Activities of Mutant Prevention Concentration-Targeted Moxifloxacin and Levofloxacin against Streptococcus pneumoniae in an In Vitro Pharmacodynamic Model

doi:10.1128/AAC.47.8.2606-2614.2003

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Antimicrobial Agents and Chemotherapy, August 2003, p. 2606-2614, Vol. 47, No. 8
0066-4804/03/$08.00+0 DOI: 10.1128/AAC.47.8.2606-2614.2003
Copyright © 2003, American Society for Microbiology. All Rights Reserved.

Activities of Mutant Prevention Concentration-Targeted Moxifloxacin and Levofloxacin against Streptococcus pneumoniae in an In Vitro Pharmacodynamic Model

George P. Allen,¹^,2^, Glenn W. Kaatz,¹^,3^,4 and Michael J. Rybak¹^,2^,3^*

Anti-Infective Research Laboratory, Department of Pharmacy Practice, Eugene Applebaum College of Pharmacy and Health Sciences,¹ School of Medicine, Wayne State University,³ Detroit Receiving Hospital and University Health Center,² the John D. Dingell VA Medical Center, Detroit, Michigan 48201⁴

Received 11 June 2002/ Returned for modification 8 February 2003/ Accepted 10 May 2003

The differential effects of moxifloxacin and levofloxacin onthe development of resistance in four Streptococcus pneumoniaeisolates were examined by using an in vitro pharmacodynamicmodel. Therapeutic regimens (moxifloxacin: peak, 4.5 µg/ml;half-life [t_1/2], 12 h; and levofloxacin: peak, 6 µg/ml;t_1/2, 6 h) were tested against two fluoroquinolone-susceptibleisolates (strains 79 and ATCC 49619) and KD2138 and KD2139 (parCand gyrA mutants, respectively, of ATCC 49619). Mutant preventionconcentration (MPC)-targeted regimens with modified pharmacokineticsof each drug were simulated to match the area under the concentration-timecurve (AUC) above the MPC for the two fluoroquinolones. MoxifloxacinMICs and MPCs (MIC/MPC) for isolates 79, ATCC 49619, KD2138,and KD2139, respectively, were 0.125 and 0.5, 0.125 and 0.5,0.25 and 8, and 0.25 and 4 µg/ml. Levofloxacin MICs andMPCs for the same isolates were 1 and 4, 0.5 and 2, 1 and 64,and 0.5 and 32 µg/ml, respectively. Therapeutic levofloxacinconcentrations led to isolation of mutants of ATCC 49619 (S79Yin ParC), KD2138 (S81Y in GyrA), and KD2139 (S79Y in ParC).Therapeutic moxifloxacin concentrations against the gyrA mutantKD2139 resulted in outgrowth of a mutant with a ParC substitution(S79Y) but caused no emergence of mutants of the other threeisolates. MPC-targeted moxifloxacin (lower-than-normal peak= 0.75 to 1.5 µg/ml, administered at levofloxacin's t_1/2)caused growth of a GyrA variant (S81Y) of KD2138 and a ParCvariant (S79Y) of KD2139, while no mutants of ATCC 49619 wererecovered. MPC-targeted levofloxacin (higher-than-normal peak= 14.5 to 29.5 µg/ml, administered at moxifloxacin's t_1/2)against KD2138 and KD2139 did not prevent the development ofthe mutations observed in therapeutic regimens, but resistancein the fluoroquinolone-susceptible ATCC 49619 was no longernoted. Normalization of the respective AUC/MPC ratios of moxifloxacinand levofloxacin did not eliminate differences in resistanceselectivity of the two agents in all cases. We conclude thatthe reduced recovery of resistant mutants of S. pneumoniae followingmoxifloxacin exposure compared to levofloxacin may be due tointrinsic differences between the drugs. Increasing the concentrationand exposure (t_1/2) to exceed the MPC may prevent mutationsfrom occurring in fluoroquinolone-susceptible strains. However,this strategy did not prevent the selection of secondary mutantsin strains with preexisting mutations. Further study of theMPC concept to evaluate these relationships is warranted.

* Corresponding author. Mailing address: Anti-Infective Research Laboratory, Eugene Applebaum College of Pharmacy and Health Sciences, Wayne State University, Detroit, MI 48201. Phone: (313) 577-4376. Fax: (313) 577-8915. E-mail: m.rybak{at}wayne.edu.

Present address: Oregon State University College of Pharmacyat OHSU, Portland, OR 97239-3098.

Antimicrobial Agents and Chemotherapy, August 2003, p. 2606-2614, Vol. 47, No. 8
0066-4804/03/$08.00+0 DOI: 10.1128/AAC.47.8.2606-2614.2003
Copyright © 2003, American Society for Microbiology. All Rights Reserved.

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