Therapeutic potential of injectable nano-mupirocin liposomes for infections involving multidrug-resistant bacteria

Ahuva Cern; Yaelle Bavli; Atara Hod; Daniel Zilbersheid; Shazad Mushtaq; Ayelet Michael-Gayego; Dinorah Barasch; Yael Feinstein Rotkopf; Allon E. Moses; David M. Livermore; Yechezkel Barenholz

doi:10.3390/pharmaceutics13122186

Therapeutic potential of injectable nano-mupirocin liposomes for infections involving multidrug-resistant bacteria

Ahuva Cern, Yaelle Bavli, Atara Hod, Daniel Zilbersheid, Shazad Mushtaq, Ayelet Michael-Gayego, Dinorah Barasch, Yael Feinstein Rotkopf, Allon E. Moses, David M. Livermore, Yechezkel Barenholz^*

^*Corresponding author for this work

Department of Biochemistry and Molecular Biology

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Antibiotic resistance is a global health threat. There are a few antibiotics under development, and even fewer with new modes of action and no cross-resistance to established antibiotics. Accordingly, reformulation of old antibiotics to overcome resistance is attractive. Nano-mupirocin is a PEGylated nano-liposomal formulation of mupirocin, potentially enabling parenteral use in deep infections, as previously demonstrated in several animal models. Here, we describe extensive in vitro profiling of mupirocin and Nano-mupirocin and correlate the resulting MIC data with the pharmacokinetic profiles seen for Nano-mupirocin in a rat model. Nano-mupirocin showed no cross-resistance with other antibiotics and retained full activity against vancomycin-, daptomycin-, linezolid-and methicillinresistant Staphylococcus aureus, against vancomycin-resistant Enterococcus faecium, and cephalosporinresistant Neisseria gonorrhoeae. Following Nano-mupirocin injection to rats, plasma levels greatly exceeded relevant MICs for >24 h, and a biodistribution study in mice showed that mupirocin concentrations in vaginal secretions greatly exceeded the MIC₉₀ for N. gonorrhoeae (0.03 µg/mL) for >24 h. In summary, Nano-mupirocin has excellent potential for treatment of several infection types involving multiresistant bacteria. It has the concomitant benefits from utilizing an established antibiotic and liposomes of the same size and lipid composition as Doxil®, an anticancer drug product now used for the treatment of over 700,000 patients globally.

Original language	American English
Article number	2186
Journal	Pharmaceutics
Volume	13
Issue number	12
DOIs	https://doi.org/10.3390/pharmaceutics13122186
State	Published - Dec 2021

Bibliographical note

Funding Information:
Funding: The two years support of Integra Holdings (Israel) to this work that ended on Apr 2019 is acknowledged with pleasure. The work was also supported by the Barenholz Fund. The Barenholz fund was established by the Hebrew University of Jerusalem with a portion of YB Royalties from his Doxil and other inventions royalties to support research activities in the Barenholz Lab.

Publisher Copyright:
© 2021 by the authors. Licensee MDPI, Basel, Switzerland.

Keywords

Cross resistance
Injection
Multi-drug resistant bacteria
Mupirocin
Nano-liposomes
Neisseria gonorrhoeae
Pharmacokinetics
Vaginal distribution
Vancomycin-resistant E. faecium
cross resistance
mupirocin
vaginal distribution
nano-liposomes
multi-drug resistant bacteria
faecium
pharmacokinetics
vancomycin-resistant E
injection

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10.3390/pharmaceutics13122186

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title = "Therapeutic potential of injectable nano-mupirocin liposomes for infections involving multidrug-resistant bacteria",

abstract = "Antibiotic resistance is a global health threat. There are a few antibiotics under development, and even fewer with new modes of action and no cross-resistance to established antibiotics. Accordingly, reformulation of old antibiotics to overcome resistance is attractive. Nano-mupirocin is a PEGylated nano-liposomal formulation of mupirocin, potentially enabling parenteral use in deep infections, as previously demonstrated in several animal models. Here, we describe extensive in vitro profiling of mupirocin and Nano-mupirocin and correlate the resulting MIC data with the pharmacokinetic profiles seen for Nano-mupirocin in a rat model. Nano-mupirocin showed no cross-resistance with other antibiotics and retained full activity against vancomycin-, daptomycin-, linezolid-and methicillinresistant Staphylococcus aureus, against vancomycin-resistant Enterococcus faecium, and cephalosporinresistant Neisseria gonorrhoeae. Following Nano-mupirocin injection to rats, plasma levels greatly exceeded relevant MICs for >24 h, and a biodistribution study in mice showed that mupirocin concentrations in vaginal secretions greatly exceeded the MIC90 for N. gonorrhoeae (0.03 µg/mL) for >24 h. In summary, Nano-mupirocin has excellent potential for treatment of several infection types involving multiresistant bacteria. It has the concomitant benefits from utilizing an established antibiotic and liposomes of the same size and lipid composition as Doxil{\textregistered}, an anticancer drug product now used for the treatment of over 700,000 patients globally.",

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author = "Ahuva Cern and Yaelle Bavli and Atara Hod and Daniel Zilbersheid and Shazad Mushtaq and Ayelet Michael-Gayego and Dinorah Barasch and Rotkopf, {Yael Feinstein} and Moses, {Allon E.} and Livermore, {David M.} and Yechezkel Barenholz",

note = "Funding Information: Funding: The two years support of Integra Holdings (Israel) to this work that ended on Apr 2019 is acknowledged with pleasure. The work was also supported by the Barenholz Fund. The Barenholz fund was established by the Hebrew University of Jerusalem with a portion of YB Royalties from his Doxil and other inventions royalties to support research activities in the Barenholz Lab. Publisher Copyright: {\textcopyright} 2021 by the authors. Licensee MDPI, Basel, Switzerland.",

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doi = "10.3390/pharmaceutics13122186",

language = "American English",

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AU - Cern, Ahuva

AU - Bavli, Yaelle

AU - Hod, Atara

AU - Zilbersheid, Daniel

AU - Mushtaq, Shazad

AU - Michael-Gayego, Ayelet

AU - Barasch, Dinorah

AU - Rotkopf, Yael Feinstein

AU - Moses, Allon E.

AU - Livermore, David M.

AU - Barenholz, Yechezkel

N1 - Funding Information: Funding: The two years support of Integra Holdings (Israel) to this work that ended on Apr 2019 is acknowledged with pleasure. The work was also supported by the Barenholz Fund. The Barenholz fund was established by the Hebrew University of Jerusalem with a portion of YB Royalties from his Doxil and other inventions royalties to support research activities in the Barenholz Lab. Publisher Copyright: © 2021 by the authors. Licensee MDPI, Basel, Switzerland.

PY - 2021/12

Y1 - 2021/12

N2 - Antibiotic resistance is a global health threat. There are a few antibiotics under development, and even fewer with new modes of action and no cross-resistance to established antibiotics. Accordingly, reformulation of old antibiotics to overcome resistance is attractive. Nano-mupirocin is a PEGylated nano-liposomal formulation of mupirocin, potentially enabling parenteral use in deep infections, as previously demonstrated in several animal models. Here, we describe extensive in vitro profiling of mupirocin and Nano-mupirocin and correlate the resulting MIC data with the pharmacokinetic profiles seen for Nano-mupirocin in a rat model. Nano-mupirocin showed no cross-resistance with other antibiotics and retained full activity against vancomycin-, daptomycin-, linezolid-and methicillinresistant Staphylococcus aureus, against vancomycin-resistant Enterococcus faecium, and cephalosporinresistant Neisseria gonorrhoeae. Following Nano-mupirocin injection to rats, plasma levels greatly exceeded relevant MICs for >24 h, and a biodistribution study in mice showed that mupirocin concentrations in vaginal secretions greatly exceeded the MIC90 for N. gonorrhoeae (0.03 µg/mL) for >24 h. In summary, Nano-mupirocin has excellent potential for treatment of several infection types involving multiresistant bacteria. It has the concomitant benefits from utilizing an established antibiotic and liposomes of the same size and lipid composition as Doxil®, an anticancer drug product now used for the treatment of over 700,000 patients globally.

AB - Antibiotic resistance is a global health threat. There are a few antibiotics under development, and even fewer with new modes of action and no cross-resistance to established antibiotics. Accordingly, reformulation of old antibiotics to overcome resistance is attractive. Nano-mupirocin is a PEGylated nano-liposomal formulation of mupirocin, potentially enabling parenteral use in deep infections, as previously demonstrated in several animal models. Here, we describe extensive in vitro profiling of mupirocin and Nano-mupirocin and correlate the resulting MIC data with the pharmacokinetic profiles seen for Nano-mupirocin in a rat model. Nano-mupirocin showed no cross-resistance with other antibiotics and retained full activity against vancomycin-, daptomycin-, linezolid-and methicillinresistant Staphylococcus aureus, against vancomycin-resistant Enterococcus faecium, and cephalosporinresistant Neisseria gonorrhoeae. Following Nano-mupirocin injection to rats, plasma levels greatly exceeded relevant MICs for >24 h, and a biodistribution study in mice showed that mupirocin concentrations in vaginal secretions greatly exceeded the MIC90 for N. gonorrhoeae (0.03 µg/mL) for >24 h. In summary, Nano-mupirocin has excellent potential for treatment of several infection types involving multiresistant bacteria. It has the concomitant benefits from utilizing an established antibiotic and liposomes of the same size and lipid composition as Doxil®, an anticancer drug product now used for the treatment of over 700,000 patients globally.

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Therapeutic potential of injectable nano-mupirocin liposomes for infections involving multidrug-resistant bacteria

Abstract

Bibliographical note

Keywords

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