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Fig. 2. Ngn2-expressing progenitors give rise to post-mitotic dentate granule
neurons. (A-C) Sections through the hippocampus of
Ngn2KIGFP/+ embryos at E18.5 (A), P1 (B) and P5 (C)
immunolabelled for GFP. (D-G') Hippocampal sections of P1
Ngn2KIGFP/+ brains showing the secondary matrix
immunostained for GFP and BrdU after a 30 minutes pulse (D,D'), Prox1
(E,E'), HuC/D (F,F') and Neurod1 (G,G'). Arrows indicate
double-labelled cells.
(D'',E'',F'',G'') Histograms
representing (D'') the percentage of GFP-expressing cells that have
incorporated BrdU (blue bars) and the percentage of BrdU-labelled cells
expressing GFP (red bars), (E'') the percentage of GFP+ cells
expressing Prox1 at a low level (light blue bars) or at a high level (blue
bars) and (F'',G'') the percentage of GFP+ cells
expressing HuC/D (F'') and Neurod1 (G''). The high level of GFP
expression in Ngn2KIGFP/+ mice (A) compared with Ngn2
expression (Fig. 1B) reflects
the greater stability of GFP. Almost all post-mitotic dentate granule neurons
are GFP+ and therefore originate from Ngn2-expressing progenitors.
Differences in GFP labelling in E-E' and other panels are due to the
lower signal obtained with chicken anti-GFP antibody. Scale bars: 100 µm in
A-C; 20 µm in D-G. 1ry, primary matrix; 2ry, secondary matrix; 3ry,
tertiary matrix; DG, dentate gyrus.
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