Blockage of regulatory T cells augments induction of protective immune responses by influenza virus-like particles in aged mice

Wen, Zhiyuan; Wang, Xi; Dong, Ke; Zhang, Huizhong; Bu, Zhigao; Ye, Ling; Yang, Chinglai

doi:10.1016/j.micinf.2017.08.013

Cited by 16 publications

(9 citation statements)

References 53 publications

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“…In general, Treg function is activated in the elderly, 14 which reduces the effectiveness of influenza virus and varicella‐zoster virus (VZV) vaccines. 15 , 16 Moreover, the lower number of Tregs are also implicated in autoimmune diseases such as immune thrombocytopenia or transfusion‐related acute lung injury. 17 , 18 However, there are very few reports on the effect of Tregs on COVID‐19 vaccines, as aforementioned.…”

Section: Resultsmentioning

confidence: 99%

Depletion of CD38‐positive regulatory T cells by anti‐CD38 monoclonal antibodies induces a durable response to SARS‐CoV‐2 vaccination in patients with plasma cell dyscrasia

et al. 2022

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Summary This study reports the relationship between CD38+ regulatory T cells (Tregs) and messenger RNA coronavirus disease 2019 (mRNA‐COVID‐19) vaccination in 60 patients with plasma cell dyscrasia. Patients treated with anti‐CD38 monoclonal antibodies (mAbs) had significantly lower CD38+ Tregs than those not treated (0.9 vs. 13.2/μl). Late‐responders, whose antibody titres increased from weeks 4–12 after the second vaccination, had significantly lower CD38+ Treg counts than non‐late‐responders (2.5 vs. 10.3/μl). Antibody titres in patients with lower CD38+ Treg levels were maintained from weeks 4–12 but decreased in those with higher CD38+ Treg levels. Therefore, depletion of CD38+ Tregs by anti‐CD38 mAbs may induce a durable response to mRNA‐COVID‐19 vaccination.

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Section: Resultsmentioning

confidence: 99%

Depletion of CD38‐positive regulatory T cells by anti‐CD38 monoclonal antibodies induces a durable response to SARS‐CoV‐2 vaccination in patients with plasma cell dyscrasia

et al. 2022

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“…Along these lines, another study in aged patients showed that non-responder individuals to influenza vaccination have a higher frequency of Treg as well as a higher inflammatory status compared to responders ( 128 ). Depletion of Treg with anti-CD25 treatment prior to influenza infection protected against lethal viral challenge in aged mice ( 129 ). In another study, responders to influenza vaccination showed a higher frequency of Treg compared to non-responders, together with an elevated frequency of early differentiated CD4 + T cells and lower proportion of memory CD4 + cells ( 130 ).…”

Section: Treg Homeostasis and Function In Agingmentioning

confidence: 99%

The Complex Role of Regulatory T Cells in Immunity and Aging

et al. 2021

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The immune system is a tightly regulated network which allows the development of defense mechanisms against foreign antigens and tolerance toward self-antigens. Regulatory T cells (Treg) contribute to immune homeostasis by maintaining unresponsiveness to self-antigens and suppressing exaggerated immune responses. Dysregulation of any of these processes can lead to serious consequences. Classically, Treg cell functions have been described in CD4+ T cells, but other immune cells also harbour the capacity to modulate immune responses. Regulatory functions have been described for different CD8+ T cell subsets, as well as other T cells such as γδT cells or NKT cells. In this review we describe the diverse populations of Treg cells and their role in different scenarios. Special attention is paid to the aging process, which is characterized by an altered composition of immune cells. Treg cells can contribute to the development of various age-related diseases but they are poorly characterized in aged individuals. The huge diversity of cells that display immune modulatory functions and the lack of universal markers to identify Treg make the expanding field of Treg research complex and challenging. There are still many open questions that need to be answered to solve the enigma of regulatory T cells.

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“…If there are too many Treg cells, the antiviral immunity and vaccination efficiency mediated by effector T cells and B cells may be suppressed, resulting in reduced inhibition of viral replication in the elderly; whereas, if Treg cells are insufficient in the inflammatory lung, the excessive immune reaction-induced tissue damage could be detrimental. Utilizing anti-CD25 to block Treg cell function has been demonstrated to augment protective immune responses to influenza virus-like particles in aged mice [ 128 ]. Induced Treg (iTreg) cells can be generated via transforming growth factor- β (TGF-β), while blocking TGF-β signaling impedes the conversion of CD4 T cells into iTreg cells and thereby facilitates immune responses abrogated by Treg suppression [ 129 ].…”

Section: How Can We Sufficiently Restore Antiviral Immunity and Immentioning

confidence: 99%

Thymic Aging May Be Associated with COVID-19 Pathophysiology in the Elderly

Wang

Thomas

et al. 2021

Cells

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Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) caused the global pandemic of coronavirus disease 2019 (COVID-19) and particularly exhibits severe symptoms and mortality in elderly individuals. Mounting evidence shows that the characteristics of the age-related clinical severity of COVID-19 are attributed to insufficient antiviral immune function and excessive self-damaging immune reaction, involving T cell immunity and associated with pre-existing basal inflammation in the elderly. Age-related changes to T cell immunosenescence is characterized by not only restricted T cell receptor (TCR) repertoire diversity, accumulation of exhausted and/or senescent memory T cells, but also by increased self-reactive T cell- and innate immune cell-induced chronic inflammation, and accumulated and functionally enhanced polyclonal regulatory T (Treg) cells. Many of these changes can be traced back to age-related thymic involution/degeneration. How these changes contribute to differences in COVID-19 disease severity between young and aged patients is an urgent area of investigation. Therefore, we attempt to connect various clues in this field by reviewing and discussing recent research on the role of the thymus and T cells in COVID-19 immunity during aging (a synergistic effect of diminished responses to pathogens and enhanced responses to self) impacting age-related clinical severity of COVID-19. We also address potential combinational strategies to rejuvenate multiple aging-impacted immune system checkpoints by revival of aged thymic function, boosting peripheral T cell responses, and alleviating chronic, basal inflammation to improve the efficiency of anti-SARS-CoV-2 immunity and vaccination in the elderly.

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Blockage of regulatory T cells augments induction of protective immune responses by influenza virus-like particles in aged mice

Cited by 16 publications

References 53 publications

Depletion of CD38‐positive regulatory T cells by anti‐CD38 monoclonal antibodies induces a durable response to SARS‐CoV‐2 vaccination in patients with plasma cell dyscrasia

Depletion of CD38‐positive regulatory T cells by anti‐CD38 monoclonal antibodies induces a durable response to SARS‐CoV‐2 vaccination in patients with plasma cell dyscrasia

The Complex Role of Regulatory T Cells in Immunity and Aging

Thymic Aging May Be Associated with COVID-19 Pathophysiology in the Elderly

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