- THIS ARTICLE
- Full Text (Rapid PDF)
-
All Versions of this Article:
genetics.105.055152v1
174/2/693 most recent - Alert me when this article is cited
- Alert me if a correction is posted
- SERVICES
- Similar articles in this journal
- Similar articles in PubMed
- Alert me to new issues of the journal
- Download to citation manager
- Reprints & Permissions
- CITING ARTICLES
- Citing Articles via Google Scholar
- GOOGLE SCHOLAR
- Articles by Dürr, K.
- Articles by Driever, W.
- Search for Related Content
- PUBMED
- PubMed Citation
- Articles by Dürr, K.
- Articles by Driever, W.
doi:10.1534/genetics.105.055152
A more recent version of this article appeared on October 1, 2006.
REGULAR RESEARCH PAPERS |
Differential roles of transcriptional mediator complex subunits Crsp34/Med27, Crsp150/Med14, and Trap100/Med24 during zebrafish retinal development
Katrin Dürr 1, Jochen Holzschuh 1, Alida Filippi 1, Anne-Kathrin Ettl 1, Soojin Ryu 1, Iain T Shepherd 2 and Wolfgang Driever 3*
1 University of Freiburg
2 Emory University
3 Unversitat Freiburg
* To whom correspondence should be addressed. E-mail: driever{at}biologie.uni-freiburg.de.
Submitted on December 23, 2005
Revised on January 19, 2006
Accepted on 20 March 2006
The transcriptional mediator complex has emerged as an important component of transcriptional regulation, yet it is largely unknown whether its subunits have differential functions in development. We demonstrate that the zebrafish mutation m885 disrupts a subunit of the mediator complex, Crsp34/Med27. In order to explore the role of the mediator in the control of retinal differentiation, we employed two additional mutations disrupting the mediator subunits Trap100/Med24 and Crsp150/Med14. Our analysis shows that loss of Crsp34/Med27 decreases amacrine cell number, but increases the number of rod photoreceptor cells. In contrast, loss of Trap100/Med24 decreases rod photoreceptor cells. Loss of Crsp150/Med14, on the other hand, only slightly reduces dopaminergic amacrine cells, which are absent from both crsp34m885 and trap100lessen mutant embryos. Our data provide evidence for differential requirements for Crsp34/Med27 in developmental processes. In addition, our data point to divergent functions of the mediator subunits Crsp34/Med27, Trap100/Med24 and Crsp150/Med14, and thus, suggest that subunit composition of the mediator contributes to the control of differentiation in the vertebrate CNS.
Key Words: cell differentiation, mutational analysis, retina, transcriptional mediator complex, zebrafish