Liver X receptors (LXRs) α and β are transcriptional regulators of cholesterol homeostasis and potential targets for the development of antiatherosclerosis drugs. However, the specific roles of individual LXR isotypes in atherosclerosis and the pharmacological effects of synthetic agonists remain unclear. Previous work has shown that mice lacking LXRα accumulate cholesterol in the liver but not in peripheral tissues. In striking contrast, we demonstrate here that LXRα–/–apoE–/– mice exhibit extreme cholesterol accumulation in peripheral tissues, a dramatic increase in whole-body cholesterol burden, and accelerated atherosclerosis. The phenotype of these mice suggests that the level of LXR pathway activation in macrophages achieved by LXRβ and endogenous ligand is unable to maintain homeostasis in the setting of hypercholesterolemia. Surprisingly, however, a highly efficacious synthetic agonist was able to compensate for the loss of LXRα. Treatment of LXRα–/–apoE–/– mice with synthetic LXR ligand ameliorates the cholesterol overload phenotype and reduces atherosclerosis. These observations indicate that LXRα has an essential role in maintaining peripheral cholesterol homeostasis in the context of hypercholesterolemia and provide in vivo support for drug development strategies targeting LXRβ.
Michelle N. Bradley, Cynthia Hong, Mingyi Chen, Sean B. Joseph, Damien C. Wilpitz, Xuping Wang, Aldons J. Lusis, Allan Collins, Willa A. Hseuh, Jon L. Collins, Rajendra K. Tangirala, Peter Tontonoz
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Loss of the liver X receptor LXRα/β in peripheral sensory neurons modifies energy expenditure: ( A ) Regulation of selected target genes in nodose ganglia (NG) following liver X receptor (LXR) agonist treatment in vivo (left panel) n = 5–8 per group. **p < 0.005. ( B ) NG organotypic slices were prepared from LXRs Nav or LXRs fl/fl treated with GW3965 (5 μM) or vehicle for 4 hr. Quantitative PCR (qPCR) data are expressed as average fold-change relative to vehicle ± S.E.M., n = 3 independent experiments. # and *indicates p < 0.5, **p < 0.005. ( C ) Quantification of total cholesterol. Values were expressed as ng of cholesterol per NG, n = 6. ## and **p < 0.001. (right panel). Neurons isolated from LXRs Nav or control mice NG were subjected to Filipin staining (representative images of staining from 3 individual mice)
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Advanced Drug Delivery Reviews | 2010 |
GPS2-dependent corepressor/SUMO pathways govern anti-inflammatory actions of LRH-1 and LXRβ in the hepatic acute phase response
N Venteclef, T Jakobsson, A Ehrlund, A Damdimopoulos, L Mikkonen, E Ellis, LM Nilsson, P Parini, OA Jänne, JÅ Gustafsson, KR Steffensen, E Treuter |
Genes & development | 2010 |
Macrophage death and defective inflammation resolution in atherosclerosis
I Tabas |
Nature Reviews Immunology | 2010 |
Pharmacological manipulations of CNS sirtuins: Potential effects on metabolic homeostasis
G Ramadori, R Coppari |
Pharmacological research : the official journal of the Italian Pharmacological Society | 2010 |
Functions of cholesterol ester transfer protein and relationship to coronary artery disease risk
AR Tall |
Journal of Clinical Lipidology | 2010 |
Liver x receptor signaling pathways and atherosclerosis
AC Calkin, P Tontonoz |
Arteriosclerosis, thrombosis, and vascular biology | 2010 |
Non-redundant roles for LXRalpha and LXRbeta in atherosclerosis susceptibility in low density lipoprotein receptor knockout mice
ED Bischoff, CL Daige, M Petrowski, H Dedman, J Pattison, J Juliano, AC Li, IG Schulman |
Journal of lipid research | 2010 |
Nuclear receptor engineering based on novel structure activity relationships revealed by farnesyl pyrophosphate
R Goyanka, S Das, HH Samuels, T Cardozo |
Protein Engineering Design and Selection | 2010 |
Controllable Inhibition of Cellular Uptake of Oxidized Low Density Lipoprotein: Structure-Function Relationships for Nanoscale Amphiphilic Polymers
N Iverson, SM Sparks, B Demirdirek, KE Uhrich, PV Moghe |
Acta Biomaterialia | 2010 |
Minireview: Liver X Receptor β: Emerging Roles in Physiology and Diseases
C Gabbi, M Warner, JÅ Gustafsson |
Molecular Endocrinology | 2009 |
LXR ligand lowers LDL cholesterol in primates, is lipid neutral in hamster, and reduces atherosclerosis in mouse
EM Quinet, MD Basso, AR Halpern, DW Yates, RJ Steffan, V Clerin, C Resmini, JC Keith, TJ Berrodin, I Feingold, W Zhong, HB Hartman, MJ Evans, SJ Gardell, E DiBlasio-Smith, WM Mounts, ER LaVallie, J Wrobel, P Nambi, GP Vlasuk |
Journal of lipid research | 2009 |
Inactivation of hypothalamic FAS protects mice from diet-induced obesity and inflammation
MV Chakravarthy, Y Zhu, L Yin, T Coleman, KL Pappan, CA Marshall, ML McDaniel, CF Semenkovich |
Journal of lipid research | 2009 |
Liver X Receptors as Therapeutic Targets for Managing Cholesterol: Implications for Atherosclerosis and Other Inflammatory Conditions
Y Zhang, JF Chan, CL Cummins |
Clinical Lipidology | 2009 |
The synthetic liver X receptor agonist GW3965 reduces tissue factor production and inflammatory responses in human islets in vitro
H Scholz, T Lund, MK Dahle, JL Collins, O Korsgren, JE Wang, A Foss |
Diabetologia | 2009 |
Insulin resistance and altered systemic glucose metabolism in mice lacking Nur77
LC Chao, K Wroblewski, Z Zhang, L Pei, L Vergnes, OR Ilkayeva, SY Ding, K Reue, MJ Watt, CB Newgard, PF Pilch, AL Hevener, P Tontonoz |
Diabetes | 2009 |
T0901317, an LXR agonist, augments PKA-induced vascular cell calcification
JJ Hsu, J Lu, MS Huang, Y Geng, AP Sage, MN Bradley, P Tontonoz, LL Demer, Y Tintut |
FEBS Letters | 2009 |
Characterization of ASC-2 as an Antiatherogenic Transcriptional Coactivator of Liver X Receptors in Macrophages
GH Kim, K Park, SY Yeom, KJ Lee, G Kim, J Ko, DK Rhee, YH Kim, HK Lee, HW Kim, GT Oh, KU Lee, JW Lee, SW Kim |
Molecular Endocrinology | 2009 |
Apolipoprotein A-I and Its Role in Lymphocyte Cholesterol Homeostasis and Autoimmunity
AJ Wilhelm, M Zabalawi, JM Grayson, AE Weant, AS Major, J Owen, M Bharadwaj, R Walzem, L Chan, K Oka, MJ Thomas, MG Sorci-Thomas |
Arteriosclerosis, thrombosis, and vascular biology | 2009 |
ROCK1 Mediates Leukocyte Recruitment and Neointima Formation Following Vascular Injury
Kensuke Noma, Yoshiyuki Rikitake, Naotsugu Oyama, Guijun Yan, Pilar Alcaide, Ping-Yen Liu, Hongwei Wang, Daniella Ahl, Naoki Sawada, Ryuji Okamoto, Yukio Hiroi, Koichi Shimizu, Francis W. Luscinskas, Jianxin Sun, James K. Liao |
Journal of Clinical Investigation | 2008 |
Host-derived oxidized phospholipids and high density lipoprotein regulate innate immunity in mycobacterial infection
Daniel Cruz, Andrew D. Watson, Christopher S. Miller, Dennis Montoya, Maria-Teresa Ochoa, Peter A. Sieling, Miguel A. Gutierrez, Mohamad Navab, Srinivasa T. Reddy, Joseph L. Witztum, Alan M. Fogelman, Thomas H. Rea, David Eisenberg, Judith Berliner, and Robert L. Modlin |
Journal of Clinical Investigation | 2008 |
Synthetic LXR agonist attenuates plaque formation in apoE-/- mice without inducing liver steatosis and hypertriglyceridemia
A Kratzer, M Buchebner, T Pfeifer, TM Becker, G Uray, M Miyazaki, S Miyazaki-Anzai, B Ebner, PG Chandak, RS Kadam, E Calayir, N Rathke, H Ahammer, B Radovic, M Trauner, G Hoefler, UB Kompella, G Fauler, M Levi, S Levak-Frank, GM Kostner, D Kratky |
Journal of lipid research | 2008 |
Liver X receptors as therapeutic targets in metabolism and atherosclerosis
T Nomiyama, D Bruemmer |
Current Atherosclerosis Reports | 2008 |
Coordination of inflammation and metabolism by PPAR and LXR nuclear receptors
C Hong, P Tontonoz |
Current Opinion in Genetics & Development | 2008 |
HRASLS3 is a PPARgamma-selective target gene that promotes adipocyte differentiation
S Hummasti, C Hong, SJ Bensinger, P Tontonoz |
Journal of lipid research | 2008 |
TLR/MyD88 and LXRα Signaling Pathways Reciprocally Control Chlamydia Pneumoniae-Induced Acceleration of Atherosclerosis
Naiki Y, Sorrentino R, Wong MH, Michelsen KS, Shimada K, Chen S, Yilmaz A, Slepenkin A, Schröder NW, Crother TR, Bulut Y, Doherty TM, Bradley M, Shaposhnik Z, Peterson EM, Tontonoz P, Shah PK, Arditi M |
Journal of immunology (Baltimore, Md. : 1950) | 2008 |
Chlamydia pneumoniae-induced foam cell formation requires MyD88-dependent and -independent signaling and is reciprocally modulated by liver X receptor activation.
Chen S, Sorrentino R, Shimada K, Bulut Y, Doherty TM, Crother TR, Arditi M |
Journal of immunology (Baltimore, Md. : 1950) | 2008 |