Annotating Cancer-Related Variants at Protein–Protein Interface with Structure-PPi
Cita com:
hdl:2117/370820
Document typePart of book or chapter of book
Defense date2022
PublisherSpringer US
Rights accessOpen Access
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Abstract
A comprehensive analysis of germline and somatic variants requires complex computational approaches that combine next-generation sequencing (NGS)-based omics data with curated annotations from public repositories. Here, we describe Structure-PPi, which facilitates the analysis of cancer-related variants onto protein 3D structures, interaction interfaces, and other important functional sites (i.e., catalytic, ligand-binding, posttranslational modification). Our approach relies on features extracted from Interactome3D, UniProtKB, InterPro, APPRIS, dbNSFP, and COSMIC databases and provides complementary information to pathogenicity prediction methods. Thus, Structure-PPi helps in the discrimination of false-positive predictions and adds both mechanistic and biological insights into the role of variants in a given cancer. An online version of the tools is available at https://rbbt.bsc.es/StructurePPI/.
CitationVazquez, M.; Pons, T. Annotating Cancer-Related Variants at Protein–Protein Interface with Structure-PPi. A: Piscuoglio, S.; Ng, C.. "Variant Calling: Methods and Protocols". Humana, New York, NY: Springer US, 2022, p. 315-330.
Is part ofPart of the Methods in Molecular Biology book series (MIMB,volume 2493)
ISBN978-1-0716-2292-6
978-1-0716-2293-3
978-1-0716-2293-3
Publisher versionhttps://link.springer.com/protocol/10.1007/978-1-0716-2293-3_20
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StructurePPI - Methods - v2.3_CN_vTP_MV.pdf | 296,6Kb | View/Open |