Literature DB >> 27048986

MIR retroposon exonization promotes evolutionary variability and generates species-specific expression of IGF-1 splice variants.

Giosuè Annibalini1, Pamela Bielli2, Mauro De Santi3, Deborah Agostini3, Michele Guescini3, Davide Sisti3, Serena Contarelli3, Giorgio Brandi3, Anna Villarini4, Vilberto Stocchi3, Claudio Sette2, Elena Barbieri5.   

Abstract

Insulin-like growth factor (IGF) -1 is a pleiotropic hormone exerting mitogenic and anti-apoptotic effects. Inclusion or exclusion of exon 5 into the IGF-1 mRNA gives rise to three transcripts, IGF-1Ea, IGF-1Eb and IGF-1Ec, which yield three different C-terminal extensions called Ea, Eb and Ec peptides. The biological significance of the IGF-1 splice variants and how the E-peptides affect the actions of mature IGF-1 are largely unknown. In this study we investigated the origin and conservation of the IGF-1 E-peptides and we compared the pattern of expression of the IGF-1 isoforms in vivo, in nine mammalian species, and in vitro using human and mouse IGF-1 minigenes. Our analysis showed that only IGF-1Ea is conserved among all vertebrates, whereas IGF-1Eb and IGF-1Ec are an evolutionary novelty originated from the exonization of a mammalian interspersed repetitive-b (MIR-b) element. Both IGF-1Eb and IGF-1Ec mRNAs were constitutively expressed in all mammalian species analyzed but their expression ratio varies greatly among species. Using IGF-1 minigenes we demonstrated that divergence in cis-acting regulatory elements between human and mouse conferred species-specific features to the exon 5 region. Finally, the protein-coding sequences of exon 5 showed low rate of synonymous mutations and contain disorder-promoting amino acids, suggesting a regulatory role for these domains. In conclusion, exonization of a MIR-b element in the IGF-1 gene determined gain of exon 5 during mammalian evolution. Alternative splicing of this novel exon added new regulatory elements at the mRNA and protein level potentially able to regulate the mature IGF-1 across tissues and species.
Copyright © 2016 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Alternative splicing; IGF-1 isoforms; Intrinsically disordered regions; Retroposon exonization; Synonymous sites

Mesh:

Substances:

Year:  2016        PMID: 27048986     DOI: 10.1016/j.bbagrm.2016.03.014

Source DB:  PubMed          Journal:  Biochim Biophys Acta        ISSN: 0006-3002


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