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Crystal Structure andSpecific Binding Mode of Sisomicinto the Bacterial Ribosomal Decoding Site

机译:晶体结构与Sisomicin的特异性结合模式细菌核糖体解码位点

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摘要

Sisomicin with an unsaturated sugar ring I displays better antibacterial activity than other structurally related aminoglycosides, such as gentamicin, tobramycin, and amikacin. In the present study, we have confirmed by X-ray analyses that the binding mode of sisomicin is basically similar but not identical to that of the related compounds having saturated ring I. A remarkable difference is found in the stacking interaction between ring I and G1491. While the typical saturated ring I with a chair conformation stacks on G1491 through CH/π interactions, the unsaturated ring I of sisomicin with a partially planar conformation can share its π-electron density with G1491 and fits well within the A-site helix.
机译:具有不饱和糖环I的Sisomicin表现出比其他与结构相关的氨基糖苷(如庆大霉素,妥布霉素和丁胺卡那霉素)更好的抗菌活性。在本研究中,我们已经通过X射线分析证实,西索米星的结合模式与具有饱和环I的相关化合物的结合模式基本相似,但并不相同。在环I与G1491的堆叠相互作用中发现了显着差异。尽管具有椅构象的典型饱和环I通过CH /π相互作用堆积在G1491上,但具有部分平面构象的西索霉素的不饱和环I可以与G1491共享其π电子密度,并且非常适合A位螺旋。

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