Structural Basis of Antisickling Effects of Selected FDA Approved Drugs: A Drug Repurposing Study

Olubiyi Olujide O.; Olagunju Maryam O.; Oni James O.; Olubiyi Abidemi O.

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Structural Basis of Antisickling Effects of Selected FDA Approved Drugs: A Drug Repurposing Study

机译：选定的FDA批准药物抗皱效应的结构依据：一种药物重新调整研究

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Introduction: Sickle cell disease is characterized by a point mutation involving substitution of glutamic acid at position 6 to valine. Encoded in this hydrophobic mutation is both an intrinsic capacity for the beta globin molecules to assemble into thermodynamically favoured polymeric states as well as a rational way of interrupting the aggregation.

机译：介绍：镰状细胞疾病的特征在于涉及在6位谷氨酸替代谷氨酸的点突变。在这种疏水性突变中编码是β球蛋白分子组装成热力学最有利的聚合物状态的固有容量以及中断聚集的合理方式。

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《Current computer-aided drug design 》 |2018年第2期| 共11页
作者
Olubiyi Olujide O.; Olagunju Maryam O.; Oni James O.; Olubiyi Abidemi O.;
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作者单位

Obafemi Awolowo Univ Fac Pharm Dept Pharmaceut Chem Ife Nigeria;

Afe Babalola Univ Coll Sci Dept Biol Sci PMB 5454 Ado Ekiti Nigeria;

Afe Babalola Univ Coll Med &

Hlth Sci Dept Pharmacol &

Therapeut PMB 5454 Ado Ekiti Nigeria;

State Specialist Hosp Ikere Ekiti Nigeria;

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原文格式 PDF
正文语种 eng
中图分类药学 ;
关键词
Sickle cell; mutation; beta globin; pharmacophore models; antisickling; glutamic acid;

机译：镰状细胞;突变;β珠蛋白;药物团模型;反分辨率;谷氨酸;

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1. Structural Basis of Antisickling Effects of Selected FDA Approved Drugs: A Drug Repurposing Study [J] . Olubiyi Olujide O., Olagunju Maryam O., Oni James O., Current computer-aided drug design . 2018 ,第2期

机译：选定的FDA批准药物抗皱效应的结构依据：一种药物重新调整研究
2. Molecular docking, molecular dynamics and MM/PBSA studies of FDA approved drugs for protein kinase a of Mycobacterium tuberculosis; application insights of drug repurposing [J] . Shobana Sundar, Lokesh Thangamani, Gowdham Manivel, Informatics in Medicine Unlocked . 2019 ,第1期

机译：FDA批准的蛋白质激酶A的FDA批准药物的分子对接，分子动力学和MM / PBSA研究;药物重新施用的应用洞察
3. Drug repurposing screens reveal cell-type-specific entry pathways and FDA-approved drugs active against SARS-Cov-2 [J] . Mark Dittmar, Jae Seung Lee, Kanupriya Whig, Cell Reports . 2021 ,第1期

机译：药物修复筛查揭示了对针对SARS-COV-2有效的细胞类型特异性进入途径和FDA批准的药物
4. UHPLC-HRMS Method for Repurposing FDA Approved Drugs: Primaquine and its Metabolites as Anticancer Therapeutics [C] . Samantha M. Mahmoud, Dil Ramanathan American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2012

机译：用于修复FDA批准的药物的UHPLC-HRMS方法：原序及其代谢产物作为抗癌治疗方法
5. Molecular Determinants for Binding of the FDA-Approved Drugs in Proteins – A Data Mining and Advanced Quantum Chemical Study [D] . Alqahtani, Saad. 2017

机译：FDA批准的药物与蛋白质结合的分子决定因素–数据挖掘和先进的量子化学研究
6. Large-Scale Drug Screen Identifies FDA-Approved Drugs for Repurposing in Sickle-Cell Disease [O] . Matthew Cannon, Hannah Phillips, Sidney Smith, 2020

机译：大规模药物筛选识别FDA批准的药物用于在镰状细胞病中重新估算
7. Drug repurposing screens reveal FDA approved drugs active against SARS-Cov-2 [O] . Mark Dittmar, Jae Seung Lee, Kanupriya Whig, 2020

机译：药物修复屏幕揭示FDA批准的药物对抗SARS-COV-2
8. New Drug Approval: FDA Needs to Enhance Its Oversight of Drugs Approved on the Basis of Surrogate Endpoints [R] . 2009

机译：新药批准：FDa需要加强对基于代理终点批准的药物的监督

Structural Basis of Antisickling Effects of Selected FDA Approved Drugs: A Drug Repurposing Study

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