Comparison of inbred mouse strains shows diverse phenotypic outcomes of intervertebral disc aging

Novais, Emanuel J. and Tran, Victoria A. and Miao, Jingya and Slaver, Katie and Sinensky, Andrew and Szeri, Flóra (2020) Comparison of inbred mouse strains shows diverse phenotypic outcomes of intervertebral disc aging. AGING CELL, 19 (5). ISSN 1474-9718

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Official URL: https://doi.org/10.1111/acel.13148

Abstract

Intervertebral disc degeneration presents a wide spectrum of clinically degenerative disc phenotypes; however, the contribution of genetic background to the degenerative outcomes has not been established. We characterized the spinal phenotype of 3 mouse strains with varying cartilage-regenerative potential at 6 and 23 months: C57BL/6, LG/J and SM/J. All strains showed different aging phenotypes. Importantly, LG/J mice showed an increased prevalence of dystrophic disc calcification in caudal discs with aging. Quantitative-histological analyses of LG/J and SM/J caudal discs evidenced accelerated degeneration compared to BL6, with cellular disorganization and cell loss together with fibrosis of the NP, respectively. Along with the higher grades of disc degeneration, SM/J, at 6M, also differed the most in terms of NP gene expression compared to other strains. Moreover, although we found common DEGs between BL6 and LG/J aging, most of them were divergent between the strains. Noteworthy, the common DEGs altered in both LG/J and BL6 aging were associated with inflammatory processes, response to stress, cell differentiation, cell metabolism and cell division. Results suggested that disc calcification in LG/J resulted from a dystrophic calcification process likely aggravated by cell death, matrix remodelling, changes in calcium/phosphate homeostasis and cell transformation. Lastly, we report 7 distinct phenotypes of human disc degeneration based on transcriptomic profiles, that presented similar pathways and DEGs found in aging mouse strains. Together, our results suggest that disc aging and degeneration depends on the genetic background and involves changes in various molecular pathways, which might help to explain the diverse phenotypes seen during disc disease. © 2020 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.

Item Type:	Article
Uncontrolled Keywords:	PREVALENCE; PHENOTYPE; ARTICLE; MOUSE; Cell Differentiation; Cell Division; comparative study; priority journal; controlled study; nonhuman; animal tissue; animal model; animal experiment; animal cell; Aging; Gene Expression; DNA Repair; immune response; CALCINOSIS; transcriptomics; extracellular matrix; micro-computed tomography; Cell Death; real time polymerase chain reaction; cell metabolism; Calcification; Calcification; bone mineralization; phenotypic variation; Cell Aging; cortical bone; RNA isolation; intervertebral disc; Transcriptome; phosphate metabolism; bone age; intervertebral disk degeneration; glucose homeostasis; TUNEL assay; genetic background; LG/J; SM/J;
Subjects:	Q Science / természettudomány > QH Natural history / természetrajz > QH301 Biology / biológia
SWORD Depositor:	MTMT SWORD
Depositing User:	MTMT SWORD
Date Deposited:	28 Sep 2021 06:39
Last Modified:	28 Sep 2021 06:39
URI:	http://real.mtak.hu/id/eprint/130867

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