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Active-site protonation states in an Acyl-Enzyme intermediate of a Class A β-Lactamase with a Monobactam Substrate

机译：具有单环内酰胺底物的a类β-内酰胺酶的酰基 - 酶中间体的活性位点质子化状态

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The monobactam antibiotic aztreonam is used to treat cystic fibrosis patients with chronic pulmonary infections colonized by Pseudomonas aeruginosa strains expressing CTX-M extended-spectrum β-lactamases. The protonation states of active-site residues that are responsible for hydrolysis have been determined previously for the apo form of a CTX-M β-lactamase but not for a monobactam acyl-enzyme intermediate. Here we used neutron and high-resolution X-ray crystallography to probe the mechanism by which CTX-M extended-spectrum β-lactamases hydrolyze monobactam antibiotics. In these first reported structures of a class A β-lactamase in an acyl-enzyme complex with aztreonam, we directly observed most of the hydrogen atoms (as deuterium) within the active site. Although Lys 234 is fully protonated in the acyl intermediate, we found that Lys 73 is neutral. These findings are consistent with Lys 73 being able to serve as a general base during the acylation part of the catalytic mechanism, as previously proposed.

机译：单bactam抗生素氨曲南被用于治疗患有慢性肺部感染的囊性纤维化患者，所述慢性肺部感染由表达CTX-M超广谱β-内酰胺酶的铜绿假单胞菌菌株定殖。先前已经确定了CTX-Mβ-内酰胺酶的载脂蛋白形式而不是单bactam酰基酶中间体确定了负责水解的活性位点残基的质子化状态。在这里，我们使用中子和高分辨率X射线晶体学来探究CTX-M超广谱β-内酰胺酶水解单bactam抗生素的机理。在这些与氨曲南的酰基酶复合物中，A类β-内酰胺酶的首次报道结构中，我们直接观察到了活性位点中的大部分氢原子（如氘）。尽管Lys 234在酰基中间体中被完全质子化，但我们发现Lys 73是中性的。这些发现与Lys 73能够如先前所提出的那样在催化机理的酰化部分中用作一般碱是一致的。

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Vandavasi V.G.; Langan P.S.; Weiss K.L.; Parks J.M.; Cooper Jonathan B.; Ginell S.L.; Coates L.;
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1. Active-Site Protonation States in an Acyl-Enzyme Intermediate of a Class A beta-Lactamase with a Monobactam Substrate [J] . Vandavasi Venu Gopal, Langan Patricia S., Weiss Kevin L., Antimicrobial agents and chemotherapy. . 2017,第1期

机译：活性位点质量态在β-内酰胺酶的酰基酶中间体中，具有单离酰胺基材
2. Accumulation of acyl-enzyme intermediates during turnover of penicillins by the class A β-lactamase of Staphylococcus aureus PC1 [J] . R F Pratt, S J Murphy, T S McConnell The biochemical journal . 1988,第3期

机译：金黄色葡萄球菌PC1的A类β-内酰胺酶在青霉素更新过程中积累的酰基酶中间体
3. Active-site mutants of class B β-lactamases: substrate binding and mechanistic study [J] . C. Prosperi-Meys, D. de Seny, G. Llabres, Cellular and molecular life sciences: CMLS . 2002,第12期

机译：B类β-内酰胺酶活性位点突变体：底物结合和机理研究
4. MASS SPECTROMETRIC ANALYSIS OF POLYKETIDE BIOSYNTHESIS: FTICR-MS VERSUS LOW-RESOLUTION LC-MS FOR ANALYSIS OF ACTIVE-SITE BOUND INTERMEDIATES [C] . Christopher M. Rath, Shilah Bonnet, Kevin Renoylds, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2009

机译：聚酮化合物生物合成的质谱分析：FTICR-MS与低分辨率LC-MS分析，用于分析有源点结合的中间体
5. Active site studies of beta-lactamases and DD-peptidases: Part 1. Kinetic and thermodynamic evaluation of phosphonates as beta-lactamase inhibitors. Part 2. Peptide substrate specificity studies in DD-peptidases. [D] . Nagarajan, Rajesh. 2004

机译：β-内酰胺酶和DD-肽酶的活性部位研究：第1部分。作为β-内酰胺酶抑制剂的膦酸酯的动力学和热力学评估。第2部分。DD肽酶中的肽底物特异性研究。
6. Active-Site Protonation States in an Acyl-Enzyme Intermediate of a Class A β-Lactamase with a Monobactam Substrate [O] . Venu Gopal Vandavasi, Patricia S. Langan, Kevin L. Weiss, 2017

机译：A类β-内酰胺酶与Monobactam底物的酰基酶中间体中的活性位质子态。
7. Active-site protonation states in an Acyl-Enzyme intermediate of a Class A β-Lactamase with a Monobactam Substrate [O] . Vandavasi V.G., Langan P.S., Weiss K.L., 2016

机译：A类β-内酰胺酶的酰基酶中间体与Monobactam底物的活性位点质子化状态

Active-site protonation states in an Acyl-Enzyme intermediate of a Class A β-Lactamase with a Monobactam Substrate

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