Expanding the molecular glycophenotype ontology to include model organisms and acquired diseases

Jean Philippe Gourdine; Nicole Vasilevsky; Lilly Winfree; Matthew Brush; Melissa Haendel

Expanding the molecular glycophenotype ontology to include model organisms and acquired diseases

Jean Philippe Gourdine, Nicole Vasilevsky, Lilly Winfree, Matthew Brush, Melissa Haendel

Research output: Contribution to journal › Conference article › peer-review

Abstract

Glycans are an underappreciated class of molecules despite the fact that they are implicated in more than 100 known diseases. We have developed an ontology model that captures glycan abnormalities at the molecular level (glycophenotypes) called the molecular glycophenotype ontology (MGPO). Only 30% of known glycosyltransferases have been implicated in human genetic disorders of glycosylation. Ortholog glycosyltransferases from model organism can cover relevant biological information on potential human diseases. Thus, extending MGPO to represent additional phenotypes and support annotation of model organism data will help cross-species comparison. Expansion of MGPO will also include annotation of glycophenotypes from acquired diseases.

Original language	English (US)
Journal	CEUR Workshop Proceedings
Volume	2285
State	Published - 2018
Event	9th International Conference on Biological Ontology, ICBO 2018 - Corvallis, United States Duration: Aug 7 2018 → Aug 10 2018

Keywords

Diseases
Glycans
Glycophenotypes
Model organisms

ASJC Scopus subject areas

General Computer Science

Cite this

@article{189062bf54654ed9808a58c3ece85a71,

title = "Expanding the molecular glycophenotype ontology to include model organisms and acquired diseases",

abstract = "Glycans are an underappreciated class of molecules despite the fact that they are implicated in more than 100 known diseases. We have developed an ontology model that captures glycan abnormalities at the molecular level (glycophenotypes) called the molecular glycophenotype ontology (MGPO). Only 30% of known glycosyltransferases have been implicated in human genetic disorders of glycosylation. Ortholog glycosyltransferases from model organism can cover relevant biological information on potential human diseases. Thus, extending MGPO to represent additional phenotypes and support annotation of model organism data will help cross-species comparison. Expansion of MGPO will also include annotation of glycophenotypes from acquired diseases.",

keywords = "Diseases, Glycans, Glycophenotypes, Model organisms",

author = "Gourdine, {Jean Philippe} and Nicole Vasilevsky and Lilly Winfree and Matthew Brush and Melissa Haendel",

note = "Publisher Copyright: {\textcopyright} 2018 CEUR-WS.; 9th International Conference on Biological Ontology, ICBO 2018 ; Conference date: 07-08-2018 Through 10-08-2018",

year = "2018",

language = "English (US)",

volume = "2285",

journal = "CEUR Workshop Proceedings",

issn = "1613-0073",

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TY - JOUR

T1 - Expanding the molecular glycophenotype ontology to include model organisms and acquired diseases

AU - Gourdine, Jean Philippe

AU - Vasilevsky, Nicole

AU - Winfree, Lilly

AU - Brush, Matthew

AU - Haendel, Melissa

PY - 2018

Y1 - 2018

N2 - Glycans are an underappreciated class of molecules despite the fact that they are implicated in more than 100 known diseases. We have developed an ontology model that captures glycan abnormalities at the molecular level (glycophenotypes) called the molecular glycophenotype ontology (MGPO). Only 30% of known glycosyltransferases have been implicated in human genetic disorders of glycosylation. Ortholog glycosyltransferases from model organism can cover relevant biological information on potential human diseases. Thus, extending MGPO to represent additional phenotypes and support annotation of model organism data will help cross-species comparison. Expansion of MGPO will also include annotation of glycophenotypes from acquired diseases.

AB - Glycans are an underappreciated class of molecules despite the fact that they are implicated in more than 100 known diseases. We have developed an ontology model that captures glycan abnormalities at the molecular level (glycophenotypes) called the molecular glycophenotype ontology (MGPO). Only 30% of known glycosyltransferases have been implicated in human genetic disorders of glycosylation. Ortholog glycosyltransferases from model organism can cover relevant biological information on potential human diseases. Thus, extending MGPO to represent additional phenotypes and support annotation of model organism data will help cross-species comparison. Expansion of MGPO will also include annotation of glycophenotypes from acquired diseases.

KW - Diseases

KW - Glycans

KW - Glycophenotypes

KW - Model organisms

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UR - http://www.scopus.com/inward/citedby.url?scp=85059865319&partnerID=8YFLogxK

M3 - Conference article

AN - SCOPUS:85059865319

SN - 1613-0073

VL - 2285

JO - CEUR Workshop Proceedings

JF - CEUR Workshop Proceedings

T2 - 9th International Conference on Biological Ontology, ICBO 2018

Y2 - 7 August 2018 through 10 August 2018

ER -

Expanding the molecular glycophenotype ontology to include model organisms and acquired diseases

Abstract

Keywords

ASJC Scopus subject areas

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