Identification and optimization of small-molecule agonists of the human relaxin hormone receptor RXFP1

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作者
Jingbo Xiao
Zaohua Huang
Catherine Z. Chen
Irina U. Agoulnik
Noel Southall
Xin Hu
Raisa E. Jones
Marc Ferrer
Wei Zheng
Alexander I. Agoulnik
Juan J. Marugan
机构
[1] NIH Chemical Genomics Center,Department of Human and Molecular Genetics
[2] Discovery Innovation,Department of Cellular Biology and Pharmacology
[3] National Center for Advancing Translational Sciences,undefined
[4] National Institutes of Health,undefined
[5] Herbert Wertheim College of Medicine,undefined
[6] Florida International University,undefined
[7] Herbert Wertheim College of Medicine,undefined
[8] Florida International University,undefined
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The anti-fibrotic, vasodilatory and pro-angiogenic therapeutic properties of recombinant relaxin peptide hormone have been investigated in several diseases, and recent clinical trial data has shown benefit in treating acute heart failure. However, the remodelling capacity of these peptide hormones is difficult to study in chronic settings because of their short half-life and the need for intravenous administration. Here we present the first small-molecule series of human relaxin/insulin-like family peptide receptor 1 agonists. These molecules display similar efficacy as the natural hormone in several functional assays. Mutagenesis studies indicate that the small molecules activate relaxin receptor through an allosteric site. These compounds have excellent physical and in vivo pharmacokinetic properties to support further investigation of relaxin biology and animal efficacy studies of the therapeutic benefits of relaxin/insulin-like family peptide receptor 1 activation.
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