Increased Neutrophil Aging Contributes to T Cell Immune Suppression by PD-L1 and Arginase-1 in HIV-1 Treatment Naïve Patients.

Kai Liu,Ming-Ju Zhou,Wen-Jing Cao,Ruonan Xu,Jin-Wen Song,Ming Shi,Chun-Bao Zhou,Xiu-Ying Mu,Hua-Jie Li,Jin-Hong Yuan,Tao Yang,Hui-Huang Huang,Ji-Yuan Zhang,Yan-Mei Jiao,Chao Zhang,Fu-Sheng Wang

doi:10.3389/fimmu.2021.670616

Abstract

Neutrophils are characterized by their heterogeneity. They fight against pathogens and are involved in tissue injury repair and immune system regulation. Neutrophils have an extremely short life span in the peripheral blood and undergo aging after being released from the bone marrow. The over-aggregation of aged neutrophils is associated with phenotypical and functional changes. Here, we aimed to investigate the dynamics of neutrophil aging and its relationship with T cell exhaustion in HIV-1 infection, as they are not well understood. In this study, we enrolled 23 treatment naïve (TN) patients, 23 individuals that had received antiretroviral therapy (ART), and 21 healthy controls (HC). In these cohorts, we measured the degree of neutrophil aging, and its possible correlation with T cell dysfunction. In TN patients, peripheral neutrophils showed a more distinct aging phenotype and were over-activated compared to those in ART-treated patients. The degree of neutrophil aging was positively correlated with HIV-1 RNA viral load and negatively correlated with CD4+ T cell count. Moreover, aged neutrophils had impaired reactive oxygen species (ROS) production after lipopolysaccharide (LPS) stimulation, and were characterized by increased PD-L1 and arginase-1 expression in a time-dependent manner. Aged neutrophils demonstrated an increased inhibition of IFN-γ and TNF-α secretion by CD8+ T cell compared to non-aged neutrophils. The inhibition effect could be partially reversed by blocking PD-L1 and arginase-1 in vitro, and LPS was identified as an important activator of neutrophil aging. These results provide evidence that dampening neutrophil aging may provide a novel approach to recover T cell dysfunction in patients with HIV-1 infection.

Highlights

Immune aging is a significant feature of chronic HIV-1 infection and is associated with non-AIDS-related events
To identify the degree of neutrophil aging in HIV-1-infected patients, we measured the percentage of CD62LloCXCR4+ neutrophils, as previously described [13, 16], which was increased in treatment naïve (TN) patients and was not fully recovered under efficient antiretroviral therapy (ART) treatment (Figures 1A, B)
The mean fluorescence intensity (MFI) of CD49d and CD11b showed no significant difference within different groups, all five markers showed a correlation with the aging score (Supplementary Figure 1F)

Summary

Introduction

Immune aging is a significant feature of chronic HIV-1 infection and is associated with non-AIDS-related events. The occurrence of immune aging is closely related to the activation of the immune system [1, 2]. Significant evidence points toward a close relationship and synergy among aging, immune activation, and immunosuppression [3]. Neutrophils are the most abundant type of white blood cells in the peripheral blood, and their aging is associated with the circadian rhythm and affected by exogenous activators [4]. The complete understanding of neutrophil aging and its role in T cell exhaustion and involvement in the complete immune reconstitution of patients with HIV-1 infection are lacking [5]

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Conclusion