A general and flexible method for signal extraction from single-cell RNA-seq data

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作者
Davide Risso
Fanny Perraudeau
Svetlana Gribkova
Sandrine Dudoit
Jean-Philippe Vert
机构
[1] Weill Cornell Medicine,Division of Biostatistics and Epidemiology, Department of Healthcare Policy and Research
[2] University of California,Division of Biostatistics, School of Public Health
[3] Université Paris Diderot,Laboratoire de Probabilités et Modèles Aléatoires
[4] University of California,Department of Statistics
[5] PSL Research University,CBIO
[6] Institut Curie,Centre for Computational Biology, MINES ParisTech
[7] INSERM U900,Department of Mathematics and Applications
[8] Ecole Normale Supérieure,undefined
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摘要
Single-cell RNA-sequencing (scRNA-seq) is a powerful high-throughput technique that enables researchers to measure genome-wide transcription levels at the resolution of single cells. Because of the low amount of RNA present in a single cell, some genes may fail to be detected even though they are expressed; these genes are usually referred to as dropouts. Here, we present a general and flexible zero-inflated negative binomial model (ZINB-WaVE), which leads to low-dimensional representations of the data that account for zero inflation (dropouts), over-dispersion, and the count nature of the data. We demonstrate, with simulated and real data, that the model and its associated estimation procedure are able to give a more stable and accurate low-dimensional representation of the data than principal component analysis (PCA) and zero-inflated factor analysis (ZIFA), without the need for a preliminary normalization step.
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