Excretion of the Polymyxin Derivative NAB739 in Murine Urine

Extremely multiresistant strains of Enterobacteriaceae are emerging and spreading at a worrisome pace. Polymyxins are used as the last-resort therapy against such strains, in spite of their nephrotoxicity. We have previously shown that novel polymyxin derivatives NAB739 and NAB815 are less nephrotox...

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Vydáno v:Antibiotics (Basel) Ročník 9; číslo 4; s. 143
Hlavní autoři: Vaara, Martti, Vaara, Timo, Kuka, Janis, Sevostjanovs, Eduards, Grinberga, Solveiga, Dambrova, Maija, Liepinsh, Edgars
Médium: Journal Article
Jazyk:angličtina
Vydáno: Switzerland MDPI AG 27.03.2020
MDPI
Témata:
Calibration
Chemical properties
Composition
E coli
Excretion
extremely multiresistant strains of Enterobacteriaceae
Identification and classification
Kidneys
Linearity
Monkeys
mouse pyelonephritis
NAB739
Polymyxin B
Polymyxins
Pyelonephritis
Quality control
Urinary tract diseases
Urinary tract infections
Urine
Urogenital system
Finland
United Kingdom > UK
United States > US
Germany
mouse pyelonephritis
NAB739
extremely multiresistant strains of Enterobacteriaceae
polymyxin B
ISSN:2079-6382, 2079-6382
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Shrnutí:Extremely multiresistant strains of Enterobacteriaceae are emerging and spreading at a worrisome pace. Polymyxins are used as the last-resort therapy against such strains, in spite of their nephrotoxicity. We have previously shown that novel polymyxin derivatives NAB739 and NAB815 are less nephrotoxic in cynomolgus monkeys than polymyxin B and are therapeutic in murine Escherichia coli pyelonephritis at doses only one-tenth of that needed for polymyxin B. Here we evaluated whether the increased efficacy is due to increased excretion of NAB739 in urine. Mice were treated with NAB739 and polymyxin B four times subcutaneously at doses of 0.25, 0.5, 1, 2, and 4 mg/kg. In plasma, a clear dose–response relationship was observed. The linearity of Cmax with the dose was 0.9987 for NAB739 and 0.975 for polymyxin B. After administration of NAB739 at a dose of 0.25 mg/kg, its plasma concentrations at all tested time points were above 0.5 µg/mL while after administration at a dose of 0.5 mg/kg its plasma concentrations exceeded 1 µg/mL. The Cmax of NAB739 in plasma was up to 1.5-times higher after single (first) administration and up to two-times higher after the last administration when compared to polymyxin B. Polymyxin B was not detected in urine samples even when administered at 4 mg/kg. In contrast, the concentration of NAB739 in urine after single administration at a dose of 0.25 mg/kg was above 1 µg/mL and after administration of 0.5 mg/kg its average urine concentration exceeded 2 µg/mL. At the NAB739 dose of 4 mg/kg, the urinary concentrations were higher than 35 µg/mL. These differences explain our previous finding that NAB739 is much more efficacious than polymyxin B in the therapy of murine E. coli pyelonephritis.
Bibliografie:ObjectType-Article-1
SourceType-Scholarly Journals-1
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ISSN:2079-6382
2079-6382
DOI:10.3390/antibiotics9040143