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  A single-cell transcriptional atlas reveals resident progenitor cell niche functions in TMJ disc development and injury

Bi, R., Yin, Q., Li, H., Yang, X., Wang, Y., Li, Q., et al. (2023). A single-cell transcriptional atlas reveals resident progenitor cell niche functions in TMJ disc development and injury. NATURE COMMUNICATIONS, 14(1): 830. doi:10.1038/s41467-023-36406-2.

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 Creators:
Bi, Ruiye, Author
Yin, Qing1, Author           
Li, Haohan, Author
Yang, Xianni, Author
Wang, Yiru, Author
Li, Qianli, Author
Fang, Han, Author
Li, Peiran, Author
Lyu, Ping, Author
Fan, Yi, Author
Ying, Binbin, Author
Zhu, Songsong, Author
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1Cardiac Development and Remodeling, Max Planck Institute for Heart and Lung Research, Max Planck Society, ou_2591695              

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 Abstract: The biological characteristics of the temporomandibular joint disc involve complex cellular network in cell identity and extracellular matrix composition to modulate jaw function. The lack of a detailed characterization of the network severely limits the development of targeted therapies for temporomandibular joint-related diseases. Here we profiled single-cell transcriptomes of disc cells from mice at different postnatal stages, finding that the fibroblast population could be divided into chondrogenic and non-chondrogenic clusters. We also find that the resident mural cell population is the source of disc progenitors, characterized by ubiquitously active expression of the NOTCH3 and THY1 pathways. Lineage tracing reveals that Myh11(+) mural cells coordinate angiogenesis during disc injury but lost their progenitor characteristics and ultimately become Sfrp2(+) non-chondrogenic fibroblasts instead of Chad(+) chondrogenic fibroblasts. Overall, we reveal multiple insights into the coordinated development of disc cells and are the first to describe the resident mural cell progenitor during disc injury.
The transcriptional network in TMJ disc development and injury remains poorly characterized. Here they generate a scRNA-seq atlas of mouse TMJ disc, and identify the resident progenitor population and how its transcriptional reprogramming contributes to disc repair.

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 Dates: 2023-02-14
 Publication Status: Published online
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Title: NATURE COMMUNICATIONS
Source Genre: Journal
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Pages: - Volume / Issue: 14 (1) Sequence Number: 830 Start / End Page: - Identifier: -