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靶向Egr-1信使核糖核酸的新型脱氧核糖核酸酶可抑制损伤后血管平滑肌的增殖和再生。

New DNA enzyme targeting Egr-1 mRNA inhibits vascular smooth muscle proliferation and regrowth after injury.

作者信息

Santiago F S, Lowe H C, Kavurma M M, Chesterman C N, Baker A, Atkins D G, Khachigian L M

机构信息

Centre for Thrombosis and Vascular Research, The University of New South Wales and Prince of Wales Hospital, Sydney, Australia.

出版信息

Nat Med. 1999 Nov;5(11):1264-9. doi: 10.1038/15215.

Abstract

Early growth response factor-1 (Egr-1) binds to the promoters of many genes whose products influence cell movement and replication in the artery wall. Here we targeted Egr-1 using a new class of DNA-based enzyme that specifically cleaved Egr-1 mRNA, blocked induction of Egr-1 protein, and inhibited cell proliferation and wound repair in culture. The DNA enzyme also inhibited Egr-1 induction and neointima formation after balloon injury to the rat carotid artery wall. These findings demonstrate the utility of DNA enzymes as biological tools to delineate the specific functions of a given gene, and implicate catalytic nucleic acid molecules composed entirely of DNA as potential therapeutic agents.

摘要

早期生长反应因子-1(Egr-1)可与许多基因的启动子结合,这些基因的产物会影响动脉壁中的细胞运动和复制。在此,我们使用一类新型的基于DNA的酶靶向作用于Egr-1,该酶能特异性切割Egr-1 mRNA,阻断Egr-1蛋白的诱导,并抑制培养中的细胞增殖和伤口修复。这种DNA酶还能抑制大鼠颈动脉壁球囊损伤后的Egr-1诱导和新生内膜形成。这些发现证明了DNA酶作为一种生物学工具来描绘特定基因的特定功能的实用性,并表明完全由DNA组成的催化核酸分子作为潜在治疗剂的可能性。

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