Your search keyword '"Simon C Mendelsohn"' showing total 40 results

1. Systematic review of diagnostic and prognostic host blood transcriptomic signatures of tuberculosis disease in people living with HIV [version 2; peer review: 2 approved]

Author

Simon C Mendelsohn, Humphrey Mulenga, Savannah Verhage, Thomas J Scriba, and Mark Hatherill

Subjects

Host, blood, diagnostic, prognostic, gene, signatures, eng, Medicine

Abstract

Background HIV-associated tuberculosis (TB) has high mortality; however, current triage and prognostic tools offer poor sensitivity and specificity, respectively. We conducted a systematic review of diagnostic and prognostic host-blood transcriptomic signatures of TB in people living with HIV (PLHIV). Methods We systematically searched online databases for studies published in English between 1990-2020. Eligible studies included PLHIV of any age in test or validation cohorts, and used microbiological or composite reference standards for TB diagnosis. Inclusion was not restricted by setting or participant age. Study selection, quality appraisal using the QUADAS-2 tool, and data extraction were conducted independently by two reviewers. Thereafter, narrative synthesis of included studies, and comparison of signatures performance, was performed. Results We screened 1,580 records and included 12 studies evaluating 31 host-blood transcriptomic signatures in 10 test or validation cohorts of PLHIV that differentiated individuals with TB from those with HIV alone, latent Mycobacterium tuberculosis infection, or other diseases (OD). Two (2/10; 20%) cohorts were prospective (29 TB cases; 51 OD) and 8 (80%) case-control (353 TB cases; 606 controls) design. All cohorts (10/10) were recruited in Sub-Saharan Africa and 9/10 (90%) had a high risk of bias. Ten signatures (10/31; 32%) met minimum WHO Target Product Profile (TPP) criteria for TB triage tests. Only one study (1/12; 8%) evaluated prognostic performance of a transcriptomic signature for progression to TB in PLHIV, which did not meet the minimum WHO prognostic TPP. Conclusions Generalisability of reported findings is limited by few studies enrolling PLHIV, limited geographical diversity, and predominantly case-control design, which also introduces spectrum bias. New prospective cohort studies are needed that include PLHIV and are conducted in diverse settings. Further research exploring the effect of HIV clinical, virological, and immunological factors on diagnostic performance is necessary for development and implementation of TB transcriptomic signatures in PLHIV.

Published

2023

2. Systematic review of diagnostic and prognostic host blood transcriptomic signatures of tuberculosis disease in people living with HIV [version 1; peer review: 2 approved]

Author

Simon C Mendelsohn, Humphrey Mulenga, Savannah Verhage, Thomas J Scriba, and Mark Hatherill

Subjects

Host, blood, diagnostic, prognostic, gene, signatures, eng, Medicine

Abstract

Background HIV-associated tuberculosis (TB) has high mortality; however, current triage and prognostic tools offer poor sensitivity and specificity, respectively. We conducted a systematic review of diagnostic and prognostic host-blood transcriptomic signatures of TB in people living with HIV (PLHIV). Methods We systematically searched online databases for studies published in English between 1990-2020. Eligible studies included PLHIV of any age in test or validation cohorts, and used microbiological or composite reference standards for TB diagnosis. Inclusion was not restricted by setting or participant age. Study selection, quality appraisal using the QUADAS-2 tool, and data extraction were conducted independently by two reviewers. Thereafter, narrative synthesis of included studies, and comparison of signatures performance, was performed. Results We screened 1,580 records and included 12 studies evaluating 31 host-blood transcriptomic signatures in 10 test or validation cohorts of PLHIV that differentiated individuals with TB from those with HIV alone, latent Mycobacterium tuberculosis infection, or other diseases (OD). Two (2/10; 20%) cohorts were prospective (29 TB cases; 51 OD) and 8 (80%) case-control (353 TB cases; 606 controls) design. All cohorts (10/10) were recruited in Sub-Saharan Africa and 9/10 (90%) had a high risk of bias. Ten signatures (10/31; 32%) met minimum WHO Target Product Profile (TPP) criteria for TB triage tests. Only one study (1/12; 8%) evaluated prognostic performance of a transcriptomic signature for progression to TB in PLHIV, which did not meet the minimum WHO prognostic TPP. Conclusions Generalisability of reported findings is limited by few studies enrolling PLHIV, limited geographical diversity, and predominantly case-control design, which also introduces spectrum bias. New prospective cohort studies are needed that include PLHIV and are conducted in diverse settings. Further research exploring the effect of HIV clinical, virological, and immunological factors on diagnostic performance is necessary for development and implementation of TB transcriptomic signatures in PLHIV.

Published

2023

3. Mycobacterium tuberculosis infection, immune activation, and risk of HIV acquisition.

Author

Rachel A Bender Ignacio, Jessica Long, Aparajita Saha, Felicia K Nguyen, Lara Joudeh, Ethan Valinetz, Simon C Mendelsohn, Thomas J Scriba, Mark Hatherill, Holly Janes, Gavin Churchyard, Susan Buchbinder, Ann Duerr, Javeed A Shah, and Thomas R Hawn

Subjects

Medicine, Science

Abstract

BackgroundAlthough immune activation is associated with HIV acquisition, the nature of inflammatory profiles that increase HIV risk, which may include responses to M. tuberculosis (Mtb) infection, are not well characterized.MethodsWe conducted a nested case-control study using cryopreserved samples from persons who did and did not acquire HIV during the multinational Step clinical trial of the MRKAd5 HIV-1 vaccine. PBMCs from the last HIV-negative sample from incident HIV cases and controls were stimulated with Mtb-specific antigens (ESAT-6/CFP-10) and analyzed by flow cytometry with intracellular cytokine staining and scored with COMPASS. We measured inflammatory profiles with five Correlates of TB Risk (CoR) transcriptomic signatures. Our primary analysis examined the association of latent Mtb infection (LTBI; IFNγ+CD4+ T cell frequency) or RISK6 CoR signature with HIV acquisition. Conditional logistic regression analyses, adjusted for known predictors of HIV acquisition, were employed to assess whether TB-associated immune markers were associated with HIV acquisition.ResultsAmong 465 participants, LTBI prevalence (21.5% controls vs 19.1% cases, p = 0.51) and the RISK6 signature were not higher in those who acquired HIV. In exploratory analyses, Mtb antigen-specific polyfunctional CD4+ T cell COMPASS scores (aOR 0.96, 95% CI 0.77, 1.20) were not higher in those who acquired HIV. Two CoR signatures, Sweeney3 (aOR 1.38 (1.07, 1.78) per SD change) and RESPONSE5 (0.78 (0.61, 0.98)), were associated with HIV acquisition. The transcriptomic pattern used to differentiate active vs latent TB (Sweeney3) was most strongly associated with acquiring HIV.ConclusionsLTBI, Mtb polyfunctional antigen-specific CD4+ T cell activation, and RISK6 were not identified as risks for HIV acquisition. In exploratory transcriptomic analyses, two CoR signatures were associated with HIV risk after adjustment for known behavioral and clinical risk factors. We identified host gene expression signatures associated with HIV acquisition, but the observed effects are likely not mediated through Mtb infection.

Published

2022

4. Host blood transcriptomic biomarkers of tuberculosis disease in people living with HIV: a systematic review protocol

Author

Mary Shelton, Humphrey Mulenga, Stanley Kimbung Mbandi, Simon C Mendelsohn, Mark Hatherill, Fatoumatta Darboe, and Thomas J Scriba

Subjects

Medicine

Abstract

Introduction Current tuberculosis triage and predictive tools offer poor accuracy and are ineffective for detecting asymptomatic disease in people living with HIV (PLHIV). Host tuberculosis transcriptomic biomarkers hold promise for diagnosing prevalent and predicting progression to incident tuberculosis and guiding further investigation, preventive therapy and follow-up. We aim to conduct a systematic review of performance of transcriptomic signatures of tuberculosis in PLHIV.Methods and analysis We will search MEDLINE (PubMed), WOS Core Collection, Biological Abstracts, and SciELO Citation Index (Web of Science), Africa-Wide Information and General Science Abstracts (EBSCOhost), Scopus, and Cochrane Central Register of Controlled Trials databases for articles published in English between 1990 and 2020. Case–control, cross-sectional, cohort and randomised controlled studies evaluating performance of diagnostic and prognostic host-response transcriptomic signatures in PLHIV of all ages and settings will be included. Eligible studies will include PLHIV in signature test or validation cohorts, and use microbiological, clinical, or composite reference standards for pulmonary or extrapulmonary tuberculosis diagnosis. Study quality will be evaluated using the ‘Quality Assessment of Diagnostic Accuracy Studies-2’ tool and cumulative review evidence assessed using the ‘Grading of Recommendations Assessment, Development and Evaluation’ approach. Study selection, quality appraisal and data extraction will be performed independently by two reviewers. Study, cohort and signature characteristics of included studies will be tabulated, and a narrative synthesis of findings presented. Primary outcomes of interest, biomarker sensitivity and specificity with estimate precision, will be summarised in forest plots. Expected heterogeneity in signature characteristics, study settings, and study designs precludes meta-analysis and pooling of results. Review reporting will follow the Preferred Reporting Items for Systematic Reviews and Meta-Analyses of Diagnostic Test Accuracy Studies guidelines.Ethics and dissemination Formal ethics approval is not required as primary human participant data will not be collected. Results will be disseminated through peer-reviewed publication and conference presentation.PROSPERO registration number CRD42021224155.

Published

2021

5. Validation of a host blood transcriptomic biomarker for pulmonary tuberculosis in people living with HIV: a prospective diagnostic and prognostic accuracy study

Author

Simon C Mendelsohn, MBChB, Andrew Fiore-Gartland, PhD, Adam Penn-Nicholson, PhD, Humphrey Mulenga, MPH, Stanley Kimbung Mbandi, PhD, Bhavesh Borate, MS, Katie Hadley, PhD, Chris Hikuam, PhD, Munyaradzi Musvosvi, PhD, Nicole Bilek, PhD, Mzwandile Erasmus, BSc, Lungisa Jaxa, BTech, Rodney Raphela, BSc, Onke Nombida, GT, Masooda Kaskar, MBChB, Tom Sumner, PhD, Richard G White, PhD, Craig Innes, MBChB, William Brumskine, MBChB, Andriëtte Hiemstra, MBChB, Stephanus T Malherbe, MBChB, Razia Hassan-Moosa, MPH, Michèle Tameris, MBChB, Gerhard Walzl, MBChB, Kogieleum Naidoo, PhD, Gavin Churchyard, PhD, Thomas J Scriba, DPhil, Mark Hatherill, ProfMD, Charmaine Abrahams, Hadn Africa, Petri Ahlers, Denis Arendsen, Tebogo Badimo, Kagiso Baepanye, Kesenogile Edna Baepanye, Bianca Bande, Nomfuneko Cynthia Batyi, Roslyn Beukes, Laudicia Tshenolo Bontsi, Obakeng Peter Booi, Mari Cathrin Botha, Samentra Braaf, Sivuyile Buhlungu, Alida Carstens, Kgomotso Violet Chauke, Thilagavathy Chinappa, Eva Chung, Michelle Chung, Ken Clarke, Yolundi Cloete, Lorraine Coetzee, Marelize Collignon, Alessandro Companie, Cara-mia Corris, Mooketsi Theophillius Cwaile, Thobelani Cwele, Ilse Davids, Isabella Johanna Davies, Emilia De Klerk, Marwou de Kock, Audrey Lebohang Dhlamini, Bongani Diamond, Maria Didloff, Celaphiwe Dlamini, Palesa Dolo, Candice Eyre, Tebogo Feni, Juanita Ferreira, Christal Ferus, Michelle Fisher, Marika Flinn, Bernadine Fransman, Welseh Phindile Galane, Hennie Geldenhuys, Diann Gempies, Thelma Goliath, Dhineshree Govender, Yolande Gregg, Goodness Gumede, Zanele Gwamada, Senzo Halti, Rieyaat Hassiem, Roxane Herling, Yulandi Herselman, Ellis Hughes, Henry Issel, Blanchard Mbay Iyemosolo, Zandile Jali, Bonita Janse Van Rensburg, Ruwiyda Jansen, James Michael Jeleni, Olebogeng Jonkane, Fabio Julies, Fazlin Kafaar, Christian Mabika Kasongo, Sophie Keffers, Boitumelo Sophy Kekana, Sebaetseng Jeanette Kekana, Xoliswa Kelepu, Lungile Khanyile, Gomotsegang Virginia Khobedi, Gloria Khomba, Lucky Sipho Khoza, Marietjie King, Gloria Keitumetse Kolobe, Sandra Kruger, Jaftha Kruger, Ndlela Israel Kunene, Sunelza Lakay, Aneesa Lakhi, Nondumiso Langa, Hildah Ledwaba, Lerato Julia Lekagane, Sheiley Christina Lekotloane, Thelma Leopeng, Ilze Jeanette Louw, Angelique Kany Kany Luabeya, Sarah Teboso Lusale, Perfect Tiisetso Maatjie, Immaculate Mabasa, Tshegofatso Dorah Mabe, Kamogelo Fortunate Mabena, Nkosinathi Charles Mabuza, Simbarashe Mabwe, Johanna Thapelo Madikwe, Octavia Mahkosazana Madikwe, Rapontwana Letlhogonolo Maebana, Malobisa Sylvester Magwasha, Molly Majola, Mantai Makhetha, Lebohang Makhethe, Vernon Malay, Vutlhari-I-Vunhenha Fairlord Manzini, Jabu Maphanga, Nonhle Maphanga, Juanita Market, Isholedi Samuel Maroele, Omphile Petunia Masibi, July Rocky Mathabanzini, Tendamudzimu Ivan Mathode, Ellen Ditaba Matsane, Lungile Mbata, Faheema Meyer, Nyasha Karen Mhandire, Thembisiwe Miga, Nosisa Charity Thandeka Mkhize, Caroline Mkhokho, Neo Hilda Mkwalase, Nondzakazi Mnqonywa, Karabo Moche, Brenda Matshidiso Modisaotsile, Patricia Pakiso Mokgetsengoane, Selemeng Matseliso Carol Mokone, Kegomoditswe Magdeline Molatlhegi, Thuso Andrew Molefe, Joseph Panie Moloko, Kabelo Molosi, Motlatsi Evelyn Molotsi, Tebogo Edwin Montwedi, Boikanyo Dinah Monyemangene, Hellen Mokopi Mooketsi, Miriam Moses, Boitumelo Mosito, Tshplpfelo Mapula Mosito, Ireen Lesebang Mosweu, Primrose Mothaga, Banyana Olga Motlagomang, Angelique Mouton, Onesisa Mpofu, Funeka Nomvula Mthembu, Mpho Mtlali, Nhlamulo Ndlovu, Nompumelelo Ngcobo, Julia Noble, Bantubonke Bertrum Ntamo, Gloria Ntanjana, Tedrius Ntshauba, Fajwa Opperman, Nesri Padayatchi, Thandiwe Papalagae, Christel Petersen, Themba Phakathi, Mapule Ozma Phatshwane, Patiswa Plaatjie, Abe Pretorius, Victor Kgothatso Rameetse, Dirhona Ramjit, Frances Ratangee, Maigan Ratangee, Pearl Nomsa Sanyaka, Alicia Sato, Elisma Schoeman, Constance Schreuder, Letlhogonolo Seabela, Kelebogile Magdeline Segaetsho, Ni Ni Sein, Raesibe Agnes Pearl Selepe, Melissa Neo Senne, Alison September, Cashwin September, Moeti Serake, Justin Shenje, Thandiwe Shezi, Sifiso Cornelius Shezi, Phindile Sing, Chandrapharbha Singh, Zona Sithetho, Dorothy Solomons, Kim Stanley, Marcia Steyn, Bongiwe Stofile, Sonia Stryers, Liticia Swanepoel, Anne Swarts, Mando Mmakhora Thaba, Lethabo Collen Theko, Philile Thembela, Mugwena Thompo, Asma Toefy, Khayalethu Toto, Dimakatso Sylvia Tsagae, Ayanda Tsamane, Vincent Tshikovhi, Lebogang Isaac Tswaile, Petrus Tyambetyu, Susanne Tönsing, Habibullah Valley, Linda van der Merwe, Elma van Rooyen, Ashley Veldsman, Helen Veldtsman, Kelvin Vollenhoven, Londiwe Zaca, Elaine Zimri, and Mbali Zulu

Subjects

Public aspects of medicine, RA1-1270

Abstract

Summary: Background: A rapid, blood-based triage test that allows targeted investigation for tuberculosis at the point of care could shorten the time to tuberculosis treatment and reduce mortality. We aimed to test the performance of a host blood transcriptomic signature (RISK11) in diagnosing tuberculosis and predicting progression to active pulmonary disease (prognosis) in people with HIV in a community setting. Methods: In this prospective diagnostic and prognostic accuracy study, adults (aged 18–59 years) with HIV were recruited from five communities in South Africa. Individuals with a history of tuberculosis or household exposure to multidrug-resistant tuberculosis within the past 3 years, comorbid risk factors for tuberculosis, or any condition that would interfere with the study were excluded. RISK11 status was assessed at baseline by real-time PCR; participants and study staff were masked to the result. Participants underwent active surveillance for microbiologically confirmed tuberculosis by providing spontaneously expectorated sputum samples at baseline, if symptomatic during 15 months of follow-up, and at 15 months (the end of the study). The coprimary outcomes were the prevalence and cumulative incidence of tuberculosis disease confirmed by a positive Xpert MTB/RIF, Xpert Ultra, or Mycobacteria Growth Indicator Tube culture, or a combination of such, on at least two separate sputum samples collected within any 30-day period. Findings: Between March 22, 2017, and May 15, 2018, 963 participants were assessed for eligibility and 861 were enrolled. Among 820 participants with valid RISK11 results, eight (1%) had prevalent tuberculosis at baseline: seven (2·5%; 95% CI 1·2–5·0) of 285 RISK11-positive participants and one (0·2%; 0·0–1·1) of 535 RISK11-negative participants. The relative risk (RR) of prevalent tuberculosis was 13·1 times (95% CI 2·1–81·6) greater in RISK11-positive participants than in RISK11-negative participants. RISK11 had a diagnostic area under the receiver operating characteristic curve (AUC) of 88·2% (95% CI 77·6–96·7), and a sensitivity of 87·5% (58·3–100·0) and specificity of 65·8% (62·5–69·0) at a predefined score threshold (60%). Of those with RISK11 results, eight had primary endpoint incident tuberculosis during 15 months of follow-up. Tuberculosis incidence was 2·5 per 100 person-years (95% CI 0·7–4·4) in the RISK11-positive group and 0·2 per 100 person-years (0·0–0·5) in the RISK11-negative group. The probability of primary endpoint incident tuberculosis was greater in the RISK11-positive group than in the RISK11-negative group (cumulative incidence ratio 16·0 [95% CI 2·0–129·5]). RISK11 had a prognostic AUC of 80·0% (95% CI 70·6–86·9), and a sensitivity of 88·6% (43·5–98·7) and a specificity of 68·9% (65·3–72·3) for incident tuberculosis at the 60% threshold. Interpretation: RISK11 identified prevalent tuberculosis and predicted risk of progression to incident tuberculosis within 15 months in ambulant people living with HIV. RISK11's performance approached, but did not meet, WHO's target product profile benchmarks for screening and prognostic tests for tuberculosis. Funding: Bill & Melinda Gates Foundation and the South African Medical Research Council.

Published

2021

6. Regional changes in tuberculosis disease burden among adolescents in South Africa (2005-2015).

Author

Erick Wekesa Bunyasi, Humphrey Mulenga, Angelique K K Luabeya, Justin Shenje, Simon C Mendelsohn, Elisa Nemes, Michele Tameris, Robin Wood, Thomas J Scriba, and Mark Hatherill

Subjects

Medicine, Science

Abstract

BACKGROUND:Adolescents in the Western Cape Province of South Africa had high force of Mycobacterium tuberculosis (MTB) infection (14% per annum) and high TB incidence (710 per 100,000 person-years) in 2005. We describe subsequent temporal changes in adolescent TB disease notification rates for the decade 2005-2015. METHOD:We conducted an analysis of patient-level adolescent (age 10-19 years) TB disease data, obtained from an electronic TB register in the Breede Valley sub-district, Western Cape Province, South Africa, for 2005-2015. Numerators were annual TB notifications (HIV-related and HIV-unrelated); denominators were mid-year population estimates. Period averages of TB rates were obtained using time series modeling. Temporal trends in TB rates were explored using the Mann-Kendall test. FINDINGS:The average adolescent TB disease notification rate was 477 per 100,000 for all TB patients (all-TB) and 361 per 100,000 for microbiologically-confirmed patients. The adolescent all-TB rate declined by 45% from 662 to 361 per 100,000 and the microbiologically-confirmed TB rate by 38% from 492 to 305 per 100,000 between 2005-2015, driven mainly by rapid decreases for the period 2005-2009. There was a statistically significant negative temporal trend in both all-TB (per 100,000) (declined by 48%; from 662 to 343; p = 0·028) and microbiologically confirmed TB (per 100,000) (declined by 49%; from 492 to 252; p = 0·027) for 2005-2009, which was not observed for the period 2009-2015 (rose 5%; from 343 to 361; p = 0·764 and rose 21%; from 252 to 305; p = 1·000, respectively). INTERPRETATION:We observed an encouraging fall in adolescent TB disease rates between 2005-2009 with a subsequent plateau during 2010-2015, suggesting that additional interventions are needed to sustain initial advances in TB control.

Published

2020

7. Performance of diagnostic and predictive host blood transcriptomic signatures for Tuberculosis disease: A systematic review and meta-analysis.

Author

Humphrey Mulenga, Chambrez-Zita Zauchenberger, Erick W Bunyasi, Stanley Kimbung Mbandi, Simon C Mendelsohn, Benjamin Kagina, Adam Penn-Nicholson, Thomas J Scriba, and Mark Hatherill

Subjects

Medicine, Science

Abstract

IntroductionHost blood transcriptomic biomarkers have potential as rapid point-of-care triage, diagnostic, and predictive tests for Tuberculosis disease. We aimed to summarise the performance of host blood transcriptomic signatures for diagnosis of and prediction of progression to Tuberculosis disease; and compare their performance to the recommended World Health Organisation target product profile.MethodsA systematic review and meta-analysis of the performance of host blood mRNA signatures for diagnosing and predicting progression to Tuberculosis disease in HIV-negative adults and adolescents, in studies with an independent validation cohort. Medline, Scopus, Web of Science, and EBSCO libraries were searched for articles published between January 2005 and May 2019, complemented by a search of bibliographies. Study selection, data extraction and quality assessment were done independently by two reviewers. Meta-analysis was performed for signatures that were validated in ≥3 comparable cohorts, using a bivariate random effects model.ResultsTwenty studies evaluating 25 signatures for diagnosis of or prediction of progression to TB disease in a total of 68 cohorts were included. Eighteen studies evaluated 24 signatures for TB diagnosis and 17 signatures met at least one TPP minimum performance criterion. Three diagnostic signatures were validated in clinically relevant cohorts to differentiate TB from other diseases, with pooled sensitivity 84%, 87% and 90% and pooled specificity 79%, 88% and 74%, respectively. Four studies evaluated signatures for progression to TB disease and performance of one signature, assessed within six months of TB diagnosis, met the minimal TPP for a predictive test for progression to TB disease.ConclusionHost blood mRNA signatures hold promise as triage tests for TB. Further optimisation is needed if mRNA signatures are to be used as standalone diagnostic or predictive tests for therapeutic decision-making.

Published

2020

8. Prospective multicentre head-to-head validation of host blood transcriptomic biomarkers for pulmonary tuberculosis by real-time PCR

Author

Simon C. Mendelsohn, Stanley Kimbung Mbandi, Andrew Fiore-Gartland, Adam Penn-Nicholson, Munyaradzi Musvosvi, Humphrey Mulenga, Michelle Fisher, Katie Hadley, Mzwandile Erasmus, Onke Nombida, Michèle Tameris, Gerhard Walzl, Kogieleum Naidoo, Gavin Churchyard, Mark Hatherill, and Thomas J. Scriba

Subjects

Medicine

Abstract

Plain Language Summary Delays in tuberculosis (TB) diagnosis result in increased disease severity, risk of death, and infection of further individuals. The presence of symptoms is typically used to find people with TB. However, about half of individuals with TB are asymptomatic. We evaluated blood samples from individuals living in areas with high incidence of TB to see whether there were changes in components of the blood following infection with TB. Markers were identified that diagnosed TB in symptomatic adults, but were not as accurate to detect TB in those without symptoms. Most markers tested were able to accurately predict progression to TB within 6 months in HIV-uninfected individuals. These markers in the blood could enable the screening of symptomatic adults and predict TB risk, thus enabling targeting of therapy.

Published

2022

9. The impact of blood transcriptomic biomarker targeted tuberculosis preventive therapy in people living with HIV: a mathematical modelling study

Author

Tom Sumner, Simon C. Mendelsohn, Thomas J. Scriba, Mark Hatherill, and Richard G. White

Subjects

Tuberculosis, HIV, Preventive therapy, Biomarker, Modelling, Medicine

Abstract

Abstract Background Tuberculosis (TB) preventive therapy is recommended for all people living with HIV (PLHIV). Despite the elevated risk of TB amongst PLHIV, most of those eligible for preventive therapy would never develop TB. Tests which can identify individuals at greatest risk of disease would allow more efficient targeting of preventive therapy. Methods We used mathematical modelling to estimate the potential impact of using a blood transcriptomic biomarker (RISK11) to target preventive therapy amongst PLHIV. We compared universal treatment to RISK11 targeted treatment and explored the effect of repeat screening of the population with RISK11. Results Annual RISK11 screening, with preventive therapy provided to those testing positive, could avert 26% (95% CI 13–34) more cases over 10 years compared to one round of universal treatment. For the cost per case averted to be lower than universal treatment, the maximum cost of the RISK11 test was approximately 10% of the cost of preventive therapy. The benefit of RISK11 screening may be greatest amongst PLHIV on ART (compared to ART naïve individuals) due to the increased specificity of the test in this group. Conclusions Biomarker targeted preventive therapy may be more effective than universal treatment amongst PLHIV in high incidence settings but would require repeat screening.

Published

2021

10. The effect of host factors on discriminatory performance of a transcriptomic signature of tuberculosis risk

Author

Humphrey Mulenga, Andrew Fiore-Gartland, Simon C. Mendelsohn, Adam Penn-Nicholson, Stanley Kimbung Mbandi, Bhavesh Borate, Munyaradzi Musvosvi, Michèle Tameris, Gerhard Walzl, Kogieleum Naidoo, Gavin Churchyard, Thomas J. Scriba, and Mark Hatherill

Subjects

Mycobacterium tuberculosis, Transcriptomic, Signature, RNA, Host factors, Performance, Medicine, Medicine (General), R5-920

Abstract

Summary: Background: We aimed to understand host factors that affect discriminatory performance of a transcriptomic signature of tuberculosis risk (RISK11). Methods: HIV-negative adults aged 18–60 years were evaluated in a prospective study of RISK11 and surveilled for tuberculosis through 15 months. Generalised linear models and receiver-operating characteristic (ROC) regression were used to estimate effect of host factors on RISK11 score (%marginal effect) and on discriminatory performance for tuberculosis disease (area under the curve, AUC), respectively. Findings: Among 2923 participants including 74 prevalent and 56 incident tuberculosis cases, percentage marginal effects on RISK11 score were increased among those with prevalent tuberculosis (+18·90%, 95%CI 12·66−25·13), night sweats (+14·65%, 95%CI 5·39−23·91), incident tuberculosis (+7·29%, 95%CI 1·46−13·11), flu-like symptoms (+5·13%, 95%CI 1·58−8·68), and smoking history (+2·41%, 95%CI 0·89−3·93) than those without; and reduced in males (−6·68%, 95%CI −8·31−5·04) and with every unit increase in BMI (−0·13%, −95%CI −0·25−0·01). Adjustment for host factors affecting controls did not change RISK11 discriminatory performance. Cough was associated with 72·55% higher RISK11 score in prevalent tuberculosis cases. Stratification by cough improved diagnostic performance from AUC = 0·74 (95%CI 0·67−0·82) overall, to 0·97 (95%CI 0·90−1·00, p

Published

2022

11. Clinical predictors of pulmonary tuberculosis among South African adults with HIV

Author

Simon C. Mendelsohn, Andrew Fiore-Gartland, Denis Awany, Humphrey Mulenga, Stanley Kimbung Mbandi, Michèle Tameris, Gerhard Walzl, Kogieleum Naidoo, Gavin Churchyard, Thomas J. Scriba, and Mark Hatherill

Subjects

Tuberculosis, Mycobacterium tuberculosis, HIV, Clinical, Model, Prediction, Medicine (General), R5-920

Abstract

Summary: Background: Tuberculosis (TB) clinical prediction rules rely on presence of symptoms, however many undiagnosed cases in the community are asymptomatic. This study aimed to explore the utility of clinical factors in predicting TB among people with HIV not seeking care. Methods: Baseline data were analysed from an observational cohort of ambulant adults with HIV in South Africa. Participants were tested for Mycobacterium tuberculosis (Mtb) sensitisation (interferon-γ release assay, IGRA) and microbiologically-confirmed prevalent pulmonary TB disease at baseline, and actively surveilled for incident TB through 15 months. Multivariable LASSO regression with post-selection inference was used to test associations with Mtb sensitisation and TB disease. Findings: Between March 22, 2017, and May 15, 2018, 861 participants were enrolled; Among 851 participants included in the analysis, 94·5% were asymptomatic and 45·9% sensitised to Mtb. TB prevalence was 2·0% at baseline and incidence 2·3/100 person-years through 15 months follow-up. Study site was associated with baseline Mtb sensitisation (p 1000, p = 0·005) and antiretroviral initiation (aHR 1·48, 95%CI 1·01–929·93, p = 0·023) were independently associated with incident TB. Models incorporating clinical features alone performed poorly in diagnosing prevalent (AUC 0·65, 95%CI 0·44–0·85) or predicting progression to incident (0·67, 0·46–0·88) TB. Interpretation: CD4 count and antiretroviral initiation, proxies for immune status and HIV stage, were associated with Mtb sensitisation and TB disease. Inadequate performance of clinical prediction models may reflect predominantly subclinical disease diagnosed in this setting and unmeasured local site factors affecting transmission and progression. Funding: The CORTIS-HR study was funded by the Bill & Melinda Gates Foundation (OPP1151915) and by the Strategic Health Innovation Partnerships Unit of the South African Medical Research Council with funds received from the South African Department of Science and Technology. The regulatory sponsor was the University of Cape Town.

Published

2022

12. Isoniazid preventive therapy and tuberculosis transcriptional signatures in people with HIV

Author

Ethan D. Valinetz, Daniel Matemo, Jill K. Gersh, Lara L. Joudeh, Simon C. Mendelsohn, Thomas J. Scriba, Mark Hatherill, John Kinuthia, Anna Wald, Gerard A. Cangelosi, Ruanne V. Barnabas, Thomas R. Hawn, and David J. Horne

Subjects

Adult, Infectious Diseases, Cross-Sectional Studies, Immunology, Antitubercular Agents, Isoniazid, Immunology and Allergy, Humans, Tuberculosis, HIV Infections

Abstract

To examine the association between isoniazid preventive therapy (IPT) or nontuberculous mycobacteria (NTM) sputum culture positivity and tuberculosis (TB) transcriptional signatures in people with HIV.Cross-sectional study.We enrolled adults living with HIV who were IPT-naive or had completed IPT more than 6 months prior at HIV care clinics in western Kenya. We calculated TB signatures using gene expression data from qRT-PCR. We used multivariable linear regression to analyze the association between prior receipt of IPT or NTM sputum culture positivity with a transcriptional TB risk score, RISK6 (range 0-1). In secondary analyses, we explored the association between IPT or NTM positivity and four other TB transcriptional signatures.Among 381 participants, 99.7% were receiving antiretroviral therapy and 86.6% had received IPT (completed median of 1.1 years prior). RISK6 scores were lower (mean difference 0.10; 95% confidence interval (CI): 0.06-0.15; P 0.001) among participants who received IPT than those who did not. In a model that adjusted for age, sex, duration of ART, and plasma HIV RNA, the RISK6 score was 52.8% lower in those with a history of IPT ( P 0.001). No significant association between year of IPT receipt and RISK6 scores was detected. There was no association between NTM sputum culture positivity and RISK6 scores.In people with HIV, IPT was associated with significantly lower RISK6 scores compared with persons who did not receive IPT. These data support investigations of its performance as a TB preventive therapy response biomarker.

Published

2023

13. Therapeutic Monoclonal Antibodies for Ebola Virus Infection Derived from Vaccinated Humans

Author

Pramila Rijal, Sean C. Elias, Samara Rosendo Machado, Julie Xiao, Lisa Schimanski, Victoria O’Dowd, Terry Baker, Emily Barry, Simon C. Mendelsohn, Catherine J. Cherry, Jing Jin, Geneviève M. Labbé, Francesca R. Donnellan, Tommy Rampling, Stuart Dowall, Emma Rayner, Stephen Findlay-Wilson, Miles Carroll, Jia Guo, Xiao-Ning Xu, Kuan-Ying A. Huang, Ayato Takada, Gillian Burgess, David McMillan, Andy Popplewell, Daniel J. Lightwood, Simon J. Draper, and Alain R. Townsend

Subjects

Biology (General), QH301-705.5

Abstract

Summary: We describe therapeutic monoclonal antibodies isolated from human volunteers vaccinated with recombinant adenovirus expressing Ebola virus glycoprotein (EBOV GP) and boosted with modified vaccinia virus Ankara. Among 82 antibodies isolated from peripheral blood B cells, almost half neutralized GP pseudotyped influenza virus. The antibody response was diverse in gene usage and epitope recognition. Although close to germline in sequence, neutralizing antibodies with binding affinities in the nano- to pico-molar range, similar to “affinity matured” antibodies from convalescent donors, were found. They recognized the mucin-like domain, glycan cap, receptor binding region, and the base of the glycoprotein. A cross-reactive cocktail of four antibodies, targeting the latter three non-overlapping epitopes, given on day 3 of EBOV infection, completely protected guinea pigs. This study highlights the value of experimental vaccine trials as a rich source of therapeutic human monoclonal antibodies. : Most antibodies used for Ebola virus treatment originate from convalescent donors or highly immunized animals. Rijal et al. find that monoclonal antibodies isolated early after vaccination from humans can be powerfully therapeutic, despite the relative immaturity of their sequences. Vaccine trials therefore can provide a valuable source of therapeutic antibodies. Keywords: Ebola virus, human monoclonal antibodies, immunotherapy, therapeutic antibodies, guinea pig model, Ebola virus glycoprotein epitopes, E-S-FLU virus, antibody binding kinetics, affinity maturation

Published

2019

14. Molecular Detection of Airborne Mycobacterium tuberculosis in South African High Schools

Author

Jason R. Andrews, Erick Wekesa Bunyasi, Humphrey Mulenga, Mark Hatherill, Justin Shenje, Angelique Kany Kany Luabeya, Anastasia Koch, Simon C Mendelsohn, Keren Middelkoop, Zeenat Hoosen, Digby F. Warner, Robin Wood, Michele Tameris, and Thomas J. Scriba

Subjects

Pulmonary and Respiratory Medicine, Air filtration, medicine.medical_specialty, Average risk, Tuberculosis, biology, business.industry, education, Tb screening, Critical Care and Intensive Care Medicine, biology.organism_classification, medicine.disease, Sputum sample, Mycobacterium tuberculosis, Interquartile range, Co2 concentration, Internal medicine, medicine, business

Abstract

Rationale South African adolescents carry a high tuberculosis disease burden. It is not known if schools are high-risk settings for Mycobacterium tuberculosis (MTB) transmission. Objectives To detect airborne MTB genomic DNA in classrooms. Methods We studied 72 classrooms occupied by 1,836 students in two South African schools. High-volume air filtration was performed for median 40 minutes (interquartile range 35-54) and assayed by droplet digital PCR (ddPCR) targeting MTB Region of Difference 9 (RD9), with concurrent CO2 concentration measurement. Classroom data were benchmarked against public health clinics. Students who consented to individual TB screening completed a questionnaire and sputum collection (Xpert MTB/RIF Ultra) if symptom-positive. Poisson statistics were used for MTB RD9 copy quantification. Measurements and Main Results ddPCR assays were positive in 13/72 (18.1%) classroom and 4/39 (10.3%) clinic measurements (p=0.276). Median ambient CO2 concentration was 886 ppm (IQR 747-1223) in classrooms vs. 490 ppm (IQR 405-587) in clinics (p

Published

2022

15. Molecular Detection of Airborne

Author

Erick W, Bunyasi, Keren, Middelkoop, Anastasia, Koch, Zeenat, Hoosen, Humphrey, Mulenga, Angelique K K, Luabeya, Justin, Shenje, Simon C, Mendelsohn, Michele, Tameris, Thomas J, Scriba, Digby F, Warner, Robin, Wood, Jason R, Andrews, and Mark, Hatherill

Subjects

DNA, Bacterial, Male, Risk, Inhalation Exposure, South Africa, Cross-Sectional Studies, Schools, Adolescent, Air Microbiology, Humans, Tuberculosis, Female, Mycobacterium tuberculosis

Published

2023

16. The impact of blood transcriptomic biomarker targeted tuberculosis preventive therapy in people living with HIV: a mathematical modelling study

Author

Thomas J. Scriba, Tom Sumner, Simon C Mendelsohn, Mark Hatherill, Richard G. White, Department of Pathology, and Faculty of Health Sciences

Subjects

medicine.medical_specialty, Tuberculosis, Human immunodeficiency virus (HIV), Antitubercular Agents, HIV Infections, Disease, medicine.disease_cause, Tuberculosis preventive therapy, Modelling, Transcriptome, medicine, Isoniazid, Humans, Mass Screening, Intensive care medicine, business.industry, HIV, General Medicine, Biomarker, medicine.disease, Preventive therapy, Biomarker (medicine), Medicine, business, Biomarkers, Research Article

Abstract

Background Tuberculosis (TB) preventive therapy is recommended for all people living with HIV (PLHIV). Despite the elevated risk of TB amongst PLHIV, most of those eligible for preventive therapy would never develop TB. Tests which can identify individuals at greatest risk of disease would allow more efficient targeting of preventive therapy. Methods We used mathematical modelling to estimate the potential impact of using a blood transcriptomic biomarker (RISK11) to target preventive therapy amongst PLHIV. We compared universal treatment to RISK11 targeted treatment and explored the effect of repeat screening of the population with RISK11. Results Annual RISK11 screening, with preventive therapy provided to those testing positive, could avert 26% (95% CI 13–34) more cases over 10 years compared to one round of universal treatment. For the cost per case averted to be lower than universal treatment, the maximum cost of the RISK11 test was approximately 10% of the cost of preventive therapy. The benefit of RISK11 screening may be greatest amongst PLHIV on ART (compared to ART naïve individuals) due to the increased specificity of the test in this group. Conclusions Biomarker targeted preventive therapy may be more effective than universal treatment amongst PLHIV in high incidence settings but would require repeat screening.

Published

2021

17. Meeting report: 6th Global Forum on Tuberculosis Vaccines, 22–25 February 2022, Toulouse, France

Author

Carly Young, Sara Suliman, Virginie Rozot, and Simon C. Mendelsohn

Subjects

Infectious Diseases, General Veterinary, General Immunology and Microbiology, Public Health, Environmental and Occupational Health, Molecular Medicine

Published

2023

18. Peripheral Blood Mucosal-Associated Invariant T Cells in Tuberculosis Patients and Healthy Mycobacterium tuberculosis-Exposed Controls

Author

David M. Lewinsohn, Sarah K. Iwany, Fatoumatta Darboe, Anele Gela, James McCluskey, Zibiao Zhang, Mark Hatherill, Leonid Lecca, Thomas J. Scriba, Sidonia B G Eckle, Jamie Rossjohn, Kattya Lopez Tamara, D. Branch Moody, Megan Murray, Nicole Bilek, Alexandra J. Corbett, Segundo R. Leon, Roger Calderon, Sara Suliman, Ildiko Van Rhijn, Simon C Mendelsohn, Lars Kjer-Nielsen, Michelle Fisher, Simbarashe Mabwe, and Chuan-Chin Huang

Subjects

Adult, Male, 0301 basic medicine, Tuberculosis, Mucosal associated invariant T cell, Major histocompatibility complex, Risk Assessment, Mucosal-Associated Invariant T Cells, Immunophenotyping, Mycobacterium tuberculosis, Major Articles and Brief Reports, 03 medical and health sciences, 0302 clinical medicine, Antigen, Risk Factors, Prevalence, Humans, Immunology and Allergy, Medicine, Public Health Surveillance, biology, Cluster of differentiation, business.industry, Middle Aged, biology.organism_classification, medicine.disease, 3. Good health, 030104 developmental biology, Infectious Diseases, Case-Control Studies, Immunology, biology.protein, Female, business, Biomarkers, 030215 immunology, Mycobacterium

Abstract

Background In human blood, mucosal-associated invariant T (MAIT) cells are abundant T cells that recognize antigens presented on non-polymorphic major histocompatibility complex-related 1 (MR1) molecules. The MAIT cells are activated by mycobacteria, and prior human studies indicate that blood frequencies of MAIT cells, defined by cell surface markers, decline during tuberculosis (TB) disease, consistent with redistribution to the lungs. Methods We tested whether frequencies of blood MAIT cells were altered in patients with TB disease relative to healthy Mycobacterium tuberculosis-exposed controls from Peru and South Africa. We quantified their frequencies using MR1 tetramers loaded with 5-(2-oxopropylideneamino)-6-D-ribitylaminouracil. Results Unlike findings from prior studies, frequencies of blood MAIT cells were similar among patients with TB disease and latent and uninfected controls. In both cohorts, frequencies of MAIT cells defined by MR1-tetramer staining and coexpression of CD161 and the T-cell receptor alpha variable gene TRAV1-2 were strongly correlated. Disease severity captured by body mass index or TB disease transcriptional signatures did not correlate with MAIT cell frequencies in patients with TB. Conclusions Major histocompatibility complex (MHC)-related 1-restrictied MAIT cells are detected at similar levels with tetramers or surface markers. Unlike MHC-restricted T cells, blood frequencies of MAIT cells are poor correlates of TB disease but may play a role in pathophysiology.

Published

2020

19. Evaluation of a transcriptomic signature of tuberculosis risk in combination with an interferon gamma release assay: A diagnostic test accuracy study

Author

Humphrey Mulenga, Andrew Fiore-Gartland, Simon C. Mendelsohn, Adam Penn-Nicholson, Stanley Kimbung Mbandi, Elisa Nemes, Bhavesh Borate, Munyaradzi Musvosvi, Michèle Tameris, Gerhard Walzl, Kogieleum Naidoo, Gavin Churchyard, Thomas J. Scriba, and Mark Hatherill

Subjects

General Medicine

Abstract

We evaluated the diagnostic and prognostic performance of a transcriptomic signature of tuberculosis (TB) risk (RISK11) and QuantiFERON-TB Gold-plus (QFTPlus) as combination biomarkers of TB risk.Healthy South Africans who were HIV-negative aged 18-60 years with baseline RISK11 and QFTPlus results were evaluated in a prospective cohort study conducted between Sept 20, 2016 and Dec 20, 2019. Prevalence and incidence-rate ratios were used to evaluate risk of TB. Positive (LR+) and negative (LR-) likelihood ratios were used to compare individual tests versus Both-Positive (RISK11+/QFTPlus+) and Either-Positive (RISK11+ or QFTPlus+) combinations.Among 2912 participants, prevalent TB in RISK11+/QFTPlus+ participants was 13·3-fold (95% CI 4·2-42·7) higher than RISK11-/QFTPlus-; 2·4-fold (95% CI 1·2-4·8) higher than RISK11+/QFTPlus-; and 4·5-fold (95% CI 2·5-8·0) higher than RISK11-/QFTPlus+ participants. Risk of incident TB in RISK11+/QFTPlus+ participants was 8·3-fold (95% CI 2·5-27·0) higher than RISK11-/QFTPlus-; 2·5-fold (95% CI 1·0-6·6) higher than RISK11+/QFTPlus-; and 2·1-fold (95% CI 1·2-3·4) higher than RISK11-/QFTPlus+ participants, respectively. Compared to QFTPlus, the Both-Positive test combination increased diagnostic LR+ from 1·3 (95% CI 1·2-1·5) to 4·7 (95% CI 3·2-7·0), and prognostic LR+ from 1·4 (95% CI 1·2-1·5) to 2·8 (95% CI 1·5-5·1), but did not improve upon RISK11 alone. Compared with RISK11, the Either-Positive test combination decreased diagnostic LR- from 0·7 (95% CI 0·6-0·9) to 0·3 (95% CI 0·2-0·6), and prognostic LR- from 0·9 (95% CI 0·8-1·0) to 0·3 (0·1-0·7), but did not improve upon QFTPlus alone.Combining two tests such as RISK11 and QFTPlus, with discordant individual performance characteristics does not improve overall discriminatory performance, relative to the individual tests.Bill and Melinda Gates Foundation, South African Medical Research Council.

Published

2022

20. Mycobacterium tuberculosisinfection, immune activation, and risk of HIV acquisition

Author

Rachel A. Bender Ignacio, Jessica Long, Aparajita Saha, Felicia K. Nguyen, Lara Joudeh, Ethan Valinetz, Simon C. Mendelsohn, Thomas J. Scriba, Mark Hatherill, Holly Janes, Gavin Churchyard, Susan Buchbinder, Ann Duerr, Javeed A. Shah, and Thomas R. Hawn

Abstract

BackgroundAlthough immune activation is associated with HIV acquisition, the nature of inflammatory profiles that increase HIV risk, which may include responses toM. tuberculosis(Mtb) infection, are not well characterized.MethodsWe conducted a nested case-control study within the Step MRKAd5 HIV-1 vaccine study. PBMCs from the last HIV-negative sample from incident HIV cases and controls who did not acquire HIV were stimulated withMtb-specific antigens (ESAT-6/CFP-10) and analyzed by flow cytometry with intracellular cytokine staining.Combinatorialpolyfunctionality analysis ofantigen-specific T-cellsubsets (COMPASS) determined overallMtb-antigen-specific T cell activation. We measured inflammatory profiles with five Correlates of TB Risk (CoR) peripheral blood transcriptomic signatures. Conditional logistic regression analyses, adjusted for known predictors of HIV acquisition, were employed to assess whether either cellular markers of TB-associated immune activation or transcriptomic predictors of TB disease states were associated with HIV acquisition.ResultsAmong 465 participants, latentMtbinfection (LTBI) prevalence (21.5% controls vs 19.1% cases, p=0.51) andMtbantigen-specific polyfunctional CD4+ T cell COMPASS scores (aOR 0.96, 95% CI 0.77, 1.20) were not higher in those who acquired HIV. Two CoR signatures, Sweeney3 (aOR 1.38 (1.07, 1.78) per SD change) and RESPONSE5 (0.76 (0.60, 0.95)), were associated with HIV acquisition in multivariable analysis. The Sweeney3 signature best predicted odds of acquiring HIV in unadjusted and adjusted analyses, including when restricted to LTBI-negative participants.ConclusionsLTBI andMtbpolyfunctional antigen-specific CD4+ T cell immune activation were not identified as risk factors for HIV acquisition, but transcriptomic analyses demonstrated that two CoR signatures predicted HIV risk after adjustment for known behavioral and clinical risk factors. CoR signatures can demonstrate host gene expression associated with HIV acquisition, but the observed effects are likely not mediated throughMtbinfection.

Published

2021

21. Clinical predictors of pulmonary tuberculosis among South African adults with HIV

Author

Simon C. Mendelsohn, Andrew Fiore-Gartland, Denis Awany, Humphrey Mulenga, Stanley Kimbung Mbandi, Michèle Tameris, Gerhard Walzl, Kogieleum Naidoo, Gavin Churchyard, Thomas J. Scriba, and Mark Hatherill

Subjects

General Medicine

Abstract

Tuberculosis (TB) clinical prediction rules rely on presence of symptoms, however many undiagnosed cases in the community are asymptomatic. This study aimed to explore the utility of clinical factors in predicting TB among people with HIV not seeking care.Baseline data were analysed from an observational cohort of ambulant adults with HIV in South Africa. Participants were tested forBetween March 22, 2017, and May 15, 2018, 861 participants were enrolled; Among 851 participants included in the analysis, 94·5% were asymptomatic and 45·9% sensitised to Mtb. TB prevalence was 2·0% at baseline and incidence 2·3/100 person-years through 15 months follow-up. Study site was associated with baseline Mtb sensitisation (CD4 count and antiretroviral initiation, proxies for immune status and HIV stage, were associated with Mtb sensitisation and TB disease. Inadequate performance of clinical prediction models may reflect predominantly subclinical disease diagnosed in this setting and unmeasured local site factors affecting transmission and progression.The CORTIS-HR study was funded by the BillMelinda Gates Foundation (OPP1151915) and by the Strategic Health Innovation Partnerships Unit of the South African Medical Research Council with funds received from the South African Department of Science and Technology. The regulatory sponsor was the University of Cape Town.

Published

2021

22. Longitudinal Dynamics of a Blood Transcriptomic Signature of Tuberculosis

Author

Andrew-Fiore Gartland, Lungisa Jaxa, Humphrey Mulenga, Thomas J. Scriba, Hadn Africa, Stephanus T. Malherbe, Gavin J. Churchyard, Fazlin Kafaar, Craig Innes, Andriëtte Hiemstra, Slindile Mbhele, Mzwandile Erasmus, Stanley Kimbung Mbandi, Adam Penn-Nicholson, Shabaana A. Khader, Munyaradzi Musvosvi, Judi van Heerden, Chris Hikuam, Katie Hadley, Razia Hassan-Moosa, Mark Hatherill, Onke Nombida, Masooda Kaskar, Rodney Raphela, Gerhard Walzl, Kogieleum Naidoo, Balie Carstens, Mark P. Nicol, Simon C Mendelsohn, William Brumskine, Nicole Bilek, Michele Tameris, and Simbarashe Mabwe

Subjects

Pulmonary and Respiratory Medicine, Adult, Male, Tuberculosis, Adolescent, Anti-HIV Agents, Human immunodeficiency virus (HIV), Antitubercular Agents, HIV Infections, Critical Care and Intensive Care Medicine, medicine.disease_cause, Risk Assessment, Sensitivity and Specificity, Transcriptome, Mycobacterium tuberculosis, Young Adult, Clinical Decision Rules, Medicine, Humans, Longitudinal Studies, Respiratory system, Respiratory Tract Infections, Respiratory tract infections, biology, business.industry, Coinfection, Gene Expression Profiling, Middle Aged, biology.organism_classification, medicine.disease, Cross-Sectional Studies, Treatment Outcome, Immunology, Linear Models, Female, business, Biomarkers

Abstract

Objectives We evaluated longitudinal kinetics of an 11-gene blood transcriptomic tuberculosis (TB) signature, RISK11, and effects of TB preventative therapy (TPT) and respiratory organisms on RISK1...

Published

2021

23. The effect of host factors on discriminatory performance of a transcriptomic signature of tuberculosis risk

Author

Humphrey Mulenga, Andrew Fiore-Gartland, Simon C. Mendelsohn, Adam Penn-Nicholson, Stanley Kimbung Mbandi, Bhavesh Borate, Munyaradzi Musvosvi, Michèle Tameris, Gerhard Walzl, Kogieleum Naidoo, Gavin Churchyard, Thomas J. Scriba, and Mark Hatherill

Subjects

Adult, Male, Adolescent, General Medicine, Mycobacterium tuberculosis, Middle Aged, Prognosis, General Biochemistry, Genetics and Molecular Biology, Young Adult, ROC Curve, Humans, Tuberculosis, Prospective Studies, Transcriptome

Abstract

We aimed to understand host factors that affect discriminatory performance of a transcriptomic signature of tuberculosis risk (RISK11).HIV-negative adults aged 18-60 years were evaluated in a prospective study of RISK11 and surveilled for tuberculosis through 15 months. Generalised linear models and receiver-operating characteristic (ROC) regression were used to estimate effect of host factors on RISK11 score (%marginal effect) and on discriminatory performance for tuberculosis disease (area under the curve, AUC), respectively.Among 2923 participants including 74 prevalent and 56 incident tuberculosis cases, percentage marginal effects on RISK11 score were increased among those with prevalent tuberculosis (+18·90%, 95%CI 12·66-25·13), night sweats (+14·65%, 95%CI 5·39-23·91), incident tuberculosis (+7·29%, 95%CI 1·46-13·11), flu-like symptoms (+5·13%, 95%CI 1·58-8·68), and smoking history (+2·41%, 95%CI 0·89-3·93) than those without; and reduced in males (-6·68%, 95%CI -8·31- -5·04) and with every unit increase in BMI (-0·13%, 95%CI -0·25- -0·01). Adjustment for host factors affecting controls did not change RISK11 discriminatory performance. Cough was associated with 72·55% higher RISK11 score in prevalent tuberculosis cases. Stratification by cough improved diagnostic performance from AUC = 0·74 (95%CI 0·67-0·82) overall, to 0·97 (95%CI 0·90-1·00, p 0·001) in cough-positive participants. Combining host factors with RISK11 improved prognostic performance, compared to RISK11 alone, (AUC = 0·76, 95%CI 0·69-0·83 versus 0·56, 95%CI 0·46-0·68, p 0·001) over a 15-month predictive horizon.Several host factors affected RISK11 score, but only adjustment for cough affected diagnostic performance. Combining host factors with RISK11 should be considered to improve prognostic performance.Bill and Melinda Gates Foundation, South African Medical Research Council.

Published

2021

24. Prospective validation of host transcriptomic biomarkers for pulmonary tuberculosis by real-time PCR

Author

Munyaradzi Musvosvi, Humphrey Mulenga, Michelle Fisher, Adam Penn-Nicholson, Onke Nombida, Andrew Fiore-Gartland, Gerhard Walzl, Kogieleum Naidoo, Stanley Kimbung Mbandi, Simon C Mendelsohn, Mark Hatherill, Katie Hadley, Thomas J. Scriba, Mzwandile Erasmus, Gavin Churchyard, and Michele Tameris

Subjects

medicine.medical_specialty, Tuberculosis, business.industry, Product profile, Disease, medicine.disease, Asymptomatic, Triage, Real-time polymerase chain reaction, Pulmonary tuberculosis, Internal medicine, medicine, medicine.symptom, Pulmonary tb, business

Abstract

We tested performance of host-blood transcriptomic tuberculosis (TB) signatures for active case-finding. Among 20,207 HIV-uninfected and 963 HIV-infected adults screened; 2,923 and 861 were enrolled from five South African communities. Eight signatures were measured by microfluidic RT-qPCR and participants were microbiologically-investigated for pulmonary TB at baseline, and actively surveilled for incident disease through 15 months. Diagnostic AUCs for 61 HIV-uninfected (weighted-prevalence 1.1%) and 10 HIV-infected (prevalence 1.2%) prevalent TB cases for the 8 signatures were 0.63–0.79 and 0.65–0.88, respectively. Thereafter, 24 HIV-uninfected and 9 HIV-infected participants progressed to incident TB (1.1 and 1.0 per 100 person-years, respectively). Prognostic AUCs through 15-months follow-up were 0.49–0.66 and 0.54–0.81, respectively. Prognostic performance for incident TB occurring within 6-12 months in HIV-negative participants was higher for all signatures. None of the signatures met WHO Target Product Profile criteria for a triage test to diagnose asymptomatic TB; most signatures met the criteria for symptomatic TB. Prognostic accuracy of most signatures for incident TB within six months of testing met the criteria for an incipient TB test.

Published

2021

25. Meeting report: Virtual Global Forum on Tuberculosis Vaccines, 20-22 April 2021

Author

Virginie Rozot, Sara Suliman, Simon C Mendelsohn, Puck T. Pelzer, and Moagi Shaku

Subjects

Vaccine research, 2019-20 coronavirus outbreak, Tuberculosis, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Political science, Pipeline, Pandemic, medicine, Humans, BCG, Tuberculosis Vaccines, Pandemics, Funding, General Veterinary, General Immunology and Microbiology, business.industry, SARS-CoV-2, Public Health, Environmental and Occupational Health, COVID-19, Conference Report, Public relations, medicine.disease, Research findings, Infectious Diseases, Molecular Medicine, Tuberculosis vaccines, business, Vaccine

Abstract

The Global Forum on Tuberculosis (TB) Vaccines was held virtually from 20 to 22 April 2021, marking its 20th anniversary. The Global Forum on TB Vaccines is the world's largest gathering of stakeholders striving to develop new vaccines to prevent TB. The program included more than 60 speakers in 11 scientific sessions, panel discussions, and workshops. It provided an overview of the state of the field, and an opportunity to share the latest research findings, as well as new and innovative approaches to TB vaccine research and development (R&D). This year, it was held against the backdrop of the COVID-19 pandemic and convened researchers, developers, funders, and other stakeholders remotely to discuss opportunities and challenges for TB vaccine R&D in these unprecedented times.

Published

2021

26. Headway made towards biosignatures for incipient tuberculosis

Author

Simon C Mendelsohn and Thomas J. Scriba

Subjects

Pulmonary and Respiratory Medicine, Tuberculosis, Extramural, business.industry, Headway, MEDLINE, Medicine, Medical emergency, Automobile driving, business, medicine.disease

Published

2020

27. Therapeutic Monoclonal Antibodies for Ebola Virus Infection Derived from Vaccinated Humans

Author

Terry Baker, Francesca R. Donnellan, Geneviève M. Labbé, Andy Popplewell, Alain Townsend, Daniel John Lightwood, Gillian Burgess, Victoria O’Dowd, David McMillan, Jing Jin, Jia Guo, Pramila Rijal, Julie Xiao, Miles W. Carroll, Samara Rosendo Machado, Xiao-Ning Xu, Sean C. Elias, Simon J. Draper, Tommy Rampling, Catherine J. Cherry, Emma Rayner, Ayato Takada, Stuart D. Dowall, Lisa Schimanski, Stephen-Findlay Wilson, Kuan-Ying A. Huang, Emily Barry, and Simon C Mendelsohn

Subjects

0301 basic medicine, Male, viruses, therapeutic antibodies, medicine.disease_cause, 0601 Biochemistry and Cell Biology, Antibodies, Viral, Epitope, law.invention, Madin Darby Canine Kidney Cells, chemistry.chemical_compound, Ebola virus, 0302 clinical medicine, AFFINITY MATURATION, law, guinea pig model, PROTECTION, lcsh:QH301-705.5, Cells, Cultured, biology, Vaccination, GLYCOPROTEIN, NONHUMAN-PRIMATES, Antibodies, Monoclonal, Middle Aged, Ebolavirus, human monoclonal antibodies, Recombinant DNA, Female, immunotherapy, Antibody, MEDIATED NEUTRALIZATION, Life Sciences & Biomedicine, Adult, Adolescent, medicine.drug_class, Guinea Pigs, Monoclonal antibody, General Biochemistry, Genetics and Molecular Biology, Virus, NEUTRALIZING ANTIBODIES, Affinity maturation, 03 medical and health sciences, Young Adult, Dogs, medicine, Animals, Humans, Ebola Vaccines, VULNERABILITY, Science & Technology, Ebola virus glycoprotein epitopes, E-S-FLU virus, Cell Biology, Hemorrhagic Fever, Ebola, Virology, Antibodies, Neutralizing, antibody binding kinetics, 030104 developmental biology, HEK293 Cells, chemistry, lcsh:Biology (General), 1116 Medical Physiology, CELLS, biology.protein, Vaccinia, 030217 neurology & neurosurgery, RESPONSES, GENERATION

Abstract

Summary: We describe therapeutic monoclonal antibodies isolated from human volunteers vaccinated with recombinant adenovirus expressing Ebola virus glycoprotein (EBOV GP) and boosted with modified vaccinia virus Ankara. Among 82 antibodies isolated from peripheral blood B cells, almost half neutralized GP pseudotyped influenza virus. The antibody response was diverse in gene usage and epitope recognition. Although close to germline in sequence, neutralizing antibodies with binding affinities in the nano- to pico-molar range, similar to “affinity matured” antibodies from convalescent donors, were found. They recognized the mucin-like domain, glycan cap, receptor binding region, and the base of the glycoprotein. A cross-reactive cocktail of four antibodies, targeting the latter three non-overlapping epitopes, given on day 3 of EBOV infection, completely protected guinea pigs. This study highlights the value of experimental vaccine trials as a rich source of therapeutic human monoclonal antibodies. : Most antibodies used for Ebola virus treatment originate from convalescent donors or highly immunized animals. Rijal et al. find that monoclonal antibodies isolated early after vaccination from humans can be powerfully therapeutic, despite the relative immaturity of their sequences. Vaccine trials therefore can provide a valuable source of therapeutic antibodies. Keywords: Ebola virus, human monoclonal antibodies, immunotherapy, therapeutic antibodies, guinea pig model, Ebola virus glycoprotein epitopes, E-S-FLU virus, antibody binding kinetics, affinity maturation

Published

2019

28. Biomarker-guided tuberculosis preventive therapy (CORTIS): a randomised controlled trial

Author

Thomas J Scriba, Andrew Fiore-Gartland, Adam Penn-Nicholson, Humphrey Mulenga, Stanley Kimbung Mbandi, Bhavesh Borate, Simon C Mendelsohn, Katie Hadley, Chris Hikuam, Masooda Kaskar, Munyaradzi Musvosvi, Nicole Bilek, Steven Self, Tom Sumner, Richard G White, Mzwandile Erasmus, Lungisa Jaxa, Rodney Raphela, Craig Innes, William Brumskine, Andriëtte Hiemstra, Stephanus T Malherbe, Razia Hassan-Moosa, Michèle Tameris, Gerhard Walzl, Kogieleum Naidoo, Gavin Churchyard, Mark Hatherill, Kesenogile Baepanye, Tshepiso Baepanye, Ken Clarke, Marelize Collignon, Audrey Dlamini, Candice Eyre, Tebogo Feni, Moogo Fikizolo, Phinda Galane, Thelma Goliath, Alia Gangat, Shirley Malefo-Grootboom, Elba Janse van Rensburg, Bonita Janse van Rensburg, Sophy Kekana, Marietjie Zietsman, Adrianne Kock, Israel Kunene, Aneessa Lakhi, Nondumiso Langa, Hilda Ledwaba, Marillyn Luphoko, Immaculate Mabasa, Dorah Mabe, Nkosinathi Mabuza, Molly Majola, Mantai Makhetha, Mpho Makoanyane, Blossom Makhubalo, Vernon Malay, Juanita Market, Selvy Matshego, Nontsikelelo Mbipa, Tsiamo Mmotsa, Sylvester Modipa, Samuel Mopati, Palesa Moswegu, Primrose Mothaga, Dorothy Muller, Grace Nchwe, Maryna Nel, Lindiwe Nhlangulela, Bantubonke Ntamo, Lawerence Ntoahae, Tedrius Ntshauba, Nomsa Sanyaka, Letlhogonolo Seabela, Pearl Selepe, Melissa Senne, MG Serake, Maria Thlapi, Vincent Tshikovhi, Lebogang Tswaile, Amanda van Aswegen, Lungile Mbata, Constance Takavamanya, Pedro Pinho, John Mdlulu, Marthinette Taljaard, Naydene Slabbert, Sharfuddin Sayed, Tanya Nielson, Ni Ni Sein, Dhineshree Govender, Tilagavathy Chinappa, Mbali Ignatia Zulu, Nonhle Bridgette Maphanga, Senzo Ralph Hlathi, Goodness Khanyisile Gumede, Thandiwe Yvonne Shezi, Jabulisiwe Lethabo Maphanga, Zandile Patrica Jali, Thobelani Cwele, Nonhlanhla Zanele Elsie Gwamanda, Celaphiwe Dlamini, Zibuyile Phindile Penlee Sing, Ntombozuko Gloria Ntanjana, Sphelele Simo Nzimande, Siyabonga Mbatha, Bhavna Maharaj, Atika Moosa, Cara-Mia Corris, Fazlin Kafaar, Hennie Geldenhuys, Angelique Kany Kany Luabeya, Justin Shenje, Natasja Botes, Susan Rossouw, Hadn Africa, Bongani Diamond, Samentra Braaf, Sonia Stryers, Alida Carstens, Ruwiyda Jansen, Simbarashe Mabwe, Roxane Herling, Ashley Veldsman, Lebohgang Makhete, Marcia Steyn, Sivuyile Buhlungu, Margareth Erasmus, Ilse Davids, Patiswa Plaatjie, Alessandro Companie, Frances Ratangee, Helen Veldtsman, Christel Petersen, Charmaine Abrahams, Miriam Moses, Xoliswa Kelepu, Yolande Gregg, Liticia Swanepoel, Nomsitho Magawu, Nompumelelo Cetywayo, Lauren Mactavie, Habibullah Valley, Elizabeth Filander, Nambitha Nqakala, Elizna Maasdorp, Justine Khoury, Belinda Kriel, Bronwyn Smith, Liesel Muller, Susanne Tonsing, Andre Loxton, Andriette Hiemstra, Petri Ahlers, Marika Flinn, Eva Chung, Michelle Chung, and Alicia Sato

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Tuberculosis, Antitubercular Agents, Disease, Tuberculosis preventive therapy, Drug Administration Schedule, law.invention, 03 medical and health sciences, South Africa, Young Adult, 0302 clinical medicine, Randomized controlled trial, law, Internal medicine, HIV Seronegativity, medicine, Isoniazid, Humans, Cumulative incidence, 030212 general & internal medicine, Adverse effect, business.industry, Transmission (medicine), Reverse Transcriptase Polymerase Chain Reaction, Incidence, Computational Biology, Articles, Mycobacterium tuberculosis, medicine.disease, RNA, Bacterial, 030104 developmental biology, Infectious Diseases, Treatment Outcome, Biomarker (medicine), Female, Rifampin, business, Transcriptome, Biomarkers

Abstract

Summary Background Targeted preventive therapy for individuals at highest risk of incident tuberculosis might impact the epidemic by interrupting transmission. We tested performance of a transcriptomic signature of tuberculosis (RISK11) and efficacy of signature-guided preventive therapy in parallel, using a hybrid three-group study design. Methods Adult volunteers aged 18–59 years were recruited at five geographically distinct communities in South Africa. Whole blood was sampled for RISK11 by quantitative RT-PCR assay from eligible volunteers without HIV, recent previous tuberculosis (ie

Published

2020

29. Regional changes in tuberculosis disease burden among adolescents in South Africa (2005–2015)

Author

Thomas J. Scriba, Mark Hatherill, Elisa Nemes, Erick Wekesa Bunyasi, Robin Wood, Justin Shenje, Humphrey Mulenga, Angelique Kany Kany Luabeya, Michele Tameris, and Simon C Mendelsohn

Subjects

Bacterial Diseases, RNA viruses, Male, Epidemiology, Adolescents, Pathology and Laboratory Medicine, Disease rates, Families, South Africa, 0302 clinical medicine, Immunodeficiency Viruses, Medicine and Health Sciences, Medicine, 030212 general & internal medicine, Tuberculosis Disease, Children, Multidisciplinary, biology, Incidence (epidemiology), Incidence, Age Factors, HIV diagnosis and management, Actinobacteria, Infectious Diseases, Medical Microbiology, HIV epidemiology, Viral Pathogens, Disease Notification, Viruses, Tuberculosis Diagnosis and Management, Female, Pathogens, Research Article, Tuberculosis, Infectious Disease Control, Adolescent, Science, 030231 tropical medicine, Microbiology, Mycobacterium tuberculosis, 03 medical and health sciences, Population estimate, Retroviruses, Humans, Microbial Pathogens, Bacteria, business.industry, Lentivirus, Organisms, Biology and Life Sciences, HIV, biology.organism_classification, medicine.disease, Tropical Diseases, Diagnostic medicine, Time series modeling, Age Groups, People and Places, Population Groupings, business, Demography

Abstract

Background Adolescents in the Western Cape Province of South Africa had high force of Mycobacterium tuberculosis (MTB) infection (14% per annum) and high TB incidence (710 per 100,000 person-years) in 2005. We describe subsequent temporal changes in adolescent TB disease notification rates for the decade 2005-2015. Method We conducted an analysis of patient-level adolescent (age 10-19 years) TB disease data, obtained from an electronic TB register in the Breede Valley sub-district, Western Cape Province, South Africa, for 2005-2015. Numerators were annual TB notifications (HIV-related and HIV-unrelated); denominators were mid-year population estimates. Period averages of TB rates were obtained using time series modeling. Temporal trends in TB rates were explored using the Mann-Kendall test. Findings The average adolescent TB disease notification rate was 477 per 100,000 for all TB patients (all-TB) and 361 per 100,000 for microbiologically-confirmed patients. The adolescent all-TB rate declined by 45% from 662 to 361 per 100,000 and the microbiologically-confirmed TB rate by 38% from 492 to 305 per 100,000 between 2005-2015, driven mainly by rapid decreases for the period 2005-2009. There was a statistically significant negative temporal trend in both all-TB (per 100,000) (declined by 48%; from 662 to 343; p = 0·028) and microbiologically confirmed TB (per 100,000) (declined by 49%; from 492 to 252; p = 0·027) for 2005-2009, which was not observed for the period 2009-2015 (rose 5%; from 343 to 361; p = 0·764 and rose 21%; from 252 to 305; p = 1·000, respectively). Interpretation We observed an encouraging fall in adolescent TB disease rates between 2005-2009 with a subsequent plateau during 2010-2015, suggesting that additional interventions are needed to sustain initial advances in TB control.

Published

2020

30. Colonization or Infection with Respiratory Viruses Is Associated with Elevated Tuberculosis Transcriptomic Signature of Risk Scores

Author

Simon C Mendelsohn, M. Tameris, Mark Hatherill, Erick Wekesa Bunyasi, Fazlin Kafaar, Thomas J. Scriba, Shabaana A. Khader, Humphrey Mulenga, Stanley Kimbung Mbandi, and Munyaradzi Musvosvi

Subjects

Mycoplasma pneumoniae, Tuberculosis, biology, business.industry, Area under the curve, medicine.disease_cause, medicine.disease, biology.organism_classification, Virus, Mycobacterium tuberculosis, medicine.anatomical_structure, Immunology, medicine, Respiratory system, business, Coronavirus, Respiratory tract

Abstract

Introduction Respiratory pathogens such as influenza viruses may play an influential role in the pathogenesis of TB by negatively affecting immunity against Mycobacterium tuberculosis (MTB) We discovered and validated a transcriptomic signature of risk (SOR), based on mRNA expression of 11 IFN stimulated genes (ISG), which prospectively differentiates between incident TB cases and healthy controls The SOR score is computed from expression abundance of multiple ISG transcript pairs in peripheral blood, whereby each pair functions as a ?vote? for or against TB risk We aimed to identify respiratory pathogens other than MTB that might also associate with this SOR score and test whether the SOR score differentiates between individuals with and without respiratory pathogens Methods We conducted a nested cross-sectional study of the upper respiratory tract microbiome Upon consent, participants were consecutively enrolled into the study and provided one nasopharyngeal, one oropharyngeal and a PAXgene blood sample Host blood SOR scores were computed from Ct values for each of the 11 genes, measured by microfluidic qRT-PCR We used multiplex real-time PCR to detect 33 pathogens including bacteria, viruses and fungi in the nasopharyngeal and oropharyngeal samples Multivariate linear regression was used to identify pathogens associated with, and estimate their effect on, the SOR score Wilcoxon rank sum tests and receiver-operating-characteristic (ROC) curves were used to differentiate participants with and without respiratory pathogens Results 1,000 HIV-negative volunteers aged between 18 and 60 years were enrolled 13 viral and nine bacterial pathogens were detected Overall prevalence of respiratory pathogens was 43%: 4% were viruses only, 35 8% bacteria only, and 3 2% were a combination of viruses and bacteria Influenza C, rhinoviruses, coronavirus OC43, adenoviruses, and mycoplasma pneumoniae were significantly associated (Table 1) with a high SOR score In ROC curve analysis the SOR score differentiated participants as follows;virus vs no-pathogen (area under the curve;AUC) AUC=0 72, 95% CI: 0 63-0 81, virus vs bacteria AUC=0 72, 95% CI: 0 63-0 81, bacteria vs no-pathogen AUC=0 51, 95% CI: 0 48-0 55 (no difference) Participants with either viruses only or both viruses and bacteria had significantly higher (P=0 001) SOR scores (median 47% and 43%, respectively) compared to participants without pathogens (median 14%) or participants with bacteria only (median 13%) Conclusion Participants with upper respiratory tract viral colonization or infection had elevated SOR scores, suggesting induction of interferon signalling Infection or colonization with respiratory viruses is likely to result in false positive results for other transcriptomic signatures of tuberculosis based on ISGs (Table Presented)

Published

2020

31. Blood transcriptional signatures for tuberculosis testing

Author

Mark Hatherill, Simon C Mendelsohn, Thomas J. Scriba, and Stanley Kimbung Mbandi

Subjects

Pulmonary and Respiratory Medicine, Tuberculosis, business.industry, MEDLINE, medicine.disease, Bioinformatics, Article, medicine, Humans, Prospective Studies, business, Lung, Tuberculosis, Pulmonary, Biomarkers

Abstract

Summary Background Blood transcriptional signatures are candidates for non-sputum triage or confirmatory tests of tuberculosis. Prospective head-to-head comparisons of their diagnostic accuracy in real-world settings are necessary to assess their clinical use. We aimed to compare the diagnostic accuracy of candidate transcriptional signatures identified by systematic review, in a setting with a high burden of tuberculosis and HIV. Methods We did a prospective observational study nested within a diagnostic accuracy study of sputum Xpert MTB/RIF (Xpert) and Xpert MTB/RIF Ultra (Ultra) tests for pulmonary tuberculosis. We recruited consecutive symptomatic adults aged 18 years or older self-presenting to a tuberculosis clinic in Cape Town, South Africa. Participants provided blood for RNA sequencing, and sputum samples for liquid culture and molecular testing using Xpert and Ultra. We assessed the diagnostic accuracy of candidate blood transcriptional signatures for active tuberculosis (including those intended to distinguish active tuberculosis from other diseases) identified by systematic review, compared with culture or Xpert MTB/RIF positivity as the standard reference. In our primary analysis, patients with tuberculosis were defined as those with either a positive liquid culture or Xpert result. Patients with missing blood RNA or sputum results were excluded. Our primary objective was to benchmark the diagnostic accuracy of candidate transcriptional signatures against the WHO target product profile (TPP) for a tuberculosis triage test. Findings Between Feb 12, 2016, and July 18, 2017, we obtained paired sputum and RNA sequencing data from 181 participants, 54 (30%) of whom had confirmed pulmonary tuberculosis. Of 27 eligible signatures identified by systematic review, four achieved the highest diagnostic accuracy with similar area under the receiver operating characteristic curves (Sweeney3: 90·6% [95% CI 85·6–95·6]; Kaforou25: 86·9% [80·9–92·9]; Roe3: 86·9% [80·3–93·5]; and BATF2: 86·8% [80·6–93·1]), independent of age, sex, HIV status, previous tuberculosis, or sputum smear result. At test thresholds that gave 70% specificity (the minimum WHO TPP specificity for a triage test), these four signatures achieved sensitivities between 83·3% (95% CI 71·3–91·0) and 90·7% (80·1–96·0). No signature met the optimum criteria, of 95% sensitivity and 80% specificity proposed by WHO for a triage test, or the minimum criteria (of 65% sensitivity and 98% specificity) for a confirmatory test, but all four correctly identified Ultra-positive, culture-negative patients. Interpretation Selected blood transcriptional signatures met the minimum WHO benchmarks for a tuberculosis triage test but not for a confirmatory test. Further development of the signatures is warranted to investigate their possible effects on clinical and health economic outcomes as part of a triage strategy, or when used as add-on confirmatory test in conjunction with the highly sensitive Ultra test for Mycobacterium tuberculosis DNA. Funding Royal Society Newton Advanced Fellowship, Wellcome Trust, National Institute of Health Research, and UK Medical Research Council.

Published

2020

32. Prospective Validation of a Host Blood Transcriptomic Biomarker for Pulmonary Tuberculosis in People Living with HIV: A Diagnostic and Prognostic Accuracy Study

Author

Humphrey Mulenga, Thomas J. Scriba, Cortis-Hr Study Team, Lungisa Jaxa, Michele Tameris, Gavin J. Churchyard, Richard G. White, Rodney Raphela, Katie Hadley, Nicole Bilek, William Brumskine, Andriëtte Hiemstra, Bhavesh Borate, Andrew Fiore-Gartland, Munyaradzi Musvosvi, Simon C Mendelsohn, Masooda Kaskar, Stanley Kimbung Mbandi, Gerhard Walzl, Tom Sumner, Adam Penn-Nicholson, Kogieleum Naidoo, Chris Hikuam, Mark Hatherill, Mzwandile Erasmus, Razia Hassan-Moosa, Onke Nombida, Craig Innes, and Stephanus T. Malherbe

Subjects

medicine.medical_specialty, Tuberculosis, business.industry, Human immunodeficiency virus (HIV), medicine.disease, medicine.disease_cause, QuantiFERON, Pulmonary tuberculosis, Informed consent, Internal medicine, Cohort, medicine, Biomarker (medicine), Cumulative incidence, business

Abstract

Background: We tested diagnostic and prognostic performance of a host blood transcriptomic signature of tuberculosis (RISK11) for screening of people living with HIV (PLHIV) in a prospective, community-based cohort. Methods: Ambulant adult volunteers living with HIV were enrolled at five South African sites. RISK11 status was assessed at baseline by real-time PCR. Participants and study staff were blinded to the result. Participants underwent active surveillance for microbiologically-confirmed tuberculosis from enrolment through 15 months. The primary outcomes were prevalence and cumulative incidence of two-sputum-sample positive tuberculosis in RISK11+ versus RISK11- participants. Findings: Among 820 participants with valid RISK11 results, eight (1%) tuberculosis cases were identified at baseline. Risk of prevalent tuberculosis was 13·1-fold (95%CI 2·1-81·6) greater in RISK11+ than RISK11- participants, with tuberculosis prevalence of 2·5% and 0·2%, respectively. RISK11 had diagnostic area under the receiver-operating-characteristic curve (AUC) 88·2%; sensitivity 87·5% and specificity 65·8% at the pre-defined threshold (60%).Thereafter, eight tuberculosis cases were identified through median 15 months follow-up. Tuberculosis incidence was 2·5 vs 0·2 per 100 person-years in RISK11+ compared to RISK11- participants with cumulative incidence ratio 16·0 (95%CI 2·0-129·5); AUC 80·0%; sensitivity 88·6% and specificity 68·9%. By comparison, QuantiFERON TB Gold-Plus (QFT) had a cumulative incidence ratio of 2·0 (95%CI 0·5-8·4); AUC 70·8%; sensitivity 62·1% and specificity 56·2%. Interpretation: RISK11 identified prevalent tuberculosis and predicted risk of progression to incident tuberculosis within 15 months in ambulant PLHIV. Performance approached the World Health Organization Target Product Profile benchmarks for screening and prognostic tests for tuberculosis. QFT performance fell short of the prognostic benchmark. Funding Statement: The study was funded by the Bill & Melinda Gates Foundation (BMGF) (OPP1151915) and by the Strategic Health Innovation Partnerships Unit of the South African Medical Research Council with funds received from the South African Department of Science and Technology. The BMGF contributed to the study design. The regulatory sponsor was the University of Cape Town. Declaration of Interests: AP-N, GW, GC, TJS, and MH report grants from the Bill & Melinda Gates Foundation, during the conduct of the study; AP-N and GW report grants from the South African Medical Research Council, during the conduct of the study; GW and TJS report grants from the South African National Research Foundation, during the conduct of the study. In addition, AP-N and TJS have patents of the RISK11 and RISK6 signatures pending; GW has a patent “TB diagnostic markers” (PCT/IB2013/054377) issued and a patent “Method for diagnosing TB” (PCT/IB2017/052142) pending. The remaining authors have no competing interests to declare. Ethics Approval Statement: The study protocol (Supplement) was approved by the Institutional Human Ethics Committees of each participating site. All participants provided written informed consent in their language of choice.

Published

2020

33. Host blood transcriptomic biomarkers of tuberculosis disease in people living with HIV: a systematic review protocol

Author

Humphrey Mulenga, Simon C Mendelsohn, Fatoumatta Darboe, Stanley Kimbung Mbandi, Mark Hatherill, Thomas J. Scriba, and Mary Shelton

Subjects

medicine.medical_specialty, Tuberculosis, MEDLINE, HIV & AIDS, HIV Infections, Disease, molecular diagnostics, medicine, Forest plot, Humans, Intensive care medicine, business.industry, Clinical study design, General Medicine, medicine.disease, Infectious Diseases, Cross-Sectional Studies, Systematic review, tuberculosis, Data extraction, Research Design, Cohort, Medicine, Transcriptome, business, Biomarkers, Systematic Reviews as Topic

Abstract

IntroductionCurrent tuberculosis triage and predictive tools offer poor accuracy and are ineffective for detecting asymptomatic disease in people living with HIV (PLHIV). Host tuberculosis transcriptomic biomarkers hold promise for diagnosing prevalent and predicting progression to incident tuberculosis and guiding further investigation, preventive therapy and follow-up. We aim to conduct a systematic review of performance of transcriptomic signatures of tuberculosis in PLHIV.Methods and analysisWe will search MEDLINE (PubMed), WOS Core Collection, Biological Abstracts, and SciELO Citation Index (Web of Science), Africa-Wide Information and General Science Abstracts (EBSCOhost), Scopus, and Cochrane Central Register of Controlled Trials databases for articles published in English between 1990 and 2020. Case–control, cross-sectional, cohort and randomised controlled studies evaluating performance of diagnostic and prognostic host-response transcriptomic signatures in PLHIV of all ages and settings will be included. Eligible studies will include PLHIV in signature test or validation cohorts, and use microbiological, clinical, or composite reference standards for pulmonary or extrapulmonary tuberculosis diagnosis. Study quality will be evaluated using the ‘Quality Assessment of Diagnostic Accuracy Studies-2’ tool and cumulative review evidence assessed using the ‘Grading of Recommendations Assessment, Development and Evaluation’ approach. Study selection, quality appraisal and data extraction will be performed independently by two reviewers. Study, cohort and signature characteristics of included studies will be tabulated, and a narrative synthesis of findings presented. Primary outcomes of interest, biomarker sensitivity and specificity with estimate precision, will be summarised in forest plots. Expected heterogeneity in signature characteristics, study settings, and study designs precludes meta-analysis and pooling of results. Review reporting will follow the Preferred Reporting Items for Systematic Reviews and Meta-Analyses of Diagnostic Test Accuracy Studies guidelines.Ethics and disseminationFormal ethics approval is not required as primary human participant data will not be collected. Results will be disseminated through peer-reviewed publication and conference presentation.PROSPERO registration numberCRD42021224155.

Published

2021

34. RISK6, a universal 6-gene transcriptomic signature of TB disease risk, diagnosis and treatment response

Author

Robin Wood, Nesri Padayatchi, Timothy R Sterling, Thomas J. Scriba, Nicole Bilek, Jayne S. Sutherland, Daniel E. Zak, Simon C Mendelsohn, Mark Hatherill, Kogieleum Naidoo, Fatoumatta Darboe, Willem A. Hanekom, Melissa Murphy, Sara Suliman, Stefan H. E. Kaufmann, Adam Penn-Nicholson, Stephanus T. Malherbe, Bruno B. Andrade, Megan Murray, Michelle Fisher, Stanley Kimbung Mbandi, D. Branch Moody, Ildiko Van Rhijn, Gerhard Walzl, Jill Winter, Novel N. Chegou, Carl A. Morrow, Mzwandile Erasmus, and Ethan G. Thompson

Subjects

Oncology, 0303 health sciences, medicine.medical_specialty, Tuberculosis, medicine.diagnostic_test, business.industry, Venous blood, Disease, medicine.disease, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, Positron emission tomography, Internal medicine, Immunopathology, Cohort, medicine, Biomarker (medicine), 030212 general & internal medicine, business, 030304 developmental biology, Subclinical infection

Abstract

Improved tuberculosis diagnostics and tools for monitoring treatment response are urgently needed. We developed a robust and simple, PCR-based host-blood transcriptomic signature, RISK6, for multiple applications: identifying individuals at risk of incident disease, as a screening test for subclinical or clinical tuberculosis, and for monitoring tuberculosis treatment. RISK6 utility was validated by blind prediction using quantitative real-time (qRT) PCR in seven independent cohorts.Prognostic performance significantly exceeded that of previous signatures discovered in the same cohort. Performance for diagnosing subclinical and clinical disease in HIV-uninfected and HIV-infected persons, assessed by area under the receiver-operating characteristic curve, exceeded 85%. As a screening test for tuberculosis, the sensitivity at 90% specificity met or approached the benchmarks set out in World Health Organization target product profiles for non-sputum-based tests. RISK6 scores correlated with lung immunopathology activity, measured by positron emission tomography, and tracked treatment response, demonstrating utility as treatment response biomarker, while predicting treatment failure prior to treatment initiation. Performance of the test in capillary blood samples collected by finger-prick was noninferior to venous blood collected in PAXgene tubes. These results support incorporation of RISK6 into rapid, capillary blood-based point-of-care PCR devices for prospective assessment in field studies.

Published

2019

35. Changes in Tuberculosis Disease Burden Among South African Adolescents, 2005-2015

Author

Humphrey Mulenga, Thomas J. Scriba, Elisa Nemes, Simon C Mendelsohn, Erick Wekesa Bunyasi, Robin Wood, Justin Shenje, Angelique Kany Kany Luabeya, Mark Hatherill, and Michele Tameris

Subjects

medicine.medical_specialty, education.field_of_study, Tuberculosis, Transmission (medicine), business.industry, Public health, Population, Psychological intervention, Census, medicine.disease, Confidence interval, Epidemiology, medicine, Population growth, education, business, Demography

Abstract

Background: South African adolescents have a high force of Mycobacterium tuberculosis (MTB) infection, exceeding 10% per annum, which acts as a barometer of tuberculosis (TB) transmission. We described temporal changes in adolescent TB notification rates to evaluate impact of TB and HIV control measures and inform public health strategy. Method: We conducted a cross-sectional analysis of patient-level TB case data obtained from a regional health authority in Western Cape Province, South Africa, for the decade 2005–2015. Numerators were annual TB notifications (HIV-related and HIV-unrelated); denominators were mid-year population estimates from the national census, adjusted for population growth. Period averages of TB rates were obtained using Auto-Regressive Integrated Moving Average (ARIMA) time series modeling. The Agresti Coull method was used to derive confidence intervals for TB rates. Temporal trends in TB rates were explored using the Mann-Kendall test. Findings: The average adolescent TB notification rate was 477 (95% Confidence Interval (CI): 313–641) per 100,000 for all cases (all-TB) and 361 (CI: 280–441) per 100,000 for microbiologically confirmed cases. However, the adolescent all-TB rate fell by 45% from 662 to 361 per 100,000 (p=0·005) and the microbiologically-confirmed TB rate by 38% from 492 to 305 per 100,000 (p=0·008) between 2005-2015, driven mainly by rapid decreases for the period 2005–2009 (p=0·028 and p=0·027, respectively). Between 2005–2009, 21% (156/732) of adolescent TB notifications were HIV tested, 12% (19/156) of whom were HIV-positive. In the general population, the proportion of HIV-positive persons receiving antiretroviral therapy (ART) increased from

Published

2019

36. Performance of host blood transcriptomic signatures for diagnosing and predicting progression to tuberculosis disease in HIV-negative adults and adolescents: a systematic review protocol

Author

Simon C Mendelsohn, Mark Hatherill, Thomas J. Scriba, Humphrey Mulenga, Erick Wekesa Bunyasi, Stanley Kimbung Mbandi, Benjamin M. Kagina, and Adam Penn-Nicholson

Subjects

Adult, medicine.medical_specialty, Tuberculosis, Adolescent, MEDLINE, Disease, Mycobacterium tuberculosis, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, HIV Seronegativity, Forest plot, medicine, False positive paradox, Protocol, Prevalence, Humans, 030212 general & internal medicine, 030304 developmental biology, Protocol (science), 0303 health sciences, biology, business.industry, General Medicine, transcriptomic, medicine.disease, biology.organism_classification, tuberculosis, sensitivity and specificity, Research Design, Cohort, Disease Progression, Public Health, business, Transcriptome, signature, Systematic Reviews as Topic

Abstract

IntroductionOne-quarter of the global population, including the majority of adults in tuberculosis (TB) endemic countries, are estimated to beMycobacterium tuberculosis(MTB) infected. An estimated 10 million new TB cases occurred in 2017. One of the biggest challenges confronting TB control is the lack of accurate diagnosis and prediction of prevalent and incident TB disease, respectively. Several host blood transcriptomic messenger RNA (mRNA) signatures that reflect the host immune response following infection with MTB and progression to TB disease in different study populations have recently been published, but these TB biomarkers have not been systematically described. We will conduct a systematic review of the performance of host blood transcriptional signatures for TB diagnosis and prediction of progression to TB disease.Methods and analysisThis systematic review will involve conducting a comprehensive literature search of cohort, case–control, cross-sectional and randomised-controlled studies of the performance of host blood transcriptomic signatures for TB diagnosis and prediction of progression to TB disease. We will search Medline via PubMed, Scopus, Web of Science and EBSCO libraries, complemented by a search of bibliographies of selected articles for other relevant articles. The literature search will be restricted to studies published in English from 2005 to 2018 and conducted in HIV-uninfected adults and adolescents (≥12 years old). Forest plots and a narrative synthesis of the findings will be provided. The primary outcomes will be sensitivity, specificity, as well as true/false positives and true/false negatives. Heterogeneity resulting from differences in the design, composition and structure of individual signatures will preclude meta-analysis and pooling of results.Ethics and disseminationEthics approval is not required for this systematic review protocol. The results of this review will be disseminated through a peer-reviewed journal as well as conference presentations.PROSPERO registration numberCRD42017073817.

Published

2019

37. Performance of diagnostic and predictive host blood transcriptomic signatures for Tuberculosis disease: A systematic review and meta-analysis

Author

Erick Wekesa Bunyasi, Humphrey Mulenga, Stanley Kimbung Mbandi, Thomas J. Scriba, Chambrez-Zita Zauchenberger, Adam Penn-Nicholson, Simon C Mendelsohn, Mark Hatherill, and Benjamin M. Kagina

Subjects

Bacterial Diseases, 0301 basic medicine, Oncology, Critical Care and Emergency Medicine, Disease, Biochemistry, Medical Conditions, Mathematical and Statistical Techniques, 0302 clinical medicine, Medicine and Health Sciences, Medicine, 030212 general & internal medicine, Predictive testing, Multidisciplinary, biology, Statistics, Genomics, Metaanalysis, Actinobacteria, Infectious Diseases, Meta-analysis, Physical Sciences, Disease Progression, Tuberculosis Diagnosis and Management, Transcriptome Analysis, Research Article, medicine.medical_specialty, Tuberculosis, Science, MEDLINE, Research and Analysis Methods, Mycobacterium tuberculosis, 03 medical and health sciences, Tuberculosis diagnosis, Diagnostic Medicine, Internal medicine, Genetics, Humans, Statistical Methods, Bacteria, business.industry, Organisms, Biology and Life Sciences, Computational Biology, Tropical Diseases, Genome Analysis, biology.organism_classification, medicine.disease, Triage, 030104 developmental biology, Transcriptome, business, Biomarkers, Mathematics

Abstract

IntroductionHost blood transcriptomic biomarkers have potential as rapid point-of-care triage, diagnostic, and predictive tests for Tuberculosis disease. We aimed to summarise the performance of host blood transcriptomic signatures for diagnosis of and prediction of progression to Tuberculosis disease; and compare their performance to the recommended World Health Organisation target product profile.MethodsA systematic review and meta-analysis of the performance of host blood mRNA signatures for diagnosing and predicting progression to Tuberculosis disease in HIV-negative adults and adolescents, in studies with an independent validation cohort. Medline, Scopus, Web of Science, and EBSCO libraries were searched for articles published between January 2005 and May 2019, complemented by a search of bibliographies. Study selection, data extraction and quality assessment were done independently by two reviewers. Meta-analysis was performed for signatures that were validated in ≥3 comparable cohorts, using a bivariate random effects model.ResultsTwenty studies evaluating 25 signatures for diagnosis of or prediction of progression to TB disease in a total of 68 cohorts were included. Eighteen studies evaluated 24 signatures for TB diagnosis and 17 signatures met at least one TPP minimum performance criterion. Three diagnostic signatures were validated in clinically relevant cohorts to differentiate TB from other diseases, with pooled sensitivity 84%, 87% and 90% and pooled specificity 79%, 88% and 74%, respectively. Four studies evaluated signatures for progression to TB disease and performance of one signature, assessed within six months of TB diagnosis, met the minimal TPP for a predictive test for progression to TB disease.ConclusionHost blood mRNA signatures hold promise as triage tests for TB. Further optimisation is needed if mRNA signatures are to be used as standalone diagnostic or predictive tests for therapeutic decision-making.

Published

2020

38. The Students’ Health and Welfare Centres Organisation (SHAWCO) of the University of Cape Town: A review of the past 69 years

Author

Simon C Mendelsohn and David M Favara

Subjects

Gerontology, Economic growth, Students, Medical, Universities, Free clinic, business.industry, media_common.quotation_subject, General Medicine, History, 20th Century, History, 21st Century, film.subject, South Africa, film, Cape, Medicine, Community Health Services, Community development, business, Welfare, Social responsibility, Schools, Medical, media_common

Abstract

The Students' Health and Welfare Centres Organisation (SHAWCO) is a student-run non-profit community development organisation based at the University of Cape Town (UCT). In 2012, SHAWCO celebrates its 69th anniversary, making it the oldest active student-run free clinic in South Africa. Over the past 7 decades, SHAWCO has become an integral part of the UCT Faculty of Health Sciences. This article reviews its history, current activities, and plans for the future.

Published

2012

39. Indoor Air Quality and Tuberculosis Risk in Two South African Schools

Author

Simon C Mendelsohn, Erick Wekesa Bunyasi, Jason R. Andrews, Mark Hatherill, Angelique Kany Kany Luabeya, Anastasia Koch, M. Tameris, Justin Shenje, Digby F. Warner, Keren Middelkoop, Humphrey Mulenga, Thomas J. Scriba, and Robin Wood

Subjects

Indoor air quality, Tuberculosis, Geography, Environmental health, medicine, medicine.disease

40. IL27 gene expression distinguishes multisystem inflammatory syndrome in children from febrile illness in a South African cohort

Author

Timothy F. Spracklen, Simon C. Mendelsohn, Claire Butters, Heidi Facey-Thomas, Raphaella Stander, Debbie Abrahams, Mzwandile Erasmus, Richard Baguma, Jonathan Day, Christiaan Scott, Liesl J. Zühlke, George Kassiotis, Thomas J. Scriba, and Kate Webb

Subjects

COVID-19, multisystem inflammatory syndrome, children, South Africa, SARS-CoV-2, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionMultisystem inflammatory syndrome in children (MIS-C) is a severe acute inflammatory reaction to SARS-CoV-2 infection in children. There is a lack of data describing differential expression of immune genes in MIS-C compared to healthy children or those with other inflammatory conditions and how expression changes over time. In this study, we investigated expression of immune-related genes in South African MIS-C patients and controls.MethodsThe cohort included 30 pre-treatment MIS-C cases and 54 healthy non-inflammatory paediatric controls. Other controls included 34 patients with juvenile systemic lupus erythematosus, Kawasaki disease or other inflammatory conditions. Longitudinal post-treatment MIS-C specimens were available at various timepoints. Expression of 80 immune-related genes was determined by real-time quantitative PCR.ResultsA total of 29 differentially expressed genes were identified in pre-treatment MIS-C compared to healthy controls. Up-regulated genes were found to be overrepresented in innate immune pathways including interleukin-1 processing and pyroptosis. Post-treatment follow-up data were available for up to 1,200 hours after first treatment. All down-regulated genes and 17/18 up-regulated genes resolved to normal levels in the timeframe, and all patients clinically recovered. When comparing MIS-C to other febrile conditions, only IL27 expression could differentiate these two groups with high sensitivity and specificity.ConclusionsThese data indicate a unique 29-gene signature of MIS-C in South African children. The up-regulation of interleukin-1 and pyroptosis pathway genes highlights the role of the innate immune system in MIS-C. IL-27 is a potent anti-inflammatory and antiviral cytokine that may distinguish MIS-C from other conditions in our setting.

Published

2022