Abstract

Each olfactory neuron responds to a characteristic subset of odorants. Little is known about the pathways by which specific signalling molecules are expressed in particular olfactory neuron types. C. Elegans provides an excellent system in which to investigate how the diversity of the olfactory system is achieved. Mutations in the gene odr-7 were shown to specifically effect the sensory functions of the AWA olfactory neuron type. odr-7 encodes a novel member of the nuclear receptor family, and was shown to regulate the expression of an AWA-specific olfactory receptor.
Our specific aims i n this proposal are three-fold: 1) Identification and Characterization of targets of odr-7 regulation in AWA. The goal is to investigate mechanisms of regulation by odr-7, and to identify signalling genes that function downstream of odr-7. An olfactory receptor gene and a gene encoding a channel- like protein were shown to be regulated by odr-7. The molecular mechanisms of regulation of these genes by odr-7 will be explored, and genetic and behavioral scenes will be used to identify additional targets of odr-7 regulation. 2) Analysis of the effects of spatial control of odr-7 expression. The goal is to determine if odr-7 is sufficient for the expression of AWA-like functions. The effect of odr-7 misexpression on gene expression and function of other chemosensory neuron types will be examined. 3) Identification of additional genes required for the determination of sensory specificity of the AWA neurons. The goal is to identify genes that interact with odr-7 to regulate AWA neuron function. Suppressors of a mutation in the putative DNA- binding domain of Odr-7 will be characterized to identify genes that function together with odr-7. Nuclear receptor proteins have been implicated in immune responses, development and oncogenesis. Investigation of the mechanisms of odr-7 action, and identification of its target will yield new insights into the functions of this important class of transcriptional regulators. Our long term goals are to elucidate the pathways in which odr-7 like genes act in the development and function of sensory neuron types in C. elegans.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Program Projects (P01)
Project #
3P01GM033205-15S1
Application #
6296693
Study Section
Project Start
1998-07-01
Project End
1999-06-30
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
15
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Brandeis University
Department
Type
DUNS #
616845814
City
Waltham
State
MA
Country
United States
Zip Code
02454

  Publications

Vodala, Sadanand; Pescatore, Stefan; Rodriguez, Joseph et al. (2012) The oscillating miRNA 959-964 cluster impacts Drosophila feeding time and other circadian outputs. Cell Metab 16:601-12
Shang, Yuhua; Haynes, Paula; Pírez, Nicolás et al. (2011) Imaging analysis of clock neurons reveals light buffers the wake-promoting effect of dopamine. Nat Neurosci 14:889-95
Hall, Jeffrey C (2005) Systems approaches to biological rhythms in Drosophila. Methods Enzymol 393:61-185
Choi, James C; Park, Demian; Griffith, Leslie C (2004) Electrophysiological and morphological characterization of identified motor neurons in the Drosophila third instar larva central nervous system. J Neurophysiol 91:2353-65
Busza, Ania; Emery-Le, Myai; Rosbash, Michael et al. (2004) Roles of the two Drosophila CRYPTOCHROME structural domains in circadian photoreception. Science 304:1503-6
Park, Demian; Coleman, Melissa J; Hodge, James J L et al. (2002) Regulation of neuronal excitability in Drosophila by constitutively active CaMKII. J Neurobiol 52:24-42
McDonald, M J; Rosbash, M; Emery, P (2001) Wild-type circadian rhythmicity is dependent on closely spaced E boxes in the Drosophila timeless promoter. Mol Cell Biol 21:1207-17
Joiner, M A; Griffith, L C (2000) Visual input regulates circuit configuration in courtship conditioning of Drosophila melanogaster. Learn Mem 7:32-42
Joiner, M A; Griffith, L C (1999) Mapping of the anatomical circuit of CaM kinase-dependent courtship conditioning in Drosophila. Learn Mem 6:177-92
DeSimone, S; Coelho, C; Roy, S et al. (1996) ERECT WING, the Drosophila member of a family of DNA binding proteins is required in imaginal myoblasts for flight muscle development. Development 122:31-9

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