肺炎克雷伯氏菌烯酰-ACP 还原酶(FabI)的结构和生化研究表明底物结合位点灵活。

IF 1.9 4区 生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY
Soumya Biswas, Anupam Patra, Prajita Paul, Namrata Misra, Gajraj Singh Kushwaha, Mrutyunjay Suar
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引用次数: 0

摘要

肺炎克雷伯氏菌(Klebsiella pneumoniae)是一种以抗生素耐药性而臭名昭著的细菌病原体,由于其发展多种药物耐药性的非凡能力,被各种公共卫生组织列入优先病原体名单。细菌脂肪酸生物合成途径-II(FAS-II)一直被认为是抗菌药物研发的治疗靶点。抑制 FAS-II 酶--烯酰-酰基载体蛋白还原酶 FabI,不仅能抑制细菌感染,还能逆转抗生素耐药性。在此,我们采用互补实验方法,包括生物化学、X 射线晶体学和分子动力学模拟研究,对肺炎克雷伯菌 FabI(KpFabI)进行了表征。生物物理研究表明,KpFabI 在溶液和晶体结构中都以四聚体分子组装的形式存在。酶动力学研究表明,KpFabI 对巴豆酰 CoA 和还原性辅助因子 NADH 具有独特的催化特性。底物的迈克尔斯-门顿常数(Km)值表明,与巴豆基 CoA 相比,KpFabI 对 NADH 的偏好更高。四聚体 apo KpFabI 的晶体结构折叠成典型的罗斯曼折叠,其中 β 链夹在α 螺旋之间。高度灵活的底物结合区位于四聚体组装的内部。KpFabI 与底物的热稳定性分析表明,这种灵活性主要是由辅助因子 NADH 稳定的。此外,分子动力学研究进一步证实,KpFabI 在底物结合位点具有高度柔性区域。这些发现共同证明了 KpFabI 底物结合位点的高度动态性,因此,这些信息对于发现针对肺炎克雷伯氏菌的特异性抑制剂至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Structural and Biochemical Studies on Klebsiella Pneumoniae Enoyl-ACP Reductase (FabI) Suggest Flexible Substrate Binding Site

Structural and Biochemical Studies on Klebsiella Pneumoniae Enoyl-ACP Reductase (FabI) Suggest Flexible Substrate Binding Site

Klebsiella pneumoniae, a bacterial pathogen infamous for antibiotic resistance, is included in the priority list of pathogens by various public health organizations due to its extraordinary ability to develop multidrug resistance. Bacterial fatty acid biosynthesis pathway-II (FAS-II) has been considered a therapeutic drug target for antibacterial drug discovery. Inhibition of FAS-II enzyme, enoyl-acyl carrier protein reductase, FabI, not only inhibits bacterial infections but also reverses antibiotic resistance. Here, we characterized Klebsiella pneumoniae FabI (KpFabI) using complementary experimental approaches including, biochemical, x-ray crystallography, and molecular dynamics simulation studies. Biophysical studies shows that KpFabI organizes as a tetramer molecular assembly in solution as well as in the crystal structure. Enzyme kinetics studies reveal a distinct catalytic property towards crotonyl CoA and reducing cofactor NADH. Michaelis-Menten constant (Km) values of substrates show that KpFabI has higher preference towards NADH as compared to crotonyl CoA. The crystal structure of tetrameric apo KpFabI folds into a classic Rossman fold in which β-strands are sandwiched between α-helices. A highly flexible substrate binding region is located toward the interior of the tetrameric assembly. Thermal stability assay on KpFabI with its substrate shows that the flexibility is primarily stabilized by cofactor NADH. Moreover, the molecular dynamics further supports that KpFabI has highly flexible regions at the substrate binding site. Together, these findings provide evidence for highly dynamic substrate binding sites in KpFabI, therefore, this information will be vital for specific inhibitors discovery targeting Klebsiella pneumoniae.

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来源期刊
The Protein Journal
The Protein Journal 生物-生化与分子生物学
CiteScore
5.20
自引率
0.00%
发文量
57
审稿时长
12 months
期刊介绍: The Protein Journal (formerly the Journal of Protein Chemistry) publishes original research work on all aspects of proteins and peptides. These include studies concerned with covalent or three-dimensional structure determination (X-ray, NMR, cryoEM, EPR/ESR, optical methods, etc.), computational aspects of protein structure and function, protein folding and misfolding, assembly, genetics, evolution, proteomics, molecular biology, protein engineering, protein nanotechnology, protein purification and analysis and peptide synthesis, as well as the elucidation and interpretation of the molecular bases of biological activities of proteins and peptides. We accept original research papers, reviews, mini-reviews, hypotheses, opinion papers, and letters to the editor.
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