A Family of Insulin-Like Growth Factor II mRNA-Binding Proteins Represses Translation in Late Development

Author:

Nielsen Jacob1,Christiansen Jan1,Lykke-Andersen Jens1,Johnsen Anders H.2,Wewer Ulla M.3,Nielsen Finn C.2

Affiliation:

1. RNA Regulation Centre, Institute of Molecular Biology, 1 and

2. Department of Clinical Biochemistry, Rigshospitalet, 3 Copenhagen, Denmark

3. Institute of Molecular Pathology, 2 University of Copenhagen, and

Abstract

ABSTRACT Insulin-like growth factor II (IGF-II) is a major fetal growth factor. The IGF-II gene generates multiple mRNAs with different 5′ untranslated regions (5′ UTRs) that are translated in a differential manner during development. We have identified a human family of three IGF-II mRNA-binding proteins (IMPs) that exhibit multiple attachments to the 5′ UTR from the translationally regulated IGF-II leader 3 mRNA but are unable to bind to the 5′ UTR from the constitutively translated IGF-II leader 4 mRNA. IMPs contain the unique combination of two RNA recognition motifs and four hnRNP K homology domains and are homologous to the Xenopus Vera and chicken zipcode-binding proteins. IMP localizes to subcytoplasmic domains in a growth-dependent and cell-specific manner and causes a dose-dependent translational repression of IGF-II leader 3 –luciferase mRNA. Mouse IMPs are produced in a burst at embryonic day 12.5 followed by a decline towards birth, and, similar to IGF-II, IMPs are especially expressed in developing epithelia, muscle, and placenta in both mouse and human embryos. The results imply that cytoplasmic 5′ UTR-binding proteins control IGF-II biosynthesis during late mammalian development.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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