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基于 DNA 转座子的基因载体——进化驱动力的场景。

DNA transposon-based gene vehicles - scenes from an evolutionary drive.

机构信息

Department of Biomedicine, Aarhus University, Wilh, Meyers Allé 4, DK-8000, Aarhus C, Denmark.

出版信息

J Biomed Sci. 2013 Dec 9;20(1):92. doi: 10.1186/1423-0127-20-92.

Abstract

DNA transposons are primitive genetic elements which have colonized living organisms from plants to bacteria and mammals. Through evolution such parasitic elements have shaped their host genomes by replicating and relocating between chromosomal loci in processes catalyzed by the transposase proteins encoded by the elements themselves. DNA transposable elements are constantly adapting to life in the genome, and self-suppressive regulation as well as defensive host mechanisms may assist in buffering 'cut-and-paste' DNA mobilization until accumulating mutations will eventually restrict events of transposition. With the reconstructed Sleeping Beauty DNA transposon as a powerful engine, a growing list of transposable elements with activity in human cells have moved into biomedical experimentation and preclinical therapy as versatile vehicles for delivery and genomic insertion of transgenes. In this review, we aim to link the mechanisms that drive transposon evolution with the realities and potential challenges we are facing when adapting DNA transposons for gene transfer. We argue that DNA transposon-derived vectors may carry inherent, and potentially limiting, traits of their mother elements. By understanding in detail the evolutionary journey of transposons, from host colonization to element multiplication and inactivation, we may better exploit the potential of distinct transposable elements. Hence, parallel efforts to investigate and develop distinct, but potent, transposon-based vector systems will benefit the broad applications of gene transfer. Insight and clever optimization have shaped new DNA transposon vectors, which recently debuted in the first DNA transposon-based clinical trial. Learning from an evolutionary drive may help us create gene vehicles that are safer, more efficient, and less prone for suppression and inactivation.

摘要

DNA 转座子是原始的遗传元件,从植物到细菌和哺乳动物,它们已经在各种生物中定殖。通过进化,这些寄生元件通过复制和在转座酶蛋白的催化下在染色体位点之间重新定位,从而塑造了宿主基因组。DNA 转座元件不断适应基因组中的生活,自我抑制调节和防御性宿主机制可能有助于缓冲“切和粘贴”DNA 动员,直到积累的突变最终限制转座事件。利用重建的 Sleeping Beauty DNA 转座子作为强大的引擎,越来越多在人类细胞中具有活性的转座元件已经进入生物医学实验和临床前治疗,作为基因转移的多功能载体。在这篇综述中,我们旨在将驱动转座子进化的机制与我们在适应 DNA 转座子进行基因转移时所面临的现实和潜在挑战联系起来。我们认为,DNA 转座子衍生的载体可能携带其母元件固有的、潜在的限制特征。通过详细了解转座子从宿主定殖到元件增殖和失活的进化历程,我们可以更好地利用不同转座元件的潜力。因此,平行努力研究和开发不同但有效的转座子载体系统将有益于基因转移的广泛应用。深入的了解和巧妙的优化已经塑造了新的 DNA 转座子载体,这些载体最近在第一个基于 DNA 转座子的临床试验中首次亮相。从进化驱动力中学习可能有助于我们创造更安全、更高效、更不易受抑制和失活的基因载体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ee70/3878927/67694e383686/1423-0127-20-92-1.jpg

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