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Jorge Oscanoa

Researcher at Queen Mary University of London

Publications -  5
Citations -  246

Jorge Oscanoa is an academic researcher from Queen Mary University of London. The author has contributed to research in topics: Web server & Biobank. The author has an hindex of 2, co-authored 3 publications receiving 132 citations.

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SNPnexus: assessing the functional relevance of genetic variation to facilitate the promise of precision medicine.

TL;DR: SNPnexus has now integrated rich resources from ENCODE and Roadmap Epigenomics Consortium to map and annotate the noncoding variants onto different classes of regulatory regions and nonCoding RNAs as well as providing their predicted functional impact from eight popular non-coding variant scoring algorithms and computational methods.
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SNPnexus: a web server for functional annotation of human genome sequence variation (2020 update).

TL;DR: The scope for data annotation has been substantially expanded to enhance biological interpretations of queried variants and this includes the addition of pathway analysis for the identification of enriched biological pathways and molecular processes.
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Dynamic Biobanking for Advancing Breast Cancer Research

TL;DR: The Breast Cancer Now Tissue Bank at the Barts Cancer Institute as discussed by the authors is an exemplar of a dynamic biobanking ecosystem that hosts and links longitudinal biospecimens and multimodal data including electronic health records, genomic and imaging data, offered alongside integrated data sharing and analytics tools.
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902 Development of a web-based platform to facilitate research to uncover the skin ageing mechanism

TL;DR: In this paper , a health informatics/bioinformatics platform for skin aging focused on a sub-set of the Nagahama cohort with molecular data and scores for over 20 clinical traits is presented.
Posted ContentDOI

SNPnexus COVID: Facilitating the analysis of COVID-19 host genetics

TL;DR: SNP-nexus COVID is a cutting-edge web-based analytical platform that allows researchers to analyse and interpret the functional implications of genetic variants in COVID-19 patient genomes and to prioritise those that demonstrate clinical utility for the prevention, management and/or treatment of CO VID-19.