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Published online before print October 2, 2007, 10.1101/gad.1592107
GENES & DEVELOPMENT 21:2593-2606, 2007
©2007 by Cold Spring Harbor Laboratory Press; ISSN 0890-9369/ $5.00
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The requirement for Phr1 in CNS axon tract formation reveals the corticostriatal boundary as a choice point for cortical axons

A. Joseph Bloom1, Bradley R. Miller1, Joshua R. Sanes2, and Aaron DiAntonio1,3

1 Department of Molecular Biology and Pharmacology, Washington University, Saint Louis, Missouri 63110, USA; 2 Department of Molecular and Cellular Biology, Harvard University, Cambridge, Massachusetts 02138, USA

Phr1 is the single well-conserved murine ortholog of the invertebrate ubiquitin ligase genes highwire (in Drosophila) and rpm-1 (in Caenorhabditis elegans). The function and mechanism of action of highwire and rpm-1 are similar—both cell-autonomously regulate synaptogenesis by down-regulating the ortholog of the mitogen-activated protein kinase kinase kinase dual leucine zipper kinase (MAPKKK DLK). Here, using a targeted conditional mutant, we demonstrate that Phr1 also plays essential roles in mammalian neural development. As in invertebrates, Phr1 functions cell-autonomously to sculpt motor nerve terminals. In addition, Phr1 plays essential roles in the formation of major CNS axon tracts including those of the internal capsule, in part via cell-nonautonomous mechanisms, and these results reveal a choice point for cortical axons at the corticostriatal boundary. Furthermore, whereas the neurite morphology phenotypes of highwire and rpm-1 are suppressed by loss of DLK in flies and worms, Phr1-dependent CNS defects persist in Phr1, DLK double mutants. Thus, in the mammalian nervous system Phr1 is required for formation of major CNS axon tracts via a mechanism that is both cell-nonautonomous and independent of DLK.

[Keywords: Axon guidance; synapse formation; internal capsule; neuromuscular junction; DLK]

Received July 11, 2007; revised version accepted August 17, 2007.

3 Corresponding author.

E-MAIL diantonio{at}wustl.edu; FAX (314) 362-7058.

Supplemental material is available at http://www.genesdev.org.

Article published online ahead of print. Article and publication date are online at http://www.genesdev.org/cgi/doi/10.1101/gad.1592107


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