SpliceAI: A deep learning-based tool to identify splice variants
Project description
SpliceAI: A deep learning-based tool to identify splice variants
This package annotates genetic variants with their predicted effect on splicing, as described in Jaganathan et al, Cell 2019 in press.
Update: The annotations for all possible substitutions, 1 base insertions, and 1-4 base deletions within genes are available here for download.
Installation
The simplest way to install SpliceAI is through pip or conda:
pip install spliceai
# or
conda install -c bioconda spliceai
Alternately, SpliceAI can be installed from the github repository:
git clone https://github.com/Illumina/SpliceAI.git
cd SpliceAI
python setup.py install
SpliceAI requires tensorflow>=1.2.0
, which is best installed separately via pip or conda (see the TensorFlow website for other installation options):
pip install tensorflow
# or
conda install tensorflow
Usage
SpliceAI can be run from the command line:
spliceai -I input.vcf -O output.vcf -R genome.fa -A grch37
# or you can pipe the input and output VCFs
cat input.vcf | spliceai -R genome.fa -A grch37 > output.vcf
Required parameters:
-I
: Input VCF with variants of interest.-O
: Output VCF with SpliceAI predictionsALLELE|SYMBOL|DS_AG|DS_AL|DS_DG|DS_DL|DP_AG|DP_AL|DP_DG|DP_DL
included in the INFO column (see table below for details). Only SNVs and simple INDELs (REF or ALT is a single base) within genes are annotated. Variants in multiple genes have separate predictions for each gene.-R
: Reference genome fasta file. Can be downloaded from GRCh37/hg19 or GRCh38/hg38.-A
: Gene annotation file. Can instead providegrch37
orgrch38
to use GENCODE V24 canonical annotation files included with the package. To create custom gene annotation files, usespliceai/annotations/grch37.txt
in repository as template.
Optional parameters:
-D
: Maximum distance between the variant and gained/lost splice site (default: 50).-M
: Mask scores representing annotated acceptor/donor gain and unannotated acceptor/donor loss (default: 0).
Details of SpliceAI INFO field:
ID | Description |
---|---|
ALLELE | Alternate allele |
SYMBOL | Gene symbol |
DS_AG | Delta score (acceptor gain) |
DS_AL | Delta score (acceptor loss) |
DS_DG | Delta score (donor gain) |
DS_DL | Delta score (donor loss) |
DP_AG | Delta position (acceptor gain) |
DP_AL | Delta position (acceptor loss) |
DP_DG | Delta position (donor gain) |
DP_DL | Delta position (donor loss) |
Delta score of a variant, defined as the maximum of (DS_AG, DS_AL, DS_DG, DS_DL), ranges from 0 to 1 and can be interpreted as the probability of the variant being splice-altering. In the paper, a detailed characterization is provided for 0.2 (high recall), 0.5 (recommended), and 0.8 (high precision) cutoffs. Delta position conveys information about the location where splicing changes relative to the variant position (positive values are downstream of the variant, negative values are upstream).
Examples
A sample input file and the corresponding output file can be found at examples/input.vcf
and examples/output.vcf
respectively. The output T|RYR1|0.00|0.00|0.91|0.08|-28|-46|-2|-31
for the variant 19:38958362 C>T
can be interpreted as follows:
- The probability that the position 19:38958360 (=38958362-2) is used as a splice donor increases by 0.91.
- The probability that the position 19:38958331 (=38958362-31) is used as a splice donor decreases by 0.08.
Similarly, the output CA|TTN|0.07|1.00|0.00|0.00|-7|-1|35|-29
for the variant 2:179415988 C>CA
has the following interpretation:
- The probability that the position 2:179415981 (=179415988-7) is used as a splice acceptor increases by 0.07.
- The probability that the position 2:179415987 (=179415988-1) is used as a splice acceptor decreases by 1.00.
Contact
Kishore Jaganathan: kishorejaganathan@gmail.com
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