Selenoether oxytocin analogues have analgesic properties in a mouse model of chronic abdominal pain

Aline Dantas De Araujo; Mehdi Mobli; Joel Castro; Andrea M. Harrington; Irina Vetter; Zoltan Dekan; Markus Muttenthaler; Jing Jing Wan; Richard J. Lewis; Glenn F. King; Stuart M. Brierley; Paul F. Alewood

doi:10.1038/ncomms4165

Selenoether oxytocin analogues have analgesic properties in a mouse model of chronic abdominal pain

Aline Dantas De Araujo, Mehdi Mobli, Joel Castro, Andrea M. Harrington, Irina Vetter, Zoltan Dekan, Markus Muttenthaler, Jing Jing Wan, Richard J. Lewis, Glenn F. King, Stuart M. Brierley, Paul F. Alewood

Nutrition, Diabetes And Gut Health

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

92 Citations (Scopus)

Abstract

Poor oral availability and susceptibility to reduction and protease degradation is a major hurdle in peptide drug development. However, drugable receptors in the gut present an attractive niche for peptide therapeutics. Here we demonstrate, in a mouse model of chronic abdominal pain, that oxytocin receptors are significantly upregulated in nociceptors innervating the colon. Correspondingly, we develop chemical strategies to engineer non-reducible and therefore more stable oxytocin analogues. Chemoselective selenide macrocyclization yields stabilized analogues equipotent to native oxytocin. Ultra-high-field nuclear magnetic resonance structural analysis of native oxytocin and the seleno-oxytocin derivatives reveals that oxytocin has a pre-organized structure in solution, in marked contrast to earlier X-ray crystallography studies. Finally, we show that these seleno-oxytocin analogues potently inhibit colonic nociceptors both in vitro and in vivo in mice with chronic visceral hypersensitivity. Our findings have potentially important implications for clinical use of oxytocin analogues and disulphide-rich peptides in general.

Original language	English
Article number	3165
Journal	Nature Communications
Volume	5
DOIs	https://doi.org/10.1038/ncomms4165
Publication status	Published or Issued - 30 Jan 2014

ASJC Scopus subject areas

Chemistry(all)
Biochemistry, Genetics and Molecular Biology(all)
Physics and Astronomy(all)

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@article{4eabf365daa5405e8e90136240286036,

title = "Selenoether oxytocin analogues have analgesic properties in a mouse model of chronic abdominal pain",

abstract = "Poor oral availability and susceptibility to reduction and protease degradation is a major hurdle in peptide drug development. However, drugable receptors in the gut present an attractive niche for peptide therapeutics. Here we demonstrate, in a mouse model of chronic abdominal pain, that oxytocin receptors are significantly upregulated in nociceptors innervating the colon. Correspondingly, we develop chemical strategies to engineer non-reducible and therefore more stable oxytocin analogues. Chemoselective selenide macrocyclization yields stabilized analogues equipotent to native oxytocin. Ultra-high-field nuclear magnetic resonance structural analysis of native oxytocin and the seleno-oxytocin derivatives reveals that oxytocin has a pre-organized structure in solution, in marked contrast to earlier X-ray crystallography studies. Finally, we show that these seleno-oxytocin analogues potently inhibit colonic nociceptors both in vitro and in vivo in mice with chronic visceral hypersensitivity. Our findings have potentially important implications for clinical use of oxytocin analogues and disulphide-rich peptides in general.",

author = "{De Araujo}, {Aline Dantas} and Mehdi Mobli and Joel Castro and Harrington, {Andrea M.} and Irina Vetter and Zoltan Dekan and Markus Muttenthaler and Wan, {Jing Jing} and Lewis, {Richard J.} and King, {Glenn F.} and Brierley, {Stuart M.} and Alewood, {Paul F.}",

note = "Funding Information: This work was funded in part by the National Health and Medical Research Council of Australia (NHMRC) Project Grant no. 1063803 to P.F.A. and S.M.B. A.M.H received funding via the Australian Research Council Discovery Early Career Research Award. S.M.B received funding via an NHMRC R.D Wright Biomedical Research Fellowship.",

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doi = "10.1038/ncomms4165",

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AU - De Araujo, Aline Dantas

AU - Mobli, Mehdi

AU - Castro, Joel

AU - Harrington, Andrea M.

AU - Vetter, Irina

AU - Dekan, Zoltan

AU - Muttenthaler, Markus

AU - Wan, Jing Jing

AU - Lewis, Richard J.

AU - King, Glenn F.

AU - Brierley, Stuart M.

AU - Alewood, Paul F.

N1 - Funding Information: This work was funded in part by the National Health and Medical Research Council of Australia (NHMRC) Project Grant no. 1063803 to P.F.A. and S.M.B. A.M.H received funding via the Australian Research Council Discovery Early Career Research Award. S.M.B received funding via an NHMRC R.D Wright Biomedical Research Fellowship.

PY - 2014/1/30

Y1 - 2014/1/30

N2 - Poor oral availability and susceptibility to reduction and protease degradation is a major hurdle in peptide drug development. However, drugable receptors in the gut present an attractive niche for peptide therapeutics. Here we demonstrate, in a mouse model of chronic abdominal pain, that oxytocin receptors are significantly upregulated in nociceptors innervating the colon. Correspondingly, we develop chemical strategies to engineer non-reducible and therefore more stable oxytocin analogues. Chemoselective selenide macrocyclization yields stabilized analogues equipotent to native oxytocin. Ultra-high-field nuclear magnetic resonance structural analysis of native oxytocin and the seleno-oxytocin derivatives reveals that oxytocin has a pre-organized structure in solution, in marked contrast to earlier X-ray crystallography studies. Finally, we show that these seleno-oxytocin analogues potently inhibit colonic nociceptors both in vitro and in vivo in mice with chronic visceral hypersensitivity. Our findings have potentially important implications for clinical use of oxytocin analogues and disulphide-rich peptides in general.

AB - Poor oral availability and susceptibility to reduction and protease degradation is a major hurdle in peptide drug development. However, drugable receptors in the gut present an attractive niche for peptide therapeutics. Here we demonstrate, in a mouse model of chronic abdominal pain, that oxytocin receptors are significantly upregulated in nociceptors innervating the colon. Correspondingly, we develop chemical strategies to engineer non-reducible and therefore more stable oxytocin analogues. Chemoselective selenide macrocyclization yields stabilized analogues equipotent to native oxytocin. Ultra-high-field nuclear magnetic resonance structural analysis of native oxytocin and the seleno-oxytocin derivatives reveals that oxytocin has a pre-organized structure in solution, in marked contrast to earlier X-ray crystallography studies. Finally, we show that these seleno-oxytocin analogues potently inhibit colonic nociceptors both in vitro and in vivo in mice with chronic visceral hypersensitivity. Our findings have potentially important implications for clinical use of oxytocin analogues and disulphide-rich peptides in general.

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Selenoether oxytocin analogues have analgesic properties in a mouse model of chronic abdominal pain

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