Modeling of Skeletal Development and Diseases Using Human Pluripotent Stem Cells.

J Bone Miner Res

Department of Tissue and Developmental Biology, Graduate School of Dentistry, Osaka University, Osaka 565-0871, Japan.

Published: November 2024

AI Article Synopsis

  • Human skeletal elements originate from different parts of the embryo, with specific tissues responsible for the formation of facial bones, the axial skeleton, and the appendicular skeleton.
  • The development of skeletal cells can be modeled using human pluripotent stem cells to replicate the stages of embryonic development and the complexities of skeletal metabolism.
  • Recent advancements include developing organoids and using genome-editing technologies to study genetic skeletal diseases, alongside prospects for precision medicine applications in this field.

Article Abstract

Human skeletal elements are formed from distinct origins at distinct positions of the embryo. For example, the neural crest produces the facial bones, the paraxial mesoderm produces the axial skeleton, and the lateral plate mesoderm produces the appendicular skeleton. During skeletal development, different combinations of signaling pathways are coordinated from distinct origins during the sequential developmental stages. Models for human skeletal development have been established using human pluripotent stem cells (hPSCs) and by exploiting our understanding of skeletal development. Stepwise protocols for generating skeletal cells from different origins have been designed to mimic developmental trails. Recently, organoid methods have allowed the multicellular organization of skeletal cell types to recapitulate complicated skeletal development and metabolism. Similarly, several genetic diseases of the skeleton have been modeled using patient-derived induced pluripotent stem cells and genome-editing technologies. Model-based drug screening is a powerful tool for identifying drug candidates. This review briefly summarizes our current understanding of the embryonic development of skeletal tissues and introduces the current state-of-the-art hPSC methods for recapitulating skeletal development, metabolism, and diseases. We also discuss the current limitations and future perspectives for applications of the hPSC-based modeling system in precision medicine in this research field.

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Source
http://dx.doi.org/10.1093/jbmr/zjae178DOI Listing

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