Abstract

Component Project I: Position-Specific Functions of no tail (ntl): Untangling the Pleiotropy of the no tail Mutant Principal Investigator: David Jonah Grunwald;Co-Investigator: H. Joseph Yost T-box genes encode related transcription factors that regulate development of organs and regions of the body. Of the >20 known members of the family, mutations in five genes have been linked to human congenital disorders. Despite extensive study, the phenotypes caused by T-box mutations in humans, mice, or zebrafish are complex and poorly understood: multiple tissue types are affected, and in no case has a unifying cellular defect been identified that accounts for all developmental defects of a mutant. We propose that pleiotropy is an intrinsic feature of T-box genes that needs to be deconvoluted to understand the cellular basis of T-box mutant phenotypes. Here we test two hypotheses that that would account for why loss of a Tbox transcription factor frequently results in a multiplicity of cell type defects. First, we propose that individual T-box transcription factors have different sets of downstream target genes in different regions of the embryo, thus explaining the recurrent pleiotropy of T-box mutants. Second, we propose that one factor that contributes to diversification of T-box factor function is interaction with additional T-box transcription factors. Hence loss of one T-box transcription factor affects the function of other T-box factors that continue to be expressed in a developmental field. Component Project I analyzes the downstream functions controlled by no tail, the zebrafish orthologue of the vertebrate Brachyury/TJ-box gene, no tail is expressed throughout the mesoderm and required for development of the notochord, the posterior mesoderm, and the tail organ, Kupffer's Vesicle. The goals of Component Project I are: 1) identify the position-specific transcription activities of the No Tail protein;2) analyze how interactions with additional T-box factors contribute to the position-specific activities of No Tail; and 3) test the idea that distinct direct target genes of NTL carry out independent position/tissue-specific developmental functions of no tail.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
5P01HD048886-04
Application #
8053381
Study Section
Pediatrics Subcommittee (CHHD)
Project Start
Project End
Budget Start
2010-03-01
Budget End
2011-02-28
Support Year
4
Fiscal Year
2010
Total Cost
$205,490
Indirect Cost

  Institution

Name
University of Utah
Department
Type
DUNS #
009095365
City
Salt Lake City
State
UT
Country
United States
Zip Code
84112

  Publications

Morrow, Zachary T; Maxwell, Adrienne M; Hoshijima, Kazuyuki et al. (2017) tbx6l and tbx16 are redundantly required for posterior paraxial mesoderm formation during zebrafish embryogenesis. Dev Dyn 246:759-769
Yabe, Taijiro; Hoshijima, Kazuyuki; Yamamoto, Takashi et al. (2016) Quadruple zebrafish mutant reveals different roles of Mesp genes in somite segmentation between mouse and zebrafish. Development 143:2842-52
Ota, Satoshi; Hisano, Yu; Muraki, Michiko et al. (2013) Efficient identification of TALEN-mediated genome modifications using heteroduplex mobility assays. Genes Cells 18:450-8
Kruse-Bend, Renee; Rosenthal, Jude; Quist, Tyler S et al. (2012) Extraocular ectoderm triggers dorsal retinal fate during optic vesicle evagination in zebrafish. Dev Biol 371:57-65
Xing, Lingyan; Hoshijima, Kazuyuki; Grunwald, David J et al. (2012) Zebrafish foxP2 zinc finger nuclease mutant has normal axon pathfinding. PLoS One 7:e43968
Dahlem, Timothy J; Hoshijima, Kazuyuki; Jurynec, Michael J et al. (2012) Simple methods for generating and detecting locus-specific mutations induced with TALENs in the zebrafish genome. PLoS Genet 8:e1002861
Bisgrove, Brent W; Makova, Svetlana; Yost, H Joseph et al. (2012) RFX2 is essential in the ciliated organ of asymmetry and an RFX2 transgene identifies a population of ciliated cells sufficient for fluid flow. Dev Biol 363:166-78
Wang, Xu; Kopinke, Daniel; Lin, Junji et al. (2012) Wnt signaling regulates postembryonic hypothalamic progenitor differentiation. Dev Cell 23:624-36
Demarest, Bradley L; Horsley, Wyatt H; Locke, Erin E et al. (2011) Trans-centromere effects on meiotic recombination in the zebrafish. Genetics 187:333-6
Wythe, Joshua D; Jurynec, Michael J; Urness, Lisa D et al. (2011) Hadp1, a newly identified pleckstrin homology domain protein, is required for cardiac contractility in zebrafish. Dis Model Mech 4:607-21

Showing the most recent 10 out of 13 publications