Synthesis and activity of an octapeptide inhibitor designed for SARS coronavirus main proteinase.

Gan YR; Huang H; Huang YD; Rao CM; Zhao Y; Liu JS; Wu L; Wei DQ

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Synthesis and activity of an octapeptide inhibitor designed for SARS coronavirus main proteinase.

机译：设计用于SARS冠状病毒主要蛋白酶的八肽抑制剂的合成和活性。

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The outbreak of SARS, a life-threatening disease, has spread over many countries around the world. So far there is no effective drug for the treatment of SARS. Stimulated by the binding mechanism of SARS-CoV Mpro with the octapeptide AVLQSGFR reported recently as well as the "Chou's distorted key" theory, we synthesized the octapeptide AVLQSGFR for conducting various biochemical experiments to investigate the antiviral potential of the octapeptide against SARS coronavirus (BJ-01). The results demonstrate that, compared with other compounds reported so far, AVLQSGFR is the most active in inhibiting replication of the SARS coronavirus, and that no detectable toxicity is observed on Vero cells under the condition of experimental concentration.

机译：SARS是一种威胁生命的疾病，已在世界许多国家蔓延。到目前为止，还没有有效的药物可以治疗SARS。受最近报道的SARS-CoV Mpro与八肽AVLQSGFR的结合机制以及“周氏扭曲键”理论的刺激，我们合成了八肽AVLQSGFR以进行各种生化实验，以研究八肽对SARS冠状病毒（BJ）的抗病毒潜力-01）。结果表明，与迄今报道的其他化合物相比，AVLQSGFR在抑制SARS冠状病毒复制方面最活跃，在实验浓度条件下对Vero细胞未观察到可检测的毒性。

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来源
《Peptides: An International Journal》 |2006年第4期|共4页
作者
Gan YR; Huang H; Huang YD; Rao CM; Zhao Y; Liu JS; Wu L; Wei DQ;
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原文格式 PDF
正文语种 eng
中图分类基础医学;
关键词
Synthesis; Endopeptidases; g lt; 3gt; experiment;

机译：合成;内肽酶;g 3;实验;

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1. Synthesis and activity of an octapeptide inhibitor designed for SARS coronavirus main proteinase. [J] . Gan YR, Huang H, Huang YD, Peptides: An International Journal . 2006,第4期

机译：设计用于SARS冠状病毒主要蛋白酶的八肽抑制剂的合成和活性。
2. Generation of predictive pharmacophore model for SARS-coronavirus main proteinase. [J] . Zhang XW, Yap YL, Altmeyer RM European Journal of Medicinal Chemistry: Chimie Therapeutique . 2005,第1期

机译：SARS冠状病毒主要蛋白酶的预测药效团模型的生成。
3. An efficient method for the synthesis of peptide aldehyde libraries employed in the discovery of reversible SARS coronavirus main protease (SARS-CoV M-pro) inhibitors [J] . Al-Gharabli SI, Shah STA, Weik S, Chembiochem: A European journal of chemical biology . 2006,第7期

机译：发现可逆SARS冠状病毒主要蛋白酶（SARS-CoV M-pro）抑制剂时采用的合成醛醛肽库的有效方法
4. Structure Activity Relationship Study of SARS Coronavirus 3CL Protease Inhibitors with an Electrophilic Aryl Ketone Structure [C] . Sho Konno, Kiyohiko Nakada, Rie Kakiuchi Japanese peptide symposium . 2011

机译：SARS Coronavirus 3CL蛋白酶抑制剂用电泳芳基酮结构的结构活性关系研究
5. Total synthesis of platensimycin and platencin and design and synthesis of SARS coronavirus chymotrypsin-like protease inhibitors. [D] . Xi, Kai. 2009

机译：板霉素和板霉素的全合成以及SARS冠状病毒胰凝乳蛋白酶样蛋白酶抑制剂的设计和合成。
6. Synthesis and activity of an octapeptide inhibitor designed for SARS coronavirus main proteinase [O] . Yi-Ru Gan, He Huang, Yong-Dong Huang, -1

机译：设计用于SARS冠状病毒主要蛋白酶的八肽抑制剂的合成和活性
7. Synthesis and activity of an octapeptide inhibitor designed for SARS coronavirus main proteinase [O] . Yi-Ru Gan, He Huang, Yong-Dong Huang, 2006

机译：用于SARS Coronavirus主要蛋白酶蛋白酶的八肽抑制剂的合成与活性

Synthesis and activity of an octapeptide inhibitor designed for SARS coronavirus main proteinase.

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