Literature DB >> 30542533

Novel tricyclic glycal-based TRIB1 inducers that reprogram LDL metabolism in hepatic cells.

Marek M Nagiec1, Jeremy R Duvall1, Adam P Skepner1, Eleanor A Howe1, Jessica Bastien1, Eamon Comer1, Jean-Charles Marie1, Stephen E Johnston1, Joseph Negri1, Michelle Eichhorn1, Julien Vantourout1, Clary Clish2, Kiran Musunuru3, Michael Foley1, Jose R Perez1, Michelle A J Palmer1.   

Abstract

Increased expression of the Tribbles pseudokinase 1 gene (TRIB1) is associated with lower plasma levels of LDL cholesterol and triglycerides, higher levels of HDL cholesterol and decreased risk of coronary artery disease and myocardial infarction. We identified a class of tricyclic glycal core-based compounds that upregulate TRIB1 expression in human HepG2 cells and phenocopy the effects of genetic TRIB1 overexpression as they inhibit expression of triglyceride synthesis genes and ApoB secretion in cells. In addition to predicted effects related to downregulation of VLDL assembly and secretion these compounds also have unexpected effects as they upregulate expression of LDLR and stimulate LDL uptake. This activity profile is unique and favorably differs from profiles produced by statins or other lipoprotein targeting therapies. BRD8518, the initial lead compound from the tricyclic glycal class, exhibited stereochemically dependent activity and the potency far exceeding previously described benzofuran BRD0418. Gene expression profiling of cells treated with BRD8518 demonstrated the anticipated changes in lipid metabolic genes and revealed a broad stimulation of early response genes. Consistently, we found that BRD8518 activity is MEK1/2 dependent and the treatment of HepG2 cells with BRD8518 stimulates ERK1/2 phosphorylation. In agreement with down-regulation of genes controlling triglyceride synthesis and assembly of lipoprotein particles, the mass spectrometry analysis of cell extracts showed reduced rate of incorporation of stable isotope labeled glycerol into triglycerides in BRD8518 treated cells. Furthermore, we describe medicinal chemistry efforts that led to identification of BRD8518 analogs with enhanced potency and pharmacokinetic properties suitable for in vivo studies.

Entities:  

Year:  2018        PMID: 30542533      PMCID: PMC6247893          DOI: 10.1039/c8md00297e

Source DB:  PubMed          Journal:  Medchemcomm        ISSN: 2040-2503            Impact factor:   3.597


  22 in total

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2.  Activation of LDL receptor gene expression in HepG2 cells by hepatocyte growth factor.

Authors:  Y K Pak; M P Kanuck; D Berrios; M R Briggs; A D Cooper; J L Ellsworth
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4.  TRIB1 downregulates hepatic lipogenesis and glycogenesis via multiple molecular interactions.

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Journal:  J Mol Endocrinol       Date:  2014-02-24       Impact factor: 5.098

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8.  Multi-ethnic analysis of lipid-associated loci: the NHLBI CARe project.

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Journal:  PLoS One       Date:  2012-05-21       Impact factor: 3.240

9.  A method for high-throughput gene expression signature analysis.

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Journal:  Genome Biol       Date:  2006       Impact factor: 13.583

10.  Modulators of hepatic lipoprotein metabolism identified in a search for small-molecule inducers of tribbles pseudokinase 1 expression.

Authors:  Marek M Nagiec; Adam P Skepner; Joseph Negri; Michelle Eichhorn; Nicolas Kuperwasser; Eamon Comer; Giovanni Muncipinto; Aravind Subramanian; Clary Clish; Kiran Musunuru; Jeremy R Duvall; Michael Foley; Jose R Perez; Michelle A J Palmer
Journal:  PLoS One       Date:  2015-03-26       Impact factor: 3.240

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Journal:  Bioorg Med Chem Lett       Date:  2019-06-12       Impact factor: 2.823

2.  From methylene bridged diindole to carbonyl linked benzimidazoleindole: Development of potent and metabolically stable PCSK9 modulators.

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