Opportunities and Challenges in Functional Genomics Research in Osteoporosis: Report From a Workshop Held by the Causes Working Group of the Osteoporosis and Bone Research Academy of the Royal Osteoporosis Society on October 5th 2020

The discovery that sclerostin is the defective protein underlying the rare heritable bone mass disorder, sclerosteosis, ultimately led to development of anti-sclerostin antibodies as a new treatment for osteoporosis. In the era of large scale GWAS, many additional genetic signals associated with bon...

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Autores principales: Tobias, Jonathan H., Duncan, Emma L., Kague, Erika, Hammond, Chrissy L., Gregson, Celia L., Bassett, Duncan, Williams, Graham R., Min, Josine L., Gaunt, Tom R., Karasik, David, Ohlsson, Claes, Rivadeneira, Fernando, Edwards, James R., Hannan, Fadil M., Kemp, John P., Gilbert, Sophie J., Alonso, Nerea, Hassan, Neelam, Compston, Juliet E., Ralston, Stuart H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Endocrinology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7917291/
https://www.ncbi.nlm.nih.gov/pubmed/33658983
http://dx.doi.org/10.3389/fendo.2020.630875
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author Tobias, Jonathan H.
Duncan, Emma L.
Kague, Erika
Hammond, Chrissy L.
Gregson, Celia L.
Bassett, Duncan
Williams, Graham R.
Min, Josine L.
Gaunt, Tom R.
Karasik, David
Ohlsson, Claes
Rivadeneira, Fernando
Edwards, James R.
Hannan, Fadil M.
Kemp, John P.
Gilbert, Sophie J.
Alonso, Nerea
Hassan, Neelam
Compston, Juliet E.
Ralston, Stuart H.
author_facet Tobias, Jonathan H.
Duncan, Emma L.
Kague, Erika
Hammond, Chrissy L.
Gregson, Celia L.
Bassett, Duncan
Williams, Graham R.
Min, Josine L.
Gaunt, Tom R.
Karasik, David
Ohlsson, Claes
Rivadeneira, Fernando
Edwards, James R.
Hannan, Fadil M.
Kemp, John P.
Gilbert, Sophie J.
Alonso, Nerea
Hassan, Neelam
Compston, Juliet E.
Ralston, Stuart H.
author_sort Tobias, Jonathan H.
collection PubMed
description The discovery that sclerostin is the defective protein underlying the rare heritable bone mass disorder, sclerosteosis, ultimately led to development of anti-sclerostin antibodies as a new treatment for osteoporosis. In the era of large scale GWAS, many additional genetic signals associated with bone mass and related traits have since been reported. However, how best to interrogate these signals in order to identify the underlying gene responsible for these genetic associations, a prerequisite for identifying drug targets for further treatments, remains a challenge. The resources available for supporting functional genomics research continues to expand, exemplified by “multi-omics” database resources, with improved availability of datasets derived from bone tissues. These databases provide information about potential molecular mediators such as mRNA expression, protein expression, and DNA methylation levels, which can be interrogated to map genetic signals to specific genes based on identification of causal pathways between the genetic signal and the phenotype being studied. Functional evaluation of potential causative genes has been facilitated by characterization of the “osteocyte signature”, by broad phenotyping of knockout mice with deletions of over 7,000 genes, in which more detailed skeletal phenotyping is currently being undertaken, and by development of zebrafish as a highly efficient additional in vivo model for functional studies of the skeleton. Looking to the future, this expanding repertoire of tools offers the hope of accurately defining the major genetic signals which contribute to osteoporosis. This may in turn lead to the identification of additional therapeutic targets, and ultimately new treatments for osteoporosis.
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spelling pubmed-79172912021-03-02 Opportunities and Challenges in Functional Genomics Research in Osteoporosis: Report From a Workshop Held by the Causes Working Group of the Osteoporosis and Bone Research Academy of the Royal Osteoporosis Society on October 5th 2020 Tobias, Jonathan H. Duncan, Emma L. Kague, Erika Hammond, Chrissy L. Gregson, Celia L. Bassett, Duncan Williams, Graham R. Min, Josine L. Gaunt, Tom R. Karasik, David Ohlsson, Claes Rivadeneira, Fernando Edwards, James R. Hannan, Fadil M. Kemp, John P. Gilbert, Sophie J. Alonso, Nerea Hassan, Neelam Compston, Juliet E. Ralston, Stuart H. Front Endocrinol (Lausanne) Endocrinology The discovery that sclerostin is the defective protein underlying the rare heritable bone mass disorder, sclerosteosis, ultimately led to development of anti-sclerostin antibodies as a new treatment for osteoporosis. In the era of large scale GWAS, many additional genetic signals associated with bone mass and related traits have since been reported. However, how best to interrogate these signals in order to identify the underlying gene responsible for these genetic associations, a prerequisite for identifying drug targets for further treatments, remains a challenge. The resources available for supporting functional genomics research continues to expand, exemplified by “multi-omics” database resources, with improved availability of datasets derived from bone tissues. These databases provide information about potential molecular mediators such as mRNA expression, protein expression, and DNA methylation levels, which can be interrogated to map genetic signals to specific genes based on identification of causal pathways between the genetic signal and the phenotype being studied. Functional evaluation of potential causative genes has been facilitated by characterization of the “osteocyte signature”, by broad phenotyping of knockout mice with deletions of over 7,000 genes, in which more detailed skeletal phenotyping is currently being undertaken, and by development of zebrafish as a highly efficient additional in vivo model for functional studies of the skeleton. Looking to the future, this expanding repertoire of tools offers the hope of accurately defining the major genetic signals which contribute to osteoporosis. This may in turn lead to the identification of additional therapeutic targets, and ultimately new treatments for osteoporosis. Frontiers Media S.A. 2021-02-15 /pmc/articles/PMC7917291/ /pubmed/33658983 http://dx.doi.org/10.3389/fendo.2020.630875 Text en Copyright © 2021 Tobias, Duncan, Kague, Hammond, Gregson, Bassett, Williams, Min, Gaunt, Karasik, Ohlsson, Rivadeneira, Edwards, Hannan, Kemp, Gilbert, Alonso, Hassan, Compston and Ralston http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Endocrinology
Tobias, Jonathan H.
Duncan, Emma L.
Kague, Erika
Hammond, Chrissy L.
Gregson, Celia L.
Bassett, Duncan
Williams, Graham R.
Min, Josine L.
Gaunt, Tom R.
Karasik, David
Ohlsson, Claes
Rivadeneira, Fernando
Edwards, James R.
Hannan, Fadil M.
Kemp, John P.
Gilbert, Sophie J.
Alonso, Nerea
Hassan, Neelam
Compston, Juliet E.
Ralston, Stuart H.
Opportunities and Challenges in Functional Genomics Research in Osteoporosis: Report From a Workshop Held by the Causes Working Group of the Osteoporosis and Bone Research Academy of the Royal Osteoporosis Society on October 5th 2020
title Opportunities and Challenges in Functional Genomics Research in Osteoporosis: Report From a Workshop Held by the Causes Working Group of the Osteoporosis and Bone Research Academy of the Royal Osteoporosis Society on October 5th 2020
title_full Opportunities and Challenges in Functional Genomics Research in Osteoporosis: Report From a Workshop Held by the Causes Working Group of the Osteoporosis and Bone Research Academy of the Royal Osteoporosis Society on October 5th 2020
title_fullStr Opportunities and Challenges in Functional Genomics Research in Osteoporosis: Report From a Workshop Held by the Causes Working Group of the Osteoporosis and Bone Research Academy of the Royal Osteoporosis Society on October 5th 2020
title_full_unstemmed Opportunities and Challenges in Functional Genomics Research in Osteoporosis: Report From a Workshop Held by the Causes Working Group of the Osteoporosis and Bone Research Academy of the Royal Osteoporosis Society on October 5th 2020
title_short Opportunities and Challenges in Functional Genomics Research in Osteoporosis: Report From a Workshop Held by the Causes Working Group of the Osteoporosis and Bone Research Academy of the Royal Osteoporosis Society on October 5th 2020
title_sort opportunities and challenges in functional genomics research in osteoporosis: report from a workshop held by the causes working group of the osteoporosis and bone research academy of the royal osteoporosis society on october 5th 2020
topic Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7917291/
https://www.ncbi.nlm.nih.gov/pubmed/33658983
http://dx.doi.org/10.3389/fendo.2020.630875
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