Design and synthesis of non-peptidic inhibitors for the Syk C-terminal SH2 domain based on structure-based in-silico screening.

Niimi T; Orita M; Okazawa-Igarashi M; Sakashita H; Kikuchi K; Ball E; Ichikawa A; Yamagiwa Y; Sakamoto S; Tanaka A; Tsukamoto S; Fujita S; Tatsuta K; Maeda Y; Chikauchi K

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Design and synthesis of non-peptidic inhibitors for the Syk C-terminal SH2 domain based on structure-based in-silico screening.

机译：基于基于结构的计算机筛选，设计和合成Syk C端SH2域的非肽类抑制剂。

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Structure-based in-silico screening was carried out for the Syk C-terminal SH2 domain. Fragments that could interact with the pY or pY+1 pockets were selected by our in-silico screening. After tethering two fragments bound to these pockets, we have designed and synthesized new compounds that show favorable interaction with the pY+3 pocket. One such compound, having a cyclohexylmalonic acid moiety identified as a novel potent phosphotyrosyl mimetic, exhibited an affinity comparable to that of the monophosphorylated ligand peptide.

机译：针对Syk C端SH2域进行了基于结构的计算机内筛选。通过我们的计算机筛选，选择了可能与pY或pY + 1口袋相互作用的片段。在将两个片段束缚在这些口袋上后，我们设计并合成了与pY + 3口袋具有良好相互作用的新化合物。具有环己基丙二酸部分被鉴定为新型有效的磷酸酪氨酰模拟物的一种这样的化合物表现出与单磷酸化的配体肽相当的亲和力。

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《Journal of Medicinal Chemistry》 |2001年第26期|共4页
作者
Niimi T; Orita M; Okazawa-Igarashi M; Sakashita H; Kikuchi K; Ball E; Ichikawa A; Yamagiwa Y; Sakamoto S; Tanaka A; Tsukamoto S; Fujita S; Tatsuta K; Maeda Y; Chikauchi K;
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正文语种 eng
中图分类药学;
关键词
Cyclohexanes; Enzyme Precursors; Malonates; Protein-Tyrosine Kinase; src Homology Domains; 环己烷类; 酶前体; 丙二酸盐类; 蛋白质酪氨酸激酶; src同源域;

机译：Cyclohexanes;Enzyme Precursors;Malonates;Protein-Tyrosine Kinase;src Homology Domains;环己烷类;酶前体;丙二酸盐类;蛋白质酪氨酸激酶;src同源域;

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1. Design and synthesis of non-peptidic inhibitors for the Syk C-terminal SH2 domain based on structure-based in-silico screening. [J] . Niimi T, Orita M, Okazawa-Igarashi M, Journal of Medicinal Chemistry . 2001,第26期

机译：基于基于结构的计算机筛选，设计和合成Syk C端SH2域的非肽类抑制剂。
2. Structure-based design of novel nonpeptide inhibitors of the Src SH2 domain: Phosphotyrosine mimetics exploiting multifunctional group replacement chemistry [J] . Sundaramoorthi R., Kawahata N., Yang MG., Biopolymers: Original Research on Biomolecules and Biomolecular Assemblies . 2003,第6期

机译：Src SH2域的新型非肽抑制剂的基于结构的设计：利用多功能基团替代化学的磷酸酪氨酸模拟物
3. Structure-based design of novel bicyclic nonpeptide inhibitors for the Src SH2 domain [J] . Shakespeare WC., Azimioara MD., Macek KJ., Journal of Medicinal Chemistry . 2000,第21期

机译：Src SH2域的新型双环非肽抑制剂的基于结构的设计
4. Structure-based design,synthesis,and surface plasmon resonance (SPR) detection of antagonists of the Grb2 SH2 domain [C] . Feng-Di T.Lung, Jia-Yin Tsai, Shu-Yie Wei, the International Peptide Symposium . 2001

机译：基于结构的设计，合成和表面等离子体共振（SPR）检测GRB2 SH2结构域的拮抗剂
5. Biophysical studies of the allosteric regulatory mechanism of Syk tandem SH2 domains interacting with immunoreceptor tyrosine-based activation motifs [D] . Feng, Chao. 2016

机译：Syk串联SH2域与基于免疫受体酪氨酸的激活基序相互作用的变构调节机制的生物物理研究。
6. Design and synthesis of a potential SH2 domain inhibitor bearing a stereodiversified 14-cis-enediol scaffold [O] . Christine Marian, Rong Huang, Richard F. Borch -1

机译：设计和合成轴承型14-CIS-己二醇支架的潜在SH2结构域抑制剂
7. Solution structure of the C-terminal SH2 domain of the human tyrosine kinase Syk complexed with a phosphotyrosine pentapeptide [O] . Narula SS, Yuan RW, Adams SE, 1995

机译：人酪氨酸激酶Syk C末端SH2结构域与磷酸酪氨酸五肽复合的溶液结构

Design and synthesis of non-peptidic inhibitors for the Syk C-terminal SH2 domain based on structure-based in-silico screening.

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