The interpretation of human genetic variation is one of the greatest challenges of modern genetics. New approaches are urgently needed to prioritize variants, especially those that are rare or lack a definitive clinical interpretation. We examined 10,136,597 human missense genetic variants from GnomAD, ClinVar and UniProt. We were able to perform large-scale atom-based mapping and phenotype interpretation of 3,960,015 of these variants onto 18,874 experimental and 84,818 in house predicted three-dimensional coordinates of the human proteome. We demonstrate that 14% of amino acid substitutions from the GnomAD database that could be structurally analysed are predicted to affect protein structure (n = 568,548, of which 566,439 rare or extremel...
BACKGROUND: The ever on-going technical developments in Next Generation Sequencing have led to an in...
Background: The phenotypic effects of sequence variations in protein-coding regions come about prima...
The incomplete identification of structural variants from whole-genome sequencing data limits studie...
Interpretation of the colossal number of genetic variants identified from sequencing applications is...
Inference of the structural and functional consequences of amino acid-altering missense variants is ...
The translation of personal genomics to precision medicine depends on the accurate interpretation of...
peer reviewedElucidating molecular consequences of amino-acid-altering missense variants at scale is...
The translation of personal genomics to precision medicine depends on the accurate interpretation of...
peer reviewedInterpretation of the colossal number of genetic variants identified from sequencing ap...
The translation of personal genomics to precision medicine depends on the accurate interpretation of...
Human genome sequencing efforts have greatly expanded, and a plethora of missense variants identifie...
While the first version of the human genome sequence was completed two decades ago, the understand...
Sequence variation data of the human proteome can be used to analyze 3D protein structures to derive...
Over the past fifty years, the genetic bases for many human diseases have been discovered. Genome-wi...
BACKGROUND: The widespread clinical application of genome-wide sequencing has resulted in many new d...
BACKGROUND: The ever on-going technical developments in Next Generation Sequencing have led to an in...
Background: The phenotypic effects of sequence variations in protein-coding regions come about prima...
The incomplete identification of structural variants from whole-genome sequencing data limits studie...
Interpretation of the colossal number of genetic variants identified from sequencing applications is...
Inference of the structural and functional consequences of amino acid-altering missense variants is ...
The translation of personal genomics to precision medicine depends on the accurate interpretation of...
peer reviewedElucidating molecular consequences of amino-acid-altering missense variants at scale is...
The translation of personal genomics to precision medicine depends on the accurate interpretation of...
peer reviewedInterpretation of the colossal number of genetic variants identified from sequencing ap...
The translation of personal genomics to precision medicine depends on the accurate interpretation of...
Human genome sequencing efforts have greatly expanded, and a plethora of missense variants identifie...
While the first version of the human genome sequence was completed two decades ago, the understand...
Sequence variation data of the human proteome can be used to analyze 3D protein structures to derive...
Over the past fifty years, the genetic bases for many human diseases have been discovered. Genome-wi...
BACKGROUND: The widespread clinical application of genome-wide sequencing has resulted in many new d...
BACKGROUND: The ever on-going technical developments in Next Generation Sequencing have led to an in...
Background: The phenotypic effects of sequence variations in protein-coding regions come about prima...
The incomplete identification of structural variants from whole-genome sequencing data limits studie...