| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5893871 | International Journal of Developmental Neuroscience | 2015 | 7 Pages |
â¢Activin receptor 2B expression is regulated in ciliary ganglion development.â¢Its knockdown decreases ontogenetic programmed cell death in vivo.â¢Differentiation of choroid neurons is delayed after knockdown.â¢BMP antagonist noggin affects cell death to a similar extent.
The TGF-β ligand superfamily members activin A and BMP control important aspects of embryonic neuronal development and differentiation. Both are known to bind to activin receptor subtypes IIA (ActRIIA) and IIB, while in the avian ciliary ganglion (CG), so far only ActRIIA-expression has been described. We show that the expression of ACVR2B, coding for the ActRIIB, is tightly regulated during CG development and the knockdown of ACVR2B expression leads to a deregulation in the execution of neuronal apoptosis and therefore affects ontogenetic programmed cell death in vivo. While the differentiation of choroid neurons was impeded in the knockdown, pointing toward a reduction in activin A-mediated neural differentiation signaling, naturally occurring neuronal cell death in the CG was not prevented by follistatin treatment. Systemic injections of the BMP antagonist noggin, on the other hand, reduced the number of apoptotic neurons to a similar extent as ACVR2B knockdown. We therefore propose a novel pathway in the regulation of CG neuron ontogenetic programmed cell death, which could be mediated by BMP and signals via the ActRIIB.
