Experimental colitis in SIV-uninfected rhesus macaques recapitulates important features of pathogenic SIV infection

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作者
Xing Pei Hao
Carissa M. Lucero
Baris Turkbey
Marcelino L. Bernardo
David R. Morcock
Claire Deleage
Charles M. Trubey
Jeremy Smedley
Nichole R. Klatt
Luis D. Giavedoni
Jan Kristoff
Amy Xu
Gregory Q. Del Prete
Brandon F. Keele
Srinivas S. Rao
W. Gregory Alvord
Peter L. Choyke
Jeffrey D. Lifson
Jason M. Brenchley
Cristian Apetrei
Ivona Pandrea
Jacob D. Estes
机构
[1] Pathology and Histotechnology Laboratory,Department of Pharmaceutics
[2] Leidos Biomedical Research,Department of Virology and Immunology
[3] Inc.,Department of Microbiology and Molecular Genetics
[4] Frederick National Laboratory for Cancer Research,Department of Pathology and School of Medicine
[5] AIDS and Cancer Virus Program,undefined
[6] Leidos Biomedical Research,undefined
[7] Inc.,undefined
[8] Frederick National Laboratory for Cancer Research,undefined
[9] Molecular Imaging Program,undefined
[10] National Cancer Institute,undefined
[11] Laboratory Animal Science Program,undefined
[12] Leidos Biomedical Research,undefined
[13] Inc.,undefined
[14] Frederick National Laboratory for Cancer Research,undefined
[15] Washington National Primate Research Center,undefined
[16] University of Washington,undefined
[17] WaNPRC,undefined
[18] University of Washington,undefined
[19] Southwest National Primate Research Center,undefined
[20] Texas Biomedical Research Institute,undefined
[21] Center for Vaccine Research,undefined
[22] University of Pittsburgh,undefined
[23] School of Public Health,undefined
[24] University of Pittsburgh,undefined
[25] University of Pittsburgh,undefined
[26] Laboratory Animal Medicine,undefined
[27] Vaccine Research Center,undefined
[28] NIAID,undefined
[29] NIH,undefined
[30] Statistical Consulting,undefined
[31] Data Management Services,undefined
[32] Inc.,undefined
[33] National Cancer Institute at Frederick,undefined
[34] Immunopathogenesis Section,undefined
[35] Lab of Molecular Microbiology,undefined
[36] NIAID,undefined
[37] NIH,undefined
[38] University of Pittsburgh,undefined
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摘要
Mucosal damage to the gastrointestinal (GI) tract with resulting microbial translocation is hypothesized to significantly contribute to the heightened and persistent chronic inflammation and immune activation characteristic to HIV infection. Here we employ a non-human primate model of chemically induced colitis in SIV-uninfected rhesus macaques that we developed using dextran sulfate sodium (DSS), to directly test this hypothesis. DSS treatment results in GI barrier damage with associated microbial translocation, inflammation and immune activation. The progression and severity of colitis are longitudinally monitored by a magnetic resonance imaging approach. DSS treatment of SIV-infected African green monkeys, a natural host species for SIV that does not manifest GI tract damage or chronic immune activation during infection, results in colitis with elevated levels of plasma SIV RNA, sCD14, LPS, CRP and mucosal CD4+ T-cell loss. Together these results support the hypothesis that GI tract damage leading to local and systemic microbial translocation, and associated immune activation, are important determinants of AIDS pathogenesis.
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