A Novel 4EHP-GIGYF2 Translational Repressor Complex Is Essential for Mammalian Development |
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Authors: | Morita Masahiro Ler Lian Wee Fabian Marc R Siddiqui Nadeem Mullin Michael Henderson Valerie C Alain Tommy Fonseca Bruno D Karashchuk Galina Bennett Christopher F Kabuta Tomohiro Higashi Shinji Larsson Ola Topisirovic Ivan Smith Robert J Gingras Anne-Claude Sonenberg Nahum |
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Affiliation: | Department of Biochemistry and Goodman Cancer Research Centre, McGill University, Montréal, Quebec, Canada. |
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Abstract: | The binding of the eukaryotic initiation factor 4E (eIF4E) to the mRNA 5' cap structure is a rate-limiting step in mRNA translation initiation. eIF4E promotes ribosome recruitment to the mRNA. In Drosophila, the eIF4E homologous protein (d4EHP) forms a complex with binding partners to suppress the translation of distinct mRNAs by competing with eIF4E for binding the 5' cap structure. This repression mechanism is essential for the asymmetric distribution of proteins and normal embryonic development in Drosophila. In contrast, the physiological role of the mammalian 4EHP (m4EHP) was not known. In this study, we have identified the Grb10-interacting GYF protein 2 (GIGYF2) and the zinc finger protein 598 (ZNF598) as components of the m4EHP complex. GIGYF2 directly interacts with m4EHP, and this interaction is required for stabilization of both proteins. Disruption of the m4EHP-GIGYF2 complex leads to increased translation and perinatal lethality in mice. We propose a model by which the m4EHP-GIGYF2 complex represses translation of a subset of mRNAs during embryonic development, as was previously reported for d4EHP. |
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