Primary cilium-mediated MSC mechanotransduction is dependent on Gpr161 regulation of hedgehog signalling

Johnson, Gillian P.; Fair, Sean; Hoey, David A.

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Primary cilium-mediated MSC mechanotransduction is dependent on Gpr161 regulation of hedgehog signalling

Johnson, Gillian P.; Fair, Sean; Hoey, David A.

Date

2021

Abstract

The benefits of physical loading to skeletal mass are well known. The primary cilium has emerged as an important organelle in bone mechanobiology/mechanotransduction, particularly in mesenchymal stem/stromal cells, yet the molecular mechanisms of cilium mechanotransduction are poorly understood. In this study, we demonstrate that Gpr161 is a mechanoresponsive GPCR, that localises to the cilium, and is involved in fluid shear-induced cAMP signalling and downstream osteogenesis. This Gpr161-mediated mechanotransduction is dependent on IFT88/cilium and may act through adenylyl cyclase 6 (AC6) to regulate cAMP and MSC osteogenesis. Moreover, we demonstrate that Hh signalling is positively associated with osteogenesis and that Hh gene expression is mechanically regulated and required for loading-induced osteogenic differentiation through a mechanism that involves IFT88, Gpr161, AC6, and cAMP. Therefore, we have delineated a molecular mechanism of MSC mechanotransduction which likely occurs at the cilium, leading to MSC osteogenesis, highlighting novel mechanotherapeutic targets to enhance osteogenesis.

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peer-reviewed

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Elsevier

Citation

Bone;145, 115846

Funding Information

European Union (EU), European Research Council (ERC), Irish Research Council (IRC), Science Foundation Ireland (SFI)

Primary cilium-mediated MSC mechanotransduction is dependent on Gpr161 regulation of hedgehog signalling

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Sustainable Development Goals

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