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Intracellular miRNA or siRNA delivery and function

机译:细胞内miRNA或siRNA递送和功能

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摘要

Nanocarrier-mediated delivery and release of short non-coding RNA (e.g., miRNA or siRNA) into the cells with subsequent suppression of the populations of some of the mRNAs and proteins is of interest in the context of the development of a new generation of drugs. Bearing in mind such applications, the author shows the specifics of the corresponding transient kinetics by using three generic models without and with feedback resulting in bistability in the gene expression. In the absence of feedback, the suppression of the mRNA and protein population is transient. In the case of bistable kinetics, non-coding RNA can induce transition from the initial steady state to another steady state. The duration of this transition can be much longer than the time scale characterizing the drop of the non-coding RNA population. Quantitatively, the effect of the delivered non-coding RNA on gene expression can be appreciable if the maximum non-coding RNA population in the cytoplasm is comparable to or above 1000. All these conclusions have been drawn on the basis of calculations performed with the kinetic parameters typical for human cells.
机译:纳米载流子介导的递送和释放到具有随后抑制某些MRNA和蛋白质的群体的细胞中的短的非编码RNA(例如,miRNA或siRNA)对新一代药物的发展的感兴趣。在介入这种应用中,作者通过使用三个通用模型来显示相应的瞬态动力学的细节,没有反馈,导致基因表达中的双稳态。在没有反馈的情况下,抑制mRNA和蛋白质群是短暂的。在双稳态动力学的情况下,非编码RNA可以诱导从初始稳态到另一个稳态的转变。这种转变的持续时间可以比表征非编码RNA群落的时间表长得多。定量地,如果细胞质中的最大未编码RNA群与1000以上的最大非编码RNA群,则可以明显地显着的递送的非编码RNA对基因表达的影响。根据随动力学进行的计算,已经绘制了所有这些结论人体细胞典型的参数。

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