Human β-Defensin 1 and β-Defensin 3 (Mouse Ortholog mBD14) Function as Full Endogenous Agonists at Select Melanocortin Receptors

Mark D. Ericson,Anamika Singh,Srinivasa R. Tala,Erica M. Haslach,Marvin Dirain,Jay W. Schaub,Viktor Flores,Natalie Eick,Cody J. Lensing,Katie T. Freeman,Branden A. Smeester,Danielle N. Adank,Stacey L. Wilber,Robert C. Speth,Carrie Haskell-Luevano

Human β-Defensin 1 and β-Defensin 3 (Mouse Ortholog mBD14) Function as Full Endogenous Agonists at Select Melanocortin Receptors

2018

Mark D. Ericson
Anamika Singh
Srinivasa R. Tala
Erica M. Haslach
Marvin Dirain
Jay W. Schaub
Viktor Flores
Natalie Eick
Cody J. Lensing
Katie T. Freeman
Branden A. Smeester
Danielle N. Adank
Stacey L. Wilber
Robert C. Speth
Carrie Haskell-Luevano

β-Defensin 3 (BD3) was identified as a ligand for the melanocortin receptors (MCRs) in 2007, although the pharmacology activity of BD3 has not been clearly elucidated. Herein, it is demonstrated that human BD3 and mouse BD3 are full micromolar agonists at the MCRs. Furthermore, mouse β-defensin 1 (BD1) and human BD1 are also MCR micromolar agonists. This work identifies BD1 as an endogenous MCR ligand and clarifies the controversial role of BD3 as a micromolar agonist.

Keywords:

Agonist
Endogeny
Biochemistry
Defensin
Melanocortin
Receptor
Chemistry
Ligand

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