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巨噬细胞肝X受体是LXR激动剂抗动脉粥样硬化活性所必需的。

Macrophage liver X receptor is required for antiatherogenic activity of LXR agonists.

作者信息

Levin Nancy, Bischoff Eric D, Daige Chris L, Thomas Diane, Vu Calvin T, Heyman Richard A, Tangirala Rajendra K, Schulman Ira G

机构信息

X-Ceptor Therapeutics Inc, San Diego, Calif 92121, USA.

出版信息

Arterioscler Thromb Vasc Biol. 2005 Jan;25(1):135-42. doi: 10.1161/01.ATV.0000150044.84012.68. Epub 2004 Nov 11.

DOI:10.1161/01.ATV.0000150044.84012.68
PMID:15539622
Abstract

OBJECTIVE

Complications of atherosclerotic cardiovascular disease due to elevated blood cholesterol levels are the major cause of death in the Western world. The liver X receptors, LXRalpha and LXRbeta (LXRs), are ligand-dependent transcription factors that act as cholesterol sensors and coordinately control transcription of genes involved in cholesterol and lipid homeostasis as well as macrophage inflammatory gene expression. LXRs regulate cholesterol balance through activation of ATP-binding cassette transporters that promote cholesterol transport and excretion from the liver, intestine, and macrophage. Although LXR agonists are known to delay progression of atherosclerosis in mouse models, their ability to abrogate preexisting cardiovascular disease by inducing regression and stabilization of established atherosclerotic lesions has not been addressed.

METHODS AND RESULTS

We demonstrate that LXR agonist treatment increases ATP-binding cassette transporter expression within preexisting atherosclerotic lesions, resulting in regression of these lesions as well as remodeling from vulnerable to stable lesions and a reduction in macrophage content. Further, using macrophage-selective LXR-deficient mice created by bone marrow transplantation, we provide the first evidence that macrophage LXR expression is necessary for the atheroprotective actions of an LXR agonist.

CONCLUSIONS

These data substantiate that drugs targeting macrophage LXR activity may offer therapeutic benefit in the treatment of atherosclerotic cardiovascular disease.

摘要

目的

血液胆固醇水平升高所致的动脉粥样硬化性心血管疾病并发症是西方世界的主要死因。肝脏X受体LXRα和LXRβ(LXRs)是配体依赖性转录因子,作为胆固醇传感器,协同控制参与胆固醇和脂质稳态以及巨噬细胞炎症基因表达的基因转录。LXRs通过激活ATP结合盒转运蛋白来调节胆固醇平衡,这些转运蛋白促进胆固醇从肝脏、肠道和巨噬细胞的转运和排泄。虽然已知LXR激动剂在小鼠模型中可延缓动脉粥样硬化进展,但它们通过诱导已形成的动脉粥样硬化病变的消退和稳定来消除已存在的心血管疾病的能力尚未得到研究。

方法和结果

我们证明,LXR激动剂治疗可增加已存在的动脉粥样硬化病变内ATP结合盒转运蛋白的表达,导致这些病变消退,以及从易损病变重塑为稳定病变,并减少巨噬细胞含量。此外,通过骨髓移植创建巨噬细胞选择性LXR缺陷小鼠,我们首次证明巨噬细胞LXR表达对于LXR激动剂的抗动脉粥样硬化作用是必需的。

结论

这些数据证实,靶向巨噬细胞LXR活性的药物可能在动脉粥样硬化性心血管疾病的治疗中提供治疗益处。

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