Zebrafish fins provide an excellent model system for revealing the molecular mechanisms controlling size and shape. Fins grow by the addition of bony segments to the distal ends of growing fin rays. Therefore, fin length mutants that produce short segments may identify molecules that regulate bone morphogenesis. Indeed, the short fin mutant produces short fin ray segments, and this phenotype is caused by mutations in zebrafish connexin43. Interestingly, mutations in human connexin43 cause oculodentodigital dysplasia, a syndrome which results in craniofacial and limb malformations. Thus, connexin43 controls the morphology of dermal bone in both zebrafish and humans, and may therefore play similar roles in the regulation of size and shape in these tissues. The underlying goal of this proposal is to correlate the function of connexin43 with the cellular and molecular events of segment morphogenesis. This will be accomplished by four aims. First, several new alleles of connexin43 that modify or limit gap junction intercellular communication will be generated. Second, gap junction communication will be monitored in different alleles of connexin43 in a heterologous assay for cell-cell communication. Third, connexin43 expression will be monitored with respect to the cellular events required for segment morphogenesis, such as cell proliferation and osteoblast differentiation. Finally, the cellular basis for short segments will be examined by monitoring these processes in short fin mutants. Thus, the aims of this proposal will provide immediate insights into the control of bony segment growth in zebrafish. Furthermore, these insights will directly facilitate future understanding of the biology of human bone malformations.

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD047737-02
Application #
7048627
Study Section
Special Emphasis Panel (ZRG1-DEV-1 (01))
Program Officer
Javois, Lorette Claire
Project Start
2005-04-01
Project End
2010-03-31
Budget Start
2006-04-01
Budget End
2007-03-31
Support Year
2
Fiscal Year
2006
Total Cost
$221,534
Indirect Cost
Name
Lehigh University
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
808264444
City
Bethlehem
State
PA
Country
United States
Zip Code
18015
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Ton, Quynh V; Iovine, M Kathryn (2013) Determining how defects in connexin43 cause skeletal disease. Genesis 51:75-82
Ton, Quynh V; Kathryn Iovine, M (2012) Semaphorin3d mediates Cx43-dependent phenotypes during fin regeneration. Dev Biol 366:195-203
Gerhart, Sarah V; Jefferis, Rebecca; Iovine, M Kathryn (2009) Cx40.8, a Cx43-like protein, forms gap junction channels inefficiently and may require Cx43 for its association at the plasma membrane. FEBS Lett 583:3419-24
Gumm, Jennifer M; Snekser, Jennifer L; Iovine, M Kathryn (2009) Fin-mutant female zebrafish (Danio rerio) exhibit differences in association preferences for male fin length. Behav Processes 80:35-8
Sims Jr, Kenneth; Eble, Diane M; Iovine, M Kathryn (2009) Connexin43 regulates joint location in zebrafish fins. Dev Biol 327:410-8
Brown, Andrew M; Fisher, Shannon; Iovine, M Kathryn (2009) Osteoblast maturation occurs in overlapping proximal-distal compartments during fin regeneration in zebrafish. Dev Dyn 238:2922-8
Hoptak-Solga, Angela D; Nielsen, Sarah; Jain, Isha et al. (2008) Connexin43 (GJA1) is required in the population of dividing cells during fin regeneration. Dev Biol 317:541-8
Hoptak-Solga, Angela D; Klein, Kathryn A; DeRosa, Adam M et al. (2007) Zebrafish short fin mutations in connexin43 lead to aberrant gap junctional intercellular communication. FEBS Lett 581:3297-302
Goldsmith, Matthew I; Iovine, M Kathryn; O'Reilly-Pol, Thomas et al. (2006) A developmental transition in growth control during zebrafish caudal fin development. Dev Biol 296:450-7