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Citations to this article

PLA2G1B is involved in CD4 anergy and CD4 lymphopenia in HIV-infected patients
Julien Pothlichet, … , Gérard Lambeau, Jacques Thèze
Julien Pothlichet, … , Gérard Lambeau, Jacques Thèze
Published March 3, 2020
Citation Information: J Clin Invest. 2020;130(6):2872-2887. https://doi.org/10.1172/JCI131842.
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Research Article AIDS/HIV Immunology Article has an altmetric score of 47

PLA2G1B is involved in CD4 anergy and CD4 lymphopenia in HIV-infected patients

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Abstract

The precise mechanism leading to profound immunodeficiency of HIV-infected patients is still only partially understood. Here, we show that more than 80% of CD4+ T cells from HIV-infected patients have morphological abnormalities. Their membranes exhibited numerous large abnormal membrane microdomains (aMMDs), which trap and inactivate physiological receptors, such as that for IL-7. In patient plasma, we identified phospholipase A2 group IB (PLA2G1B) as the key molecule responsible for the formation of aMMDs. At physiological concentrations, PLA2G1B synergized with the HIV gp41 envelope protein, which appears to be a driver that targets PLA2G1B to the CD4+ T cell surface. The PLA2G1B/gp41 pair induced CD4+ T cell unresponsiveness (anergy). At high concentrations in vitro, PLA2G1B acted alone, independently of gp41, and inhibited the IL-2, IL-4, and IL-7 responses, as well as TCR-mediated activation and proliferation, of CD4+ T cells. PLA2G1B also decreased CD4+ T cell survival in vitro, likely playing a role in CD4 lymphopenia in conjunction with its induced IL-7 receptor defects. The effects on CD4+ T cell anergy could be blocked by a PLA2G1B-specific neutralizing mAb in vitro and in vivo. The PLA2G1B/gp41 pair constitutes what we believe is a new mechanism of immune dysfunction and a compelling target for boosting immune responses in HIV-infected patients.

Authors

Julien Pothlichet, Thierry Rose, Florence Bugault, Louise Jeammet, Annalisa Meola, Ahmed Haouz, Frederick Saul, David Geny, José Alcami, Ezequiel Ruiz-Mateos, Luc Teyton, Gérard Lambeau, Jacques Thèze

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Total citations by year

Year: 2025 2024 2023 2022 2021 2020 Total
Citations: 1 2 2 5 3 2 15
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Citations to this article (15)

Title and authors Publication Year
Based on the immune system: the role of the IL-2 family in pancreatic disease
Zhu Y, Lu Z, Wang Z, Liu J, Ning K
Frontiers in Immunology 2025
SARS-CoV-2-associated lymphopenia: possible mechanisms and the role of CD147
Shouman S, El-Kholy N, Hussien AE, El-Derby AM, Magdy S, Abou-Shanab AM, Elmehrath AO, Abdelwaly A, Helal M, El-Badri N
Cell communication and signaling : CCS 2024
Adding-on nivolumab to chemotherapy-stabilized patients is associated with improved survival in advanced pancreatic ductal adenocarcinoma.
Yang SH, Kuo SH, Lee JC, Chen BB, Shan YS, Tien YW, Chiu SC, Cheng AL, Yeh KH
Cancer immunology, immunotherapy : CII 2024
A BRAF mutation-associated gene risk model for predicting the prognosis of melanoma.
Huang X, Gou W, Song Q, Huang Y, Wen C, Bo X, Jiang X, Feng J, Gao H
Heliyon 2023
Plasma metabolomics by nuclear magnetic resonance reveals biomarkers and metabolic pathways associated with the control of HIV-1 infection/progression
Gómez-Archila LG, Palomino-Schätzlein M, Zapata-Builes W, Rugeles MT, Galeano E
Frontiers in Molecular Biosciences 2023
HIV Reservoirs: Methods and Protocols
G Poli, E Vicenzi, F Romerio
2022
Anti-HIV Activity of Snake Venom Phospholipase A2s: Updates for New Enzymes and Different Virus Strains
A Siniavin, S Grinkina, A Osipov, V Starkov, V Tsetlin, Y Utkin
International journal of molecular sciences 2022
Microbial Protein Binding to gC1qR Drives PLA2G1B-Induced CD4 T-Cell Anergy
J Pothlichet, A Meola, F Bugault, L Jeammet, A Savitt, B Ghebrehiwet, L Touqui, P Pouletty, F Fiore, A Sauvanet, J Thèze
Frontiers in immunology 2022
Null Function of Npr1 Disturbs Immune Response in Colonic Inflammation During Early Postnatal Stage.
Long C, Liu H, Zhan W, Chen L, Wu A, Yang L, Chen S
Inflammation 2022
Multimodal regulation of the osteoclastogenesis process by secreted group IIA phospholipase A2.
Mangini M, D'Angelo R, Vinciguerra C, Payré C, Lambeau G, Balestrieri B, Charles JF, Mariggiò S
Frontiers in Cell and Developmental Biology 2022
What do secreted phospholipases A2 have to offer in combat against different viruses up to SARS-CoV-2?
J Pungerčar, F Bihl, G Lambeau, I Križaj
Biochimie 2021
Increased homeostatic cytokines and stability of HIV-infected memory CD4 T-cells identify individuals with suboptimal CD4 T-cell recovery on-ART
M Pino, SP Ribeiro, A Pagliuzza, K Ghneim, A Khan, E Ryan, JL Harper, CT King, S Welbourn, L Micci, S Aldrete, KA Delman, T Stuart, M Lowe, JM Brenchley, CA Derdeyn, K Easley, RP Sekaly, N Chomont, M Paiardini, VC Marconi, JL Riley
PLoS pathogens 2021
MicroPhenoDB Associates Metagenomic Data with Pathogenic Microbes, Microbial Core Genes, and Human Disease Phenotypes
G Yao, W Zhang, M Yang, H Yang, J Wang, H Zhang, L Wei, Z Xie, W Li
Genomics, proteomics & bioinformatics / Beijing Genomics Institute 2021
Updating Phospholipase A2 Biology
M Murakami, H Sato, Y Taketomi
Biomolecules 2020
Sharing CD4+ T Cell Loss: When COVID-19 and HIV Collide on Immune System
X Peng, J Ouyang, S Isnard, J Lin, B Fombuena, B Zhu, JP Routy
Frontiers in immunology 2020

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