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单碱基损伤和错配改变 DNA 的骨架构象动力学。

Single-Base Lesions and Mismatches Alter the Backbone Conformational Dynamics in DNA.

机构信息

Department of Chemistry, Missouri State University, 901 South National Avenue, Springfield, Missouri 65897, United States.

Department of Chemistry and Biochemistry, University of San Diego, San Diego, California 92110, United States.

出版信息

Biochemistry. 2021 Mar 23;60(11):873-885. doi: 10.1021/acs.biochem.0c00784. Epub 2021 Mar 10.

Abstract

DNA damage has been implicated in numerous human diseases, particularly cancer, and the aging process. Single-base lesions and mismatches in DNA can be cytotoxic or mutagenic and are recognized by a DNA glycosylase during the process of base excision repair. Altered local dynamics and conformational properties in damaged DNAs have previously been suggested to assist in recognition and specificity. Herein, we use solution nuclear magnetic resonance to quantify changes in BI-BII backbone conformational dynamics due to the presence of single-base lesions in DNA, including uracil, dihydrouracil, 1,-ethenoadenine, and T:G mismatches. Stepwise changes to the %BII and Δ of the BI-BII dynamic equilibrium compared to those of unmodified sequences were observed. Additionally, the equilibrium skews toward endothermicity for the phosphates nearest the lesion/mismatched base pair. Finally, the phosphates with the greatest alterations correlate with those most relevant to the repair of enzyme binding. All of these results suggest local conformational rearrangement of the DNA backbone may play a role in lesion recognition by repair enzymes.

摘要

DNA 损伤与许多人类疾病有关,特别是癌症和衰老过程。DNA 中的单碱基损伤和错配可能具有细胞毒性或致突变性,并在碱基切除修复过程中被 DNA 糖苷酶识别。先前已经提出,损伤 DNA 中局部动力学和构象特性的改变有助于识别和特异性。在此,我们使用溶液核磁共振来量化 DNA 中单碱基损伤(包括尿嘧啶、二氢尿嘧啶、1, -乙烯腺嘌呤和 T:G 错配)存在时 BI-BII 骨架构象动力学的变化。与未修饰序列相比,观察到 BI-BII 动态平衡的 %BII 和 Δ 呈逐步变化。此外,最接近损伤/错配碱基对的磷酸的平衡向吸热方向倾斜。最后,变化最大的磷酸与最相关的酶结合修复的磷酸相关。所有这些结果表明,DNA 骨架的局部构象重排可能在修复酶识别损伤中起作用。

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