DigitalCommons@University of Nebraska - Lincoln - Rebecca LaRue, Stefán Jónsson, Kevin Silverstein, Mathieu Lajoie, Denis Bertrand, Nadia El-Mabrouk, Isidro Hötzel, Valgerdur Andrésdóttir, Timothy Smith, and Reuben Harris: The Artiodactyl <i>APOBEC3</i> Innate Immune Repertoire Shows Evidence for a Multi-Functional Domain Organization that Existed in the Ancestor of Placental Mammals

USDA Agricultural Research Service --Lincoln, Nebraska

Publications from USDA-ARS / UNL Faculty

Title

The Artiodactyl APOBEC3 Innate Immune Repertoire Shows Evidence for a Multi-Functional Domain Organization that Existed in the Ancestor of Placental Mammals

Authors

Rebecca LaRue, University of Minnesota, Minneapolis, Minnesota
Stefán Jónsson, University of Minnesota, Minneapolis, Minnesota
Kevin Silverstein, University of Minnesota, Minneapolis, Minnesota
Mathieu Lajoie, University of Minnesota, Minneapolis, Minnesota
Denis Bertrand, University of Minnesota, Minneapolis, Minnesota
Nadia El-Mabrouk, University of Minnesota, Minneapolis, Minnesota
Isidro Hötzel, Washington State University, Pullman, Washington
Valgerdur Andrésdóttir, University of Iceland, Institute for Experimental Pathology, Keldur v/Vesturlandsveg, 112 Reykjavík, Iceland
Timothy Smith, USDA/ARS
Reuben Harris, University of Minnesota, Minneapolis, Minnesota

Document Type

Article

Date of this Version

2008

Comments

Published in BMC Molecular Biology 2008, 9:104.

Abstract

Background: APOBEC3 (A3) proteins deaminate DNA cytosines and block the replication of retroviruses and retrotransposons. Each A3 gene encodes a protein with one or two conserved zinccoordinating
motifs (Z1, Z2 or Z3). The presence of one A3 gene in mice (Z2–Z3) and seven in humans, A3A-H (Z1a, Z2a-Z1b, Z2b, Z2c-Z2d, Z2e-Z2f, Z2g-Z1c, Z3), suggests extraordinary evolutionary flexibility. To gain insights into the mechanism and timing of A3 gene expansion and into the functional modularity of these genes, we analyzed the genomic sequences, expressed cDNAs and activities of the full A3 repertoire of three artiodactyl lineages: sheep, cattle and pigs.
Results: Sheep and cattle have three A3 genes, A3Z1, A3Z2 and A3Z3, whereas pigs only have two, A3Z2 and A3Z3. A comparison between domestic and wild pigs indicated that A3Z1 was deleted in the pig lineage. In all three species, read-through transcription and alternative splicing also produced a catalytically active double domain A3Z2-Z3 protein that had a distinct cytoplasmic localization. Thus, the three A3 genes of sheep and cattle encode four conserved and active proteins. These data, together with phylogenetic analyses, indicated that a similar, functionally modular A3 repertoire existed in the common ancestor of artiodactyls and primates (i.e., the ancestor of placental mammals). This mammalian ancestor therefore possessed the minimal A3 gene set, Z1-Z2-Z3, required to evolve through a remarkable series of eight recombination events into the present day eleven Z domain human repertoire.
<bi>Conclusion: The dynamic recombination-filled history of the mammalian A3 genes is consistent with the modular nature of the locus and a model in which most of these events (especially the expansions) were selected by ancient pathogenic retrovirus infections.

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