A conserved RNA-protein complex component involved in physiological germline apoptosis regulation in C. elegans

doi:10.1242/dev.02060

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First published online 12 October 2005
doi: 10.1242/dev.02060

Development 132, 4975-4986 (2005)
Published by The Company of Biologists 2005

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A conserved RNA-protein complex component involved in physiological germline apoptosis regulation in C. elegans

Peter R. Boag¹, Akira Nakamura² and T. Keith Blackwell¹^,*

¹ Joslin Diabetes Center and Department of Pathology, Harvard Medical School, One Joslin Place, Boston, MA 02215, USA
² Laboratory for Germline Development, RIKEN Center for Developmental Biology, Kobe, Hyogo 650-0047, Japan

^* Author for correspondence (e-mail: keith.blackwell{at}joslin.harvard.edu)

Accepted 24 August 2005

Two conserved features of oogenesis are the accumulation oftranslationally quiescent mRNA, and a high rate of stage-specificapoptosis. Little is understood about the function of this celldeath. In C. elegans, apoptosis occurring through a specific`physiological' pathway normally claims about half of all developingoocytes. The frequency of this germ cell death is dramaticallyincreased by a lack of the RNA helicase CGH-1, orthologs ofwhich are involved in translational control in oocytes and decapping-dependentmRNA degradation in yeast processing (P) bodies. Here, we describea predicted RNA-binding protein, CAR-1, that associates withCGH-1 and Y-box proteins within a conserved germline RNA-protein(RNP) complex, and in cytoplasmic particles in the gonad andearly embryo. The CGH-1/CAR-1 interaction is conserved in Drosophilaoocytes. When car-1 expression is depleted by RNA interference(RNAi), physiological apoptosis is increased, brood size ismodestly reduced, and early embryonic cytokinesis is abnormal. Surprisingly,if apoptosis is prevented car-1(RNAi) animals are characterizedby a progressive oogenesis defect that leads rapidly to gonad failure.Elevated germ cell death similarly compensates for lack of the translationalregulator CPB-3 (CPEB), orthologs of which function together withCGH-1 in diverse organisms. We conclude that CAR-1 is of critical importancefor oogenesis, that the association between CAR-1 and CGH-1has been conserved, and that the regulation of physiologicalgerm cell apoptosis is specifically influenced by certain functionsof the CGH-1/CAR-1 RNP complex. We propose that this cell deathpathway facilitates the formation of functional oocytes, possiblyby monitoring specific cytoplasmic events during oogenesis.

Key words: Germline, Oocyte, Caenorhabditis elegans, Drosophila, RNA binding, Apoptosis, Cytokinesis, P body

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