TGF beta 2-induced senescence during early inner ear development
Identifiers
Identifiers
Files view or download
Files view or download
Date issued
2019Journal title
Scientific Reports
Type of content
Artigo
DeCS
organogénesis | animales | diferenciación celular | regulación de la expresión génica | factor de crecimiento transformador beta2 | transducción de señales | pollos | oído | ratonesMeSH
Cell Differentiation | Transforming Growth Factor beta2 | Ear | Organogenesis | Chickens | Mice | Signal Transduction | Animals | Gene Expression RegulationAbstract
Embryonic development requires the coordinated regulation of apoptosis, survival, autophagy, proliferation and differentiation programs. Senescence has recently joined the cellular processes required to master development, in addition to its well-described roles in cancer and ageing. Here, we show that senescent cells are present in a highly regulated temporal pattern in the developing vertebrate inner ear, first, surrounding the otic pore and, later, in the otocyst at the endolymphatic duct. Cellular senescence is associated with areas of increased apoptosis and reduced proliferation consistent with the induction of the process when the endolymphatic duct is being formed. Modulation of senescence disrupts otic vesicle morphology. Transforming growth factor beta (TGFbeta) signaling interacts with signaling pathways elicited by insulin-like growth factor type 1 (IGF-1) to jointly coordinate cellular dynamics required for morphogenesis and differentiation. Taken together, these results show that senescence is a natural occurring process essential for early inner ear development.