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  1. 岐阜藥科大學紀要
  2. 43号(平成6年6月30日発行)

<Review>Biochemical Study on Nicotinic Acetylcholine Receptor

https://gifu-pu.repo.nii.ac.jp/records/9832
https://gifu-pu.repo.nii.ac.jp/records/9832
04137651-f777-46f4-acd1-bdb74a9f9d1c
名前 / ファイル ライセンス アクション
KJ00000073007.pdf KJ00000073007.pdf (1.5 MB)
Item type 紀要論文(ELS) / Departmental Bulletin Paper(1)
公開日 1994-06-30
タイトル
タイトル <Review>Biochemical Study on Nicotinic Acetylcholine Receptor
言語 en
言語
言語 eng
資源タイプ
資源タイプ識別子 http://purl.org/coar/resource_type/c_6501
資源タイプ departmental bulletin paper
ページ属性
内容記述タイプ Other
内容記述 P(論文)
著者名(英) NOMOTO, HIROSHI

× NOMOTO, HIROSHI

WEKO 24428

en NOMOTO, HIROSHI

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SHOJI, HIROKI

× SHOJI, HIROKI

WEKO 24694

en SHOJI, HIROKI

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HAYASHI, KYOZO

× HAYASHI, KYOZO

WEKO 24106

en HAYASHI, KYOZO

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著者所属(日)
値 岐阜薬科大学/岐阜薬科大学/岐阜薬科大学
著者所属(英)
言語 en
値 Department of Molecular Biology, Gifu Pharmaceutical University/Department of Molecular Biology, Gifu Pharmaceutical University/Department of Molecular Biology, Gifu Pharmaceutical University
抄録(英)
内容記述タイプ Other
内容記述 Nicotinic acetylcholine receptor (AChR) is a multisubunit membrane glycoprotein which functions as a ligand-triggered cation channel. Receptors from electric tissues and skeletal muscle have a molecular weight of approximately 290,000 as a monomer and are composed of four types of polypeptide chains which assemble into a heterologous α_2βγδ pentamer. We determined the carbohydrate structure of Torpedo AChR, which was the first determination for neurotransmitter receptors. About 70 % of the oligosaccharides of the AChR were of the high mannose-type, Man_9GlcNAc_2 and Man_8GlcNAc_2. These two types of oligosaccharides were distributed in all the subunits. The remaining were various kinds of complex-type oligosaccharides, existing mainly in the γ and δ subunits. The α and β subunits had only one carbohydrate chain each, while the γ and δ subunits had two and three carbohydrate chains, respectively. These glycosylation sites were identified by sequencing glycopeptides obtained by lectin-affinity chromatography. The participation of oligosaccharides in ligand-binding of AChR was examined using a newly developed binding assay. The sialic acids and high mannose-type oligosaccharides on AChR were found to be unnecessary for its ligand binding. Next we found that the β and δ subunits of Torpedo AChR were phosphorylated on their tyrosine residues. The level of the phosphorylation was enhanced by incubating the AChR-rich membrane fraction with cholinergic ligands. This suggests that cholinergic agonists physiologically regulate phosphorylation on tyrosine in vivo, which might be included in the desensitization mechanism of the receptor. We also examined the spatial relation of proteins surrounding AChR using Torpedo AChR-rich membrane fraction. Bifunctional crosslinkers revealed an intimate relation among the AChR γ subunit, 43-kD protein, and dystrophin. Finally, we found neurotoxin-binding activities in the su-pernatant fraction obtained by ultracentrifugation of a homogenate of the electric organ, which usually does not contain AChR. This new activity was different in nature from AChR, and could function as a regulator or a modulator for AChR function.
雑誌書誌ID
収録物識別子タイプ NCID
収録物識別子 AN00053514
書誌情報 岐阜藥科大學紀要
en : The annual proceedings of Gifu College of Pharmacy

巻 43, p. 19-41, 発行日 1994-06-30
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