Discovery of candidate HIV-1 latency biomarkers using an OMICs approach

Michael Belshan; Alexander Holbrook; Joseph W. George; Hannah E. Durant; Michael Callahan; Spencer Jaquet; John T. West; Jacob Siedlik; Pawel Ciborowski

doi:10.1016/j.virol.2021.03.003

Discovery of candidate HIV-1 latency biomarkers using an OMICs approach

Michael Belshan, Alexander Holbrook, Joseph W. George, Hannah E. Durant, Michael Callahan, Spencer Jaquet, John T. West, Jacob Siedlik, Pawel Ciborowski

Research output: Contribution to journal › Article › peer-review

1 Scopus citations

Abstract

Infection with HIV-1 remains uncurable due to reservoirs of latently infected cells. Any potential cure for HIV will require a mechanism to identify and target these cells in vivo. We created a panel of Jurkat cell lines latently infected with the HIV DuoFlo virus to identify candidate biomarkers of latency. SWATH mass spectrometry was used to compare the membrane proteomes of one of the cell lines to parental Jurkat cells. Several candidate proteins with significantly altered expression were identified. The differential expression of several candidates was validated in multiple latently infected cell lines. Three factors (LAG-3, CD147,CD231) were altered across numerous cell lines, but the expression of most candidate biomarkers was variable. These results confirm that phenotypic differences in latently infected cells exists and identify additional novel biomarkers. The variable expression of biomarkers across different cell clones suggests universal antigen-based detection of latently infected cells may require a multiplex approach.

Original language	English (US)
Pages (from-to)	86-95
Number of pages	10
Journal	Virology
Volume	558
DOIs	https://doi.org/10.1016/j.virol.2021.03.003
State	Published - Jun 2021

Keywords

Biomarker discovery
HIV
Latency
Proteomics
SWATH-MS

ASJC Scopus subject areas

Virology

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10.1016/j.virol.2021.03.003

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title = "Discovery of candidate HIV-1 latency biomarkers using an OMICs approach",

abstract = "Infection with HIV-1 remains uncurable due to reservoirs of latently infected cells. Any potential cure for HIV will require a mechanism to identify and target these cells in vivo. We created a panel of Jurkat cell lines latently infected with the HIV DuoFlo virus to identify candidate biomarkers of latency. SWATH mass spectrometry was used to compare the membrane proteomes of one of the cell lines to parental Jurkat cells. Several candidate proteins with significantly altered expression were identified. The differential expression of several candidates was validated in multiple latently infected cell lines. Three factors (LAG-3, CD147,CD231) were altered across numerous cell lines, but the expression of most candidate biomarkers was variable. These results confirm that phenotypic differences in latently infected cells exists and identify additional novel biomarkers. The variable expression of biomarkers across different cell clones suggests universal antigen-based detection of latently infected cells may require a multiplex approach.",

keywords = "Biomarker discovery, HIV, Latency, Proteomics, SWATH-MS",

author = "Michael Belshan and Alexander Holbrook and George, {Joseph W.} and Durant, {Hannah E.} and Michael Callahan and Spencer Jaquet and West, {John T.} and Jacob Siedlik and Pawel Ciborowski",

note = "Funding Information: This study was funded by Creighton University Health Science Strategic Investment Fund (MB). The following reagent was obtained through the NIH AIDS Reagent Program, Division of AIDS, NIAID, NIH: Cat# 12595 DuoFlo (R7GEmC) from Drs. Vincenzo Calvanez and Eric Verdin. Publisher Copyright: {\textcopyright} 2021 Elsevier Inc.",

year = "2021",

month = jun,

doi = "10.1016/j.virol.2021.03.003",

language = "English (US)",

volume = "558",

pages = "86--95",

journal = "Virology",

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AU - Belshan, Michael

AU - Holbrook, Alexander

AU - George, Joseph W.

AU - Durant, Hannah E.

AU - Callahan, Michael

AU - Jaquet, Spencer

AU - West, John T.

AU - Siedlik, Jacob

AU - Ciborowski, Pawel

N1 - Funding Information: This study was funded by Creighton University Health Science Strategic Investment Fund (MB). The following reagent was obtained through the NIH AIDS Reagent Program, Division of AIDS, NIAID, NIH: Cat# 12595 DuoFlo (R7GEmC) from Drs. Vincenzo Calvanez and Eric Verdin. Publisher Copyright: © 2021 Elsevier Inc.

PY - 2021/6

Y1 - 2021/6

N2 - Infection with HIV-1 remains uncurable due to reservoirs of latently infected cells. Any potential cure for HIV will require a mechanism to identify and target these cells in vivo. We created a panel of Jurkat cell lines latently infected with the HIV DuoFlo virus to identify candidate biomarkers of latency. SWATH mass spectrometry was used to compare the membrane proteomes of one of the cell lines to parental Jurkat cells. Several candidate proteins with significantly altered expression were identified. The differential expression of several candidates was validated in multiple latently infected cell lines. Three factors (LAG-3, CD147,CD231) were altered across numerous cell lines, but the expression of most candidate biomarkers was variable. These results confirm that phenotypic differences in latently infected cells exists and identify additional novel biomarkers. The variable expression of biomarkers across different cell clones suggests universal antigen-based detection of latently infected cells may require a multiplex approach.

AB - Infection with HIV-1 remains uncurable due to reservoirs of latently infected cells. Any potential cure for HIV will require a mechanism to identify and target these cells in vivo. We created a panel of Jurkat cell lines latently infected with the HIV DuoFlo virus to identify candidate biomarkers of latency. SWATH mass spectrometry was used to compare the membrane proteomes of one of the cell lines to parental Jurkat cells. Several candidate proteins with significantly altered expression were identified. The differential expression of several candidates was validated in multiple latently infected cell lines. Three factors (LAG-3, CD147,CD231) were altered across numerous cell lines, but the expression of most candidate biomarkers was variable. These results confirm that phenotypic differences in latently infected cells exists and identify additional novel biomarkers. The variable expression of biomarkers across different cell clones suggests universal antigen-based detection of latently infected cells may require a multiplex approach.

KW - Biomarker discovery

KW - HIV

KW - Latency

KW - Proteomics

KW - SWATH-MS

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Discovery of candidate HIV-1 latency biomarkers using an OMICs approach

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Keywords

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