Prospective comparative study of efficacy and toxicity of netilmicin and amikacin

Bock, Bonnie V.; Edelstein, Paul H.; Meyer, Richard D.

doi:10.1128/aac.17.2.217

Cited by 50 publications

(15 citation statements)

References 26 publications

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“…However, if more than one high-dose level is employed and renal histopathology is examined, a comparatively less steep dose-response slope has been suggested for netilmicin (10,21). The safety advantage predicted by such high-dose comparisons in rats has not extrapolated to the lower doses used in clinics, in which the nephrotoxicity of netilmicin cannot be differentiated from other aminoglycosides (1,15,20,22). Such a lack of extrapolation from high to low doses might be a function of a flatter dose-response slope.…”

Section: Resultsmentioning

confidence: 99%

“…Despite the advantages predicted in high-dose comparisons in rats, appreciable nephrotoxicity has been observed with netilmicin in clinics (1,15,20,22) and in rats at low multiples of the human dose. In addition, the slope of the nephrotoxicity dose-response curve of netilmicin was flatter and not parallel with the slopes of gentamicin and amikacin, confiming the suggestions made at high doses.…”

Section: Resultsmentioning

confidence: 99%

“…The distribution of casts excreted in the urine after 2 weeks of dosing and the terminal gross observations corroborated the flatter dose-response slope of netilmicin. Nephrotoxicity advantages predicted by high-dose comparisons with netilmicin in rats are apparently a function of its less steep dose-response slope and therefore may have no relevance to lower doses.When large multiples of the human dose of netilmicin are administered to rats, the drug is less nephrotoxic than gentamicin (2, 7, 10, 11, 13, 21), tobramycin (10,16,21), and amikacin (10), but netilmicin has appreciable nephrotoxicity in humans and cannot be differentiated from other aminoglycosides in clinics (1,15,20,22). Highdose toxicity comparisons in animals may be inappropriate for extrapolations to lower doses unless the slopes of their respective dose-response curves are linear and parallel (9).…”

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confidence: 99%

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Nonparallel nephrotoxicity dose-response curves of aminoglycosides

Hottendorf¹,

Barnett²,

Gordon³

et al. 1981

Antimicrob Agents Chemother

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Nephrotoxicity comparisons of aminoglycosides in rats, utilizing large multiples of human doses, have indicated an advantage for netilmicin. However, no nephrotoxicity advantage of netilmicin has been demonstrated at the lower doses used in clinics. Some high-dose studies in rats have also suggested that the slope of the nephrotoxicity dose-response curve of netilmicin was less steep than the slopes of other aminoglycosides. Therefore, the slopes of the nephrotoxicity dose-response curves of gentamicin, amikacin, and netilmicin were compared in 200 rats at low multiples (one to five times) of human clinical doses. Histopathological evaluations of both kidneys from each rat revealed that netilmicin produced equivalent or greater nephrotoxicity as compared with gentamicin and amikacin and that the slope of the nephrotoxicity dose-response curve of netilmicin was approximately one-half as steep as the slopes of amikacin and gentamicin, which were parallel. The distribution of casts excreted in the urine after 2 weeks of dosing and the terminal gross observations corroborated the flatter dose-response slope of netilmicin. Nephrotoxicity advantages predicted by high-dose comparisons with netilmicin in rats are apparently a function of its less steep dose-response slope and therefore may have no relevance to lower doses.When large multiples of the human dose of netilmicin are administered to rats, the drug is less nephrotoxic than gentamicin (2, 7, 10, 11, 13, 21), tobramycin (10,16,21), and amikacin (10), but netilmicin has appreciable nephrotoxicity in humans and cannot be differentiated from other aminoglycosides in clinics (1,15,20,22). Highdose toxicity comparisons in animals may be inappropriate for extrapolations to lower doses unless the slopes of their respective dose-response curves are linear and parallel (9). Comparative nephrotoxicity results with netilmicin in rats have suggested a relatively flat dose response at high multiples of the human dose (10, 21), although these studies did not employ sufficient numbers of dose levels to describe a nephrotoxic dose-response curve. Utilizing the dose-response model recently described (5), the nephrotoxicity dose-response curves of netilmicin, gentamicin, and amikacin were compared in rats at low multiples of the human dose. ( (Charles River Breeding Laboratories, Inc.) weighing between 75 and 100 g upon arrival were acclimated for 14 days before the initiation of this study. The rats were housed in individual cages of appropriate type and size in an environmentally controlled room and were given Purina Laboratory Rodent Chow and fresh drinking water ad libitum. Subsequently, the animals were ranked by body weight and randomly divided into groups of 10 before being individually identified by a tag number attached to an ear.Aminoglycoside administration. The doses (based on activity) were split and administered subcutaneously to the rats twice a day at approximately 9 a.m. and 3 p.m. Because of the differences in therapeutic doses, the daily doses of each amino...

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

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Nonparallel nephrotoxicity dose-response curves of aminoglycosides

Hottendorf¹,

Barnett²,

Gordon³

et al. 1981

Antimicrob Agents Chemother

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“…Most studies consider ototoxicity to have occurred if at any time after a base-line audiogram has been obtained an increase occurs in the auditory threshold of 15 dB or more at any two frequencies (38,45,52,53,55,58,61,72) or 20 dB at one or more frequencies (5, 21,25,27). Some investigators consider a 15-dB or greater change at any frequency to represent ototoxicity (4, 29,40,50,76,[80][81][82][83]94), and others use some combination of criteria (10,32,33,66). The basis for accepting a 15-dB change in threshold as a meaningful change is that it is standard procedure to use 5-dB steps in sound intensity when obtaining auditory thresholds.…”

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confidence: 99%

Aminoglycoside-induced hearing loss in humans

Brummett

Fox

1989

Antimicrob Agents Chemother

160

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“…The development of new aminoglycosides followed a pattern aimed at identifying SAR that blocked susceptible sites for enzymatic modification on the molecule while retaining the acceptable safety profile of the earlier agents (9,17). While many new analogs were tested clinically (33,126,138), amikacin remains one of the most useful due to the relatively infrequent occurrence of resistance encountered (13,107). Amikacin use was often restricted in many hospitals in hopes of preventing the emergence of resistant strains, but its use for empiric therapy in combination with beta-lactams has been widely adopted in centers where resistance to the older aminoglycosides is common.…”

Section: Discovery Of Penicillin Gmentioning

confidence: 99%

Discovery and development of new antimicrobial agents

Gootz

1990

Clin Microbiol Rev

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The unprecedented growth in the number of new antibiotics over the past two decades has been the result of extensive research efforts that have exploited the growing body of knowledge describing the interactions of antibiotics with their targets in bacterial cells. Information gained from one class of antimicrobial agents has often been used to advance the development of other classes. In the case of beta-lactams, information on structure-activity relationships gleaned from penicillins and cephalosporins was rapidly applied to the cephamycins, monobactams, penems, and carbapenems in order to discover broad-spectrum agents with markedly improved potency. These efforts have led to the introduction of many new antibiotics that demonstrate outstanding clinical efficacy and improved pharmacokinetics in humans. The current review discusses those factors that have influenced the rapid proliferation of new antimicrobial agents, including the discovery of new lead structures from natural products and the impact of bacterial resistance development in the clinical setting. The development process for a new antibiotic is discussed in detail, from the stage of early safety testing in animals through phase I, II, and III clinical trials.

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Prospective comparative study of efficacy and toxicity of netilmicin and amikacin

Cited by 50 publications

References 26 publications

Nonparallel nephrotoxicity dose-response curves of aminoglycosides

Nonparallel nephrotoxicity dose-response curves of aminoglycosides

Aminoglycoside-induced hearing loss in humans

Discovery and development of new antimicrobial agents

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