Annual Report 2002
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DIVISION OF BEHAVIOR AND NEUROBIOLOGY (ADJUNCT)

Professor:MURAKAMI, Fujio
Associate Professor:NAKAFUKU, Masato
Research Associate:TAMADA, Atsushi
Postdoctoral Fellow:HANAMURA, Kenji 1)
TANIGUCHI, Hiroki 4)
HATANAKA, Yumiko 4)
KUMADA, Tatsuro 4)

The vertebrate nervous system contains a large number of neurons that are connected to each other by specific axonal projections. We are interested in how the complex but precise neuronal network, which is indispensable for functioning of the nervous system, is constructed during development. The goal of our research in this division is to elucidate the cellular and molecular mechanisms underlying the neuronal network formation in vertebrates, with current focuses on the mechanisms of axon guidance and neuronal migration.

I. Mechanism of Axonal Guidance

During development of the nervous system, growing axons are guided through specific pathways to correct targets. Our research interest focuses on the cellular and molecular mechanisms of axon guidance in the vertebrate nervous system. We are particularly inter-ested in how guidance mechanisms operating in differ-ent phases of axonal growth are assembled to generate the complex but precise axonal wiring patterns in the brain. To address these issues, we are first trying to understand axonal wiring patterns during development with reference to the structural organiza-tion of the brain. Using whole-mounted preparations of embry-onic rat brains, we will reveal whole axonal trajectories by labeling with neuronal tracers, such as DiI, or by immunohistochemical staining with antibodies against molecular markers expressed in a subset of neurons. We will next explore the axonal guidance mechanisms generating these wiring patterns. Following questions will be addressed. 1) What structures along the path-way have key roles in axonal guidance? 2) What guidance cues exist in these structures? Are these attractive cues or repulsive cues? Are these short-range cues or long-range cues? 3) What molecules are responsible for these cues? 4) How do multiple guid-ance mechanisms work in concert to generate specific wiring patterns? To answer these questions, we use neuroanatomical techniques, in vitro culture techniques including dissociated cell, explant and whole-mount cultures, and biochemical and molecular biological techniques.

II. Mechanism of Neuronal Migration

A variety of neurons migrate from their birthplace to the position where they finally settle. Neuronal migration in the vertebrate central nervous system occurs both along the radial axis and along the tangential axis of the neural tube. Another interest of our research focuses on the cellular and molecular mechanisms un-derlying the radial and tangential neuronal migration. In many regions of the central nervous system, neurons migrate radially from the ventricular zone where they are born toward the pial surface. We are investigating the mechanisms of radial migration, using neurons in the neocortex as a model system. In addition to the radial migration, some neurons in the brain, such as interneurons in the forebrain, move tangentially for a long distance. We are also investigating how tangentially migrating neurons are guided for a long distance through specific routes to the final positions, using neurons that migrate from the rhombic lip at the dorsal rim of the hindbrain, such as cerebellar granule cells and precerebellar neurons.

To address these issues, we developed in vitro culture systems that reconstruct migratory events occurring in vivo. We labeled migrating neurons with green fluorescent protein (GFP) by transplantation of small piece of explant taken from a transgenic rat expressing GFP or by introducing GFP cDNA into limited regions of the brain by electroporation. Slices of the brain or flat-mounted brain preparation are then cultured on perme-able membrane filters. These culture systems enable us to analyze migration pattern of neurons in real time (Fig. 1). Using these in vitro culture systems, we are currently investigating the cellular and molecular mechanisms of neuronal migration.

Publication List:

Hatanaka, Y. and Murakami, F. (2002) In vitro analysis of the origin, migratory behavior, and maturation of cortical pyramidal cells. J. Comp. Neurol. 454, 1-14.

Saito, Y., Katsumaru, H., Wilson, C. J. and Murakami, F. (2001) Light and electron microscopic study of corticorubral synapses in adult cat: evidence for extensive synaptic remodeling during postnatal development. J. Comp. Neurol. 440, 236-44.

Takemoto, M., Fukuda, T., Sonoda, R., Murakami, F., Tanaka, H. and Yamamoto, N. (2002) Ephrin-B3-EphA4 interactions regulate the growth of specific thalamocortical axon populations in vitro. Eur. J. Neurosci. 16, 1168-72.

Taniguchi, H., Tamada, A., Kennedy, T. E. and Murakami, F. (2002) Crossing the ventral midline causes neurons to change their response to floor plate and alar plate attractive cues during transmedian migration. Dev. Biol. 249, 321-32.

Yamamoto, N., Tamada, A. and Murakami, F. Wiring of the brain by a range of guidance cues. Prog. Neurobiol. (in press)

Figure 1. Migrating neocortical neurons visualized with green fluorescent protein (GFP) in vitro.
(Left) Slice culture of rat neocortex that was introduced with GFP cDNA into the ventricular zone by electroporation. A broken line shows the outer margin of the slice. GFP-positive neurons were moving radially from the ventricular zone (bottom) toward the pial surface (top).
(Right) High power view of labeled migrating neurons. Leading processes of neurons extended toward the pial surface.

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