Direct Interaction of Nuclear Liver X Receptor-β with ABCA1 Modulates Cholesterol Efflux

Hozoji, Masako; Munehira, Youichi; Ikeda, Yuika; Makishima, Makoto; Matsuo, Masaru; Kioka, Noriyuki; Ueda, Kazumitsu

doi:10.1074/jbc.m804599200

Cited by 67 publications

(50 citation statements)

References 22 publications

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“…Cholesterol efflux by cells expressing mutant ABCA1 was not affected by the addition of TO901317 either in the presence or absence of LXR␤. Co-expression of LXR␤ doubled the plasma membrane levels of WT ABCA1 as shown previously (16), but surface levels of the mutants (L2247A, L2251A, and L2247/L2251A) were not affected by LXR␤ expression (Fig. 3C).…”

Section: Leucine Residues Of Abca1 Mediate Its Interaction Withmentioning

confidence: 48%

“…However, addition of TO901317 to the membrane fraction of cells co-expressing ABCA1 and LXR␤ led to photoaffinity labeling of ABCA1 (lane 8) comparable with that seen in the absence of LXR␤ (lane 6). Under the same conditions, the co-precipitation of ABCA1 with LXR␤ was abrogated (16). ABCA1-L2247A/L2251A double mutant was labeled as efficiently as WT ABCA1 (lane 9), but this was not inhibited by LXR␤ co-expression (lanes 11 and 12), suggesting that the interaction of LXR␤ with ABCA1 via Leu 2247 and Leu 2251 prevents tight ATP binding.…”

Section: Leucine Residues Of Abca1 Mediate Its Interaction Withmentioning

confidence: 85%

“…Antibodies-Rabbit anti-human ABCA1 polyclonal antiserum was generated against the linker region (amino acids 1134 -1345) of human ABCA1 as described previously (16). The rat anti-human ABCA1 monoclonal antibody KM3073 was generated against the first extracellular domain (amino acids 45-639) of human ABCA1 as described previously (13).…”

Section: Methodsmentioning

confidence: 99%

“…B and C, HEK293 cells were co-transfected with LXR␤ and WT or mutant ABCA1. At 28 h after transfection, membranes prepared by nitrogen cavitation were subjected to immunoprecipitation (IP) with anti-ABCA1 polyclonal antiserum (16). Cell lysates (10%) (B) and precipitated proteins (C) were subjected to immunoblotting with the anti-ABCA1 monoclonal antibody KM3073 or anti-LXR␤ monoclonal antibody.…”

Section: Leucine Residues Of Abca1 Mediate Its Interaction Withmentioning

confidence: 99%

“…Consequently, ABCA1-mediated cholesterol release is also regulated at the post-translational level. Several proteins, including syntrophins (13,14), JAK2 (15), and LXR␤ (16), have been reported to interact with ABCA1 and modulate its degradation and function. However, the precise mechanism(s) by which ABCA1 activity is regulated post-translationally remains unclear.…”

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Liver X Receptor β (LXRβ) Interacts Directly with ATP-binding Cassette A1 (ABCA1) to Promote High Density Lipoprotein Formation during Acute Cholesterol Accumulation

Hozoji-Inada

Munehira

Nagao

et al. 2011

Journal of Biological Chemistry

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Cells have evolved multiple mechanisms for maintaining cholesterol homeostasis, and, among these, ATP-binding cassette protein A1 (ABCA1)-mediated cholesterol efflux is highly regulated at the transcriptional level through the activity of the nuclear receptor liver X receptor (LXR). Here, we show that in addition to its well defined role in transcription, LXR␤ directly binds to the C-terminal region ( Disruption of cellular cholesterol homeostasis can lead to a variety of pathological conditions, including cardiovascular disease (1). ATP-binding cassette protein A1 (ABCA1), 2 an important regulator of cholesterol homeostasis, mediates the release of cellular excess free cholesterol and phospholipids to apolipoprotein A-I (apoA-I), an extracellular acceptor circulating in plasma, to form high density lipoprotein (HDL) (2-5). HDL formation is the only pathway through which excess cholesterol can be eliminated from nonhepatic cells. Defects in ABCA1 cause Tangier disease (6 -8), a condition in which patients have a near absence of circulating HDL, prominent cholesterol-ester accumulation in tissue macrophages, and premature atherosclerotic vascular disease (1, 9).The ABCA1-mediated release of cholesterol is highly regulated at the transcriptional level. When excess cholesterol accumulates in cells, intracellular concentrations of oxysterols increase and activate liver X receptor (LXR), which, in turn, stimulates ABCA1 gene transcription and increased expression of ABCA1 with associated elimination of excess cholesterol (10 -12). However, cholesterol is required for cell function and proliferation, and the intracellular cholesterol concentration must be maintained within a narrow range. Consequently, ABCA1-mediated cholesterol release is also regulated at the post-translational level. Several proteins, including syntrophins (13, 14), JAK2 (15), and LXR␤ (16), have been reported to interact with ABCA1 and modulate its degradation and function. However, the precise mechanism(s) by which ABCA1 activity is regulated post-translationally remains unclear.We previously reported (16) that a fraction of cytosolically localized LXR␤ may interact with ABCA1 on the plasma membrane and modulate the function of ABCA1. In WI-38 and THP-1 cells, endogenous LXR␤ interacts with ABCA1 under conditions in which LXR ligands do not accumulate, i.e. when cholesterol is not in excess. LXR␤ suppresses ABCA1-mediated cholesterol efflux. However, the mechanism by which LXR␤ suppresses ABCA1 functions was not clear. In this study, we identified two leucine residues in the C-terminal region of ABCA1 responsible for the interaction with LXR␤ and showed that LXR␤ interaction suppresses ATP binding to ABCA1 and thereby keeps ABCA1 standby on the plasma membrane for acute cholesterol accumulation. EXPERIMENTAL PROCEDURESMaterials-The LXR ligand TO901317, 22(R)-hydroxycholesterol, 25-hydroxycholesterol, and Alexa Fluor 546 succinimidyl esters were purchased from Cayman Co., Sigma, Stelaroids, and Molecular Probes, respectively. A cholesterol oxidas...

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Section: Leucine Residues Of Abca1 Mediate Its Interaction Withmentioning

confidence: 48%

Section: Leucine Residues Of Abca1 Mediate Its Interaction Withmentioning

confidence: 85%

Section: Methodsmentioning

confidence: 99%

Section: Leucine Residues Of Abca1 Mediate Its Interaction Withmentioning

confidence: 99%

mentioning

confidence: 99%

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Liver X Receptor β (LXRβ) Interacts Directly with ATP-binding Cassette A1 (ABCA1) to Promote High Density Lipoprotein Formation during Acute Cholesterol Accumulation

Hozoji-Inada

Munehira

Nagao

et al. 2011

Journal of Biological Chemistry

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Nuclear Hormone Receptor Medicinal Chemistry

Cheng

Kick

Mukherjee

2010

Burger's Medicinal Chemistry and Drug Discovery

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This chapter will be focused on recent advances in the medicinal chemistry of agonist, antagonist, and modulator ligands of selected nuclear hormone receptors (NHRs) that are of special interest in the metabolic diseases therapeutic area (diabetes, obesity and dyslipidemia/atherosclerosis). These NHRs include established biological targets such as the peroxisome proliferator‐activated receptors (PPARs), the liver X receptors (LXRs), and the farnesoid X receptors (FXRs), for which ligands have reached either clinical development or have been approved for clinical usage. Other more recent targets of interest to metabolic diseases include HNF and Rev‐erb.

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Nuclear Hormone Receptor Medicinal Chemistry

Cheng

Kick

Mukherjee

2021

Burger's Medicinal Chemistry and Drug Discovery

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This article will be focused on recent advances in the medicinal chemistry of agonist, antagonist, and modulator ligands of selected nuclear hormone receptors (NHRs) that are of special interest in the metabolic diseases therapeutic area (diabetes, obesity and dyslipidemia/atherosclerosis). These NHRs include established biological targets such as the peroxisome proliferator‐activated receptors (PPARs), the liver X receptors (LXRs), and the farnesoid X receptors (FXRs), for which ligands have reached either clinical development or have been approved for clinical usage. Other more recent targets of interest to metabolic diseases include HNF and Rev‐erb.

show abstract

Direct Interaction of Nuclear Liver X Receptor-β with ABCA1 Modulates Cholesterol Efflux

Cited by 67 publications

References 22 publications

Liver X Receptor β (LXRβ) Interacts Directly with ATP-binding Cassette A1 (ABCA1) to Promote High Density Lipoprotein Formation during Acute Cholesterol Accumulation

Liver X Receptor β (LXRβ) Interacts Directly with ATP-binding Cassette A1 (ABCA1) to Promote High Density Lipoprotein Formation during Acute Cholesterol Accumulation

Nuclear Hormone Receptor Medicinal Chemistry

Nuclear Hormone Receptor Medicinal Chemistry

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