TY - JOUR
T1 - An infectious progenitor for the murine IAP retrotransposon
T2 - Emergence of an intracellular genetic parasite from an ancient retrovirus
AU - Ribet, David
AU - Harper, Francis
AU - Dupressoir, Anne
AU - Dewannieux, Marie
AU - Pierron, Gérard
AU - Heidmann, Thierry
PY - 2008/4/1
Y1 - 2008/4/1
N2 - Mammalian genomes contain a high load of mobile elements among which long terminal repeat (LTR)-retrotransposons may represent up to 10% of the genomic DNA. The murine intracisternal A-type particle (IAP) sequences, the prototype of these mammalian "genetic parasites," have an intracellular replicative life cycle and are responsible for a very large fraction of insertional mutagenesis in mice. Yet, phylogenetic analyses strongly suggest that they derive from an ancestral retrovirus that has reached the germline of a remote rodent ancestor and has been "endogenized." A genome-wide screening of the mouse genome now has led us to identify the likely progenitor of the intracellular IAP retrotransposons. This identified "living fossil" - that we found to be present only as a single fully active copy - discloses all the characteristics of a bona fide retrovirus, with evidence for particle formation at the cell membrane, and release of virions with a mature morphology that are infectious. We show, by generating appropriate chimeras, that IAPs derive from this element via passive loss of its env gene, and gain of an endoplasmic reticulum targeting signal, resulting in its "intracellularization" and in the gain of transpositional activity. The identification within the mouse genome of the still active retroviral progenitor of the IAP endogenous mobile elements and the experimental dissection of the molecular events responsible for the shift in its life cycle provide a conclusive illustration of the process that has led, during evolution, to the generation of very successful intracellular retrotransposons from ancient retroviruses.
AB - Mammalian genomes contain a high load of mobile elements among which long terminal repeat (LTR)-retrotransposons may represent up to 10% of the genomic DNA. The murine intracisternal A-type particle (IAP) sequences, the prototype of these mammalian "genetic parasites," have an intracellular replicative life cycle and are responsible for a very large fraction of insertional mutagenesis in mice. Yet, phylogenetic analyses strongly suggest that they derive from an ancestral retrovirus that has reached the germline of a remote rodent ancestor and has been "endogenized." A genome-wide screening of the mouse genome now has led us to identify the likely progenitor of the intracellular IAP retrotransposons. This identified "living fossil" - that we found to be present only as a single fully active copy - discloses all the characteristics of a bona fide retrovirus, with evidence for particle formation at the cell membrane, and release of virions with a mature morphology that are infectious. We show, by generating appropriate chimeras, that IAPs derive from this element via passive loss of its env gene, and gain of an endoplasmic reticulum targeting signal, resulting in its "intracellularization" and in the gain of transpositional activity. The identification within the mouse genome of the still active retroviral progenitor of the IAP endogenous mobile elements and the experimental dissection of the molecular events responsible for the shift in its life cycle provide a conclusive illustration of the process that has led, during evolution, to the generation of very successful intracellular retrotransposons from ancient retroviruses.
UR - http://www.scopus.com/inward/record.url?scp=41649117808&partnerID=8YFLogxK
U2 - 10.1101/gr.073486.107
DO - 10.1101/gr.073486.107
M3 - Article
C2 - 18256233
AN - SCOPUS:41649117808
SN - 1088-9051
VL - 18
SP - 597
EP - 609
JO - Genome Research
JF - Genome Research
IS - 4
ER -