Regulation of Glia Number in Drosophila by Rap/Fzr, an Activator of the Anaphase-Promoting Complex, and Loco, an RGS Protein

doi:10.1534/genetics.107.086397

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Regulation of Glia Number in Drosophila by Rap/Fzr, an Activator of the Anaphase-Promoting Complex, and Loco, an RGS Protein

Margarita E. Kaplow, Adam H. Korayem and Tadmiri R. Venkatesh¹

Department of Biology, City College and The Graduate Center, City University of New York, New York 10031

^¹ Corresponding author: Department of Biology, 138th St. and Convent Ave., City College of New York, New York, NY 10031.
E-mail: venky{at}sci.ccny.cuny.edu

Glia mediate a vast array of cellular processes and are criticalfor nervous system development and function. Despite their immenseimportance in neurobiology, glia remain understudied and themolecular mechanisms that direct their differentiation are poorlyunderstood. Rap/Fzr is the Drosophila homolog of the mammalianCdh1, a regulatory subunit of the anaphase-promoting complex/cyclosome(APC/C). APC/C is an E3 ubiquitin ligase complex well characterizedfor its role in cell cycle progression. In this study, we haveuncovered a novel cellular role for Rap/Fzr. Loss of rap/fzrfunction leads to a marked increase in the number of glia inthe nervous system of third instar larvae. Conversely, ectopicexpression of UAS-rap/fzr, driven by repo-GAL4, results in thedrastic reduction of glia. Data from clonal analyses using theMARCM technique show that Rap/Fzr regulates the differentiationof surface glia in the developing larval nervous system. Ourgenetic and biochemical data further indicate that Rap/Fzr regulatesglial differentiation through its interaction with Loco, a regulatorof G-protein signaling (RGS) protein and a known effector ofglia specification. We propose that Rap/Fzr targets Loco forubiquitination, thereby regulating glial differentiation inthe developing nervous system.