TY - JOUR
T1 - Restricted replication of xenotropic murine leukemia virus-related virus in pigtailed macaques
AU - Del Prete, Gregory Q.
AU - Kearney, Mary F.
AU - Spindler, Jon
AU - Wiegand, Ann
AU - Chertova, Elena
AU - Roser, James D.
AU - Estes, Jacob D.
AU - Hao, Xing Pei
AU - Trubey, Charles M.
AU - Lara, Abigail
AU - Lee, Kyeong Eun
AU - Chaipan, Chawaree
AU - Bess, Julian W.
AU - Nagashima, Kunio
AU - Keele, Brandon F.
AU - Macallister, Rhonda
AU - Smedley, Jeremy
AU - Pathak, Vinay K.
AU - KewalRamani, Vineet N.
AU - Coffin, John M.
AU - Lifson, Jeffrey D.
PY - 2012/3
Y1 - 2012/3
N2 - Although xenotropic murine leukemia virus-related virus (XMRV) has been previously linked to prostate cancer and myalgic encephalomyelitis/chronic fatigue syndrome, recent data indicate that results interpreted as evidence of human XMRV infection reflect laboratory contamination rather than authentic in vivo infection. Nevertheless, XMRV is a retrovirus of undefined pathogenic potential that is able to replicate in human cells. Here we describe a comprehensive analysis of two male pigtailed macaques (Macaca nemestrina) experimentally infected with XMRV. Following intravenous inoculation with>1010 RNA copy equivalents of XMRV, viral replication was limited and transient, peaking at<2,200 viral RNA (vRNA) copies/ml plasma and becoming undetectable by 4 weeks postinfection, though viral DNA (vDNA) in peripheral blood mononuclear cells remained detectable through 119 days of follow-up. Similarly, vRNA was not detectable in lymph nodes by in situ hybridization despite detectable vDNA. Sequencing of cell-associated vDNA revealed extensive G-to-A hypermutation, suggestive of APOBECmediated viral restriction. Consistent with limited viral replication, we found transient upregulation of type I interferon responses that returned to baseline by 2 weeks postinfection, no detectable cellular immune responses, and limited or no spread to prostate tissue. Antibody responses, including neutralizing antibodies, however, were detectable by 2 weeks postinfection and maintained throughout the study. Both animals were healthy for the duration of follow-up. These findings indicate that XMRV replication and spread were limited in pigtailed macaques, predominantly by APOBEC-mediated hypermutation. Given that human APOBEC proteins restrict XMRV infection in vitro, human XMRV infection, if it occurred, would be expected to be characterized by similarly limited viral replication and spread.
AB - Although xenotropic murine leukemia virus-related virus (XMRV) has been previously linked to prostate cancer and myalgic encephalomyelitis/chronic fatigue syndrome, recent data indicate that results interpreted as evidence of human XMRV infection reflect laboratory contamination rather than authentic in vivo infection. Nevertheless, XMRV is a retrovirus of undefined pathogenic potential that is able to replicate in human cells. Here we describe a comprehensive analysis of two male pigtailed macaques (Macaca nemestrina) experimentally infected with XMRV. Following intravenous inoculation with>1010 RNA copy equivalents of XMRV, viral replication was limited and transient, peaking at<2,200 viral RNA (vRNA) copies/ml plasma and becoming undetectable by 4 weeks postinfection, though viral DNA (vDNA) in peripheral blood mononuclear cells remained detectable through 119 days of follow-up. Similarly, vRNA was not detectable in lymph nodes by in situ hybridization despite detectable vDNA. Sequencing of cell-associated vDNA revealed extensive G-to-A hypermutation, suggestive of APOBECmediated viral restriction. Consistent with limited viral replication, we found transient upregulation of type I interferon responses that returned to baseline by 2 weeks postinfection, no detectable cellular immune responses, and limited or no spread to prostate tissue. Antibody responses, including neutralizing antibodies, however, were detectable by 2 weeks postinfection and maintained throughout the study. Both animals were healthy for the duration of follow-up. These findings indicate that XMRV replication and spread were limited in pigtailed macaques, predominantly by APOBEC-mediated hypermutation. Given that human APOBEC proteins restrict XMRV infection in vitro, human XMRV infection, if it occurred, would be expected to be characterized by similarly limited viral replication and spread.
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U2 - 10.1128/JVI.06886-11
DO - 10.1128/JVI.06886-11
M3 - Article
C2 - 22238316
AN - SCOPUS:84863230248
SN - 0022-538X
VL - 86
SP - 3152
EP - 3166
JO - Journal of virology
JF - Journal of virology
IS - 6
ER -