README.md
In patrickCNMartin/ChIPanalyser: ChIPanalyser: Predicting Transcription Factor Binding Sites
ChIPanalyser
ChIPanalyser
ChIPanalyser: Predicting Transcription Factor Binding Sites
Authors
Patrick C.N. Martin pcnmartin@gmail.com
and
Dr. Nicolae Radu Zabet nzabet@essex.ac.uk
Description
Based on a statistical thermodynamic framework, ChIPanalyser
tries to produce ChIP-seq like profile.
The model relies on four consideration:
TF binding sites can be scored using a Position weight Matrix,
DNA accessibility plays a role in Transcription Factor binding,
binding profiles are dependant on the number of transcription
factors bound to DNA and finally binding energy
(another way of describing PWM's) or binding specificity should be
modulated (hence the introduction of a binding specificity modulator).
The end result of ChIPanalyser is to produce profiles simulating
real ChIP-seq profile and provide accuracy measurements
of these predicted profiles after being compared to real ChIP-seq data.
The ultimate goal is to produce ChIP-seq like profiles predicting ChIP-seq
like profile to circumvent the need to produce costly ChIP-seq experiments.
References
Zabet NR, Adryan B (2015) Estimating binding properties of transcription
factors from genome-wide binding profiles. Nucleic Acids Res., 43, 84–94.
Patrick C.N. Martin and Nicolae Radu Zabe (2020) Dissecting the binding mechanisms of transcription factors to DNA using a statistical thermodynamics framework. CSBJ, 18, 3590-3605.
patrickCNMartin/ChIPanalyser documentation built on Nov. 24, 2022, 12:02 a.m.
R Package Documentation
Browse R Packages
We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
ChIPanalyser
ChIPanalyser
ChIPanalyser: Predicting Transcription Factor Binding Sites
Authors
Patrick C.N. Martin pcnmartin@gmail.com
and
Dr. Nicolae Radu Zabet nzabet@essex.ac.uk
Description
Based on a statistical thermodynamic framework, ChIPanalyser tries to produce ChIP-seq like profile. The model relies on four consideration: TF binding sites can be scored using a Position weight Matrix, DNA accessibility plays a role in Transcription Factor binding, binding profiles are dependant on the number of transcription factors bound to DNA and finally binding energy (another way of describing PWM's) or binding specificity should be modulated (hence the introduction of a binding specificity modulator). The end result of ChIPanalyser is to produce profiles simulating real ChIP-seq profile and provide accuracy measurements of these predicted profiles after being compared to real ChIP-seq data. The ultimate goal is to produce ChIP-seq like profiles predicting ChIP-seq like profile to circumvent the need to produce costly ChIP-seq experiments.
References
Zabet NR, Adryan B (2015) Estimating binding properties of transcription factors from genome-wide binding profiles. Nucleic Acids Res., 43, 84–94.
Patrick C.N. Martin and Nicolae Radu Zabe (2020) Dissecting the binding mechanisms of transcription factors to DNA using a statistical thermodynamics framework. CSBJ, 18, 3590-3605.
R Package Documentation
Browse R Packages
We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
Embedding an R snippet on your website
Add the following code to your website.
For more information on customizing the embed code, read Embedding Snippets.