Molecular Characterization and Placental Expression of HERV-W, a New Human Endogenous Retrovirus Family

Jean-Luc Blond(École Normale Supérieure de Lyon), F. Besème(École Normale Supérieure de Lyon), Laurent Duret(Université Claude Bernard Lyon 1), Olivier Bouton(École Normale Supérieure de Lyon), F. Bedin(École Normale Supérieure de Lyon), Hervé Perron(École Normale Supérieure de Lyon), Bernard Mandrand(École Normale Supérieure de Lyon), François Mallet(École Normale Supérieure de Lyon)
Journal of Virology
February 1, 1999
Cited by 366Open Access
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Abstract

The multiple sclerosis-associated retrovirus (MSRV) isolated from plasma of MS patients was found to be phylogenetically and experimentally related to human endogenous retroviruses (HERVs). To characterize the MSRV-related HERV family and to test the hypothesis of a replication-competent HERV, we have investigated the expression of MSRV-related sequences in healthy tissues. The expression of MSRV-related transcripts restricted to the placenta led to the isolation of overlapping cDNA clones from a cDNA library. These cDNAs spanned a 7.6-kb region containing gag, pol, and env genes; RU5 and U3R flanking sequences; a polypurine tract; and a primer binding site (PBS). As this PBS showed similarity to avian retrovirus PBSs used by tRNATrp, this new HERV family was named HERV-W. Several genomic elements were identified, one of them containing a complete HERV-W unit, spanning all cDNA clones. Elements of this multicopy family were not replication competent, as gag and pol open reading frames (ORFs) were interrupted by frameshifts and stop codons. A complete ORF putatively coding for an envelope protein was found both on the HERV-W DNA prototype and within an RU5-env-U3R polyadenylated cDNA clone. Placental expression of 8-, 3.1-, and 1.3-kb transcripts was observed, and a putative splicing strategy was described. The apparently tissue-restricted HERV-W long terminal repeat expression is discussed with respect to physiological and pathological contexts.


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