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著作: [片山 将一]/Sueyoshi Noriyuki/Kameshita Isamu/Critical Determinants of Substrate Recognition by Cyclin-Dependent Kinase-like 5 (CDKL5)./[Biochemistry]

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EID
377995
EOID
1011449
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LastModified
2021年8月3日(火) 15:57:20
Operator
片山 将一
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片山 将一
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種別 必須 学術論文(審査論文)
言語 必須 英語
招待 推奨
審査 推奨
カテゴリ 推奨
共著種別 推奨
学究種別 推奨
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著者 必須
  1. 片山 将一([徳島大学.大学院医歯薬学研究部.薬学域.先端薬学教育研究プロジェクト]/[徳島大学.大学院医歯薬学研究部.薬学域.薬科学部門.生命薬学系.医薬品病態生化学])
    役割 任意
    貢献度 任意
    学籍番号 推奨
  2. (英) Sueyoshi Noriyuki
    役割 任意
    貢献度 任意
    学籍番号 推奨
  3. (英) Kameshita Isamu
    役割 任意
    貢献度 任意
    学籍番号 推奨
題名 必須

(英) Critical Determinants of Substrate Recognition by Cyclin-Dependent Kinase-like 5 (CDKL5).

副題 任意
要約 任意

(英) Cyclin-dependent kinase-like 5 (CDKL5) is a Ser/Thr protein kinase known to be associated with X-linked neurodevelopmental disorders. In a previous study, we identified amphiphysin 1 (Amph1) as a potential substrate for CDKL5 and identified a single phosphorylation site at Ser-293. In this study, we investigated the molecular mechanisms of substrate recognition by CDKL5 using Amph1 as a model substrate. Amph1 served as an efficient CDKL5 substrate, whereas Amph2, a structurally related homologue of Amph1, was not phosphorylated by CDKL5. The sequence around the Amph1 phosphorylation site is RPR(293)SPSQ, while the corresponding sequence in Amph2 is IPK(332)SPSQ. To define the amino acid sequence specificity of the substrate, various point mutants of Amph1 and Amph2 were prepared and phosphorylated by CDKL5. Both Amph2(I329R) and Amph1 served as efficient CDKL5 substrates, but Amph1(R290I) did not, indicating that the arginyl residue at the P -3 position is critical for substrate recognition. With regard to prolyl residues around the phosphorylation site of Amph1, Pro-291 at the P -2 position, but not Pro-294 at the P +1 position, is indispensable for phosphorylation by CDKL5. Phosphorylation experiments using various deletion mutants of Amph1 revealed that the proline-rich domain (PRD) (amino acids 247-315) alone was not phosphorylated by CDKL5. In contrast, Amph1(247-385), which comprised the PRD and CLAP domains, served as an efficient CDKL5 substrate. These results, taken together, suggest that both the phosphorylation site sequence (RPXSX) and the CLAP domain structure in Amph1 play crucial roles in recognition and phosphorylation by CDKL5.

キーワード 推奨
  1. (英) Animals
  2. (英) Electrophoresis, Polyacrylamide Gel
  3. (英) Glyceraldehyde-3-Phosphate Dehydrogenase (Phosphorylating)
  4. (英) Humans
  5. (英) Mice
  6. (英) Models, Biological
  7. (英) Nerve Tissue Proteins
  8. (英) Protein-Serine-Threonine Kinases
  9. (英) Substrate Specificity
発行所 推奨
誌名 必須 Biochemistry([アメリカ化学会])
(pISSN: 0006-2960, eISSN: 1520-4995)
ISSN 任意 1520-4995
ISSN: 0006-2960 (pISSN: 0006-2960, eISSN: 1520-4995)
Title: Biochemistry
Title(ISO): Biochemistry
Publisher: American Chemical Society
 (NLM Catalog  (Scopus  (CrossRef (Scopus information is found. [need login])
必須 54
必須 19
必須 2975 2987
都市 任意
年月日 必須 2015年 5月 5日
URL 任意
DOI 任意 10.1021/bi501308k    (→Scopusで検索)
PMID 任意 25905439    (→Scopusで検索)
CRID 任意
WOS 任意
Scopus 任意
評価値 任意
被引用数 任意
指導教員 推奨
備考 任意
  1. (英) PublicationType: Journal Article

  2. (英) PublicationType: Research Support, Non-U.S. Gov't