GDNF availability determines
enteric neuron number by controlling precursor proliferation
Gianino S, Grider J R, Cresswell J, Enomoto H and Heuckeroth R O
Development 130(10):2187-98 (2003)
SUMMARY
To clarify the role of Ret signaling components in enteric nervous system
(ENS) development, we evaluated ENS anatomy and intestinal contractility
in mice heterozygous for Ret, GFRalpha1 and Ret ligands. These analyses
demonstrate that glial cell line-derived neurotrophic factor (GDNF) and
neurturin are important for different aspects of ENS development. Neurturin
is essential for maintaining the size of mature enteric neurons and the
extent of neuronal projections, but does not influence enteric neuron
number. GDNF availability determines enteric neuron number by controlling
ENS precursor proliferation. However, we were unable to find evidence
of programmed cell death in the wild type ENS by immunohistochemistry
for activated caspase 3. In addition, enteric neuron number is normal
in Bax(-/-) and Bid(-/-) mice, suggesting that, in contrast to most of
the rest of the nervous system, programmed cell death is not important
for determining enteric neuron numbers. Only mild reductions in neuron
size and neuronal fiber counts occur in Ret(+/-) and Gfra1(+/-) mice.
All of these heterozygous mice, however, have striking problems with intestinal
contractility and neurotransmitter release, demonstrating that Ret signaling
is critical for both ENS structure and function.
LINK
http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&dopt=Citation&list_uids=12668632
