Long-Term Depletion of Naive T Cells in Patients Treated for Hodgkin's Disease

Abstract We investigated the representation of T cells in patients who had been treated for Hodgkin's disease (HD). We found a marked depletion in both CD4 and CD8 naive T-cell counts that persists up to 30 years after completion of treatment. In contrast, CD4 and CD8 memory T-cell subsets recovered to normal or above normal levels by 5 years posttreatment. Thus, the previously-reported long-term deficit in total CD4 T-cell counts after treatment for HD is due to specific depletion of naive T cells. Similarly, total CD8 T-cell counts return to normal by 5 years only because CD8 memory T cells expand to higher than normal levels. These findings suggest that the treatment (mediastinal irradiation) results in a longterm dysregulation of T-cell subset homeostasis. The profound depletion of naive T cells may explain the altered T-cell function in treated patients, including the poor response to immunization after treatment for HD. Further, in some individuals, we identified expansions of unusual subsets expressing low levels of CD8. Eight-color fluorescence-activated cell sorting analyses showed that these cells largely express CD8αα homodimers and CD57, consistent with the phenotype of potentially extrathymically derived T cells. In addition, these cells, both CD4+ and CD4−, are probably cytotoxic lymphocytes, as they express high levels of intracellular perforin. In adults treated for HD, an increased activity of extrathymic T-cell differentiation may partially compensate for the loss of thymic-derived T cells.

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Cortisol and epinephrine control opposing circadian rhythms in T cell subsets

Blood ◽

10.1182/blood-2008-11-190769 ◽

2009 ◽

Vol 113 (21) ◽

pp. 5134-5143 ◽

Cited By ~ 172

Author(s):

Stoyan Dimitrov ◽

Christian Benedict ◽

Dennis Heutling ◽

Jürgen Westermann ◽

Jan Born ◽

...

Keyword(s):

T Cells ◽

T Cell ◽

Circadian Rhythms ◽

Cd8 T Cells ◽

Low Dose ◽

Cd8 T Cell ◽

T Cell Subsets ◽

Naive T Cells ◽

Naïve T Cells ◽

Cell Counts

Abstract Pronounced circadian rhythms in numbers of circulating T cells reflect a systemic control of adaptive immunity whose mechanisms are obscure. Here, we show that circadian variations in T cell subpopulations in human blood are differentially regulated via release of cortisol and catecholamines. Within the CD4+ and CD8+ T cell subsets, naive cells show pronounced circadian rhythms with a daytime nadir, whereas (terminally differentiated) effector CD8+ T cell counts peak during daytime. Naive T cells were negatively correlated with cortisol rhythms, decreased after low-dose cortisol infusion, and showed highest expression of CXCR4, which was up-regulated by cortisol. Effector CD8+ T cells were positively correlated with epinephrine rhythms, increased after low-dose epinephrine infusion, and showed highest expression of β-adrenergic and fractalkine receptors (CX3CR1). Daytime increases in cortisol via CXCR4 probably act to redistribute naive T cells to bone marrow, whereas daytime increases in catecholamines via β-adrenoceptors and, possibly, a suppression of fractalkine signaling promote mobilization of effector CD8+ T cells from the marginal pool. Thus, activation of the major stress hormones during daytime favor immediate effector defense but diminish capabilities for initiating adaptive immune responses.

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VISTA is a checkpoint regulator for naïve T cell quiescence and peripheral tolerance

Science ◽

10.1126/science.aay0524 ◽

2020 ◽

Vol 367 (6475) ◽

pp. eaay0524 ◽

Cited By ~ 22

Author(s):

Mohamed A. ElTanbouly ◽

Yanding Zhao ◽

Elizabeth Nowak ◽

Jiannan Li ◽

Evelien Schaafsma ◽

...

Keyword(s):

T Cells ◽

T Cell ◽

T Cell Activation ◽

Cell Subset ◽

Peripheral Tolerance ◽

Cell Immune Response ◽

Naive T Cells ◽

Naïve T Cells ◽

Naïve T Cell ◽

Naive T Cell

Negative checkpoint regulators (NCRs) temper the T cell immune response to self-antigens and limit the development of autoimmunity. Unlike all other NCRs that are expressed on activated T lymphocytes, V-type immunoglobulin domain-containing suppressor of T cell activation (VISTA) is expressed on naïve T cells. We report an unexpected heterogeneity within the naïve T cell compartment in mice, where loss of VISTA disrupted the major quiescent naïve T cell subset and enhanced self-reactivity. Agonistic VISTA engagement increased T cell tolerance by promoting antigen-induced peripheral T cell deletion. Although a critical player in naïve T cell homeostasis, the ability of VISTA to restrain naïve T cell responses was lost under inflammatory conditions. VISTA is therefore a distinctive NCR of naïve T cells that is critical for steady-state maintenance of quiescence and peripheral tolerance.

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Abstract 424: Effector T Cells Induce Cardiac Fibroblasts Transition to Myofibroblasts & Contribute to Pressure Overload Induced Cardiac Fibrosis

Circulation Research ◽

10.1161/res.119.suppl_1.424 ◽

2016 ◽

Vol 119 (suppl_1) ◽

Author(s):

Tania A Nevers ◽

Ane Salvador ◽

Francisco Velazquez ◽

Mark Aronovitz ◽

Robert Blanton

Keyword(s):

T Cells ◽

T Cell ◽

Cardiac Fibrosis ◽

Cardiac Fibroblasts ◽

Pressure Overload ◽

Effector T Cells ◽

T Cell Subsets ◽

Naive T Cells ◽

Effector T Cell ◽

Naïve T Cells

Background: Cardiac fibrogenesis is a major pathogenic factor that occurs in heart failure (HF) and results in contractile dysfunction and ventricular dilation. Recently, we showed that T cell deficient mice (TCRα -/- ) do not develop cardiac fibrosis (CF) and have preserved cardiac function in the thoracic aortic constriction (TAC) mouse model of pressure overload (PO). Specifically, CD4 + T cells are activated in the cardiac draining lymph nodes and infiltrate the LV, where the Th1 and Th17 effector T cell signature transcription factors are significantly upregulated as compared with control mice. However, the T cell subsets involved and the mechanisms by which they contribute to CF and pathogenesis of non-ischemic HF remains to be determined. Thus, we hypothesize that heart infiltrated effector T cells perpetuate the fibrotic response by regulating the differentiation and activation of extracellular matrix-producing cardiac myofibroblasts. Methods and Results: Naïve or effector T cells differentiated in vitro or isolated from mice undergoing TAC or Sham surgery were co-cultured with adult C57BL/6 cardiac fibroblasts (CFB). In contrast with naïve T cells, effector T cells and PO activated T cells strongly adhered to CFB and mediated fibroblast to myofibroblasts transition as depicted by immunofluorescence expression of SMAα. Effector T cell supernatants only slightly mediated this transition, indicating that effector T cells direct contact with CFB, rather than cytokine release is required to mediate CFB transformation. Adoptive transfer of effector, but not naïve T cells, into TCRα -/- recipient mice in the onset of TAC resulted in T cells infiltration into the left ventricle and increased CF. Conclusions: Our data indicate that CD4+ effector T cells directly interact with CFB to induce CF in response to PO induced CF. Future studies will determine the adhesion mechanisms regulating this crosstalk and evaluate the pro-fibrotic mechanisms induced and whether this is a T effector cell specific subset. These results will provide an attractive tool to counteract the inflammatory/fibrotic process as an alternative option for the treatment of CF in non- ischemic HF.

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CRTAM determines the CD4+ cytotoxic T lymphocyte lineage

Journal of Experimental Medicine ◽

10.1084/jem.20150519 ◽

2015 ◽

Vol 213 (1) ◽

pp. 123-138 ◽

Cited By ~ 68

Author(s):

Arata Takeuchi ◽

Mohamed El Sherif Gadelhaq Badr ◽

Kosuke Miyauchi ◽

Chitose Ishihara ◽

Reiko Onishi ◽

...

Keyword(s):

T Cells ◽

T Cell ◽

Cytotoxic Activity ◽

Cd4 T Cells ◽

Intracellular Signaling ◽

Ectopic Expression ◽

T Cell Subsets ◽

Naive T Cells ◽

Naïve T Cells ◽

Ifn Γ

Naive T cells differentiate into various effector T cells, including CD4+ helper T cell subsets and CD8+ cytotoxic T cells (CTL). Although cytotoxic CD4+ T cells (CD4+CTL) also develop from naive T cells, the mechanism of development is elusive. We found that a small fraction of CD4+ T cells that express class I–restricted T cell–associated molecule (CRTAM) upon activation possesses the characteristics of both CD4+ and CD8+ T cells. CRTAM+ CD4+ T cells secrete IFN-γ, express CTL-related genes, such as eomesodermin (Eomes), Granzyme B, and perforin, after cultivation, and exhibit cytotoxic function, suggesting that CRTAM+ T cells are the precursor of CD4+CTL. Indeed, ectopic expression of CRTAM in T cells induced the production of IFN-γ, expression of CTL-related genes, and cytotoxic activity. The induction of CD4+CTL and IFN-γ production requires CRTAM-mediated intracellular signaling. CRTAM+ T cells traffic to mucosal tissues and inflammatory sites and developed into CD4+CTL, which are involved in mediating protection against infection as well as inducing inflammatory response, depending on the circumstances, through IFN-γ secretion and cytotoxic activity. These results reveal that CRTAM is critical to instruct the differentiation of CD4+CTL through the induction of Eomes and CTL-related gene.

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In vitro responses of human CD45R0brightRA− and CD45R0−RAbright T cell subsets and their relationship to memory and naive T cells

European Journal of Immunology ◽

10.1002/eji.1830270937 ◽

1997 ◽

Vol 27 (9) ◽

pp. 2383-2390 ◽

Cited By ~ 72

Author(s):

Joyce L. Young ◽

Judith M. Ramage ◽

J. S. Hill Gaston ◽

Peter C. L. Beverley

Keyword(s):

T Cells ◽

T Cell ◽

T Cell Subsets ◽

Naive T Cells ◽

Naïve T Cells

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Lipid Microbubble–Conjugated Anti-CD3 and Anti-CD28 Antibodies (Microbubble-Based Human T Cell Activator) Offer Superior Long-Term Expansion of Human Naive T Cells In Vitro

ImmunoHorizons ◽

10.4049/immunohorizons.2000056 ◽

2020 ◽

Vol 4 (8) ◽

pp. 475-484

Author(s):

Ana Lustig ◽

Ty’Keemi Manor ◽

Guixin Shi ◽

Jiangyuan Li ◽

Ying-Ting Wang ◽

...

Keyword(s):

T Cells ◽

T Cell ◽

Naive T Cells ◽

Naïve T Cells ◽

Human T Cell ◽

Cell Activator

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Dysregulated lymphocyte proliferation and differentiation in patients with rheumatoid arthritis

Blood ◽

10.1182/blood-2002-03-0671 ◽

2002 ◽

Vol 100 (13) ◽

pp. 4550-4556 ◽

Cited By ~ 102

Author(s):

Frederique Ponchel ◽

Ann W. Morgan ◽

Sarah J. Bingham ◽

Mark Quinn ◽

Maya Buch ◽

...

Keyword(s):

Rheumatoid Arthritis ◽

T Cells ◽

Cell Differentiation ◽

T Cell ◽

Large Population ◽

Chronic Inflammatory Disease ◽

T Cell Differentiation ◽

T Cell Subsets ◽

Naive T Cells ◽

Naïve T Cells

Rheumatoid arthritis (RA) is a chronic, inflammatory disease of the synovium of uncertain pathogenesis. A number of phenotypic and functional T-cell defects have been described in RA, including abnormal clonal expansions and suppressed proliferative responses, which suggest a defect in T-cell differentiation. Here, we show that RA patients possess fewer naive CD4+ T cells than healthy controls. Furthermore, a smaller proportion of these cells contains a T-cell receptor excision circle (TREC). Patients with RA also have unusual populations of T cells. These include immature cells characterized as CD45RBbrightCD45RA+CD62L− by flow cytometry and a large population that coexpresses CD45RA and CD45RO. These cells are hyperresponsive to mitogen and TCR stimulation when compared to naive cells. Additionally, an unusual putative central memory subset expressing CD62L, but not CD45RA, appears in RA patients at the expense of more typical cells. Levels of C-reactive protein correlate inversely with the TREC content of naive T cells and positively with the sizes of naive and immature atypical T-cell subsets. These data suggest that inflammation drives proliferation of naive T cells in RA and encourages their differentiation into atypical, hyperresponsive progeny. TREC content of individual naive and atypical T-cell subsets suggests an ontogeny consistent with this hypothesis. These studies provide further evidence of a T-cell differentiation defect in RA, which could explain some of the well-characterized immunologic features of the disease.

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One naive T cell, multiple fates in CD8+ T cell differentiation

Journal of Experimental Medicine ◽

10.1084/jem.20091175 ◽

2010 ◽

Vol 207 (6) ◽

pp. 1235-1246 ◽

Cited By ~ 112

Author(s):

Carmen Gerlach ◽

Jeroen W.J. van Heijst ◽

Erwin Swart ◽

Daoud Sie ◽

Nicola Armstrong ◽

...

Keyword(s):

T Cells ◽

T Cell ◽

Large Scale ◽

Cd8 T Cell ◽

T Cell Subsets ◽

High Avidity ◽

Naive T Cells ◽

Memory T Cell ◽

Naïve T Cells ◽

Large Scale Assessment

The mechanism by which the immune system produces effector and memory T cells is largely unclear. To allow a large-scale assessment of the development of single naive T cells into different subsets, we have developed a technology that introduces unique genetic tags (barcodes) into naive T cells. By comparing the barcodes present in antigen-specific effector and memory T cell populations in systemic and local infection models, at different anatomical sites, and for TCR–pMHC interactions of different avidities, we demonstrate that under all conditions tested, individual naive T cells yield both effector and memory CD8+ T cell progeny. This indicates that effector and memory fate decisions are not determined by the nature of the priming antigen-presenting cell or the time of T cell priming. Instead, for both low and high avidity T cells, individual naive T cells have multiple fates and can differentiate into effector and memory T cell subsets.

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Cytokine transcriptional events during helper T cell subset differentiation.

Journal of Experimental Medicine ◽

10.1084/jem.184.2.397 ◽

1996 ◽

Vol 184 (2) ◽

pp. 397-406 ◽

Cited By ~ 117

Author(s):

J A Lederer ◽

V L Perez ◽

L DesRoches ◽

S M Kim ◽

A K Abbas ◽

...

Keyword(s):

T Cells ◽

Transcription Factors ◽

T Cell ◽

Cell Subset ◽

Cytokine Gene Expression ◽

Ifn Gamma ◽

Naive T Cells ◽

Naïve T Cells ◽

Th2 Differentiation

The molecular basis for changes in cytokine expression during T helper (Th) cell subset differentiation is not well understood. We have characterized transcriptional events related to cytokine gene expression in populations of naive T cell receptor-transgenic T cells as they are driven in vitro toward Th1 or Th2 phenotypes by interleukin (IL)-12 or IL-4 treatment, respectively. Quantitative reverse transcriptase-polymerase chain reaction analysis of cytokine transcripts indicates that interferon (IFN) gamma, IL-4, and IL-2 mRNA are expressed with distinct kinetics after naive T cells are stimulated with antigen and either IL-4 or IL-12. IFN-gamma mRNA appears as early as 6 h in IL-12-treated cultures, IL-4 appears only after 48 h in IL-4-treated cultures, and IL-2 is equivalently expressed in both types of cultures. Analyses were performed to determine if there were any differences in activation of IL-2 or IL-4 transcription factors that accompanied Th1 versus Th2 differentiation. These studies demonstrated that signal transducer and activator of transcription 6 (STAT6) binds to a sequence in the IL-4 promoter and that this STAT6-binding site can support IL-4-dependent transcription of a linked heterologous promoter. Prolonged activation of STAT6 is characteristic of populations undergoing Th2 differentiation. Furthermore, STAT6 is activated in an autocrine manner when differentiated Th2 populations are stimulated by antigen receptor ligation. Th1 populations derived from IL-12 plus antigen treatment of naive T cells remain responsive to IL-4 as indicated by induction of STAT6 and IL-4 mRNA. These data indicate that Th1 and Th2 differentiation represents the combination of different, apparently independently regulated transcriptional events. Furthermore, among transcription factors that bind to the IL-4 or IL-2 promoters, STAT6 is the one whose activation distinguishes Th2 versus Th1 development.

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Age related human T cell subset evolution and senescence

Immunity & Ageing ◽

10.1186/s12979-019-0165-8 ◽

2019 ◽

Vol 16 (1) ◽

Cited By ~ 23

Author(s):

Mingde Li ◽

Danlin Yao ◽

Xiangbo Zeng ◽

Dimitri Kasakovski ◽

Yikai Zhang ◽

...

Keyword(s):

Immune Response ◽

T Cells ◽

T Cell ◽

Peripheral Blood ◽

Memory T Cells ◽

Cell Subset ◽

Absolute Number ◽

T Cell Subsets ◽

And Gender

Abstract T cells are fundamental effector cells against viruses and cancers that can be divided into different subsets based on their long-term immune protection and immediate immune response effects. The percentage and absolute number of these subsets change with ageing, which leads to a reduced immune response in older individuals. Stem cell memory T cells (TSCM) represent a small population of memory T cells with enhanced proliferation and differentiation properties that are endowed with high potential for maintaining T cell homeostasis. However, whether these cells change with ageing and gender remains unknown. Here, we assayed the distribution of TSCM and other T cell subsets in peripheral blood from 92 healthy subjects (44 females and 48 males) ranging from 3 to 88 years old by flow cytometry. We found that CD4+ and CD8+ TSCM in the circulation have relatively stable frequencies, and the absolute number of CD8+ TSCM decreased with age; however, the ratio of TSCM to the CD4+ or CD8+ naïve population increased with age. Unlike the obvious changes in other T cell subsets with age and gender, the stable level of TSCM in peripheral blood may support their capacity for sustaining long-term immunological memory, while their importance may increase together with ageing.

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