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Visualizing Genomic Variation
Prof Jan Aerts

Faculty of Engineering - ESAT/STADIUS

iMinds Medical ICT Department

KU Leuven

!
jan.aerts@esat.kuleuven.be

http://visualanalyticsleuven.be
What is genomic variation?
transitions
transversions

“copy number variation”
Aerts & Tyler-Smith, In: Encyclopedia of Life Sciences, 2009
Effects of variation on phenotype
• change in protein abundance

• level of transcription or translation (loss/gain)

• stability

• change in protein structure (partly deleted, fusion genes, …)
What are we interested in?
•

multiple samples
•
•

•

show all affected genes (or functional units)
cluster individuals

functional effect of structural variation
•
•

•

gene-centric instead of positionally ordered: coordinate-free view
high-level annotations (pathways, GO-terms)

uncertainty (statistical & positional) and underlying evidence
DNA sequencing

QC

read mapping
variant calling
variant filtering

what is effect of variant?
check signal

QC
Single Nucleotide Polymorphisms
General approach: reference-based
UCSC

Ensembl
Variant View

sequence variants in gene context

Ferstay et al, IEEE InfoVis, 2013
Integrative Genome Viewer (IGV)
Sequence
logo
Sequence Diversity Diagram
Structural Variation
dotplot

Pevzner & Tessler, Genome Research, 2003
read depth information: arrayCGH and next-generation sequencing

Xie & Tammi, BMC Bioinformatics, 2009
next-generation sequencing: read-pair information

Medvedev, Nature Methods, 2009

Stephens et al, Cell, 2011
Integrate read-depth and read-pair information

Stephens et al, Cell, 2010

Meander

Pavlopoulos et al, Nucleic Acids Research, 2013
From data generation to data interpretation:
understanding the effect of structural variation
linearity of reference chromosome broken by structural variation, but still using
the reference for comparison


!

!
UCSC Genome Browser

=> domain expert needs to try and “wrap his head around” the data


=> need to lessen the cognitive load in interpretation: change a cognitive task
into a perceptual one
Nielsen & Wong, Nat Methods, 2012
represent the chromosome as it is in vivo (=~ FISH)

Feuk, Nature Reviews Genetics, 2006

reconstruct rearranged chromosome
based on graph structure of segments
breakpoint graph

Pevzner & Tessler, Genome Research, 2003
focus on functional impact - Pipit

Sakai et al, submitted
Challenges
Challenges
•

visual and interaction scalability
•

•

deep sequencing => very high depth per track

•

high-dimensional data: many tracks (n=98!)

•

•

genome size: HSA1 = 240Mb = 240,000 screens at 1pixel/bp = 72km

compare multiple samples

computational scalability
•

how to compute fast enough to make interactivity possible? (e.g. switching
between data resolutions)
Thank you
• Authors of papers mentioned

• Bioinformatics/Visual Analytics Leuven

• Ryo Sakai

• Raf Winand

• Thomas Boogaerts

• Toni Verbeiren

• Georgios Pavlopoulos

• Data Visualization Lab (datavislab.org)

• Erik Duval

• Andrew Vande Moere
33
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