Literature DB >> 33390931

Synergetic Effect of rHDL and LXR Agonist on Reduction of Atherosclerosis in Mice.

Emily E Morin1, Yanhong Guo2, Hongliang He1, Wenmin Yuan1, Whitney N Souery1, Maria V Fawaz3, Yuqing Eugene Chen2, Anna Schwendeman1,4.   

Abstract

High-density lipoproteins (HDLs) are unique in that they play an important role in the reverse cholesterol transport process. However, reconstituted HDL (rHDL) infusions have demonstrated limited beneficial effect in clinical practice. This is perhaps a consequence of the limited cholesterol efflux abilities of atheroma macrophages due to decreased expression of cholesterol transporters in advanced atheromas and following rHDL infusion treatment. Thus, we propose that a combination therapy of rHDL and a liver X receptor (LXR) agonist could maximize the therapeutic benefit of rHDL by upregulating ATP-binding cassette transporters A-1 (ABCA1) and ATP-binding cassette transporter G-1 (ABCG1), and enhancing cholesterol efflux to rHDL. In macrophages, rHDL downregulated the expression of ABCA1/G1 in a dose- and rHDL composition-dependent manner. Although LXR agonist, T0901317 (T1317), upregulated the expression of ABCA1 and ABCG1, the drug itself did not have any effect on cholesterol efflux (6.6 ± 0.5%) while the combination of rHDL and T1317 exhibited enhanced cholesterol efflux from [3H]-cholesterol loaded J774A.1 macrophages (23.3 ± 1.3%). Treatment with rHDL + T1317 significantly reduced the area of aortic plaque in ApoE-/- mice compared to PBS treated control animals (24.16 ± 1.42% vs. 31.59 ± 1.93%, p < 0.001), while neither rHDL nor T1317 treatment alone had a significant effect. Together, we show that rHDL paired with an LXR agonist can induce a synergetic effect in reducing atheroma burden. This synergy could lead to lower overall effective dose for both drugs, potentially overcoming the existing barriers in clinical development and renewing pharmaceutical interest in these two drug classes.
Copyright © 2020 Morin, Guo, He, Yuan, Souery, Fawaz, Chen and Schwendeman.

Entities:  

Keywords:  atherosclerosis; cholesterol efflux; coronary artery disease; high-density lipoprotein; liver X receptor

Year:  2020        PMID: 33390931      PMCID: PMC7772318          DOI: 10.3389/fphar.2020.513031

Source DB:  PubMed          Journal:  Front Pharmacol        ISSN: 1663-9812            Impact factor:   5.810


  56 in total

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Journal:  N Engl J Med       Date:  2011-01-13       Impact factor: 91.245

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Journal:  Biochemistry       Date:  2010-09-07       Impact factor: 3.162

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Journal:  Cell Metab       Date:  2016-08-09       Impact factor: 27.287

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Journal:  Nat Commun       Date:  2014       Impact factor: 14.919

9.  Discovery of Highly Potent Liver X Receptor β Agonists.

Authors:  Ellen K Kick; Brett B Busch; Richard Martin; William C Stevens; Venkataiah Bollu; Yinong Xie; Brant C Boren; Michael C Nyman; Max H Nanao; Lam Nguyen; Artur Plonowski; Ira G Schulman; Grace Yan; Huiping Zhang; Xiaoping Hou; Meriah N Valente; Rangaraj Narayanan; Kamelia Behnia; A David Rodrigues; Barry Brock; James Smalley; Glenn H Cantor; John Lupisella; Paul Sleph; Denise Grimm; Jacek Ostrowski; Ruth R Wexler; Todd Kirchgessner; Raju Mohan
Journal:  ACS Med Chem Lett       Date:  2016-10-23       Impact factor: 4.345

10.  CSL112 (Apolipoprotein A-I [Human]) Enhances Cholesterol Efflux Similarly in Healthy Individuals and Stable Atherosclerotic Disease Patients.

Authors:  Andreas Gille; Denise D'Andrea; Michael A Tortorici; Gunter Hartel; Samuel D Wright
Journal:  Arterioscler Thromb Vasc Biol       Date:  2018-02-08       Impact factor: 8.311

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