GnomXMiss: AlphaMissense variants enriched with annotations from gnomAD, VEP, and ClinVar
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File descriptions
GnomXMiss per-protein files
<uniprot_id>_GnomXMiss.tsv
Files contain missense variants for a UniProt canonical protein from the original Alphamissense data dump, enriched with:
gnomAD allele frequencies (overall + subpopulation-specific)
VEP annotations (GENCODE v46)
ClinVar variant metadata
These files are sorted by residue_number and include substitutions that were present in the AlphaMissense hg38 missense data dump and for which matching genomic coordinates could be retrieved in the gnomad.joint.v4.1.sites.ht table, enriched with external annotations where available.
Column descriptions
Below is the full set of columns that appear across the *_GnomXMiss.tsv files
🔹 Primary identifiers
uniprot_id
Canonical UniProtKB accession for the protein associated with the variant.
#CHROM
Chromosome name (e.g., chr1, chr2, chrX, chrY) based on GRCh38.
POS
1-based genomic coordinate of the variant (GRCh38).
REF, ALT
Reference and alternate nucleotides from gnomAD.
🔹 Protein-level variant information
protein_variant
Amino-acid substitution in the format <RefAA><Position><AltAA>, e.g. V600E.Derived from AlphaMissense or imputed using VEP when missing.
residue_number
Integer position of the substitution extracted from protein_variant.
🔹 AlphaMissense annotation
am_class
Classification of variant pathogenicity:
likely_benign
ambiguous
likely_pathogenic
am_pathogenicity
Calibrated AlphaMissense pathogenicity score (0–1).
(Exact integration pipeline described in Zenodo README.)
🔹 ClinVar annotations (if available)
existing_variation
ClinVar or dbSNP IDs extracted via Ensembl VEP.
clinvar_significance
e.g., Benign, Likely_pathogenic, VUS, etc.
clinvar_condition
Name(s) of associated disease conditions.
clinvar_disease_id
Disease database identifiers (MEDGEN, MONDO, OMIM, etc.).
clinvar_variant_id
ClinVar Variation ID.
🔹 gnomAD allele frequency data (v4)
These fields are derived from the joint gnomAD v4 release and represent population-level statistics (no individual data).
Overall
allele_count
allele_number
allele_frequency
homozygote_count
Population-specific allele frequencies
The dataset includes AF values for multiple ancestry groups:
nfe_allele_frequency — Non-Finnish European
fin_allele_frequency — Finnish
afr_allele_frequency — African/African American
eas_allele_frequency — East Asian
sas_allele_frequency — South Asian
amr_allele_frequency — Latino/Admixed American
ami_allele_frequency — Amish
asj_allele_frequency — Ashkenazi Jewish
mid_allele_frequency — Middle Eastern
remaining_allele_frequency — Remaining ancestry group
Sex-specific allele frequencies
XX_allele_frequency
XY_allele_frequency
📜 Copyright & Licensing
1. Copyright (this dataset)
All processed data files in this deposit (*_GnomXMiss.tsv) and all accompanying scripts are released under:
Creative Commons Attribution 4.0 International (CC-BY-4.0)© 2025 Chataigner Lucas
You are free to:
Share and Adapt
Under the terms:
Attribution must be given to the original authors and sources (see below).
This work is provided “AS IS” with no warranty.
2. Attribution for Upstream Sources
This dataset is a derived work built from several openly licensed public resources.No raw datasets are redistributed, only derived, merged annotations.
AlphaMissense (DeepMind)
Source predictions © DeepMind Technologies LimitedLicensed under Creative Commons Attribution 4.0 International (CC-BY-4.0).You must cite:
Cheng et al. Accurate proteome-wide missense variant effect prediction with AlphaMissense.CC-BY-4.0.https://doi.org/10.1038/s41586-023-06668-0
AlphaMissense licensing and disclaimer apply:“Not intended for clinical use.”
gnomAD (Broad Institute / gnomAD Consortium)
This deposit includes derived allele frequency statistics only extracted from the gnomAD v4 joint release.gnomAD is licensed under CC-BY-4.0.Citation:
Karczewski et al. The mutational constraint spectrum quantified using variation in 141,456 humans.Nature (2020). doi:10.1038/s41586-020-2308-7
No raw gnomAD data are redistributed.
ClinVar (NCBI / NIH / NLM)
ClinVar data are in the public domain (CC0).This deposit redistributes only derived annotations (significance, condition, disease IDs, variant IDs).
Citation:
Landrum et al. ClinVar: improving access to variant interpretations and supporting evidence.Nucleic Acids Research (2018). doi:10.1093/nar/gkx1153
NIH disclaimer applies:Not intended for clinical decision making.
Ensembl VEP & GENCODE
This dataset includes only VEP-derived annotations, not the software itself.VEP is © EMBL-EBI, distributed under GPLv3.GENCODE v46 transcript models are used for annotations.
Citations:
McLaren et al. The Ensembl Variant Effect Predictor. Genome Biology (2016).Frankish et al. GENCODE reference annotation for the human genome.
UniProt
UniProt identifiers are free to use and redistribute.
Citation:
UniProt Consortium. UniProt: the Universal Protein Knowledgebase. Nucleic Acids Research (2023).
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Zenodo创建时间:
2026-01-06



