Your search keyword '"regulatory T-cells (Tregs)"' showing total 42 results

1. Double-Negative T-Cells during Acute Human Immunodeficiency Virus and Simian Immunodeficiency Virus Infections and Following Early Antiretroviral Therapy Initiation.

Author

Yero, Alexis, Shi, Tao, Clain, Julien A., Zghidi-Abouzid, Ouafa, Racine, Gina, Costiniuk, Cecilia T., Routy, Jean-Pierre, Estaquier, Jérôme, and Jenabian, Mohammad-Ali

Subjects

*REGULATORY T cells, *HIV, *HIV infections, *T cells, *VIRUS diseases, *SIMIAN immunodeficiency virus

Abstract

HIV infection significantly affects the frequencies and functions of immunoregulatory CD3+CD4−CD8− double-negative (DN) T-cells, while the effect of early antiretroviral therapy (ART) initiation on these cells remains understudied. DN T-cell subsets were analyzed prospectively in 10 HIV+ individuals during acute infection and following early ART initiation compared to 20 HIV-uninfected controls. In this study, 21 Rhesus macaques (RMs) were SIV-infected, of which 13 were assessed during acute infection and 8 following ART initiation four days post-infection. DN T-cells and FoxP3+ DN Treg frequencies increased during acute HIV infection, which was not restored by ART. The expression of activation (HLA-DR/CD38), immune checkpoints (PD-1/CTLA-4), and senescence (CD28−CD57+) markers by DN T-cells and DN Tregs increased during acute infection and was not normalized by ART. In SIV-infected RMs, DN T-cells remained unchanged despite infection or ART, whereas DN Treg frequencies increased during acute SIV infection and were not restored by ART. Finally, frequencies of CD39+ DN Tregs increased during acute HIV and SIV infections and remained elevated despite ART. Altogether, acute HIV/SIV infections significantly changed DN T-cell and DN Treg frequencies and altered their immune phenotype, while these changes were not fully normalized by early ART, suggesting persistent HIV/SIV-induced immune dysregulation despite early ART initiation. [ABSTRACT FROM AUTHOR]

Published

2024

2. Double-Negative T-Cells during Acute Human Immunodeficiency Virus and Simian Immunodeficiency Virus Infections and Following Early Antiretroviral Therapy Initiation

Author

Alexis Yero, Tao Shi, Julien A. Clain, Ouafa Zghidi-Abouzid, Gina Racine, Cecilia T. Costiniuk, Jean-Pierre Routy, Jérôme Estaquier, and Mohammad-Ali Jenabian

Subjects

CD4−CD8− T-cells, double negative (DN) T-cells, acute SIV infection, acute HIV infection, early ART, regulatory T-cells (Tregs), Microbiology, QR1-502

Abstract

HIV infection significantly affects the frequencies and functions of immunoregulatory CD3+CD4−CD8− double-negative (DN) T-cells, while the effect of early antiretroviral therapy (ART) initiation on these cells remains understudied. DN T-cell subsets were analyzed prospectively in 10 HIV+ individuals during acute infection and following early ART initiation compared to 20 HIV-uninfected controls. In this study, 21 Rhesus macaques (RMs) were SIV-infected, of which 13 were assessed during acute infection and 8 following ART initiation four days post-infection. DN T-cells and FoxP3+ DN Treg frequencies increased during acute HIV infection, which was not restored by ART. The expression of activation (HLA-DR/CD38), immune checkpoints (PD-1/CTLA-4), and senescence (CD28−CD57+) markers by DN T-cells and DN Tregs increased during acute infection and was not normalized by ART. In SIV-infected RMs, DN T-cells remained unchanged despite infection or ART, whereas DN Treg frequencies increased during acute SIV infection and were not restored by ART. Finally, frequencies of CD39+ DN Tregs increased during acute HIV and SIV infections and remained elevated despite ART. Altogether, acute HIV/SIV infections significantly changed DN T-cell and DN Treg frequencies and altered their immune phenotype, while these changes were not fully normalized by early ART, suggesting persistent HIV/SIV-induced immune dysregulation despite early ART initiation.

Published

2024

3. Regulatory T cells in the peripheral blood of women with gestational diabetes: a systematic review and meta-analysis.

Author

Arain, Hania, Patel, Tina, Mureanu, Nicoleta, Efthymiou, Athina, Lombardi, Giovanna, Tree, Timothy, Nicolaides, Kypros H., and Shangaris, Panicos

Subjects

REGULATORY T cells, GESTATIONAL diabetes, BLOOD cells, PREGNANT women

Abstract

Background: Gestational diabetes (GDM) affects approximately 14% of pregnancies globally and is associated with short- and long-term complications for both the mother and child. In addition, GDM has been linked to chronic low-grade inflammation with recent research indicating a potential immune dysregulation in pathophysiology and a disparity in regulatory T cells.Objective: This systematic review and meta-analysis aimed to determine whether there is an association between GDM and the level of Tregs in the peripheral blood.Methods: Literature searches were conducted in PubMed, Embase, and Ovid between the 7th and 14th of February 2022. The inclusion criteria were any original studies published in the English language, measuring differentiated Tregs in women with GDM compared with glucose-tolerant pregnant women. Meta-analysis was performed between comparable Treg markers. Statistical tests were used to quantify heterogeneity: τ², χ², and I². Study quality was assessed using a modified version of the Newcastle-Ottawa scale.Results: The search yielded 223 results: eight studies were included in the review and seven in the meta-analysis (GDM = 228, control = 286). Analysis of Tregs across all trimesters showed significantly lower Treg numbers in women with GDM (SMD, −0.76; 95% CI, −1.37, −0.15; I² = 90%). This was reflected in the analysis by specific Treg markers (SMD −0.55; 95% CI, −1.04, −0.07; I² = 83%; third trimester, five studies). Non-significant differences were found within subgroups (differentiated by CD4+FoxP3+, CD4+CD127−, and CD4+CD127−FoxP3) of both analyses.Conclusion: GDM is associated with lower Treg numbers in the peripheral maternal blood. In early pregnancy, there is clinical potential to use Treg levels as a predictive tool for the subsequent development of GDM. There is also a potential therapeutic intervention to prevent the development of GDM by increasing Treg populations. However, the precise mechanism by which Tregs mediate GDM remains unclear. [ABSTRACT FROM AUTHOR]

Published

2023

4. Regulatory T cells in the peripheral blood of women with gestational diabetes: a systematic review and meta-analysis

Author

Hania Arain, Tina Patel, Nicoleta Mureanu, Athina Efthymiou, Giovanna Lombardi, Timothy Tree, Kypros H. Nicolaides, and Panicos Shangaris

Subjects

gestational diabetes mellitus (GDM), regulatory T-cells (Tregs), immune dysregulation, chronic low-grade inflammation, treg markers, systematic review & meta-analysis, Immunologic diseases. Allergy, RC581-607

Abstract

BackgroundGestational diabetes (GDM) affects approximately 14% of pregnancies globally and is associated with short- and long-term complications for both the mother and child. In addition, GDM has been linked to chronic low-grade inflammation with recent research indicating a potential immune dysregulation in pathophysiology and a disparity in regulatory T cells.ObjectiveThis systematic review and meta-analysis aimed to determine whether there is an association between GDM and the level of Tregs in the peripheral blood.MethodsLiterature searches were conducted in PubMed, Embase, and Ovid between the 7th and 14th of February 2022. The inclusion criteria were any original studies published in the English language, measuring differentiated Tregs in women with GDM compared with glucose-tolerant pregnant women. Meta-analysis was performed between comparable Treg markers. Statistical tests were used to quantify heterogeneity: τ2, χ2, and I2. Study quality was assessed using a modified version of the Newcastle-Ottawa scale.ResultsThe search yielded 223 results: eight studies were included in the review and seven in the meta-analysis (GDM = 228, control = 286). Analysis of Tregs across all trimesters showed significantly lower Treg numbers in women with GDM (SMD, −0.76; 95% CI, −1.37, −0.15; I2 = 90%). This was reflected in the analysis by specific Treg markers (SMD −0.55; 95% CI, −1.04, −0.07; I2 = 83%; third trimester, five studies). Non-significant differences were found within subgroups (differentiated by CD4+FoxP3+, CD4+CD127−, and CD4+CD127−FoxP3) of both analyses.ConclusionGDM is associated with lower Treg numbers in the peripheral maternal blood. In early pregnancy, there is clinical potential to use Treg levels as a predictive tool for the subsequent development of GDM. There is also a potential therapeutic intervention to prevent the development of GDM by increasing Treg populations. However, the precise mechanism by which Tregs mediate GDM remains unclear.Systematic review registrationhttps://www.crd.york.ac.uk/prospero, identifier CRD42022309796.

Published

2023

5. Acquisition of Immune Privilege in GBM Tumors: Role of Prostaglandins and Bile Salts.

Author

Sharpe, Martyn A., Baskin, David S., Johnson, Ryan D., and Baskin, Alexandra M.

Subjects

*BILE salts, *PROSTAGLANDIN receptors, *FARNESOID X receptor, *MICROGLIA, *GLIOBLASTOMA multiforme, *PROSTAGLANDINS, *SUPPRESSOR cells

Abstract

Based on the postulate that glioblastoma (GBM) tumors generate anti-inflammatory prostaglandins and bile salts to gain immune privilege, we analyzed 712 tumors in-silico from three GBM transcriptome databases for prostaglandin and bile synthesis/signaling enzyme-transcript markers. A pan-database correlation analysis was performed to identify cell-specific signal generation and downstream effects. The tumors were stratified by their ability to generate prostaglandins, their competency in bile salt synthesis, and the presence of bile acid receptors nuclear receptor subfamily 1, group H, member 4 (NR1H4) and G protein-coupled bile acid receptor 1 (GPBAR1). The survival analysis indicates that tumors capable of prostaglandin and/or bile salt synthesis are linked to poor outcomes. Tumor prostaglandin D2 and F2 syntheses are derived from infiltrating microglia, whereas prostaglandin E2 synthesis is derived from neutrophils. GBMs drive the microglial synthesis of PGD2/F2 by releasing/activating complement system component C3a. GBM expression of sperm-associated heat-shock proteins appears to stimulate neutrophilic PGE2 synthesis. The tumors that generate bile and express high levels of bile receptor NR1H4 have a fetal liver phenotype and a RORC-Treg infiltration signature. The bile-generating tumors that express high levels of GPBAR1 are infiltrated with immunosuppressive microglia/macrophage/myeloid-derived suppressor cells. These findings provide insight into how GBMs generate immune privilege and may explain the failure of checkpoint inhibitor therapy and provide novel targets for treatment. [ABSTRACT FROM AUTHOR]

Published

2023

6. Immuno-metabolic control of the balance between Th17-polarized and regulatory T-cells during HIV infection.

Author

Yero, Alexis, Bouassa, Ralph-Sydney Mboumba, Ancuta, Petronela, Estaquier, Jerome, and Jenabian, Mohammad-Ali

Subjects

*REGULATORY T cells, *HIV infections, *CHOLESTEROL metabolism, *T helper cells, *FATTY acid oxidation, *T cells, *PURINERGIC receptors

Abstract

Th17-polarized CD4+ effector T-cells together with their immunosuppressive regulatory T-cell (Treg) counterparts, with transcriptional profiles governed by the lineage transcription factors RORγt/RORC2 and FOXP3, respectively, are important gatekeepers at mucosal interfaces. Alterations in the Th17/Treg ratios, due to the rapid depletion of Th17 cells and increased Treg frequencies, are a hallmark of both HIV and SIV infections and a marker of disease progression. The shift in Th17/Treg balance, in favor of increased Treg frequencies, contributes to gut mucosal permeability, immune dysfunction, and microbial translocation, subsequently leading to chronic immune activation/inflammation and disease progression. Of particular interest, Th17 cells and Tregs share developmental routes, with changes in the Th17 versus Treg fate decision influencing the pro-inflammatory versus anti-inflammatory responses. The differentiation and function of Th17 cells and Tregs rely on independent yet complementary metabolic pathways. Several pathways have been described in the literature to be involved in Th17 versus Treg polarization, including 1) the activity of ectonucleotidases CD39/CD73; 2) the increase in TGF-β1 production; 3) a hypoxic environment, and subsequent upregulation in hypoxia-inducible factor-1α (HIF-1α); 4) the increased mTOR activity and glycolysis induction; 5) the lipid metabolism, including fatty acid synthesis, fatty acids oxidation, cholesterol synthesis, and lipid storage, which are regulated by the AMPK, mevalonate and PPARγ pathways; and 6) the tryptophan catabolism. These metabolic pathways are understudied in the context of HIV-1 infection. The purpose of this review is to summarize the current knowledge on metabolic pathways that are dysregulated during HIV-1 infection and their impact on Th17/Treg balance. [Display omitted] • HIV infection shifts the Th17/Treg imbalance in favor of Tregs, contributing to chronic immune dysfunction. • Th17 cells and Tregs share developmental routes regulated by their metabolism and microenvironment. • HIV infection upregulates mTOR, glycolysis, fatty acid synthesis and HIF-1α, related to Th17 cell differentiation. • HIV infection upregulates TGF-β1, purinergic and Kynurenine pathways, in favor of Tregs differentiation. • HIV infection downregulates AMKP, mevalonate pathway and PPAR-γ activity, which are related to Treg differentiation. [ABSTRACT FROM AUTHOR]

Published

2023

7. Calcium controlled NFATc1 activation enhances suppressive capacity of regulatory T cells isolated from generalized vitiligo patients.

Author

Giri, Prashant S., Bharti, Ankit H., Begum, Rasheedunnisa, and Dwivedi, Mitesh

Subjects

*REGULATORY T cells, *CALCIUM, *VITILIGO, *INTRACELLULAR calcium, *CALCIUM channels

Abstract

NFATs and FOXP3 are linked with impaired regulatory T‐cells (Tregs) in generalized vitiligo (GV). To elucidate calcium mediated NFATc1 signalling pathway and its effect on Treg suppressive capacity in GV. Calcium levels, calcineurin, NFATc1 and GSK‐3β activity and cell proliferation were assessed in 52 GV patients and 50 controls by calcium assay kit, calcineurin phosphatase assay kit, TransAM NFATc1 kit, GSK‐3β ELISA and BrdU cell proliferation assay. Transcripts (CNB, CAM, GSK3B, DYRK1A and calcium channel genes) and protein (IFN‐γ, IL‐10 and TGF‐β) expressions were assessed by qPCR and ELISA, respectively. Reduced plasma and intracellular Tregs calcium levels and ORAI1 transcripts suggested altered calcium homeostasis in GV Tregs (p = 0.00387, p = 0.0048, p < 0.0001), which led to decreased calcineurin and NFATc1 activity in GV Tregs (p = 0.0299, p < 0.0001). CNB and CAM transcripts were reduced in GV Tregs (p < 0.0001, p = 0.0004). GSK‐3β activity, GSK3B and DYRK1A transcripts significantly increased in GV Tregs (p = 0.0134, p < 0.0001 and p < 0.0001). Plasma (p = 0.0225, p = 0.032) and intracellular Treg (p = 0.0035, p = 0.005) calcium levels, calcineurin (p = 0.001) and NFATc1 (p = 0.001, p < 0.0001) activity and ORAI1 (p = 0.0093, p < 0.0001), CAM and CNB (p = 0.0214) transcripts significantly decreased in active vitiligo (AV) and severe GV (sGV) Tregs. Calcium treatment significantly increased intracellular calcium and ORAI1 transcripts in GV Tregs (p = 0.0042, p = 0.0035). Moreover, calcium treatment enhanced calcineurin and NFATc1 activity in GV Tregs (p = 0.0128, p < 0.0001). Remarkably, calcium treatment increased Treg mediated suppression of CD4+ and CD8+ T‐cells (p = 0.015, p = 0.006) in GV and increased Tregs associated cytokines: IL‐10 (p = 0.0323, p = 0.009), TGF‐β (p = 0.0321, p = 0.01) and decreased IFN‐γ production (p = 0.001, p = 0.016) by CD4+ and CD8+ T‐cells. Intracellular calcium levels positively correlated with calcineurin (r = 0.83; p < 0.0001) and NFATc1 (r = 0.61; p < 0.0001) activity, suggesting the enhanced Treg immunosuppressive capacity after calcium treatment. Our study for the first time suggests that reduced plasma calcium and ORAI1 transcripts are linked to calcium uptake defects in Tregs, which leads to reduced calcineurin and NFATc1 activation, thereby contributing to decreased Tregs immunosuppressive capacity in GV. Elevated GSK‐3β activity and GSKB and DYRK1A transcripts are involved in reduced NFATc1 activity in GV Tregs. Overall, the study suggests that calcium‐NFATc1‐signalling pathway is likely to be involved in defective Tregs function and can be implicated for development of effective Treg mediated therapeutics for GV. [ABSTRACT FROM AUTHOR]

Published

2022

8. The Microenvironment in Follicular Lymphoma

Author

Puebla-Osorio, Nahum, Strati, Paolo, Neelapu, Sattva S., and Fowler, Nathan H., editor

Published

2020

9. Acquisition of Immune Privilege in GBM Tumors: Role of Prostaglandins and Bile Salts

Author

Martyn A. Sharpe, David S. Baskin, Ryan D. Johnson, and Alexandra M. Baskin

Subjects

glioblastoma (GBM), regulatory T-cells (Tregs), microglia, prostaglandins, bile, sperm, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Based on the postulate that glioblastoma (GBM) tumors generate anti-inflammatory prostaglandins and bile salts to gain immune privilege, we analyzed 712 tumors in-silico from three GBM transcriptome databases for prostaglandin and bile synthesis/signaling enzyme-transcript markers. A pan-database correlation analysis was performed to identify cell-specific signal generation and downstream effects. The tumors were stratified by their ability to generate prostaglandins, their competency in bile salt synthesis, and the presence of bile acid receptors nuclear receptor subfamily 1, group H, member 4 (NR1H4) and G protein-coupled bile acid receptor 1 (GPBAR1). The survival analysis indicates that tumors capable of prostaglandin and/or bile salt synthesis are linked to poor outcomes. Tumor prostaglandin D2 and F2 syntheses are derived from infiltrating microglia, whereas prostaglandin E2 synthesis is derived from neutrophils. GBMs drive the microglial synthesis of PGD2/F2 by releasing/activating complement system component C3a. GBM expression of sperm-associated heat-shock proteins appears to stimulate neutrophilic PGE2 synthesis. The tumors that generate bile and express high levels of bile receptor NR1H4 have a fetal liver phenotype and a RORC-Treg infiltration signature. The bile-generating tumors that express high levels of GPBAR1 are infiltrated with immunosuppressive microglia/macrophage/myeloid-derived suppressor cells. These findings provide insight into how GBMs generate immune privilege and may explain the failure of checkpoint inhibitor therapy and provide novel targets for treatment.

Published

2023

10. Dynamics and epigenetic signature of regulatory T-cells following antiretroviral therapy initiation in acute HIV infection

Author

Alexis Yero, Tao Shi, Omar Farnos, Jean-Pierre Routy, Cécile Tremblay, Madeleine Durand, Christos Tsoukas, Cecilia T. Costiniuk, and Mohammad-Ali Jenabian

Subjects

HIV, antiretroviral therapy (ART), regulatory T-cells (Tregs), FoxP3, TGF-β1, CD39, Medicine, Medicine (General), R5-920

Abstract

Background: HIV infection promotes the expansion of immunosuppressive regulatory T-cells (Tregs), contributing to immune dysfunction, tissue fibrosis and disease progression. Early antiretroviral treatment (ART) upon HIV infection improves CD4 count and decreases immune activation. However, Treg dynamics and their epigenetic regulation following early ART initiation remain understudied. Methods: Treg subsets were characterized by flow cytometry in 103 individuals, including untreated HIV-infected participants in acute and chronic phases, ART-treated in early infection, elite controllers (ECs), immunological controllers (ICs), and HIV-uninfected controls. The methylation status of six regulatory regions of the foxp3 gene was assessed using MiSeq technology. Findings: Total Treg frequency increased overtime during HIV infection, which was normalized in early ART recipients. Tregs in untreated individuals expressed higher levels of activation and immunosuppressive markers (CD39, and LAP(TGF-β1)), which remained unchanged following early ART. Expression of gut migration markers (CCR9, Integrin-β7) by Tregs was elevated during untreated HIV infection, while they declined with the duration of ART but not upon early ART initiation. Notably, gut-homing Tregs expressing LAP(TGF-β1) and CD39 remained higher despite early treatment. Additionally, the increase in LAP(TGF-β1)+ Tregs overtime were consistent with higher demethylation of conserved non-coding sequence (CNS)-1 in the foxp3 gene. Remarkably, LAP(TGF-β1)-expressing Tregs in ECs were significantly higher than in uninfected subjects, while the markers of Treg activation and gut migration were not different. Interpretation: Early ART initiation was unable to control the levels of immunosuppressive Treg subsets and their gut migration potential, which could ultimately contribute to gut tissue fibrosis and HIV disease progression. Funding: This study was funded by the Canadian Institutes of Health Research (CIHR, grant MOP 142294) and in part by the AIDS and Infectious Diseases Network of the Réseau SIDA et maladies infectieuses du Fonds de recherche du Québec-Santé (FRQ-S).

Published

2021

11. Higher infiltration of intratumoral CD25+ FOXP3+ lymphocytes correlates with a favorable prognosis in patients with diffuse large B-cell lymphoma.

Author

Chang, Chen, Chen, Ya-Ping, Medeiros, L. Jeffrey, Chen, Tsai-Yun, and Chang, Kung-Chao

Subjects

*LYMPHOCYTES, *DIFFUSE large B-cell lymphomas, *T cells, *LYMPHOMAS, *SUPPRESSOR cells, *DENDRITIC cells

Abstract

Regulatory T-cells (Tregs) play an important role in cancer immunity but their prognostic impact is controversial in diffuse large B-cell lymphoma (DLBCL). Intratumoral Tregs in DLBCL (n = 70) were evaluated by double-stained CD25 and FOXP3 lymphocytes in formalin-fixed paraffin-embedded tissues, and correlated with clinicopathologic features. We found that increased numbers of intratumoral FOXP3+ lymphocytes (>2.4/HPF) and CD25 + FOXP3+ lymphocytes (>0.8/HPF) are favorable prognosticators (p =.004 and p <.001, respectively) in DLBCL patients, along with age <70 years, stage I–II disease, normal serum LDH level and low IPI scores (p <.001,.002,.002, and <.001, respectively). On multivariate analyses, a higher number of CD25 + FOXP3+ lymphocytes retained prognostic significance (p =.040). Interestingly, higher Treg infiltration correlated with increased infiltration by cytotoxic T-lymphocytes (γ = 0.294, p =.038) and nodal location (γ = 0.390, p =.004), but not with infiltration by CD123+ plasmacytoid dendritic cells, which were reported to induce Tregs with immune tolerance. Therefore, congruent with literature meta-analyses, higher intratumoral CD25 + FOXP3+ lymphocytes have a beneficial impact on DLBCL. [ABSTRACT FROM AUTHOR]

Published

2021

12. T-Cell Hyperactivation and Paralysis in Severe COVID-19 Infection Revealed by Single-Cell Analysis

Author

Bahire Kalfaoglu, José Almeida-Santos, Chanidapa Adele Tye, Yorifumi Satou, and Masahiro Ono

Subjects

T-cells, CD25, FOXP3, regulatory T-cells (Tregs), single cell RNA-seq, Furin, Immunologic diseases. Allergy, RC581-607

Abstract

Severe COVID-19 patients show various immunological abnormalities including T-cell reduction and cytokine release syndrome, which can be fatal and is a major concern of the pandemic. However, it is poorly understood how T-cell dysregulation can contribute to the pathogenesis of severe COVID-19. Here we show single cell-level mechanisms for T-cell dysregulation in severe COVID-19, demonstrating new pathogenetic mechanisms of T-cell activation and differentiation underlying severe COVID-19. By in silico sorting CD4+ T-cells from a single cell RNA-seq dataset, we found that CD4+ T-cells were highly activated and showed unique differentiation pathways in the lung of severe COVID-19 patients. Notably, those T-cells in severe COVID-19 patients highly expressed immunoregulatory receptors and CD25, whilst repressing the expression of FOXP3. Furthermore, we show that CD25+ hyperactivated T-cells differentiate into multiple helper T-cell lineages, showing multifaceted effector T-cells with Th1 and Th2 characteristics. Lastly, we show that CD25-expressing hyperactivated T-cells produce the protease Furin, which facilitates the viral entry of SARS-CoV-2. Collectively, CD4+ T-cells from severe COVID-19 patients are hyperactivated and FOXP3-mediated negative feedback mechanisms are impaired in the lung, which may promote immunopathology. Therefore, our study proposes a new model of T-cell hyperactivation and paralysis that drives immunopathology in severe COVID-19.

Published

2020

13. Impaired Differentiation of Highly Proliferative ICOS+-Tregs Is Involved in the Transition from Low to High Disease Activity in Systemic Lupus Erythematosus (SLE) Patients

Author

Florian Kälble, Lisa Wu, Hanns-Martin Lorenz, Martin Zeier, Matthias Schaier, and Andrea Steinborn

Subjects

systemic lupus erythematosus (SLE), active disease, inducible costimulatory molecule (ICOS), regulatory T-cells (Tregs), recent thymic emigrants (RTEs), resting mature naïve cells (MNs), Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Dysregulations in the differentiation of CD4+-regulatory-T-cells (Tregs) and CD4+-responder-T-cells (Tresps) are involved in the development of active systemic lupus erythematosus (SLE). Three differentiation pathways of highly proliferative inducible costimulatory molecule (ICOS)+- and less proliferative ICOS−-CD45RA+CD31+-recent-thymic-emigrant (RTE)-Tregs/Tresps via CD45RA−CD31+-memory-Tregs/Tresps (CD31+-memory-Tregs/Tresps), their direct proliferation via CD45RA+CD31−-mature naïve (MN)-Tregs/Tresps, and the production and differentiation of resting MN-Tregs/Tresp into CD45RA−CD31−-memory-Tregs/Tresps (CD31−-memory-Tregs/Tresps) were examined in 115 healthy controls, 96 SLE remission patients, and 20 active disease patients using six color flow cytometric analysis. In healthy controls an appropriate sequence of these pathways ensured regular age-dependent differentiation. In SLE patients, an age-independently exaggerated differentiation was observed for all Treg/Tresp subsets, where the increased conversion of resting MN-Tregs/Tresps particularly guaranteed the significantly increased ratios of ICOS+-Tregs/ICOS+-Tresps and ICOS−-Tregs/ICOS−-Tresps during remission. Changes in the differentiation of resting ICOS+-MN-Tresps and ICOS−-MN-Tregs from conversion to proliferation caused a significant shift in the ratio of ICOS+-Tregs/ICOS+-Tresps in favor of ICOS+-Tresps and a further increase in the ratio of ICOS−-Tregs/ICOS−-Tresps with active disease. The differentiation of ICOS+-RTE-Tregs/Tresps seems to be crucial for keeping patients in remission, where their limited production of proliferating resting MN-Tregs may be responsible for the occurrence of active disease flares.

Published

2021

14. Akt3-Mediated Protection Against Inflammatory Demyelinating Disease

Author

Juwen C. DuBois, Alex K. Ray, Ross C. Gruber, Yongwei Zhang, Ranee Aflakpui, Fernando Macian-Juan, and Bridget Shafit-Zagardo

Subjects

Akt3, neuroprotection, neuroinflammation, demyelination, EAE, regulatory T-cells (Tregs), Immunologic diseases. Allergy, RC581-607

Abstract

Akt is a serine/threonine protein kinase that plays a major role in regulating multiple cellular processes. While the isoforms Akt1 and Akt2 are involved in apoptosis and insulin signaling, respectively, the role for Akt3 remains uncertain. Akt3 is predominantly expressed in the brain, and total deletion of Akt3 in mice results in a reduction in brain size and neurodegeneration following injury. Previously, we found that Akt3−/− mice have a significantly worse clinical course during myelin-oligodendrocyte glycoprotein (MOG)-induced experimental autoimmune encephalomyelitis (EAE), an animal model in which autoreactive immune cells enter the CNS, resulting in inflammation, demyelination, and axonal injury. Spinal cords of Akt3−/− mice are severely demyelinated and have increased inflammation compared to WT, suggesting a neuroprotective role for Akt3 during EAE. To specifically address the role of Akt3 in neuroinflammation and maintaining neuronal integrity, we used several mouse strains with different manipulations to Akt3. During EAE, Akt3Nmf350 mice (with enhanced Akt3 kinase activity) had lower clinical scores, a lag in disease onset, a delay in the influx of inflammatory cells into the CNS, and less axonal damage compared to WT mice. A significant increased efficiency of differentiation toward FOXP3 expressing iTregs was also observed in Akt3Nmf350 mice relative to WT. Mice with a conditional deletion of Akt3 in CD4+ T-cells had an earlier onset of EAE symptoms, increased inflammation in the spinal cord and brain, and had fewer FOXP3+ cells and FOXP3 mRNA expression. No difference in EAE outcome was observed when Akt3 expression was deleted in neurons (Syn1-CKO). These results indicate that Akt3 signaling in T-cells and not neurons is necessary for maintaining CNS integrity during an inflammatory demyelinating disease.

Published

2019

15. Immunological and vascular characteristics in cavernous sinus meningioma.

Author

Kosugi, Kenzo, Tamura, Ryota, Ohara, Kentaro, Morimoto, Yukina, Kuranari, Yuki, Oishi, Yumiko, Yoshida, Kazunari, and Toda, Masahiro

Abstract

• Immune cells infiltrated significantly lower in cavernous sinus (CS) meningiomas compared with convexity meningiomas. • The expression of vascular endothelial growth factor (VEGF)-A and VEGFRs-1 & 2 was lower in CS meningioma. • The vascular structure in CS meningiomas differed from convexity meningiomas. • Lower VEGF expression and vascular construction contribute to the specific immune microenvironment in CS meningiomas. It is difficult to treat cavernous sinus (CS) meningiomas because of their complex vascular and neurological structures. Recently, immunotherapy has become an attractive therapeutic modality, but the role of tumor immune microenvironment is yet to be investigated for CS meningiomas. In the current study, these molecular and histopathological characteristics were examined in CS meningiomas. The present study used twenty-eight meningioma tissues arising in two different locations (8 CS and 20 convexity meningiomas). Immunohistochemical analyses were performed with CD3, CD4, CD8, Foxp3, CD163, PDGFR-β, VEGF receptors 1 & 2 (VEGFR-1, VEGFR-2), VEGF-A and HIF-1α. Quantitative polymerase chain reaction (qPCR) was performed to assess the expression of Foxp3, VEGF-A, CD163, VEGFRs-1 & 2 and HIF-1α. The numbers of different tumor-infiltrating immune cells, such as immunosuppressive cells, were significantly lower in CS meningiomas compared with convexity meningiomas. Analysis of the vascular characteristics showed the vessels in the CS meningiomas were covered with PDGFR-β-positive pericytes and were negative or had only very low amounts of VEGFR-1 and VEGFR-2. However, most vessels in convexity meningiomas showed high VEGFRs expression and were not covered with pericytes. Immunohistochemical and qPCR analyses revealed that the expression of HIF-1α, VEGF-A and VEGFRs-1 & 2 was lower in CS meningiomas. Fewer immunocompetent cells were observed in CS meningiomas compared with convexity meningiomas. Lower expression of VEGF-A, VEGFRs-1 and 2, and the vascular structure may contribute to this specific immune microenvironment. [ABSTRACT FROM AUTHOR]

Published

2019

16. Akt3-Mediated Protection Against Inflammatory Demyelinating Disease.

Author

DuBois, Juwen C., Ray, Alex K., Gruber, Ross C., Zhang, Yongwei, Aflakpui, Ranee, Macian-Juan, Fernando, and Shafit-Zagardo, Bridget

Subjects

CENTRAL nervous system injuries, MYELITIS, PROTEIN kinases, ENCEPHALOMYELITIS, INFLAMMATION, T cells, BRAIN

Abstract

Akt is a serine/threonine protein kinase that plays a major role in regulating multiple cellular processes. While the isoforms Akt1 and Akt2 are involved in apoptosis and insulin signaling, respectively, the role for Akt3 remains uncertain. Akt3 is predominantly expressed in the brain, and total deletion of Akt3 in mice results in a reduction in brain size and neurodegeneration following injury. Previously, we found that Akt3−/− mice have a significantly worse clinical course during myelin-oligodendrocyte glycoprotein (MOG)-induced experimental autoimmune encephalomyelitis (EAE), an animal model in which autoreactive immune cells enter the CNS, resulting in inflammation, demyelination, and axonal injury. Spinal cords of Akt3−/− mice are severely demyelinated and have increased inflammation compared to WT, suggesting a neuroprotective role for Akt3 during EAE. To specifically address the role of Akt3 in neuroinflammation and maintaining neuronal integrity, we used several mouse strains with different manipulations to Akt3. During EAE, Akt3 Nmf350 mice (with enhanced Akt3 kinase activity) had lower clinical scores, a lag in disease onset, a delay in the influx of inflammatory cells into the CNS, and less axonal damage compared to WT mice. A significant increased efficiency of differentiation toward FOXP3 expressing iTregs was also observed in Akt3 Nmf350 mice relative to WT. Mice with a conditional deletion of Akt3 in CD4+ T-cells had an earlier onset of EAE symptoms, increased inflammation in the spinal cord and brain, and had fewer FOXP3+ cells and FOXP3 mRNA expression. No difference in EAE outcome was observed when Akt3 expression was deleted in neurons (Syn1-CKO). These results indicate that Akt3 signaling in T-cells and not neurons is necessary for maintaining CNS integrity during an inflammatory demyelinating disease. [ABSTRACT FROM AUTHOR]

Published

2019

17. Control of Germinal Center Responses by T-Follicular Regulatory Cells

Author

James B. Wing, Murat Tekgüç, and Shimon Sakaguchi

Subjects

regulatory T-cells (Tregs), T follicular helper (Tfh) cell, T follicular regulatory (Tfr) cell, germinal center (GC), autoimmunity, Immunologic diseases. Allergy, RC581-607

Abstract

Regulatory T-cells (Treg cells), expressing the transcription factor Foxp3, have an essential role in the control of immune homeostasis. In order to control diverse types of immune responses Treg cells must themselves show functional heterogeneity to control different types of immune responses. Recent advances have made it clear that Treg cells are able to mirror the homing capabilities of known T-helper subtypes such as Th1, Th2, Th17, and T-follicular helper cells (Tfh), allowing them to travel to the sites of inflammation and deliver suppression in situ. One of the more recent discoveries in this category is the description of T-follicular regulatory (Tfr) cells, a specialized subset of Treg cells that control Tfh and resulting antibody responses. In this review we will discuss recent advances in our understanding of Tfr biology and the role of both Tfr and activated extra-follicular Tregs (eTreg) in the control of humoral immunity.

Published

2018

18. Control of Germinal Center Responses by T-Follicular Regulatory Cells.

Author

Wing, James B., Tekgüç, Murat, and Sakaguchi, Shimon

Subjects

T helper cells, IMMUNE response, GERMINAL centers

Abstract

Regulatory T-cells (Treg cells), expressing the transcription factor Foxp3, have an essential role in the control of immune homeostasis. In order to control diverse types of immune responses Treg cells must themselves show functional heterogeneity to control different types of immune responses. Recent advances have made it clear that Treg cells are able to mirror the homing capabilities of known T-helper subtypes such as Th1, Th2, Th17, and T-follicular helper cells (Tfh), allowing them to travel to the sites of inflammation and deliver suppression in situ. One of the more recent discoveries in this category is the description of T-follicular regulatory (Tfr) cells, a specialized subset of Treg cells that control Tfh and resulting antibody responses. In this review we will discuss recent advances in our understanding of Tfr biology and the role of both Tfr and activated extra-follicular Tregs (eTreg) in the control of humoral immunity. [ABSTRACT FROM AUTHOR]

Published

2018

19. Evaluation of T‐lymphocyte subpopulations in actinic keratosis, in situ and invasive squamous cell carcinoma of the skin.

Author

Stravodimou, Aristea, Tzelepi, Vassiliki, Papadaki, Helen, Mouzaki, Athanasia, Georgiou, Sophia, Melachrinou, Maria, and Kourea, Eleni P.

Subjects

*SQUAMOUS cell carcinoma, *SKIN diseases, *SKIN disease diagnosis, *ACTINIC keratosis, *PATIENTS, *GENETICS

Abstract

Background: Tumor infiltrating lymphocytes (TILs) represent important regulators of carcinogenesis. Cutaneous invasive squamous cell carcinoma (inSCC) develops through precursor lesions, namely in situ squamous cell carcinoma (isSCC) and actinic keratosis (AK), representing a natural model of carcinogenesis. The study evaluates TIL subpopulations in inSCC and its precursors by comparing 2 semiquantitative scoring systems, and assesses the presence of regulatory T‐cells (Tregs) in these lesions. Methods: Paraffin sections from 33 cases of AK, 19 isSCCs and 34 inSCCs with adjacent precursor lesions or normal skin (NS) were immunostained for CD3, CD4, CD8 and Foxp3. TIL subgroups were evaluated by the semiquantitative Klintrup‐Mäkinen (K‐M) score, and by a more detailed modification of this system. Treg counts were assessed by image analysis quantification. Results: An increase of all TIL subpolulations from precursor lesions toward inSCC was shown by both scoring systems. Treg counts progressively increased from NS to AK and isSCC, but decreased in inSCC. Tregs were more numerous in pT2 and around indolent inSCCs compared to T1 and aggressive subtypes. Conclusions: T‐cells and cytotoxic T‐cells progressively increase in cutaneous squamous cell carcinogenesis, while Treg counts diminish in inSCC. The K‐M score is an appropriate, easily applicable TIL scoring system in cutaneous inSCC. [ABSTRACT FROM AUTHOR]

Published

2018

20. Dynamics and epigenetic signature of regulatory T-cells following antiretroviral therapy initiation in acute HIV infection

Author

Cecilia T. Costiniuk, Madeleine Durand, Jean-Pierre Routy, Cécile Tremblay, Christos M. Tsoukas, Omar Farnós, Tao Shi, Alexis Yero, and Mohammad-Ali Jenabian

Subjects

Male, Medicine (General), Research paper, Integrin beta Chains, CCR9, HIV Infections, antiretroviral therapy (ART), T-Lymphocytes, Regulatory, Epigenesis, Genetic, 0302 clinical medicine, Transforming Growth Factor beta, TGF-β1, Medicine, Sida, 0303 health sciences, medicine.diagnostic_test, biology, Apyrase, FOXP3, Forkhead Transcription Factors, General Medicine, Methylation, 3. Good health, Regulatory sequence, Female, Adult, Anti-HIV Agents, chemical and pharmacologic phenomena, General Biochemistry, Genetics and Molecular Biology, Flow cytometry, Receptors, CCR, 03 medical and health sciences, R5-920, Acquired immunodeficiency syndrome (AIDS), Antigens, CD, FoxP3, Humans, Epigenetics, 030304 developmental biology, CD39, business.industry, regulatory T-cells (Tregs), HIV, DNA Methylation, medicine.disease, biology.organism_classification, Immunology, business, 030215 immunology

Abstract

Background HIV infection promotes the expansion of immunosuppressive regulatory T-cells (Tregs), contributing to immune dysfunction, tissue fibrosis and disease progression. Early antiretroviral treatment (ART) upon HIV infection improves CD4 count and decreases immune activation. However, Treg dynamics and their epigenetic regulation following early ART initiation remain understudied. Methods Treg subsets were characterized by flow cytometry in 103 individuals, including untreated HIV-infected participants in acute and chronic phases, ART-treated in early infection, elite controllers (ECs), immunological controllers (ICs), and HIV-uninfected controls. The methylation status of six regulatory regions of the foxp3 gene was assessed using MiSeq technology. Findings Total Treg frequency increased overtime during HIV infection, which was normalized in early ART recipients. Tregs in untreated individuals expressed higher levels of activation and immunosuppressive markers (CD39, and LAP(TGF-β1)), which remained unchanged following early ART. Expression of gut migration markers (CCR9, Integrin-β7) by Tregs was elevated during untreated HIV infection, while they declined with the duration of ART but not upon early ART initiation. Notably, gut-homing Tregs expressing LAP(TGF-β1) and CD39 remained higher despite early treatment. Additionally, the increase in LAP(TGF-β1)+ Tregs overtime were consistent with higher demethylation of conserved non-coding sequence (CNS)-1 in the foxp3 gene. Remarkably, LAP(TGF-β1)-expressing Tregs in ECs were significantly higher than in uninfected subjects, while the markers of Treg activation and gut migration were not different. Interpretation Early ART initiation was unable to control the levels of immunosuppressive Treg subsets and their gut migration potential, which could ultimately contribute to gut tissue fibrosis and HIV disease progression. Funding This study was funded by the Canadian Institutes of Health Research (CIHR, grant MOP 142294) and in part by the AIDS and Infectious Diseases Network of the Reseau SIDA et maladies infectieuses du Fonds de recherche du Quebec-Sante (FRQ-S).

Published

2021

21. Impaired Differentiation of Highly Proliferative ICOS+-Tregs Is Involved in the Transition from Low to High Disease Activity in Systemic Lupus Erythematosus (SLE) Patients

Author

Hanns-Martin Lorenz, Martin Zeier, Lisa Wu, Florian Kälble, Matthias Schaier, and Andrea Steinborn

Subjects

CD31, resting mature naïve cells (MNs), QH301-705.5, chemical and pharmacologic phenomena, Catalysis, recent thymic emigrants (RTEs), Inorganic Chemistry, Disease activity, inducible costimulatory molecule (ICOS), TheoryofComputation_ANALYSISOFALGORITHMSANDPROBLEMCOMPLEXITY, Active disease, Medicine, active disease, Biology (General), Physical and Theoretical Chemistry, Treg/Tresp cell differentiation, QD1-999, Molecular Biology, Spectroscopy, systemic lupus erythematosus (SLE), Transition (genetics), business.industry, regulatory T-cells (Tregs), Organic Chemistry, hemic and immune systems, General Medicine, Computer Science Applications, Costimulatory Molecule, Chemistry, Immunology, Color flow, business

Abstract

Dysregulations in the differentiation of CD4+-regulatory-T-cells (Tregs) and CD4+-responder-T-cells (Tresps) are involved in the development of active systemic lupus erythematosus (SLE). Three differentiation pathways of highly proliferative inducible costimulatory molecule (ICOS)+- and less proliferative ICOS−-CD45RA+CD31+-recent-thymic-emigrant (RTE)-Tregs/Tresps via CD45RA−CD31+-memory-Tregs/Tresps (CD31+-memory-Tregs/Tresps), their direct proliferation via CD45RA+CD31−-mature naïve (MN)-Tregs/Tresps, and the production and differentiation of resting MN-Tregs/Tresp into CD45RA−CD31−-memory-Tregs/Tresps (CD31−-memory-Tregs/Tresps) were examined in 115 healthy controls, 96 SLE remission patients, and 20 active disease patients using six color flow cytometric analysis. In healthy controls an appropriate sequence of these pathways ensured regular age-dependent differentiation. In SLE patients, an age-independently exaggerated differentiation was observed for all Treg/Tresp subsets, where the increased conversion of resting MN-Tregs/Tresps particularly guaranteed the significantly increased ratios of ICOS+-Tregs/ICOS+-Tresps and ICOS−-Tregs/ICOS−-Tresps during remission. Changes in the differentiation of resting ICOS+-MN-Tresps and ICOS−-MN-Tregs from conversion to proliferation caused a significant shift in the ratio of ICOS+-Tregs/ICOS+-Tresps in favor of ICOS+-Tresps and a further increase in the ratio of ICOS−-Tregs/ICOS−-Tresps with active disease. The differentiation of ICOS+-RTE-Tregs/Tresps seems to be crucial for keeping patients in remission, where their limited production of proliferating resting MN-Tregs may be responsible for the occurrence of active disease flares.

Published

2021

22. Immunosuppressive Tryptophan Catabolism and Gut Mucosal Dysfunction Following Early HIV Infection.

Author

Jenabian, Mohammad-Ali, El-Far, Mohamed, Vyboh, Kishanda, Kema, Ido, Costiniuk, Cecilia T., Thomas, Rejean, Baril, Jean-Guy, LeBlanc, Roger, Kanagaratham, Cynthia, Radzioch, Danuta, Allam, Ossama, Ahmad, Ali, Lebouché, Bertrand, Tremblay, Cécile, Ancuta, Petronela, and Routy, Jean-Pierre

Subjects

*TRYPTOPHAN metabolism, *INFLAMMATION, *GASTROINTESTINAL mucosa, *ANTIRETROVIRAL agents, *HIV infections, *T cells, *DENDRITIC cells, *LIPOPOLYSACCHARIDES, *DISEASES

Abstract

Background. Tryptophan (Trp) catabolism into kynurenine (Kyn) contributes to immune dysfunction in chronic human immunodeficiency virus (HIV) infection. To better define the relationship between Trp catabolism, inflammation, gut mucosal dysfunction, and the role of early antiretroviral therapy (ART), we prospectively assessed patients early after they acquired HIV. Methods. Forty patients in the early phase of infection were longitudinally followed for 12 months after receiving a diagnosis of HIV infection; 24 were untreated, and 16 were receiving ART. Kyn/Trp ratio, regulatory T-cells (Tregs) frequency, T-cell activation, dendritic cell counts, and plasma levels of gut mucosal dysfunction markers intestinal-type fatty acid-binding protein, soluble suppression of tumorigenicity 2, and lipopolysaccharide were assessed. Results. Compared with healthy subjects, patients in the early phase of infection presented with elevated Kyn/Trp ratios, which further increased in untreated patients but normalized in ART recipients. Accordingly, in untreated subjects, the elevated Treg frequency observed at baseline continued to increase over time. The highest CD8+ T-cell activation was observed during the early phase of infection and decreased in untreated patients, whereas activation normalized in ART recipients. The Kyn/Trp ratio was positively associated with CD8+ T-cell activation and levels of inflammatory cytokines (interleukin 6, interferon γ-inducible protein 10, interleukin 18, and tumor necrosis factor α) and negatively associated with dendritic cell frequencies at baseline and in untreated patients. However, ART did not normalize plasma levels of gut mucosal dysfunction markers. Conclusions. Early initiation of ART normalized enhanced Trp catabolism and immune activation but did not improve plasma levels of gut mucosal dysfunction markers. [ABSTRACT FROM AUTHOR]

Published

2015

23. Activation of GILZ gene by photoactivated 8-methoxypsoralen: Potential role of immunoregulatory dendritic cells in extracorporeal photochemotherapy.

Author

Futterleib, Jeffrey S., Feng, Hao, Tigelaar, Robert E., Choi, Jaehyuk, and Edelson, Richard L.

Subjects

*GLUCOCORTICOIDS, *LEUCINE zippers, *PHOTOACTIVATION, *PSORALENS, *IMMUNOREGULATION, *DENDRITIC cells, *PHOTOCHEMOTHERAPY

Abstract

Abstract: Extracorporeal photochemotherapy (ECP) is a widely used method for either immunization against cutaneous T cell lymphoma or immunosuppression of graft-versus-host disease and organ transplant rejection (OTR). Leukapheresed blood is routed through a chamber, in which 8-methoxypsoralen is activated by ultraviolet energy (PUVA), thereby causing DNA crosslinks in processed leukocytes. Return of ECP-processed mononuclear leukocytes to the patient then modulates aberrant T cell immunity. Since interaction with the ECP flow chamber induces monocyte-to-dendritic antigen presenting cell (DC) maturation, we examined the possibility that PUVA may direct the most heavily exposed monocytes to differentiate into tolerogenic DC, while the least exposed DC might remain immunogenic. Expression of the glucocorticoid-induced leucine zipper (GILZ) gene is a distinguishing marker of tolerogenic DC. We report that PUVA directly stimulates GILZ expression. PUVA-exposed DC up-regulated GILZ, down-regulated costimulatory CD80 and CD86, became resistant to Toll-like receptor-induced maturation, increased IL-10 production and decreased IL-12p70 production, all features of immunosuppressive DC. Knockdown of GILZ with siRNA reduced IL-10 and increased IL-12p70 production, demonstrating that GILZ is critical for this profile. PUVA-induction of GILZ expression by DC may help explain how ECP suppresses GVHD and OTR. Conversely, those ECP-processed monocytes minimally exposed to PUVA may mediate ECP’s immunogenic effects. [Copyright &y& Elsevier]

Published

2014

24. Circulating IL-35 in pancreatic ductal adenocarcinoma patients.

Author

Jin, Peng, Ren, He, Sun, Wei, Xin, Wen, Zhang, Huan, and Hao, Jihui

Subjects

*INTERLEUKINS, *PANCREATIC duct, *ADENOCARCINOMA, *CYTOKINES, *IMMUNOSUPPRESSION, *T cells, *PATIENTS

Abstract

Abstract: IL-35 is a novel inhibitory cytokine that is mainly produced by regulatory T-cells (Tregs) and is required for Treg-mediated immunosuppression. However, the plasma levels of IL-35 in patients with pancreatic ductal adenocarcinoma (PDAC) have never been investigated. In this study, we found that plasma IL-35 levels more significantly increased in PDAC patients than in normal controls (134.53±92.45pg/mL vs. 14.26±6.56pg/mL). IL-35 mRNA levels were positively correlated with plasma IL-35 levels (EBI3, R =0.925, p <0.01; p35, R =0.916, p <0.01). Furthermore, IL-35 expression levels were associated with lymph node metastasis (p =0.001) and late tumor stage (p =0.002). For the resected patients, high IL-35 expression levels were associated with large tumor size (p <0.01), higher TNM classification T staging (p <0.05), and late tumor stage (p <0.05). In conclusion, circulating IL-35 in PDAC patients significantly increased, suggesting that regulating the expression of IL-35 may provide a new possible target for the treatment of PDAC patients, especially for the resectable ones. [Copyright &y& Elsevier]

Published

2014

25. T-cell hyperactivation and paralysis in severe COVID-19 infection revealed by single-cell analysis

Author

Chanidapa Adele Tye, Bahire Kalfaoglu, Masahiro Ono, Yorifumi Satou, José Almeida-Santos, and Medical Research Council (MRC)

Subjects

Lymphocyte Activation, Severity of Illness Index, T-Lymphocytes, Regulatory, 0302 clinical medicine, 1108 Medical Microbiology, Immunopathology, Databases, Genetic, Immunology and Allergy, IL-2 receptor, RNA-Seq, Receptor, Furin, Original Research, 0303 health sciences, Hyperactivation, Effector, FOXP3, Forkhead Transcription Factors, 3. Good health, Cytokine release syndrome, medicine.anatomical_structure, 1107 Immunology, Single-Cell Analysis, lcsh:Immunologic diseases. Allergy, T cell, Immunology, Receptors, Antigen, T-Cell, macromolecular substances, Biology, 03 medical and health sciences, Viral entry, medicine, Humans, Paralysis, single cell RNA-seq, CD25, 030304 developmental biology, business.industry, SARS-CoV-2, regulatory T-cells (Tregs), T-cells, Interleukin-2 Receptor alpha Subunit, COVID-19, Virus Internalization, medicine.disease, biology.protein, lcsh:RC581-607, business, Transcriptome, 030215 immunology

Abstract

Severe COVID-19 patients can show respiratory failure, T-cell reduction, and cytokine release syndrome (CRS), which can be fatal in both young and aged patients and is a major concern of the pandemic. However, the pathogenetic mechanisms of CRS in COVID-19 are poorly understood. Here we show single cell-level mechanisms for T-cell dysregulation in severe SARS-CoV-2 infection, and thereby demonstrate the mechanisms underlying T-cell hyperactivation and paralysis in severe COVID-19 patients. By in silico sorting CD4+ T-cells from a single cell RNA-seq dataset, we found that CD4+ T-cells were highly activated and showed unique differentiation pathways in the lung of severe COVID-19 patients. Notably, those T-cells in severe COVID-19 patients highly expressed immunoregulatory receptors and CD25, whilst repressing the expression of the transcription factor FOXP3 and interestingly, both the differentiation of regulatory T-cells (Tregs) and Th17 was inhibited. Meanwhile, highly activated CD4+ T-cells express PD-1 alongside macrophages that express PD-1 ligands in severe patients, suggesting that PD-1-mediated immunoregulation was partially operating. Furthermore, we show that CD25+ hyperactivated T-cells differentiate into multiple helper T-cell lineages, showing multifaceted effector T-cells with Th1 and Th2 characteristics. Lastly, we show that CD4+ T-cells, particularly CD25-expressing hyperactivated T-cells, produce the protease Furin, which facilitates the viral entry of SARS-CoV-2. Collectively, CD4+ T-cells from severe COVID-19 patients are hyperactivated and FOXP3-mediated negative feedback mechanisms are impaired in the lung, while activated CD4+ T-cells continue to promote further viral infection through the production of Furin. Therefore, our study proposes a new model of T-cell hyperactivation and paralysis that drives pulmonary damage, systemic CRS and organ failure in severe COVID-19 patients.

Published

2020

26. Regulation of the MIR155 host gene in physiological and pathological processes.

Author

Elton, Terry S., Selemon, Helina, Elton, Shane M., and Parinandi, Narasimham L.

Subjects

*GENETIC regulation, *MICRORNA genetics, *ADAPTOR proteins, *MACROPHAGES, *VIRUS diseases, *CARDIOVASCULAR diseases

Abstract

Abstract: MicroRNAs (miRNAs), a family of small nonprotein-coding RNAs, play a critical role in posttranscriptional gene regulation by acting as adaptors for the miRNA-induced silencing complex to inhibit gene expression by targeting mRNAs for translational repression and/or cleavage. miR-155-5p and miR-155-3p are processed from the B-cell Integration Cluster (BIC) gene (now designated, MIR155 host gene or MIR155HG). MiR-155-5p is highly expressed in both activated B- and T-cells and in monocytes/macrophages. MiR-155-5p is one of the best characterized miRNAs and recent data indicate that miR-155-5p plays a critical role in various physiological and pathological processes such as hematopoietic lineage differentiation, immunity, inflammation, viral infections, cancer, cardiovascular disease, and Down syndrome. In this review we summarize the mechanisms by which MIR155HG expression can be regulated. Given that the pathologies mediated by miR-155-5p result from the over-expression of this miRNA it may be possible to therapeutically attenuate miR-155-5p levels in the treatment of several pathological processes. [Copyright &y& Elsevier]

Published

2013

27. Mucosal application of cationic poly(d,l-lactide-co-glycolide) microparticles as carriers of DNA vaccine and adjuvants to protect chickens against infectious bursal disease.

Author

Negash, Tamiru, Liman, Martin, and Rautenschlein, Silke

Subjects

*POLYLACTIC acid, *GLYCOLIC acid, *DNA vaccines, *CHICKEN diseases, *VIRUS diseases, *T cells, *CELLULAR control mechanisms, *VIRAL load

Abstract

Highlights: [•] Cationic PLGA-MP based IBDV-DNA vaccine efficacy was evaluated in chickens. [•] Mucosal application of MP-IBDV-DNA vaccine and adjuvants conferred protection. [•] The protected chickens showed less bursal lesions and antigen load in the bursa. [Copyright &y& Elsevier]

Published

2013

28. Regulatory T-cells in systemic lupus erythematosus and rheumatoid arthritis

Author

Chavele, Konstantia-Maria and Ehrenstein, Michael R.

Subjects

*SYSTEMIC lupus erythematosus, *RHEUMATOID arthritis, *T cells, *AUTOIMMUNE diseases, *PHENOTYPES, *ANIMAL disease models

Abstract

Abstract: Regulatory T-cells (Tregs) are the guardians of peripheral tolerance acting to prevent autoimmune diseases such as systemic lupus erythomatosus (SLE) and rheumatoid arthritis (RA). Defects in Tregs have been reported in these two diseases despite significant differences in their clinical phenotype and pathogenesis. In both diseases the potency of Treg fails to keep pace with the activation of effector cells and are unable to resist the ensuing inflammation. This review will discuss the phenotypic, numeric, and functional abnormalities in Tregs and their role in patients and murine models of SLE and RA. [Copyright &y& Elsevier]

Published

2011

29. Immunoprofile Changes during Dasatinib Treatment in Patients with Chronic Myeloid Leukemia : A Prospective Observational Study

Author

Kuno, Masatomo, Nakane, Takahiko, Katayama, Takako, Koh, Hideo, Nakashima, Yasuhiro, Nishimoto, Mitsutaka, Nakamae, Mika, Hirose, Asao, Hino, Masayuki, and Nakamae, Hirohisa

Subjects

hemic and lymphatic diseases, Large granular lymphocytes (LGLs), Dasatinib, Regulatory T-cells (Tregs), Natural killer (NK)-cell reactivity

Abstract

Background : Clonal expansion of large granular lymphocytes (LGLs) induced by dasatinib treatment was related to favorable prognosis. However, the detailed mechanism of the expansion of LGLs and the characteristics of patients who develop LGL lymphocytosis remains unclear. It also remains uncertain that LGLs actually have anti-tumor effects. To address these issues, we conducted a prospective observational study in chronic-phase chronic myeloid leukemia (CML) patients. / Methods : We analyzed cell counts of lymphocyte subsets, immunophenotyping of immune cells, natural killer (NK) -cell reactivity, and plasma concentration levels of soluble factors in 30 CML patients. Quantification of BCR-ABL mRNA transcripts by real-time quantitative PCR was periodically conducted after the start of tyrosine kinase inhibitor treatment....

Published

2017

30. Akt3-Mediated Protection Against Inflammatory Demyelinating Disease

Author

Yongwei Zhang, Bridget Shafit-Zagardo, Fernando Macian-Juan, Juwen C. DuBois, Alex K. Ray, Ranee Aflakpui, and Ross C. Gruber

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, Encephalomyelitis, Autoimmune, Experimental, Immunology, Fluorescent Antibody Technique, AKT1, Inflammation, Biology, Neuroprotection, AKT3, Immunophenotyping, neuroinflammation, Mice, 03 medical and health sciences, 0302 clinical medicine, T-Lymphocyte Subsets, medicine, Animals, Immunology and Allergy, RNA, Messenger, Kinase activity, Protein kinase B, Neuroinflammation, Original Research, Mice, Knockout, Akt3, EAE, regulatory T-cells (Tregs), Experimental autoimmune encephalomyelitis, Forkhead Transcription Factors, medicine.disease, Immunohistochemistry, Disease Models, Animal, 030104 developmental biology, Spinal Cord, neuroprotection, Disease Susceptibility, demyelination, medicine.symptom, lcsh:RC581-607, Proto-Oncogene Proteins c-akt, Biomarkers, Demyelinating Diseases, Signal Transduction, 030215 immunology

Abstract

Akt is a serine/threonine protein kinase that plays a major role in regulating multiple cellular processes. While the isoforms Akt1 and Akt2 are involved in apoptosis and insulin signaling, respectively, the role for Akt3 remains uncertain. Akt3 is predominantly expressed in the brain, and total deletion of Akt3 in mice results in a reduction in brain size and neurodegeneration following injury. Previously, we found that Akt3-/- mice have a significantly worse clinical course during myelin-oligodendrocyte glycoprotein (MOG)-induced experimental autoimmune encephalomyelitis (EAE), an animal model in which autoreactive immune cells enter the CNS, resulting in inflammation, demyelination, and axonal injury. Spinal cords of Akt3-/- mice are severely demyelinated and have increased inflammation compared to WT, suggesting a neuroprotective role for Akt3 during EAE. To specifically address the role of Akt3 in neuroinflammation and maintaining neuronal integrity, we used several mouse strains with different manipulations to Akt3. During EAE, Akt3 Nmf350 mice (with enhanced Akt3 kinase activity) had lower clinical scores, a lag in disease onset, a delay in the influx of inflammatory cells into the CNS, and less axonal damage compared to WT mice. A significant increased efficiency of differentiation toward FOXP3 expressing iTregs was also observed in Akt3 Nmf350 mice relative to WT. Mice with a conditional deletion of Akt3 in CD4+ T-cells had an earlier onset of EAE symptoms, increased inflammation in the spinal cord and brain, and had fewer FOXP3+ cells and FOXP3 mRNA expression. No difference in EAE outcome was observed when Akt3 expression was deleted in neurons (Syn1-CKO). These results indicate that Akt3 signaling in T-cells and not neurons is necessary for maintaining CNS integrity during an inflammatory demyelinating disease.

Published

2019

31. Impaired Differentiation of Highly Proliferative ICOS + -Tregs Is Involved in the Transition from Low to High Disease Activity in Systemic Lupus Erythematosus (SLE) Patients.

Author

Kälble, Florian, Wu, Lisa, Lorenz, Hanns-Martin, Zeier, Martin, Schaier, Matthias, and Steinborn, Andrea

Subjects

*SYSTEMIC lupus erythematosus, *REGULATORY T cells

Abstract

Dysregulations in the differentiation of CD4+-regulatory-T-cells (Tregs) and CD4+-responder-T-cells (Tresps) are involved in the development of active systemic lupus erythematosus (SLE). Three differentiation pathways of highly proliferative inducible costimulatory molecule (ICOS)+- and less proliferative ICOS−-CD45RA+CD31+-recent-thymic-emigrant (RTE)-Tregs/Tresps via CD45RA−CD31+-memory-Tregs/Tresps (CD31+-memory-Tregs/Tresps), their direct proliferation via CD45RA+CD31−-mature naïve (MN)-Tregs/Tresps, and the production and differentiation of resting MN-Tregs/Tresp into CD45RA−CD31−-memory-Tregs/Tresps (CD31−-memory-Tregs/Tresps) were examined in 115 healthy controls, 96 SLE remission patients, and 20 active disease patients using six color flow cytometric analysis. In healthy controls an appropriate sequence of these pathways ensured regular age-dependent differentiation. In SLE patients, an age-independently exaggerated differentiation was observed for all Treg/Tresp subsets, where the increased conversion of resting MN-Tregs/Tresps particularly guaranteed the significantly increased ratios of ICOS+-Tregs/ICOS+-Tresps and ICOS−-Tregs/ICOS−-Tresps during remission. Changes in the differentiation of resting ICOS+-MN-Tresps and ICOS−-MN-Tregs from conversion to proliferation caused a significant shift in the ratio of ICOS+-Tregs/ICOS+-Tresps in favor of ICOS+-Tresps and a further increase in the ratio of ICOS−-Tregs/ICOS−-Tresps with active disease. The differentiation of ICOS+-RTE-Tregs/Tresps seems to be crucial for keeping patients in remission, where their limited production of proliferating resting MN-Tregs may be responsible for the occurrence of active disease flares. [ABSTRACT FROM AUTHOR]

Published

2021

32. Memory and naïve gamma delta regulatory T-cell gene expression in the first 24-weeks of peanut oral immunotherapy.

Author

Anvari, Sara, Watkin, Levi, Rajapakshe, Kimal, Hassan, Oluwatomi, Schuster, Kimberly, Coarfa, Cristian, and Davis, Carla M.

Subjects

*REGULATOR genes, *GENE expression, *IMMUNOTHERAPY, *REGULATORY T cells, *PEANUTS, *PSYCHONEUROIMMUNOLOGY

Abstract

Peanut oral immunotherapy (POIT) has provided desensitization to peanut allergic individuals. Limited immunological evaluation exists during the first 24-weeks of POIT. Regulatory T-cells (Tregs) are antigen induced immunosuppressive T-cells important in establishing tolerance. Delineation of early immunologic changes contributing to the development of peanut desensitization would help clarify the mechanism of action in POIT. We performed single-cell RNA sequencing (scRNAseq) on Tregs in pediatric subjects undergoing POIT during the first 24-weeks of therapy to evaluate early immunological changes induced by POIT. PBMC samples from peanut allergic subjects between 5 and 12 years of age enrolled in a Phase 1/2a POIT study were collected and analyzed at 0, 6, and 24-weeks after POIT initiation and samples were compared to healthy non-peanut allergic controls. Tregs were enriched from PBMCs and scRNAseq analysis performed. Cell Ranger 3.1.0 (10× Genomics) was utilized to identify cell clusters and differentially expressed genes, and results were analyzed with Seurat suite version 3.0.0. Gene analysis revealed 10 major clusters corresponding to different cell types observed to change during POIT when compared to the healthy, non-peanut-allergic state. scRNAseq analysis of Tregs revealed strong CD3G expression correlating with gdTregs. scRNAseq analysis of gdTregs revealed dynamic changes occurring within the first 6-weeks of treatment and cell frequencies of naïve and memory gdTregs at 24-weeks of treatment reducing to levels similar to healthy controls. Analysis of transcriptomic cell identity analysis using SingleR showed gene expression in gdTregs similar to healthy control after 24-weeks of POIT treatment. scRNAseq analysis revealed alterations in gene expression for memory and naïve gdTregs during this timeframe. Specifically, expression of OX40R (TNFRSF4), GITR (TNFRSF18), TGFB1, CTLA4, ISG20, CD69 were upregulated in memory gdTregs compared to naive gdTregs by 24-weeks of POIT, while IL7R and SELL were downregulated in memory gdTregs compared to naïve gdTregs. There are specific expression profiles of peripheral naïve and mature gdTreg cells in peanut allergic patients undergoing POIT in the first 24-weeks of treatment implicating pathways involved in maintenance of immune homeostasis. gdTreg cells may contribute to the tolerogenic effect of POIT within the first 24-weeks of POIT treatment. These findings suggest that gdTregs cells may be an early marker of desensitization in subjects undergoing POIT. • gdTreg modulation is observed in the 1st 6-weeks of peanut oral immunotherapy, a potential early marker of desensitization. • At 24-weeks of POIT, gdTregs upregulate OX40R, GITR, TFGB1, CTLA4, ISG20, CD69, and downregulate IL7R and SELL. • gdTreg expression suggests POIT modulates type-2 inflammatory responses. [ABSTRACT FROM AUTHOR]

Published

2021

33. Heterogeneous Tumor-Immune Microenvironments between Primary and Metastatic Tumors in a Patient with ALK Rearrangement-Positive Large Cell Neuroendocrine Carcinoma

Author

Daisuke Tamanoi, Koichi Saruwatari, Naomi Hirata, Shinya Sakata, Sunao Ushijima, Takuro Sakagami, Yusuke Tomita, Kazuaki Sugahara, Akira Takaki, Kosuke Imamura, Takahiro Tashiro, Megumi Inaba, and Ryo Sato

Subjects

Lung Neoplasms, medicine.medical_treatment, Neuroendocrine tumors, lcsh:Chemistry, large cell neuroendocrine carcinoma (LCNEC), Tumor Microenvironment, Anaplastic lymphoma kinase, Anaplastic Lymphoma Kinase, lcsh:QH301-705.5, Spectroscopy, Gene Rearrangement, tumor-immune microenvironments (TIME), B cell, medicine.diagnostic_test, Communication, General Medicine, Prognosis, Computer Science Applications, medicine.anatomical_structure, Female, Adult, Catalysis, Inorganic Chemistry, Lymphocytes, Tumor-Infiltrating, Biopsy, medicine, Humans, Physical and Theoretical Chemistry, Lung cancer, Protein Kinase Inhibitors, immune checkpoint, Molecular Biology, regulatory T-cells (Tregs), business.industry, Organic Chemistry, Immunotherapy, programmed death-ligand 1 (PD-L1), medicine.disease, Immune checkpoint, Carcinoma, Neuroendocrine, tumor-infiltrating lymphocyte (TIL), anaplastic lymphoma kinase (ALK), lcsh:Biology (General), lcsh:QD1-999, Cancer cell, Cancer research, heterogeneity, neuroendocrine tumors (NET), business

Abstract

Evolution of tumor-immune microenviroments (TIMEs) occurs during tumor growth and dissemination. Understanding inter-site tumor-immune heterogeneity is essential to harness the immune system for cancer therapy. While the development of immunotherapy against lung cancer with driver mutations and neuroendocrine tumors is ongoing, little is known about the TIME of large cell neuroendocrine carcinoma (LCNEC) or anaplastic lymphoma kinase (ALK) rearrangement-positive lung cancer. We present a case study of a 32-year-old female patient with ALK-rearrangement-positive LCNEC, who had multiple distant metastases including mediastinal lymph-node, bilateral breasts, multiple bones, liver and brain. Multiple biopsy samples obtained from primary lung and three metastatic tumors were analyzed by fluorescent multiplex immunohistochemistry. Tissue localizations of tumor-infiltrating lymphocytes in the tumor nest and surrounding stroma were evaluated. T cell and B cell infiltrations were decreased with distance from primary lung lesion. Although each tumor displayed a unique TIME, all tumors exhibited concomitant regression after treatment with an ALK-inhibitor. This study provides the first evidence of the coexistence of distinct TIME within a single individual with ALK-rearrangement-positive LCNEC. The present study contributes to our understanding of heterogeneous TIMEs between primary and metastatic lesions and provides new insights into the complex interplay between host-immunity and cancer cells in primary and metastatic lesions.

Published

2020

34. Opportunities and challenges of bi-specific antibodies.

Author

Segués A, Huang S, Sijts A, Berraondo P, and Zaiss DM

Subjects

Antibodies, Bispecific, Antibodies, Monoclonal, Humans, Tumor Microenvironment, Autoimmune Diseases, Neoplasms drug therapy

Abstract

The recent clinical approval of different Bi-specific antibodies (BsAbs) has revealed the great therapeutic potential of this novel class of biologicals. For example, the bispecific T-cell engager (BiTE), Blinatumomab, demonstrated the unique capacity of BsAbs to link T-cells with tumor cells, inducing targeted tumor cell removal. Additionally, Amivantamab, recognizing the EGFR and cMet in cis, revealed a substantial improvement of therapeutic efficacy by concomitantly targeting two tumor antigens. Cis-targeting BsAbs furthermore allow discerning cell populations which concurrently express two antigens, for which each antigen expression pattern in itself might not be selective. In this way, BsAbs harbor the great prospect of being more specific and showing fewer side effects than monoclonal antibodies. Nevertheless, BsAbs have also faced major obstacles, for instance, in ensuring reliable assembly and clinical-grade purification. In this review, we summarize the different available antibody platforms currently used for the generation of IgG-like and non-IgG-like BsAbs and explain which approaches have been used to assemble those BsAbs which are currently approved for clinical application. By focusing on the example of regulatory T-cells (Tregs) and the different, ongoing approaches to develop BsAbs specifically targeting Tregs within the tumor microenvironment, our review highlights the huge potential as well as the pitfalls BsAb face in order to emerge as one of the most effective therapeutic biologicals targeting desired cell populations in a highly selective way. Such BsAb may improve treatment efficacy and reduce side effects, thereby opening novel treatment opportunities for a range of different diseases, such as cancer or autoimmune diseases., Competing Interests: Disclosure statement The authors declare no competing interests. Figures created by BioRender., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

35. The Role of Inflammatory and Cytokine Biomarkers in the Pathogenesis of Frailty Syndrome.

Author

Mir R, Jha CK, Khullar N, Maqbool M, Dabla PK, Mathur S, Moustafa A, Faridi UA, Hamadi A, Mir MM, and Abu Duhier FM

Subjects

Humans, Aged, Cytokines, Frail Elderly, Biomarkers metabolism, Inflammation, Aging, Vitamin D, Frailty

Abstract

Frailty is a conglomerated elderly disorder that includes multiple abnormalities, like anemia, an increased titer of catabolic hormones, and compromised physiology of most of the body systems. Many studies have established the biomarkers that correlate with physical function and immune aging; however, people can age differently, so chronological age is not a sufficient marker of susceptibility to disabilities, morbidities, and mortality. The pathophysiology of frailty is not clearly understood, but a critical role of enhanced inflammation in the body is hypothesized. Many factors contribute to the development of frailty syndrome, such as pro-inflammatory cytokines, inflammatory markers, inflammatory cytokines, and secosteroids, like vitamin D. This review aims to highlight the role of inflammatory and cytokine biomarkers and vitamin D in the pathogenesis of Frailty Syndrome., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2022

36. Early IL-10 producing B-cells and coinciding Th/Tr17 shifts during three year grass-pollen AIT

Author

Bernhard Haller, Katharina Dietz, Guido Piontek, Zuzana Hajdu, Adam Chaker, Kathrin Suttner, Carsten B. Schmidt-Weber, Lisa Pechtold, Constanze A. Jakwerth, Juan Antonio Aguilar-Pimentel, Matthias Schiemann, Ulrich M. Zissler, and Ferdinand Guerth

Subjects

0301 basic medicine, Allergic Rhinitis, Allergy, Research paper, medicine.medical_treatment, T-Lymphocytes, InformationSystems_INFORMATIONSTORAGEANDRETRIEVAL, ComputingMethodologies_IMAGEPROCESSINGANDCOMPUTERVISION, Specific Immunotherapy, C-C chemokine receptor type 6, medicine.disease_cause, Poaceae, ComputingMethodologies_ARTIFICIALINTELLIGENCE, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Allergen, Regulatory B-cells (Bregs), medicine, Humans, Specific Immunot Herapy, Biomarker, Prediction, Surrogate, Tolerance, Regulatory Bells (bregs), Regulatory T-cells (tregs), Cells, Cultured, ComputingMethodologies_COMPUTERGRAPHICS, B-Lymphocytes, business.industry, FOXP3, Rhinitis, Allergic, Seasonal, General Medicine, Immunotherapy, medicine.disease, Interleukin-10, ddc, Interleukin 10, 030104 developmental biology, ComputingMethodologies_PATTERNRECOGNITION, Desensitization, Immunologic, Immunology, Biomarker (medicine), Pollen, business, Ex vivo, Regulatory T-cells (Tregs), 030215 immunology

Abstract

Background Allergen-specific immunotherapy (AIT) is a causative treatment in allergic airway disease, comprising long-term allergen administration and requiring three years of treatment. Mechanisms and biomarkers that translate into clinical efficacy remain urgently needed. Methods In an exploratory observational allergy cohort we phenotyped 32 grass-pollen allergic patients with hayfever undergoing AIT for over three years and controls using local and systemic samples for ex vivo FACS, nasal transcriptomes and in vitro phleum-stimulation at critical time windows six hours after therapeutic allergen administration and during peak-season responses. Findings The up-dosing phase is marked by increased IL-10+ B-cells with allergen-specific PD-L1 up-regulation, while effector Th1/Th17 cells and CCR6+IL-17+FoxP3+T-cells decrease. The conversion phase exhibits Th17 recovery in the absence of Th2 cells. The tolerance-mounting phase after three years of treatment is characterized by induction of Tregs while Th2 and phleum-specific Th17 responses decrease. Notably, high ratios of circulating Breg/Th17 following initial AIT correlate significantly with clinical improvement after three years. Interpretation Our exploratory data hypothezise differential shifts in the hierarchy of tolerance in three distinct phases of AIT characterized by conversion of regulatory against pro-inflammatory mechanisms, of which the Breg/Th17 ratio after initial treatment emerges as potential early prediction of AIT efficacy. Fund This study was partially funded by Allergopharma GmbH & Co. KG, intramural funding and the German Center for Lung Research (DZL).

Published

2018

37. Dynamics and epigenetic signature of regulatory T-cells following antiretroviral therapy initiation in acute HIV infection.

Author

Yero A, Shi T, Farnos O, Routy JP, Tremblay C, Durand M, Tsoukas C, Costiniuk CT, and Jenabian MA

Subjects

Adult, Anti-HIV Agents administration & dosage, Anti-HIV Agents therapeutic use, Antigens, CD genetics, Antigens, CD metabolism, Apyrase genetics, Apyrase metabolism, Female, Forkhead Transcription Factors genetics, HIV Infections drug therapy, HIV Infections immunology, Humans, Integrin beta Chains genetics, Integrin beta Chains metabolism, Male, Receptors, CCR genetics, Receptors, CCR metabolism, T-Lymphocytes, Regulatory immunology, Transforming Growth Factor beta genetics, Transforming Growth Factor beta metabolism, Anti-HIV Agents pharmacology, DNA Methylation, Epigenesis, Genetic, HIV Infections genetics, T-Lymphocytes, Regulatory drug effects

Abstract

Background: HIV infection promotes the expansion of immunosuppressive regulatory T-cells (Tregs), contributing to immune dysfunction, tissue fibrosis and disease progression. Early antiretroviral treatment (ART) upon HIV infection improves CD4 count and decreases immune activation. However, Treg dynamics and their epigenetic regulation following early ART initiation remain understudied., Methods: Treg subsets were characterized by flow cytometry in 103 individuals, including untreated HIV-infected participants in acute and chronic phases, ART-treated in early infection, elite controllers (ECs), immunological controllers (ICs), and HIV-uninfected controls. The methylation status of six regulatory regions of the foxp3 gene was assessed using MiSeq technology., Findings: Total Treg frequency increased overtime during HIV infection, which was normalized in early ART recipients. Tregs in untreated individuals expressed higher levels of activation and immunosuppressive markers (CD39, and LAP(TGF-β1)), which remained unchanged following early ART. Expression of gut migration markers (CCR9, Integrin-β7) by Tregs was elevated during untreated HIV infection, while they declined with the duration of ART but not upon early ART initiation. Notably, gut-homing Tregs expressing LAP(TGF-β1) and CD39 remained higher despite early treatment. Additionally, the increase in LAP(TGF-β1) + Tregs overtime were consistent with higher demethylation of conserved non-coding sequence (CNS)-1 in the foxp3 gene. Remarkably, LAP(TGF-β1)-expressing Tregs in ECs were significantly higher than in uninfected subjects, while the markers of Treg activation and gut migration were not different., Interpretation: Early ART initiation was unable to control the levels of immunosuppressive Treg subsets and their gut migration potential, which could ultimately contribute to gut tissue fibrosis and HIV disease progression., Funding: This study was funded by the Canadian Institutes of Health Research (CIHR, grant MOP 142294) and in part by the AIDS and Infectious Diseases Network of the Réseau SIDA et maladies infectieuses du Fonds de recherche du Québec-Santé (FRQ-S)., Competing Interests: Declaration of Competing Interest We have no competing of interest to declare., (Copyright © 2021 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2021

38. Heterogeneous Tumor-Immune Microenvironments between Primary and Metastatic Tumors in a Patient with ALK Rearrangement-Positive Large Cell Neuroendocrine Carcinoma.

Author

Tashiro, Takahiro, Imamura, Kosuke, Tomita, Yusuke, Tamanoi, Daisuke, Takaki, Akira, Sugahara, Kazuaki, Sato, Ryo, Saruwatari, Koichi, Sakata, Shinya, Inaba, Megumi, Ushijima, Sunao, Hirata, Naomi, and Sakagami, Takuro

Subjects

*NEUROENDOCRINE cells, *ANAPLASTIC lymphoma kinase, *CANCER invasiveness, *METASTASIS, *TUMOR growth, *B cells

Abstract

Evolution of tumor-immune microenviroments (TIMEs) occurs during tumor growth and dissemination. Understanding inter-site tumor-immune heterogeneity is essential to harness the immune system for cancer therapy. While the development of immunotherapy against lung cancer with driver mutations and neuroendocrine tumors is ongoing, little is known about the TIME of large cell neuroendocrine carcinoma (LCNEC) or anaplastic lymphoma kinase (ALK) rearrangement-positive lung cancer. We present a case study of a 32-year-old female patient with ALK-rearrangement-positive LCNEC, who had multiple distant metastases including mediastinal lymph-node, bilateral breasts, multiple bones, liver and brain. Multiple biopsy samples obtained from primary lung and three metastatic tumors were analyzed by fluorescent multiplex immunohistochemistry. Tissue localizations of tumor-infiltrating lymphocytes in the tumor nest and surrounding stroma were evaluated. T cell and B cell infiltrations were decreased with distance from primary lung lesion. Although each tumor displayed a unique TIME, all tumors exhibited concomitant regression after treatment with an ALK-inhibitor. This study provides the first evidence of the coexistence of distinct TIME within a single individual with ALK-rearrangement-positive LCNEC. The present study contributes to our understanding of heterogeneous TIMEs between primary and metastatic lesions and provides new insights into the complex interplay between host-immunity and cancer cells in primary and metastatic lesions. [ABSTRACT FROM AUTHOR]

Published

2020

39. T-Cell Hyperactivation and Paralysis in Severe COVID-19 Infection Revealed by Single-Cell Analysis.

Author

Kalfaoglu B, Almeida-Santos J, Tye CA, Satou Y, and Ono M

Subjects

COVID-19 virology, Databases, Genetic, Forkhead Transcription Factors metabolism, Furin metabolism, Humans, Interleukin-2 Receptor alpha Subunit metabolism, RNA-Seq, Receptors, Antigen, T-Cell metabolism, Transcriptome, Virus Internalization, COVID-19 immunology, Lymphocyte Activation immunology, Paralysis immunology, SARS-CoV-2 immunology, Severity of Illness Index, Single-Cell Analysis methods, T-Lymphocytes, Regulatory immunology

Abstract

Severe COVID-19 patients show various immunological abnormalities including T-cell reduction and cytokine release syndrome, which can be fatal and is a major concern of the pandemic. However, it is poorly understood how T-cell dysregulation can contribute to the pathogenesis of severe COVID-19. Here we show single cell-level mechanisms for T-cell dysregulation in severe COVID-19, demonstrating new pathogenetic mechanisms of T-cell activation and differentiation underlying severe COVID-19. By in silico sorting CD4+ T-cells from a single cell RNA-seq dataset, we found that CD4+ T-cells were highly activated and showed unique differentiation pathways in the lung of severe COVID-19 patients. Notably, those T-cells in severe COVID-19 patients highly expressed immunoregulatory receptors and CD25, whilst repressing the expression of FOXP3. Furthermore, we show that CD25 + hyperactivated T-cells differentiate into multiple helper T-cell lineages, showing multifaceted effector T-cells with Th1 and Th2 characteristics. Lastly, we show that CD25-expressing hyperactivated T-cells produce the protease Furin, which facilitates the viral entry of SARS-CoV-2. Collectively, CD4 + T-cells from severe COVID-19 patients are hyperactivated and FOXP3-mediated negative feedback mechanisms are impaired in the lung, which may promote immunopathology. Therefore, our study proposes a new model of T-cell hyperactivation and paralysis that drives immunopathology in severe COVID-19., (Copyright © 2020 Kalfaoglu, Almeida-Santos, Tye, Satou and Ono.)

Published

2020

40. Immunosuppressive Tryptophan Catabolism and Gut Mucosal Dysfunction Following Early HIV Infection

Author

Mohammad-Ali, Jenabian, Mohamed, El-Far, Kishanda, Vyboh, Ido, Kema, Cecilia T, Costiniuk, Rejean, Thomas, Jean-Guy, Baril, Roger, LeBlanc, Cynthia, Kanagaratham, Danuta, Radzioch, Ossama, Allam, Ali, Ahmad, Bertrand, Lebouché, Cécile, Tremblay, Petronela, Ancuta, Jean-Pierre, Routy, Annie, Gosselin, Guided Treatment in Optimal Selected Cancer Patients (GUTS), and Lifestyle Medicine (LM)

Subjects

Adult, microbial translocation, HIV Infections, Inflammation, PERIPHERAL-BLOOD, T-Lymphocytes, Regulatory, DENDRITIC CELLS, 3-dioxygenase-1 (IDO-1), Proinflammatory cytokine, chemistry.chemical_compound, medicine, Humans, Immunology and Allergy, indoleamine 2,3-dioxygenase-1 (IDO-1), tryptophan, Longitudinal Studies, Intestinal Mucosa, Interleukin 6, Kynurenine, Aged, sST2, ACTIVE ANTIRETROVIRAL THERAPY, biology, SERUM I-FABP, Catabolism, regulatory T-cells (Tregs), gut mucosal dysfunction, SIV INFECTION, CELIAC-DISEASE, Middle Aged, HIV early infection, Infectious Diseases, Anti-Retroviral Agents, chemistry, inflammation, MARKER, Immunology, HUMAN-IMMUNODEFICIENCY-VIRUS, biology.protein, T-CELLS, indoleamine 2, Interleukin 18, Tumor necrosis factor alpha, medicine.symptom, Biomarkers, CD8, ART

Abstract

Background. Tryptophan (Trp) catabolism into kynurenine (Kyn) contributes to immune dysfunction in chronic human immunodeficiency virus (HIV) infection. To better define the relationship between Trp catabolism, inflammation, gut mucosal dysfunction, and the role of early antiretroviral therapy (ART), we prospectively assessed patients early after they acquired HIV.Methods. Forty patients in the early phase of infection were longitudinally followed for 12 months after receiving a diagnosis of HIV infection; 24 were untreated, and 16 were receiving ART. Kyn/Trp ratio, regulatory T-cells (Tregs) frequency, T-cell activation, dendritic cell counts, and plasma levels of gut mucosal dysfunction markers intestinal-type fatty acid-binding protein, soluble suppression of tumorigenicity 2, and lipopolysaccharide were assessed.Results. Compared with healthy subjects, patients in the early phase of infection presented with elevated Kyn/Trp ratios, which further increased in untreated patients but normalized in ART recipients. Accordingly, in untreated subjects, the elevated Treg frequency observed at baseline continued to increase over time. The highest CD8+ T-cell activation was observed during the early phase of infection and decreased in untreated patients, whereas activation normalized in ART recipients. The Kyn/Trp ratio was positively associated with CD8+ T-cell activation and levels of inflammatory cytokines (interleukin 6, interferon gamma-inducible protein 10, interleukin 18, and tumor necrosis factor alpha) and negatively associated with dendritic cell frequencies at baseline and in untreated patients. However, ART did not normalize plasma levels of gut mucosal dysfunction markers.Conclusions. Early initiation of ART normalized enhanced Trp catabolism and immune activation but did not improve plasma levels of gut mucosal dysfunction markers.

Published

2015

41. Regulatory T-cells in systemic lupus erythematosus and rheumatoid arthritis

Author

Konstantia-Maria Chavele and Michael R. Ehrenstein

Subjects

SLE, Biophysics, Arthritis, Autoimmunity, chemical and pharmacologic phenomena, Inflammation, medicine.disease_cause, Biochemistry, T-Lymphocytes, Regulatory, Pathogenesis, Arthritis, Rheumatoid, Structural Biology, Genetics, medicine, Animals, Humans, Lupus Erythematosus, Systemic, skin and connective tissue diseases, Molecular Biology, Lupus erythematosus, business.industry, Models, Immunological, Peripheral tolerance, hemic and immune systems, Cell Biology, medicine.disease, Disease Models, Animal, Rheumatoid arthritis, Self Tolerance, Immunology, medicine.symptom, business, RA, Regulatory T-cells (Tregs)

Abstract

Regulatory T-cells (Tregs) are the guardians of peripheral tolerance acting to prevent autoimmune diseases such as systemic lupus erythomatosus (SLE) and rheumatoid arthritis (RA). Defects in Tregs have been reported in these two diseases despite significant differences in their clinical phenotype and pathogenesis. In both diseases the potency of Treg fails to keep pace with the activation of effector cells and are unable to resist the ensuing inflammation. This review will discuss the phenotypic, numeric, and functional abnormalities in Tregs and their role in patients and murine models of SLE and RA.

Published

2011

42. Early IL-10 producing B-cells and coinciding Th/Tr17 shifts during three year grass-pollen AIT.

Author

Zissler UM, Jakwerth CA, Guerth FM, Pechtold L, Aguilar-Pimentel JA, Dietz K, Suttner K, Piontek G, Haller B, Hajdu Z, Schiemann M, Schmidt-Weber CB, and Chaker AM

Subjects

B-Lymphocytes immunology, Cells, Cultured, Humans, Poaceae immunology, B-Lymphocytes metabolism, Desensitization, Immunologic, Interleukin-10 metabolism, Pollen immunology, Rhinitis, Allergic, Seasonal therapy, T-Lymphocytes immunology

Published

2018