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细菌和人类来源的修饰 69 号螺旋 RNA 类似物的构象和稳定性比较。

Comparison of solution conformations and stabilities of modified helix 69 rRNA analogs from bacteria and human.

机构信息

Department of Chemistry, Wayne State University, Detroit, MI 48202, USA.

出版信息

Biopolymers. 2012 Feb;97(2):94-106. doi: 10.1002/bip.21706. Epub 2011 Aug 19.

Abstract

The helix 69 (H69) region of the large subunit (28S) ribosomal RNA (rRNA) of Homo sapiens contains five pseudouridine (Ψ) residues out of 19 total nucleotides, three of which are highly conserved. In this study, the effects of this abundant modified nucleotide on the structure and stability of H69 were compared with those of uridine in double-stranded (stem) regions. These results were compared with previous hairpin (stem plus single-stranded loop) studies to understand the contributions of the loop sequences to H69 structure and stability. The role of a loop nucleotide substitution from an A in bacteria (position 1918 in Escherichia coli 23S rRNA) to a G in eukaryotes (position 3734 in H. sapiens 28S rRNA) was examined. Thermodynamic parameters for the duplex RNAs were obtained through UV melting studies, and differences in the modified and unmodified RNA structures were examined by circular dichroism spectroscopy. The overall folded structure of human H69 appears to be similar to the bacterial RNA, consistent with the idea that ribosome structure and function are highly conserved; however, our results reveal subtle differences in structure and stability between the bacterial and human H69 RNAs in both the stem and loop regions. These findings may be significant with respect to H69 as a potential drug target site.

摘要

人类大亚基(28S)核糖体 RNA(rRNA)的螺旋 69(H69)区域包含 19 个总核苷酸中的 5 个假尿嘧啶核苷(Ψ)残基,其中 3 个高度保守。在这项研究中,与双链(茎)区域中的尿嘧啶相比,研究了这种丰富的修饰核苷酸对 H69 结构和稳定性的影响。将细菌(大肠杆菌 23S rRNA 中的位置 1918)中一个环核苷酸取代为腺嘌呤(位置 3734)的 loop 序列的作用与以前的发夹(茎加单链环)研究进行了比较,以了解 loop 序列对 H69 结构和稳定性的贡献。通过紫外光解研究获得了双链 RNA 的热力学参数,并通过圆二色性光谱检查了修饰和未修饰 RNA 结构的差异。人 H69 的整体折叠结构似乎与细菌 RNA 相似,这与核糖体结构和功能高度保守的观点一致;然而,我们的结果揭示了细菌和人 H69 RNA 在茎和环区域的结构和稳定性之间的细微差异。这些发现对于 H69 作为潜在的药物靶标位点可能具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f2c/3269404/4fafb1292e5b/nihms339174f1.jpg

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