Your search keyword '"Manzo RH"' showing total 4 results

1. Clomipramine and Benznidazole Act Synergistically and Ameliorate the Outcome of Experimental Chagas Disease.

Author

García MC, Ponce NE, Sanmarco LM, Manzo RH, Jimenez-Kairuz AF, and Aoki MP

Subjects

Animals, Chagas Disease parasitology, Disease Models, Animal, Drug Administration Schedule, Drug Combinations, Drug Synergism, Heart drug effects, Heart physiopathology, Male, Mice, Mice, Inbred BALB C, Parasitemia parasitology, Parasitic Sensitivity Tests, Treatment Outcome, Trypanosoma cruzi growth & development, Trypanosoma cruzi pathogenicity, Chagas Disease drug therapy, Clomipramine pharmacology, Nitroimidazoles pharmacology, Parasitemia drug therapy, Trypanocidal Agents pharmacology, Trypanosoma cruzi drug effects

Abstract

Chagas disease is an important public health problem in Latin America, and its treatment by chemotherapy with benznidazole (BZ) or nifurtimox remains unsatisfactory. In order to design new alternative strategies to improve the current etiological treatments, in the present work, we comprehensively evaluated the in vitro and in vivo anti-Trypanosoma cruzi effects of clomipramine (CMP) (a parasite-trypanothione reductase-specific inhibitor) combined with BZ. In vitro studies, carried out using a checkerboard technique on trypomastigotes (T. cruzi strain Tulahuen), revealed a combination index (CI) of 0.375, indicative of a synergistic effect of the drug combination. This result was correlated with the data obtained in infected BALB/c mice. We observed that during the acute phase (15 days postinfection [dpi]), BZ at 25 mg/kg of body weight/day alone decreased the levels of parasitemia compared with those of the control group, but when BZ was administered with CMP, the drug combination completely suppressed the parasitemia due to the observed synergistic effect. Furthermore, in the chronic phase (90 dpi), mice treated with both drugs showed less heart damage as assessed by the histopathological analysis, index of myocardial inflammation, and levels of heart injury biochemical markers than mice treated with BZ alone at the reference dose (100 mg/kg/day). Collectively, these data support the notion that CMP combined with low doses of BZ diminishes cardiac damage and inflammation during the chronic phase of cardiomyopathy. The synergistic activity of BZ-CMP clearly suggests a potential drug combination for Chagas disease treatment, which would allow a reduction of the effective dose of BZ and an increase in therapeutic safety., (Copyright © 2016, American Society for Microbiology. All Rights Reserved.)

Published

2016

2. Small-colony mutants of Staphylococcus aureus allow selection of gyrase-mediated resistance to dual-target fluoroquinolones.

Author

Pan XS, Hamlyn PJ, Talens-Visconti R, Alovero FL, Manzo RH, and Fisher LM

Subjects

Coagulase metabolism, DNA Gyrase biosynthesis, DNA Gyrase genetics, DNA Topoisomerase IV genetics, DNA Topoisomerase IV metabolism, Drug Resistance, Microbial, Hemin metabolism, Microbial Sensitivity Tests, Phenotype, Quinolones pharmacology, Staphylococcus aureus enzymology, Thymidine metabolism, Vitamin K 3 metabolism, Anti-Infective Agents pharmacology, DNA Gyrase metabolism, Fluoroquinolones, Mutation genetics, Staphylococcus aureus genetics

Abstract

Fluoroquinolones acting equally through DNA gyrase and topoisomerase IV in vivo are considered desirable in requiring two target mutations for emergence of resistant bacteria. To investigate this idea, we have studied the response of Staphylococcus aureus RN4220 to stepwise challenge with sparfloxacin, a known dual-target agent, and with NSFQ-105, a more potent sulfanilyl fluoroquinolone that behaves similarly. First-step mutants were obtained with both drugs but only at the MIC. These mutants exhibited distinctive small-colony phenotypes and two- to fourfold increases in MICs of NSFQ-105, sparfloxacin, and ciprofloxacin. No changes were detected in the quinolone resistance-determining regions of the gyrA, gyrB, grlA, or grlB gene. Quinolone-induced small-colony mutants shared the delayed coagulase response but not the requirement for menadione, hemin, or thymidine characteristic of small-colony variants, a subpopulation of S. aureus that is often defective in electron transport. Second-step mutants selected with NSFQ-105 had gyrA(S84L) alterations; those obtained with sparfloxacin carried a gyrA(D83A) mutation or a novel gyrB deletion (DeltaRKSAL, residues 405 to 409) affecting a trypsin-sensitive region linking functional domains of S. aureus GyrB. Each mutation was associated with four- to eightfold increases in MICs of NSFQ-105 and sparfloxacin, but not of ciprofloxacin, which we confirm targets topoisomerase IV. The presence of wild-type grlB-grlA gene sequences in second-step mutants excluded involvement of topoisomerase IV in the small-colony phenotype. Growth revertants retaining mutant gyrA or gyrB alleles were quinolone susceptible, indicating that resistance to NSFQ-105 and sparfloxacin was contingent on the small-colony mutation. We propose that small-colony mutations unbalance target sensitivities, perhaps through altered ATP or topoisomerase levels, such that gyrase becomes the primary drug target. Breaking of target parity by genetic or physiological means eliminates the need for two target mutations and provides a novel mechanism for stepwise selection of quinolone resistance.

Published

2002

3. Engineering the specificity of antibacterial fluoroquinolones: benzenesulfonamide modifications at C-7 of ciprofloxacin change its primary target in Streptococcus pneumoniae from topoisomerase IV to gyrase.

Author

Alovero FL, Pan XS, Morris JE, Manzo RH, and Fisher LM

Subjects

Anti-Infective Agents chemistry, Catalysis, Ciprofloxacin chemistry, DNA Gyrase, DNA Topoisomerase IV, DNA Topoisomerases, Type II genetics, DNA Topoisomerases, Type II metabolism, Drug Design, Drug Resistance, Microbial, Humans, Microbial Sensitivity Tests, Mutation, Quinolones pharmacology, Streptococcus pneumoniae enzymology, Topoisomerase II Inhibitors, Benzenesulfonamides, Anti-Infective Agents pharmacology, Ciprofloxacin pharmacology, Fluoroquinolones, Streptococcus pneumoniae drug effects, Sulfonamides chemistry

Abstract

We have examined the antipneumococcal mechanisms of a series of novel fluoroquinolones that are identical to ciprofloxacin except for the addition of a benzenesulfonylamido group to the C-7 piperazinyl ring. A number of these derivatives displayed enhanced activity against Streptococcus pneumoniae strain 7785, including compound NSFQ-105, bearing a 4-(4-aminophenylsulfonyl)-1-piperazinyl group at C-7, which exhibited an MIC of 0.06 to 0.125 microg/ml compared with a ciprofloxacin MIC of 1 microg/ml. Several complementary approaches established that unlike the case for ciprofloxacin (which targets topoisomerase IV), the increased potency of NSFQ-105 was associated with a target preference for gyrase: (i) parC mutants of strain 7785 that were resistant to ciprofloxacin remained susceptible to NSFQ-105, whereas by contrast, mutants bearing a quinolone resistance mutation in gyrA were four- to eightfold more resistant to NSFQ-105 (MIC of 0.5 microg/ml) but susceptible to ciprofloxacin; (ii) NSFQ-105 selected first-step gyrA mutants (MICs of 0.5 microg/ml) encoding Ser-81-to-Phe or -Tyr mutations, whereas ciprofloxacin selects parC mutants; and (iii) NSFQ-105 was at least eightfold more effective than ciprofloxacin at inhibiting DNA supercoiling by S. pneumoniae gyrase in vitro but was fourfold less active against topoisomerase IV. These data show unequivocally that the C-7 substituent determines not only the potency but also the target preference of fluoroquinolones. The importance of the C-7 substituent in drug-enzyme contacts demonstrated here supports one key postulate of the Shen model of quinolone action.

Published

2000

4. Mode of action of sulfanilyl fluoroquinolones.

Author

Alovero F, Nieto M, Mazzieri MR, Then R, and Manzo RH

Subjects

Anti-Infective Agents chemistry, Hydrogen-Ion Concentration, Microbial Sensitivity Tests, Quinolones chemistry, Structure-Activity Relationship, Anti-Infective Agents pharmacology, Escherichia coli drug effects, Fluoroquinolones, Quinolones pharmacology, Staphylococcus aureus drug effects

Abstract

The mode of action of sulfanilyl fluoroquinolones (NSFQs) was investigated with NSFQ-104, NSFQ-105, and some structurally related compounds. Evidence arising from interactions with p-aminobenzoic acid and trimethoprim suggested that a sulfonamidelike mechanism of action makes little or no contribution to the in vitro activity of NSFQs. NSFQ-105 showed an activity that inhibits gyrase-catalyzed DNA supercoiling that is similar to the activity of other fluoroquinolones. Also, NSFQ-105 uptake was decreased by the presence of Mg2+ and increased by a lower pH. These results indicate that NSFQs having only one ionizable group could exhibit more favorable kinetics of access to the bacterial cell than zwitterionic fluoroquinolones.

Published

1998