Abstract

The establishment of specific axon connections depends on the interaction of growth cone receptors with positive and negative guidance cues in the neuronal environment. T-cadherin (Ranscht and Dours-Zimmermann, Neuron 7:391-402) is distributed on subpopulations of growing axons and delineates specific regions in the pathway of growing commissural and motor axons. Preliminary functional studies suggest that T-cadherin acts as an inhibitor of neurite growth. The current proposal aims to extend knowledge about the distribution of T-cadherin to the CNS and to experimentally define the function and mechanism of T-cadherin in axon growth and pathway selection using in vitro assays. First, we will study T-cadherin's spatial and temporal distribution in the developing chick brain and specifically focus on the expression pattern during early neurogenesis. Second, we will determine the effect of T-cadherin substrates on neurite growth and growth cone recognition in vitro. Different neuron populations will be tested for their responses to T-cadherin using both uniform T-cadherin substrates and choice assays. In both assays, growth cone interactions with T-cadherin will be compared to those with neurite-promoting N-cadherin. Possible effects will be neutralized with specific antibodies, recombinant proteins and antisense oligonucleotides. Third, to study the mechanism of T- cadherin-induced growth cone responses, we will determine if T-cadherin- elicited growth cone responses involve homophilic or heterophilic recognition. We will determine if T-cadherin-induced growth cone interaction induce signal transduction events in the growth cone and obtain evidence for or against the participation of G-proteins, calcium-signaling and phosphorylation events. Fourth, we will define the responsible molecular domains that regulate T-cadherin-induced growth cone avoidance and N-cadherin-simulated neurite growth. We will test mutated T-cadherin molecule, in which selected regions of T-cadherin are eliminated or replaced with the corresponding region of N-cadherin and vice versa, in neurite growth and choice assays.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
5P01HD025938-07
Application #
5212712
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
7
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Yotsumoto, Fusanori; You, Weon-Kyoo; Cejudo-Martin, Pilar et al. (2015) NG2 proteoglycan-dependent recruitment of tumor macrophages promotes pericyte-endothelial cell interactions required for brain tumor vascularization. Oncoimmunology 4:e1001204
Arranz, Amaia M; Perkins, Katherine L; Irie, Fumitoshi et al. (2014) Hyaluronan deficiency due to Has3 knock-out causes altered neuronal activity and seizures via reduction in brain extracellular space. J Neurosci 34:6164-76
Vargas, Lina M; Leal, Nancy; Estrada, Lisbell D et al. (2014) EphA4 activation of c-Abl mediates synaptic loss and LTP blockade caused by amyloid-? oligomers. PLoS One 9:e92309
You, Weon-Kyoo; Yotsumoto, Fusanori; Sakimura, Kenji et al. (2014) NG2 proteoglycan promotes tumor vascularization via integrin-dependent effects on pericyte function. Angiogenesis 17:61-76
Cattaruzza, Sabrina; Ozerdem, Ugur; Denzel, Martin et al. (2013) Multivalent proteoglycan modulation of FGF mitogenic responses in perivascular cells. Angiogenesis 16:309-27
Tigges, Ulrich; Komatsu, Masanobu; Stallcup, William B (2013) Adventitial pericyte progenitor/mesenchymal stem cells participate in the restenotic response to arterial injury. J Vasc Res 50:134-44
Falivelli, Giulia; Lisabeth, Erika Mathes; Rubio de la Torre, Elena et al. (2013) Attenuation of eph receptor kinase activation in cancer cells by coexpressed ephrin ligands. PLoS One 8:e81445
Noberini, Roberta; Koolpe, Mitchell; Lamberto, Ilaria et al. (2012) Inhibition of Eph receptor-ephrin ligand interaction by tea polyphenols. Pharmacol Res 66:363-73
Gibby, Krissa; You, Weon-Kyoo; Kadoya, Kuniko et al. (2012) Early vascular deficits are correlated with delayed mammary tumorigenesis in the MMTV-PyMT transgenic mouse following genetic ablation of the NG2 proteoglycan. Breast Cancer Res 14:R67
Noberini, Roberta; Rubio de la Torre, Elena; Pasquale, Elena B (2012) Profiling Eph receptor expression in cells and tissues: a targeted mass spectrometry approach. Cell Adh Migr 6:102-12

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