Waldsich Christina, Masquida Benoît, Westhof Eric, Schroeder Renée
Institute of Microbiology and Genetics, Vienna Biocenter, Dr. Bohrgasse 9, A-1030 Vienna, Austria.
EMBO J. 2002 Oct 1;21(19):5281-91. doi: 10.1093/emboj/cdf504.
Group I introns consist of two major structural domains, the P4-P6 and P3-P9 domains, which assemble through interactions with peripheral extensions to fold into an active ribozyme. To assess group I intron folding in vivo, we probed the structure of td wild-type and mutant introns using dimethyl sulfate. The results suggest that the majority of the intron population is in the native state in accordance with the current structural model, which was refined to include two novel tertiary contacts. The importance of the loop E motif in the P7.1-P7.2 extension in assisting ribozyme folding was deduced from modeling and mutational analyses. Destabilization of stem P6 results in a deficiency in tertiary structure formation in both major domains, while weakening of stem P7 only interferes with folding of the P3-P9 domain. The different impact of mutations on the tertiary structure suggests that they interfere with folding at different stages. These results provide a first insight into the structure of folding intermediates and suggest a putative order of events in a hierarchical folding pathway in vivo.
I 组内含子由两个主要结构域组成,即P4 - P6和P3 - P9结构域,它们通过与外围延伸部分相互作用进行组装,折叠成一个活性核酶。为了评估I组内含子在体内的折叠情况,我们使用硫酸二甲酯探测了td野生型和突变型内含子的结构。结果表明,根据当前的结构模型,大多数内含子群体处于天然状态,该模型经过完善,纳入了两个新的三级接触。通过建模和突变分析推断出P7.1 - P7.2延伸中的环E基序在协助核酶折叠方面的重要性。茎P6的不稳定导致两个主要结构域的三级结构形成不足,而茎P7的减弱仅干扰P3 - P9结构域的折叠。突变对三级结构的不同影响表明它们在不同阶段干扰折叠。这些结果首次深入了解了折叠中间体的结构,并暗示了体内分层折叠途径中可能的事件顺序。