AI Article Synopsis
- Neuroblasts of the statoacoustic ganglion (SAG) develop from the otic vesicle, undergoing proliferation and migration before differentiating to connect with inner ear hair cells and hindbrain targets.
- Fgf signaling is crucial in this process, where it specifies neuroblasts locally and coordinates the timing of neuroblast differentiation.
- Disruption of Fgf signaling leads to imbalanced neuron production, while proper Fgf activity maintains a self-regulating system to ensure an adequate number of SAG neurons as the larva grows.
Article Abstract
Neuroblasts of the statoacoustic ganglion (SAG) initially form in the floor of the otic vesicle during a relatively brief developmental window. They soon delaminate and undergo a protracted phase of proliferation and migration (transit-amplification). Neuroblasts eventually differentiate and extend processes bi-directionally to synapse with hair cells in the inner ear and various targets in the hindbrain. Our studies in zebrafish have shown that Fgf signaling controls multiple phases of this complex developmental process. Moderate levels of Fgf in a gradient emanating from the nascent utricular macula specify SAG neuroblasts in laterally adjacent otic epithelium. At a later stage, differentiating SAG neurons express Fgf5, which serves two functions: First, as SAG neurons accumulate, increasing levels of Fgf exceed an upper threshold that terminates the initial phase of neuroblast specification. Second, elevated Fgf delays differentiation of transit-amplifying cells, balancing the rate of progenitor renewal with neuronal differentiation. Laser-ablation of mature SAG neurons abolishes feedback-inhibition and causes precocious neuronal differentiation. Similar effects are obtained by Fgf5-knockdown or global impairment of Fgf signaling, whereas Fgf misexpression has the opposite effect. Thus Fgf signaling renders SAG development self-regulating, ensuring steady production of an appropriate number of neurons as the larva grows.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3499369 | PMC |
| http://dx.doi.org/10.1371/journal.pgen.1003068 | DOI Listing |
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