1. Notch inhibition induces mitotically generated hair cells in mammalian cochleae via activating the Wnt pathway
- Author
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Wenyan Li, Renjie Chai, Huawei Li, Jingfang Wu, Shan Sun, Zheng-Yi Chen, and Jianming Yang
- Subjects
Labyrinth Supporting Cells ,Notch signaling pathway ,Mitosis ,Biology ,Receptors, G-Protein-Coupled ,Mice ,Hair Cells, Auditory ,medicine ,otorhinolaryngologic diseases ,Animals ,Cell Lineage ,Progenitor cell ,Wnt Signaling Pathway ,Cell Proliferation ,Multidisciplinary ,Receptors, Notch ,Regeneration (biology) ,SOXB1 Transcription Factors ,Transdifferentiation ,LGR5 ,Wnt signaling pathway ,Biological Sciences ,Cell biology ,medicine.anatomical_structure ,Hair cell ,sense organs - Abstract
The activation of cochlear progenitor cells is a promising approach for hair cell (HC) regeneration and hearing recovery. The mechanisms underlying the initiation of proliferation of postnatal cochlear progenitor cells and their transdifferentiation to HCs remain to be determined. We show that Notch inhibition initiates proliferation of supporting cells (SCs) and mitotic regeneration of HCs in neonatal mouse cochlea in vivo and in vitro. Through lineage tracing, we identify that a majority of the proliferating SCs and mitotic-generated HCs induced by Notch inhibition are derived from the Wnt-responsive leucine-rich repeat-containing G protein-coupled receptor 5 (Lgr5(+)) progenitor cells. We demonstrate that Notch inhibition removes the brakes on the canonical Wnt signaling and promotes Lgr5(+) progenitor cells to mitotically generate new HCs. Our study reveals a new function of Notch signaling in limiting proliferation and regeneration potential of postnatal cochlear progenitor cells, and provides a new route to regenerate HCs from progenitor cells by interrupting the interaction between the Notch and Wnt pathways.
- Published
- 2014