2006
DOI: 10.1073/pnas.0600636103
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Upgrading antibiotic use within a class: Tradeoff between resistance and treatment success

Abstract: Increasing resistance to antibiotics creates the need for prudent antibiotic use. When resistance to various antibiotics within a class is driven by stepwise accumulation of mutations, a dilemma may exist in regard to replacing an antibiotic that is losing effectiveness due to resistance with a new drug within the same class. Such replacement may enhance treatment success in the short term but promote the spread of highly resistant strains. We used mathematical models to quantify the tradeoff between minimizin… Show more

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Cited by 48 publications
(43 citation statements)
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“…However, the unexpected lack of a significant fitness cost associated with carriage in CC30 SCCmecII isolates implies that there may be no barrier to their spread amongst CC22 SCCmecIV isolates. This lack of fitness cost associated with plasmid carriage has been previously noted in other bacteria (Andersson & Hughes, 2010;Bouma & Lenski, 1988;Helling et al, 1981;Lenski et al, 1994;Maisnier-Patin & Andersson, 2004;McDermott et al, 1993;Modi & Adams, 1991), but worryingly rarely influences clinical decisions nor the size of fitness costs in mathematical models of clinical MRSA populations (Bergstrom et al, 2004;D'Agata et al, 2007;Levin & Rozen, 2006;Wang & Lipsitch, 2006;Webb et al, 2005). It is likely that some level of co-evolution has occurred, with compensatory mutations allowing some isolates to cope better with the fitness cost than others.…”
Section: Discussionmentioning
confidence: 95%
“…However, the unexpected lack of a significant fitness cost associated with carriage in CC30 SCCmecII isolates implies that there may be no barrier to their spread amongst CC22 SCCmecIV isolates. This lack of fitness cost associated with plasmid carriage has been previously noted in other bacteria (Andersson & Hughes, 2010;Bouma & Lenski, 1988;Helling et al, 1981;Lenski et al, 1994;Maisnier-Patin & Andersson, 2004;McDermott et al, 1993;Modi & Adams, 1991), but worryingly rarely influences clinical decisions nor the size of fitness costs in mathematical models of clinical MRSA populations (Bergstrom et al, 2004;D'Agata et al, 2007;Levin & Rozen, 2006;Wang & Lipsitch, 2006;Webb et al, 2005). It is likely that some level of co-evolution has occurred, with compensatory mutations allowing some isolates to cope better with the fitness cost than others.…”
Section: Discussionmentioning
confidence: 95%
“…In vitro and in vivo studies and clinical trials have determined that maintenance of an unbound AUC/ MIC ratio of 30 to 40 maximizes the bactericidal efficacy of fluoroquinolones against S. pneumoniae and minimizes the selection of resistant isolates during therapy (2). Ciprofloxacin at doses used for therapy never achieves this target, levofloxacin at a dose of 500 mg once a day will just achieve it, and moxifloxacin and gatifloxacin used at recommended daily doses will achieve AUC/MIC ratios well above it (19,27,28). The inherent activity of levofloxacin, gatifloxacin, and moxifloxacin against pneumococci may thus minimize the emergence of resistance during therapy and, thus, the broader selection of resistance in a population (14).…”
Section: Discussionmentioning
confidence: 99%
“…There is concern that this change may enhance treatment success in the short term but promote the spread of highly resistant strains in the long term (28).…”
mentioning
confidence: 99%
“…Considering the widespread resistance problem and the propensity to intensify the effect of class-specific resistance mechanisms, most specialists would prefer a novel chemical class with no pre-existing potential cross-resistance [21]. Discovery …”
Section: Novel Molecules New Targetsmentioning
confidence: 99%