Computational Biochemistry/Bioinformatics, University of Bayreuth, Universitätsstr., Bayreuth, Germany.
J Mol Biol. 2011 Jun 10;409(3):450-65. doi: 10.1016/j.jmb.2011.03.061. Epub 2011 Apr 6.
The bacterial enzyme aminoglycoside phosphotransferase(3')-IIIa (APH) confers resistance against a wide range of aminoglycoside antibiotics. In this study, we use the Gaussian network model to investigate how the binding of nucleotides and antibiotics influences the dynamics and thereby the ligand binding properties of APH. Interestingly, in NMR experiments, the dynamics differ significantly in various APH complexes, although crystallographic studies indicate that no larger conformational changes occur upon ligand binding. Isothermal titration calorimetry also shows different thermodynamic contributions to ligand binding. Formation of aminoglycoside-APH complexes is enthalpically driven, while the enthalpic change upon aminoglycoside binding to the nucleotide-APH complex is much smaller. The differential effects of nucleotide binding and antibiotic binding to APH can be explained theoretically by single-residue fluctuations and correlated motions of the enzyme. The surprising destabilization of β-sheet residues upon nucleotide binding, as seen in hydrogen/deuterium exchange experiments, shows that the number of closest neighbors does not fully explain residue flexibility. Additionally, we must consider correlated motions of dynamic protein domains, which show that not only connectivity but also the overall protein architecture is important for protein dynamics.
细菌酶氨基糖苷磷酸转移酶(3')-IIIa(APH)赋予了对抗广泛的氨基糖苷类抗生素的抗性。在这项研究中,我们使用高斯网络模型来研究核苷酸和抗生素的结合如何影响 APH 的动力学,从而影响配体结合特性。有趣的是,尽管晶体学研究表明配体结合时不会发生较大的构象变化,但在各种 APH 复合物的 NMR 实验中,动力学差异非常明显。等温滴定量热法也显示出配体结合的不同热力学贡献。氨基糖苷-APH 复合物的形成是焓驱动的,而氨基糖苷与核苷酸-APH 复合物结合时的焓变要小得多。核苷酸结合和抗生素结合对 APH 的不同影响可以通过单残基波动和酶的相关运动从理论上解释。正如氢/氘交换实验中所看到的,核苷酸结合后β-折叠残基的惊人失稳表明,最近邻的数量并不能完全解释残基的柔韧性。此外,我们还必须考虑动态蛋白质结构域的相关运动,这表明不仅连接性,而且整体蛋白质结构对于蛋白质动力学也很重要。
