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首页> 外文期刊>Bioorganic and medicinal chemistry >Novel thrombopoietin mimetic peptides bind c-Mpl receptor: Synthesis, biological evaluation and molecular modeling
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Novel thrombopoietin mimetic peptides bind c-Mpl receptor: Synthesis, biological evaluation and molecular modeling

机译:新型血小板生成素模拟肽结合C-MPL受体:合成,生物学评估和分子建模

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摘要

Thrombopoietin (TPO) acts in promoting the proliferation of hematopoietic stem cells and by initiating specific maturation events in megakaryocytes. Now, TPO-mimetic peptides with amino acid sequences unrelated to TPO are of considerable pharmaceutical interest. In the present paper, four new TPO mimetic peptides that bind and activate c-Mpl receptor have been identified, synthesized and tested by Dual-Luciferase reporter gene assay for biological activities. The molecular modeling research was also approached to understand key molecular mechanisms and structural features responsible for peptide binding with c-Mpl receptor. The results presented that three of four mimetic peptides showed significant activities. In addition, the molecular modeling approaches proved hydrophobic interactions were the driven positive forces for binding behavior between peptides and c-Mpl receptor. TPO peptide residues in P7, P13 and P7' positions were identified by the analysis of hydrogen bonds and energy decompositions as the key ones for benefiting better biological activities. Our data suggested the synthesized peptides have considerable potential for the future development of stable and highly active TPO mimetic peptides. (C) 2016 Elsevier Ltd. All rights reserved.
机译:血小板生成素(TPO)作用于促进造血干细胞的增殖,并通过在巨核细胞中启动特异性成熟事件。现在,具有与TPO无关的氨基酸序列的TPO模拟肽具有相当大的药物兴趣。在本文中,已经鉴定了结合和激活C-MPL受体的四种新的TPO模拟肽,由双荧光素酶报告基因测定进行生物活性合成和测试。还接近分子建模研究以了解负责肽与C-MPL受体结合的关键分子机制和结构特征。结果表明,四种模拟肽中的三种表现出显着的活性。此外,分子建模方法被证明是疏水相互作用是用于肽和C-MPL受体之间结合行为的驱动的正力。通过分析氢键和能量分解作为受益于更好的生物活性的关键活性的P7,P13和P7'位置中的TPO肽残基。我们的数据表明,合成的肽对未来的稳定和高活性TPO模拟肽的发展具有相当大的潜力。 (c)2016 Elsevier Ltd.保留所有权利。

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