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The Mouse Age Phenome Knowledgebase and Disease-Specific Inter-Species Age Mapping

BACKGROUND: Similarities between mice and humans lead to generation of many mouse models of human disease. However, differences between the species often result in mice being unreliable as preclinical models for human disease. One difference that might play a role in lowering the predictivity of mic...

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Autores principales: Geifman, Nophar, Rubin, Eitan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3849212/
https://www.ncbi.nlm.nih.gov/pubmed/24312529
http://dx.doi.org/10.1371/journal.pone.0081114
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author Geifman, Nophar
Rubin, Eitan
author_facet Geifman, Nophar
Rubin, Eitan
author_sort Geifman, Nophar
collection PubMed
description BACKGROUND: Similarities between mice and humans lead to generation of many mouse models of human disease. However, differences between the species often result in mice being unreliable as preclinical models for human disease. One difference that might play a role in lowering the predictivity of mice models to human diseases is age. Despite the important role age plays in medicine, it is too often considered only casually when considering mouse models. METHODS: We developed the mouse-Age Phenotype Knowledgebase, which holds knowledge about age-related phenotypic patterns in mice. The knowledgebase was extensively populated with literature-derived data using text mining techniques. We then mapped between ages in humans and mice by comparing the age distribution pattern for 887 diseases in both species. RESULTS: The knowledgebase was populated with over 9800 instances generated by a text-mining pipeline. The quality of the data was manually evaluated, and was found to be of high accuracy (estimated precision >86%). Furthermore, grouping together diseases that share similar age patterns in mice resulted in clusters that mirror actual biomedical knowledge. Using these data, we matched age distribution patterns in mice and in humans, allowing for age differences by shifting either of the patterns. High correlation (r(2)>0.5) was found for 223 diseases. The results clearly indicate a difference in the age mapping between different diseases: age 30 years in human is mapped to 120 days in mice for Leukemia, but to 295 days for Anemia. Based on these results we generated a mice-to-human age map which is publicly available. CONCLUSIONS: We present here the development of the mouse-APK, its population with literature-derived data and its use to map ages in mice and human for 223 diseases. These results present a further step made to bridging the gap between humans and mice in biomedical research.
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spelling pubmed-38492122013-12-05 The Mouse Age Phenome Knowledgebase and Disease-Specific Inter-Species Age Mapping Geifman, Nophar Rubin, Eitan PLoS One Research Article BACKGROUND: Similarities between mice and humans lead to generation of many mouse models of human disease. However, differences between the species often result in mice being unreliable as preclinical models for human disease. One difference that might play a role in lowering the predictivity of mice models to human diseases is age. Despite the important role age plays in medicine, it is too often considered only casually when considering mouse models. METHODS: We developed the mouse-Age Phenotype Knowledgebase, which holds knowledge about age-related phenotypic patterns in mice. The knowledgebase was extensively populated with literature-derived data using text mining techniques. We then mapped between ages in humans and mice by comparing the age distribution pattern for 887 diseases in both species. RESULTS: The knowledgebase was populated with over 9800 instances generated by a text-mining pipeline. The quality of the data was manually evaluated, and was found to be of high accuracy (estimated precision >86%). Furthermore, grouping together diseases that share similar age patterns in mice resulted in clusters that mirror actual biomedical knowledge. Using these data, we matched age distribution patterns in mice and in humans, allowing for age differences by shifting either of the patterns. High correlation (r(2)>0.5) was found for 223 diseases. The results clearly indicate a difference in the age mapping between different diseases: age 30 years in human is mapped to 120 days in mice for Leukemia, but to 295 days for Anemia. Based on these results we generated a mice-to-human age map which is publicly available. CONCLUSIONS: We present here the development of the mouse-APK, its population with literature-derived data and its use to map ages in mice and human for 223 diseases. These results present a further step made to bridging the gap between humans and mice in biomedical research. Public Library of Science 2013-12-03 /pmc/articles/PMC3849212/ /pubmed/24312529 http://dx.doi.org/10.1371/journal.pone.0081114 Text en © 2013 Geifman, Rubin http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Geifman, Nophar
Rubin, Eitan
The Mouse Age Phenome Knowledgebase and Disease-Specific Inter-Species Age Mapping
title The Mouse Age Phenome Knowledgebase and Disease-Specific Inter-Species Age Mapping
title_full The Mouse Age Phenome Knowledgebase and Disease-Specific Inter-Species Age Mapping
title_fullStr The Mouse Age Phenome Knowledgebase and Disease-Specific Inter-Species Age Mapping
title_full_unstemmed The Mouse Age Phenome Knowledgebase and Disease-Specific Inter-Species Age Mapping
title_short The Mouse Age Phenome Knowledgebase and Disease-Specific Inter-Species Age Mapping
title_sort mouse age phenome knowledgebase and disease-specific inter-species age mapping
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3849212/
https://www.ncbi.nlm.nih.gov/pubmed/24312529
http://dx.doi.org/10.1371/journal.pone.0081114
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