The scope of the antimicrobial resistance challenge
- PMID: 38797176
- DOI: 10.1016/S0140-6736(24)00876-6
The scope of the antimicrobial resistance challenge
Erratum in
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Department of Error.Lancet. 2024 Sep 14;404(10457):1018. doi: 10.1016/S0140-6736(24)01879-8. Lancet. 2024. PMID: 39277287 No abstract available.
Abstract
Each year, an estimated 7·7 million deaths are attributed to bacterial infections, of which 4.95 million are associated with drug-resistant pathogens, and 1·27 million are caused by bacterial pathogens resistant to the antibiotics available. Access to effective antibiotics when indicated prolongs life, reduces disability, reduces health-care expenses, and enables access to other life-saving medical innovations. Antimicrobial resistance undoes these benefits and is a major barrier to attainment of the Sustainable Development Goals, including targets for newborn survival, progress on healthy ageing, and alleviation of poverty. Adverse consequences from antimicrobial resistance are seen across the human life course in both health-care-associated and community-associated infections, as well as in animals and the food chain. The small set of effective antibiotics has narrowed, especially in resource-poor settings, and people who are very young, very old, and severely ill are particularly susceptible to resistant infections. This paper, the first in a Series on the challenge of antimicrobial resistance, considers the global scope of the problem and how it should be measured. Robust and actionable data are needed to drive changes and inform effective interventions to contain resistance. Surveillance must cover all geographical regions, minimise biases towards hospital-derived data, and include non-human niches.
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Conflict of interest statement
Declaration of interests A meeting held to coordinate this paper was supported by the Bill & Melinda Gates Foundation (BMGF; INV-055356 to RL) and the Africa Centres for Disease Control and Prevention (to all authors). Neither funder had any role in the design, writing, or decision to submit this paper for publication. RL has received grant funding from the US National Science Foundation (CCF1918628). INO is a Calestous Juma Science Leadership fellow supported by BMGF (INV-036234, as well as INV-067684, INV-048135, and OPP1210746); receives grant funding from the UK National Institute for Health and Care Research (project number NIHR133307), Wellcome Trust, Public Health Alliance for Genomic Epidemiology, SEQAFRICA, Grand Challenges Africa Award (GCA/DD/rnd3/021), and International Vaccine Institute Award; receives royalties from Oxford University Press, Cornell University Press, and Springer; receives consulting fees from the Wellcome Trust; has received payment for lectures from the UK Microbiology Society; received travel support from BMGF, the European Society for Clinical Microbiology and Infectious Disease, and the American Society for Microbiology; has or had paid leadership roles in BMGF's surveillance advisory group (2019–21), the Thomas Bassir Biomedical Foundation Nigeria (2019 to present), and The International Centre for Antimicrobial Resistance Solutions Technical Advisory Forum (2021 to present); and has other unpaid positions in the African Journal of Laboratory Medicine, Microbial Genomics, The Lancet Infectious Diseases, Nigeria Center for Disease Control, and the Lancet Commission for Nigeria. SB is a member of staff at WHO; the views presented in this Series paper are those of the authors and do not reflect those of WHO. ACG receives consulting fees from Aché, Eurofarma, and União Química; receives payment for lectures from bioMérieux, Eurofarma, MSD, Pfizer, and Sandoz; received travel support from MSD and Pfizer; participates on the data monitoring board of Aché, Eurofarma, Hypera Pharma, MSD, Pfizer, Roche, Sandoz, United Medical, União, and Química; is a member of the Scientific Advisory Committee of the Global Antibiotic Research and Development Partnership (GARDP), the Health 1 Area Coordination board, and Fundação de Amparo à Pesquisa do Estado de São Paulo; and is a researcher for the Brazilian National Council for Scientific and Technological Development. MS receives funding from the Wellcome Trust (222051/Z/20/Z), GARDP, and EDCTP (NeoSep1); has unpaid leadership positions on the WHO Essential Medicine List Antibiotics Working Group and GARDP; and has been the Chief Investigator of clinical trials in children, where generic antibiotics have been donated by Sandoz, InfectoPharm, and Shionogi. All other authors report no competing interests.
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