Identification of Receptors for Pig Endogenous Retrovirus

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2003 May 13

PMID 12740431

Citations 49

Authors

Thomas A Ericsson

Yasuhiro Takeuchi

Christian Templin

Gary Quinn

Shelli F Farhadian

James C Wood

Beth A Oldmixon

Kristen M Suling

Jennifer K Ishii

Yoshinori Kitagawa

Takayuki Miyazawa

Daniel R Salomon

Robin A Weiss

Clive Patience

Affiliations

Soon will be listed here.

Abstract

Xenotransplantation of porcine tissues has the potential to treat a wide variety of major health problems including organ failure and diabetes. Balanced against the potential benefits of xenotransplantation, however, is the risk of human infection with a porcine microorganism. In particular, the transmission of porcine endogenous retrovirus (PERV) is a major concern [Chapman, L. E. & Bloom, E. T. (2001) J. Am. Med. Assoc. 285, 2304-2306]. Here we report the identification of two, sequence-related, human proteins that act as receptors for PERV-A, encoded by genes located on chromosomes 8 and 17. We also describe homologs from baboon and porcine cells that also are active as receptors. Conversely, activity could not be demonstrated with a syntenic murine receptor homolog. Sequence analysis indicates that PERV-A receptors [human PERV-A receptor (HuPAR)-1, HuPAR-2, baboon PERV-A receptor 2, and porcine PERV-A receptor] are multiple membrane-spanning proteins similar to receptors for other gammaretroviruses. Expression is widespread in human tissues including peripheral blood mononuclear cells, but their biological functions are unknown. The identification of the PERV-A receptors opens avenues of research necessary for a more complete assessment of the retroviral risks of pig to human xenotransplantation.

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