The Role of Protein Kinase C in the Transient Association of p57, a Coronin Family Actin-Binding Protein, with Phagosomes
スポンサーリンク
概要
- 論文の詳細を見る
Phagocytosis of opsonized zymosan (OpZ) particles by differentiated cells of the human leukemic cell line HL-60 induced transient periphagosomal association of p57, a coronin family actin-binding protein, and F-actin with dissociation from the phagosomes after ingestion was completed. Coincident with OpZ ingestion, p57 phosphorylation increased transiently and peaked with its dissociation from phagosomes. Since p57 contains several putative sites for protein kinase C (PKC) phosphorylation, we examined the effect of PKC on p57 phosphorylation and association with the phagosome. Purified p57 was phosphorylated in vitro by PKC isoforms α and δ, and PMA, an activator of PKC, induced p57 phosphorylation in HL-60 cells. Furthermore, chelerythrine, a specific PKC inhibitor, blocked p57 phosphorylation and the dissociation of p57 and F-actin from phagosomes, whereas wortmannin, genistein, and H-89 did not. Chelerythrine also inhibited the translocation of LAMP-1, a marker protein of lysosomes, to the OpZ-containing phagosomes, indicating that PKC-mediated phosphorylation is required for phagosome-lysosome fusion. Taken together, these data suggest that PKC-mediated phosphorylation of p57 triggers its dissociation from phagosomes, an event that may be necessary for the fusion of phagosomes with lysosomes.
- 公益社団法人日本薬学会の論文
- 2002-07-01
著者
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鈴木 和美
Showa College of Pharmaceutical Sciences
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Suzuki Kazutoshi
放射線医学総合研究所分子イメージング研究センター
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Suzuki K
Pharmaceutical Frontier Research Laboratories Japan Tobacco Inc.
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Suzuki Kenji
Suntory Institute For Biomedical Research Wakayamadai
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Suzuki K
Noda Research Laboratories Drug Delivery System Institute Ltd.:(present Address)pharmaceutics Resear
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Nakajin Shizuo
Department of Biochemistry, Hoshi University School of Pharmacy and Pharmaceutical Sciences
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Kato Shingo
Research Center Hospital For Charged Particle Therapy National Institute Of Radiological Sciences
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OKU Teruaki
Department of Biochemistry, Hoshi University
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TOYOSHIMA Satoshi
Pharmaceuticals and Medical Devices Evaluation Center National Institute of Health Sciences
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Oku Teruaki
Department Of Microbiology Hoshi University School Of Pharmacy And Pharmaceutical Sciences
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Oku Teruaki
Department Of Microbiology School Of Pharmacy Hoshi University
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SUZUKI Kensuke
Pharmaceutical Frontier Research Laboratories, Japan Tobacco, Inc.
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NAKAJIN Shizuo
Hoshi University School of Pharmacy and Pharmaceutical Sciences
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ITOH Saotomo
Department of Biochemistry, Hoshi University
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NISHIHATA Jun
Pharmaceutical Frontier Research Laboratories; Japan Tobacco Inc.
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IWASA Mitsusada
Department of Biochemistry, Hoshi University
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NAUSEEF William
Inflammation Program and Department of Medicine, University of Iowa
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Suzuki Kazutoshi
Department Of Medical Imaging National Institute Of Radiological Sciences
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Suzuki Kazutoshi
Clinical Neuroimaging Section Department Of Molecular Neuroimaging Molecular Imaging Center National
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Suzuki Kensuke
Pharmaceutical Frontier Research Laboratories Japan Tobacco Inc.
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Toyoshima S
Department Of Biochemistry Faculty Of Pharmaceutical Sciences Hoshi University
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Toyoshima S
Pharmaceuticals And Medical Devices Agency
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Toyoshima Satoshi
Pharmaceutical And Medical Devices Evaluation Center National Institute Of Health Science
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Suzuki K
Molecular Imaging Center National Institute Of Radiological Sciences
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Oku T
Amagasaki Chemical Industries Co.
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Nakajin S
Hoshi University School Of Pharmacy And Pharmaceutical Sciences
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Nakajin Shizuo
Department Of Biochemistry Faculty Of Pharmaceutical Sciences Hoshi University
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Iwasa Mitsusada
Department Of Biochemistry Hoshi University
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Nauseef William
The Inflammation Program And Department Of Medicine University Of Iowa And Veterans Affairs Medical
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Itoh Saotomo
Department Of Microbiology Hoshi University School Of Pharmacy And Pharmaceutical Sciences
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Sakane T
St. Marianna Univ. School Of Medicine Kanagawa Jpn
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