Backbone 1H, 13C, and 15N chemical shift assignment for HIV-1 protease subtypes and multi-drug resistant variant MDR 769

Xi Huang; Ian Mitchelle S. de Vera; Angelo M. Veloro; James R. Rocca; Carlos Simmerling; Ben M. Dunn; Gail E. Fanucci

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Backbone 1H, 13C, and 15N chemical shift assignment for HIV-1 protease subtypes and multi-drug resistant variant MDR 769

机译：HIV-1蛋白酶亚型和耐多药变体MDR 769的骨干1H，13C和15N化学位移分配

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HIV-1 protease (HIV-1PR) is an essential drug target in the treatment of patients infected with HIV-1. Mutations are found to arise in over 38 of 99 amino acid sites in this protein in response to drug therapy or natural selection, where many are found combinations that alter enzyme kinetics or inhibitor susceptibility without a clear structural mechanism. In efforts to understand how these mutations alter the flexibility and dynamics of HIV-1PR, we report the backbone 1H, 13C, and 15N chemical shiftassignments for subtypes C, circulating recombinant form CRF01_AE and a multi-drug resistant variant MDR 769. These assignments are essential for future work aimed at characterizing backbone dynamics, exchange dynamics and dynamics of protein/substrateor protein/inhibitor interactions.

机译：HIV-1蛋白酶（HIV-1PR）是治疗感染HIV-1的患者的基本药物靶标。响应药物治疗或自然选择，发现该蛋白质中99个氨基酸位点中的超过38个位点发生了突变，其中发现了许多组合，这些组合改变了酶的动力学或抑制剂的敏感性而没有明确的结构机制。在努力了解这些突变如何改变HIV-1PR的灵活性和动态性的过程中，我们报告了C型亚型，循环重组形式CRF01_AE和多药耐药性MDR 769的骨架1H，13C和15N化学位移分配。这些分配是旨在表征骨干动力学，交换动力学和蛋白质/底物蛋白质/抑制剂相互作用的动力学的未来工作必不可少。

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《Biomolecular NMR assignments》 |2013年第2期|共4页
作者
Xi Huang; Ian Mitchelle S. de Vera; Angelo M. Veloro; James R. Rocca; Carlos Simmerling; Ben M. Dunn; Gail E. Fanucci;
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正文语种 eng
中图分类分子生物学;
关键词
HIV-1 protease; Naturally occurring polymorphism; Multi-drug resistance; Resonance assignments;

机译：HIV-1蛋白酶;自然发生的多态性;多药耐药性;共振分配;

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1. Backbone 1H, 13C, and 15N chemical shift assignment for HIV-1 protease subtypes and multi-drug resistant variant MDR 769 [J] . Xi Huang, Ian Mitchelle S. de Vera, Angelo M. Veloro, Biomolecular NMR assignments . 2013,第2期

机译：HIV-1蛋白酶亚型和耐多药变体MDR 769的骨干1H，13C和15N化学位移分配
2. Backbone and sidechain 1H, 13C and 15N chemical shift assignments of the hydrophobin MPG1 from the rice blast fungus Magnaporthe oryzae [J] . Anthony A. Rey, Antoine Hocher, Ann H. Kwan, Biomolecular NMR assignments . 2013,第1期

机译：稻瘟病菌Magnaporthe oryzae的疏水蛋白MPG1的骨架和侧链1H，13C和15N化学位移分配
3. 1H, 13C, and 15N backbone chemical shift assignments of StAR-related lipid transfer domain protein 5 (STARD5) [J] . Aurélien Lorin, Danny Létourneau, Andrée Lefebvre, Biomolecular NMR assignments . 2013,第1期

机译：StAR相关脂质转移域蛋白5（STARD5）的1H，13C和15N主链化学位移分配
4. SOLID-STATE 15N/1H CHEMICAL SHIFT CORRELATION EXPERIMENTS OF ALIGNED SAMPLES AT HIGH FIELDS [C] . . 2005

机译：高场校准样品的固态15N / 1H化学位移相关实验
5. Crystallographic, molecular dynamics, and enzymatic studies of multi-drug resistant HIV-1 protease and implications for structure based drug design (project 1); crystallographic studies of human myelin protein zero (project 2). [D] . Liu, Zhigang. 2011

机译：多药耐药HIV-1蛋白酶的晶体学，分子动力学和酶学研究及其对基于结构的药物设计的启示（项目1）；人髓磷脂蛋白零的晶体学研究（项目2）。
6. Backbone 1H 13C and 15N Chemical Shift Assignment for HIV-1 Protease Subtypes and Multi-Drug Resistant Variant MDR 769 [O] . Xi Huang, Ian Mitchelle S. de Vera, Angelo M. Veloro, -1

机译：HIV-1蛋白酶亚型和多毒性变体MDR 769的骨干1H13C和15N化学换档分配
7. 1H, 13C and 15N backbone chemical shift assignments of SARS-CoV-2 nsp3a [O] . Nicola Salvi, Luiza Mamigonian Bessa, Serafima Guseva, 2021

机译：SARS-COV-2 NSP3A的1H，13C和15N骨干化学转移分配

Backbone 1H, 13C, and 15N chemical shift assignment for HIV-1 protease subtypes and multi-drug resistant variant MDR 769

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