School of Biomedical Sciences - Research Publications

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Author: Davies, Mark × End date: 2023 × Start date: 2020 × Type: Journal Article ×

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    The evolutionary mechanism of non-carbapenemase carbapenem-resistant phenotypes in Klebsiella spp
    Rosas, NC ; Wilksch, J ; Barber, J ; Li, J ; Wang, Y ; Sun, Z ; Rocker, A ; Webb, CT ; Perlaza-Jimenez, L ; Stubenrauch, CJ ; Dhanasekaran, V ; Song, J ; Taiaroa, G ; Davies, M ; Strugnell, RA ; Bao, Q ; Zhou, T ; McDonald, MJ ; Lithgow, T (eLIFE SCIENCES PUBL LTD, 2023-07-06)
    Antibiotic resistance is driven by selection, but the degree to which a bacterial strain's evolutionary history shapes the mechanism and strength of resistance remains an open question. Here, we reconstruct the genetic and evolutionary mechanisms of carbapenem resistance in a clinical isolate of Klebsiella quasipneumoniae. A combination of short- and long-read sequencing, machine learning, and genetic and enzymatic analyses established that this carbapenem-resistant strain carries no carbapenemase-encoding genes. Genetic reconstruction of the resistance phenotype confirmed that two distinct genetic loci are necessary in order for the strain to acquire carbapenem resistance. Experimental evolution of the carbapenem-resistant strains in growth conditions without the antibiotic revealed that both loci confer a significant cost and are readily lost by de novo mutations resulting in the rapid evolution of a carbapenem-sensitive phenotype. To explain how carbapenem resistance evolves via multiple, low-fitness single-locus intermediates, we hypothesised that one of these loci had previously conferred adaptation to another antibiotic. Fitness assays in a range of drug concentrations show how selection in the antibiotic ceftazidime can select for one gene (blaDHA-1) potentiating the evolution of carbapenem resistance by a single mutation in a second gene (ompK36). These results show how a patient's treatment history might shape the evolution of antibiotic resistance and could explain the genetic basis of carbapenem-resistance found in many enteric-pathogens.
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    Detection of Streptococcus pyogenes M1UK in Australia and characterization of the mutation driving enhanced expression of superantigen SpeA
    Davies, MRR ; Keller, N ; Brouwer, S ; Jespersen, MGG ; Cork, AJJ ; Hayes, AJ ; Pitt, MEE ; De Oliveira, DMP ; Harbison-Price, N ; Bertolla, OMM ; Mediati, DGG ; Curren, BFF ; Taiaroa, G ; Lacey, JAA ; Smith, HVV ; Fang, N-X ; Coin, LJM ; Stevens, K ; Tong, SYC ; Sanderson-Smith, M ; Tree, JJJ ; Irwin, ADD ; Grimwood, K ; Howden, BPP ; Jennison, AVV ; Walker, MJJ (NATURE PORTFOLIO, 2023-02-24)
    A new variant of Streptococcus pyogenes serotype M1 (designated 'M1UK') has been reported in the United Kingdom, linked with seasonal scarlet fever surges, marked increase in invasive infections, and exhibiting enhanced expression of the superantigen SpeA. The progenitor S. pyogenes 'M1global' and M1UK clones can be differentiated by 27 SNPs and 4 indels, yet the mechanism for speA upregulation is unknown. Here we investigate the previously unappreciated expansion of M1UK in Australia, now isolated from the majority of serious infections caused by serotype M1 S. pyogenes. M1UK sub-lineages circulating in Australia also contain a novel toxin repertoire associated with epidemic scarlet fever causing S. pyogenes in Asia. A single SNP in the 5' transcriptional leader sequence of the transfer-messenger RNA gene ssrA drives enhanced SpeA superantigen expression as a result of ssrA terminator read-through in the M1UK lineage. This represents a previously unappreciated mechanism of toxin expression and urges enhanced international surveillance.
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    Evaluating the role of asymptomatic throat carriage of Streptococcus pyogenes in impetigo transmission in remote Aboriginal communities in Northern Territory, Australia: a retrospective genomic analysis
    Lacey, JA ; Marcato, AJ ; Chisholm, RH ; Campbell, P ; Zachreson, C ; Price, DJ ; James, TB ; Morris, JM ; Gorrie, CL ; McDonald, M ; Bowen, AC ; Giffard, PM ; Holt, DC ; Currie, BJ ; Carapetis, JR ; Andrews, RM ; Davies, MR ; Geard, N ; McVernon, J ; Tong, SYC (ELSEVIER, 2023-07)
    BACKGROUND: Streptococcus pyogenes, or group A Streptococcus (GAS), infections contribute to a high burden of disease in Aboriginal Australians, causing skin infections and immune sequelae such as rheumatic heart disease. Controlling skin infections in these populations has proven difficult, with transmission dynamics being poorly understood. We aimed to identify the relative contributions of impetigo and asymptomatic throat carriage to GAS transmission. METHODS: In this genomic analysis, we retrospectively applied whole genome sequencing to GAS isolates that were collected as part of an impetigo surveillance longitudinal household survey conducted in three remote Aboriginal communities in the Northern Territory of Australia between Aug 6, 2003, and June 22, 2005. We included GAS isolates from all throats and impetigo lesions of people living in two of the previously studied communities. We classified isolates into genomic lineages based on pairwise shared core genomes of more than 99% with five or fewer single nucleotide polymorphisms. We used a household network analysis of epidemiologically and genomically linked lineages to quantify the transmission of GAS within and between households. FINDINGS: We included 320 GAS isolates in our analysis: 203 (63%) from asymptomatic throat swabs and 117 (37%) from impetigo lesions. Among 64 genomic lineages (encompassing 39 emm types) we identified 264 transmission links (involving 93% of isolates), for which the probable source was asymptomatic throat carriage in 166 (63%) and impetigo lesions in 98 (37%). Links originating from impetigo cases were more frequent between households than within households. Households were infected with GAS for a mean of 57 days (SD 39 days), and once cleared, reinfected 62 days (SD 40 days) later. Increased household size and community presence of GAS and scabies were associated with slower clearance of GAS. INTERPRETATION: In communities with high prevalence of endemic GAS-associated skin infection, asymptomatic throat carriage is a GAS reservoir. Public health interventions such as vaccination or community infection control programmes aimed at interrupting transmission of GAS might need to include consideration of asymptomatic throat carriage. FUNDING: Australian National Health and Medical Research Council.
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    Host-dependent resistance of Group A Streptococcus to sulfamethoxazole mediated by a horizontally-acquired reduced folate transporter
    Rodrigo, MKD ; Saiganesh, A ; Hayes, AJ ; Wilson, AM ; Anstey, J ; Pickering, JL ; Iwasaki, J ; Hillas, J ; Winslow, S ; Woodman, T ; Nitschke, P ; Lacey, JA ; Breese, KJ ; van der Linden, MPG ; Giffard, PM ; Tong, SYC ; Gray, N ; Stubbs, KA ; Carapetis, JR ; Bowen, AC ; Davies, MR ; Barnett, TC (NATURE PORTFOLIO, 2022-11-30)
    Described antimicrobial resistance mechanisms enable bacteria to avoid the direct effects of antibiotics and can be monitored by in vitro susceptibility testing and genetic methods. Here we describe a mechanism of sulfamethoxazole resistance that requires a host metabolite for activity. Using a combination of in vitro evolution and metabolic rescue experiments, we identify an energy-coupling factor (ECF) transporter S component gene (thfT) that enables Group A Streptococcus to acquire extracellular reduced folate compounds. ThfT likely expands the substrate specificity of an endogenous ECF transporter to acquire reduced folate compounds directly from the host, thereby bypassing the inhibition of folate biosynthesis by sulfamethoxazole. As such, ThfT is a functional equivalent of eukaryotic folate uptake pathways that confers very high levels of resistance to sulfamethoxazole, yet remains undetectable when Group A Streptococcus is grown in the absence of reduced folates. Our study highlights the need to understand how antibiotic susceptibility of pathogens might function during infections to identify additional mechanisms of resistance and reduce ineffective antibiotic use and treatment failures, which in turn further contribute to the spread of antimicrobial resistance genes amongst bacterial pathogens.