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Publication : Reduced mTORC1-signalling in retinal progenitor cells leads to visual pathway dysfunction.

First Author  Jones I Year  2019
Journal  Biol Open Volume  8
Issue  8 PubMed ID  31285269
Mgi Jnum  J:279675 Mgi Id  MGI:6343157
Doi  10.1242/bio.044370 Citation  Jones I, et al. (2019) Reduced mTORC1-signalling in retinal progenitor cells leads to visual pathway dysfunction. Biol Open 8(8):bio044370
abstractText  Development of the vertebrate central nervous system involves the co-ordinated differentiation of progenitor cells and the establishment of functional neural networks. This neurogenic process is driven by both intracellular and extracellular cues that converge on the mammalian target of rapamycin complex 1 (mTORC1). Here we demonstrate that mTORC1-signalling mediates multi-faceted roles during central nervous system development using the mouse retina as a model system. Downregulation of mTORC1-signalling in retinal progenitor cells by conditional ablation of Rptor leads to proliferation deficits and an over-production of retinal ganglion cells during embryonic development. In contrast, reduced mTORC1-signalling in postnatal animals leads to temporal deviations in programmed cell death and the consequent production of asymmetric retinal ganglion cell mosaics and associated loss of axonal termination topographies in the dorsal lateral geniculate nucleus of adult mice. In combination these developmental defects induce visually mediated behavioural deficits. These collective observations demonstrate that mTORC1-signalling mediates critical roles during visual pathway development and function.
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