The objective of this program is to identify and functionally characterize neurogenic genes that are required for CNS development. Given the high conservation in basic mechanisms used by all metazoans, our search was initiated in the fruit fly (Drosophila melanogaster) where these genes are more accessible for study. Utilizing classical genetic, molecular biology and transgenic techniques, we have continued to study both the function and the regulatory mechanisms that control the expression of castor, a novel Zinc finger gene required for Drosophila CNS development and pollux, castor's close genomic neighbor. Based on its predicted primary structure and the high expression levels in CNS neuro~blasts, castor may regulate itself and other genes involved in neuroblast maturation. To test this hypothesis, we are currently mapping the cis~regulatory elements that control its in vivo expression. Located in its 5' flank, we have found a near perfect 880bp inverted repeat and are now determining if it harbors cis~elements that regulate expression. Once identified, we will assess if lack of or ectopic castor expression modulates reporters that respond to these cis~elements. We are also determining if the pollux protein functions as a membrane~associated adhesion molecule. Analysis of its primary structure reveals that pollux contains an integrin~binding tetrapeptide RGD sequence, multiple glycosaminoglycan~binding sites, and a potential glycosaminoglycan~linkage site. pollux immunostainings have shown that a portion or all of the protein is located on the plasma membrane extracellular surface. In addition, we have observed that misexpression of pollux leads to high levels of mature male homosexual activity. Protein data bank searches, have revealed that pollux shares a 70 amino acid domain with the human tre~1 oncogene and a predicted human myoblast protein (84% and 87% similarity). We have also continued our functional analysis of the murine homeobox gene Hox 1.3 by identifying genes that it regulates. We have observed that ectopic expression of Hox 1.3 in transgenic mice correlates with the apparent repression of a hepatocyte nuclear transcription factor, HNF~3beta. During development, we have also discovered that HNF~3beta is expressed in the CNS and are now assessing if in utero ectopic Hox 1.3 expression modulates its expression.

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Intramural Research (Z01)
Project #
1Z01NS002820-04
Application #
3782408
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
4
Fiscal Year
1993
Total Cost
Indirect Cost
City
State
Country
United States
Zip Code
Yavatkar, Amarendra S; Lin, Yong; Ross, Jermaine et al. (2008) Rapid detection and curation of conserved DNA via enhanced-BLAT and EvoPrinterHD analysis. BMC Genomics 9:106
Brody, Thomas; Rasband, Wayne; Baler, Kevin et al. (2008) Sequence conservation and combinatorial complexity of Drosophila neural precursor cell enhancers. BMC Genomics 9:371
Brody, Thomas; Yavatkar, Amarendra S; Lin, Yong et al. (2008) Horizontal gene transfers link a human MRSA pathogen to contagious bovine mastitis bacteria. PLoS ONE 3:e3074
Kuzin, Alexander; Kundu, Mukta; Brody, Thomas et al. (2007) The Drosophila nerfin-1 mRNA requires multiple microRNAs to regulate its spatial and temporal translation dynamics in the developing nervous system. Dev Biol 310:35-43
Missirlis, Fanis; Kosmidis, Stylianos; Brody, Tom et al. (2007) Homeostatic mechanisms for iron storage revealed by genetic manipulations and live imaging of Drosophila ferritin. Genetics 177:89-100
Brody, Thomas; Rasband, Wayne; Baler, Kevin et al. (2007) cis-Decoder discovers constellations of conserved DNA sequences shared among tissue-specific enhancers. Genome Biol 8:R75
Kuzin, Alexander; Brody, Thomas; Moore, Adrian W et al. (2005) Nerfin-1 is required for early axon guidance decisions in the developing Drosophila CNS. Dev Biol 277:347-65
Brody, Thomas; Odenwald, Ward F (2005) Regulation of temporal identities during Drosophila neuroblast lineage development. Curr Opin Cell Biol 17:672-5
Odenwald, Ward F; Rasband, Wayne; Kuzin, Alexander et al. (2005) EVOPRINTER, a multigenomic comparative tool for rapid identification of functionally important DNA. Proc Natl Acad Sci U S A 102:14700-5
Odenwald, Ward F (2005) Changing fates on the road to neuronal diversity. Dev Cell 8:133-4

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