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从单细胞RNA测序时间快照数据推断基因调控网络需要高阶矩。

Inferring gene regulatory networks from single-cell RNA-seq temporal snapshot data requires higher-order moments.

作者信息

Raharinirina N Alexia, Peppert Felix, von Kleist Max, Schütte Christof, Sunkara Vikram

机构信息

Mathematics of Complex Systems, Zuse Institute Berlin, 14195 Berlin, Germany.

Explainable A.I. for Biology, Zuse Institute Berlin, 14195 Berlin, Germany.

出版信息

Patterns (N Y). 2021 Aug 18;2(9):100332. doi: 10.1016/j.patter.2021.100332. eCollection 2021 Sep 10.

Abstract

Single-cell RNA sequencing (scRNA-seq) has become ubiquitous in biology. Recently, there has been a push for using scRNA-seq snapshot data to infer the underlying gene regulatory networks (GRNs) steering cellular function. To date, this aspiration remains unrealized due to technical and computational challenges. In this work we focus on the latter, which is under-represented in the literature. We took a systemic approach by subdividing the GRN inference into three fundamental components: data pre-processing, feature extraction, and inference. We observed that the regulatory signature is captured in the statistical moments of scRNA-seq data and requires computationally intensive minimization solvers to extract it. Furthermore, current data pre-processing might not conserve these statistical moments. Although our moment-based approach is a didactic tool for understanding the different compartments of GRN inference, this line of thinking-finding computationally feasible multi-dimensional statistics of data-is imperative for designing GRN inference methods.

摘要

单细胞RNA测序(scRNA-seq)在生物学领域已变得十分普遍。最近,人们一直在推动使用scRNA-seq快照数据来推断指导细胞功能的潜在基因调控网络(GRN)。迄今为止,由于技术和计算方面的挑战,这一愿望尚未实现。在这项工作中,我们关注的是后者,而这在文献中较少被提及。我们采用了一种系统的方法,将GRN推断细分为三个基本组成部分:数据预处理、特征提取和推断。我们观察到,调控特征是在scRNA-seq数据的统计矩中捕获的,并且需要计算密集型的最小化求解器来提取它。此外,当前的数据预处理可能无法保留这些统计矩。尽管我们基于矩的方法是理解GRN推断不同部分的一个教学工具,但这种思考方式——找到计算上可行的数据多维统计——对于设计GRN推断方法来说是必不可少的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e86f/8441581/e4f7aad4f80e/gr1.jpg

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