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使用位置特异性序列决定因素预测碱基编辑结果。

Predicting base editing outcomes using position-specific sequence determinants.

机构信息

Wellcome Sanger Institute, Hinxton, UK.

Center for Integrative Genomics, University of Lausanne, Lausanne, Switzerland.

出版信息

Nucleic Acids Res. 2022 Apr 8;50(6):3551-3564. doi: 10.1093/nar/gkac161.

Abstract

CRISPR/Cas base editors promise nucleotide-level control over DNA sequences, but the determinants of their activity remain incompletely understood. We measured base editing frequencies in two human cell lines for two cytosine and two adenine base editors at ∼14 000 target sequences and find that base editing activity is sequence-biased, with largest effects from nucleotides flanking the target base. Whether a base is edited depends strongly on the combination of its position in the target and the preceding base, acting to widen or narrow the effective editing window. The impact of features on editing rate depends on the position, with sequence bias efficacy mainly influencing bases away from the center of the window. We use these observations to train a machine learning model to predict editing activity per position, with accuracy ranging from 0.49 to 0.72 between editors, and with better generalization across datasets than existing tools. We demonstrate the usefulness of our model by predicting the efficacy of disease mutation correcting guides, and find that most of them suffer from more unwanted editing than pure outcomes. This work unravels the position-specificity of base editing biases and allows more efficient planning of editing campaigns in experimental and therapeutic contexts.

摘要

CRISPR/Cas 碱基编辑器有望实现对 DNA 序列的核苷酸水平控制,但它们的活性决定因素仍不完全清楚。我们在两种人类细胞系中测量了两种胞嘧啶碱基编辑器和两种腺嘌呤碱基编辑器在约 14000 个靶序列上的碱基编辑频率,发现碱基编辑活性具有序列偏向性,靶碱基侧翼的核苷酸影响最大。碱基是否被编辑强烈依赖于其在靶位和前一个碱基的位置组合,作用是扩大或缩小有效编辑窗口。特征对编辑率的影响取决于位置,序列偏向性的有效性主要影响窗口中心以外的碱基。我们利用这些观察结果训练机器学习模型来预测每个位置的编辑活性,编辑之间的准确率在 0.49 到 0.72 之间,并且比现有工具具有更好的跨数据集泛化能力。我们通过预测疾病突变校正指南的功效来展示我们模型的实用性,发现它们中的大多数比纯结果有更多的不需要的编辑。这项工作揭示了碱基编辑偏差的位置特异性,并允许在实验和治疗背景下更有效地规划编辑活动。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a13/8989541/7df380cecb3b/gkac161fig1.jpg

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