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Cadherin‐8 and N‐cadherin differentially regulate pre‐ and postsynaptic development of the hippocampal mossy fiber pathway
Author(s) -
Bekirov Iddil H.,
Nagy Vanja,
Svoronos Alexandra,
Huntley George W.,
Benson Deanna L.
Publication year - 2008
Publication title -
hippocampus
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.767
H-Index - 155
eISSN - 1098-1063
pISSN - 1050-9631
DOI - 10.1002/hipo.20395
Subject(s) - cadherin , mossy fiber (hippocampus) , neuroscience , postsynaptic potential , hippocampal formation , dentate gyrus , synaptogenesis , biology , axon guidance , axon , microbiology and biotechnology , biological neural network , receptor , cell , genetics
Cells sort into regions and groups in part by their selective surface expression of particular classic cadherins during development. In the nervous system, cadherin‐based sorting can define axon tracts, restrict axonal and dendritic arbors to particular regions or layers, and may encode certain aspects of synapse specificity. The underlying model has been that afferents and their targets hold in common the expression of a particular cadherin, thereby providing a recognition code of homophilic cadherin binding. However, most neurons express multiple cadherins, and it is not clear whether multiple cadherins all act similarly in shaping neural circuitry. Here we asked how two such cadherins, cadherin‐8 and N‐cadherin, influence the guidance and differentiation of hippocampal mossy fibers. Using organotypic hippocampal cultures, we find that cadherin‐8 regulates mossy fiber fasciculation and targeting, but has little effect on CA3 dendrites. In contrast, N‐cadherin regulates mossy fiber fasciculation, but has little impact on axonal growth and targeting. However, N‐cadherin is essential for CA3 dendrite arborization. Both cadherins are required for formation of proper numbers of presynaptic terminals. Mechanistically, such differential actions of these two cadherins could, in theory, reflect coupling to distinct intracellular binding partners. However, we find that both cadherins bind β‐catenin in dentate gyrus (DG). This suggests that cadherins may engage different intracellular signaling cascades downstream of β‐catenin, coopt different extracellular binding partners, or target distinct subcellular domains. Together our findings demonstrate that cadherin‐8 and N‐cadherin are critical for generating the mossy fiber pathway, but that each contributes differentially to afferent and target differentiation, thereby complementing one another in the assembly of a synaptic circuit. © 2007 Wiley‐Liss, Inc.

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