PRIMUS: Comprehensive proteomics of mouse intervertebral discs that inform novel biology and relevance to human disease modelling

Mice are commonly used to study intervertebral disc (IVD) biology and related diseases such as IVD degeneration. Discs from both the lumbar and tail regions are used. However, little is known about compartmental characteristics in the different regions, nor their relevance to the human setting, wher...

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Autores principales: Kudelko, Mateusz, Chen, Peikai, Tam, Vivian, Zhang, Ying, Kong, Oi-Yin, Sharma, Rakesh, Au, Tiffany Y.K., To, Michael Kai-Tsun, Cheah, Kathryn S.E., Chan, Wilson C.W., Chan, Danny
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Full Length Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8361275/
https://www.ncbi.nlm.nih.gov/pubmed/34409283
http://dx.doi.org/10.1016/j.mbplus.2021.100082
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author Kudelko, Mateusz
Chen, Peikai
Tam, Vivian
Zhang, Ying
Kong, Oi-Yin
Sharma, Rakesh
Au, Tiffany Y.K.
To, Michael Kai-Tsun
Cheah, Kathryn S.E.
Chan, Wilson C.W.
Chan, Danny
author_facet Kudelko, Mateusz
Chen, Peikai
Tam, Vivian
Zhang, Ying
Kong, Oi-Yin
Sharma, Rakesh
Au, Tiffany Y.K.
To, Michael Kai-Tsun
Cheah, Kathryn S.E.
Chan, Wilson C.W.
Chan, Danny
author_sort Kudelko, Mateusz
collection PubMed
description Mice are commonly used to study intervertebral disc (IVD) biology and related diseases such as IVD degeneration. Discs from both the lumbar and tail regions are used. However, little is known about compartmental characteristics in the different regions, nor their relevance to the human setting, where a functional IVD unit depends on a homeostatic proteome. Here, we address these major gaps through comprehensive proteomic profiling and in-depth analyses of 8-week-old healthy murine discs, followed by comparisons with human. Leveraging on a dataset of over 2,700 proteins from 31 proteomic profiles, we identified key molecular and cellular differences between disc compartments and spine levels, but not gender. The nucleus pulposus (NP) and annulus fibrosus (AF) compartments differ the most, both in matrisome and cellularity contents. Differences in the matrisome are consistent with the fibrous nature required for tensile strength in the AF and hydration property in the NP. Novel findings for the NP cells included an enrichment in cell junction proteins for cell–cell communication (Cdh2, Dsp and Gja1) and osmoregulation (Slc12a2 and Wnk1). In NP cells, we detected heterogeneity of vacuolar organelles; where about half have potential lysosomal function (Vamp3, Copb2, Lamp1/2, Lamtor1), some contain lipid droplets and others with undefined contents. The AF is enriched in proteins for the oxidative stress responses (Sod3 and Clu). Interestingly, mitochondrial proteins are elevated in the lumbar than tail IVDs that may reflect differences in metabolic requirement. Relative to the human, cellular and structural information are conserved for the AF. Even though the NP is more divergent between mouse and human, there are similarities at the level of cell biology. Further, common cross-species markers were identified for both NP (KRT8/19, CD109) and AF (COL12A1). Overall, mouse is a relevant model to study IVD biology, and an understanding of the limitation will facilitate research planning and data interpretation, maximizing the translation of research findings to human IVDs.
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spelling pubmed-83612752021-08-17 PRIMUS: Comprehensive proteomics of mouse intervertebral discs that inform novel biology and relevance to human disease modelling Kudelko, Mateusz Chen, Peikai Tam, Vivian Zhang, Ying Kong, Oi-Yin Sharma, Rakesh Au, Tiffany Y.K. To, Michael Kai-Tsun Cheah, Kathryn S.E. Chan, Wilson C.W. Chan, Danny Matrix Biol Plus Full Length Article Mice are commonly used to study intervertebral disc (IVD) biology and related diseases such as IVD degeneration. Discs from both the lumbar and tail regions are used. However, little is known about compartmental characteristics in the different regions, nor their relevance to the human setting, where a functional IVD unit depends on a homeostatic proteome. Here, we address these major gaps through comprehensive proteomic profiling and in-depth analyses of 8-week-old healthy murine discs, followed by comparisons with human. Leveraging on a dataset of over 2,700 proteins from 31 proteomic profiles, we identified key molecular and cellular differences between disc compartments and spine levels, but not gender. The nucleus pulposus (NP) and annulus fibrosus (AF) compartments differ the most, both in matrisome and cellularity contents. Differences in the matrisome are consistent with the fibrous nature required for tensile strength in the AF and hydration property in the NP. Novel findings for the NP cells included an enrichment in cell junction proteins for cell–cell communication (Cdh2, Dsp and Gja1) and osmoregulation (Slc12a2 and Wnk1). In NP cells, we detected heterogeneity of vacuolar organelles; where about half have potential lysosomal function (Vamp3, Copb2, Lamp1/2, Lamtor1), some contain lipid droplets and others with undefined contents. The AF is enriched in proteins for the oxidative stress responses (Sod3 and Clu). Interestingly, mitochondrial proteins are elevated in the lumbar than tail IVDs that may reflect differences in metabolic requirement. Relative to the human, cellular and structural information are conserved for the AF. Even though the NP is more divergent between mouse and human, there are similarities at the level of cell biology. Further, common cross-species markers were identified for both NP (KRT8/19, CD109) and AF (COL12A1). Overall, mouse is a relevant model to study IVD biology, and an understanding of the limitation will facilitate research planning and data interpretation, maximizing the translation of research findings to human IVDs. Elsevier 2021-07-24 /pmc/articles/PMC8361275/ /pubmed/34409283 http://dx.doi.org/10.1016/j.mbplus.2021.100082 Text en © 2021 The Author(s) https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Full Length Article
Kudelko, Mateusz
Chen, Peikai
Tam, Vivian
Zhang, Ying
Kong, Oi-Yin
Sharma, Rakesh
Au, Tiffany Y.K.
To, Michael Kai-Tsun
Cheah, Kathryn S.E.
Chan, Wilson C.W.
Chan, Danny
PRIMUS: Comprehensive proteomics of mouse intervertebral discs that inform novel biology and relevance to human disease modelling
title PRIMUS: Comprehensive proteomics of mouse intervertebral discs that inform novel biology and relevance to human disease modelling
title_full PRIMUS: Comprehensive proteomics of mouse intervertebral discs that inform novel biology and relevance to human disease modelling
title_fullStr PRIMUS: Comprehensive proteomics of mouse intervertebral discs that inform novel biology and relevance to human disease modelling
title_full_unstemmed PRIMUS: Comprehensive proteomics of mouse intervertebral discs that inform novel biology and relevance to human disease modelling
title_short PRIMUS: Comprehensive proteomics of mouse intervertebral discs that inform novel biology and relevance to human disease modelling
title_sort primus: comprehensive proteomics of mouse intervertebral discs that inform novel biology and relevance to human disease modelling
topic Full Length Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8361275/
https://www.ncbi.nlm.nih.gov/pubmed/34409283
http://dx.doi.org/10.1016/j.mbplus.2021.100082
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