Identification of an infectious progenitor for the multiple-copy HERV-K human endogenous retroelements

doi:10.1101/gr.5565706

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Published online before print October 31, 2006, 10.1101/gr.5565706
Genome Res. 16:1548-1556, 2006
©2006 by Cold Spring Harbor Laboratory Press; ISSN 1088-9051/06 $5.00

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Letter

Identification of an infectious progenitor for the multiple-copy HERV-K human endogenous retroelements

Marie Dewannieux¹^,3, Francis Harper²^,4, Aurélien Richaud¹^,4, Claire Letzelter¹, David Ribet¹, Gérard Pierron², and Thierry Heidmann¹^,5

¹ Unité des Rétrovirus Endogènes et Eléments Rétroïdes des Eucaryotes Supérieurs, UMR 8122 CNRS, Institut Gustave Roussy, 94805 Villejuif Cedex, France; ² Laboratoire de Réplication de l’ADN et Ultrastructure du Noyau, UPR1983 Institut André Lwoff, 94801 Villejuif Cedex, France

Human Endogenous Retroviruses are expected to be the remnantsof ancestral infections of primates by active retroviruses thathave thereafter been transmitted in a Mendelian fashion. Here,we derived in silico the sequence of the putative ancestral"progenitor" element of one of the most recently amplified family—theHERV-K family—and constructed it. This element, Phoenix,produces viral particles that disclose all of the structuraland functional properties of a bona-fide retrovirus, can infectmammalian, including human, cells, and integrate with the exactsignature of the presently found endogenous HERV-K progeny.We also show that this element amplifies via an extracellularpathway involving reinfection, at variance with the non-LTR-retrotransposons(LINEs, SINEs) or LTR-retrotransposons, thus recapitulatingex vivo the molecular events responsible for its disseminationin the host genomes. We also show that in vitro recombinationsamong present-day human HERV-K (also known as ERVK) loci cansimilarly generate functional HERV-K elements, indicating thathuman cells still have the potential to produce infectious retroviruses.

³ Present address: Department of Immunology and Molecular Pathology,University College of London, Windeyer Institute, London W1T4JF, UK.

⁴ These authors contributed equally to this work.

⁵ Corresponding author.

E-mail heidmann{at}igr.fr; fax 33-1-42-11-53-42.

[Supplemental material is available online at www.genome.org.]

Article published online before print. Article and publicationdate are at http://www.genome.org/cgi/doi/10.1101/gr.5565706

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