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吗啉代反义寡聚体:一种不依赖核糖核酸酶H的结构类型的情况

Morpholino antisense oligomers: the case for an RNase H-independent structural type.

作者信息

Summerton J

机构信息

Gene Tools, Corvallis, OR 97339, USA.

出版信息

Biochim Biophys Acta. 1999 Dec 10;1489(1):141-58. doi: 10.1016/s0167-4781(99)00150-5.

Abstract

RNase H-competent phosphorothioates (S-DNAs) have dominated the antisense field in large part because they offer reasonable resistance to nucleases, they afford good efficacy in cell-free test systems, they can be targeted against sites throughout the RNA transcript of a gene, and they are widely available from commercial sources at modest prices. However, these merits are counterbalanced by significant limitations, including: degradation by nucleases, poor in-cell targeting predictability, low sequence specificity, and a variety of non-antisense activities. In cell-free and cultured-cell systems where one wishes to block the translation of a messenger RNA coding for a normal protein, RNase H-independent morpholino antisense oligos provide complete resistance to nucleases, generally good targeting predictability, generally high in-cell efficacy, excellent sequence specificity, and very preliminary results suggest they may exhibit little non-antisense activity.

摘要

具有核糖核酸酶H活性的硫代磷酸酯(S-DNA)在很大程度上主导了反义领域,因为它们对核酸酶具有合理的抗性,在无细胞测试系统中具有良好的功效,可以靶向基因RNA转录本的各个位点,并且可以从商业来源以适中的价格广泛获得。然而,这些优点被显著的局限性所抵消,包括:被核酸酶降解、细胞内靶向预测性差、序列特异性低以及各种非反义活性。在无细胞和培养细胞系统中,若要阻断编码正常蛋白质的信使RNA的翻译,不依赖核糖核酸酶H的吗啉代反义寡核苷酸对核酸酶具有完全抗性,通常具有良好的靶向预测性、较高的细胞内功效、出色的序列特异性,并且非常初步的结果表明它们可能几乎没有非反义活性。

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