Directed differentiation
of telencephalic precursors from embryonic stem cells
Watanabe K, Kamiya D, Nishiyama A, Katayama T, Nozaki S, Kawasaki H, Watanabe
Y, Mizuseki K and Sasai Y
Nat Neurosci (2005)
SUMMARY
We demonstrate directed differentiation of telencephalic precursors from
mouse embryonic stem (ES) cells using optimized serum-free suspension
culture (SFEB culture). Treatment with Wnt and Nodal antagonists (Dkk1
and LeftyA) during the first 5 d of SFEB culture causes nearly selective
neural differentiation in ES cells ( approximately 90%). In the presence
of Dkk1, with or without LeftyA, SFEB induces efficient generation ( approximately
35%) of cells expressing telencephalic marker Bf1. Wnt3a treatment during
the late culture period increases the pallial telencephalic population
(Pax6(+) cells yield up to 75% of Bf1(+) cells), whereas Shh promotes
basal telencephalic differentiation (into Nkx2.1(+) and/or Islet1/2(+)
cells) at the cost of pallial telencephalic differentiation. Thus, in
the absence of caudalizing signals, floating aggregates of ES cells generate
naive telencephalic precursors that acquire subregional identities by
responding to extracellular patterning signals.
LINK
http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&dopt=Citation&list_uids=15696161
