*Motivation:* High-throughput nucleotide sequencing provides quantitative readouts in assays for RNA expression (RNA-Seq), protein-DNA binding (ChIP-Seq) or cell counting (barcode sequencing). Statistical inference of differential signal in such data requires estimation of their variability throughout the dynamic range. When the number of replicates is small, error modelling is needed to achieve statistical power.&#xd;&#xa;&#xd;&#xa;*Results:* We propose an error model that uses the negative binomial distribution, with variance and mean linked by local regression, to model the null distribution of the count data. The method controls type-I error and provides good detection power. &#xd;&#xa;&#xd;&#xa;*Availability:* A free open-source R software package, _DESeq_, is available from the Bioconductor project and from &#x22;http://www-huber.embl.de/users/anders/DESeq&#x22;:http://www-huber.embl.de/users/anders/DESeq

A Agresti

A Mortazavi

AC Cameron

AM Smith

AS Morrissy

B Langmead

C Loader

CI Bliss

DD Licatalosi

G Robertson

GK Smyth

I Lönnstedt

J Bullard

JC Marioni

JF Lawless

JS Bloom

K Saha

L Wang

L Whitaker

M Kasowski

MD Robinson

P Engström

P McCullagh

RC Gentleman

Simon Anders

SJ Clark

U Nagalakshmi

Wolfgang Huber

Y Benjamini

English

PubMed

Springer

Differential expression analysis for sequence count data

summary:Modern biology is interested in better understanding mechanisms within cells. For this purpose, products of cells like metabolites, peptides, proteins or mRNA are measured and compared under different conditions, for instance healthy cells vs. infected cells. Such experiments usually yield regulation or expression values – the abundance or absence of a cell product in one condition compared to another one – for a large number of cell products, but with only a few replicates. In order to distinguish random fluctuations and noise from true regulations, suitable significance tests are needed. Here we propose a simple model which is based on the assumption that the regulation factors follow normal distributions with different expected values, but with the same standard deviation. Before suitable significance tests can be derived from this model, a reliable estimation for the standard deviation in the context of many small samples is needed. We therefore also include a discussion on the properties of the sample MAD (Median Absolute Deviation from the median) and the sample standard deviation for small samples sizes

Klawonn, Frank

Czech digital mathematics library

Significance tests to identify regulated proteins based on a large number of small samples

Institute of Mathematics AS CR, v. v. i.

Springer - Publisher Connector

Nature Precedings

Bias-corrected maximum likelihood estimator of the negative binomial dispersion parameter.

Categorical Data Analysis.

Controlling the false discovery rate: a practical and powerful approach to multiple testing.

Core Team

edgeR: a Bioconductor package for dierential expression analysis of digital gene expression data.

Estimation of the negative binomial parameter  by maximum quasi-likelihood.

Fast and accurate computation of binomial probabilities. http://projects.scipy.org/scipy/rawattachment/ticket/620/loader2000Fast.pdf (Note: This is a copy of the original paper, which is no longer available online.).

Fitting the negative binomial distribution to biological data.

Generalized Linear Models. Chapman & Hall/CRC, 2nd edition.

Genome-wide pro of STAT1 DNA association using chromatin immunoprecipitation and massively parallel sequencing.

HITS-CLIP yields genomewide insights into brain alternative RNA processing.

Let fmq be a function that maps a true raw SCV value to the expectation of the estimate ^

Linear models and empirical bayes methods for assessing dierential expression in microarray experiments.

Local Regression and Likelihood.

Mapping and quantifying mammalian transcriptomes by RNA-Seq.

Moderated statistical tests for assessing dierences in tag abundance.

Negative binomial and mixed poisson regression.

Next-generation tag sequencing for cancer gene expression pro

On the Poisson law of small numbers.

Quantitative phenotyping via deep barcode sequencing.

Regression analysis of count data.

RNA-seq: An assessment of technical reproducibility and comparison with gene expression arrays.

Small-sample estimation of negative binomial dispersion, with applications to SAGE data.

Statistical inferences for isoform expression in RNA-Seq.

The transcriptional landscape of the yeast genome de by RNA sequencing.

Transcriptional characterization of glioblastoma stem cell lines using tag sequencing.

Crossref

A Language and Environment for Statistical Computing.

accurate computation of binomial probabilities. [http://projects. scipy.org/scipy/raw-attachment/ticket/620/loader2000Fast.pdf], (Note: This is a copy of the original paper, which is no longer available online.).

Bioconductor: Open software development for computational biology and bioinformatics.

Caudy AA: Measuring differential gene expression by short read sequencing: quantitative comparison to 2-channel gene expression microarrays.

Dudoit S: Evaluation of statistical methods for normalization and differential expression in mRNA-Seq experiments.

Estimation of the negative binomial parameter κ by maximum quasi-likelihood. Biometrics

GK: edgeR: a Bioconductor package for differential expression analysis of digital gene expression data. Bioinformatics

HTSeq: Analysing high-throughput sequencing data with Python.

Limma: linear models for microarray data. In Bioinformatics and Computational Biology Solutions Using R and Bioconductor. Edited by: Gentleman

Linear models and empirical Bayes methods for assessing differential expression in microarray experiments.

Local Regression and Likelihood Springer;

locfit: Local regression, likelihood and density estimation.

Mapping and quantifying mammalian transcriptomes by RNA-Seq. Nat Methods

Negative binomial and mixed Poisson regression.

Nelder JA: Generalized Linear Models.

Next-generation tag sequencing for cancer gene expression profiling. Genome Res

Nislow C: Quantitative phenotyping via deep barcode sequencing. Genome Res

On the Poisson law of small numbers. Biometrika

Oshlack A: A scaling normalization method for differential expression analysis of RNA-seq data. Genome Biol

RB: HITS-CLIP yields genome-wide insights into brain alternative RNA processing. Nature

S: Bias-corrected maximum likelihood estimator of the negative binomial dispersion parameter. Biometrics

S: Genome-wide profiles of STAT1 DNA association using chromatin immunoprecipitation and massively parallel sequencing. Nat Methods

SL: Ultrafast and memoryefficient alignment of short DNA sequences to the human genome. Genome Biol

Smyth GK: Moderated statistical tests for assessing differences in tag abundance. Bioinformatics

Smyth GK: Small-sample estimation of negative binomial dispersion, with applications to SAGE data. Biostatistics

Speed T: Replicated microarray data. Stat Sin

The transcriptional landscape of the yeast genome defined by RNA sequencing. Science

Trivedi PK: Regression Analysis of Count Data

Variation in transcription factor binding among humans. Science

Y: RNA-seq: An assessment of technical reproducibility and comparison with gene expression arrays. Genome Res

Zhang X: DEGseq: an R package for identifying differentially expressed genes from RNA-seq data. Bioinformatics

http://dml.cz/bitstream/handle/10338.dmlcz/142950/Kybernetika_48-2012-3_9.pdf

Differential expression analysis for sequence count data

Abstract

Similar works

Full text

Available Versions