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3. Epidemiology, antimicrobial resistance and outcomes of Staphylococcus aureus bacteraemia in a tertiary hospital in Fiji: A prospective cohort study

Author

Loftus, MJ, Young-Sharma, TEMW, Wati, S, Badoordeen, GZ, Blakeway, L, Byers, SMH, Cheng, AC, Jenney, AWJ, Naidu, R, Prasad, A, Prasad, V, Tudravu, L, Vakatawa, T, van Gorp, E, Wisniewski, JA, Rafai, E, Stewardson, AJ, Peleg, AY, Loftus, MJ, Young-Sharma, TEMW, Wati, S, Badoordeen, GZ, Blakeway, L, Byers, SMH, Cheng, AC, Jenney, AWJ, Naidu, R, Prasad, A, Prasad, V, Tudravu, L, Vakatawa, T, van Gorp, E, Wisniewski, JA, Rafai, E, Stewardson, AJ, and Peleg, AY

Abstract

BACKGROUND: Staphylococcus aureus bacteraemia (SAB) is one of the commonest bloodstream infections globally and is associated with a high mortality rate. Most published data comes from temperate, high-income countries. We describe the clinical epidemiology, microbiology, management and outcomes of patients with SAB treated in a tropical, middle-income setting at Fiji's largest hospital. METHODS: A prospective, observational study was performed of consecutive SAB cases admitted to Colonial War Memorial Hospital (CWMH) in Suva, between July 2020 and February 2021. Detailed demographic, clinical and microbiological data were collected, including the key outcome of in-patient mortality. To estimate the population incidence, all SAB cases diagnosed at the CWMH laboratory were included - even if not admitted to CWMH - with the population of Fiji's Central Division used as the denominator. FINDINGS: A total of 176 cases of SAB were detected over eight-months, which equated to an incidence of 68.8 cases per 100,000 population per year. Of these, 95 cases were admitted to CWMH within 48 h of index culture. Approximately 8.4% (8/95) of admitted cases were caused by methicillin-resistant Staphylococcus aureus (MRSA). All cause in-patient mortality was 25.3%, increasing to 55% among patients aged 60 or older. INTERPRETATION: This reported incidence of SAB in central Fiji is one of the highest in the world. SAB was associated with significant mortality, especially in those over 60 years of age, despite a relatively low frequency of methicillin resistance. FUNDING: Supported by the National Health and Medical Research Council (Australia) and the GRAM (Global Research on Antimicrobial Resistance) Project, Oxford University (United Kingdom).

Published
2022

4. ESBL plasmids in Klebsiella pneumoniae: diversity, transmission and contribution to infection burden in the hospital setting

Author

Hawkey, J, Wyres, KL, Judd, LM, Harshegyi, T, Blakeway, L, Wick, RR, Jenney, AWJ, Holt, KE, Hawkey, J, Wyres, KL, Judd, LM, Harshegyi, T, Blakeway, L, Wick, RR, Jenney, AWJ, and Holt, KE

Abstract

BACKGROUND: Resistance to third-generation cephalosporins, often mediated by extended-spectrum beta-lactamases (ESBLs), is a considerable issue in hospital-associated infections as few drugs remain for treatment. ESBL genes are often located on large plasmids that transfer horizontally between strains and species of Enterobacteriaceae and frequently confer resistance to additional drug classes. Whilst plasmid transmission is recognised to occur in the hospital setting, the frequency and impact of plasmid transmission on infection burden, compared to ESBL + strain transmission, is not well understood. METHODS: We sequenced the genomes of clinical and carriage isolates of Klebsiella pneumoniae species complex from a year-long hospital surveillance study to investigate ESBL burden and plasmid transmission in an Australian hospital. Long-term persistence of a key transmitted ESBL + plasmid was investigated via sequencing of ceftriaxone-resistant isolates during 4 years of follow-up, beginning 3 years after the initial study. RESULTS: We found 25 distinct ESBL plasmids. We identified one plasmid, which we called Plasmid A, that carried blaCTX-M-15 in an IncF backbone similar to pKPN-307. Plasmid A was transmitted at least four times into different Klebsiella species/lineages and was responsible for half of all ESBL episodes during the initial 1-year study period. Three of the Plasmid A-positive strains persisted locally 3-6 years later, and Plasmid A was detected in two additional strain backgrounds. Overall Plasmid A accounted for 21% of ESBL + infections in the follow-up period. CONCLUSIONS: Here, we systematically surveyed ESBL strain and plasmid transmission over 1 year in a single hospital network. Whilst ESBL plasmid transmission events were rare in this setting, they had a significant and sustained impact on the burden of ceftriaxone-resistant and multidrug-resistant infections. If onward transmission of Plasmid A-carrying strains could have been prevented, this m

Published
2022

5. Favipiravir in early symptomatic COVID-19, a randomised placebo-controlled trial

Author

McMahon, JH, Lau, JSY, Coldham, A, Roney, J, Hagenauer, M, Price, S, Bryant, M, Garlick, J, Paterson, A, Lee, SJ, O'Bryan, J, Hearps, A, Tachedjian, G, Pinskier, H, Phillips, C, Garrow, S, Pinskier, N, Melvin, R, Blakeway, L, Wisniewski, JA, Byers, S, Badoordeen, GZ, Pereira, S, Pragastis, K, Trubiano, JA, Chua, KYL, Kainer, M, Molton, JS, Gardiner, BJ, Pierce, AB, Cheng, A, Rogers, BA, Peleg, AY, McMahon, JH, Lau, JSY, Coldham, A, Roney, J, Hagenauer, M, Price, S, Bryant, M, Garlick, J, Paterson, A, Lee, SJ, O'Bryan, J, Hearps, A, Tachedjian, G, Pinskier, H, Phillips, C, Garrow, S, Pinskier, N, Melvin, R, Blakeway, L, Wisniewski, JA, Byers, S, Badoordeen, GZ, Pereira, S, Pragastis, K, Trubiano, JA, Chua, KYL, Kainer, M, Molton, JS, Gardiner, BJ, Pierce, AB, Cheng, A, Rogers, BA, and Peleg, AY

Abstract

BACKGROUND: Well tolerated antivirals administered early in the course of COVID-19 infection when the viremia is highest could prevent progression to severe disease. Favipiravir inhibits SARS-CoV-2 viral replication in vitro with evidence of clinical benefit in open label trials. Placebo controlled studies of people with early symptomatic COVID-19 with regular assessments of SARS-CoV-2 viral load can determine if it has an antiviral effect and improves clinical outcomes. METHODS: People with PCR-confirmed COVID-19 and 5 days or less of symptoms were randomised 1:1 to favipiravir 1800 mg on day 1, then 800 mg twice daily or matched placebo for 14 days. SARS-CoV-2 viral load was quantitated from second daily self-collected nose-throat swabs while receiving study drug. The primary endpoint was time to virological cure defined as 2 successive swabs negative for SARS-CoV-2 by PCR and secondary outcomes were progression of disease severity, symptom resolution and safety. FINDINGS: Between 31 July 2020 and 19 September 2021, 200 people were enrolled (199 in the community, 1 in hospital) with 190 receiving one or more doses of drug (modified intention to treat [mITT] population). There was no difference in time to virological cure (Log-rank p=0.6 comparing Kaplan Meier curves), progression to hospitalisation (14 favipiravir, 9 placebo; p=0.38), time to symptom resolution (cough, fever, sore throat) and there were no deaths. 51 people related an adverse event that was possibly drug related, but these were evenly distributed (n=24 favipiravir, n=27 placebo). Sensitivity analyses where the definition of virological cure was changed to: a single negative PCR, exclude datapoints based on the presence or absence of human DNA in the swab, a SARS-CoV-2 viral load < 300 copies/mL being considered negative all demonstrated no difference between arms. INTERPRETATION: Favipiravir does not improve the time to virological cure or clinical outcomes and shows no evidence of an antiviral ef

Published
2022

6. 178. Endemic Carbapenem Resistance Driven By Clonal and Horizontal Spread of blaIMP-4 Across Diverse Enterobacterales: Jumping Genes, Promiscuous Plasmids and Killer Clones

Author

Macesic, N, Blakeway, L, Jenney, AW, Peleg, A, Macesic, N, Blakeway, L, Jenney, AW, and Peleg, A

Abstract

Background Carbapenem-resistant Enterobacterales (CRE) have become endemic and cause significant morbidity and mortality globally. The metallo-beta-lactamase gene blaIMP-4 is a key CRE resistance determinant in Australia and Asia but its genomic context remains unknown. We aimed to determine the genomic epidemiology of blaIMP-4 in clinical and environmental isolates from 2008 – 2020 at our institution. Methods We performed whole genome sequencing on 219 blaIMP-4-carrying isolates from 134 patients (219 short-read and 75 long-read). Multi-locus sequence types (MLSTs), resistance determinants and plasmid replicons were assessed. High-quality de novo hybrid assemblies were used to identify location of blaIMP-4 gene. We conducted phylogenetic analysis for key MLSTs and plasmids. Results Bla IMP-4 was noted on a class I integron also harboring aminoglycoside, sulfamethoxazole, chloramphenicol and quaternary ammonium compound resistance genes. This integron was able to migrate over time to 10 bacterial species (42 STs) and 6 different plasmid types (Figure 1 and Figure 2). From 2008-2020, blaIMP-4 was present on IncC plasmids in Serratia marcescens and Klebsiella pneumoniae. We noted small outbreaks of Pseudomonas aeruginosa ST111 with chromosomal integration of blaIMP-4 from 2008-2018 (16 isolates) and Enterobacter cloacae complex ST114 with blaIMP-4 on IncFIB(K)/IncFIA(HI1) plasmids from 2011-2020 (19 isolates). From 2016-2020, there was an explosion of diverse IncHI2 plasmids carrying blaIMP-4. This was driven by clonal expansion of E. cloacae complex ST93/ST190 (79 isolates), with spillover of IncHI2 plasmids to Klebsiella spp (13 isolates), Citrobacter spp (2 isolates), S. marcescens (1 isolate), Escherichia coli (4 isolates). In addition to blaIMP-4, these plasmids carried mcr-9.1, a colistin resistance gene, and resistance determinants to nearly all key classes of Gram-negative antimicrobials. Figure 1. Bacterial species harboring blaIMP-4 2008-2020 BlaIMP

Published
2021

7. Proteome of a Moraxella catarrhalis Strain under Iron-Restricted Conditions

Author

Newton, ILG, Blakeway, L, Tan, A, Peak, IR, Atack, JM, Seib, KL, Newton, ILG, Blakeway, L, Tan, A, Peak, IR, Atack, JM, and Seib, KL

Abstract

Moraxella catarrhalis is a leading cause of otitis media and exacerbations of chronic obstructive pulmonary disease; however, its response to iron starvation during infection is not completely understood. Here, we announce a sequential window acquisition of all theoretical fragment ion spectra mass spectrometry (SWATH-MS) data set describing the differential expression of the M. catarrhalis CCRI-195ME proteome under iron-restricted versus iron-replete conditions.

Published
2020

8. Patient deprivation and perceived scan burden negatively impact the quality of whole-body MRI

Author

Evans, R.E.C., primary, Taylor, S.A., additional, Kalasthry, J., additional, Sakai, N.S., additional, Miles, A., additional, Aboagye, A., additional, Agoramoorthy, L., additional, Ahmed, S., additional, Amadi, A., additional, Anand, G., additional, Atkin, G., additional, Austria, A., additional, Ball, S., additional, Bazari, F., additional, Beable, R., additional, Beare, S., additional, Beedham, H., additional, Beeston, T., additional, Bharwani, N., additional, Bhatnagar, G., additional, Bhowmik, A., additional, Blakeway, L., additional, Blunt, D., additional, Boavida, P., additional, Boisfer, D., additional, Breen, D., additional, Bridgewater, J., additional, Burke, S., additional, Butawan, R., additional, Campbell, Y., additional, Chang, E., additional, Chao, D., additional, Chukundah, S., additional, Clarke, C.S., additional, Collins, B., additional, Collins, C., additional, Conteh, V., additional, Couture, J., additional, Crosbie, J., additional, Curtis, H., additional, Daniel, A., additional, Davis, L., additional, Desai, K., additional, Duggan, M., additional, Ellis, S., additional, Elton, C., additional, Engledow, A., additional, Everitt, C., additional, Ferdous, S., additional, Frow, A., additional, Furneaux, M., additional, Gibbons, N., additional, Glynne-Jones, R., additional, Gogbashian, A., additional, Goh, V., additional, Gourtsoyianni, S., additional, Green, A., additional, Green, Laura, additional, Green, Liz, additional, Groves, A., additional, Guthrie, A., additional, Hadley, E., additional, Halligan, S., additional, Hameeduddin, A., additional, Hanid, G., additional, Hans, S., additional, Hans, B., additional, Higginson, A., additional, Honeyfield, L., additional, Hughes, H., additional, Hughes, J., additional, Hurl, L., additional, Isaac, E., additional, Jackson, M., additional, Jalloh, A., additional, Janes, S., additional, Jannapureddy, R., additional, Jayme, A., additional, Johnson, A., additional, Johnson, E., additional, Julka, P., additional, Karapanagiotou, E., additional, Karp, S., additional, Kay, C., additional, Kellaway, J., additional, Khan, S., additional, Koh, D., additional, Light, T., additional, Limbu, P., additional, Lock, S., additional, Locke, I., additional, Loke, T., additional, Lowe, A., additional, Lucas, N., additional, Maheswaran, S., additional, Mallett, S., additional, Marwood, E., additional, McGowan, J., additional, Mckirdy, F., additional, Mills-Baldock, T., additional, Moon, T., additional, Morgan, V., additional, Morris, S., additional, Morton, A., additional, Nasseri, S., additional, Navani, N., additional, Nichols, P., additional, Norman, C., additional, Ntala, E., additional, Nunes, A., additional, Obichere, A., additional, O'Donohue, J., additional, Olaleye, I., additional, Oliver, A., additional, Onajobi, A., additional, O'Shaughnessy, T., additional, Padhani, A., additional, Pardoe, H., additional, Partridge, W., additional, Patel, U., additional, Perry, K., additional, Piga, W., additional, Prezzi, D., additional, Prior, K., additional, Punwani, S., additional, Pyers, J., additional, Rafiee, H., additional, Rahman, F., additional, Rajanpandian, I., additional, Ramesh, S., additional, Raouf, S., additional, Reczko, K., additional, Reinhardt, A., additional, Robinson, D., additional, Rockall, A., additional, Russell, P., additional, Sargus, K., additional, Scurr, E., additional, Shahabuddin, K., additional, Sharp, A., additional, Shepherd, B., additional, Shiu, K., additional, Sidhu, H., additional, Simcock, I., additional, Simeon, C., additional, Smith, A., additional, Smith, D., additional, Snell, D., additional, Spence, J., additional, Srirajaskanthan, R., additional, Stachini, V., additional, Stegner, S., additional, Stirling, J., additional, Strickland, N., additional, Tarver, K., additional, Teague, J., additional, Thaha, M., additional, Train, M., additional, Tulmuntaha, S., additional, Tunariu, N., additional, van Ree, K., additional, Verjee, A., additional, Wanstall, C., additional, Weir, S., additional, Wijeyekoon, S., additional, Wilson, J., additional, Wilson, S., additional, Win, T., additional, Woodrow, L., additional, and Yu, D., additional

Published
2020
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9. Patient preferences for whole-body MRI or conventional staging pathways in lung and colorectal cancer: a discrete choice experiment

Author

Miles, A, Taylor, SA, Evans, REC, Halligan, S, Beare, S, Bridgewater, J, Goh, V, Janes, S, Navani, N, Oliver, A, Morton, A, Rockall, A, Clarke, CS, Morris, S, Aboagye, A, Agoramoorthy, L, Ahmed, S, Amadi, A, Anand, G, Atkin, G, Austria, A, Ball, S, Bazari, F, Beable, R, Beedham, H, Beeston, T, Bharwani, N, Bhatnagar, G, Bhowmik, A, Blakeway, L, Blunt, D, Boavida, P, Boisfer, D, Breen, D, Burke, S, Butawan, R, Campbell, Y, Chang, E, Chao, D, Chukundah, S, Collins, B, Collins, C, Conteh, V, Couture, J, Crosbie, J, Curtis, H, Daniel, A, Davis, L, Desai, K, Duggan, M, Ellis, S, Elton, C, Engledow, A, Everitt, C, Ferdous, S, Frow, A, Furneaux, M, Gibbons, N, Glynne-Jones, R, Gogbashian, A, Gourtsoyianni, S, Green, A, Green, L, Groves, A, Guthrie, A, Hadley, E, Hameeduddin, A, Hanid, G, Hans, S, Hans, B, Higginson, A, Honeyfield, L, Hughes, H, Hughes, J, Hurl, L, Isaac, E, Jackson, M, Jalloh, A, Jannapureddy, R, Jayme, A, Johnson, A, Johnson, E, Julka, P, Kalasthry, J, Karapanagiotou, E, Karp, S, Kay, C, Kellaway, J, Khan, S, Koh, D-M, Light, T, Limbu, P, Lock, S, Locke, I, Loke, T, Lowe, A, Lucas, N, Maheswaran, S, Mallett, S, Marwood, E, McGowan, J, Mckirdy, F, Mills-Baldock, T, Moon, T, Morgan, V, Nasseri, S, Nichols, P, Norman, C, Ntala, E, Nunes, A, Obichere, A, O'Donohue, J, Olaleye, I, Onajobi, A, O'Shaughnessy, T, Padhani, A, Pardoe, H, Partridge, W, Patel, U, Perry, K, Piga, W, Prezzi, D, Prior, K, Punwani, S, Pyers, J, Rafiee, H, Rahman, F, Rajanpandian, I, Ramesh, S, Raouf, S, Reczko, K, Reinhardt, A, Robinson, D, Russell, P, Sargus, K, Scurr, E, Shahabuddin, K, Sharp, A, Shepherd, B, Shiu, K, Sidhu, H, Simcock, I, Simeon, C, Smith, A, Smith, D, Snell, D, Spence, J, Srirajaskanthan, R, Stachini, V, Stegner, S, Stirling, J, Strickland, N, Tarver, K, Teague, J, Thaha, M, Train, M, Tulmuntaha, S, Tunariu, N, Van Ree, K, Verjee, A, Wanstall, C, Weir, S, Wijeyekoon, S, Wilson, J, Wilson, S, Win, T, Woodrow, L, Yu, D, Imperial College Healthcare NHS Trust- BRC Funding, and Department of Health

Subjects
Adult, Male, Positron emission tomography, Lung Neoplasms, Social Sciences, X-ray computed, Magnetic resonance imaging, Psychology, Multidisciplinary, Positron Emission Tomography Computed Tomography, Surveys and Questionnaires, Psychology, Humans, Whole Body Imaging, Patient preference, Prospective Studies, Tomography, Cancer, Aged, Neoplasm Staging, Science & Technology, Radiology, Nuclear Medicine & Medical Imaging, Tomography, X-ray computed, 1103 Clinical Sciences, CARE, Middle Aged, NEGATIVE AFFECT, Biomedical Social Sciences, Social Sciences, Biomedical, Nuclear Medicine & Medical Imaging, PANAS, Oncology, Positron-Emission Tomography, Regression Analysis, CLAUSTROPHOBIA, Female, STREAMLINE investigators, Colorectal Neoplasms, Life Sciences & Biomedicine
Abstract

Objectives To determine the importance placed by patients on attributes associated with whole-body MRI (WB-MRI) and standard cancer staging pathways and ascertain drivers of preference. Methods Patients recruited to two multi-centre diagnostic accuracy trials comparing WB-MRI with standard staging pathways in lung and colorectal cancer were invited to complete a discrete choice experiment (DCE), choosing between a series of alternate pathways in which 6 attributes (accuracy, time to diagnosis, scan duration, whole-body enclosure, radiation exposure, total scan number) were varied systematically. Data were analysed using a conditional logit regression model and marginal rates of substitution computed. The relative importance of each attribute and probabilities of choosing WB-MRI-based pathways were estimated. Results A total of 138 patients (mean age 65, 61% male, lung n = 72, colorectal n = 66) participated (May 2015 to September 2016). Lung cancer patients valued time to diagnosis most highly, followed by accuracy, radiation exposure, number of scans, and time in the scanner. Colorectal cancer patients valued accuracy most highly, followed by time to diagnosis, radiation exposure, and number of scans. Patients were willing to wait 0.29 (lung) and 0.45 (colorectal) weeks for a 1% increase in pathway accuracy. Patients preferred WB-MRI-based pathways (probability 0.64 [lung], 0.66 [colorectal]) if they were equivalent in accuracy, total scan number, and time to diagnosis compared with a standard staging pathway. Conclusions Staging pathways based on first-line WB-MRI are preferred by the majority of patients if they at least match standard pathways for diagnostic accuracy, time to diagnosis, and total scan number.

Published
2019

11. Chemoenzymatic surface decoration of Nisin-shelled nanoemulsions: Novel targeted drug-nanocarriers for cancer applications.

Author

Hashad RA, Singla R, Kaur Bhangu S, Jap E, Zhu H, Peleg AY, Blakeway L, Hagemeyer CE, Cavalieri F, Ashokkumar M, and Alt K

Subjects
Humans, Azides, Doxorubicin pharmacology, Immunoglobulin G, Nisin pharmacology, Neoplasms
Abstract

Nisin, a peptide used as a natural food preservative, is employed in this work for the development of a novel nanocarrier system. Stable and uniform nisin-shelled nanoemulsions (NSNE) with a diameter of 100 ± 20 nm were successfully prepared using 20 kHz flow-through ultrasonication technique. The NSNE showed limited toxicity, high bactericidal activity and high drug loading capacity (EE 65 % w/w). In addition, the nisin shell was exploited for the site-specific attachment of a recombinantly produced cancer targeting ligand (αHER2 LPETG IgG). Employing a unique two phases (bio-click) approach which involved both Sortase A mediated Azide Bioconjugation (SMAB) and Strain Promoted Azide Alkyne Cycloaddition (SPAAC) reactions, targeted NSNE (NSNE DOX -αHER2 IgG) were successfully assembled and loaded with the chemotherapeutic drug Doxorubicin (DOX). Finally, NSNE DOX -αHER2 IgG showed cancer-specific binding and augmented cytotoxicity to HER2 expressing tumour cells., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published
2022
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12. Favipiravir in early symptomatic COVID-19, a randomised placebo-controlled trial.

Author

McMahon JH, Lau JSY, Coldham A, Roney J, Hagenauer M, Price S, Bryant M, Garlick J, Paterson A, Lee SJ, O'Bryan J, Hearps A, Tachedjian G, Pinskier H, Phillips C, Garrow S, Pinskier N, Melvin R, Blakeway L, Wisniewski JA, Byers S, Badoordeen GZ, Pereira S, Pragastis K, Trubiano JA, Chua KYL, Kainer M, Molton JS, Gardiner BJ, Pierce AB, Cheng A, Rogers BA, and Peleg AY

Abstract

Background: Well tolerated antivirals administered early in the course of COVID-19 infection when the viremia is highest could prevent progression to severe disease. Favipiravir inhibits SARS-CoV-2 viral replication in vitro with evidence of clinical benefit in open label trials. Placebo controlled studies of people with early symptomatic COVID-19 with regular assessments of SARS-CoV-2 viral load can determine if it has an antiviral effect and improves clinical outcomes., Methods: People with PCR-confirmed COVID-19 and 5 days or less of symptoms were randomised 1:1 to favipiravir 1800 mg on day 1, then 800 mg twice daily or matched placebo for 14 days. SARS-CoV-2 viral load was quantitated from second daily self-collected nose-throat swabs while receiving study drug. The primary endpoint was time to virological cure defined as 2 successive swabs negative for SARS-CoV-2 by PCR and secondary outcomes were progression of disease severity, symptom resolution and safety., Findings: Between 31 July 2020 and 19 September 2021, 200 people were enrolled (199 in the community, 1 in hospital) with 190 receiving one or more doses of drug (modified intention to treat [mITT] population). There was no difference in time to virological cure (Log-rank p =0.6 comparing Kaplan Meier curves), progression to hospitalisation (14 favipiravir, 9 placebo; p =0.38), time to symptom resolution (cough, fever, sore throat) and there were no deaths. 51 people related an adverse event that was possibly drug related, but these were evenly distributed ( n =24 favipiravir, n =27 placebo). Sensitivity analyses where the definition of virological cure was changed to: a single negative PCR, exclude datapoints based on the presence or absence of human DNA in the swab, a SARS-CoV-2 viral load < 300 copies/mL being considered negative all demonstrated no difference between arms., Interpretation: Favipiravir does not improve the time to virological cure or clinical outcomes and shows no evidence of an antiviral effect when treating early symptomatic COVID-19 infection., Funding: The study was supported in part by grants from the Commonwealth Bank Australia, the Lord Mayor's Charitable Foundation, Melbourne Australia and the Orloff Family Charitable Trust, Melbourne, Australia. JHM is supported by the Medical Research Future Fund, AYP, JT are supported by the Australian National Health and Medical Research Council., Competing Interests: All authors declare no competing interests., (© 2022 The Authors.)

Published
2022
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13. ESBL plasmids in Klebsiella pneumoniae: diversity, transmission and contribution to infection burden in the hospital setting.

Author

Hawkey J, Wyres KL, Judd LM, Harshegyi T, Blakeway L, Wick RR, Jenney AWJ, and Holt KE

Subjects
Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents therapeutic use, Australia epidemiology, Ceftriaxone, Hospitals, Humans, Plasmids genetics, Klebsiella pneumoniae genetics, beta-Lactamases genetics
Abstract

Background: Resistance to third-generation cephalosporins, often mediated by extended-spectrum beta-lactamases (ESBLs), is a considerable issue in hospital-associated infections as few drugs remain for treatment. ESBL genes are often located on large plasmids that transfer horizontally between strains and species of Enterobacteriaceae and frequently confer resistance to additional drug classes. Whilst plasmid transmission is recognised to occur in the hospital setting, the frequency and impact of plasmid transmission on infection burden, compared to ESBL + strain transmission, is not well understood., Methods: We sequenced the genomes of clinical and carriage isolates of Klebsiella pneumoniae species complex from a year-long hospital surveillance study to investigate ESBL burden and plasmid transmission in an Australian hospital. Long-term persistence of a key transmitted ESBL + plasmid was investigated via sequencing of ceftriaxone-resistant isolates during 4 years of follow-up, beginning 3 years after the initial study., Results: We found 25 distinct ESBL plasmids. We identified one plasmid, which we called Plasmid A, that carried bla CTX-M-15 in an IncF backbone similar to pKPN-307. Plasmid A was transmitted at least four times into different Klebsiella species/lineages and was responsible for half of all ESBL episodes during the initial 1-year study period. Three of the Plasmid A-positive strains persisted locally 3-6 years later, and Plasmid A was detected in two additional strain backgrounds. Overall Plasmid A accounted for 21% of ESBL + infections in the follow-up period., Conclusions: Here, we systematically surveyed ESBL strain and plasmid transmission over 1 year in a single hospital network. Whilst ESBL plasmid transmission events were rare in this setting, they had a significant and sustained impact on the burden of ceftriaxone-resistant and multidrug-resistant infections. If onward transmission of Plasmid A-carrying strains could have been prevented, this may have reduced the number of opportunities for Plasmid A to transmit and create novel ESBL + strains, as well as reducing overall ESBL infection burden., (© 2022. The Author(s).)

Published
2022
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15. SARS-CoV-2 infection results in immune responses in the respiratory tract and peripheral blood that suggest mechanisms of disease severity.

Author

Zhang W, Chua BY, Selva KJ, Kedzierski L, Ashhurst TM, Haycroft ER, Shoffner-Beck SK, Hensen L, Boyd DF, James F, Mouhtouris E, Kwong JC, Chua KYL, Drewett G, Copaescu A, Dobson JE, Rowntree LC, Habel JR, Allen LF, Koay HF, Neil JA, Gartner MJ, Lee CY, Andersson P, Khan SF, Blakeway L, Wisniewski J, McMahon JH, Vine EE, Cunningham AL, Audsley J, Thevarajan I, Seemann T, Sherry NL, Amanat F, Krammer F, Londrigan SL, Wakim LM, King NJC, Godfrey DI, Mackay LK, Thomas PG, Nicholson S, Arnold KB, Chung AW, Holmes NE, Smibert OC, Trubiano JA, Gordon CL, Nguyen THO, and Kedzierska K

Subjects
Antibodies, Viral, Humans, Immunity, Immunoglobulin G, Immunoglobulin M, Respiratory System, SARS-CoV-2, Severity of Illness Index, Spike Glycoprotein, Coronavirus, COVID-19
Abstract

Respiratory tract infection with SARS-CoV-2 results in varying immunopathology underlying COVID-19. We examine cellular, humoral and cytokine responses covering 382 immune components in longitudinal blood and respiratory samples from hospitalized COVID-19 patients. SARS-CoV-2-specific IgM, IgG, IgA are detected in respiratory tract and blood, however, receptor-binding domain (RBD)-specific IgM and IgG seroconversion is enhanced in respiratory specimens. SARS-CoV-2 neutralization activity in respiratory samples correlates with RBD-specific IgM and IgG levels. Cytokines/chemokines vary between respiratory samples and plasma, indicating that inflammation should be assessed in respiratory specimens to understand immunopathology. IFN-α2 and IL-12p70 in endotracheal aspirate and neutralization in sputum negatively correlate with duration of hospital stay. Diverse immune subsets are detected in respiratory samples, dominated by neutrophils. Importantly, dexamethasone treatment does not affect humoral responses in blood of COVID-19 patients. Our study unveils differential immune responses between respiratory samples and blood, and shows how drug therapy affects immune responses during COVID-19., (© 2022. The Author(s).)

Published
2022
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16. Depiction of lower limb venous anatomy in patients undergoing interventional deep venous reconstruction-the role of balanced steady state free precession MRI.

Author

Helyar VG, Gupta Y, Blakeway L, Charles-Edwards G, Katsanos K, and Karunanithy N

Subjects
Adolescent, Adult, Aged, Contrast Media, Female, Humans, Iohexol, Likelihood Functions, Lower Extremity diagnostic imaging, Male, Middle Aged, Retrospective Studies, Sensitivity and Specificity, Triiodobenzoic Acids, Young Adult, Angiography, Digital Subtraction, Lower Extremity blood supply, Magnetic Resonance Imaging, Postthrombotic Syndrome diagnostic imaging, Veins diagnostic imaging, Venous Thrombosis diagnostic imaging
Abstract

Objectives: This study evaluates the use of balanced steady-state free precession MRI (bSSFP-MRI) in the diagnostic work-up of patients undergoing interventional deep venous reconstruction (I-DVR). Intravenous digital subtraction angiography (IVDSA) was used as the gold-standard for comparison to assess disease extent and severity., Methods: A retrospective comparison of bSSFP-MRI to IVDSA was performed in all patients undergoing both examinations for treatment planning prior to I-DVR. The severity of disease in each venous segment was graded by two board-certified radiologists working independently, according to a predetermined classification system., Results: In total, 44 patients (225 venous segments) fulfilled the inclusion criteria. A total of 156 abnormal venous segments were diagnosed using bSSFP-MRI compared with 151 using IVDSA. The prevalence of disease was higher in the iliac and femoral segments (range, 79.6-88.6%). Overall sensitivity, specificity, positive likelihood ratio, negative likelihood ratio and the diagnostic ratio for bSSFP-MRI were 99.3%, 91.9%, 12.3, 0.007 and 1700, respectively., Conclusion: This study supports the use of non-contrast balanced SSFP-MRI in the assessment of the deep veins of the lower limb prior to I-DVR. The technique offers an accurate, fast and non-invasive alternative to IVDSA. Advances in Knowledge: Although balanced SSFP-MRI is commonly used in cardiac imaging, its use elsewhere is limited and its use in evaluating the deep veins prior to interventional reconstruction is not described. Our study demonstrates the usefulness of this technique in the work-up of patients awaiting interventional venous reconstruction compared with the current gold standard.

Published
2018
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