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一种通用的深度学习模型可用于锌指设计,从而实现转录因子的重新编程。

A universal deep-learning model for zinc finger design enables transcription factor reprogramming.

机构信息

Institute for Systems Genetics, NYU Grossman School of Medicine, New York, NY, USA.

Department of Biochemistry and Molecular Pharmacology, NYU Grossman School of Medicine, New York, NY, USA.

出版信息

Nat Biotechnol. 2023 Aug;41(8):1117-1129. doi: 10.1038/s41587-022-01624-4. Epub 2023 Jan 26.

Abstract

CysHis zinc finger (ZF) domains engineered to bind specific target sequences in the genome provide an effective strategy for programmable regulation of gene expression, with many potential therapeutic applications. However, the structurally intricate engagement of ZF domains with DNA has made their design challenging. Here we describe the screening of 49 billion protein-DNA interactions and the development of a deep-learning model, ZFDesign, that solves ZF design for any genomic target. ZFDesign is a modern machine learning method that models global and target-specific differences induced by a range of library environments and specifically takes into account compatibility of neighboring fingers using a novel hierarchical transformer architecture. We demonstrate the versatility of designed ZFs as nucleases as well as activators and repressors by seamless reprogramming of human transcription factors. These factors could be used to upregulate an allele of haploinsufficiency, downregulate a gain-of-function mutation or test the consequence of regulation of a single gene as opposed to the many genes that a transcription factor would normally influence.

摘要

CysHis 锌指 (ZF) 结构域经过工程设计可与基因组中的特定靶序列结合,为可编程调控基因表达提供了一种有效策略,具有许多潜在的治疗应用。然而,ZF 结构域与 DNA 的结构复杂相互作用使得它们的设计具有挑战性。在这里,我们描述了对 490 亿个蛋白质-DNA 相互作用的筛选,以及开发了一种深度学习模型 ZFDesign,该模型可针对任何基因组靶标进行 ZF 设计。ZFDesign 是一种现代机器学习方法,可模拟由一系列文库环境引起的全局和目标特异性差异,并特别使用新颖的分层转换器架构考虑相邻手指的兼容性。我们通过无缝重编程人类转录因子,展示了设计 ZF 作为核酸酶以及激活子和抑制剂的多功能性。这些因子可用于上调单等位基因的杂合不足,下调功能获得性突变,或测试单个基因的调控后果,而不是转录因子通常会影响的许多基因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dcc8/10421740/f41ad7481572/41587_2022_1624_Fig1_HTML.jpg

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