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Persistent HIV Transcription Induces Sialyl-Lewis-X Glyco-Antigen Cell-Surface Expression

60 Pages Posted: 14 Apr 2020 Publication Status: Published

See all articles by Florent Colomb

Florent Colomb

University of Pennsylvania, The Wistar Institute of Anatomy and Biology

Leila B. Giron

University of Pennsylvania, The Wistar Institute of Anatomy and Biology

Leticia Kuri Cervantes

University of Pennsylvania - Department of Microbiology and Institute for Immunology

Tongcui Ma

University of California, San Francisco (UCSF)

Samson Adeniji

University of Pennsylvania, The Wistar Institute of Anatomy and Biology

Harsh Dweep

University of Pennsylvania, The Wistar Institute of Anatomy and Biology

Emilie Battivelli

Buck Institute for Research on Aging

Eric Verdin

Buck Institute for Research on Aging

Clovis Palmer

Burnet Institute

Hiroaki Tateno

National Institute of Advanced Industrial Science and Technology (AIST)

Andrew V. Kossenkov

University of Pennsylvania, The Wistar Institute of Anatomy and Biology

Nadia Roan

University of California, San Francisco (UCSF)

Michael R. Betts

University of Pennsylvania - Department of Microbiology

Mohamed Abdel-Mohsen

University of Pennsylvania, The Wistar Institute of Anatomy and Biology

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Abstract

A comprehensive understanding of the phenotype of persistent HIV-infected cells, both transcriptionally-active and/or inactive, is imperative for developing a cure. The relevance of cell-surface glycosylation to HIV persistence has never been explored. We characterized the relationship between cell-surface glycomic signatures and persistent HIV transcription in vitro and in vivo. We found that the cell-surface of CD4+ T cells actively transcribing HIV, despite suppressive therapy, harbors high levels of fucosylated carbohydrate ligands, including the cell extravasation mediator Sialyl-Lewis-X (SLeX), as compared to HIV-infected transcriptionally-inactive cells. These high levels of SLeX are induced by HIV transcription, but not by cellular activation, and are maintained after therapy. Cells with high SLeX are enriched for leukocyte extravasation pathways and for signaling pathways that drive HIV transcription. Together, we describe a novel glycomic signature of HIV-infected transcriptionally-active cells that not only differentiates them from their transcriptionally-inactive counterparts, but also can impact their tissue trafficking abilities.

Keywords: HIV persistence, HIV transcription, Glycosylation, Fucose, Sialyl-Lewis-X, T-cell trafficking

Suggested Citation

Colomb, Florent and Giron, Leila B. and Kuri Cervantes, Leticia and Ma, Tongcui and Adeniji, Samson and Dweep, Harsh and Battivelli, Emilie and Verdin, Eric and Palmer, Clovis and Tateno, Hiroaki and Kossenkov, Andrew V. and Roan, Nadia and Betts, Michael R. and Abdel-Mohsen, Mohamed, Persistent HIV Transcription Induces Sialyl-Lewis-X Glyco-Antigen Cell-Surface Expression. Available at SSRN: https://ssrn.com/abstract=3565035 or http://dx.doi.org/10.2139/ssrn.3565035
This version of the paper has not been formally peer reviewed.

Florent Colomb

University of Pennsylvania, The Wistar Institute of Anatomy and Biology ( email )

3601 Spruce Street
Philadelphia, PA
United States

Leila B. Giron

University of Pennsylvania, The Wistar Institute of Anatomy and Biology ( email )

3601 Spruce Street
Philadelphia, PA
United States

Leticia Kuri Cervantes

University of Pennsylvania - Department of Microbiology and Institute for Immunology ( email )

Philadelphia, PA 19104
United States

Tongcui Ma

University of California, San Francisco (UCSF) ( email )

Third Avenue and Parnassus
San Francisco, CA CA 94143
United States

Samson Adeniji

University of Pennsylvania, The Wistar Institute of Anatomy and Biology ( email )

3601 Spruce Street
Philadelphia, PA
United States

Harsh Dweep

University of Pennsylvania, The Wistar Institute of Anatomy and Biology ( email )

3601 Spruce Street
Philadelphia, PA
United States

Emilie Battivelli

Buck Institute for Research on Aging ( email )

8001 Redwood Boulevard
Novato, CA 94945
United States

Eric Verdin

Buck Institute for Research on Aging ( email )

8001 Redwood Boulevard
Novato, CA 94945
United States

Clovis Palmer

Burnet Institute ( email )

85 Commercial Road
Melbourne, VIC, 3004
Australia

Hiroaki Tateno

National Institute of Advanced Industrial Science and Technology (AIST) ( email )

1-3-1 Kasumigaseki
Chiyoda-ku
Tokyo, 100-8921
Japan

Andrew V. Kossenkov

University of Pennsylvania, The Wistar Institute of Anatomy and Biology ( email )

3601 Spruce Street
Philadelphia, PA
United States

Nadia Roan

University of California, San Francisco (UCSF) ( email )

Third Avenue and Parnassus
San Francisco, CA CA 94143
United States

Michael R. Betts

University of Pennsylvania - Department of Microbiology

Philadelphia, PA 19104
United States

Mohamed Abdel-Mohsen (Contact Author)

University of Pennsylvania, The Wistar Institute of Anatomy and Biology ( email )

3601 Spruce Street
Philadelphia, PA
United States

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