB reports patent applications in the field of tuberculosis detection and is a shareholder of Avelo. MP serves as an adviser for non-profits such as the Bill & Melinda Gates Foundation, FIND, WHO, and the Stop TB Partnership. All other authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2024

27. Clinic-based evaluation of point-of-care dual HIV/syphilis rapid diagnostic tests at primary healthcare antenatal facilities in South Africa and Zambia.

Author

Kularatne R, Blondeel K, Kasaro M, Maseko V, Bosomprah S, Silva R, Laverty M, Kurbonov F, Mirandola M, and Peeling RW

Subjects

Humans, Zambia epidemiology, Female, Pregnancy, South Africa epidemiology, Adult, Young Adult, Adolescent, Point-of-Care Systems, Primary Health Care, Point-of-Care Testing, Prevalence, Mass Screening methods, Prenatal Care, Diagnostic Tests, Routine methods, Rapid Diagnostic Tests, Syphilis diagnosis, Syphilis epidemiology, HIV Infections diagnosis, HIV Infections epidemiology, Sensitivity and Specificity, Pregnancy Complications, Infectious diagnosis, Pregnancy Complications, Infectious epidemiology

Abstract

Background: Southern African countries have the largest global burden of HIV and syphilis, with a high prevalence among women of reproductive age. Although antenatal screening is standard of care, syphilis screening has generally lagged behind HIV screening. We aimed to evaluate the performance and operational characteristics of two commercial dual HIV/syphilis point-of-care tests (POCTs) for simultaneous maternal HIV/syphilis screening., Methods: A clinic-based evaluation of dual HIV/syphilis POCTs (SD Bioline and Chembio) was conducted at five primary healthcare centres (PHCs) in South Africa and Zambia. POCT results using capillary fingerprick blood were compared to reference laboratory syphilis and HIV serological assays., Results: Three thousand four hundred twelve consenting pregnant women aged ≥ 18 years were enrolled. The prevalence of treponemal antibody seropositivity and HIV infection ranged from 3.7 to 9.9% (n = 253) and 17.8 to 21.3% (n = 643), respectively. Pooled sensitivity for syphilis compared to the reference assay was 66.0% (95%CI 57.7-73.4) with SD Bioline and 67.9% (95%CI 58.2-76.3) with Chembio. Pooled specificity for syphilis was above 98% with both POCTs. The sensitivities of SD Bioline and Chembio assays were 78.0% (95%CI 68.6-85.7) and 81.0% (95%CI 71.9-88.2), respectively compared to an active syphilis case definition of treponemal test positive with a rapid plasma reagin titre of ≥ 8. The negative predictive values (NPVs) based on various prevalence estimates for syphilis with both assays ranged from 97 to 99%. The pooled sensitivity for HIV was 92.1% (95%CI 89.4-94.2) with SD Bioline; and 91.5% (95%CI 88.2-93.9) with Chembio. The pooled specificities for HIV were 97.2% (95%CI 94.8-98.5) with SD Bioline and 96.7% (95%CI 95.1-97.8) with Chembio. The NPV based on various prevalence estimates for HIV with both assays was approximately 98%. Most participating women (91%) preferred dual POCTs over two single POCTs for HIV and syphilis, and healthcare providers gave favourable feedback on the utility of both assays at PHC level., Conclusions: Based on the need to improve antenatal screening coverage for syphilis, dual HIV/syphilis POCTs could be effectively incorporated into antenatal testing algorithms to enhance efforts towards elimination of mother-to-child transmission of these infections., (© 2024. The Author(s).)

Published

2024

28. Standardised protocol for a prospective international multicentre clinical-based evaluation of point-of-care tests for the screening of genital and extragenital chlamydial and gonococcal infections in men who have sex with men and for the screening of genital chlamydial, gonococcal and Trichomonas vaginalis infections in at risk women.

Author

Cordioli M, Gios L, Mirandola M, Zorzi A, Barbara C, Padovese V, Hancali A, Oumzi H, Kularatne R, Jiang TT, Caceres CF, Vargas S, Alvarez CS, Camey E, Peeling RW, Unemo M, Ballard R, Blondeel K, Kiarie J, Thwin SS, and Toskin I

Subjects

Humans, Male, Female, Prospective Studies, Mass Screening methods, Trichomonas vaginalis isolation & purification, Sexually Transmitted Diseases diagnosis, Trichomonas Vaginitis diagnosis, Trichomonas Vaginitis epidemiology, Multicenter Studies as Topic, Sensitivity and Specificity, Adult, Point-of-Care Systems, Chlamydia Infections diagnosis, Gonorrhea diagnosis, Point-of-Care Testing, Homosexuality, Male

Abstract

Introduction: In 2016, WHO estimated there were roughly 374 million new infections among adults of the following four curable sexually transmitted infections (STIs): chlamydia (caused by Chlamydia trachomatis (CT)), gonorrhoea ( Neisseria gonorrhoeae (NG)), syphilis ( Treponema pallidum ) and trichomoniasis ( Trichomonas vaginalis (TV)). Accurate point-of-care tests (POCTs) for screening of genital and extragenital CT, NG and TV infections are of great value and have been developed during recent decade. Several tests are commercially available and have shown encouraging performance compared with 'gold-standard' reference tests in laboratory-based studies. However, there is limited data on their clinical performance, including at the POC. Key populations, such as men who have sex with men (MSM), are at higher risk of these STIs at genital and extragenital sites and these STIs are often asymptomatic, especially in extragenital sites and in women. We will conduct a clinical-based evaluation to assess the performance characteristics and acceptability to end-users of molecular-based diagnostic technology for POC/near patient use of the Xpert CT/NG (Cepheid, Sunnyvale, California, USA) test for screening of genital, anorectal and pharyngeal CT and NG infections in MSM and the Xpert CT/NG and Xpert TV (Cepheid, Sunnyvale, California, USA) for screening of genital CT, NG and TV among women at risk for these STIs compared with gold-standard reference nucleic acid amplification tests. This master protocol outlines the overall research approach that will be used in seven countries., Method and Analyses: Consecutive MSM and women at risk presenting at the clinical sites in high, and low- and middle-income countries will be enrolled. The POCTs to be evaluated are Xpert CT/NG and Xpert TV. All procedures will be carried out by trained healthcare staff and tests performed in strict accordance with the manufacturer's instructions. The sensitivity, specificity, positive and negative predictive values for each POCT will be calculated. The study is ongoing with recruitment expected to be completed in all countries by mid-2022 to late-2022., Ethics and Dissemination: Prior to enrolment, this core protocol was independently peer-reviewed and approved by the research project review panel (RP2) of the WHO Department of Sexual and Reproductive Health and Research and by the WHO Ethics Review Committee (ERC). The core protocol has been slightly adapted accordingly to individual countries and adaptations approved by both RP2 and ERC, as well as all relevant institutional review boards at each participating site. Results will be disseminated through peer-reviewed journals and presented at relevant national/international conferences., Competing Interests: Competing interests: The POCT manufacturer discloses and furnishes free of charge to WHO the information and sufficient quantities of the product(s) in order to enable this evaluation as part of the WHO/RHR STI POC initiative. WHO is entitled to evaluate and publish the trial results, and to exclusively control this evaluation and the content of the aforesaid publication. WHO shall submit any proposed publication to the POCT manufacturer for review, comments received will be considered in good faith, but the decision to publish rests with WHO., (© World Health Organization 2024. Licensee BMJ.)

Published

2024

29. HIV Diagnostics and Vaccines: It Takes Two to Tango.

Author

Colón W, Oriol-Mathieu V, Hural J, Hattingh L, Adungo F, Lagatie O, Lavreys L, Allen M, Anzala O, Espy N, Fransen K, Garcia PJ, Maciel M Jr, Murtagh M, Peel SA, Peeling RW, Tan LLJ, Warren M, Pau MG, and D'Souza PM

Subjects

Humans, HIV Antibodies blood, HIV Antibodies immunology, Serologic Tests methods, HIV Infections diagnosis, HIV Infections prevention & control, AIDS Vaccines immunology, HIV-1 immunology

Abstract

Current serologic tests for HIV screening and confirmation of infection present challenges to the adoption of HIV vaccines. The detection of vaccine-induced HIV-1 antibodies in the absence of HIV-1 infection, referred to as vaccine-induced seropositivity/seroreactivity, confounds the interpretation of test results, causing misclassification of HIV-1 status with potential affiliated stigmatization. For HIV vaccines to be widely adopted with high community confidence and uptake, tests are needed that are agnostic to the vaccination status of tested individuals (ie, positive only for true HIV-1 infection). Successful development and deployment of such tests will require HIV vaccine developers to work in concert with diagnostic developers. Such tests will need to match today's high-performance standards (accuracy, cost-effectiveness, simplicity) for use in vaccinated and unvaccinated populations, especially in low- and middle-income countries with high HIV burden. Herein, we discuss the challenges and strategies for developing modified serologic HIV tests for concurrent deployment with HIV vaccines., Competing Interests: Potential conflicts of interest. W. C. and O. L. are former and current employees of Janssen Pharmaceutica N.V., respectively, and V. O. M. and M. G. P. are current employees of Janssen Vaccines and Prevention B.V. Both are Johnson & Johnson companies, and the authors may own stock or stock options in them. L. L. is a consultant for Janssen Pharmaceutica N.V. All other authors report no potential conflicts. All authors have submitted the ICMJE Form for Disclosure of Potential Conflicts of Interest. Conflicts that the editors consider relevant to the content of the manuscript have been disclosed., (© The Author(s) 2024. Published by Oxford University Press on behalf of Infectious Diseases Society of America. All rights reserved. For commercial re-use, please contact reprints@oup.com for reprints and translation rights for reprints. All other permissions can be obtained through our RightsLink service via the Permissions link on the article page on our site—for further information please contact journals.permissions@oup.com.)

Published

2024

30. Point-of-care testing and treatment of sexually transmitted and genital infections to improve birth outcomes in high-burden, low-resource settings (WANTAIM): a pragmatic cluster randomised crossover trial in Papua New Guinea.

Author

Riddell MA, Vallely LM, Mengi A, Badman SG, Low N, Wand H, Bolnga JW, Babona D, Mola GDL, Wiseman V, Kelly-Hanku A, Homer CSE, Morgan C, Luchters S, Whiley DM, Robinson LJ, Au L, Pukai-Gani I, Laman M, Kariwiga G, Toliman PJ, Batura N, Tabrizi SN, Rogerson SJ, Garland SM, Guy RJ, Peeling RW, Pomat WS, Kaldor JM, and Vallely AJB

Subjects

Adolescent, Adult, Female, Humans, Infant, Newborn, Pregnancy, Young Adult, Birth Weight, Chlamydia trachomatis, Cross-Over Studies, Genitalia, Neisseria gonorrhoeae, Pacific Island People statistics & numerical data, Papua New Guinea epidemiology, Point-of-Care Testing, Premature Birth prevention & control, Urinary Tract Infections, Vaginosis, Bacterial diagnosis, Vaginosis, Bacterial drug therapy

Abstract

Background: Chlamydia trachomatis, Neisseria gonorrhoeae, Trichomonas vaginalis, and bacterial vaginosis have been associated with adverse maternal and perinatal outcomes, but there is conflicting evidence on the benefits of antenatal screening and treatment for these conditions. We aimed to determine the effect of antenatal point-of-care testing and immediate treatment of C trachomatis, N gonorrhoeae, T vaginalis, and bacterial vaginosis on preterm birth, low birthweight, and other adverse maternal and perinatal outcomes compared with current standard of care, which included symptom-based treatment without laboratory confirmation., Methods: In this pragmatic cluster randomised crossover trial, we enrolled women (aged ≥16 years) attending an antenatal clinic at 26 weeks' gestation or earlier (confirmed by obstetric ultrasound), living within approximately 1 h drive of a study clinic, and able to provide reliable contact details at ten primary health facilities and their catchment communities (clusters) in Papua New Guinea. Clusters were randomly allocated 1:1 to receive either the intervention or control (standard care) in the first phase of the trial. Following an interval (washout period) of 2-3 months at the end of the first phase, each cluster crossed over to the other group. Randomisation was stratified by province. Individual participants were informed about trial group allocation only after completing informed consent procedures. The primary outcome was a composite of preterm birth (livebirth before 37 weeks' gestation), low birthweight (<2500 g), or both, analysed according to the intention-to-treat population. This study is registered with ISRCTN Registry, ISRCTN37134032, and is completed., Findings: Between July 26, 2017, and Aug 30, 2021, 4526 women were enrolled (2210 [63·3%] of 3492 women in the intervention group and 2316 [62·8%] of 3687 in the control group). Primary outcome data were available for 4297 (94·9%) newborn babies of 4526 women. The proportion of preterm birth, low birthweight, or both, in the intervention group, expressed as the mean of crude proportions across clusters, was 18·8% (SD 4·7%) compared with 17·8% in the control group (risk ratio [RR] 1·06, 95% CI 0·78-1·42; p=0·67). There were 1052 serious adverse events reported (566 in the intervention group and 486 in the control group) among 929 trial participants, and no differences by trial group., Interpretation: Point-of-care testing and treatment of C trachomatis, N gonorrhoeae, T vaginalis, and bacterial vaginosis did not reduce preterm birth or low birthweight compared with standard care. Within the subgroup of women with N gonorrhoeae, there was a substantial reduction in the primary outcome., Funding: UK Department of Health and Social Care; UK Foreign, Commonwealth and Development Office; UK Medical Research Council; the Wellcome Trust; the Australian National Health and Medical Research Council; and Swiss National Science Foundation., Competing Interests: Declaration of interests The Papua New Guinea Institute of Medical Research (MAR, LMV, AM, LJR, AK-H, JWB, IP-G, ML, LA, PJT, WSP, and AJBV) and the Kirby Institute at the University of New South Wales (MAR, LMV, SGB, HW, AK-H, VW, RJG, JMK, and AJBV) have received subsidised test kits for research from Cepheid (Sunnyvale, CA, USA). All other authors declare no competing interests. All authors declare that neither they or their institutions have received direct funding from industry for this or any other research project., (Copyright © 2024 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2024

31. A multi-country comparative study of two treponemal tests for the serodiagnosis of syphilis amongst men who have sex with men (MSM): Chemo-luminescent assay vs Treponema pallidum particle agglutination assay.

Author

Gios L, Mirandola M, Cordioli M, Zorzi A, Sherriff N, Vera J, Wlazly D, Hassan-Ibrahim MO, Padovese V, Anabel Darmanin, Peeling RW, Unemo M, Blondeel K, and Toskin I

Subjects

Male, Humans, Treponema pallidum, Homosexuality, Male, Antibodies, Bacterial, Syphilis Serodiagnosis methods, Serologic Tests methods, Sensitivity and Specificity, Luminescent Measurements methods, Agglutination, Syphilis, Sexual and Gender Minorities

Abstract

Introduction: International guidelines recommend routine screening for syphilis (aetiological agent: Treponema pallidum subspecies pallidum) amongst key populations and vulnerable populations using tests detecting treponemal and non-treponemal antibodies. Whilst treponemal tests have high sensitivities and specificities, they differ regarding subjective or objective interpretation, throughput and workload. Chemiluminescence immunoassays (CLIAs) are cost- and time-effective automated methods for detecting treponemal antibodies. The Treponema pallidum particle agglutination assay (TPPA) has been considered the "gold standard" treponemal assay, however, this includes a highly manual procedure, low throughput and subjective interpretation. The present multi-country study evaluated the ADVIA Centaur® Syphilis CLIA (Siemens Healthcare) assay compared to the reference SERODIA-TP·PA® (Fujirebio Diagnostics) for the serodiagnosis of syphilis amongst men who have sex with men (MSM)., Method: 1,485 MSM were enrolled in Brighton (UK), Malta, and Verona (Italy) as part of a larger WHO multi-country and multi-site ProSPeRo study. Ethical approval was obtained. Serum was tested with the ADVIA Centaur® Syphilis CLIA assay and SERODIA-TP·PA®, in accordance with the manufacturers' instructions, for a first round of validation. A second round of validation was carried out for discrepant results that were additionally tested with both Western Blot (Westernblot EUROIMMUN®) and an Immunoblot (INNO-LIA, Fujirebio Diagnostics). Sensitivity, specificity, positive and negative predictive value (PPV and NPV), likelihood ratios (positive/negative), and the Diagnostic Odds Ratio (DOR)/pre-post-test probability (Fagan's nomogram) were calculated., Results: Out of 1,485 eligible samples analysed in the first phase, the SERODIA-TP·PA® identified 360 positive and 1,125 negative cases. The ADVIA Centaur® Syphilis CLIA assay (Siemens) identified 366 positives, missclassifying one TPPA-positive sample. In the second phase, the ADVIA Centaur® Syphilis CLIA resulted in 1 false negative and 4 false positive results. Considering the syphilis study prevalence of 24% (95% CI: 22-26.7), The sensitivity of the ADVIA Centaur® Syphilis CLIA assay was 99.7% (95% CI: 98.5-100), and the specificity was 99.4% (95% CI: 98.7-99.7). The ROC area values were 0.996 (95% CI: 0.992-0.999), and both the PPV and NPV values were above 98% (PPV 98.1%, 95% CI: 96.1-99.2; NPV 99.9%, 95% CI: 99.5-100)., Conclusions: The ADVIA Centaur® Syphilis CLIA assay showed similar performance compared to the SERODIA-TP·PA®. Considering the study is based on QUADAS principles and with a homogeneous population, results are also likely to be generalisable to MSM population but potentially not applicable to lower prevalence populations routinely screened for syphilis. The automated CLIA treponemal assay confirmed to be accurate and appropriate for routine initial syphilis screening, i.e. when the reverse testing algorithm is applied., (© 2024. The Author(s).)

Published

2024

32. Independent clinic-based evaluation of point-of-care testing for the screening of Chlamydia trachomatis, Neisseria gonorrhoea and Trichomonas vaginalis in women-at-risk in Australia, Guatemala, Morocco, and South Africa.

Author

Shephard M, Matthews S, Kularatne R, Andrewartha K, Blondeel K, Alvarez C, Camey E, Hançali A, Müller E, Haw A, Oumzil H, Golparian D, Ramirez DE, Kiarie J, Kurbonov F, Mirandola M, Peeling RW, Silva R, Thwin SS, Unemo M, and Toskin I

Subjects

Female, Humans, Chlamydia trachomatis genetics, Guatemala epidemiology, Morocco epidemiology, South Africa epidemiology, Neisseria gonorrhoeae genetics, Australia, Point-of-Care Testing, Trichomonas vaginalis genetics, Gonorrhea diagnosis, Gonorrhea epidemiology

Abstract

Background: In 2018, the World Health Organization commenced a multi-country validation study of the Cepheid GeneXpert for a range of molecular-based point-of-care (POC) tests in primary care settings. One study arm focused on the evaluation of POC tests for screening 'women at risk' for chlamydia (CT), gonorrhoea (NG) and trichomonas (TV) in four countries - Australia, Guatemala, Morocco and South Africa., Methods: Study participants completed a pre-test questionnaire which included demographics, clinical information and general questions on POC testing (POCT). Two vaginal swab samples (either self-collected or clinician collected) from each patient were tested on the GeneXpert at the POC and at a reference laboratory using quality-assured nucleic acid amplification tests (NAATs)., Results: One thousand three hundred and eighty-three women were enrolled: 58.6% from South Africa, 29.2% from Morocco, 6.2% from Guatemala, and 6.0% from Australia. 1296 samples for CT/NG and 1380 samples for TV were tested by the GeneXpert and the reference NAAT. The rate of unsuccessful tests on the GeneXpert was 1.9% for CT, 1.5% for NG and 0.96% for TV. The prevalence of CT, NG and TV was 31%, 13% and 23%, respectively. 1.5% of samples were positive for all three infections; 7.8% were positive for CT and NG; 2.4% were positive for NG and TV; and 7.3% were positive for CT and TV. Compared to reference NAATs, pooled estimates of sensitivity for the GeneXpert tests were 83.7% (95% confidence intervals 69.2-92.1) for CT, 90.5% (85.1-94.1) for NG and 64.7% (58.1-70.7) for TV (although estimates varied considerably between countries). Estimates for specificity were ≥96% for all three tests both within- and between-countries. Pooled positive and negative likelihood ratios were: 32.7 ([CI] 21.2-50.5) and 0.17 (0.08-0.33) for CT; 95.3 (36.9-245.7) and 0.10 (0.06-0.15) for NG; and 56.5 (31.6-101.1) and 0.35 (0.27-0.47) for TV., Conclusion: This multi-country evaluation is the first of its kind world-wide. Positive likelihood ratios, as well as specificity estimates, indicate the GeneXpert POC test results for CT, NG and TV were clinically acceptable for ruling in the presence of disease. However, negative likelihood ratios and variable sensitivity estimates from this study were poorer than expected for ruling out these infections, particularly for TV., Trial Registration: Ethics approval to conduct the ProSPeRo study was granted by the WHO Ethics Review Committee, as well as local ethics committees from all participating countries., (© 2024. The Author(s).)

Published

2024

33. Clinic-based evaluation of the dual Xpert CT/NG assay on the GeneXpert System for screening for extragenital chlamydial and gonococcal infections amongst men who have sex with men.

Author

Cordioli M, Gios L, Erbogasto A, Mirandola M, Sandri A, Padovese V, Caceres C, Vargas S, Blondeel K, Silva R, Kiarie J, Kurbonov F, Peeling RW, Thwin SS, Golparian D, Unemo M, and Toskin I

Subjects

Male, Humans, Homosexuality, Male, Neisseria gonorrhoeae genetics, Chlamydia trachomatis genetics, Nucleic Acid Amplification Techniques, Tomography, X-Ray Computed, Chlamydia Infections diagnosis, Chlamydia Infections epidemiology, Sexual and Gender Minorities, Gonorrhea diagnosis, Gonorrhea epidemiology

Abstract

Background: Chlamydia trachomatis (CT) and Neisseria gonorrhoeae (NG) infections have increased globally. Asymptomatic infections represent a significant risk of long-term complications. Men who have sex with men (MSM) are disproportionally affected, underscoring the need to offer screening programmes to this population. CT/NG Point of Care Testing (POCT) constitutes a strategic tool to improve the continuum of STI care, however extensive real-life evaluations amongst at risk populations are lacking. The aim of this study is to estimate the GeneXpert CT/NG assay performance and usability for CT and NG at genital and extragenital sites for screening amongst MSM., Methods: This study was a multi-site sexual health clinic-based evaluation (Italy, Malta and Peru) with consecutive enrolment. A first void urine sample (divided in two aliquots), two oropharyngeal and two anorectal swabs were collected for each study participant. One specimen set (one for each anatomical site) was tested with the dual index test (Cepheid) at the clinics by the healthcare staff, the other set with FDA/CE approved Nucleic Acid Amplification Tests (NAATs) at the laboratory. Clinical sites and reference laboratories participated in an internal and external quality control programme. Sensitivity, specificity, positive and negative likelihood ratios, positive and negative predictive values for each anatomical site were estimated using a meta-analytic approach., Results: One thousand seven hundred two MSM were recruited across all clinical sites for a total of 5049 biological specimens. NG and CT were respectively detected in 274 and 287 of samples. Overall, the NG POCT sensitivity and specificity was 91.43% and 99.75% in urine (LR + 372.80, LR- 0.09), 89.68% and 99.55% in rectal specimens (LR + 197.30, LR- 0.10) and 75.87% and 98.77% at the pharynx respectively (LR + 61.94, LR- 0.24). The CT component of the POCT sensitivity was 84.82% and specificity 99.63% in urine (LR + 228.68, LR- 0.15), 78.07% and 99.19% respectively on rectal site (LR + 96.23, LR-0.22), 67.79% and 99.88% respectively at pharyngeal site (LR + 554.89, LR- 0.32). 95.95% of MSM reported to be willing to wait for POCT results and no provider reported difficulties in terms of performance or interpretation of the results of the Xpert CT/NG., Conclusion: Rapid turnaround time, ease of use and high acceptability make the Xpert CT/NG testing system a strategic tool for increasing testing frequency, reaching those not yet tested and offering the possibility of immediate treatment if needed. The assay showed good negative likelihood ratios and confirms its use to rule out CT/NG infections. Sensitivity varied across sites and pathogens. Periodic staff training at the testing sites should be mandatory., (© 2024. The Author(s).)

Published

2024

34. Independent clinic-based evaluation of dual POCTs for screening for HIV and syphilis in men who have sex with men in Italy, Malta, Peru, and the United Kingdom.

Author

Sherriff N, Mirandola M, Silva R, Cordioli M, Sawyer A, Gios L, Zorzi A, Huber J, Vera J, Richardson D, Hassan-Ibrahim M, Wlazly D, Padovese V, Barbara C, Darmanin A, Schembri A, Caceres C, Vargas S, Blondeel K, Kiarie J, Kurbonov F, Peeling RW, Thwin SS, and Toskin I

Subjects

Male, Humans, Homosexuality, Male, Peru epidemiology, Malta, Cross-Sectional Studies, Treponema pallidum, Point-of-Care Testing, Syphilis Serodiagnosis methods, Sensitivity and Specificity, Antibodies, Bacterial, Syphilis diagnosis, Syphilis epidemiology, Sexual and Gender Minorities, HIV Infections diagnosis, HIV Infections epidemiology

Abstract

Introduction: Globally, the incidence of HIV and syphilis can be reduced by the use of validated point of care tests (POCTs). As part of the WHO PRoSPeRo Network, we aimed to evaluate the performance, acceptability, and operational characteristics of two dual HIV/syphilis POCTs (Bioline HIV/Syphilis Duo (Abbott) and DPP® HIV-Syphilis assay (Chembio) for the screening of HIV and syphilis amongst men who have sex with men (MSM)., Method and Analyses: A cross sectional study of 2,577 MSM in Italy, Malta, Peru, and the United Kingdom (UK) presenting to seven clinic sites, were enrolled. Finger prick blood was collected to perform POCTs and results compared with standard laboratory investigations on venepuncture blood. Acceptability and operational characteristics were assessed using questionnaires. Diagnostic meta-analysis was used to combine data from the evaluation sites., Results: Based on laboratory tests, 23.46% (n = 598/2549) of participants were confirmed HIV positive, and 35.88% of participants (n = 901/2511) were positive on treponemal reference testing. Of all participants showing evidence of antibodies to Treponema pallidum, 50.56% (n = 455/900) were Rapid Plasma Reagin (RPR) test reactive. Of HIV positive individuals, 60.62% (n = 354/584) had evidence of antibodies to T. pallidum, and of these 60.45% (n = 214/354) exhibited reactive RPR tests indicating probable (co)infection. For Bioline POCT, pooled sensitivities and specificities for HIV were 98.95% and 99.89% respectively, and for syphilis were 73.79% and 99.57%. For Chembio pooled sensitivities and specificities for HIV were 98.66% and 99.55%, and for syphilis were 78.60% and 99.48%. Both tests can detect greater than 90% of probable active syphilis cases, as defined by reactive RPR and treponemal test results. These dual POCTs were preferred by 74.77% (n = 1,926) of participants, due to their convenience, and the operational characteristics made them acceptable to health care providers (HCPs)., Conclusions: Both the Bioline and the Chembio dual POCT for syphilis and HIV had acceptable performance, acceptability and operational characteristics amongst MSM in the PRoSPeRo network. These dual POCTs could serve as a strategic, more cost effective, patient and healthcare provider (HCP) friendly alternative to conventional testing; in clinical and other field settings, especially those in resource-limited settings., (© 2024. The Author(s).)

Published

2024

35. Expert guidance on target product profile development for AMR diagnostic tests.

Author

Bachmann TT, Mitsakakis K, Hays JP, van Belkum A, Russom A, Luedke G, Simonsen GS, Abel G, Peter H, Goossens H, Moran-Gilad J, Vila J, Becker K, Moons P, Sampath R, Peeling RW, Luz S, van Staa T, and Di Gregori V

Subjects

Humans, Diagnostic Tests, Routine methods, Drug Resistance, Microbial

Abstract

Diagnostics are widely considered crucial in the fight against antimicrobial resistance (AMR), which is expected to kill 10 million people annually by 2030. Nevertheless, there remains a substantial gap between the need for AMR diagnostics versus their development and implementation. To help address this problem, target product profiles (TPP) have been developed to focus developers' attention on the key aspects of AMR diagnostic tests. However, during discussion between a multisectoral working group of 51 international experts from industry, academia and healthcare, it was noted that specific AMR-related TPPs could be extended by incorporating the interdependencies between the key characteristics associated with the development of such TPPs. Subsequently, the working group identified 46 characteristics associated with six main categories (ie, Intended Use, Diagnostic Question, Test Description, Assay Protocol, Performance and Commercial). The interdependencies of these characteristics were then identified and mapped against each other to generate new insights for use by stakeholders. Specifically, it may not be possible for diagnostics developers to achieve all of the recommendations in every category of a TPP and this publication indicates how prioritising specific TPP characteristics during diagnostics development may influence (or not) a range of other TPP characteristics associated with the diagnostic. The use of such guidance, in conjunction with specific TPPs, could lead to more efficient AMR diagnostics development., Competing Interests: Competing interests: TTB is an advisor for (compensated) CARB-X, Module Innovations, Indian Biotechnology Industry Research Assistance Council (BIRAC) and (not compensated) Longitude Prize, Joint Programming Initiative for Antimicrobial Resistance, all outside the submitted work. JPH is a member of Scientific Advisory Board of Vitamica, outside the submitted work. AvB was an employee of bioMérieux and is currently with BaseClear. GL is an employee of Curetis, but neither company had direct influence on the submitted work. KB is inventor of pending patents related to infectious disease diagnostics and received grants, honoraria and travel support from the EU/INTERREG, the German Federal Ministry of Education and Research and the Federal Ministry for Economic Affairs, the Netherlands Research Council for Applied and Technical Sciences as well as from Becton Dickinson, bioMérieux, Bruker Daltonik, Hain Lifescience, Roche Molecular Systems, ThermoFisher; outside the submitted work. TvS reports grants from GSK Research Grant, personal fees from Pfizer, outside the submitted work. VdG reports personal fees from GVM CARE AND RESEARCH, outside the submitted work., (© Author(s) (or their employer(s)) 2023. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2023

36. Role and effectiveness of telephone hotlines in outbreak response in Africa: A systematic review and meta-analysis.

Author

Fongwen NT, Nchafack A, Rohan H, Ong JJ, Tucker JD, Beckmann N, Hughes G, and Peeling RW

Subjects

Humans, Animals, Hotlines, Disease Outbreaks prevention & control, Africa epidemiology, Rift Valley Fever, Virus Diseases

Abstract

Background: In Africa, little is known about the role of telephone hotlines in outbreak response. We systematically reviewed the role and effectiveness of hotlines on outbreak response in Africa., Method: We used the Cochrane handbook and searched five databases. The protocol was registered on PROSPERO (CRD42021247141). Medline, Embase, PsycINFO, Global Health and Web of Science were searched from 30 June 2020 to August 2020 for studies on the use of telephone hotlines in outbreak response in Africa published between January 1995 and August 2020. The search was also repeated on 16 September 2022. Data on effectiveness (alerts generated, cases confirmed) were extracted from peer-reviewed studies. Meta-analysis of alerts generated, and proportion of cases confirmed was done using the random effects model. The quality of studies was assessed using the Joanna Briggs Institute (JBI) tools. The heterogeneity and publication bias were assessed using the Galbraith and funnel plots, respectively., Results: Our search yielded 1251 non-duplicate citations that were assessed. 41 full texts were identified, and 21 studies were included in the narrative synthesis, while 12 were included in the meta-analysis. The hotlines were local (seven studies) or national (three studies). A combination of a local and national hotline was used in one study. The hotlines were set up for unusual respiratory events (one study), polio (one study), Ebola (10 studies), COVID-19 (two studies), malaria (one study), influenza-like illnesses (ILI) (one study) and rift valley fever in livestock (one study). Hotlines were mainly used for outbreak surveillance at the local level. A total of 332,323 alerts were generated, and 67,658 met the case definition, corresponding to an overall pooled proportion of alerts generated(sensitivity) of 38% (95%CI: 24-52%). The sensitivity was 41% (95% CI: 24-59%) for local hotlines and 26%(95%CI:5-47%) for national hotlines. Hotlines were also used for surveillance of rift valley fever in livestock (one study) vaccination promotion (one study), death reporting (five studies), rumour tracking and fighting misinformation (two studies) and community engagement (five studies). The studies were of low to moderate quality with high publication bias and heterogeneity(I2 = 99%). The heterogeneity was not explained by the sample size., Conclusion: These data suggest that telephone hotlines can be effective in outbreak disease surveillance in Africa. Further implementation research is needed to scale up telephone hotlines in rural areas., Competing Interests: The authors have declared that no competing interests exist., (Copyright: © 2023 Fongwen et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)

Published

2023

37. Regulation of blood-screening in vitro diagnostics in sub-Saharan African countries remains a challenge.

Author

Abdurrahman G, Samukange W, Lyoko N, Shonhiwa NO, Kafere C, Nübling CM, Peeling RW, and Reinhardt J

Abstract

According to the World Health Organization, blood must be screened for major transmitted infections before transfusion to prevent the possibility of passing an infection to the recipient. For accurate detection of infectious disease pathogens in the blood of donors, in-vitro diagnostic medical devices (IVDs) of high specificity and sensitivity should be used. In mature healthcare systems, the regulatory authorities authorize the usage of devices with the highest performance capabilities, which are also controlled through active market oversight. However, in Sub-Saharan African countries, the regulation of IVDs is often poorly developed. With the lack of stringent regulatory oversight, IVDs of poor quality can be put on the market and used for blood donor screening, which, ultimately, poses a great public health threat. The BloodTrain is a humanitarian project from the Germany Federal Ministry of Health that aims to help strengthen the regulatory authorities in Sub-Saharan partner countries. Here, we present the status of IVD regulation in the partner countries and the objectives that the BloodTrain project aims to achieve in the region toward regulating IVDs., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Abdurrahman, Samukange, Lyoko, Shonhiwa, Kafere, Nübling, Peeling and Reinhardt.)

Published

2023

38. Elimination and eradication goals for communicable diseases: a systematic review.

Author

Khawar L, Donovan B, Peeling RW, Guy RJ, and McGregor S

Subjects

Humans, Disease Eradication, Public Health, Global Health, Goals, Communicable Diseases

Abstract

Objective: To consolidate recent information on elimination and eradication goals for infectious diseases and clarify the definitions and associated terminology for different goals., Methods: We conducted a systematic search of the World Health Organization's Institutional Repository for Information Sharing (WHO IRIS) and a customized systematic Google advanced search for documents published between 2008 and 2022 on elimination or eradication strategies for infectious conditions authored by WHO or other leading health organizations. We extracted information on names of infectious conditions, the elimination and eradication goals and timelines, definitions of goals, non-standardized terminology, targets and assessment processes., Findings: We identified nine goals for 27 infectious conditions, ranging from disease control to eradication. In comparison with the hierarchy of disease control, as defined at the Dahlem Workshop in 1997, six goals related to disease control with varying levels of advancement, two related to elimination and one to eradication. Goals progressed along a disease-control continuum, such as end of disease epidemic to pre-elimination to elimination as a public health problem or threat. We identified the use of non-standardized terminology with certain goals, including virtual elimination, elimination of disease epidemics, public health threat and public health concern., Conclusion: As we approach the 2030 target date to achieve many of the goals related to disease control and for other infections to become candidates for elimination in the future, clarity of definitions and objectives is important for public health professionals and policy-makers to avoid misperceptions and miscommunication., ((c) 2023 The authors; licensee World Health Organization.)

Published

2023

39. Syphilis.

Author

Peeling RW, Mabey D, Chen XS, and Garcia PJ

Subjects

Pregnancy, Male, Female, Humans, Homosexuality, Male, Treponema pallidum, Penicillins, Syphilis diagnosis, Syphilis drug therapy, Syphilis epidemiology, Sexual and Gender Minorities, Chancre

Abstract

Syphilis is a sexually and vertically transmitted bacterial infection caused by the bacterium Treponema pallidum. Its prevalence is high in low-income and middle-income countries, and its incidence has increased in high-income countries in the last few decades among men who have sex with men. Syphilis is a major cause of adverse pregnancy outcomes in low-income and middle-income countries. Clinical features include a primary chancre at the point of inoculation, followed weeks later by the rash of secondary syphilis, a latent period, and in some cases, involvement of the eyes, CNS, and cardiovascular systems. It is diagnosed serologically. A single intramuscular dose of long-acting benzathine penicillin is recommended for people who have had syphilis for less than 1 year and longer courses for people with late latent syphilis. Control strategies include screening and treatment of all pregnant women, and targeted interventions for groups at high risk. Vaccine development, research on antibiotic prophylaxis, and digital messaging as prevention strategies are ongoing., Competing Interests: Declaration of interests We declare no competing interests., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published

2023

40. Author Correction: Chikungunya fever.

Author

Bartholomeeusen K, Daniel M, LaBeaud DA, Gasque P, Peeling RW, Stephenson KE, Ng LFP, and Ariën KK

Published

2023

41. Chikungunya fever.

Author

Bartholomeeusen K, Daniel M, LaBeaud DA, Gasque P, Peeling RW, Stephenson KE, Ng LFP, and Ariën KK

Subjects

Animals, Humans, Quality of Life, Mosquito Vectors, Chikungunya Fever complications, Chikungunya Fever epidemiology, Chikungunya virus, Aedes

Abstract

Chikungunya virus is widespread throughout the tropics, where it causes recurrent outbreaks of chikungunya fever. In recent years, outbreaks have afflicted populations in East and Central Africa, South America and Southeast Asia. The virus is transmitted by Aedes aegypti and Aedes albopictus mosquitoes. Chikungunya fever is characterized by severe arthralgia and myalgia that can persist for years and have considerable detrimental effects on health, quality of life and economic productivity. The effects of climate change as well as increased globalization of commerce and travel have led to growth of the habitat of Aedes mosquitoes. As a result, increasing numbers of people will be at risk of chikungunya fever in the coming years. In the absence of specific antiviral treatments and with vaccines still in development, surveillance and vector control are essential to suppress re-emergence and epidemics., (© 2023. Springer Nature Limited.)

Published

2023

42. Lessons from COVID-19 for improving diagnostic access in future pandemics.

Author

Peeling RW and Sia SK

Subjects

Humans, Pandemics, Delivery of Health Care, COVID-19 Testing, COVID-19

Abstract

Throughout the COVID-19 pandemic, we have witnessed the critical and expanding roles of testing. Despite the development of over a thousand brand of tests - with some close to fulfilling the 4As (accuracy, access, affordability, and actionability via quick time to result) of an ideal diagnostic test - gaps persisted in developing tests to fit public health needs, and in providing equitable access. Here, we review how the use cases for testing evolved over the course of the COVID-19 pandemic, with associated engineering challenges (and potential lessons) at each phase for test developers. We summarise lessons learnt from the recent epidemic and propose four areas for future cooperative effort among test developers, government regulators and policy makers, public health experts, and the public: 1) develop new models for public sector funding and research and development; 2) increase testing capacity by investing in adaptable open-platform technologies at every level of the healthcare system; 3) build data connectivity infrastructures to support a connected diagnostic system as a backbone for surveillance; and 4) facilitate the rapid translation of innovation into use through a coordinated framework for regulatory approval and policy development.

Published

2023

43. Inadequate diagnostic capacity for monkeypox-sleeping through the alarm again.

Author

Boodman C, Heymann DL, and Peeling RW

Subjects

Humans, Monkeypox virus, Disease Outbreaks, Mpox (monkeypox) epidemiology

Abstract

Competing Interests: We declare no competing interests.

Published

2023

44. Evaluation of Zika rapid tests as aids for clinical diagnosis and epidemic preparedness.

Author

Boeras D, Diagne CT, Pelegrino JL, Grandadam M, Duong V, Dussart P, Brey P, Ruiz D, Adati M, Wilder-Smith A, Falconar AK, Romero CM, Guzman M, Hasanin N, Sall A, and Peeling RW

Abstract

Background: Development and evaluation of diagnostics for diseases of epidemic potential are often funded during epidemics, but not afterwards, leaving countries unprepared for the next epidemic. United Nations Children's Emergency Fund (UNICEF) partnered with the United States Agency for International Development (USAID) to address this important gap by investing in an advance purchase commitment (APC) mechanism to accelerate the development and evaluation of Zika rapid diagnostic tests (RDTs) for case detection and surveillance. This paper describes the performance evaluation of five Zika RDTs eligible for procurement., Methods: A network of European Union-funded ZikaPLAN sites in Africa, Asia, Latin America with access to relevant serum specimens were selected to evaluate RDTs developed for the UNICEF APC mechanism. A standardised protocol and evaluation panels were developed and a call for specimens for the evaluation panels issued to different sites. Each site contributed specimens to the evaluation from their biobank. Data were collated, analysed and presented to the UNICEF Procurement Review Group for review., Findings: Three RDTs met the criteria for UNICEF procurement of sensitivity and specificity of 85% against a refence standard. The sensitivity/specificity of the ChemBio anti-Zika Virus (ZIKV) immunoglobulin M (IgM) test was 86.4 %/86.7% and the ChemBio ZCD system for anti-ZIKV IgM was 79.0%/97.1%, anti-dengue virus (DENV) IgM 90.0%/89.2%, anti-Chikungunya virus (CHIKV) IgM 90.6%/97.2%. The sensitivity/specificity of the SD Biosensor anti-ZIKV IgM was 96.8 %/90.8%, anti-DENV IgM 71.8%/83.5%, the DENV nonstructural protein 1 (NS1) glycoprotein 90.0%/90.2%, anti- yellow fever virus (YFV) IgM 84.6%/92.4%, anti-CHIKV IgM 86.3%/97.5%., Interpretation: Three RDTs fulfilled the performance thresholds set by WHO and were eligible for UNICEF procurement. These tests will improve the diagnosis of ZIKV and other arboviral infections as well as providing countries with better tools for surveillance and response to future epidemics., Funding: This work was supported by the USAID grant GHA-G-00-07-00007 and ZikaPLAN (European Union's Horizon 2020 Research and Innovation Programme under Grant Agreement No. 734584)., Competing Interests: We declare that we have no conflicts of interest., (© 2022 The Authors.)

Published

2022

45. Travel measures in the SARS-CoV-2 variant era need clear objectives.

Author

Kucharski AJ, Jit M, Logan JG, Cotten M, Clifford S, Quilty BJ, Russell TW, Peeling RW, Antonio M, and Heymann DL

Subjects

Humans, Phylogeny, COVID-19 epidemiology, SARS-CoV-2 genetics, Travel legislation & jurisprudence

Published

2022

46. Diagnostics for COVID-19: moving from pandemic response to control.

Author

Peeling RW, Heymann DL, Teo YY, and Garcia PJ

Subjects

Antibodies, Viral blood, Antigens, Viral isolation & purification, COVID-19 epidemiology, COVID-19 transmission, COVID-19 virology, COVID-19 Testing methods, COVID-19 Vaccines administration & dosage, Communicable Disease Control methods, Communicable Disease Control trends, Humans, Mass Screening trends, RNA, Viral isolation & purification, SARS-CoV-2 genetics, SARS-CoV-2 immunology, SARS-CoV-2 isolation & purification, COVID-19 diagnosis, COVID-19 Testing trends, Communicable Disease Control organization & administration, Mass Screening organization & administration, Pandemics prevention & control

Abstract

Diagnostics have proven to be crucial to the COVID-19 pandemic response. There are three major methods for the detection of SARS-CoV-2 infection and their role has evolved during the course of the pandemic. Molecular tests such as PCR are highly sensitive and specific at detecting viral RNA, and are recommended by WHO for confirming diagnosis in individuals who are symptomatic and for activating public health measures. Antigen rapid detection tests detect viral proteins and, although they are less sensitive than molecular tests, have the advantages of being easier to do, giving a faster time to result, of being lower cost, and able to detect infection in those who are most likely to be at risk of transmitting the virus to others. Antigen rapid detection tests can be used as a public health tool for screening individuals at enhanced risk of infection, to protect people who are clinically vulnerable, to ensure safe travel and the resumption of schooling and social activities, and to enable economic recovery. With vaccine roll-out, antibody tests (which detect the host's response to infection or vaccination) can be useful surveillance tools to inform public policy, but should not be used to provide proof of immunity, as the correlates of protection remain unclear. All three types of COVID-19 test continue to have a crucial role in the transition from pandemic response to pandemic control., Competing Interests: Declaration of interests We declare no competing interests., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2022

47. The relevance of target product profiles for manufacturers, experiences from the World Health Organization initiative for point-of-care testing for sexually transmitted infections.

Author

Murtagh M, Blondeel K, Peeling RW, Kiarie J, and Toskin I

Abstract

Background: Sexually transmitted infections (STIs) are a significant global public health issue that cause a high burden of disease, especially in low- and middle-income countries. Screening of key populations and early and accurate diagnosis of infection are critical. Testing for syphilis, Chlamydia trachomatis, Neisseria gonorrhoeae, Trichomonas vaginalis, curable STIs, as well as the human papillomavirus (HPV), is frequently unavailable in low-resource settings. Tests for these STIs that can be used at the point of patient care (POCTs) are needed. In recent years, there has been increased attention for STI POCTs, but technical guidance, financial resources and advocacy for additional platforms/tests are required in order to foster the development of STI POCTs. The WHO Department of Sexual and Reproductive Health and Research (SRH) has developed target product profiles (TPPs), a form of technical guidance, for these STI diagnostics., Methods: SRH conducted a survey of selected companies that are developing POCTs for one or more of the STIs mentioned above to better understand how these TPPs influence the diagnostic development process - to assess their impact., Results: Survey respondents indicated that the STI POCT TPPs provided good guidance with respect to performance expectations and operational characteristics for the tests/platforms. In particular, optimal metrics for sensitivity, specificity, sample types, and time to result were considered to be very useful. Respondents also suggested ways to improve the relevance of the STI POCT TPPs. For example, since it is often not possible for developers to achieve every desired standard, it would be useful to prioritize each performance/operational characteristic of the test and to provide a rationale as to why certain characteristics are considered important. Respondents also emphasized the need to encourage industry participation in the TPP development process and to find creative ways, including via targeted emails, a WHO webpage directed at industry, or a coordinated communications plan to increase awareness of the TPPs., Conclusions: Companies value the STI POCT TPPs and want them to continue. In order to maximize impact, WHO should consider the proposals from the manufacturers in the interest of increasing and accelerating access to STI diagnostics and treatment in low-resource settings., (© 2021. The Author(s).)

Published

2021

48. Innovations in COVID-19 testing: the road from pandemic response to control.

Author

Peeling RW and Heymann DL

Subjects

Humans, SARS-CoV-2, COVID-19, Pandemics prevention & control

Abstract

Competing Interests: We declare no competing interests.

Published

2021

49. Scaling up COVID-19 rapid antigen tests: promises and challenges.

Author

Peeling RW, Olliaro PL, Boeras DI, and Fongwen N

Subjects

False Negative Reactions, False Positive Reactions, Humans, Predictive Value of Tests, Sensitivity and Specificity, COVID-19 diagnosis, COVID-19 Testing methods, COVID-19 Testing standards, SARS-CoV-2

Abstract

WHO recommends a minimum of 80% sensitivity and 97% specificity for antigen-detection rapid diagnostic tests (Ag-RDTs), which can be used for patients with symptoms consistent with COVID-19. However, after the acute phase when viral load decreases, use of Ag-RDTs might lead to high rates of false negatives, suggesting that the tests should be replaced by a combination of molecular and serological tests. When the likelihood of having COVID-19 is low, such as for asymptomatic individuals in low prevalence settings, for travel, return to schools, workplaces, and mass gatherings, Ag-RDTs with high negative predictive values can be used with confidence to rule out infection. For those who test positive in low prevalence settings, the high false positive rate means that mitigation strategies, such as molecular testing to confirm positive results, are needed. Ag-RDTs, when used appropriately, are promising tools for scaling up testing and ensuring that patient management and public health measures can be implemented without delay., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

50. Point-of-care testing and treatment of sexually transmitted and genital infections during pregnancy in Papua New Guinea (WANTAIM trial): protocol for an economic evaluation alongside a cluster-randomised trial.

Author

Batura N, Saweri OP, Vallely A, Pomat W, Homer C, Guy R, Luchters S, Mola G, Vallely LM, Morgan C, Kariwiga G, Wand H, Rogerson S, Tabrizi SN, Whiley DM, Low N, Peeling RW, Siba PM, Riddell M, Laman M, Bolnga J, Robinson LJ, Morewaya J, Badman S, Kelly-Hanku A, Toliman PJ, Peter W, Peach E, Garland S, Kaldor J, and Wiseman V

Subjects

Child, Cost-Benefit Analysis, Female, Genitalia, Humans, Infant, Newborn, Papua New Guinea epidemiology, Point-of-Care Testing, Pregnancy, Randomized Controlled Trials as Topic, Premature Birth, Sexually Transmitted Diseases diagnosis, Sexually Transmitted Diseases drug therapy

Abstract

Introduction: Left untreated, sexually transmitted and genital infections (henceforth STIs) in pregnancy can lead to serious adverse outcomes for mother and child. Papua New Guinea (PNG) has among the highest prevalence of curable STIs including syphilis, chlamydia, gonorrhoea, trichomoniasis and bacterial vaginosis, and high neonatal mortality rates. Diagnosis and treatment of these STIs in PNG rely on syndromic management. Advances in STI diagnostics through point-of-care (PoC) testing using GeneXpert technology hold promise for resource-constrained countries such as PNG. This paper describes the planned economic evaluation of a cluster-randomised cross-over trial comparing antenatal PoC testing and immediate treatment of curable STIs with standard antenatal care in two provinces in PNG., Methods and Analysis: Cost-effectiveness of the PoC intervention compared with standard antenatal care will be assessed prospectively over the trial period (2017-2021) from societal and provider perspectives. Incremental cost-effectiveness ratios will be calculated for the primary health outcome, a composite measure of the proportion of either preterm birth and/or low birth weight; for life years saved; for disability-adjusted life years averted; and for non-health benefits (financial risk protection and improved health equity). Scenario analyses will be conducted to identify scale-up options, and budget impact analysis will be undertaken to understand short-term financial impacts of intervention adoption on the national budget. Deterministic and probabilistic sensitivity analysis will be conducted to account for uncertainty in key model inputs., Ethics and Dissemination: This study has ethical approval from the Institutional Review Board of the PNG Institute of Medical Research; the Medical Research Advisory Committee of the PNG National Department of Health; the Human Research Ethics Committee of the University of New South Wales; and the Research Ethics Committee of the London School of Hygiene and Tropical Medicine. Findings will be disseminated through national stakeholder meetings, conferences, peer-reviewed publications and policy briefs., Trial Registration Number: ISRCTN37134032., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2021. Re-use permitted under CC BY. Published by BMJ.)

Published

2021