MMP14 cleaves PTH1R in the chondrocyte-derived osteoblast lineage, curbing signaling intensity for proper bone anabolism

Chu, Tsz Long; Chen, Peikai; Yu, Anna Xiaodan; Kong, Mingpeng; Tan, Zhijia; Tsang, Kwok Yeung; Zhou, Zhongjun; Cheah, Kathryn S. E.

doi:10.7554/elife.82142

Cited by 7 publications

(7 citation statements)

References 76 publications

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“…This possibility becomes even more fascinating if we assume that the multipotent progenitors generated are long-lived skeletal stem cells (SSCs). This assumption is supported indirectly by the following observations: (i) the multipotency discussed above, (ii) the observation that descendants of Col10-positive chondrocytes labeled on postnatal day 9 in mice can be found in the bone marrow 16 months later [ 26 , 32 ••], and (iii) the fact that descendants of hypertrophic chondrocytes begin to express LepR [ 31 ••], and LepR + cells are currently considered to be SSPCs containing mostly SSCs [ 39 , 40 ] (Fig. 2 ).…”

Section: Transdifferentiation or Dedifferentiation?mentioning

confidence: 93%

“…Today, ample evidence obtained from the clonal lineage tracing [ 16 , 25 ], single-cell RNA sequencing (scRNAseq) [ 31 ••] and functional perturbations [ 32 ••] leaves no doubt that at least some hypertrophic chondrocytes undergo lineage extension to generate osteoblasts. In fact, certain estimates indicate that as much as 83% of the intramedullary osteoblasts originate from chondrocytes [ 31 ••], although multiple other reports propose that only approximately one-third to one-half of trabecular osteoblasts come from chondrocytes.…”

Section: Two Sources Of Endosteal Osteoblasts and The Fate Of Hypertr...mentioning

confidence: 99%

“…In fact, certain estimates indicate that as much as 83% of the intramedullary osteoblasts originate from chondrocytes [ 31 ••], although multiple other reports propose that only approximately one-third to one-half of trabecular osteoblasts come from chondrocytes. The variation in these estimates reflects differences in the efficiencies of the Cre lines employed, the methods by which the osteoblasts are co-labeled, and the time-point in development when the analysis is performed [ 24 – 26 , 31 ••, 32 ••]. Nonetheless, the clearly significant contribution of chondrocytes to the formation of osteoblasts provides an entirely new perspective on bone formation during endochondral ossification, as well as in connection with skeletal disease.…”

Section: Two Sources Of Endosteal Osteoblasts and The Fate Of Hypertr...mentioning

confidence: 99%

“…Yet, another factor recently discovered to be involved is parathyroid hormone (PTH), which promotes transdifferentiation of hypertrophic chondrocytes, while cleavage of its receptor (PTH1R) by MMP14 regulates the supply of chondrocyte-derived osteoblasts [ 32 ••]. scRNA-sequencing of Col10a1-Cre:tdTomato mice reveals that these osteoblasts are transcriptionally similar to and respond to PTH in the same manner as other osteoblasts, even as mice age [ 31 ••, 32 ••]. These latter observations indicate that osteoblasts that arise from two separate sources are morphologically, transcriptionally, and functionally similar.…”

Section: Two Sources Of Endosteal Osteoblasts and The Fate Of Hypertr...mentioning

confidence: 99%

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The Origin and Fate of Chondrocytes: Cell Plasticity in Physiological Setting

Chagin,

Chu

2023

Curr Osteoporos Rep

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Purpose of Review Here, we discuss the origin of chondrocytes, their destiny, and their plasticity in relationship to bone growth, articulation, and formation of the trabeculae. We also consider these processes from a biological, clinical, and evolutionary perspective. Recent Findings Chondrocytes, which provide the template for the formation of most bones, are responsible for skeletal growth and articulation during postnatal life. In recent years our understanding of the fate of these cells has changed dramatically. Current evidence indicates a paradoxical situation during skeletogenesis, with some cells of mesenchymal condensation differentiating directly into osteoblasts, whereas others of the same kind give rise to highly similar osteoblasts via a complex process of differentiation involving several chondrocyte intermediates. The situation becomes even more paradoxical during postnatal growth when stem cells in the growth plate produce differentiated, functional progenies, which thereafter presumably dedifferentiate into another type of stem cell. Summary Such a remarkable transition from one cell type to another under postnatal physiological conditions provides a fascinating example of cellular plasticity that may have valuable clinical implications.

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Section: Transdifferentiation or Dedifferentiation?mentioning

confidence: 93%

Section: Two Sources Of Endosteal Osteoblasts and The Fate Of Hypertr...mentioning

confidence: 99%

Section: Two Sources Of Endosteal Osteoblasts and The Fate Of Hypertr...mentioning

confidence: 99%

Section: Two Sources Of Endosteal Osteoblasts and The Fate Of Hypertr...mentioning

confidence: 99%

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The Origin and Fate of Chondrocytes: Cell Plasticity in Physiological Setting

Chagin,

Chu

2023

Curr Osteoporos Rep

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“…MMP14 can cleave PTH1R, particularly at amino acid 61, inhibiting its signaling activity. This cleavage by MMP14 promotes the degradation of PTH1R, serving as a novel mechanism for modulating the stability and signaling efficacy of this G protein-coupled receptor (GPCR), thus attenuating PTH signaling [ 236 ]. Additionally, cPTH treatment may also elevate the expression of CCL2, a chemokine that works alongside RANKL to facilitate the recruitment of monocytes, which then fuse to form mature, bone-resorbing osteoclasts [ 219 ].…”

Section: The Direct Interactions Of Pth With Bm Cellsmentioning

confidence: 99%

PTH and the Regulation of Mesenchymal Cells within the Bone Marrow Niche

Liu,

Rosen

2024

Cells

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Parathyroid hormone (PTH) plays a pivotal role in maintaining calcium homeostasis, largely by modulating bone remodeling processes. Its effects on bone are notably dependent on the duration and frequency of exposure. Specifically, PTH can initiate both bone formation and resorption, with the outcome being influenced by the manner of PTH administration: continuous or intermittent. In continuous administration, PTH tends to promote bone resorption, possibly by regulating certain genes within bone cells. Conversely, intermittent exposure generally favors bone formation, possibly through transient gene activation. PTH’s role extends to various aspects of bone cell activity. It directly influences skeletal stem cells, osteoblastic lineage cells, osteocytes, and T cells, playing a critical role in bone generation. Simultaneously, it indirectly affects osteoclast precursor cells and osteoclasts, and has a direct impact on T cells, contributing to its role in bone resorption. Despite these insights, the intricate mechanisms through which PTH acts within the bone marrow niche are not entirely understood. This article reviews the dual roles of PTH—catabolic and anabolic—on bone cells, highlighting the cellular and molecular pathways involved in these processes. The complex interplay of these factors in bone remodeling underscores the need for further investigation to fully comprehend PTH’s multifaceted influence on bone health.

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