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Antiviral Agents

Influenza Viral Load and Peramivir Kinetics after Single Administration and Proposal of Regimens for Peramivir Administration against Resistant Variants

Masatoki Sato, Masaki Ito, Shigeo Suzuki, Hiroko Sakuma, Aya Takeyama, Shinichi Oda, Masahiro Watanabe, Koichi Hashimoto, Kyohei Miyazaki, Yukihiko Kawasaki, Mitsuaki Hosoya
Masatoki Sato
Department of Pediatrics, Fukushima Medical University, Fukushima, Japan
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Masaki Ito
Department of Pediatrics, Soma General Hospital, Soma, Japan
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Shigeo Suzuki
Department of Pediatrics, Ohara General Hospital, Fukushima, Japan
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Hiroko Sakuma
Department of Pediatrics, Hoshi General Hospital, Koriyama, Japan
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Aya Takeyama
Department of Pediatrics, Soma General Hospital, Soma, Japan
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Shinichi Oda
Department of Pediatrics, Iwase Hospital, Sukagawa, Japan
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Masahiro Watanabe
Department of Pediatrics, South Aizu Hospital, Minami-aizu, Japan
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Koichi Hashimoto
Department of Pediatrics, Fukushima Medical University, Fukushima, Japan
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Kyohei Miyazaki
Department of Pediatrics, Fukushima Medical University, Fukushima, Japan
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Yukihiko Kawasaki
Department of Pediatrics, Fukushima Medical University, Fukushima, Japan
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Mitsuaki Hosoya
Department of Pediatrics, Fukushima Medical University, Fukushima, Japan
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DOI: 10.1128/AAC.04263-14
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ABSTRACT

We estimated the efficacy of the current single administration of peramivir on the basis of peramivir pharmacokinetics in the upper respiratory tract (URT) and determined the predictive peramivir concentration-time curve to assess its efficacy against viruses with decreased susceptibility to neuraminidase inhibitors. Serum, nasal swab, or aspiration samples were collected from 28 patients treated with 10 mg/kg body weight peramivir. The sequential influenza viral RNA load and susceptibility after peramivir administration were measured using a quantitative real-time reverse transcription-PCR and neuraminidase inhibition assay. The peramivir concentrations in the serum and URT after a single administration at 10 mg/kg were measured, and the predictive blood and URT peramivir concentration-time curves were determined to assess various administration regimens against resistant variants. The peramivir concentration decreased to <0.1% of the maximum concentration of drug in serum (Cmax) at 24 h after administration. Rapid elimination of peramivir from the URT by 48 h after administration may contribute to an increase in the influenza A viral load after day 3 but not to a decrease in the influenza B viral load, despite the absence of a decrease in the susceptibility to peramivir. A longer maintenance of a high level of peramivir in the URT is expected by divided administration rather than once-daily administration. When no clinical improvement is observed in patients with normal susceptibility influenza A and B, peramivir readministration should be considered. In severe cases caused by resistant variants, better inhibitory effectiveness and less frequent adverse events are expected by divided administration rather than once-daily administration with an increased dosage.

FOOTNOTES

    • Received 10 September 2014.
    • Returned for modification 6 December 2014.
    • Accepted 26 December 2014.
    • Accepted manuscript posted online 29 December 2014.
  • Supplemental material for this article may be found at http://dx.doi.org/10.1128/AAC.04263-14.

  • Copyright © 2015, American Society for Microbiology. All Rights Reserved.
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Influenza Viral Load and Peramivir Kinetics after Single Administration and Proposal of Regimens for Peramivir Administration against Resistant Variants
Masatoki Sato, Masaki Ito, Shigeo Suzuki, Hiroko Sakuma, Aya Takeyama, Shinichi Oda, Masahiro Watanabe, Koichi Hashimoto, Kyohei Miyazaki, Yukihiko Kawasaki, Mitsuaki Hosoya
Antimicrobial Agents and Chemotherapy Feb 2015, 59 (3) 1643-1649; DOI: 10.1128/AAC.04263-14

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Influenza Viral Load and Peramivir Kinetics after Single Administration and Proposal of Regimens for Peramivir Administration against Resistant Variants
Masatoki Sato, Masaki Ito, Shigeo Suzuki, Hiroko Sakuma, Aya Takeyama, Shinichi Oda, Masahiro Watanabe, Koichi Hashimoto, Kyohei Miyazaki, Yukihiko Kawasaki, Mitsuaki Hosoya
Antimicrobial Agents and Chemotherapy Feb 2015, 59 (3) 1643-1649; DOI: 10.1128/AAC.04263-14
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