Abstract

The aim of this proposal is to study the earliest events in the development of the inner ear. One half of all cases of deafness in children are caused by inherited defects in genes that control the development or function of the inner ear. Despite the clinical significance of the inner ear, little is known about the early development of this sensory organ. The entire inner ear develops from a patch of thickened ectoderm on either side of the hindbrain called the otic placode. The otic placode is believed to be induced by signals from neighboring inducing tissues. We hypothesize that signaling molecules produced by these up-regulate of gene expression.
Specific Aim 1 : Induction of the otic placode is thought to be directly regulated by one or both of two candidate inducing tissues-the hind brain of the cranial paraxial mesoderm. We will test these candidate inducing tissues with responding ectoderm in a neutral tissue culture system (sufficiency experiments). Induction will be assayed using six molecular markers of the otic placode that we have recently identified. Specifc Aim 2: Two members of the fibroblast growth fibroblast growth factor (FGF) family, FGF-2 and FGF-3 have been proposed to play a role in otic placode induction, but no studies to date have rigorously tested the necessity or sufficiency of FGF signaling in this process. Accordingly, we will determine whether FGF signaling is necessary of sufficient for the induction of the otic placode by gain-and-loss of function experiment using pharmacological and dominant-negative inhibitors of FGF signaling, and application of FGF family members in vivo and in vitro.
Specific Aim 3 : We have identified 5 members of the chicken Dix family of homeobox-containing transcription factors, Dix -2,3,4,5 and 6. Several of these genes are expressed in the development of otic placode. We propose that Dix gene function is required to activate otic placode-specific gene expression in cranial ectoderm in response to inducing signals. We will determine whether members of the dix family of transcriptional regulators are necessary for the induction of the otic placode by creating dominantnegative constructs of these five Dix genes and expressing them in otic placode ectoderm

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Deafness and Other Communication Disorders (NIDCD)
Type
Research Project (R01)
Project #
5R01DC004675-04
Application #
6710654
Study Section
Special Emphasis Panel (ZRG1-IFCN-6 (01))
Program Officer
Freeman, Nancy
Project Start
2001-03-01
Project End
2006-02-28
Budget Start
2004-03-01
Budget End
2005-02-28
Support Year
4
Fiscal Year
2004
Total Cost
$261,625
Indirect Cost

  Institution

Name
House Ear Institute
Department
Type
DUNS #
062076989
City
Los Angeles
State
CA
Country
United States
Zip Code
90057

  Publications

Birol, Onur; Ohyama, Takahiro; Edlund, Renée K et al. (2016) The mouse Foxi3 transcription factor is necessary for the development of posterior placodes. Dev Biol 409:139-151
Edlund, Renée K; Ohyama, Takahiro; Kantarci, Husniye et al. (2014) Foxi transcription factors promote pharyngeal arch development by regulating formation of FGF signaling centers. Dev Biol 390:1-13
Khatri, Safia B; Edlund, Renée K; Groves, Andrew K (2014) Foxi3 is necessary for the induction of the chick otic placode in response to FGF signaling. Dev Biol 391:158-69
Groves, Andrew K; LaBonne, Carole (2014) Setting appropriate boundaries: fate, patterning and competence at the neural plate border. Dev Biol 389:2-12
Yang, Lu; O'Neill, Paul; Martin, Kareen et al. (2013) Analysis of FGF-dependent and FGF-independent pathways in otic placode induction. PLoS One 8:e55011
Khatri, Safia B; Groves, Andrew K (2013) Expression of the Foxi2 and Foxi3 transcription factors during development of chicken sensory placodes and pharyngeal arches. Gene Expr Patterns 13:38-42
Basch, Martín L; Ohyama, Takahiro; Segil, Neil et al. (2011) Canonical Notch signaling is not necessary for prosensory induction in the mouse cochlea: insights from a conditional mutant of RBPjkappa. J Neurosci 31:8046-58
Jayasena, Chathurani S; Ohyama, Takahiro; Segil, Neil et al. (2008) Notch signaling augments the canonical Wnt pathway to specify the size of the otic placode. Development 135:2251-61
Ohyama, Takahiro; Mohamed, Othman A; Taketo, Makoto M et al. (2006) Wnt signals mediate a fate decision between otic placode and epidermis. Development 133:865-75
Martin, Kareen; Groves, Andrew K (2006) Competence of cranial ectoderm to respond to Fgf signaling suggests a two-step model of otic placode induction. Development 133:877-87

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