2021
DOI: 10.1038/s41467-021-23191-z
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A trimethoprim derivative impedes antibiotic resistance evolution

Abstract: The antibiotic trimethoprim (TMP) is used to treat a variety of Escherichia coli infections, but its efficacy is limited by the rapid emergence of TMP-resistant bacteria. Previous laboratory evolution experiments have identified resistance-conferring mutations in the gene encoding the TMP target, bacterial dihydrofolate reductase (DHFR), in particular mutation L28R. Here, we show that 4’-desmethyltrimethoprim (4’-DTMP) inhibits both DHFR and its L28R variant, and selects against the emergence of TMP-resistant … Show more

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Cited by 54 publications
(62 citation statements)
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“…The L28R mutation also shows improved compactness, inferred from its reduced bis-ANS binding ( Rodrigues et al, 2016 ). Thus, among the evolved mutant E. coli strains, L28R is one of the most frequently encountered resistance mutations in folA gene which render traditional anti-folate drugs like TMP clinically ineffective ( Manna et al, 2021 ; Rodrigues et al, 2016 ; Toprak et al, 2012 ). Effectively L28R serves as a stability ‘reservoir’ providing a gateway to multiple evolutionary trajectories leading to resistance.…”
Section: Discussionmentioning
confidence: 99%
“…The L28R mutation also shows improved compactness, inferred from its reduced bis-ANS binding ( Rodrigues et al, 2016 ). Thus, among the evolved mutant E. coli strains, L28R is one of the most frequently encountered resistance mutations in folA gene which render traditional anti-folate drugs like TMP clinically ineffective ( Manna et al, 2021 ; Rodrigues et al, 2016 ; Toprak et al, 2012 ). Effectively L28R serves as a stability ‘reservoir’ providing a gateway to multiple evolutionary trajectories leading to resistance.…”
Section: Discussionmentioning
confidence: 99%
“…Moreover, it confers mutations at a markedly slower rate as compared to TMP and hampers the development of resistant mutations. 42…”
Section: ′-Desmethyltrimethoprim (4′-dtmp)mentioning
confidence: 99%
“…Through phylogenic and sequence analysis, we identified two critical residue variations as a common structural element in trimethoprim-resistant DHFR, D27E and L28Q. The potential role of mutation to the acidic residue in TMP resistance has been considered in earlier work 22 25 Complementing biochemical and biophysical analysis defined how these substitutions mediate trimethoprim-resistance in DfrA1 and DfrA5 through effects on enzyme catalysis and ligand-cofactor cooperativity. These conclusions were supported by high-resolution structural data, paving the way for a design of next-generation broad-spectrum antifolates.…”
Section: Introductionmentioning
confidence: 98%