Your search keyword '"Derek Cocker"' showing total 27 results

1. Time to define One Health approaches to tackling antimicrobial resistance

Author

Patrick Musicha, Tracy Morse, Derek Cocker, Lawrence Mugisha, Christopher P. Jewell, and Nicholas A. Feasey

Subjects

Science

Abstract

Recent data re-affirm antimicrobial resistance (AMR) as a One Health problem, particularly in low- and middle-income countries. Transdisciplinary and intersectoral collaboration are required if we are to improve environmental hygiene, addressing both AMR and a range of aligned development challenges.

Published

2024

2. Drivers of Resistance in Uganda and Malawi (DRUM): a protocol for the evaluation of One-Health drivers of Extended Spectrum Beta Lactamase (ESBL) resistance in Low-Middle Income Countries (LMICs) [version 2; peer review: 2 approved, 1 approved with reservations]

Author

Rebecca Lester, Melodie Sammarro, Christopher P. Jewell, Derek Cocker, Nicola Elviss, Kondwani Chidziwisano, Henry Kajumbula, Shevin T. Jacob, David Musoke, Lawrence Mugisha, Barry Rowlingson, Patrick Musicha, Beth Hollihead, Rachel L. Byrne, Catherine N. Wilson, Tracy Morse, Nicholas R. Thomson, Thomas Edwards, Nicholas A. Feasey, Andrew C. Singer, and Adam P. Roberts

Subjects

Antimicrobial Resistance, Africa, One Health, Environment, eng, Medicine, Science

Abstract

In sub-Saharan Africa (sSA), there is high morbidity and mortality from severe bacterial infection and this is compounded by antimicrobial resistance, in particular, resistance to 3rd-generation cephalosporins. This resistance is typically mediated by extended-spectrum beta lactamases (ESBLs). To interrupt ESBL transmission it will be important to investigate how human behaviour, water, sanitation, and hygiene (WASH) practices, environmental contamination, and antibiotic usage in both urban and rural settings interact to contribute to transmission of ESBL E. coli and ESBL K. pneumoniae between humans, animals, and the environment. Here we present the protocol for the Drivers of Resistance in Uganda and Malawi (DRUM) Consortium, in which we will collect demographic, geospatial, clinical, animal husbandry and WASH data from a total of 400 households in Uganda and Malawi. Longitudinal human, animal and environmental sampling at each household will be used to isolate ESBL E. coli and ESBL K. pneumoniae. This will be complimented by a Risks, Attitudes, Norms, Abilities and Self-Regulation (RANAS) survey and structured observations to understand the contextual and psychosocial drivers of regional WASH practices. Bacterial isolates and plate sweeps will be further characterised using a mixture of short-,long-read and metagenomic whole-genome sequencing. These datasets will be integrated into agent-based models to describe the transmission of EBSL resistance in Uganda and Malawi and allow us to inform the design of interventions for interrupting transmission of ESBL-bacteria.

Published

2023

3. Circumstances for treatment and control of invasive Enterobacterales infections in eight hospitals across sub-Saharan Africa: a cross-sectional study [version 1; peer review: 2 approved]

Author

Brian Nyamwaya, Alexander M. Aiken, Noah Obeng-Nkrumah, Appiah-Korang Labi, Mabvuto Chimenya, William Mwabaya, Kenneth C. Iregbu, Derek Cocker, Lola Madrid, Angela Dramowski, Philip I. P. Princewill-Nwajiobi, Blandina Theophil Mmbaga, Tolbert Sonda, Sombo Fwoloshi, David Ojok, Andrew Whitelaw, J Anthony G Scott, and Dumessa Edessa

Subjects

antibiotic, access, infection, resistance, Africa, eng, Medicine

Abstract

Background: Bloodstream infections caused by Enterobacterales show high frequency of antimicrobial resistance (AMR) in many Low- and Middle-Income Countries. We aimed to describe the variation in circumstances for management of such resistant infections in a group of African public-sector hospitals participating in a major research study. Methods: We gathered data from eight hospitals across sub-Saharan Africa to describe hospital services, infection prevention and antibiotic stewardship activities, using two WHO-generated tools. We collected monthly cross-sectional data on availability of antibiotics in the hospital pharmacies for bloodstream infections caused by Enterobacterales. We compared the availability of these antibiotics to actual patient-level use of antibiotics in confirmed Enterobacterales bloodstream infections (BSI). Results: Hospital circumstances for institutional management of resistant BSI varied markedly. This included self-evaluated infection prevention level (WHO-IPCAF score: median 428, range 155 to 687.5) and antibiotic stewardship activities (WHO stewardship toolkit questions: median 14.5, range 2 to 23). These results did not correlate with national income levels. Across all sites, ceftriaxone and ciprofloxacin were the most consistently available antibiotic agents, followed by amoxicillin, co-amoxiclav, gentamicin and co-trimoxazole. There was substantial variation in the availability of some antibiotics, especially carbapenems, amikacin and piperacillin-tazobactam with degree of access linked to national income level. Investigators described out-of-pocket payments for access to additional antibiotics at 7/8 sites. The in-pharmacy availability of antibiotics correlated well with actual use of antibiotics for treating BSI patients. Conclusions: There was wide variation between these African hospitals for a range of important circumstances relating to treatment and control of severe bacterial infections, though these did not all correspond to national income level. For most antibiotics, patient-level use reflected in-hospital drug availability, suggesting external antibiotics supply was infrequent. Antimicrobial resistant bacterial infections could plausibly show different clinical impacts across sub-Saharan Africa due to this contextual variation.

Published

2023

4. Lessons learnt from the rapid implementation of reusable personal protective equipment for COVID-19 in Malawi

Author

Queen Dube, Bridget Freyne, Mulinda Nyirenda, Stephen Gordon, Kwazizira Samson Mndolo, Priyanka Patel, Luis A Gadama, Fumbani Limani, David Garley, Derek Cocker, Pratiksha Patel, Servace Sakala, Feggie Bodole, and Kelvin Mponda

Subjects

Medicine (General), R5-920, Infectious and parasitic diseases, RC109-216

Abstract

The SARS-CoV-2 pandemic has challenged health systems and healthcare workers worldwide. Access to personal protective equipment (PPE) is essential to mitigate the risk of excess mortality in healthcare providers. In Malawi, the cost of PPE represents an additional drain on available resources. In the event of repeated waves of disease over several years, the development of sustainable systems of PPE is essential. We describe the development, early implementation and rapid scale up of a reusable gown service at a tertiary-level hospital in Blantyre, Malawi. Challenges included healthcare worker perceptions around the potential of reduced efficacy of cotton gowns, the need to plan for surge capacity and the need for ongoing training of laundry staff in safety and hygiene procedures. Benefits of the system included increased coverage, decreased cost and reduced waste disposal. The implementation of a reusable cotton gown service is feasible, acceptable and cost-effective in tertiary centres providing specialist COVID-19 care at the height of the pandemic. This innovation could be expanded beyond low-income settings.

Published

2021

5. Initial Accuracy of HIV Rapid Test Kits Stored in Suboptimal Conditions and Validity of Delayed Reading of Oral Fluid Tests.

Author

Augustine T Choko, Miriam Taegtmeyer, Peter MacPherson, Derek Cocker, McEwen Khundi, Deus Thindwa, Rodrick S Sambakunsi, Moses K Kumwenda, Kondwani Chiumya, Owen Malema, Simon D Makombe, Emily L Webb, and Elizabeth L Corbett

Subjects

Medicine, Science

Abstract

To evaluate the effect of storing commonly used rapid diagnostic tests above manufacturer-recommended temperature (at 37°C), and the accuracy of delayed reading of oral fluid kits with relevance to HIV self-testing programmes.A quality assurance study of OraQuick (OraSure), Determine HIV 1/2™ (Alere) and Uni-Gold™ (Recombigen®).Consecutive adults (≥18y) attending Ndirande Health Centre in urban Blantyre, Malawi in January to April 2012 underwent HIV testing with two of each of the three rapid diagnostic test kits stored for 28 days at either 18°C (optimally-stored) or at 37°C (pre-incubated). Used OraQuick test kits were stored in a laboratory for delayed day 1 and subsequent monthly re-reading was undertaken for one year.Of 378 individuals who underwent parallel testing, 5 (1.3%) were dropped from the final analysis due to discordant or missing reference standard results (optimally-stored Determine and Uni-Gold). Compared to the diagnostic reference standard, OraQuick had a sensitivity of 97.2% (95% CI: 93.6-99.6). There were 7 false negative results among all test kits stored at 37°C and three false negatives among optimally stored kits. Excellent agreement between pre-incubated tests and optimally-stored tests with Kappa values of 1.00 for Determine and Uni-Gold; and 0.97 (95% CI: 0.95; 1.00) for OraQuick were observed. There was high visual stability on re-reading of OraQuick, with only 1/375 pre-incubated and 1/371 optimally-stored OraQuick kits changing from the initial result over 12 months.Erroneous results observed during HIV testing in low income settings are likely to be due to factors other than suboptimal storage conditions. Re-reading returned OraQuick kits may offer a convenient and accurate quality assurance approach, including in HIV self-testing programmes.

Published

2016

6. Clinical features and management of individuals admitted to hospital with monkeypox and associated complications across the UK: a retrospective cohort study

Author

Douglas L Fink, Helen Callaby, Akish Luintel, William Beynon, Helena Bond, Eleanor Y Lim, Effrossyni Gkrania-Klotsas, Jospeh Heskin, Margherita Bracchi, Balram Rathish, Iain Milligan, Geraldine O'Hara, Stephanie Rimmer, Joanna R Peters, Lara Payne, Nisha Mody, Bethany Hodgson, Penny Lewthwaite, Rebecca Lester, Stephen D Woolley, Ann Sturdy, Ashley Whittington, Leann Johnson, Nathan Jacobs, John Quartey, Brendan AI Payne, Stewart Crowe, Ivo AM Elliott, Thomas Harrison, Joby Cole, Katie Beard, Tomas-Paul Cusack, Imogen Jones, Rishi Banerjee, Tommy Rampling, Jake Dunning, Iain D Milligan, Alison J Rodger, Sanjay R Bhagani, Lucy E Lamb, Rachel C Moores, Simon F K Lee, Colin S Brown, Susan Hopkins, Stephen Mepham, Simon Warren, Aoife Molloy, Ian Cropley, Alex Kew, Natasha Karunaharan, Antonia Scobie, Jennifer Hart, Dianne Irish, Tanzina Haque, Hamid Jalal, Robin Smith, Damien Mack, Tristan Barber, Fiona Burns, Robert Miller, Eleanor Hamlyn, Pedro Simoes, Breda Athan, Jennifer Abrahamsen, Jessica Joyce, Caroline Taylor, Sally Reddecliffe, Chloe Miller, Brooke Reeve, Hugh Kingston, Tim Crocker-Buque, Nicolas Massie, Ankush Dhariwal, Angelina Jayakumar, Robert Hammond, Alexandra Bramley, Tanmay Kanitkar, Laura Maynard-Smith, Eliza Gil, Cavan O'Connor, Derek Cocker, Wendy Spicer, Marisa Lanzman, Meera Thacker, Zoe O Anorson, Dharmesh Patel, Alan Williams, Catherine F Houlihan, Dominic Wakerley, Claire N Gordon, Daniel J Bailey, Jenna Furneaux, Abbie M Bown, Elizabeth J Truelove, Marian J Killip, David Jackson, Tracy L B Beetar-King, Ulrike M V Arnold, Rhea M Strachan, Jones Matthew, Hannah J Matthew, Jane C Osborne, Richard Vipond, Barry Gibney, Jodie Owen, Will Beynon, Michael Hunter, Louise McCorry, Carol Emerson, Say Quah, Suzanne Todd, Emma McCarty, Eoin Walker, Susan Feeney, Tanya Curran, Kathy Li, JD Mullan, Kate Jackson, Peter Nelson, Kevin Lewis, Mark McNicol, Marcus Pratt, Anna Smith, Erin Vos, Fahad Alsalemee, Daniel O Leary, John Canny, Katherine McGinnity, Carly Culbert, Conor McDowell, Cathy McQuillan, Eunjin Jeong, Lynsey Glass, Jessica Dyche, Paula McClean, Rebecca Stewart, Harold Ursolino, Melissa Perry, Hannah McCormick, Joseph Heskin, Nicklas Brown, Thomas Juniper, Borja Mora-Peris, Alessia Dalla-Pria, Nicola Mackie, Lucy Garvey, Alan Winston, Graham Cooke, Mark Nelson, Emer Kilbride, Ala Elbishi, William Kerrigan, Joshua Silva, Jesal Gohil, Sasha Payagala, Yasmin Walters, Joanna Smith, Jonathan Goodfellow, Kitty Lyons, Hsiu Tung, Kinjal Patel, Merle Henderson, Michael Butler, Edu Peres, Taiana Silva Carvalho, Antoine Joly, Molly Dickinson, Luke S P Moore, Nabeela Mughal, Stephen Hughes, Shrada Chitlangia, Priyanka Viramgana, Ruth Byrne, Paul Randell, Luigi Strangis, Nicola Poveda, Deborah Bovey, Poppy Richardson, Vivian Heaslip, Christopher Higgs, Marta Boffito, Nicolo Girometti, Gary Whitlock, Victoria Tittle, Rachel Jones, Michael Rayment, Christopher Scott, David Asboe, Marcus Pond, David Muir, Movin Abeywickrema, Sarah-Lou Bailey, Sara E Boyd, Dayana Da Silva Fontoura, Anna Daunt, Claire Y Mason, Jamie Murphy, Vasanth V Naidu, Aatish Patel, Caitlin Pley, Ethan Redmore, Katherine Sharrocks, Luke B Snell, Rohan Sundramoorthi, Jerry C H Tam, Aisling Brown, Sam Douthwaite, Anna Goodman, Gaia Nebbia, William Newsholme, Nicholas Price, Emily Shaw, Alex Salam, Claire van Nispen tot Pannerden, Helen Winslow, Julia Bilinska, Sarah Keegan, Harry Coleman, Jessica Doctor, Nasreen Moini, Daniella Chilton, Golaleh Haidari, Rebecca Simons, Rajababu Kulasegaram, Nick Larbalestier, Achyuta Nori, Jack R Potter, Cecilia Tuudah, Paul Wade, Alexandra Travers, Sarah Dunford, Joshua Greenwood, Georgina Oledimmah, Lesley Gyampo, Pedro SA Pinto, AbdulKadir Muse, Zoe Parker, Charlotte Alexander, Alexander Khan, Medinat Ajayi, Abigail Baltazar, Davis Sharella, Nasra Hersi, Thuy Nguyen, Rugiatu Timbo, Ismail Jalloh, Susan Bryan, Patricia Clarke, Marcia Kerr, Fidelis Amedu, Maria BohoBonaba, Sarah Haque, Michelle Howson, Norbai Tambilawan, Soledad Yupanqui Estay, Hawanatu Bangura, Tseday Gideon, Damilola Jerome-oboh, Linda Tetteh, Chioma Nwagu, Viwoalo Agbaglah, Nona Narag, Mahima Zaveri, Maedhbh Ni Luanaigh, Peggy Keane, Aula Abbara, Olamide Dosekun, Mhairi Bolland, Adam Stafford, Dina Saleh, Rhianna Sheridan, Ella Davies, Kristi Sun, Mark Gilchrist, Priti Kukadia, Muhammed Embrahimsa, Christopher Chiu, Lauren Taylor, Charlotte Short, Jasmini Alagratnam, Iresh Jayaweera, Kavitha Gundugola, Lara V S Payne, Killian Quinn, Caoimhe Nic Fhogartaigh, Nivenjit Kaur, Salmaan Bholah, Kajann Kantha, Jonathan Youngs, Temi Lampejo, Nicholas Pitto, David S Lawrence, Holly Middleditch, Lourdes Dominguez-Dominguez, Ayoma Ratnappuli, Sara Al-Hashimi, Amelia Oliveira, Zoe Ottaway, Larissa Mulka, Anne M Neary, Michael R Downey, Danielle C Lucy, Craig I McCallum, Michael Beadsworth, Libuse Ratcliffe, Tom E Fletcher, Gerry Davies, Nicholas Wong, Stephen Aston, Thomas E Wingfield, Thomas Blanchard, Paul Hine, Susie Gould, Christopher Smith, Michael Abouyannis, Abolaji Atomode, James Cruise, Merna Samual, Nicola Scott, Vino Srirathan, Joseph Lewis, Lauren Richards, Mary-Ann Cummings, Emily Gillan, Rebecca Peers, Amy Tickle, Grace Keating, Tendi Chinyanda, Mav Sanchez, Daniel Harrison, null Hoyle, Ben Metcalfe, Jennifer Taylor, Nicky Johnson, Neil Kelle, Kirsty McDowell, Ian Richardson, Monette Saguidan, Nicky Farmer, Angella Gillespie, Shay Willoughby, Samantha Parker, Shamseena Avulan, Shazia Arif, Suzanne Marshall, David Carlisle, Mohsen Rezaei, Angela Booth, Joanne Watts, Lauren Tremarco, Priyanga Jeyanayagam, Odinaka Ubochi, Daniel Vagianos, Mark Richardson, Anthony Jarvis, Kyra Gow, Jade Walmsley, Adam O'keefe, Anna Smielewska, Mark Hopkins, Fatima Balane, Sarah Bradley, Tumena Corrah, Venus Daquiz, Christopher Dugan, Joshua Elliot, Fiona Foley, Dawn Friday, May Gamit, David Garner, Karishma Gokani, Laurence John, Deepa Joseph, Nuzhath Khan, Cherifer Mamuyac, Alastair McGregor, John McSorley, Victoria Parris, Luciana Rubinstein, Julian Rycroft, Kelcy Salinas, Jason Salinas, Jency Sebatian, Melanie Smith, Marina Tejero Garcia, Uchenna Ume, Margarete Vicentine, Gabriel Wallis, Alec Bonington, Alison Uriel, Andrew Ustianowski, Balazs Dancso, Celia Hogan, Clare van Halsema, F Javier Vilar, Karen Devine, Katherine Ajdukiewicz, Rajesh Rajendran, Samit Ghosh, Michael Riste, Nicholas Machin, Chitra Babu, Shazaad Ahmad, Dorcas Obeng, Farnaz Dave, Gavin Conolley, Joseph Thompson, Maya Tickell-Painter, Prasun Chakravorty, Rachel Pringle, Mohammad R Zafar, Sarah Lawrence, Amada Sanchez-Gonzalez, Cristina Fernandez, Lynsey Goodwin, David Carey, Molly Howarth-Maddison, Samuel Moody, Rebecca Upton, Christina Apthorp, Charlotte Murray, Kirstie Salthouse, Sabah Nadeem, Grant Ridley, Francesca White, Andrew Brown, Michael Lawless, Mohamed Mohamed, Robert Mulligan, Amy Belfield, Jacob Brolly, Maria Calderon, James Cheveau, Milo Cullinan, Sophie Garrad, Will Griffiths, Aidan Ireland, Peter Ireland, Charlotte Milne, Paul Nwajiugo, Bijan Ghavami-Kia, Chris Duncan, Adam Evans, Ewan Hunter, Ashley Price, Matthias Schmid, Uli Schwab, Yusri Taha, Brendan Payne, Ivo A M Elliott, Charles J Woodrow, Drosos E Karageorgopoulos, Peter J Davis, Emily Lord, Oliver J Bannister, Andrew B Dagens, Anne Tunbridge, Saher Choudry, Adam Telfer, Ihsan Jhibril, Syed N Atta, Ben Stone, Cariad Evans, Mike Ankcorn, Suha Akili, Mehmet Yavuz, Vicky Goodall, Sam Farrow, Georgina Mountford, Kate Beard, Julian Sutton, Tristan Clark, Annette Mason, Mike Vickers, Derek Macallan, Tihana Bicanic, Angela Houston, Cassie Pope, NgeeKeong Tan, Christopher Ward, Jonathan Cohen, Marieke Emonts-le Clercq, David Porter, Andrew Riordan, Ruchi Sinha, Elizabeth Whittaker, and Monkeypox, Specialist and High Consequence Infectious Diseases Centres Network for

Subjects

Infectious Diseases

Abstract

Background:The scale of the 2022 global mpox (formerly known as monkeypox) outbreak has been unprecedented. In less than 6 months, non-endemic countries have reported more than 67 000 cases of a disease that had previously been rare outside of Africa. Mortality has been reported as rare but hospital admission has been relatively common. We aimed to describe the clinical and laboratory characteristics and outcomes of individuals admitted to hospital with mpox and associated complications, including tecovirimat recipients. Methods:In this cohort study, we undertook retrospective review of electronic clinical records and pathology data for all individuals admitted between May 6, and Aug 3, 2022, to 16 hospitals from the Specialist and High Consequence Infectious Diseases Network for Monkeypox. The hospitals were located in ten cities in England and Northern Ireland. Inclusion criteria were clinical signs consistent with mpox and MPXV DNA detected from at least one clinical sample by PCR testing. Patients admitted solely for isolation purposes were excluded from the study. Key outcomes included admission indication, complications (including pain, secondary infection, and mortality) and use of antibiotic and anti-viral treatments. Routine biochemistry, haematology, microbiology, and virology data were also collected. Outcomes were assessed in all patients with available data. Findings:156 individuals were admitted to hospital with complicated mpox during the study period. 153 (98%) were male and three (2%) were female, with a median age of 35 years (IQR 30–44). Gender data were collected from electronic patient records, which encompassed full formal review of clincian notes. The prespecified options for data collection for gender were male, female, trans, non-binary, or unknown. 105 (71%) of 148 participants with available ethnicity data were of White ethnicity and 47 (30%) of 155 were living with HIV with a median CD4 count of 510 cells per mm3(IQR 349–828). Rectal or perianal pain (including proctitis) was the most common indication for hospital admission (44 [28%] of 156). Severe pain was reported in 89 (57%) of 156, and secondary bacterial infection in 82 (58%) of 142 individuals with available data. Median admission duration was 5 days (IQR 2–9). Ten individuals required surgery and two cases of encephalitis were reported. 38 (24%) of the 156 individuals received tecovirimat with early cessation in four cases (two owing to hepatic transaminitis, one to rapid treatment response, and one to patient choice). No deaths occurred during the study period. Interpretation:Although life-threatening mpox appears rare in hospitalised populations during the current outbreak, severe mpox and associated complications can occur in immunocompetent individuals. Analgesia and management of superimposed bacterial infection are priorities for patients admitted to hospital.

Published

2023

7. A novel, magnetic bead-based extraction method for the isolation of antimicrobial resistance genes with a case study in river water in Malawi

Author

Rachel L. Byrne, Derek Cocker, Ghaith Alyayyoussi, M. Mphasa, Mary Charles, Tamandani Mandula, Christopher T. Williams, Jonathan Rigby, Jack Hearn, Nicholas Feasey, Emily R. Adams, and Thomas Edwards

Subjects

Malawi, food.ingredient, medicine.drug_class, Cephalosporin, Applied Microbiology and Biotechnology, DNA sequencing, law.invention, chemistry.chemical_compound, food, Rivers, law, Drug Resistance, Bacterial, medicine, Agar, Polymerase chain reaction, Chromatography, biology, Magnetic Phenomena, Extraction (chemistry), Water, General Medicine, biology.organism_classification, DNA extraction, Anti-Bacterial Agents, Cephalosporins, Carbapenems, chemistry, Genes, Bacterial, Bacteria, DNA, Biotechnology

Abstract

BackgroundEnvironmental water samples are increasingly recognised as an important reservoir of antimicrobial resistance (AMR) genes. Polymerase chain reaction (PCR) and next generation sequencing (NGS) offer a potentially inclusive surveillance platform for a wide range of AMR genes. However, molecular methods are dependent upon the extraction of DNA of high yield and quality. Current options for DNA extraction from complex environmental matrices for downstream molecular applications are either expensive or low yielding. We present here a novel magnetic bead-based DNA extraction method, for the detection of antimicrobial resistance genes (ARGs) from river water in Malawi, named MagnaExtract. MethodsMagnaExtract involves initial filtration of 250ml freshwater, followed by an overnight incubation of the filter in 15ml buffered peptone water (BPW), common procedure in microbiology laboratories. 200{micro}l is then taken for a boil (95{degrees}C) and spin step and mixed with magnetic beads to bind DNA. Following washes with ethanol, the DNA is eluted in nuclease-free water. To determine the effectiveness of this method, 98 freshwater samples were collected from two rivers in Southern Malawi, and DNA was isolated using the MagnaExtract method, two commercial Qiagen (Germany) kits; PowerWater and DNeasy Blood and tissue, alongside a boil and spin of BPW, and a boil and spin from bacterial isolate grown on agar media. All samples were screened with a high-resolution melt (HRM) PCR panel previously validated for the detection of third generation cephalosporin and carbapenem ARGs. We compared the DNA yield obtained using all extraction methods, as well as the identification of each ARG. ResultsDNA yield using MagnaExtract was statistically greater than both boil and spin methods and DNeasy Blood & Tissue (Qiagen, Germany). DNA yield was slightly lower than using PowerWater (Qiagen) but the difference was not statistically significant. MagnaExtract was the only method to identify ARGs in all 98 water samples compared with PowerWater (n=82), DNeasy (n=95) boilate of BPW (n=75) and boilate of bacterial isolate (n=87). The most commonly detected ARG was OXA-48 (n=93). In addition, we found overnight incubation in non-selective enrichment broth (BPW) to promote the growth of bacteria harbouring extended spectrum beta lactamase (ESBL) genes and reduction in the detection of carbapenemase genes. ConclusionThe MagnaExtract approach offers a simple, affordable, high yielding DNA extraction method for the detection of ARGs isolated from river water samples.

Published

2022

8. Investigating One Health risks for human colonisation with extended spectrum β-lactamase-producing Escherichia coli and Klebsiella pneumoniae in Malawian households: a longitudinal cohort study

Author

Derek Cocker, Kondwani Chidziwisano, Madalitso Mphasa, Taonga Mwapasa, Joseph M Lewis, Barry Rowlingson, Melodie Sammarro, Winnie Bakali, Chifundo Salifu, Allan Zuza, Mary Charles, Tamandani Mandula, Victor Maiden, Stevie Amos, Shevin T Jacob, Henry Kajumbula, Lawrence Mugisha, David Musoke, Rachel Byrne, Thomas Edwards, Rebecca Lester, Nicola Elviss, Adam P Roberts, Andrew C Singer, Christopher Jewell, Tracy Morse, and Nicholas A Feasey

Subjects

Microbiology (medical), Infectious Diseases, Virology, Microbiology

Published

2023

9. Risk Factors, Temporal Dependence, and Seasonality of Human extended-spectrum β-lactamases-producingEscherichia coliandKlebsiella pneumoniaeColonization in Malawi: A Longitudinal Model-based Approach

Author

Melodie Sammarro, Barry Rowlingson, Derek Cocker, Kondwani Chidziwisano, Shevin T Jacob, Henry Kajumbula, Lawrence Mugisha, David Musoke, Rebecca Lester, Tracy Morse, Nicholas Feasey, and Chris Jewell

Subjects

Microbiology (medical), Infectious Diseases

Abstract

BackgroundSub-Saharan Africa has the highest estimated death rate attributable to antimicrobial resistance, especially from extended-spectrum β-lactamase-producing Enterobacterales (ESBL-E). However, the dynamics of human colonization in the community with ESBL-E are not well described. Inadequate water, sanitation, and hygiene infrastructure and associated behaviors are believed to play an important role in transmission of ESBL-E, and an improved understanding of the temporal dynamics of within-household transmission could help inform the design of future policies.MethodsIn this 18-month study, using microbiological data and household surveys, we built a multivariable hierarchical harmonic logistic regression model to identify risk factors for colonization with ESBL-producing Escherichia coli and Klebsiella pneumoniae, reflecting household structure and temporal correlation of colonization status.ResultsBeing male was associated with a lower risk of colonization with ESBL-producing E. coli (odds ratio [OR], 0.786; credible interval [CrI], .678–.910), whereas the use of a tube well or a borehole was associated with an increased risk (OR, 1.550; CrI, 1.003–2.394). For ESBL-producing K. pneumoniae, recent antibiotic exposure increased risk of colonization (OR, 1.281; CrI, 1.049–1.565), whereas sharing plates decreased that risk (OR, 0.672; CrI, .460–.980). Finally, the temporal correlation range of 8 to 11 weeks provided evidence that within-household transmission occurs within this time frame.ConclusionsWe describe different risks for colonization with different enteric bacterial species. Our findings suggest interventions to reduce transmission targeted at the household level need to focus on improving water, sanitation, and hygiene infrastructure and associated behaviors, whereas at the community level, they should focus on both environmental hygiene and antibiotic stewardship.

Published

2023

10. Mortality Associated with 3 rd Generation Cephalosporin Resistance in Enterobacterales Bloodstream Infections at Eight Sub-Saharan African Hospitals, a Prospective Cohort Study (MBIRA)

Author

Alexander Michael Aiken, Andrea M. Rehman, Marlieke E. A. de Kraker, Lola Madrid, Meron Kebede, Appiah-Korang Labi, Noah Obeng-Nkrumah, Brian Nyamwaya, Wangeci Kagucia, Derek Cocker, Kondwani Kawaza, Rebecca Lester, Kenneth C. Iregbu, Nubwa Medugu, Philip I. Nwajiobi-Princewill, Angela Dramowski, Tolbert B. Sonda, Asia Hemed, Sombo Fwoloshi, David Ojok, J. Anthony G. Scott, Andrew Whitelaw, Jabir Aliye, Nega Assefa, Dumessa Edessa, Joe Oundo, Mulu Berihun, Thomas Dankwah, Mary M. Osei, Maud Fandoh, Caroline Mulunda, Benedict Mvera, Mabvuto Chimenya, Nicholas A. Feasey, Jane Mallewa, Tobechi A. Akujobi, Chinelo H. Okonkwo, Luzell Britz, Andre Bulabula, Aaqilah Fataar, Blandina T. Mmbaga, Neema Ng'unda, Uchizi Chirwa, Nyambe Kakula, Charles Mutemba, and Ruth Nakazwe

Published

2023

11. Treatment and control of invasive Gram-negative bacterial infection in eight hospitals across sub-Saharan Africa: a cross-sectional study

Author

Alexander M. Aiken, Brian Nyamwaya, Lola Madrid, Dumessa Edessa, Appiah-Korang Labi, Noah Obeng-Nkrumah, William Mwabaya, Mabvuto Chimenya, Derek Cocker, Kenneth C. Iregbu, Philip I.P. Nwajiobi-Princewill, Angela Dramowski, Tolbert Sonda, Blandina Theophil Mmbaga, David Ojok, Sombo Fwoloshi, J. Anthony G. Scott, Andrew Whitelaw, and MBIRA study collaborators

Abstract

Background: Bloodstream infections caused by Enterobacterales show high frequency of antimicrobial resistance (AMR) in many Low- and Middle-Income Countries. We aimed to describe the variation in circumstances for management of such resistant infections in a group of African public-sector hospitals participating in a major research study. Methods: We gathered data from eight hospitals across sub-Saharan Africa to describe hospital services, infection prevention and antibiotic stewardship activities, using two WHO-generated tools. We collected monthly cross-sectional data on availability of antibiotics in the hospital pharmacies for bloodstream infections caused by Enterobacterales.We compared the availability of these antibiotics to actual patient-level use of antibiotics in confirmed Enterobacterales bloodstream infections (BSI). Results: Hospital circumstances for institutional management of resistant BSI varied markedly. This included self-evaluated infection prevention level (WHO-IPCAF score: median 428, range 155 to 687.5) and antibiotic stewardship activities (WHO stewardship toolkit questions: median 14.5, range 2 to 23). These results did not correlate with national income levels. Across all sites, ceftriaxone and ciprofloxacin were the most consistently available antibiotic agents, followed by amoxicillin, co-amoxiclav, gentamicin and co-trimoxazole. There was substantial variation in the availability of some antibiotics, especially carbapenems, amikacin and piperacillin-tazobactam with degree of access linked to national income level. Investigators described out-of-pocket payments for access to additional antibiotics at 7/8 sites. The in-pharmacy availability of antibiotics correlated well with actual use of antibiotics for treating BSI patients. Conclusion: There was wide variation between these African hospitals for a range of important circumstances relating to treatment and control of severe bacterial infections, though these did not all correspond to national income level. For the majority of antibiotics and hospitals, patient-level use reflected local in-hospital drug availability, suggesting external sourcing of antibiotics was relatively infrequent. Antimicrobial resistant bacterial infections could plausibly show different clinical impacts across sub-Saharan Africa due to this contextual variation. More estimates of the impact of AMR are needed from countries of different income levels to account for these differences.

Published

2022

12. Investigating risks for human colonisation with extended spectrum beta-lactamase producing E. coli and K. pneumoniae in Malawian households: a one health longitudinal cohort study

Author

Derek Cocker, Kondwani Chidziwisano, Madalitso Mphasa, Taonga Mwapasa, Joseph M. Lewis, Barry Rowlingson, Melodie Sammarro, Winnie Bakali, Chifundo Salifu, Allan Zuza, Mary Charles, Tamandani Mandula, Victor Maiden, Stevie Amos, Shevin T Jacob, Henry Kajumbula, Lawrence Mugisha, David Musoke, Rachael Byrne, Thomas Edwards, Rebecca Lester, Nicola Elviss, Adam Roberts, Andrew C Singer, Christopher Jewell, Tracy Morse, and Nicholas A Feasey

Abstract

BackgroundLow- and middle-income countries (LMICs) have high morbidity and mortality from drug-resistant infections, especially from enteric bacteria such as Escherichia coli. LMICs have varying infrastructure and services in the community to separate people from human and animal waste, creating risks for ESBL-Enterobacterales (ESBL-E) transmission. Limited data exist from Southern Africa on the prevalence of ESBL-E the community.Methods and findingsIn this longitudinal cohort study we took a one-health approach to investigating prevalence and distribution of ESBL-E in urban, peri-urban and rural Malawian households between May 2018 and October 2020. We described human health, antibiotic usage (ABU), health seeking behaviour, structural and behavioural environmental health practices, and animal husbandry at these households. In parallel, human and animal stool and diverse environmental samples were collected and cultured to identify presence of ESBL E. coli and ESBL K. pneumoniae. Univariable and multivariable analysis was performed to determine associations with human ESBL-E colonisation.We recruited 300 households, totalling 841 visits, and a paucity of environmental health infrastructure and materials for safe sanitation was noted across all sites. In total, 11,975 samples were cultured and ESBL-E were isolated from 41.8% (n=1190) of human stool and 29.8% (n=290) of animal stool samples. Animal species with particularly high rates of ESBL-E colonisation included pigs (56.8%, n=21) poultry (32.5%, n=148) and dogs (58.8% n= 30). ESBL-E were isolated from 66.2% (n=339) of river water samples and 46.0% (n=138) of drain samples. Urban areas had greater ESBL-E contamination of food, household surfaces, floors and the external environment, alongside the highest rates of ESBL-E colonisation in humans (47.1%, n=384) and animals (55.1%, n=65). Multivariable models illustrated that human ESBL E. coli colonisation was associated with the wet season (aOR = 1.66, 95%CrI: 1.38-2.00), living in urban areas (aOR = 2.01, 95%CrI: 1.26-3.24), advanced age (aOR = 1.14, 95%CrI: 1.05-1.24) and in households where animals were observed interacting with food (aOR = 1.62, 95%CrI: 1.17-2.28) or kept inside (aOR = 1.58, 95%CrI: 1.00-2.43). Human ESBL K. pneumoniae colonisation was also associated with the wet season (aOR = 2.23, 95%CrI: 1.63-2.76.ConclusionWe identified extremely high levels of ESBL-E colonisation in humans and animals and contamination of the environment in Southern Malawi. Urbanisation and season are key risks for ESBL-E colonisation, perhaps reflecting environmental contamination as toilets overflow in high population density areas in heavy rains in the wet season. Without adequate efforts to improve environmental health, ESBL transmission is likely to persist in this setting.

Published

2022

13. Risk factors, temporal dependence, and seasonality of human ESBL-producing E. coli and K. pneumoniae colonisation in Malawi: a longitudinal model-based approach

Author

Melodie Sammarro, Barry Rowlingson, Derek Cocker, Kondwani Chidziwisano, Shevin T. Jacob, Henry Kajumbula, Lawrence Mugisha, David Musoke, Rebecca Lester, Tracy Morse, Nicholas Feasey, and Chris Jewell

Abstract

BackgroundAntimicrobial resistance (AMR) represents an important threat to achieving the sustainable development goals in Sub-Saharan Africa (sSA). sSA is reported to have the highest estimated death rate attributable to AMR, with Extended-Spectrum Beta-Lactamase-producing Enterobacterales, such as Klebsiella pneumoniae and Escherichia coli, representing the greatest challenge. However, the dynamics of human colonisation with such bacteria in the sSA community setting are not well known. Inadequate water, sanitation and hygiene (WASH) infrastructure and associated behaviours are thought to play an important role in transmission of AMR-bacteria, and an improved understanding of the temporal dynamics of within-household transmission could help inform the design of public health policies that interrupt transmission of AMR-bacteria.Methods and FindingsIn this 18-month study, individuals from households in diverse areas of Southern Malawi were recruited and human stool samples were longitudinally collected. Using microbiological data and household surveys, we built a multivariable hierarchical harmonic logistic regression model to identify risk factors for colonisation with ESBL-producing E. coli and K. pneumoniae, reflecting household structure and temporal correlation of colonisation status between timepoints.Important risk factors were identified, with men having a lower risk of becoming colonised with ESBL-producing E. coli (OR 0.786 CrI[0.678-0.910]) and the use of a tube well or a borehole as a water drinking source highly increasing the risk of becoming colonised (OR 1.550 CrI[1.003-2.394]). Coming into contact with standing water also appeared to be negatively associated with colonisation status (OR 0.749 CrI[0.574-0.978]). For ESBL-producing K. pneumoniae, having recently taken a course of antibiotics increased the risk of being colonised (OR 1.281 CrI[1.049-1.565]). We also found a negative association between eating from shared plates and colonisation with ESBL-producing K. pneumoniae (OR 0.672 CrI[0.460-0.980]). Finally, we detected a temporal correlation range of eight to eleven weeks, providing evidence that within-household transmission occurs within this time frame.ConclusionsWe suggest that interventions aimed at preventing transmission might have the best impact when targeted at the household-level and focused on a combination of improving WASH infrastructure and modifying associated behaviours. Additionally, we showed that antibiotic use is important when looking at colonisation with ESBL-producing K. pneumoniae and therefore infection prevention and control measures and antibiotic use and stewardship training could help in reducing transmission.

Published

2022

14. Drivers of resistance in Uganda and Malawi (DRUM): a protocol for the evaluation of One-Health drivers of extended spectrum beta lactamase (ESBL) resistance in low-middle income countries (LMICs)

Author

Derek Cocker, Melodie Sammarro, Kondwani Chidziwisano, Nicola Elviss, Shevin T. Jacob, Henry Kajumbula, Lawrence Mugisha, David Musoke, Patrick Musicha, Adam P. Roberts, Barry Rowlingson, Andrew C. Singer, Rachel L. Byrne, Thomas Edwards, Rebecca Lester, Catherine N. Wilson, Beth Hollihead, Nicholas Thomson, Christopher P. Jewell, Tracy Morse, and Nicholas A. Feasey

Subjects

wa_30, TA, Health, qw_138, Medicine (miscellaneous), General Biochemistry, Genetics and Molecular Biology, qw_45, wa_540

Abstract

In sub-Saharan Africa (sSA), there is high morbidity and mortality from severe bacterial infection and this is compounded by antimicrobial resistance, in particular, resistance to 3rd-generation cephalosporins. This resistance is typically mediated by extended-spectrum beta lactamases (ESBLs). To interrupt ESBL transmission it will be important to investigate how human behaviour, water, sanitation, and hygiene (WASH) practices, environmental contamination, and antibiotic usage in both urban and rural settings interact to contribute to transmission of ESBL E. coli and ESBL K. pneumoniae between humans, animals, and the environment. Here we present the protocol for the Drivers of Resistance in Uganda and Malawi (DRUM) Consortium, in which we will collect demographic, geospatial, clinical, animal husbandry and WASH data from a total of 400 households in Uganda and Malawi. Longitudinal human, animal and environmental sampling at each household will be used to isolate ESBL E. coli and ESBL K. pneumoniae. This will be complimented by a Risks, Attitudes, Norms, Abilities and Self-Regulation (RANAS) survey and structured observations to understand the contextual and psychosocial drivers of regional WASH practices. Bacterial isolates and plate sweeps will be further characterised using a mixture of short-,long-read and metagenomic whole-genome sequencing. These datasets will be integrated into agent-based models to describe the transmission of EBSL resistance in Uganda and Malawi and allow us to inform the design of interventions for interrupting transmission of ESBL-bacteria.

Published

2022

15. Community exposure assessment to anti-microbial resistance (AMR); case study of Malawi

Author

Taonga Mwapasa, Madalitso Mphasa, Derek Cocker, Nicholas Feasey, and Tracy Morse

Subjects

RA0421

Abstract

Anti-microbial resistance is currently one of the greatest global health threat (CDC, 2020, WHO, 2020). Efforts have previously focused on the healthcare sector through antibiotic stewardship and surveillance (Cueni, 2020). Poor water, sanitation and hygiene (WASH) practices and infrastructure contribute to the transmission of resistant bacteria (Iskandar et al., 2020). Low-and middle-income countries (LMICs) such as Malawi have pre-existing WASH challenges, which increase the risk of population exposure to AMR (Cassivi et al., 2020). There is an existing knowledge gap regarding the prevalence of AMR in the wider community environment (Ahammad et al., 2018).

Published

2021

16. Lessons learnt from the rapid implementation of reusable personal protective equipment for COVID-19 in Malawi

Author

Kelvin Mponda, Derek Cocker, Mulinda Nyirenda, Luis Gadama, Priyanka Patel, Fumbani Limani, Servace Sakala, Feggie Bodole, Kwazizira Samson Mndolo, Queen Dube, Bridget Freyne, Pratiksha Patel, Stephen B. Gordon, and David Garley

Subjects

Malawi, medicine.medical_specialty, Medicine (General), Laundry, wa_395, Infectious and parasitic diseases, RC109-216, wa_250, diseases, R5-920, wc_506, Health care, Pandemic, wc_505, medicine, Humans, infections, disorders, Pandemics, Personal Protective Equipment, Personal protective equipment, injuries, wa_105, Service (business), Practice, Surge Capacity, SARS-CoV-2, business.industry, Health Policy, Public health, wa_525, public health, Public Health, Environmental and Occupational Health, COVID-19, medicine.disease, Medical emergency, business, Waste disposal

Abstract

The SARS-CoV-2 pandemic has challenged health systems and healthcare workers worldwide. Access to personal protective equipment (PPE) is essential to mitigate the risk of excess mortality in healthcare providers. In Malawi, the cost of PPE represents an additional drain on available resources. In the event of repeated waves of disease over several years, the development of sustainable systems of PPE is essential. We describe the development, early implementation and rapid scale up of a reusable gown service at a tertiary-level hospital in Blantyre, Malawi. Challenges included healthcare worker perceptions around the potential of reduced efficacy of cotton gowns, the need to plan for surge capacity and the need for ongoing training of laundry staff in safety and hygiene procedures. Benefits of the system included increased coverage, decreased cost and reduced waste disposal. The implementation of a reusable cotton gown service is feasible, acceptable and cost-effective in tertiary centres providing specialist COVID-19 care at the height of the pandemic. This innovation could be expanded beyond low-income settings.

Published

2021

17. Development of a protocol for assessing the role of WASH in AMR distribution in the environment

Author

Tracy Morse, Kondwani Chidziwisano, David Musoke, Derek Cocker, and Nicholas Feasey

Subjects

TD

Abstract

Resistance in Malawi and Uganda (DRUM) consortium to measure the role of WASH in the transmission and control of AMR Abstract In Low and Middle Income countries (LMICs), there is a high incidence of severe bacterial infection, a critically inadequate health system infrastructure to diagnose and treat bacterial infections and widespread and uncontrolled availability of antimicrobials. This situation causes both a huge burden of morbidity and mortality, and is increasing selective pressure for the emergence of antimicrobial resistance (AMR) in pathogens. As LMICs will be the last to benefit from new classes of antimicrobials it is therefore urgent to undertake research addressing AMR in LMICs that aims to identify drivers and interrupt transmission of AMR determinants responsible. Exposures associated with WASH are integral to enteric bacteria and AMR transmission. AMR elements have been found in water, faeces and wastewater in LMICs, and this is compounded by a lack of faecal management (e.g. open defaecation, lack of access to faecal sludge management) and multiple uses of water (e.g. washing, irrigation, animal management and drinking). These factors contribute to community borne AMR transmission, and must be considered across multiple exposure pathways within the community. Focused in urban, peri-urban and rural settings in Malawi and Uganda, the Drivers of Antimicrobial Resistance in Uganda and Malawi (DRUM) consortium is an interdisciplinary programme funded by the Medical Research Council (2018 – 2021). The study aims to address three key questions (1) What are the drivers of ESBL E. coli and ESBL Klebsiella pneumoniae transmission in Uganda and Malawi?; (2) What are the critical points at which efforts to interrupt human AMR acquisition are likely to have the greatest impact?; and (3) Which strategies are likely to be most affordable and feasible to societies and how far is this specific to context? The research will develop agent-based models to enable us to predict how these transmission pathways can be interrupted. Data will be collated on a range of issues including: antibiotic use; antibiotic availability; illness; household demographics; and environmental contamination using both qualitative and quantitative methods. Key to this model will be the under researched area of AMR and WASH. This will develop a clear understanding of water, sanitation and hygiene (WASH) infrastructure and practices both domestically and institutionally [transect walks n=8; observations and checklists at household n=255; institutions n=50], identify the underlying influences on current practices [in depth interviews n=75; key informant interviews n=50; behavioral determinant questionnaires n=500; focus group discussions n=25] and identify drivers which may be amenable to change. These methods will be described in detail. Data will be collected with extensive environmental sampling to identify the transmission routes, support the design of the model and inform interventions. Existing national and international policies in the WASH sector do not currently consider AMR, and the production of evidence in this area is key to supporting and driving policy integration and uptake.

Published

2019

18. Linezolid for drug-resistant pulmonary tuberculosis

Author

Bhagteshwar Singh, Hannah Ryan, Derek Cocker, and Derek J. Sloan

Subjects

mesh:Tuberculosis, Pulmonary, Non-Randomized Controlled Trials as Topic, Antibiotics, mesh:Tuberculosis, Pulmonary/mortality, Drug resistance, chemistry.chemical_compound, 0302 clinical medicine, Tuberculosis, Multidrug-Resistant, mesh:Tuberculosis, Multidrug‐Resistant, Pharmacology (medical), 030212 general & internal medicine, Randomized Controlled Trials as Topic, media_common, mesh:Withholding Treatment, mesh:Tuberculosis, Multidrug‐Resistant/mortality, mesh:Linezolid, Treatment Outcome, mesh:Tuberculosis, Multidrug‐Resistant/drug therapy, mesh:Humans, mesh:Treatment Outcome, Medicine General & Introductory Medical Sciences, Drug, medicine.medical_specialty, Tuberculosis, medicine.drug_class, mesh:Withholding Treatment/statistics & numerical data, media_common.quotation_subject, mesh:Tuberculosis, Pulmonary/drug therapy, mesh:Antibiotics, Antitubercular/therapeutic use, 03 medical and health sciences, Pharmacotherapy, Internal medicine, medicine, Humans, Adverse effect, Antibiotics, Antitubercular, Tuberculosis, Pulmonary, mesh:Antibiotics, Antitubercular, business.industry, Linezolid, mesh:Antibiotics, Antitubercular/adverse effects, medicine.disease, mesh:Randomized Controlled Trials as Topic, Regimen, Withholding Treatment, chemistry, mesh:Non‐Randomized Controlled Trials as Topic, business, mesh:Linezolid/adverse effects, 030217 neurology & neurosurgery, mesh:Linezolid/therapeutic use

Abstract

Background Linezolid was recently re‐classified as a Group A drug by the World Health Organization (WHO) for treatment of multi‐drug resistant tuberculosis (MDR‐TB) and extensively drug‐resistant tuberculosis (XDR‐TB), suggesting that it should be included in the regimen for all patients unless contraindicated. Linezolid use carries a considerable risk of toxicity, with the optimal dose and duration remaining unclear. Current guidelines are mainly based on evidence from observational non‐comparative studies. Objectives To assess the efficacy of linezolid when used as part of a second‐line regimen for treating people with MDR and XDR pulmonary tuberculosis, and to assess the prevalence and severity of adverse events associated with linezolid use in this patient group. Search methods We searched the following databases: the Cochrane Infectious Diseases Specialized Register; CENTRAL; MEDLINE; Embase; and LILACS up to 13 July 2018. We also checked article reference lists and contacted researchers in the field. Selection criteria We included studies in which some participants received linezolid, and others did not. We included randomized controlled trials (RCTs) of linezolid for MDR and XDR pulmonary tuberculosis to evaluate efficacy outcomes. We added non‐randomized cohort studies to evaluate adverse events. Primary outcomes were all‐cause and tuberculosis‐associated death, treatment failure, and cure. Secondary outcomes were treatment interrupted, treatment completed, and time to sputum culture conversion. We recorded frequency of all and serious adverse events, adverse events leading to drug discontinuation or dose reduction, and adverse events attributed to linezolid, particularly neuropathy, anaemia, and thrombocytopenia. Data collection and analysis Two review authors (BS and DC) independently assessed the search results for eligibility and extracted data from included studies. All review authors assessed risk of bias using the Cochrane ‘Risk of bias' tool for RCTs and the ROBINS‐I tool for non‐randomized studies. We contacted study authors for clarification and additional data when necessary. We were unable to perform a meta‐analysis as one of the RCTs adopted a study design where participants in the study group received linezolid immediately and participants in the control group received linezolid after two months, and therefore there were no comparable data from this trial. We deemed meta‐analysis of non‐randomized study data inappropriate. Main results We identified three RCTs for inclusion. One of these studies had serious problems with allocation of the study drug and placebo, so we could not analyse data for intervention effect from it. The remaining two RCTs recruited 104 participants. One randomized 65 participants to receive linezolid or not, in addition to a background regimen; the other randomized 39 participants to addition of linezolid to a background regimen immediately, or after a delay of two months. We included 14 non‐randomized cohort studies (two prospective, 12 retrospective), with a total of 1678 participants. Settings varied in terms of income and tuberculosis burden. One RCT and 7 out of 14 non‐randomized studies commenced recruitment in or after 2009. All RCT participants and 38.7% of non‐randomized participants were reported to have XDR‐TB. Dosing and duration of linezolid in studies were variable and reported inconsistently. Daily doses ranged from 300 mg to 1200 mg; some studies had planned dose reduction for all participants after a set time, others had incompletely reported dose reductions for some participants, and most did not report numbers of participants receiving each dose. Mean or median duration of linezolid therapy was longer than 90 days in eight of the 14 non‐randomized cohorts that reported this information. Duration of participant follow‐up varied between RCTs. Only five out of 14 non‐randomized studies reported follow‐up duration. Both RCTs were at low risk of reporting bias and unclear risk of selection bias. One RCT was at high risk of performance and detection bias, and low risk for attrition bias, for all outcomes. The other RCT was at low risk of detection and attrition bias for the primary outcome, with unclear risk of detection and attrition bias for non‐primary outcomes, and unclear risk of performance bias for all outcomes. Overall risk of bias for the non‐randomized studies was critical for three studies, and serious for the remaining 11. One RCT reported higher cure (risk ratio (RR) 2.36, 95% confidence interval (CI) 1.13 to 4.90, very low‐certainty evidence), lower failure (RR 0.26, 95% CI 0.10 to 0.70, very low‐certainty evidence), and higher sputum culture conversion at 24 months (RR 2.10, 95% CI 1.30 to 3.40, very low‐certainty evidence), amongst the linezolid‐treated group than controls, with no differences in other primary and secondary outcomes. This study also found more anaemia (17/33 versus 2/32), nausea and vomiting, and neuropathy (14/33 versus 1/32) events amongst linezolid‐receiving participants. Linezolid was discontinued early and permanently in two of 33 (6.1%) participants who received it. The other RCT reported higher sputum culture conversion four months after randomization (RR 2.26, 95% CI 1.19 to 4.28), amongst the group who received linezolid immediately compared to the group who had linezolid initiation delayed by two months. Linezolid was discontinued early and permanently in seven of 39 (17.9%) participants who received it. Linezolid discontinuation occurred in 22.6% (141/624; 11 studies), of participants in the non‐randomized studies. Total, serious, and linezolid‐attributed adverse events could not be summarized quantitatively or comparatively, due to incompleteness of data on duration of follow‐up and numbers of participants experiencing events. Authors' conclusions We found some evidence of efficacy of linezolid for drug‐resistant pulmonary tuberculosis from RCTs in participants with XDR‐TB but adverse events and discontinuation of linezolid were common. Overall, there is a lack of comparative data on efficacy and safety. Serious risk of bias and heterogeneity in conducting and reporting non‐randomized studies makes the existing, mostly retrospective, data difficult to interpret. Further prospective cohort studies or RCTs in high tuberculosis burden low‐income and lower‐middle‐income countries would be useful to inform policymakers and clinicians of the efficacy and safety of linezolid as a component of drug‐resistant TB treatment regimens., Linezolid for managing people with drug‐resistant tuberculosis What is drug‐resistant tuberculosis, and how might linezolid work? Tuberculosis is caused by infection with Mycobacterium tuberculosis bacteria. When there are symptoms or signs of illness, this is called active tuberculosis. An estimated one‐third of the world's population are infected with tuberculosis, and around 1.4 million people died from active tuberculosis in 2015. Bacteria that cause tuberculosis can develop resistance to the drugs most commonly used to treat tuberculosis, also called first‐line antibiotics. This is an increasing problem that makes treatment more difficult, because second‐line tuberculosis treatment drugs are less powerful against the bacteria, and more likely to cause harmful effects. Standard treatment for drug‐resistant tuberculosis requires patients to take multiple antibiotics for nearly two years. Linezolid is a second‐line drug that laboratory studies have found to be good at killing bacteria that cause tuberculosis, but that can also cause frequent, serious harmful effects. The review question Recent international guidelines recommend trying to include linezolid in the treatment of all patients with multi‐drug resistant tuberculosis, but there is concern about whether enough good evidence exists to tell us how well it works, what dose is best, and how safe it is for people who take it. Study characteristics We searched for evidence up to 13 July 2018. We analysed data from two trials, one of which randomly allocated 65 people with drug‐resistant tuberculosis to either a linezolid‐containing or linezolid‐free drug combination, and another that randomly allocated 39 participants to receive linezolid as part of their treatment from the start or have it added after a delay of two months. We also included 14 studies, including 1678 people, in which some participants received linezolid but others did not, but this was not determined at random. What are the main results of the review? One trial showed a higher likelihood of cure and lower risk of treatment failure in participants receiving linezolid compared to those who did not. The second trial showed that participants who received linezolid immediately had a higher chance of tuberculosis being cleared from their sputum four months after the start of the study than those who added linezolid after a two‐month delay. When they examined safety, the first trial found a higher risk of developing low red blood cell counts, nausea and vomiting, and nerve damage in people receiving linezolid. From 11 of the non‐randomized studies that reported this, 22.6% of people had to stop linezolid due to adverse effects (side effects), though further comparisons of harmful effects were not possible due to incomplete reporting in the non‐randomized studies. Overall, although there is some evidence of benefit, we have very low certainty in its accuracy. More high‐quality studies are required before we can be certain how effective and safe linezolid is for drug‐resistant tuberculosis. How up‐to‐date is this review? This review is current up to 13 July 2018.

Published

2019

19. Linezolid for drug-resistant tuberculosis

Author

Derek J. Sloan, Bhagteshwar Singh, Hannah Ryan, and Derek Cocker

Subjects

0301 basic medicine, Medicine General & Introductory Medical Sciences, medicine.medical_specialty, business.industry, Drug resistant tuberculosis, 030106 microbiology, qv_38, 3. Good health, qw_45, wb_102, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, 030228 respiratory system, chemistry, Internal medicine, Linezolid, Immunology, qv_268, medicine, wf_360, Pharmacology (medical), wf_200, business

Abstract

This is a protocol for a Cochrane Review (Intervention). The objectives are as follows:\ud \ud To assess the efficacy of linezolid when used as part of a second-line regimen for treating people with multidrug-resistant (MDR-) and extensively drug-resistant (XDR-) pulmonary tuberculosis (TB), and to assess the prevalence and severity of adverse events associated with linezolid use in this patient group

Published

2017

20. Fatal oxidative haemolysis and methaemoglobinaemia in a patient with alkaptonuria and acute kidney injury

Author

Adam Mullan, Lakshminarayan Ranganath, Derek Cocker, Gordon Taylor, and Colin G M Millar

Subjects

Pathology, medicine.medical_specialty, Methemoglobinemia, oxidative haemolysis, Gastroenterology, Alkaptonuria, chemistry.chemical_compound, Rare Diseases, Internal medicine, Arthropathy, methaemoglobinaemia, Medicine, Homogentisic acid, alkaptonuria, Transplantation, business.industry, Acute kidney injury, homogentisic acid, medicine.disease, Haemolysis, Ascorbic acid, acute kidney injury, chemistry, Nephrology, Contents, business, Kidney disease

Abstract

Alkaptonuria (AKU) is a rare inherited disorder of tyrosine metabolism, which leads to an accumulation of homogentisic acid (HGA) and is associated with a progressive arthropathy. Fatal complications are unusual and usually result from cardiac disease or progressive renal impairment; rapidly fatal haematological complications are exceptionally rare and described in only a handful of case reports. This case involves a 63-year-old male with AKU and modest chronic kidney disease who developed rapidly fatal haemolysis and methaemoglobinuria following an episode of acute kidney injury triggered by an obstructing ureteric calculus and urosepsis. The patient succumbed despite aggressive antioxidant therapy with ascorbic acid and n-acetyl cysteine. A rapid build-up of HGA due to reduced renal clearance, triggering oxidative haemolysis and methaemoglobinuria is proposed as the mechanism. Alternative strategies to consider when conventional antioxidants fail are discussed including the potent inhibitor of HGA production, nitisonone.

Published

2014

21. Fahr's disease: a rare neurological presentation in a tropical setting

Author

Jude Chinedu Anikwe, Akaninyene Otu, and Derek Cocker

Subjects

Pediatrics, medicine.medical_specialty, Levodopa, Movement disorders, business.industry, Fahr's disease, Nigeria, Case Reports, General Medicine, Disease, medicine.disease, Bioinformatics, calcification, Basal ganglia, medicine, Differential diagnosis, Presentation (obstetrics), medicine.symptom, business, seizures, Calcification, medicine.drug

Abstract

Key Clinical Message While rare, Fahr's disease should be considered as a differential diagnosis for seizures, movement disorders, or cognitive impairment in tropical settings. Classically, bilateral calcification of the basal ganglia is seen on CT. Endemic infections, metabolic, and toxic causes should be excluded. Treatment using Levodopa is often beneficial.

Published

2015

22. On-going lessons in fluid prescription: assessment of adherence to weight-based intravenous fluid prescribing in medical inpatients

Author

Derek J. Sloan, Derek Cocker, Eileen Marks, Ffion Carlin, and Michael Beadsworth

Subjects

Adult, Pediatrics, medicine.medical_specialty, Teaching hospital, Nice guidance, Intravenous fluid, Medicine, Humans, Prospective Studies, Medical prescription, Letters to the Editor, Infusions, Intravenous, Aged, Aged, 80 and over, Inpatients, Errata, business.industry, Guideline adherence, General Medicine, Middle Aged, Original data, Prescriptions, Family medicine, Fluid Therapy, Guideline Adherence, business, Weight based dosing, Fluid volume, Algorithms

Abstract

Letters not directly related to articles published in Clinical Medicine and presenting unpublished original data should be submitted for publication in this section. Clinical and scientific letters should not exceed 500 words and may include one table and up to five references. Introduction Attention to detail in the prescription of intravenous (IV) fluids for medical and surgical inpatients is often less rigorous than for other drugs, with errors in fluid volume, composition and rate being commonplace.1–2 As part of a review of fluid prescribing and fluid balance we introduced a weight-based fluid prescribing policy, in a large adult teaching hospital. Including algorithms, this largely mirrors the recent NICE guidance (2014).1 Medical inpatients were prospectively assessed for adherence to local and subsequent national guidance, over four consecutive time points (May 2010, Spetember 2010, February 2013 and August 2014). Tailored education and campaigns were introduced. We report our findings, highlighting the ongoing problems in fluid prescribing.

Published

2015

23. Indolizidine derivatives as potential substance P antagonists

Author

H. Geoffrey Davies, Andrea Gore, J Derek Cocker, Richard H Green, and Chuen Chan

Subjects

Substance p antagonist, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Indolizidine, Substance P, Biological activity, Biochemistry, chemistry.chemical_compound, chemistry, Drug Discovery, Molecular Medicine, Molecular Biology

Abstract

Two novel indolizidine analogues, (7a) and (7b), of the substance P antagonist CP 99,994 have been prepared. Possible conformational factors for their low biological activity are discussed.

Published

1996

24. Clinical and scientific letters: On-going lessons in fluid prescription: assessment of adherence to weight-based intravenous fluid prescribing in medical inpatients

Author

Derek Cocker, Ffion Carlin, Michael Beadsworth, Eileen Marks, and Derek J. Sloan

Subjects

medicine.medical_specialty, Intravenous fluid, business.industry, Family medicine, medicine, Alternative medicine, General Medicine, Medical prescription, business, Weight based dosing, Spelling

Abstract

Clinical Medicine 2015;15;503–4 Derek Sloan’s name was submitted with incorrect spelling. The correct spelling is printed above

Published

2016

25. Lemierre’s disease: a case with bilateral iliopsoas abscesses and a literature review

Author

Martin Brett, Derek Cocker, Paul Cullis, Ben Challoner, Richard Schofield, Alastair Hayes, and Nicholas Te Bird

Subjects

medicine.medical_specialty, Fusobacterium Necrophorum, ved/biology.organism_classification_rank.species, Context (language use), Lemierre, Disease, Review, Sepsis, Fusobacterium necrophorum, medicine, biology, ved/biology, business.industry, Acute kidney injury, Clinical literature, Fusobacterium, Bilateral, medicine.disease, biology.organism_classification, Iliopsoas abscess, Surgery, Emergency Medicine, Psoas abscesses, business

Abstract

Lemierre’s disease is characterized by sepsis, often with an oropharyngeal source, secondary septic emboli and internal jugular vein thrombosis (Lancet 1:701–3, 1936. Clin Microbiol Rev 20(4):622–59, 2007). Septic emboli affecting many bodily sites have been reported, including the lungs, joints, bones, and brain. The case report describes an unusual case of Lemierre’s disease in a 64 year old gentleman causing profound sepsis, acute kidney injury, bilateral iliopsoas abscesses and a right hand abscess. To our knowledge, this is the first reported case of Lemierre’s disease in the context of bilateral psoas abscesses, and highlights the ambiguity surrounding the definition of Lemierre’s disease. The clinical literature review highlights the difficulty in definitively diagnosing the condition and offers some suggestions for recognising and refining the diagnostic criterion of Lemierre’s.

Published

2014

26. Relevance of photochemical transformations to the laboratory synthesis of biologically interesting molecules

Author

StanleyM. Roberts and J. Derek Cocker

Subjects

Chemistry, General Chemical Engineering, General Physics and Astronomy, Molecule, Relevance (information retrieval), General Chemistry, Photochemistry, Combinatorial chemistry

Published

1984

27. Relevance of photochemical transformations to the laboratory synthesis of biologically interesting molecules

Author

Derek Cocker, J., primary and Roberts, StanleyM., additional

Published

1984