Temporal and Quantitative Transcriptomic Differences Define Sexual Dimorphism in Murine Postnatal Bone Aging

Time is a central element of the sexual dimorphic patterns of development, pathology, and aging of the skeleton. Because the transcriptome is a representation of the phenome, we hypothesized that both sex and sex‐specific temporal, transcriptomic differences in bone tissues over an 18‐month period w...

Descripción completa

Detalles Bibliográficos
Autores principales: Lu, Darlene, Demissie, Serkalem, Horowitz, Nina B, Gower, Adam C, Lenburg, Marc E, Alekseyev, Yuriy O, Hussein, Amira I, Bragdon, Beth, Liu, Yu, Daukss, Dana, Page, Jack M, Webster, Micheal Z, Schlezinger, Jennifer J, Morgan, Elise F, Gerstenfeld, Louis C
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley & Sons, Inc. 2021
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8861981/
https://www.ncbi.nlm.nih.gov/pubmed/35229061
http://dx.doi.org/10.1002/jbm4.10579
_version_ 1784654971368636416
author Lu, Darlene
Demissie, Serkalem
Horowitz, Nina B
Gower, Adam C
Lenburg, Marc E
Alekseyev, Yuriy O
Hussein, Amira I
Bragdon, Beth
Liu, Yu
Daukss, Dana
Page, Jack M
Webster, Micheal Z
Schlezinger, Jennifer J
Morgan, Elise F
Gerstenfeld, Louis C
author_facet Lu, Darlene
Demissie, Serkalem
Horowitz, Nina B
Gower, Adam C
Lenburg, Marc E
Alekseyev, Yuriy O
Hussein, Amira I
Bragdon, Beth
Liu, Yu
Daukss, Dana
Page, Jack M
Webster, Micheal Z
Schlezinger, Jennifer J
Morgan, Elise F
Gerstenfeld, Louis C
author_sort Lu, Darlene
collection PubMed
description Time is a central element of the sexual dimorphic patterns of development, pathology, and aging of the skeleton. Because the transcriptome is a representation of the phenome, we hypothesized that both sex and sex‐specific temporal, transcriptomic differences in bone tissues over an 18‐month period would be informative to the underlying molecular processes that lead to postnatal sexual dimorphism. Regardless of age, sex‐associated changes of the whole bone transcriptomes were primarily associated not only with bone but also vascular and connective tissue ontologies. A pattern‐based approach used to screen the entire Gene Expression Omnibus (GEO) database against those that were sex‐specific in bone identified two coordinately regulated gene sets: one related to high phosphate–induced aortic calcification and one induced by mechanical stimulation in bone. Temporal clustering of the transcriptome identified two skeletal tissue‐associated, sex‐specific patterns of gene expression. One set of genes, associated with skeletal patterning and morphology, showed peak expression earlier in females. The second set of genes, associated with coupled remodeling, had quantitatively higher expression in females and exhibited a broad peak between 3 to 12 months, concurrent with the animals' reproductive period. Results of phenome‐level structural assessments of the tibia and vertebrae, and in vivo and in vitro analysis of cells having osteogenic potential, were consistent with the existence of functionally unique, skeletogenic cell populations that are separately responsible for appositional growth and intramedullary functions. These data suggest that skeletal sexual dimorphism arises through sex‐specific, temporally different processes controlling morphometric growth and later coupled remodeling of the skeleton during the reproductive period of the animal. © 2021 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research.
format Online
Article
Text
id pubmed-8861981
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher John Wiley & Sons, Inc.
record_format MEDLINE/PubMed
spelling pubmed-88619812022-02-27 Temporal and Quantitative Transcriptomic Differences Define Sexual Dimorphism in Murine Postnatal Bone Aging Lu, Darlene Demissie, Serkalem Horowitz, Nina B Gower, Adam C Lenburg, Marc E Alekseyev, Yuriy O Hussein, Amira I Bragdon, Beth Liu, Yu Daukss, Dana Page, Jack M Webster, Micheal Z Schlezinger, Jennifer J Morgan, Elise F Gerstenfeld, Louis C JBMR Plus Original Articles Time is a central element of the sexual dimorphic patterns of development, pathology, and aging of the skeleton. Because the transcriptome is a representation of the phenome, we hypothesized that both sex and sex‐specific temporal, transcriptomic differences in bone tissues over an 18‐month period would be informative to the underlying molecular processes that lead to postnatal sexual dimorphism. Regardless of age, sex‐associated changes of the whole bone transcriptomes were primarily associated not only with bone but also vascular and connective tissue ontologies. A pattern‐based approach used to screen the entire Gene Expression Omnibus (GEO) database against those that were sex‐specific in bone identified two coordinately regulated gene sets: one related to high phosphate–induced aortic calcification and one induced by mechanical stimulation in bone. Temporal clustering of the transcriptome identified two skeletal tissue‐associated, sex‐specific patterns of gene expression. One set of genes, associated with skeletal patterning and morphology, showed peak expression earlier in females. The second set of genes, associated with coupled remodeling, had quantitatively higher expression in females and exhibited a broad peak between 3 to 12 months, concurrent with the animals' reproductive period. Results of phenome‐level structural assessments of the tibia and vertebrae, and in vivo and in vitro analysis of cells having osteogenic potential, were consistent with the existence of functionally unique, skeletogenic cell populations that are separately responsible for appositional growth and intramedullary functions. These data suggest that skeletal sexual dimorphism arises through sex‐specific, temporally different processes controlling morphometric growth and later coupled remodeling of the skeleton during the reproductive period of the animal. © 2021 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research. John Wiley & Sons, Inc. 2021-12-10 /pmc/articles/PMC8861981/ /pubmed/35229061 http://dx.doi.org/10.1002/jbm4.10579 Text en © 2021 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Lu, Darlene
Demissie, Serkalem
Horowitz, Nina B
Gower, Adam C
Lenburg, Marc E
Alekseyev, Yuriy O
Hussein, Amira I
Bragdon, Beth
Liu, Yu
Daukss, Dana
Page, Jack M
Webster, Micheal Z
Schlezinger, Jennifer J
Morgan, Elise F
Gerstenfeld, Louis C
Temporal and Quantitative Transcriptomic Differences Define Sexual Dimorphism in Murine Postnatal Bone Aging
title Temporal and Quantitative Transcriptomic Differences Define Sexual Dimorphism in Murine Postnatal Bone Aging
title_full Temporal and Quantitative Transcriptomic Differences Define Sexual Dimorphism in Murine Postnatal Bone Aging
title_fullStr Temporal and Quantitative Transcriptomic Differences Define Sexual Dimorphism in Murine Postnatal Bone Aging
title_full_unstemmed Temporal and Quantitative Transcriptomic Differences Define Sexual Dimorphism in Murine Postnatal Bone Aging
title_short Temporal and Quantitative Transcriptomic Differences Define Sexual Dimorphism in Murine Postnatal Bone Aging
title_sort temporal and quantitative transcriptomic differences define sexual dimorphism in murine postnatal bone aging
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8861981/
https://www.ncbi.nlm.nih.gov/pubmed/35229061
http://dx.doi.org/10.1002/jbm4.10579
work_keys_str_mv AT ludarlene temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT demissieserkalem temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT horowitzninab temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT goweradamc temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT lenburgmarce temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT alekseyevyuriyo temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT husseinamirai temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT bragdonbeth temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT liuyu temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT daukssdana temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT pagejackm temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT webstermichealz temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT schlezingerjenniferj temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT morganelisef temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging
AT gerstenfeldlouisc temporalandquantitativetranscriptomicdifferencesdefinesexualdimorphisminmurinepostnatalboneaging

Ejemplares similares