[return to list
Xiaowei  Lu
Degree(s): Ph.D.
Graduate School: Massachusetts Institute of Technology
Primary Appointment: Assistant Professor of Cell Biology
Research Interests:
Developmental regulation of planar cell polarity in the mammalian nervous system

Email Address: xl6f@virginia.edu
Biomedical Sciences Graduate Program(s)
  • Molecular Cell and Developmental Biology
  • Neuroscience
  • Biochemistry, Molecular Biology and Genetics
    • Research Description

    Cell polarity is tightly coupled to specialized cell functions and is
    fundamental to many cellular processes in development and disease. Two forms
    of epithelial polarity have been observed: one along the apical-basal axis,
    and one orthogonal to the apical-basal axis known as planar cell polarity
    (PCP). The Lu lab is interested in dissecting the signaling events that
    generate planar asymmetry and the resulting cellular behaviors during
    mammalian development, with a specific focus on two types of polarized cells
    in the nervous system, namely neuroepithelial cells and neurons.

    It has been shown that an evolutionarily conserved noncanonical,
    b-catenin-independent Wnt pathway regulates PCP and is involved in diverse
    processes such as neural tube closure and cochlear hair cell morphogenesis.
    Recently, in a gene trap screen in the mouse, we identified PTK7, an
    atypical receptor tyrosine kinase, as a novel regulator of PCP in
    vertebrates. Interestingly, homologs of several vertebrate PCP genes,
    including PTK7, have not been implicated in PCP signaling in Drosophila,
    suggesting that vertebrates have evolved novel strategies to regulate PCP.
    Using PTK7 as an entry point, we are taking a combination of biochemical,
    genetic and cell biological approaches to further elucidate signaling
    mechanisms by which the PCP pathway exert its effect on cellular machinery,
    such as the cytoskeleton and protein trafficking network.

    The cochlear sensory epithelium of the mouse offers an attractive system to
    study PCP at a single cell resolution both in vivo and in organotypic
    cultures. PCP is manifested by the asymmetric orientation of the hair cell
    stereocilia, an actin-rich structure responsible of mechanotransduction.
    Using a variety of genetic and molecular manipulations and imaging
    techniques, experiments are underway to better understand the sequence of
    events that lead to coordinated polarized outgrowth of stereocilia across
    the sensory epithelium.

    We are extending our analysis of the PCP pathway into the development of the
    central nervous system. Our preliminary analysis of mutant phenotype
    suggests that PCP pathway is involved in patterning certain regions of the
    CNS. Currently we are investigating the molecular pathway that underlies the
    patterning defect. Furthermore, aided by expression studies, we hypothesize
    that PCP signaling also functions in later aspects of CNS development, such
    as cell and axon migration and target selection. We plan to use transgenic
    mice and in vitro neuronal cultures to test this hypothesis.

    Ultimately, we hope that our studies will shed light on how the versatile
    PCP pathway controls cell polarity in different contexts during normal
    development and how mutations disrupt polarity in related human disease and
    birth defects.

    Selected Publications
  • Friedel, R.H., Plump, A., Lu, X., Spilker, K., Jolicoeur, C., Wong, K.,Venkatesh, T., Yaron, A., Hynes, M., Chen, B., Okada, A., McConnell, S.K., Rayburn, H. and Tessier-Lavigne, M. (2005). Gene targeting using a promoterless gene trap vector (³targeted trapping²) is an efficient method to mutate a large fraction of genes. PNAS, in press.
  • Lu, X., Le Noble, F., Yuan, L., Jiang, Q., De Lafarge, B. P., Sugiyama, D., Bréant, C., Claes, F., De Smet, F., Thomas, J-L., Autiero, M., Carmeliet. P., Tessier-Lavigne, M. and Eichmann, A. (2004) The Netrin receptor UNC5B mediates guidance events controlling morphogenesis of the vascular system. Nature 432, 179-186. (*These authors contributed equally to this work.)
  • Lu, X., Borchers, A., Jolicoeur, C., Rayburn, H., Baker, J. C. and Tessier-Lavigne, M. (2004) PTK7/CCK-4 is a novel regulator of planar cell polarity in vertebrates. Nature 430, 93-98.
  • Leighton, P. A.*, Mitchell, K. J.*, Goodrich, L. V.*, Lu, X., Pinson, K., Scherz, P., Skarnes, W. C., and Tessier-Lavigne, M. (2001). Defining brain wiring patterns and mechanisms through gene trapping in mice. Nature 410, 174-179. (*These authors contributed equally to this work.)
  • PubMed Link for this Faculty Member
    • Intranet Profile
    [To add/update Intranet profile information, read these instructions.]
    Contact Information
      Office Address: PO Box 800732, 
      Office Phone: +1 434-982-6528

    (Find Out How to Update Your Faculty Profile)