Bone cell-specific deletion of thyroid hormone transporter Mct8 distinctly regulates bone volume in young versus adult male mice
Research output: Contribution to journal › Research article › Contributed › peer-review
Contributors
Abstract
Thyroid hormones are critical regulators of bone metabolism. Their cellular import is guided through transporter proteins, including the monocarboxylate transporter 8 (MCT8). Conditional Mct8 knockout in osteoblast and osteoclast precursors leads to trabecular bone gain in 12-week-old male mice. Given that thyroid hormones regulate both skeletal development and bone maintenance, we investigated the effect of bone cell-specific Mct8 deletion in 6-week-old (young) and 24-week-old (adult) male mice. Mct8 ablation in osteoclast precursors led to trabecular bone gain at the spine in 6-week-old animals compared to age-matched controls, whereas adult animals displayed a shift towards trabecular bone loss in both femur and vertebra. Mct8 deficiency in osteoprogenitors increased osteoblast numbers and trabecular bone mass at the spine of young mice, without skeletal differences between adult knockout mice and littermate controls. In contrast, young mice lacking Mct8 in late osteoblasts/osteocytes exhibited lower trabecular bone volume at the spine and femur compared to respective controls, but no differences were detected at 24 weeks of age. In vitro studies of osteoblasts with Dmp1-Cre promotor driven Mct8 deletion showed no significant alterations of osteogenic marker gene expression and mineralization capacity suggesting that MCT8 is not crucial for osteoblast maturation. Overall, we observed mild effects with conditional Mct8 knockout on bone microarchitecture and bone turnover especially during growth implying a secondary role for MCT8 as a thyroid hormone transporter in bone.
Details
Original language | English |
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Article number | 116375 |
Pages (from-to) | 116375 |
Journal | Bone |
Volume | 159 |
Publication status | Published - Jun 2022 |
Peer-reviewed | Yes |
External IDs
Scopus | 85125913284 |
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unpaywall | 10.1016/j.bone.2022.116375 |
Mendeley | 4cdcfeae-1580-3b45-9dee-2d2338df7719 |
ORCID | /0000-0002-8691-8423/work/142236010 |
Keywords
Research priority areas of TU Dresden
DFG Classification of Subject Areas according to Review Boards
Subject groups, research areas, subject areas according to Destatis
Sustainable Development Goals
ASJC Scopus subject areas
Keywords
- Animals, Cancellous Bone/metabolism, Male, Membrane Transport Proteins/metabolism, Mice, Mice, Knockout, Monocarboxylic Acid Transporters/genetics, Osteoblasts/metabolism, Osteocytes/metabolism, Symporters/genetics, Thyroid Hormones/metabolism, Bone turnover, Thyroid hormone transporter, Slc16a2, Bone homeostasis, Mct8