Your search keyword '"Michinori Matsuo"' showing total 10 results

1. ABCA1 and ABCG1 as potential therapeutic targets for the prevention of atherosclerosis

Author

Michinori Matsuo

Subjects

ABC transporter protein, Atherosclerosis, Cholesterol, High-density lipoprotein, Reverse cholesterol transport, Therapeutics. Pharmacology, RM1-950

Abstract

Prevention of atherosclerosis is important because it is a risk factor for cardiovascular diseases globally. One of the causes of atherosclerosis is accumulation of cholesterol and triglycerides in peripheral cells. ATP-binding cassette protein A1 (ABCA1) and G1 (ABCG1) are important in eliminating excess cholesterol from cells including macrophages and forming high-density lipoprotein, which contributes to the prevention and regression of atherosclerosis. Enhanced cholesterol efflux activities of ABCA1 and ABCG1 are expected to prevent the progression of atherosclerosis. ABCA1 and ABCG1 are induced by the LXR/RXR pathway and regulated transcriptionally, post-transcriptionally, and post-translationally. Their mRNAs are destabilized by microRNAs and their cellular localization and degradation are regulated by other proteins and phosphorylation. Furthermore, ABCA1 and ABCG1 suppress the inflammatory responses of macrophages. These proteins are effective targets because their increased activities can suppress cholesterol accumulation and inflammation in macrophages. Moreover, ABCA1 and ABCG1 prevent amyloid β accumulation; therefore, their increased activity may prevent Alzheimer's disease. Because ABCA1 and ABCG1 are affected by transcriptional, post-transcriptional, and post-translational regulation, the regulatory factors involved could also serve as therapeutic targets. This review highlights that ABCA1 and ABCG1 could be potential therapeutic targets for preventing atherosclerosis by regulating their expression, degradation, and localization.

Published

2022

2. Neurite outgrowth stimulation by n-3 and n-6 PUFAs of phospholipids in apoE-containing lipoproteins secreted from glial cells

Author

Mitsuhiro Nakato, Michinori Matsuo, Nozomu Kono, Makoto Arita, Hiroyuki Arai, Jun Ogawa, Noriyuki Kioka, and Kazumitsu Ueda

Subjects

polyunsaturated fatty acid, apolipoprotein E-containing lipoprotein, neuron, apolipoprotein E, low density lipoprotein receptor-related protein 1, Biochemistry, QD415-436

Abstract

PUFAs, which account for 25–30% of the total fatty acids in the human brain, are important for normal brain development and cognitive function. However, it remains unclear how PUFAs are delivered to neurons and exert their effects. In this study, we demonstrated that n-3 and n-6 PUFAs added to the medium are incorporated into membrane phospholipids of primary glial cells from rat cortices, and then secreted as the fatty acid moiety of phospholipids in apoE-containing lipoproteins (LpEs). Tandem mass spectrometry analysis further showed that LpEs secreted from glial cells contain a variety of metabolites of PUFAs produced in glial cells by elongation and unsaturation. LpEs are absorbed by endocytosis into neurons via LDL receptor-related protein 1. LpE-containing n-3 and n-6 PUFAs exhibit a strong effect on neurite outgrowth of hippocampal neurons by increasing the number of branches. This study sheds light on the novel role of LpEs in the central nervous system and also a novel pathway in which PUFAs act on neurons.

Published

2015

3. ABCB4 exports phosphatidylcholine in a sphingomyelin-dependent manner[S]

Author

Yu Zhao, Masato Ishigami, Kohjiro Nagao, Kentaro Hanada, Nozomu Kono, Hiroyuki Arai, Michinori Matsuo, Noriyuki Kioka, and Kazumitsu Ueda

Subjects

ATP binding cassette protein, ATP binding cassette transporter A1, myriosin, cholesterol, high density lipoprotein, (1R,3S)-N-(3-hydroxy-1-hydroxymethyl-3-phenylpropyl)dodecanamide, Biochemistry, QD415-436

Abstract

ABCB4, which is specifically expressed on the canalicular membrane of hepatocytes, exports phosphatidylcholine (PC) into bile. Because SM depletion increases cellular PC content and stimulates PC and cholesterol efflux by ABCA1, a key transporter involved in generation of HDL, we predicted that SM depletion also stimulates PC efflux through ABCB4. To test this prediction, we compared the lipid efflux activity of ABCB4 and ABCA1 under SM depletion induced by two different types of inhibitors for SM synthesis, myriocin and (1R,3S)-N-(3-hydroxy-1-hydroxymethyl-3-phenylpropyl)dodecanamide, in human embryonic kidney 293 and baby hamster kidney cells. Unexpectedly, SM depletion exerted opposite effects on ABCB4 and ABCA1, suppressing PC efflux through ABCB4 while stimulating efflux through ABCA1. Both ABCB4 and ABCA1 were recovered from Triton-X-100-soluble membranes, but ABCB4 was mainly recovered from CHAPS-insoluble SM-rich membranes, whereas ABCA1 was recovered from CHAPS-soluble membranes. These results suggest that a SM-rich membrane environment is required for ABCB4 to function. ABCB4 must have evolved to exert its maximum activity in the SM-rich membrane environment of the canalicular membrane, where it transports PC as the physiological substrate.

Published

2015

4. ATPase activity of human ABCG1 is stimulated by cholesterol and sphingomyelin[S]

Author

Hiroshi Hirayama, Yasuhisa Kimura, Noriyuki Kioka, Michinori Matsuo, and Kazumitsu Ueda

Subjects

ABC transporter, cholesterol homeostasis, high density lipoprotein, Biochemistry, QD415-436

Abstract

ATP-binding cassette protein G1 (ABCG1) is important for the formation of HDL. However, the biochemical properties of ABCG1 have not been reported, and the mechanism of how ABCG1 is involved in HDL formation remains unclear. We established a procedure to express and purify human ABCG1 using the suspension-adapted human cell FreeStyle293-F. ABCG1, fused at the C terminus with green fluorescent protein and Flag-peptide, was solubilized with n-dodecyl-β-D-maltoside and purified via a single round of Flag-M2 antibody affinity chromatography. The purified ABCG1 was reconstituted in liposome of various lipid compositions, and the ATPase activity was analyzed. ABCG1 reconstituted in egg lecithin showed ATPase activity (150 nmol/min/mg), which was inhibited by beryllium fluoride. The ATPase activity of ABCG1, reconstituted in phosphatidylserine liposome, was stimulated by cholesterol and choline phospholipids (especially sphingomyelin), and the affinity for cholesterol was increased by the addition of sphingomyelin. These results suggest that ABCG1 is an active lipid transporter and possesses different binding sites for cholesterol and sphingomyelin, which may be synergistically coupled.

Published

2013

5. ATP hydrolysis-dependent conformational changes in the extracellular domain of ABCA1 are associated with apoA-I binding[S]

Author

Kohjiro Nagao, Kei Takahashi, Yuya Azuma, Mie Takada, Yasuhisa Kimura, Michinori Matsuo, Noriyuki Kioka, and Kazumitsu Ueda

Subjects

ATP binding cassette protein A1, apolipoproteins, cholesterol efflux, HDL, transport, Biochemistry, QD415-436

Abstract

ATP-binding cassette protein A1 (ABCA1) plays a major role in cholesterol homeostasis and high-density lipoprotein (HDL) metabolism. Although it is predicted that apolipoprotein A-I (apoA-I) directly binds to ABCA1, the physiological importance of this interaction is still controversial and the conformation required for apoA-I binding is unclear. In this study, the role of the two nucleotide-binding domains (NBD) of ABCA1 in apoA-I binding was determined by inserting a TEV protease recognition sequence in the linker region of ABCA1. Analyses of ATP binding and occlusion to wild-type ABCA1 and various NBD mutants revealed that ATP binds equally to both NBDs and is hydrolyzed at both NBDs. The interaction with apoA-I and the apoA-I-dependent cholesterol efflux required not only ATP binding but also hydrolysis in both NBDs. NBD mutations and cellular ATP depletion decreased the accessibility of antibodies to a hemagglutinin (HA) epitope that was inserted at position 443 in the extracellular domain (ECD), suggesting that the conformation of ECDs is altered by ATP hydrolysis at both NBDs. These results suggest that ATP hydrolysis at both NBDs induces conformational changes in the ECDs, which are associated with apoA-I binding and cholesterol efflux.

Published

2012

6. Sphingomyelin-dependence of cholesterol efflux mediated by ABCG1s⃞

Author

Osamu Sano, Aya Kobayashi, Kohjiro Nagao, Keigo Kumagai, Noriyuki Kioka, Kentaro Hanada, Kazumitsu Ueda, and Michinori Matsuo

Subjects

ATP binding cassette A1, ceramide transfer protein, detergent-resistant membrane, raft, Biochemistry, QD415-436

Abstract

ABCG1, one of the half-type ATP binding cassette (ABC) proteins, mediates the efflux of cholesterol to HDL and functions in the reverse cholesterol transport from peripheral cells to the liver. We have shown that ABCG1 mediates the efflux of not only cholesterol but also sphingomyelin (SM) and phosphatidylcholine. Because SM preferentially associates with cholesterol, we examined whether it plays an important role in the ABCG1-mediated efflux of cholesterol. The efflux of cholesterol and SM mediated by ABCG1 was reduced in a mutant CHO-K1 cell line, LY-A, in which the cellular SM level is reduced because of a mutation of the ceramide transfer protein CERT. In contrast, CHO-K1 cells overexpressing CERT showed an increased efflux of cholesterol and SM mediated by ABCG1. The sensitivity of cells to methyl-β-cyclodextrin suggested that cholesterol in nonraft domains was increased due to the disruption of raft domains in LY-A cells. These results suggest that the ABCG1-mediated efflux of cholesterol and SM is dependent on the cellular SM level and distribution of cholesterol in the plasma membrane.

Published

2007

7. Efflux of sphingomyelin, cholesterol, and phosphatidylcholine by ABCG1

Author

Aya Kobayashi, Yasukazu Takanezawa, Takashi Hirata, Yuji Shimizu, Keiko Misasa, Noriyuki Kioka, Hiroyuki Arai, Kazumitsu Ueda, and Michinori Matsuo

Subjects

ATP binding cassette protein G1, ATP binding cassette protein A1, high density lipoprotein, Biochemistry, QD415-436

Abstract

Cholesterol and phospholipids are essential to the body, but an excess of cholesterol or lipids is toxic and a risk factor for arteriosclerosis. ABCG1, one of the half-type ABC proteins, is thought to be involved in cholesterol homeostasis. To explore the role of ABCG1 in cholesterol homeostasis, we examined its subcellular localization and function. ABCG1 and ABCG1-K120M, a WalkerA lysine mutant, were localized to the plasma membrane in HEK293 cells stably expressing ABCG1 and formed a homodimer. A stable transformant expressing ABCG1 exhibited efflux of cholesterol and choline phospholipids in the presence of BSA, and the cholesterol efflux was enhanced by the presence of HDL, whereas cells expressing ABCG1-K120M did not, suggesting that ATP binding and/or hydrolysis is required for the efflux. Mass and TLC analyses revealed that ABCG1 and ABCA1 secrete several species of sphingomyelin (SM) and phosphatidylcholine (PC), and SMs were preferentially secreted by ABCG1, whereas PCs were preferentially secreted by ABCA1. These results suggest that ABCA1 and ABCG1 mediate the lipid efflux in different mechanisms, in which different species of phospholipids are secreted, and function coordinately in the removal of cholesterol and phospholipids from peripheral cells.

Published

2006

8. ATPase activity of human ABCG1 is stimulated by cholesterol and sphingomyelin[S]

Author

Noriyuki Kioka, Yasuhisa Kimura, Hiroshi Hirayama, Michinori Matsuo, and Kazumitsu Ueda

Subjects

Detergents, ATP-binding cassette transporter, QD415-436, Biochemistry, Phosphates, cholesterol homeostasis, chemistry.chemical_compound, Endocrinology, Choline, Humans, Research Articles, ATP Binding Cassette Transporter, Subfamily G, Member 1, Adenosine Triphosphatases, Liposome, Egg lecithin, Binding Sites, biology, Cholesterol, Biological Transport, Drug Synergism, Cell Biology, Phosphatidylserine, Hydrogen-Ion Concentration, Molecular biology, Sphingomyelins, HEK293 Cells, ABCG1, chemistry, high density lipoprotein, biology.protein, ATP-Binding Cassette Transporters, lipids (amino acids, peptides, and proteins), ABC transporter, Sphingomyelin

Abstract

ATP-binding cassette protein G1 (ABCG1) is important for the formation of HDL. However, the biochemical properties of ABCG1 have not been reported, and the mechanism of how ABCG1 is involved in HDL formation remains unclear. We established a procedure to express and purify human ABCG1 using the suspension-adapted human cell FreeStyle293-F. ABCG1, fused at the C terminus with green fluorescent protein and Flag-peptide, was solubilized with n-dodecyl-β-D-maltoside and purified via a single round of Flag-M2 antibody affinity chromatography. The purified ABCG1 was reconstituted in liposome of various lipid compositions, and the ATPase activity was analyzed. ABCG1 reconstituted in egg lecithin showed ATPase activity (150 nmol/min/mg), which was inhibited by beryllium fluoride. The ATPase activity of ABCG1, reconstituted in phosphatidylserine liposome, was stimulated by cholesterol and choline phospholipids (especially sphingomyelin), and the affinity for cholesterol was increased by the addition of sphingomyelin. These results suggest that ABCG1 is an active lipid transporter and possesses different binding sites for cholesterol and sphingomyelin, which may be synergistically coupled.

Published

2013

9. THE SULFONYLUREA RECEPTOR: AN ABCC TRANSPORTER THAT ACTS AS AN ION CHANNEL REGULATOR

Author

Timothy J. Ryder, Kazumitsu Ueda, Frances M. Ashcroft, and Michinori Matsuo

Subjects

TRPC1, R-type calcium channel, endocrine system, biology, Biochemistry, ATP synthase gamma subunit, Protein subunit, biology.protein, Sulfonylurea receptor, N-type calcium channel, Ion channel, ATP synthase alpha/beta subunits, Cell biology

Abstract

The sulfonylurea receptor (SUR) serves as the regulatory subunit of the ATP-sensitive potassium (K ATP ) channel, endowing it with the ability to respond to changes in cell metabolism. The K ATP channel is a hetero-octameric complex of four Kir6.x and four SUR subunits. Kir6.x belongs to the family of inwardly rectifying K channels and assembles into tetramers to form the channel. Binding of ATP to the intracellular domains of Kir6.x produces channel inhibition. Associated with each Kir6.x subunit is a regulatory subunit, the sulfonylurea receptor (SUR). SUR has two large intracellular domains, containing consensus sequences for nucleotide binding and hydrolysis, which are known as the nucleotide binding domains (NBDs). Interaction of Mg-nucleotides with these NBDs mediates activation of the K ATP channel. The SUR subunit also binds therapeutic drugs, such as the sulfonyl ureas, which inhibit K ATP channel activity, and the K ATP channel openers that stimulate channel activity. Kir6.2 serves as the pore-forming subunit, but it associates with different SUR subunits: for example, SUR1 in pancreas and brain, SUR2A in heart, and skeletal muscle and SUR2B in a variety of tissues including brain and smooth muscle. In some smooth muscles, the K ATP channel comprises Kir6.1 in association with SUR2B. This chapter focuses on the physiological role of the K ATP channel and how this is impaired in disease. It then discusses the molecular composition of the K ATP channel, and details its regulation by nucleotides, metabolism and other signaling molecules. Finally, what is known of the pharmacological properties of the channel is summarized.

Published

2003

10. CONTRIBUTORS

Author

Rando Allikmets, Shlomo Almashanu, Frances M. Ashcroft, Susan E. Bates, Bettina E. Bauer, Houssain Benabdelhak, Mark A. Blight, Piet Borst, Richard Callaghan, Olivier Chambenoit, Geoffrey A. Chang, Sixue Chen, Giovanna Chimini, Susan P.C. Cole, Yunhai Cui, Elie Dassa, Michael Dean, Roger G. Deeley, Andrea de Lima Pimenta, Christopher Fielding, Markus Geisler, Martina Gentzsch, John W. Hanrahan, Christopher F. Higgins, I. Barry Holland, Dietrich Keppler, Ian D. Kerr, Gyula Kispal, Markus Klein, Jörg König, Wil N. Konings, Karl Kuchler, Brigitte Lankat-Buttgereit, Danielle Légaré, Roland Lill, Kenneth J. Linton, Enrico Martinoia, Michinori Matsuo, Anne T. Nies, Ronald Oude Elferink, Marc Ouellette, Mingsheng Peng, Gerrit J. Poelarends, Bert Poolman, Philip A. Rea, Glen Reid, John R. Riordan, Mark F. Rosenberg, Christopher B. Roth, Jean-Marie Ruysschaert, Timothy Ryder, Andrey Rzhetsky, Tohru Saeki, Rocío Sánchez-Fernández, Balázs Sarkadi, Lutz Schmitt, Erwin Schneider, Christoph Schüller, Frances J. Sharom, Robert Tampé, Gábor E. Tusnády, Kazumitsu Ueda, David Valle, Tiemen van der Heide, Gerrit van Meer, Hendrik W. van Veen, András Váradi, Koen H.G. Verschueren, Catherine Vigano, Peter Wielinga, Anthony J. Wilkinson, Joanne Young, and Noam Zelcer

Published

2003