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Dive into the research topics where Manuel A. Navia is active.

Publication


Featured researches published by Manuel A. Navia.


Journal of Pharmacology and Experimental Therapeutics | 2011

Pharmacologic inhibition of ghrelin receptor signaling is insulin sparing and promotes insulin sensitivity

Kenneth A. Longo; Elizabeth Govek; Anna Nolan; Thomas McDonagh; Soratree Charoenthongtrakul; Derek J. Giuliana; Kristen Morgan; Jeffrey Hixon; Chaoseng Zhou; Bruce Kelder; John J. Kopchick; Jeffrey O. Saunders; Manuel A. Navia; Rory Curtis; Peter S. DiStefano; Bradley Geddes

Ghrelin influences a variety of metabolic functions through a direct action at its receptor, the GhrR (GhrR-1a). Ghrelin knockout (KO) and GhrR KO mice are resistant to the negative effects of high-fat diet (HFD) feeding. We have generated several classes of small-molecule GhrR antagonists and evaluated whether pharmacologic blockade of ghrelin signaling can recapitulate the phenotype of ghrelin/GhrR KO mice. Antagonist treatment blocked ghrelin-induced and spontaneous food intake; however, the effects on spontaneous feeding were absent in GhrR KO mice, suggesting target-specific effects of the antagonists. Oral administration of antagonists to HFD-fed mice improved insulin sensitivity in both glucose tolerance and glycemic clamp tests. The insulin sensitivity observed was characterized by improved glucose disposal with dramatically decreased insulin secretion. It is noteworthy that these results mimic those obtained in similar tests of HFD-fed GhrR KO mice. HFD-fed mice treated for 56 days with antagonist experienced a transient decrease in food intake but a sustained body weight decrease resulting from decreased white adipose, but not lean tissue. They also had improved glucose disposal and a striking reduction in the amount of insulin needed to achieve this. These mice had reduced hepatic steatosis, improved liver function, and no evidence of systemic toxicity relative to controls. Furthermore, GhrR KO mice placed on low- or high-fat diets had lifespans similar to the wild type, emphasizing the long-term safety of ghrelin receptor blockade. We have therefore demonstrated that chronic pharmacologic blockade of the GhrR is an effective and safe strategy for treating metabolic syndrome.


Journal of Medicinal Chemistry | 2005

Discovery of Indoles as Potent and Selective Inhibitors of the Deacetylase SIRT1.

Andrew Napper; Jeffrey Hixon; Thomas McDonagh; Kenneth Keavey; Jean-Francois Pons; Jonathan Barker; Wei Tsung Yau; Patricia Amouzegh; Adam Flegg; Estelle Hamelin; Russell J. Thomas; Michael Kates; Stephen Jones; Manuel A. Navia; Jeffrey O. Saunders; Peter S. DiStefano; Rory Curtis


Archive | 2005

Anti-viral therapeutics

Peter S. DiStefano; Alan Watson; Rory Curtis; Bard J. Geesaman; L. Cannon; Manuel A. Navia


Archive | 2006

Sulfonamide compounds and uses thereof

Jeffrey O. Saunders; Thomas Stephen Coulter; Paul Mortenson; Manuel A. Navia; Jean-Francois Pons


Archive | 2005

Sulfonamides and uses thereof

Peter S. DiStefano; Andrew Napper; Rory Curtis; Jay Luly; Jean-Francois Pons; Russell J. Thomas; Manuel A. Navia; Thomas Stephen Coulter; Jeffrey O. Saunders; Bard J. Geesaman


Archive | 2005

Treating a viral disorder

Peter S. DiStefano; Alan Watson; L. Edward Cannon; Manuel A. Navia; Rory Curtis; Bard J. Geesaman


Archive | 2009

Compositions including clavulanic acid and related methods of use

Alan Watson; Manuel A. Navia


Archive | 2007

Ghrelin modulating compounds

Jeffrey O. Saunders; Thomas Stephen Coulter; Paul Mortenson; Manuel A. Navia; Jean-Francois Pons


Archive | 2006

Inhibiteurs de sirt qui se lient à nad

Manuel A. Navia; Jeffrey O. Saunders


Archive | 2005

Traitement d'un trouble d'origine virale

Peter S. DiStefano; Alan D. Watson; Manuel A. Navia; Rory Curtis; Bard J. Geesaman

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Dive into the Manuel A. Navia's collaboration.

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Andrew Napper

Fred Hutchinson Cancer Research Center

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Jean-Francois Pons

Centre national de la recherche scientifique

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Jeffrey Hixon

Fred Hutchinson Cancer Research Center

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Thomas McDonagh

Fred Hutchinson Cancer Research Center

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Bradley Geddes

Millennium Pharmaceuticals

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