Infectious Diseases - Research Publications

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Author: Denholm, Justin × Author: Tong, Steven × Start date: 2000 ×

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    The APPRISE Virtual Biobank for Infectious Diseases
    Smith, MZ ; Turner, M ; Haurat, J ; Thevarajan, I ; Denholm, J ; Tong, SYC ; Matthews, G ; Bull, RA ; Martinello, M ; Mcmahon, J ; Imrie, A ; Pillai, PE (AUSTRALIAN GOVERNMENT, DEPT HEALTH & AGEING, 2023-11-16)
    The Australian Partnership for Preparedness Research on InfectiouS disease Emergencies (APPRISE) has developed a virtual biobank to support infectious disease research in Australia. The virtual biobank (https://apprise.biogrid.org.au) integrates access to existing distributed infectious disease biospecimen collections comprising multiple specimen types, including plasma, serum, and peripheral blood mononuclear cells. Through the development of a common data model, multiple collections can be searched simultaneously via a secure web portal. The portal enhances the visibility and searchability of existing collections within their current governance and custodianship arrangements. The portal is easily scalable for integration of additional collections.
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    ASCOT ADAPT study of COVID-19 therapeutics in hospitalised patients: an international multicentre adaptive platform trial
    Denholm, JT ; Venkatesh, B ; Davis, J ; Bowen, AC ; Hammond, NE ; Jha, V ; McPhee, G ; McQuilten, Z ; O'Sullivan, MVN ; Paterson, D ; Price, D ; Rees, M ; Roberts, J ; Jones, M ; Totterdell, J ; Snelling, T ; Trask, N ; Morpeth, S ; Tong, SYC (BMC, 2022-12-14)
    BACKGROUND: SARS-CoV-2 infection is associated with a significant risk of hospitalisation, death, and prolonged impact on quality of life. Evaluation of new treatment options and optimising therapeutic management of people hospitalised with SARS-CoV-2 infection remains essential, but rapid changes in pandemic conditions and potential therapies have limited the utility of traditional approaches to randomised controlled trials. METHODS: ASCOT ADAPT is an international, investigator-initiated, adaptive platform, randomised controlled trial of therapeutics for non-critically ill patients hospitalised with COVID-19. The study design is open label and pragmatic. Potential participants are hospitalised adults with PCR confirmed, symptomatic, SARS-CoV-2 infection, within 14 days of symptom onset. Domains include antiviral, antibody and anticoagulant interventions, with a composite primary outcome of 28-day mortality or progression to intensive-care level respiratory or haemodynamic support. Initial interventions include intravenous nafamostat and variable dose anticoagulation. A range of secondary endpoints, and substudies for specific domains and interventions are outlined. DISCUSSION: This paper presents the trial protocol and management structure, including international governance, remote site monitoring and biobanking activities and provides commentary on ethical and pragmatic considerations in establishing the ASCOT ADAPT trial under pandemic conditions. TRIAL REGISTRATION: Australian and New Zealand Clinical Trials Registry (ACTRN12620000445976) and ClinicalTrials.gov (NCT04483960).
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    Immune profiling of SARS-CoV-2 infection during pregnancy reveals NK cell and ?? T cell perturbations
    Habel, JR ; Chua, BY ; Kedzierski, L ; Selva, KJ ; Damelang, T ; Haycroft, ER ; Nguyen, THO ; Koay, H-F ; Nicholson, S ; McQuilten, HA ; Jia, X ; Allen, LF ; Hensen, L ; Zhang, W ; Sandt, CEVD ; Neil, JA ; Pragastis, K ; Lau, JSY ; Jumarang, J ; Allen, EK ; Amanant, F ; Krammer, F ; Wragg, KM ; Juno, JA ; Wheatley, AK ; Tan, H-X ; Pell, G ; Walker, S ; Audsley, J ; Reynaldi, A ; Thevarajan, I ; Denholm, JT ; Subbarao, K ; Davenport, MP ; Hogarth, PM ; Godfrey, DI ; Cheng, AC ; Tong, SYC ; Bond, K ; Williamson, DA ; McMahon, JH ; Thomas, PG ; Pannaraj, PS ; James, F ; Holmes, NE ; Smibert, OC ; Trubiano, JA ; Gordon, CL ; Chung, AW ; Whitehead, CL ; Kent, SJ ; Lappas, M ; Rowntree, LC ; Kedzierska, K (AMER SOC CLINICAL INVESTIGATION INC, 2023-03-22)
    Pregnancy poses a greater risk for severe COVID-19; however, underlying immunological changes associated with SARS-CoV-2 during pregnancy are poorly understood. We defined immune responses to SARS-CoV-2 in unvaccinated pregnant and nonpregnant women with acute and convalescent COVID-19, quantifying 217 immunological parameters. Humoral responses to SARS-CoV-2 were similar in pregnant and nonpregnant women, although our systems serology approach revealed distinct antibody and FcγR profiles between pregnant and nonpregnant women. Cellular analyses demonstrated marked differences in NK cell and unconventional T cell activation dynamics in pregnant women. Healthy pregnant women displayed preactivated NK cells and γδ T cells when compared with healthy nonpregnant women, which remained unchanged during acute and convalescent COVID-19. Conversely, nonpregnant women had prototypical activation of NK and γδ T cells. Activation of CD4+ and CD8+ T cells and T follicular helper cells was similar in SARS-CoV-2-infected pregnant and nonpregnant women, while antibody-secreting B cells were increased in pregnant women during acute COVID-19. Elevated levels of IL-8, IL-10, and IL-18 were found in pregnant women in their healthy state, and these cytokine levels remained elevated during acute and convalescent COVID-19. Collectively, we demonstrate perturbations in NK cell and γδ T cell activation in unvaccinated pregnant women with COVID-19, which may impact disease progression and severity during pregnancy.
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    Nafamostat Mesylate for Treatment of COVID-19 in Hospitalised Patients: A Structured, Narrative Review
    Hernandez-Mitre, MP ; Tong, SYC ; Denholm, JT ; Dore, GJ ; Bowen, AC ; Lewin, SR ; Venkatesh, B ; Hills, TE ; McQuilten, Z ; Paterson, DL ; Morpeth, SC ; Roberts, JA (ADIS INT LTD, 2022-10)
    The search for clinically effective antivirals against the severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) is ongoing. Repurposing of drugs licensed for non-coronavirus disease 2019 (COVID-19) indications has been extensively investigated in laboratory models and in clinical studies with mixed results. Nafamostat mesylate (nafamostat) is a drug licensed in Japan and Korea for indications including acute pancreatitis and disseminated intravascular coagulation. It is available only for continuous intravenous infusion. In vitro human lung cell line studies with nafamostat demonstrate high antiviral potency against SARS-CoV-2 (half maximal inhibitory concentration [IC50] of 0.0022 µM [compared to remdesivir 1.3 µM]), ostensibly via inhibition of the cellular enzyme transmembrane protease serine 2 (TMPRSS2) preventing viral entry into human cells. In addition, the established antithrombotic activity is hypothesised to be advantageous given thrombosis-associated sequelae of COVID-19. Clinical reports to date are limited, but indicate a potential benefit of nafamostat in patients with moderate to severe COVID-19. In this review, we will explore the pre-clinical, pharmacokinetic and clinical outcome data presently available for nafamostat as a treatment for COVID-19. The recruitment to ongoing clinical trials is a priority to provide more robust data on the safety and efficacy of nafamostat as a treatment for COVID-19.
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    Association between convalescent plasma treatment and mortality in COVID-19: a collaborative systematic review and meta-analysis of randomized clinical trials
    Axfors, C ; Janiaud, P ; Schmitt, AM ; Van't Hooft, J ; Smith, ER ; Haber, NA ; Abayomi, A ; Abduljalil, M ; Abdulrahman, A ; Acosta-Ampudia, Y ; Aguilar-Guisado, M ; Al-Beidh, F ; Alejandria, MM ; Alfonso, RN ; Ali, M ; AlQahtani, M ; AlZamrooni, A ; Anaya, J-M ; Ang, MAC ; Aomar, IF ; Argumanis, LE ; Averyanov, A ; Baklaushev, VP ; Balionis, O ; Benfield, T ; Berry, S ; Birocco, N ; Bonifacio, LB ; Bowen, AC ; Bown, A ; Cabello-Gutierrez, C ; Camacho, B ; Camacho-Ortiz, A ; Campbell-Lee, S ; Cao, DH ; Cardesa, A ; Carnate, JM ; Castillo, GJJ ; Cavallo, R ; Chowdhury, FR ; Chowdhury, FUH ; Ciccone, G ; Cingolani, A ; Climacosa, FMM ; Compernolle, V ; Cortez, CFN ; Neto, AC ; D'Antico, S ; Daly, J ; Danielle, F ; Davis, JS ; De Rosa, FG ; Denholm, JT ; Denkinger, CM ; Desmecht, D ; Diaz-Coronado, JC ; Diaz Ponce-Medrano, JA ; Donneau, A-F ; Dumagay, TE ; Dunachie, S ; Dungog, CC ; Erinoso, O ; Escasa, IMS ; Estcourt, LJ ; Evans, A ; Evasan, ALM ; Fareli, CJ ; Fernandez-Sanchez, V ; Galassi, C ; Gallo, JE ; Garcia, PJ ; Garcia, PL ; Garcia, JA ; Garigliany, M ; Garza-Gonzalez, E ; Gauiran, DT ; Gaviria Garcia, PA ; Giron-Gonzalez, J-A ; Gomez-Almaguer, D ; Gordon, AC ; Gothot, A ; Grass Guaqueta, JS ; Green, C ; Grimaldi, D ; Hammond, NE ; Harvala, H ; Heralde, FM ; Herrick, J ; Higgins, AM ; Hills, TE ; Hines, J ; Holm, K ; Hoque, A ; Hoste, E ; Ignacio, JM ; Ivanov, A ; Janssen, M ; Jennings, JH ; Jha, V ; King, RAN ; Kjeldsen-Kragh, J ; Klenerman, P ; Kotecha, A ; Krapp, F ; Labanca, L ; Laing, E ; Landin-Olsson, M ; Laterre, P-F ; Lim, L-L ; Lim, J ; Ljungquist, O ; Llaca-Diaz, JM ; Lopez-Robles, C ; Lopez-Cardenas, S ; Lopez-Plaza, I ; Lucero, JAC ; Lundgren, M ; Macias, J ; Maganito, SC ; Malundo, AFG ; Manrique, RD ; Manzini, PM ; Marcos, M ; Marquez, I ; Javier Martinez-Marcos, F ; Mata, AM ; McArthur, CJ ; McQuilten, ZK ; McVerry, BJ ; Menon, DK ; Meyfroidt, G ; Mirasol, MAL ; Misset, B ; Molton, JS ; Mondragon, A ; Monsalve, DM ; Choghakabodi, PM ; Morpeth, SC ; Mouncey, PR ; Moutschen, M ; Muller-Tidow, C ; Murphy, E ; Najdovski, T ; Nichol, AD ; Nielsen, H ; Novak, RM ; O'Sullivan, MVN ; Olalla, J ; Osibogun, A ; Osikomaiya, B ; Oyonarte, S ; Pardo-Oviedo, JM ; Patel, MC ; Paterson, DL ; Pena-Perez, CA ; Perez-Calatayud, AA ; Perez-Alba, E ; Perkina, A ; Perry, N ; Pouladzadeh, M ; Poyato, I ; Price, DJ ; Quero, AKH ; Rahman, MM ; Rahman, MS ; Ramesh, M ; Ramirez-Santana, C ; Rasmussen, M ; Rees, MA ; Rego, E ; Roberts, JA ; Roberts, DJ ; Rodriguez, Y ; Rodriguez-Bano, J ; Rogers, BA ; Rojas, M ; Romero, A ; Rowan, KM ; Saccona, F ; Safdarian, M ; Santos, MCM ; Sasadeusz, J ; Scozzari, G ; Shankar-Hari, M ; Sharma, G ; Snelling, T ; Soto, A ; Tagayuna, PY ; Tang, A ; Tatem, G ; Teofili, L ; Tong, SYC ; Turgeon, AF ; Veloso, JD ; Venkatesh, B ; Ventura-Enriquez, Y ; Webb, SA ; Wiese, L ; Wiken, C ; Wood, EM ; Yusubalieva, GM ; Zacharowski, K ; Zarychanski, R ; Khanna, N ; Moher, D ; Goodman, SN ; Ioannidis, JPA ; Hemkens, LG (BMC, 2021-11-20)
    BACKGROUND: Convalescent plasma has been widely used to treat COVID-19 and is under investigation in numerous randomized clinical trials, but results are publicly available only for a small number of trials. The objective of this study was to assess the benefits of convalescent plasma treatment compared to placebo or no treatment and all-cause mortality in patients with COVID-19, using data from all available randomized clinical trials, including unpublished and ongoing trials (Open Science Framework, https://doi.org/10.17605/OSF.IO/GEHFX ). METHODS: In this collaborative systematic review and meta-analysis, clinical trial registries (ClinicalTrials.gov, WHO International Clinical Trials Registry Platform), the Cochrane COVID-19 register, the LOVE database, and PubMed were searched until April 8, 2021. Investigators of trials registered by March 1, 2021, without published results were contacted via email. Eligible were ongoing, discontinued and completed randomized clinical trials that compared convalescent plasma with placebo or no treatment in COVID-19 patients, regardless of setting or treatment schedule. Aggregated mortality data were extracted from publications or provided by investigators of unpublished trials and combined using the Hartung-Knapp-Sidik-Jonkman random effects model. We investigated the contribution of unpublished trials to the overall evidence. RESULTS: A total of 16,477 patients were included in 33 trials (20 unpublished with 3190 patients, 13 published with 13,287 patients). 32 trials enrolled only hospitalized patients (including 3 with only intensive care unit patients). Risk of bias was low for 29/33 trials. Of 8495 patients who received convalescent plasma, 1997 died (23%), and of 7982 control patients, 1952 died (24%). The combined risk ratio for all-cause mortality was 0.97 (95% confidence interval: 0.92; 1.02) with between-study heterogeneity not beyond chance (I2 = 0%). The RECOVERY trial had 69.8% and the unpublished evidence 25.3% of the weight in the meta-analysis. CONCLUSIONS: Convalescent plasma treatment of patients with COVID-19 did not reduce all-cause mortality. These results provide strong evidence that convalescent plasma treatment for patients with COVID-19 should not be used outside of randomized trials. Evidence synthesis from collaborations among trial investigators can inform both evidence generation and evidence application in patient care.
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    Integrated immune dynamics define correlates of COVID-19 severity and antibody responses
    Koutsakos, M ; Rowntree, LC ; Hensen, L ; Chua, BY ; van de Sandt, CE ; Habel, JR ; Zhang, W ; Jia, X ; Kedzierski, L ; Ashhurst, TM ; Putri, GH ; Marsh-Wakefield, F ; Read, MN ; Edwards, DN ; Clemens, EB ; Wong, CY ; Mordant, FL ; Juno, JA ; Amanat, F ; Audsley, J ; Holmes, NE ; Gordon, CL ; Smibert, OC ; Trubiano, JA ; Hughes, CM ; Catton, M ; Denholm, JT ; Tong, SYC ; Doolan, DL ; Kotsimbos, TC ; Jackson, DC ; Krammer, F ; Godfrey, D ; Chung, AW ; King, NJC ; Lewin, SR ; Wheatley, AK ; Kent, SJ ; Subbarao, K ; McMahon, J ; Thevarajan, I ; Thi, HON ; Cheng, AC ; Kedzierska, K (CELL PRESS, 2021-03-16)
    SARS-CoV-2 causes a spectrum of COVID-19 disease, the immunological basis of which remains ill defined. We analyzed 85 SARS-CoV-2-infected individuals at acute and/or convalescent time points, up to 102 days after symptom onset, quantifying 184 immunological parameters. Acute COVID-19 presented with high levels of IL-6, IL-18, and IL-10 and broad activation marked by the upregulation of CD38 on innate and adaptive lymphocytes and myeloid cells. Importantly, activated CXCR3+cTFH1 cells in acute COVID-19 significantly correlate with and predict antibody levels and their avidity at convalescence as well as acute neutralization activity. Strikingly, intensive care unit (ICU) patients with severe COVID-19 display higher levels of soluble IL-6, IL-6R, and IL-18, and hyperactivation of innate, adaptive, and myeloid compartments than patients with moderate disease. Our analyses provide a comprehensive map of longitudinal immunological responses in COVID-19 patients and integrate key cellular pathways of complex immune networks underpinning severe COVID-19, providing important insights into potential biomarkers and immunotherapies.