Biomarkers of Cellular Stress Do Not Associate with sCD14 in Progressive HIV and SIV Infections in Vivo

Biomarkers of Cellular Stress Do Not Associate with sCD14 in Progressive HIV and SIV Infections in Vivo

Abstract Background: Microbial translocation occurs after damage to the structural and/or immunological barrier of the gastrointestinal (GI) tract into circulation. Microbial components that translocate from the lumen of the GI tract directly stimulate the immune system and contribute to inflammati...

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Main Authors: Carol L. Vinton, Carly E. Starke, Alexandra M. Ortiz, Stephen H. Lai, Jacob K. Flynn, Ornella Sortino, Kenneth Knox, Irini Sereti, Jason Brenchley
Format: Article
Language:English
Published: Case Western Reserve University 2020-04-01
Series:Pathogens and Immunity
Subjects:
microbial translocation
hiv
siv
inflammation
Online Access:https://paijournal.com/index.php/paijournal/article/view/363
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spelling doaj-d13267769b144025882a00af089fc6cc2020-11-25T03:13:16ZengCase Western Reserve UniversityPathogens and Immunity2469-29642020-04-0151688810.20411/pai.v5i1.363120Biomarkers of Cellular Stress Do Not Associate with sCD14 in Progressive HIV and SIV Infections in VivoCarol L. Vinton0Carly E. Starke1Alexandra M. Ortiz2Stephen H. Lai3Jacob K. Flynn4Ornella Sortino5Kenneth Knox6Irini Sereti7Jason Brenchley8Barrier Immunity Section; Laboratory of Viral Diseases; NIAID, NIHBarrier Immunity Section; Laboratory of Viral Diseases; NIAID, NIHBarrier Immunity Section; Laboratory of Viral Diseases; NIAID, NIHBarrier Immunity Section; Laboratory of Viral DiseasesBarrier Immunity Section; Laboratory of Viral Diseases; NIAID, NIHHIV Pathogenesis Section; Laboratory of Immunoregulation; NIAID, NIHDepartment of Medicine; University of ArizonaHIV Pathogenesis Section; Laboratory of Immunoregulation; NIAID, NIHNational Institutes of HealthAbstract Background: Microbial translocation occurs after damage to the structural and/or immunological barrier of the gastrointestinal (GI) tract into circulation. Microbial components that translocate from the lumen of the GI tract directly stimulate the immune system and contribute to inflammation. When microbial translocation becomes chronic, the inflammation has detrimental consequences. Given that microbial translocation is an important phenomenon in many diseases, defining biomarkers that reliably reflect microbial translocation is critical. Measurement of systemic microbial products is difficult since: 1) robust assays to measure microbial antigens simultaneously are lacking; 2) confounding factors influence assays used to detect microbial products; and 3) biological clearance mechanisms limit their detection in circulation. Thus, host proteins produced in response to microbial stimulation are used as surrogates for microbial translocation; however, many of these proteins are also produced in response to host proteins expressed by dying cells. Methods: We measured plasma levels of biomarkers associated with GI tract damage, immune responses to microbial products, and cell-death in people living with HIV before and after antiretroviral administration, and in macaque nonhuman primates before and after SIV infection. Results: Proteins secreted during cellular stress (receptor for advanced glycation endproducts - RAGE and high motility group box 1 -HMGB1), which can induce sCD14 production in vitro and in vivo, do not associate with elevated levels of biomarkers associated with microbial translocation in progressively HIV-infected individuals and SIV-infected NHPs. Conclusions: Bystander cell death and generalized inflammation do not contribute to elevated levels of sCD14 observed in HIV/SIV-infected individuals.https://paijournal.com/index.php/paijournal/article/view/363microbial translocationhivsivinflammation
collection DOAJ
language English
format Article
sources DOAJ
author Carol L. Vinton
Carly E. Starke
Alexandra M. Ortiz
Stephen H. Lai
Jacob K. Flynn
Ornella Sortino
Kenneth Knox
Irini Sereti
Jason Brenchley
spellingShingle Carol L. Vinton
Carly E. Starke
Alexandra M. Ortiz
Stephen H. Lai
Jacob K. Flynn
Ornella Sortino
Kenneth Knox
Irini Sereti
Jason Brenchley
Biomarkers of Cellular Stress Do Not Associate with sCD14 in Progressive HIV and SIV Infections in Vivo
Pathogens and Immunity
microbial translocation
hiv
siv
inflammation
author_facet Carol L. Vinton
Carly E. Starke
Alexandra M. Ortiz
Stephen H. Lai
Jacob K. Flynn
Ornella Sortino
Kenneth Knox
Irini Sereti
Jason Brenchley
author_sort Carol L. Vinton
title Biomarkers of Cellular Stress Do Not Associate with sCD14 in Progressive HIV and SIV Infections in Vivo
title_short Biomarkers of Cellular Stress Do Not Associate with sCD14 in Progressive HIV and SIV Infections in Vivo
title_full Biomarkers of Cellular Stress Do Not Associate with sCD14 in Progressive HIV and SIV Infections in Vivo
title_fullStr Biomarkers of Cellular Stress Do Not Associate with sCD14 in Progressive HIV and SIV Infections in Vivo
title_full_unstemmed Biomarkers of Cellular Stress Do Not Associate with sCD14 in Progressive HIV and SIV Infections in Vivo
title_sort biomarkers of cellular stress do not associate with scd14 in progressive hiv and siv infections in vivo
publisher Case Western Reserve University
series Pathogens and Immunity
issn 2469-2964
publishDate 2020-04-01
description Abstract Background: Microbial translocation occurs after damage to the structural and/or immunological barrier of the gastrointestinal (GI) tract into circulation. Microbial components that translocate from the lumen of the GI tract directly stimulate the immune system and contribute to inflammation. When microbial translocation becomes chronic, the inflammation has detrimental consequences. Given that microbial translocation is an important phenomenon in many diseases, defining biomarkers that reliably reflect microbial translocation is critical. Measurement of systemic microbial products is difficult since: 1) robust assays to measure microbial antigens simultaneously are lacking; 2) confounding factors influence assays used to detect microbial products; and 3) biological clearance mechanisms limit their detection in circulation. Thus, host proteins produced in response to microbial stimulation are used as surrogates for microbial translocation; however, many of these proteins are also produced in response to host proteins expressed by dying cells. Methods: We measured plasma levels of biomarkers associated with GI tract damage, immune responses to microbial products, and cell-death in people living with HIV before and after antiretroviral administration, and in macaque nonhuman primates before and after SIV infection. Results: Proteins secreted during cellular stress (receptor for advanced glycation endproducts - RAGE and high motility group box 1 -HMGB1), which can induce sCD14 production in vitro and in vivo, do not associate with elevated levels of biomarkers associated with microbial translocation in progressively HIV-infected individuals and SIV-infected NHPs. Conclusions: Bystander cell death and generalized inflammation do not contribute to elevated levels of sCD14 observed in HIV/SIV-infected individuals.
topic microbial translocation
hiv
siv
inflammation
url https://paijournal.com/index.php/paijournal/article/view/363
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