Syncytin is a captive retroviral envelope protein involved in human placental morphogenesis

Mi, Sha
Lee, Xinhua
Li, Xiang-ping
Veldman, Geertruida M.
Finnerty, Heather
Racie, Lisa
LaVallie, Edward
Tang, Xiang-Yang
Edouard, Philippe
Howes, Steve
Keith, James C. Jr
McCoy, John M.

Genetics Institute, Inc., 87 CambridgePark Drive, Cambridge, Massachusetts 02140, USA

*Present address: Biogen Inc., 14 Cambridge Center, Cambridge, Massachusetts 02142, USA

Received 29 April; accepted 20 December 1999.

Correspondence should be directed to J.M.M. (e-mail [email protected]) or S.M. (e-mail [email protected]). Requests for materials should be directed to S.M. The sequence of the syncytin cDNA used in this work can be found in GenBank, accession no. AF208161.

Nature 403(6771):p 785-789, February 17, 2000.

Many mammalian viruses have acquired genes from their hosts during their evolution. The rationale for these acquisitions is usually quite clear: the captured genes are subverted to provide a selective advantage to the virus. Here we describe the opposite situation, where a viral gene has been sequestered to serve an important function in the physiology of a mammalian host. This gene, encoding a protein that we have called syncytin, is the envelope gene of a recently identified human endogenous defective retrovirus, HERV-W. We find that the major sites of syncytin expression are placental syncytiotrophoblasts, multinucleated cells that originate from fetal trophoblasts. We show that expression of recombinant syncytin in a wide variety of cell types induces the formation of giant syncytia, and that fusion of a human trophoblastic cell line expressing endogenous syncytin can be inhibited by an anti-syncytin antiserum. Our data indicate that syncytin may mediate placental cytotrophoblast fusion in vivo, and thus may be important in human placental morphogenesis.