Journal of Lipid Research

2009

DOI: 10.1194/jlr.m800374-jlr200

|View full text |Cite

|

Sign up to set email alerts

|

LXR agonist suppresses atherosclerotic lesion growth and promotes lesion regression in apoE*3Leiden mice: time course and mechanisms

Lars Verschuren

¹

,

Jitske de Vries-van der Weij

²

,

Susanne Zadelaar

³

et al.

Abstract: The aim of this study was to define the antiatherosclerotic role of liver-X-receptors (LXRs) under lesion progressive and lesion regressive conditions, to establish a temporal line of events, and to gain insights into the mechanisms underlying the anti-atherogenic potency of LXRs. We used apoE*3Leiden (E3L) mice to comprehensively and time-dependently dissect how T0901317, an LXR-agonist, inhibits initiation and progression of atherosclerotic lesions and regresses existing lipid-and macrophage-rich lesions. T0… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...

Discussion2

Citation Types

Supporting

5

Mentioning

61

Contrasting

0

Unclassified

3

Year Published

2010

2010

2020

2020

Publication Types

Select...

Article6

Book2

Other1

Relationship

Self Cite0

Independent9

Authors

Journals

Cited by 83 publications

(69 citation statements)

References 32 publications

Supporting

5

Mentioning

61

Contrasting

0

Unclassified

3

Order By: Relevance

“…The present results propose an additional mechanism for LXR-atheroprotection, namely, their stimulation of CD68 + cell emigration from plaques through the induction of Ccr7. LXR-dependent acquisition of CCR7 function in CD68 + plaque cells is also consistent with previous work by us (50) and others (24,48), as well as with the more general finding that the acquisition of migratory ability during differentiation of monocytes to DCs is concomitant with both LXR isoforms being expressed (51, 52).…”

Section: Discussionsupporting

confidence: 80%

“…Recently, it has also been shown that LXRs also negatively regulate the inflammatory state of macrophages through effects on toll-like receptors and NF-κB (46,47). Activation of LXRs and absence of LXRs have been shown to promote regression (38,48) and exacerbate progression (39,49), respectively, of atherosclerosis in mouse models. These effects of LXRs have been attributed to the aforementioned roles in RCT and inflammation.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

LXR promotes the maximal egress of monocyte-derived cells from mouse aortic plaques during atherosclerosis regression

Feig¹,

Pineda-Torra²,

et al. 2010

J. Clin. Invest.

View full text Add to dashboard Cite

We have previously shown that mouse atherosclerosis regression involves monocyte-derived (CD68 + ) cell emigration from plaques and is dependent on the chemokine receptor CCR7. Concurrent with regression, mRNA levels of the gene encoding LXRα are increased in plaque CD68 + cells, suggestive of a functional relationship between LXR and CCR7. To extend these results, atherosclerotic Apoe -/-mice sufficient or deficient in CCR7 were treated with an LXR agonist, resulting in a CCR7-dependent decrease in plaque CD68 + cells. To test the requirement for LXR for CCR7-dependent regression, we transplanted aortic arches from atherosclerotic Apoe -/-mice, or from Apoe -/-mice with BM deficiency of LXRα or LXRβ, into WT recipients. Plaques from both LXRα-and LXRβ-deficient Apoe -/-mice exhibited impaired regression. In addition, the CD68 + cells displayed reduced emigration and CCR7 expression. Using an immature DC line, we found that LXR agonist treatment increased Ccr7 mRNA levels. This increase was blunted when LXRα and LXRβ levels were reduced by siRNAs. Moreover, LXR agonist treatment of primary human immature DCs resulted in functionally significant upregulation of CCR7. We conclude that LXR is required for maximal effects on plaque CD68 + cell expression of CCR7 and monocyte-derived cell egress during atherosclerosis regression in mice.

“…The present results propose an additional mechanism for LXR-atheroprotection, namely, their stimulation of CD68 + cell emigration from plaques through the induction of Ccr7. LXR-dependent acquisition of CCR7 function in CD68 + plaque cells is also consistent with previous work by us (50) and others (24,48), as well as with the more general finding that the acquisition of migratory ability during differentiation of monocytes to DCs is concomitant with both LXR isoforms being expressed (51, 52).…”

Section: Discussionsupporting

confidence: 80%

“…Recently, it has also been shown that LXRs also negatively regulate the inflammatory state of macrophages through effects on toll-like receptors and NF-κB (46,47). Activation of LXRs and absence of LXRs have been shown to promote regression (38,48) and exacerbate progression (39,49), respectively, of atherosclerosis in mouse models. These effects of LXRs have been attributed to the aforementioned roles in RCT and inflammation.…”

Section: Discussionmentioning

confidence: 99%

LXR promotes the maximal egress of monocyte-derived cells from mouse aortic plaques during atherosclerosis regression

Feig¹,

Pineda-Torra²,

et al. 2010

J. Clin. Invest.

View full text Add to dashboard Cite

We have previously shown that mouse atherosclerosis regression involves monocyte-derived (CD68 + ) cell emigration from plaques and is dependent on the chemokine receptor CCR7. Concurrent with regression, mRNA levels of the gene encoding LXRα are increased in plaque CD68 + cells, suggestive of a functional relationship between LXR and CCR7. To extend these results, atherosclerotic Apoe -/-mice sufficient or deficient in CCR7 were treated with an LXR agonist, resulting in a CCR7-dependent decrease in plaque CD68 + cells. To test the requirement for LXR for CCR7-dependent regression, we transplanted aortic arches from atherosclerotic Apoe -/-mice, or from Apoe -/-mice with BM deficiency of LXRα or LXRβ, into WT recipients. Plaques from both LXRα-and LXRβ-deficient Apoe -/-mice exhibited impaired regression. In addition, the CD68 + cells displayed reduced emigration and CCR7 expression. Using an immature DC line, we found that LXR agonist treatment increased Ccr7 mRNA levels. This increase was blunted when LXRα and LXRβ levels were reduced by siRNAs. Moreover, LXR agonist treatment of primary human immature DCs resulted in functionally significant upregulation of CCR7. We conclude that LXR is required for maximal effects on plaque CD68 + cell expression of CCR7 and monocyte-derived cell egress during atherosclerosis regression in mice.

“…Reintroducing apolipoprotein E (ApoE) into ApoE 2/2 mice via ApoE gene transfer induces regression (3,4). Furthermore, LXR compounds induce atherosclerotic regression by promoting reverse cholesterol transport in macrophages (5). Another approach to study regression was introduced by Feig et al (6) who used a model in which atherosclerosis-containing aortic segments from ApoE 2/2 mice were transplanted into wild-type recipient mice.…”

mentioning

confidence: 99%

Interruption of the OX40–OX40 Ligand Pathway in LDL Receptor–Deficient Mice Causes Regression of Atherosclerosis

¹

,

²

,

³

et al. 2013

The Journal of Immunology

View full text Add to dashboard Cite

Patients suffering from cardiovascular disease have well-established atherosclerotic lesions, rendering lesion regression of therapeutic interest. The OX40 (TNFRSF4)–OX40 ligand (OX40L; TNFSF4) pathway is important for the proliferation and survival of T cells, stimulates B cells, and is associated with cardiovascular disease. We hypothesized that interference with the OX40–OX40L pathway, in combination with decreases in cholesterol, may induce regression of atherosclerosis. LDLr−/− mice were fed a Western-type diet for 10 wk, after which they received chow diet and were treated with anti-OX40L or PBS for 10 wk. A significant regression of lesions was observed in the aorta and aortic arch of anti-OX40L–treated mice compared with control mice. Interference of the OX40–OX40L pathway reduced Th2 responses, as shown by decreases in GATA-3 and IL-4 levels. Also, IgE levels were decreased, as demonstrated by reduced mast cell presence and activation. Notably, IL-5 production by T and B1 cells was increased, thus enhancing atheroprotective oxidized low-density lipoprotein–specific IgM production. The increase in IL-5 production and IgM was mediated by IL-33 production by APCs upon OX40L blockade. We conclude that interruption of the OX40–OX40L signaling pathway, combined with decreases in dietary cholesterol, induces the regression of atherosclerosis through induction of IL-5–producing T cells and oxidized low-density lipoprotein–specific IgM and reductions in Th2 and mast cells.

“…Freeman et al show that the liver X receptor (LXR) agonist TO901317 increases the deposition of cholesterol microdomains in the ECM produced by macrophages. It is known that, besides upregulation of ABCA1 and ABCG1, LXR agonists both in vivo and in vitro upregulate apoE expression ( 8 ). Future colocalization experiments with MAb(s) against the microdomains and against apoE in cell cultures and in human lesions could be informative in this respect.…”

mentioning

confidence: 99%

Macrophages, extracellular matrix, and lipoproteins in arterial cholesterol balance

¹

,

²

2014

Journal of Lipid Research

View full text Add to dashboard Cite

No abstract

scite is a Brooklyn-based organization that helps researchers better discover and understand research articles through Smart Citations–citations that display the context of the citation and describe whether the article provides supporting or contrasting evidence. scite is used by students and researchers from around the world and is funded in part by the National Science Foundation and the National Institute on Drug Abuse of the National Institutes of Health.

Contact Info

customersupport@researchsolutions.com

10624 S. Eastern Ave., Ste. A-614

Henderson, NV 89052, USA

Product

Browser Extension Assistant by scite Citation Statement Search Reference Check Visualizations Dashboards Explore Journals Explore Organizations Explore Funders Embedding Badge Embedding Citation Search Pricing

Resources

Blog Help & FAQ Accessibility Statement API Terms For Universities & Governments For Researchers For Publishers For Corporate, Pharma & Enterprise Author Marketing Become an Affiliate Get an organization trial or quote scite Data & Services

About

News & Press Careers Read our Paper Coverage

This site is protected by reCAPTCHA and the Google Privacy Policy and Terms of Service apply.

Blog Terms and Conditions API Terms Privacy Policy Contact Cookie Preferences Do Not Sell or Share My Personal Information

Copyright © 2024 scite LLC. All rights reserved.

Made with 💙 for researchers

Part of the Research Solutions Family.