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dc.contributor.authorFeasey, Helena R.A.
dc.contributor.authorKhundi, Mcewen
dc.contributor.authorSoko, Rebecca nzawa
dc.contributor.authorBottomley, Christian
dc.contributor.authorChiume, Lingstone
dc.contributor.authorBurchett, Helen e. d.
dc.contributor.authorNliwasa, Marriott
dc.contributor.authorTwabi, Hussein h.
dc.contributor.authorMpunga, James a.
dc.contributor.authorMacpherson, Peter
dc.contributor.authorCorbett, Elizabeth l.
dc.date.accessioned2024-03-15T10:30:24Z
dc.date.available2024-03-15T10:30:24Z
dc.date.issued2023-12-05
dc.identifier297119601
dc.identifier91725a10-bf27-4a04-8807-2dd777f8dfc1
dc.identifier85195082426
dc.identifier.citationFeasey , H R A , Khundi , M , Soko , R N , Bottomley , C , Chiume , L , Burchett , H E D , Nliwasa , M , Twabi , H H , Mpunga , J A , Macpherson , P & Corbett , E L 2023 , ' Impact of active case-finding for tuberculosis on case-notifications in Blantyre, Malawi : a community-based cluster-randomised trial (SCALE) ' , PLOS Global Public Health , vol. 3 , no. 12 , e0002683 . https://doi.org/10.1371/journal.pgph.0002683en
dc.identifier.issn2767-3375
dc.identifier.othercrossref: 10.1371/journal.pgph.0002683
dc.identifier.otherORCID: /0000-0003-3109-6722/work/148420990
dc.identifier.urihttps://hdl.handle.net/10023/29501
dc.descriptionThis work was funded through ELC's Wellcome fellowship 200901/Z/16/Z. PM was also supported through a Wellcome fellowship: 206575/Z/17/Z.en
dc.description.abstractActive case-finding (ACF) for tuberculosis can help find the “missing millions” with undiagnosed tuberculosis. In a cluster-randomised trial, we investigated impact of ACF on case-notifications in Blantyre, Malawi, where ACF has been intensively implemented following 2014 estimates of ~1,000 per 100,000 adults with undiagnosed TB. Following a pre-intervention prevalence survey (May 2019 to March 2020), constrained randomisation allocated neighbourhoods to either door-to-door ACF (sputum microscopy for reported cough >2 weeks) or standard-of-care (SOC). Implementation was interrupted by COVID-19. Cluster-level bacteriologically-confirmed case-notification rate (CNR) ratio within 91 days of ACF was our redefined primary outcome; comparison between arms used Poisson regression with random effects. Secondary outcomes were 91-day CNR ratios comparing all tuberculosis registrations and all non-ACF registrations. Interrupted time series (ITS) analysis of CNRs in the SOC arm examined prevalence survey impact. (ISRCTN11400592). 72 clusters served by 10 study-supported tuberculosis registration centres were randomised to ACF (261,244 adults, 58,944 person-years follow-up) or SOC (256,713 adults, 52,805 person-years). Of 1,192 ACF participants, 13 (1.09%) were smear-positive. Within 91 days, 113 (42 bacteriologically-confirmed) and 108 (33 bacteriologically-confirmed) tuberculosis patients were identified as ACF or SOC cluster residents, respectively. There was no difference by arm, with adjusted 91-day CNR ratios 1.12 (95% CI: 0.61–2.07) for bacteriologically-confirmed tuberculosis; 0.93 (95% CI: 0.68–1.28) for all tuberculosis registrations; and 0.86 (95%CI: 0.63–1.16) for non-ACF (routinely) diagnosed. Of 7,905 ACF and 7,992 SOC pre-intervention survey participants, 12 (0.15%) and 17 (0.21%), respectively, had culture/Xpert-confirmed tuberculosis. ITS analysis showed no survey impact on SOC CNRs. Despite residual undiagnosed tuberculosis of 150 per 100,000 population, there was no increase in tuberculosis notifications from this previously successful approach targeting symptomatic disease, likely due to previous TB ACF and rapid declines in TB burden. In such settings, future ACF should focus on targeted outreach and demand creation, alongside optimised facility-based screening.
dc.format.extent17
dc.format.extent1684725
dc.language.isoeng
dc.relation.ispartofPLOS Global Public Healthen
dc.subjectDASen
dc.subjectSDG 3 - Good Health and Well-beingen
dc.titleImpact of active case-finding for tuberculosis on case-notifications in Blantyre, Malawi : a community-based cluster-randomised trial (SCALE)en
dc.typeJournal articleen
dc.contributor.institutionUniversity of St Andrews. School of Medicineen
dc.identifier.doihttps://doi.org/10.1371/journal.pgph.0002683
dc.description.statusPeer revieweden


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