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Defining the Substrate Specificity Determinants Recognized by the Active Site of C-Terminal Src Kinase-Homologous Kinase (CHK) and Identification of beta-Synuclein as a Potential CHK Physiological Substrate

机译：确定C末端src激酶同源激酶（CHK）活性位点识别的底物特异性决定因子和作为潜在CHK生理底物的β-突触核蛋白的鉴定

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C-Terminal Src kinase-homologous kinase (CHK) exerts its tumor suppressor function by phosphorylating the C-terminal regulatory tyrosine of the Src-family kinases (SFKs). The phosphorylation suppresses their activity and oncogenic action. In addition to phosphorylating SFKs, CHK also performs non-SFK-related functions by phosphorylating other cellular protein substrates. To define these non-SFK-related functions of CHK, we used the "kinase substrate tracking and elucidation" method to search for its potential physiological substrates in rat brain cytosol. Our search revealed β-synuclein as a potential CHK substrate, and Y127 in β-synuclein as the preferential phosphorylation site. Using peptides derived from β-synuclein and positional scanning combinatorial peptide library screening, we defined the optimal substrate phosphorylation sequence recognized by the CHK active site to be E-x-[Φ/E/D]-Y-Φ-x-Φ, where Φ and x represent hydrophobic residues and any residue, respectively. Besides β-synuclein, cellular proteins containing motifs resembling this sequence are potential CHK substrates. Intriguingly, the CHK-optimal substrate phosphorylation sequence bears little resemblance to the C-terminal tail sequence of SFKs, indicating that interactions between the CHK active site and the local determinants near the C-terminal regulatory tyrosine of SFKs play only a minor role in governing specific phosphorylation of SFKs by CHK. Our results imply that recognition of SFKs by CHK is mainly governed by interactions between motifs located distally from the active site of CHK and determinants spatially separate from the C-terminal regulatory tyrosine in SFKs. Thus, besides assisting in the identification of potential CHK physiological substrates, our findings shed new light on how CHK recognizes SFKs and other protein substrates.

机译：C末端Src激酶同源激酶（CHK）通过磷酸化Src家族激酶（SFK）的C端调节酪氨酸发挥其肿瘤抑制功能。磷酸化抑制了它们的活性和致癌作用。除了磷酸化SFK外，CHK还可以通过磷酸化其他细胞蛋白底物来执行与SFK不相关的功能。为了定义CHK的这些与SFK不相关的功能，我们使用“激酶底物跟踪和阐明”方法在大鼠脑细胞溶胶中搜索其潜在的生理底物。我们的搜索显示β-突触核蛋白是潜在的CHK底物，而β-突触核蛋白中的Y127是优先的磷酸化位点。使用衍生自β-突触核蛋白的肽和位置扫描组合肽库筛选，我们将CHK活性位点识别的最佳底物磷酸化序列定义为Ex- [Φ/ E / D]-Y-Φ-x-Φ，其中Φ和x分别代表疏水性残基和任何残基。除β-突触核蛋白外，含有类似于该序列的基序的细胞蛋白是潜在的CHK底物。有趣的是，CHK的最佳底物磷酸化序列与SFK的C末端尾部序列几乎没有相似之处，这表明CHK活性位点与SFK的C末端调节酪氨酸附近的局部决定簇之间的相互作用仅在调控中起次要作用。 CHK对SFK的特定磷酸化作用。我们的结果表明，CHK对SFK的识别主要受CHK活性位点远端的基序与SFK中与C端调节酪氨酸在空间上分开的决定簇之间的相互作用所控制。因此，除了有助于识别潜在的CHK生理底物外，我们的发现还为CHK如何识别SFK和其他蛋白质底物提供了新的思路。

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orcid:0000-0002-2173-3452; orcid:0000-0003-0532-8331; orcid:0000-0002-4965-7148; Ia, KK; Jeschke, GR; Deng, Y; Kamaruddin, MA; Williamson, NA; Scanlon, DB; Culvenor, JG; Hossain, MI; Purcell, AW; Liu, S; Zhu, H-J; Catimel, B; Turk, BE; Cheng, H-C;
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年度 2011
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1. Defining the Substrate Specificity Determinants Recognized by the Active Site of C-Terminal Src Kinase-Homologous Kinase (CHK) and Identification of β-Synuclein as a Potential CHK Physiological Substrate [J] . Kim K. Ia†‡ Grace R. Jeschke Yang Deng Mohd Aizuddin Kamaruddin†‡ Nicholas A. Williamson‡ Denis B. Scanlon‡ Janetta G. Culvenor§ Mohammed Iqbal Hossain†‡ Anthony W. Purcell†‡ Sheng Liu Hong-Jian Zhu Bruno Catimel@ Benjamin E. Turk and Heung-Chin Chen Biochemisty . 2011,第31期

机译：定义由C端Src激酶-同源激酶（CHK）的活性位点识别的底物特异性决定子，并鉴定β-突触核蛋白作为潜在的CHK生理底物
2. Defining the Substrate Specificity Determinants Recognized by the Active Site of C-Terminal Src Kinase-Homologous Kinase (CHK) and Identification of β-Synuclein as a Potential CHK Physiological Substrate [J] . Kim K. Ia, Grace R. Jeschke, Yang Deng, Biochemistry . 2011,第31期

机译：定义由C-末端SRC激酶 - 同源激酶（CHK）的活性位点识别的底物特异性决定簇，以及鉴定β-突触核蛋白作为潜在的CHK生理基质
3. Csk-homologous kinase (Chk) is an efficient inhibitor of Src-family kinases but a poor catalyst of phosphorylation of their C-terminal regulatory tyrosine [J] . Gahana Advani, Ya Chee Lim, Bruno Catimel, Cell Communication and Signaling . 2017,第1期

机译：CSK - 同源激酶（CHK）是SRC-Family激酶的有效抑制剂，但其C末端调节酪氨酸的磷酸化催化剂差
4. Identification of Phosphorylation Sites in Chk2 Kinase [C] . Henry W. Rohrs, Ilan Geerlof-Vidavsky, Manolo D. Plasencia, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2013

机译：CHK2激酶中磷酸化位点的鉴定
5. Development of tools for phosphosite-specific kinase identification and discovery of phosphatase substrates [D] . Dedigama Arachchige, Pavithra. 2017

机译：开发用于磷酸位点特异性激酶鉴定和发现磷酸酶底物的工具
6. Defining the substrate specificity determinants recognized by the active site of C-terminal Src kinase-Homologous Kinase (CHK) and Identification of β-Synuclein as a Potential CHK Physiological Substrate [O] . Kim K. Ia, Grace R. Jeschke, Yang Deng, -1

机译：定义由C-末端SRC激酶 - 同源激酶（CHK）的活性位点识别的底物特异性决定簇以及作为潜在的CHK生理基质的β-突触核蛋白的鉴定
7. Defining the substrate specificity determinants recognized by the active site of C-terminal Src kinase-homologous kinase (CHK) and identification of beta-synuclein as a potential CHK physiological substrate [O] . Ia, K., Jeschke, G., Deng, Y., 2011

机译：确定C末端src激酶同源激酶（CHK）活性位点识别的底物特异性决定因子，并鉴定β-突触核蛋白作为潜在的CHK生理底物

Defining the Substrate Specificity Determinants Recognized by the Active Site of C-Terminal Src Kinase-Homologous Kinase (CHK) and Identification of beta-Synuclein as a Potential CHK Physiological Substrate

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