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The Journal of Neuroscience, January 1, 2000, 20(1):283-293
The bHLH Gene Hes1 as a Repressor of the Neuronal
Commitment of CNS Stem Cells
Yuki
Nakamura1,
Shin-ichi
Sakakibara1, 2,
Takaki
Miyata1,
Masaharu
Ogawa3,
Takuya
Shimazaki5,
Samuel
Weiss5,
Ryoichiro
Kageyama4, and
Hideyuki
Okano1, 2
1 Department of Neuroanatomy, Biomedical Research
Center, Osaka University, Suita, Osaka 565-0871, Japan,
2 Core Research for Evolutional Science and Technology,
Japan Science and Technology Corporation, Minato, Tokyo 105-0011, Japan, 3 Laboratory for Cell Culture Development, Brain
Science Institute, The Institute of Physical and Chemical Research,
Wako, Saitama 351-0198, Japan, 4 Institute for Virus
Research, Kyoto University, Kyoto 606-8507, Japan, and
5 Genes and Development Research Group, University of
Calgary Faculty of Medicine, Calgary, Alberta T2N 4N1, Canada
Hes1 is one of the basic helix-loop-helix
transcription factors that regulate mammalian CNS development, and its
loss- and gain-of-function phenotypes indicate that it negatively
regulates neuronal differentiation.
Here we report that Hes1 / mice
expressed both early (TuJ1 and Hu) and late (MAP2 and Neurofilament)
neuronal markers prematurely, and that there were approximately twice
the normal number of neurons in the
Hes1 / brain during early neural
development. However, immunochemical analyses of sections and
dissociated cells using neural progenitor markers, including nestin,
failed to detect any changes in Hes1 /
progenitor population. Therefore, further characterization of neural
progenitor cells that discriminated between multipotent and monopotent
cells was performed using two culture methods, low-density culture, and
a neurosphere assay. We demonstrate that the self-renewal activity of
multipotent progenitor cells was reduced in the
Hes1 / brain, and that their
subsequent commitment to the neuronal lineage was accelerated. The
Hes1 / neuronal progenitor cells were
functionally abnormal, in that they divided, on average, only once, and
then generated two neurons, (instead of one progenitor cell and one
neuron), whereas wild-type progenitor cells divided more. In addition,
some Hes1 / progenitors followed an
apoptotic fate. The overproduction of neurons in the early
Hes1 / brains may reflect this
premature and immediate generation of neurons as well as a net increase
in the number of neuronal progenitor cells.
Taken together, we conclude that Hes1 is important for
maintaining the self-renewing ability of progenitors and for repressing the commitment of multipotent progenitor cells to a neuronal fate, which is critical for the correct number of neurons to be produced and
for the establishment of normal neuronal function.
Key words:
Hes1; basic helix-loop-helix (bHLH)
transcription factor; neuronal commitment; multipotent progenitor cell; neurosphere assay; apoptosis
Copyright © 2000 Society for Neuroscience 0270-6474/0/201283-11$05.00/0
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S.-i. Sakakibara, Y. Nakamura, H. Satoh, and H. Okano
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T. Shimazaki, T. Shingo, and S. Weiss
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C. H. Faux, A. M. Turnley, R. Epa, R. Cappai, and P. F. Bartlett
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T. Imai, A. Tokunaga, T. Yoshida, M. Hashimoto, K. Mikoshiba, G. Weinmaster, M. Nakafuku, and H. Okano
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J. Zheng, J Shou, F Guillemot, R Kageyama, and W. Gao
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January 11, 2000;
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N Koyano-Nakagawa, J Kim, D Anderson, and C Kintner
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January 10, 2000;
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H. Hirata, T. Ohtsuka, Y. Bessho, and R. Kageyama
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T. Morimura, R. Goitsuka, Y. Zhang, I. Saito, M. Reth, and D. Kitamura
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November 17, 2000;
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T. Ohtsuka, M. Sakamoto, F. Guillemot, and R. Kageyama
Roles of the Basic Helix-Loop-Helix Genes Hes1 and Hes5 in Expansion of Neural Stem Cells of the Developing Brain
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August 3, 2001;
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Y. Yamazaki, H. Makino, K. Hamaguchi-Hamada, S. Hamada, H. Sugino, E. Kawase, T. Miyata, M. Ogawa, R. Yanagimachi, and T. Yagi
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