| Literature DB >> 24369835 |
Keiko Nonomura1, Yoshifumi Yamaguchi2, Misato Hamachi1, Masato Koike3, Yasuo Uchiyama4, Kenichi Nakazato5, Atsushi Mochizuki5, Asako Sakaue-Sawano6, Atsushi Miyawaki6, Hiroki Yoshida7, Keisuke Kuida8, Masayuki Miura9.
Abstract
Apoptotic cells are observed in the early developing brain. Apoptosis deficiency is proposed to cause brain overgrowth, but here we show that brain malformations in apoptosis-deficient mutants are due to insufficient brain ventricle expansion as a result of uncompleted cranial neural tube closure. Apoptosis eliminates Fgf8-expressing cells in the anterior neural ridge (ANR), which acts as an organizing center of the forebrain by producing FGF8 morphogen. Deficiency of apoptosis leads to the accumulation of undead and nonproliferative cells in the ventral part of the ANR. The undead cells in apoptosis-deficient mutants express Fgf8 continuously, which perturbs gene expression in the ventral forebrain. Thus, apoptosis within a specific subdomain of the ANR is required for correct temporal elimination of an FGF8-producing region within a limited developmental time window, thereby ensuring proper forebrain development.Entities:
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Year: 2013 PMID: 24369835 DOI: 10.1016/j.devcel.2013.11.015
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270