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了解在存在和不存在 AfPiwi 蛋白的情况下,锁核酸和 2'-O-甲基修饰对 miRNA-mRNA 对杂交热力学的影响。

Understanding the effect of locked nucleic acid and 2'-O-methyl modification on the hybridization thermodynamics of a miRNA-mRNA pair in the presence and absence of AfPiwi protein.

机构信息

Proteomics and Structural Biology Unit, CSIR-Institute of Genomics and Integrative Biology , Mall Road, Delhi 110 007, India.

出版信息

Biochemistry. 2014 Mar 18;53(10):1607-15. doi: 10.1021/bi401677d. Epub 2014 Mar 7.

Abstract

miRNAs are some of the key epigenetic regulators of gene expression. They act through hybridization with their target mRNA and modulate the level of respective proteins via different mechanisms. Various cancer conditions are known to be associated with up- and downregulation of the oncogenic and tumor suppressor miRNAs, respectively. The levels of aberrantly expressed oncogenic miRNAs can be downregulated in different ways. Similarly, restoration of tumor suppressor miRNAs to their normal levels can be achieved using miRNA mimics. However, the use of miRNA mimics is limited by their reduced biostability and function. We have studied the hybridization thermodynamics of the miRNA 26a (11-mer, including the seed sequence) guide strand with the mRNA (11-mer) target strand in the absence and presence of AfPiwi protein. We have also inserted locked nucleic acids (LNAs) and 2'-O-methyl-modified nucleotides into the guide strand, in a walk-through manner, to assess their effect on the binding efficiency between guide and target RNA. Insertion of LNA and 2'-O-methyl-modified nucleotides into the guide strand helped to strengthen the binding affinity irrespective of the position of insertion. However, in the presence of AfPiwi protein, these modifications reduced the binding affinity to different extents depending on the position of insertion. Insertion of a modification leads to an increase in the enthalpic contribution with an increased unfavorable entropic contribution, which negatively compensates for the higher favorable enthalpy.

摘要

miRNAs 是基因表达的主要表观遗传调控因子之一。它们通过与靶 mRNA 的杂交作用,并通过不同的机制调节相应蛋白质的水平。已知各种癌症情况与致癌和肿瘤抑制 miRNA 的上调和下调分别相关。异常表达的致癌 miRNA 的水平可以通过多种方式下调。同样,可以使用 miRNA 模拟物将肿瘤抑制 miRNA 恢复到正常水平。然而,miRNA 模拟物的使用受到其生物稳定性和功能降低的限制。我们已经研究了 miRNA 26a(11 -mer,包括种子序列)引导链与 mRNA(11-mer)靶链在不存在和存在 AfPiwi 蛋白时的杂交热力学。我们还以遍历的方式在引导链中插入了锁核酸(LNA)和 2'-O-甲基修饰的核苷酸,以评估它们对引导和靶 RNA 之间结合效率的影响。引导链中 LNA 和 2'-O-甲基修饰核苷酸的插入有助于增强结合亲和力,而与插入位置无关。然而,在 AfPiwi 蛋白存在的情况下,这些修饰根据插入位置的不同,在不同程度上降低了结合亲和力。插入修饰会导致焓贡献增加,同时不利的熵贡献增加,这会对更高的有利焓产生负面影响。

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