The miti-mere and pdm1 genes collaborate during specification of the RP2/sib lineage in Drosophila neurogenesis

Author:

Bhat K M1,Poole S J1,Schedl P1

Affiliation:

1. Department of Molecular Biology, Princeton University, New Jersey 08544, USA.

Abstract

We have investigated (i) the role of pdm1, a Drosophila POU gene, during the elaboration of the GMC-1-->RP2/sib lineage and (ii) the functional relationship between pdm1 and the closely linked second POU gene, miti-mere, in this lineage. We show that deletion of pdm1 causes a partially penetrant GMC-1 defect, while deletion of both miti and pdm1 results in a fully penetrant defect. This GMC-1 defect in miti- and pdm1- embryos can be rescued by the pdm1 or miti transgene. Rescue is observed only when these genes are expressed at the time of GMC-1 formation. Overexpression of pdm1 or miti well after GMC-1 is formed results in the duplication of RP2 and/or sib cells. Our results indicate that both genes are required for the normal development of this lineage and that the two collaborate during the specification of GMC-1 identity.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

Reference22 articles.

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3. Isolation of a family of Drosophila POU domain genes expressed in early development;Billin A. N.;Mech. Dev.,1991

4. Conservation of a large protein domain in the segmentation gene paired and functionally related genes of Drosophila;Bopp D.;Cell,1986

5. The generation of cell diversity during early neurogenesis in Drosophila;Cabrera C. V.;Development,1992

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