Post on 17-Jul-2015
Expression2KinasesMRNA PROFILING LINKED TO MULTIPLE UPSTREAM REGULATORY LAYERS
Rafael Diego Macho Reyes (b02marer@uco.es)
Summary
1. What is the X2K software?
2. Introduction: why do we need this new tool?
1. Work proposal.
3. Work flow.
4. Reviewed cases using X2K:
1. Recovering of drug-related pathways.
2. Obteining global views of cellular differentiation.
3. Unraveling regulatory mechanisms of breast cáncer.
4. Expression data from physiological process:
1. Liver fibrosis disease gene expression.
2. Hippocampal neurons development.
5. Perspectives.
6. References.
What is the X2K software?
It is software to identify, characterize and set new upstream proteinsrelated to gene expression.
http://www.maayanlab.net/X2K/documentation.html
2. Introduction:
why do we need this new tool?
Control
Treatments
Disease
Diferent times
There is always a variation within the expression of several genes,
but most of them have unknown functions in the context of a
gene network.
By a better knowledge on gene-protein networks:
1. We could improve culture and diferentiation techniques.
2. There would be able to have a better physiological
knowledge for each person, towards further indivudal
pharmacology.
KO experiments
Over-expression
3. Work flow
3. Work flow: gene differential expression.
Cluster A Cluster B Cluster C Cluster D Cluster E
3. Work flow: upstream TF ID.
Cluster C
Most likely
Transcription
Factors
• It considers variations into thechromatine under different conditions.
• DB = >36000 interactions + > 159 relationships (gene/protein)
ChEA
• It scans promotersequences.
Transfac(PWM)
• It is another PWM algorithm
analyzer.• PWMs algorithms have better number of
references in human and mice genes and TFs.
Jaspar
(PWM)
3. Work flow: connecting proteins to TFs.
• ENTREZ human references
• InteractomeDB.
Input
• It makes therelationship betweengenes and proteinswith “signalome” and “interactome”.
X2K (G2N)• Genes-
transcriptomemost suitableproteins list. (LIST)
Output
3. Work flow: connecting proteins-TFs to kinases.
•LIST
•Kinases Databases
•> 14000 interactions.
•> 3400 publications.
•>436 kinases
Input
• It compares and infersalso the most suitablekinases.
• It uses Fisher´s Test tohave more sharpenedanalysis.
X2K (KEA)•More suitable kinases
to phosphorilateprotein complexesrelated to TFs.
Output
3. Work flow
4.Reviewed cases using X2K:
Drug receptorsNetworks
X2K
Regulatormechanisms in breast cancer
subtypes
Gene expressionvariations
through celldiferentiation
Diferentiationof
hyppocampusareas
Gene expressionvariationsthroughhepatycfibrosis
Drug receptorsNetworks500 upstream genes
500 downstream genes
Results
Analysis
Kinases
TF Complexes
Transcription factors
Gene expressionvariations
through celldiferentiation
Embryo
Differentialgene
expression
Expressionmodules
TF and PseudoTF
activiy
GATE Software
Statisticanalysis
Results
Matrixes of Expression
Pij= maxM * Akj * Eij *Iij
Input
Output
Regulatormechanisms
in breastcancer
subtypes
Diferentiationof
hyppocampusareas
Gene expressionvariationsthroughhepatycfibrosis
Upregulating Proteins
Regulating proteins
Transcription factorsTcf3
Wnt4
RSK
Regulating proteins
Already confirmed
by bibliography
CamK4
CREB
5. Perspectives
1. This is a new rational approximation to the identification and ranking of upstream
regulating proteins in differential expression genes.
2. It can be widely useful to discover new drug-receptors, and new signaling networks in
different cell types and patients, giving an enormous step on individual pharmacology.
3. In a close future it would integrate new data from histone modifications, miRNA andpost-transcriptional modifications.
4. This technique is limited by the use of too many previous work and the assumption of the
Independence between targets and regulations.
References.
Chen, Xu, Gordonov, Lim, Perkins and Ma´ayan:
“Expression2Kinases: mRNA profiling linked to multiple upstream
regulatory layers”. Bioinformatics, 28, 1 (2012), 105-111.