Your search keyword '"CD8 T cell"' showing total 984 results

151. Construction and efficacy testing of DNA vaccines containing HLA-A*02:01-restricted SARS-CoV-2 T-cell epitopes predicted by immunoinformatics.

Author

Tan D, Kang N, Zhu Y, Hou J, Wang H, Xu H, Zu C, Gao Z, Liu M, Liu N, Deng Q, Lu H, Liu J, and Xie Y

Subjects

Humans, Animals, Mice, Spike Glycoprotein, Coronavirus immunology, Spike Glycoprotein, Coronavirus genetics, Female, Mice, Inbred BALB C, Immunoinformatics, Epitopes, T-Lymphocyte immunology, SARS-CoV-2 immunology, SARS-CoV-2 genetics, Vaccines, DNA immunology, Vaccines, DNA genetics, HLA-A2 Antigen immunology, HLA-A2 Antigen genetics, COVID-19 immunology, COVID-19 prevention & control, COVID-19 virology, COVID-19 Vaccines immunology, Computational Biology

Abstract

Vaccines play essential roles in the fight against the COVID-19 pandemic. The development and assessment of COVID-19 vaccines have generally focused on the induction and boosting of neutralizing antibodies targeting the SARS-CoV-2 spike (S) protein. Due to rapid and continuous variation in the S protein, such vaccines need to be regularly updated to match newly emerged dominant variants. T-cell vaccines that target MHC I- or II-restricted epitopes in both structural and non-structural viral proteins have the potential to induce broadly cross-protective and long-lasting responses. In this work, the entire proteome encoded by SARS-CoV-2 (Wuhan-hu-1) is subjected to immunoinformatics-based prediction of HLA-A*02:01-restricted epitopes. The immunogenicity of the predicted epitopes is evaluated using peripheral blood mononuclear cells from convalescent Wuhan-hu-1-infected patients. Furthermore, predicted epitopes that are conserved across major SARS-CoV-2 lineages and variants are used to construct DNA vaccines expressing multi-epitope polypeptides. Most importantly, two DNA vaccine constructs induce epitope-specific CD8 + T-cell responses in a mouse model of HLA-A*02:01 restriction and protect immunized mice from challenge with Wuhan-hu-1 virus after hACE2 transduction. These data provide candidate T-cell epitopes useful for the development of T-cell vaccines against SARS-CoV-2 and demonstrate a strategy for quick T-cell vaccine candidate development applicable to other emerging pathogens.

Published

2024

152. Multiplex Screening Assay for Identifying Cytotoxic CD8+ T Cell Epitopes.

Author

Poh, Chek Meng, Zheng, Jian, Channappanavar, Rudragouda, Chang, Zi Wei, Nguyen, Thi H. O., Rénia, Laurent, Kedzierska, Katherine, Perlman, Stanley, and Poon, Leo L. M.

Subjects

CYTOTOXIC T cells, EPITOPES, T cells

Abstract

The cytotoxicity of epitope-specific CD8+ T cells is usually measured indirectly through IFNγ production. Existing assays that directly measure this activity are limited mainly to measurements of up to two specificities in a single reaction. Here, we develop a multiplex cytotoxicity assay that allows direct, simultaneous measurement of up to 23 different specificities of CD8+ T cells in a single reaction. This can greatly reduce the amount of starting clinical materials for a systematic screening of CD8+ T cell epitopes. In addition, this greatly enhanced capacity enables the incorporation of irrelevant epitopes for determining the non-specific killing activity of CD8+ T cells, thereby allowing to measure the actual epitope-specific cytotoxicity activities. This technique is shown to be useful to study both human and mouse CD8+ T cells. Besides, our results from human PBMCs and three independent infectious animal models (MERS, influenza and malaria) further reveal that IFNγ expression by epitope-specific CD8+ T cells does not always correlate with their cell-killing potential, highlighting the need for using cytotoxicity assays in specific contexts (e.g., evaluating vaccine candidates). Overall, our approach opens up new possibilities for comprehensive analyses of CD8+ T cell cytotoxicity in a practical manner. [ABSTRACT FROM AUTHOR]

Published

2020

153. Metabolic Control of Epigenetics and Its Role in CD8+ T Cell Differentiation and Function.

Author

Yerinde, Cansu, Siegmund, Britta, Glauben, Rainer, and Weidinger, Carl

Subjects

T cell differentiation, METABOLIC regulation, CELL physiology, POST-translational modification, EPIGENETICS, T cells, EPIGENOMICS

Abstract

Epigenetic programs that control posttranslational modifications of histone proteins and DNA itself tightly regulate transcriptional networks determining the identity and function of CD8+ T cells. Chromatin-modifying enzymes such as histone acetyltransferases and deacetylases, represent key molecular determinants of the epigenetic imprinting of CD8+ T cells. The functions of these enzymes highly depend on the availability of key products of cellular metabolism pathways such as acetyl-CoA, NAD (Nicotinamide adenine dinucleotide) and SEM (S-adenosylmethionine), suggesting that there is a close crosstalk between the metabolic and the epigenetic regulation of CD8+ T cells. In this review, we will discuss the metabolic regulation of CD8+ T cell epigenetics during activation and differentiation. We will furthermore summarize how metabolic signals from the tumor microenvironment (TME) shape the epigenetic landscape of CD8+ T cells to better understand the mechanism underlying CD8+ T cell exhaustion in anti-tumor and anti-viral immunity, which might help to overcome limitations of current CD8+ T cell-based therapies. [ABSTRACT FROM AUTHOR]

Published

2019

154. Immunization of BLT Humanized Mice Redirects T Cell Responses to Gag and Reduces Acute HIV-1 Viremia.

Author

Claiborne, Daniel T., Dudek, Timothy E., Maldini, Colby R., Power, Karen A., Ghebremichael, Musie, Seung, Edward, Mellors, Elizabeth F., Vrbanac, Vladimir D., Krupp, Katharine, Bisesi, Abigail, Tager, Andrew M., Knipe, David M., Boutwell, Christian L., and Allen, Todd M.

Subjects

*VACCINE effectiveness, *T cells, *HIV infections, *CHEMOTAXIS, *GAG proteins, *IMMUNIZATION, *CHEMOTACTIC factors

Abstract

BLT (bone marrow-liver-thymus) humanized mice, which reconstitute a functional human immune system, develop prototypic human virus-specific CD8+ T cell responses following infection with human immunodeficiency virus type 1 (HIV-1). We explored the utility of the BLT model for HIV-1 vaccine development by immunizing BLT mice against the conserved viral Gag protein, utilizing a rapid prime-boost protocol of poly(lactic-co-glycolic) acid microparticles and a replicationdefective herpes simplex virus (HSV) recombinant vector. After HIV-1 challenge, the mice developed broad, proteome-wide gamma interferon-positive (IFN-γ+) T cell responses against HIV-1 that reached magnitudes equivalent to what is observed in HIV-1-infected individuals. The functionality of these responses was underscored by the consistent emergence of escape mutations in multiple CD8+ T cell epitopes during the course of infection. Although prechallenge vaccine-induced responses were largely undetectable, the Gag immunization increased both the magnitude and the kinetics of anamnestic Gag-specific T cell responses following HIV-1 infection, and the magnitude of these postchallenge Gag-specific responses was inversely correlated with acute HIV-1 viremia. Indeed, Gag immunization was associated with a modest but significant 0.5-log reduction in HIV-1 viral load when analyzed across four experimental groups of BLT mice. Notably, the HSV vector induced elevated plasma concentrations of polarizing cytokines and chemotactic factors, including interleukin-12p70 (IL-12p70) and MIP-1α, which were positively correlated with the magnitude of Gag-specific responses. Overall, these results support the ability of BLT mice to recapitulate human pathogen-specific T cell responses and to respond to immunization; however, additional improvements to the model are required to develop a robust system for testing HIV-1 vaccine efficacy. [ABSTRACT FROM AUTHOR]

Published

2019

155. Fluctuations of Spleen Cytokine and Blood Lactate, Importance of Cellular Immunity in Host Defense Against Blood Stage Malaria Plasmodium yoelii.

Author

Imai, Takashi, Suzue, Kazutomo, Ngo-Thanh, Ha, Ono, Suguri, Orita, Wakako, Suzuki, Haruka, Shimokawa, Chikako, Olia, Alex, Obi, Seiji, Taniguchi, Tomoyo, Ishida, Hidekazu, Van Kaer, Luc, Murata, Shigeo, Tanaka, Keiji, and Hisaeda, Hajime

Subjects

BLOOD lactate, PLASMODIUM yoelii, CELLULAR immunity, ERYTHROCYTES, T cells

Abstract

Our previous studies of protective immunity and pathology against blood stage malaria parasites have shown that not only CD4+ T cells, but also CD8+ T cells and macrophages, are important for host defense against blood stage malaria infection. Furthermore, we found that Plasmodium yoelii 17XNL (PyNL) parasitizes erythroblasts, the red blood cell (RBC) precursor cells, which then express MHC class I molecules. In the present study, we analyzed spleen cytokine production. In CD8+ T cell-depleted mice, IL-10 production in early stage infection was increased over two-fold relative to infected control animals and IL-10+ CD3− cells were increased, whereas IFN-γ production in the late stage of infection was decreased. At day 16 after PyNL infection, CD8+ T cells produced more IFN-γ than CD4+ T cells. We evaluated the involvement of the immunoproteasome in induction of immune CD8+ T cells, and the role of Fas in protection against PyNL both of which are downstream of IFN-γ. In cell transfer experiments, at least the single molecules LMP7, LMP2, and PA28 are not essential for CD8+ T cell induction. The Fas mutant LPR mouse was weaker in resistance to PyNL infection than WT mice, and 20% of the animals died. LPR-derived parasitized erythroid cells exhibited less externalization of phosphatidylserine (PS), and phagocytosis by macrophages was impaired. Furthermore, we tried to identify the cause of death in malaria infection. Blood lactate concentration was increased in the CD8+ T cell-depleted PyNL-infected group at day 19 (around peak parasitemia) to similar levels as day 7 after infection with a lethal strain of Py. When we injected mice with lactate at day 4 and 6 of PyNL infection, all mice died at day 8 despite demonstrating low parasitemia, suggesting that hyperlactatemia is one of the causes of death in CD8+ T cell-depleted PyNL-infected mice. We conclude that CD8+ T cells might control cytokine production to some extent and regulate hyperparasitemia and hyperlactatemia in protection against blood stage malaria parasites. [ABSTRACT FROM AUTHOR]

Published

2019

156. Human T Cell Response to Dengue Virus Infection.

Author

Tian, Yuan, Grifoni, Alba, Sette, Alessandro, and Weiskopf, Daniela

Subjects

DENGUE hemorrhagic fever, DENGUE viruses, VIRUS diseases, HUMAN T cells, T cells, CELL populations

Abstract

DENV is a major public health problem worldwide, thus underlining the overall significance of the proposed Program. The four dengue virus (DENV) serotypes (1–4) cause the most common mosquito-borne viral disease of humans, with 3 billion people at risk for infection and up to 100 million cases each year, most often affecting children. The protective role of T cells during viral infection is well-established. Generally, CD8 T cells can control viral infection through several mechanisms, including direct cytotoxicity, and production of pro-inflammatory cytokines such as IFN-γ and TNF-α. Similarly, CD4 T cells are thought to control viral infection through multiple mechanisms, including enhancement of B and CD8 T cell responses, production of inflammatory and anti-viral cytokines, cytotoxicity, and promotion of memory responses. To probe the phenotype of virus-specific T cells, epitopes derived from viral sequences need to be known. Here we discuss the identification of CD4 and CD8 T cell epitopes derived from DENV and how these epitopes have been used by researchers to interrogate the phenotype and function of DENV-specific T cell populations. [ABSTRACT FROM AUTHOR]

Published

2019

157. Similar but different: virtual memory CD8 T cells as a memory‐like cell population.

Author

Hussain, Tabinda and Quinn, Kylie M

Subjects

*CELL populations, *T cells, *IMMUNOLOGIC memory, *CELL cycle, *MEMORY

Abstract

Immunological memory is a phenomenon where the immune system can respond more rapidly to pathogens and immunological challenges that it has previously encountered. It is defined by several key hallmarks. After an initial encounter, immune cells (1) expand and (2) differentiate to form memory cell populations. Memory cells are (3) long‐lived and (4) facilitate more rapid immune responses to subsequent infection because of (i) an increase in cell number, (ii) a decrease in the signaling threshold required for entry into cell cycle or effector function and (iii) localization of cells to tissue sites for surveillance. Classically, immunological memory has been antigen specific but it is becoming apparent that mechanisms of immunological memory can be co‐opted by innate or antigen‐inexperienced immune cells to generate heterogeneity in immune responses. One such cell is the virtual memory CD8 T (TVM) cell, which is a semi‐differentiated but antigen‐naïve CD8 T‐cell population. This review will summarize current knowledge of how TVM cells are generated, their memory‐like hallmarks, how they are maintained during steady state, infection and aging, and propose a model to integrate key signaling pathways during their generation. [ABSTRACT FROM AUTHOR]

Published

2019

158. The hallmarks of CMV-specific CD8 T-cell differentiation.

Author

van den Berg, Sara P. H., Pardieck, Iris N., Lanfermeijer, Josien, Sauce, Delphine, Klenerman, Paul, van Baarle, Debbie, and Arens, Ramon

Subjects

*T cells, *ANTIBODY-dependent cell cytotoxicity, *TRANSCRIPTION factors, *LYMPHOCYTES

Abstract

Upon cytomegalovirus (CMV) infection, large T-cell responses are elicited that remain high or even increase over time, a phenomenon named memory T-cell inflation. Besides, the maintained robust T-cell response, CMV-specific T cells seem to have a distinctive phenotype, characterized by an advanced differentiation state. Here, we will review this "special" differentiation status by discussing the cellular phenotype based on the expression of CD45 isoforms, costimulatory, inhibitory and natural killer receptors, adhesion and lymphocyte homing molecules, transcription factors, cytokines and cytotoxic molecules. In addition, we focus on whether the differentiation state of CMV-specific CD8 T cells is unique in comparison with other chronic viruses and we will discuss the possible impact of factors such as antigen exposure and aging on the advanced differentiation status of CMV-specific CD8 T cells. [ABSTRACT FROM AUTHOR]

Published

2019

159. Cytomegalovirus memory inflation and immune protection.

Author

Cicin-Sain, Luka

Subjects

*HUMAN cytomegalovirus, *CYTOMEGALOVIRUSES, *IMMUNOLOGIC memory, *VIRAL antigens, *EPITOPES, *IMMUNOCOMPROMISED patients, *HAPLOTYPES

Abstract

Cytomegalovirus (CMV) infection induces powerful and sustained T-cell responses against a few selected immunodominant antigenic epitopes. This immune response was named memory inflation, because it does not contract in the long term, and may even expand over months and years of virus latency. It is by now understood that memory inflation does not occur at the expense of the naïve T-cell pool, but rather as a competitive selection process within the effector pool, where viral antigens with higher avidity of TCR binding and with earlier expression patterns outcompete those that are expressed later and bind TCRs less efficiently. It is also understood that inflationary epitopes require processing by the constitutive proteasome in non-hematopoietic cells, and this likely implies that memory inflation is fuelled by direct low-level antigenic expression in latently infected cells. This review proposes that these conditions make inflationary epitopes the optimal candidates for adoptive immunotherapy of CMV disease in the immunocompromised host. At present, functional target CMV epitopes have been defined only for the most common HLA haplotypes. Mapping the uncharacterized inflationary epitopes in less frequent HLAs may, thus, be a strategy for the identification of optimal immunotherapeutic targets in patients with uncommon haplotypes. [ABSTRACT FROM AUTHOR]

Published

2019

160. Fuel and brake of memory T cell inflation.

Author

Welten, Suzanne P. M., Baumann, Nicolas S., and Oxenius, Annette

Subjects

*T cells, *VIRUS diseases, *CYTOMEGALOVIRUS diseases, *MEMORY, *VACCINE effectiveness, *FUEL

Abstract

Memory T cell inflation is a process in which a large number of effector memory T cells accumulates in peripheral tissues. This phenomenon is observed upon certain low level persistent virus infections, but it is most commonly described upon infection with the β-herpesvirus Cytomegalovirus. Due to the induction of this large pool of functional effector CD8 T cells in peripheral tissues, the interest in using CMV-based vaccine vectors for vaccination purposes is rising. However, the exact mechanisms of memory T cell inflation are not yet fully understood. It is clear that repetitive exposure to antigen is a key determinant for memory inflation, and therefore the viral inoculum dose and the subsequent number of viral reactivation events strongly impact on the magnitude of the inflationary T cell pool. In addition, the number of CMV-specific CD8 T cells that is able to sense these reactivation events affects the size of the inflationary T cell pool. In the following, we will discuss factors that either promote or limit T cell inflation from both the virus and host perspective. These factors mostly operate by influencing the amount of available antigen or by affecting the T cell pool that is able to respond to the antigen. Furthermore, we will discuss the recent use of CMV-based vaccines in pre-clinical experimental settings, where these vectors have shown promising results by inducing prolonged effector memory T cell responses to foreign-introduced epitopes and thereby provided protection from subsequent virus or tumour challenges. [ABSTRACT FROM AUTHOR]

Published

2019

161. Comparative analysis of CDR3 regions in paired human αβ CD8 T cells.

Author

Yu, Kun, Shi, Ji, Lu, Dan, and Yang, Qiong

Subjects

T cell receptors, T cells, CYTOTOXIC T cells, HUMAN T cells, COMPARATIVE studies

Abstract

The majority of human CD8 cytotoxic T lymphocytes express αβ T‐cell receptors that recognize peptide–MHC class I complexes. Considerable attention has been devoted to TCR β repertoires, but study of TCR α chains has been limited. To gain a better understanding of the features of CDR3α and CDR3β in paired samples, we comprehensively analyzed 776 unique paired αβ TCR CDR3 regions in this study. We found that (I) the CDR3 length among paired αβ TCRs had a fairly narrow distribution due to random assortment of CDR3 length in alpha and beta chains; (II) nucleotide deletions among CDR3 regions were positively correlated with insertions in both α and β TCRs; (III) the CDR3 loops of both α and β chains contained an abundance of charged/polar residues and the CDR3 base regions contained a conserved motif; and (IV) the occurrence of Gly was CDR3 length‐ and position‐dependent in both chains, whereas the frequency of Ser at positions 106 and 107 was positively correlated with CDR3 length in TCR β. Overall, the amino acids in CDR3 loop regions were significantly different between TCR α and β, which suggests a distinct role for each chain in the recognition of antigen–MHC complexes. Here, we have provided detailed information on CDR3 in paired TCRs expressed on human CD8+ T cells and established the basis of a reference set for αβ TCR repertoires in healthy humans. [ABSTRACT FROM AUTHOR]

Published

2019

162. Dynamic Metabolic State of Tissue Resident CD8 T Cells.

Author

Konjar, Špela and Veldhoen, Marc

Subjects

T cells, CYTOLOGY, CELL death, EPITHELIAL cells, OXIDATIVE phosphorylation

Abstract

In the past years, there have been significant advances in the understanding of how environmental conditions alone or in conjunction with pathogen invasion affect the metabolism of T cells, thereby influencing their activation, differentiation, and longevity. Detailed insights of the interlinked processes of activation and metabolism can contribute to major advances in immunotherapies. Naive and memory T cells circulate the body. In a quiescent state with low metabolic demands, they predominantly use oxidative phosphorylation for their energy needs. Recognition of cognate antigen combined with costimulatory signals results in a proliferative burst and effector molecule production, requiring rapid release of energy, achieved via dynamically reprogramming metabolic pathways. After activation, most T cells succumb to activation induced cell death, but few differentiate into memory T cells. Of note, some memory T cells permanently occupy tissues without circulating. These, tissue resident T cells are predominantly CD8 T cells, maintained in a metabolic state distinct from naïve and circulating memory CD8 T cells with elements similar to effector CD8 T cells but without undergoing proliferative burst or secreting immune mediators. They continually interact with tissue cells as part of an immune surveillance network, are well-adapted to the tissues they have made their home and where they may encounter different metabolic environments. In this review, we will discuss recent insights in metabolic characteristics of CD8 T cell biology, with emphasis on tissue resident CD8 T cells at the epithelial barriers. [ABSTRACT FROM AUTHOR]

Published

2019

163. Direct CD137 costimulation of CD8 T cells promotes retention and innatelike function within nascent atherogenic foci.

Author

Xu, Maria M., Ménoret, Antoine, Nicholas, Sarah-Anne E., Günther, Sebastian, Sundberg, Eric J., Beiyan Zhou, Rodriguez, Annabelle, Murphy, Patrick A., and Vella, Anthony T.

Subjects

*T cells, *CAROTID artery, *ATHEROSCLEROTIC plaque, *VIRUS diseases, *FLOW cytometry

Abstract

Effector CD8 T cells infiltrate atherosclerotic lesions and are correlated with cardiovascular events, but the mechanisms regulating their recruitment and retention are not well understood. CD137 (4-1BB) is a costimulatory receptor induced on immune cells and expressed at sites of human atherosclerotic plaque. Genetic variants associated with decreased CD137 expression correlate with carotid-intimal thickness and its deficiency in animal models attenuates atherosclerosis. These effects have been attributed in part to endothelial responses to low and disturbed flow (LDF), but CD137 also generates robust effector CD8 T cells as a costimulatory signal. Thus, we asked whether CD8 T cell-specific CD137 stimulation contributes to their infiltration, retention, and IFNγ production in early atherogenesis. We tested this through adoptive transfer of CD8 T cells into recipient C57BL/6J mice that were then antigen primed and CD137 costimulated. We analyzed atherogenic LDF vessels in normolipidemic and PCSK9-mediated hyperlipidemic models and utilized a digestion protocol that allowed for lesional T-cell characterization via flow cytometry and in vitro stimulation. We found that CD137 activation, specifically of effector CD8 T cells, triggers their intimal infiltration into LDF vessels and promotes a persistent innatelike proinflammatory program. Residence of CD137+ effector CD8 T cells further promoted infiltration of endogenous CD8 T cells with IFNγ-producing potential, whereas CD137-deficient CD8 T cells exhibited impaired vessel infiltration, minimal IFNγ production, and reduced infiltration of endogenous CD8 T cells. Our studies thus provide novel insight into how CD137 costimulation of effector T cells, independent of plaque-antigen recognition, instigates their retention and promotes innate-like responses from immune infiltrates within atherogenic foci. NEW & NOTEWORTHY Our studies identify CD137 costimulation as a stimulus for effector CD8 T-cell infiltration and persistence within atherogenic foci, regardless of atherosclerotic-antigen recognition. These costimulated effector cells, which are generated in pathological states such as viral infection and autoimmunity, have innate-like proinflammatory programs in circulation and within the atherosclerotic microenvironment, providing mechanistic context for clinical correlations of cardiovascular morbidity with increased CD8 T-cell infiltration and markers of activation in the absence of established antigen specificity. [ABSTRACT FROM AUTHOR]

Published

2019

164. CD8+ T cell exhaustion.

Author

Kurachi, Makoto

Subjects

*T cell receptors, *T cells, *CELL populations, *CELL physiology, *INTRACELLULAR pathogens

Abstract

CD8+ T cells are important for the protective immunity against intracellular pathogens and tumor. In the case of chronic infection or cancer, CD8+ T cells are exposed to persistent antigen and/or inflammatory signals. This excessive amount of signals often leads CD8+ T cells to gradual deterioration of T cell function, a state called "exhaustion." Exhausted T cells are characterized by progressive loss of effector functions (cytokine production and killing function), expression of multiple inhibitory receptors (such as PD-1 and LAG3), dysregulated metabolism, poor memory recall response, and homeostatic proliferation. These altered functions are closely related with altered transcriptional program and epigenetic landscape that clearly distinguish exhausted T cells from normal effector and memory T cells. T cell exhaustion is often associated with inefficient control of persisting infections and cancers, but re-invigoration of exhausted T cells with inhibitory receptor blockade can promote improved immunity and disease outcome. Accumulating evidences support the therapeutic potential of targeting exhausted T cells. However, exhausted T cells comprise heterogenous cell population with distinct responsiveness to intervention. Understanding molecular mechanism of T cell exhaustion is essential to establish rational immunotherapeutic interventions. [ABSTRACT FROM AUTHOR]

Published

2019

165. Harnessing CD8+ T Cells Under HIV Antiretroviral Therapy

Author

Joanna A. Warren, Genevieve Clutton, and Nilu Goonetilleke

Subjects

HIV, CD8 T cell, antiretroviral therapy (ART), HIV cure strategies, aging, immunosenescence, Immunologic diseases. Allergy, RC581-607

Abstract

Antiretroviral therapy (ART) has transformed HIV from a fatal disease to a chronic condition. In recent years there has been considerable interest in strategies to enable HIV-infected individuals to cease ART without viral rebound, either by purging all cells infected harboring replication-competent virus (HIV eradication), or by boosting immune responses to allow durable suppression of virus without rebound (HIV remission). Both of these approaches may need to harness HIV-specific CD8+ T cells to eliminate infected cells and/or prevent viral spread. In untreated infection, both HIV-specific and total CD8+ T cells are dysfunctional. Here, we review our current understanding of both global and HIV-specific CD8+ T cell immunity in HIV-infected individuals with durably suppressed viral load under ART, and its implications for HIV cure, eradication or remission. Overall, the literature indicates significant normalization of global T cell parameters, including CD4/8 ratio, activation status, and telomere length. Global characteristics of CD8+ T cells from HIV+ART+ individuals align more closely with those of HIV-seronegative individuals than of viremic HIV-infected individuals. However, markers of senescence remain elevated, leading to the hypothesis that immune aging is accelerated in HIV-infected individuals on ART. This phenomenon could have implications for attempts to prime de novo, or boost existing HIV-specific CD8+ T cell responses. A major challenge for both HIV cure and remission strategies is to elicit HIV-specific CD8+ T cell responses superior to that elicited by natural infection in terms of response kinetics, magnitude, breadth, viral suppressive capacity, and tissue localization. Addressing these issues will be critical to the success of HIV cure and remission attempts.

Published

2019

166. The Transcription Factor TCF1 Preserves the Effector Function of Exhausted CD8 T Cells During Chronic Viral Infection

Author

Yifei Wang, Jianjun Hu, Yiding Li, Minglu Xiao, Haoqiang Wang, Qin Tian, Zhirong Li, Jianfang Tang, Li Hu, Yan Tan, Xinyuan Zhou, Ran He, Yuzhang Wu, Lilin Ye, Zhinan Yin, Qizhao Huang, and Lifan Xu

Subjects

TCF1, CD8 T cell, exhaustion, LCMV, chronic viral infection, Immunologic diseases. Allergy, RC581-607

Abstract

The long-term persistence of viral antigens drives virus-specific CD8 T cell exhaustion during chronic viral infection. Yet exhausted, CD8 T cells are still endowed with certain levels of effector function, by which they can keep viral replication in check in chronic infection. However, the regulatory factors involved in regulating the effector function of exhausted CD8 T cell are largely unknown. Using mouse model of chronic LCMV infection, we found that the deletion of transcription factor TCF-1 in LCMV-specific exhausted CD8 T cells led to the profound reduction in cytokine production and degranulation. Conversely, ectopic expression of TCF-1 or using agonist to activate TCF-1 activities promotes the effector function of exhausted CD8 T cells. Mechanistically, TCF-1 fuels the functionalities of exhausted CD8 T cells by promoting the expression of an array of key effector function-associated transcription regulators, including Foxo1, Zeb2, Id3, and Eomes. These results collectively indicate that targeting TCF-1 mediated transcriptional pathway may represent a promising immunotherapy strategy against chronic viral infections by reinvigorating the effector function of exhausted virus-specific CD8 T cells.

Published

2019

167. Transcriptional and Epigenetic Regulation of Effector and Memory CD8 T Cell Differentiation

Author

Yao Chen, Ryan Zander, Achia Khatun, David M. Schauder, and Weiguo Cui

Subjects

CD8 T cell, memory differentiation, cell fate decision, transcriptional, epigenetic, single cell sequencing, Immunologic diseases. Allergy, RC581-607

Abstract

Immune protection and lasting memory are accomplished through the generation of phenotypically and functionally distinct CD8 T cell subsets. Understanding how these effector and memory T cells are formed is the first step in eventually manipulating the immune system for therapeutic benefit. In this review, we will summarize the current understanding of CD8 T cell differentiation upon acute infection, with a focus on the transcriptional and epigenetic regulation of cell fate decision and memory formation. Moreover, we will highlight the importance of high throughput sequencing approaches and single cell technologies in providing insight into genome-wide investigations and the heterogeneity of individual CD8 T cells.

Published

2018

168. Defining Memory CD8 T Cell

Author

Matthew D. Martin and Vladimir P. Badovinac

Subjects

CD8 T cell, memory, subsets, heterogeneity, protection, outbred mice, Immunologic diseases. Allergy, RC581-607

Abstract

CD8 T cells comprising the memory pool display considerable heterogeneity, with individual cells differing in phenotype and function. This review will focus on our current understanding of heterogeneity within the antigen-specific memory CD8 T cell compartment and classifications of memory CD8 T cell subsets with defined and discrete functionalities. Recent data suggest that phenotype and/or function of numerically stable circulatory memory CD8 T cells are defined by the age of memory CD8 T cell (or time after initial antigen-encounter). In addition, history of antigen stimulations has a profound effect on memory CD8 T cell populations, suggesting that repeated infections (or vaccination) have the capacity to further shape the memory CD8 T cell pool. Finally, genetic background of hosts and history of exposure to diverse microorganisms likely contribute to the observed heterogeneity in the memory CD8 T cell compartment. Extending our tool box and exploring alternative mouse models (i.e., “dirty” and/or outbred mice) to encompass and better model diversity observed in humans will remain an important goal for the near future that will likely shed new light into the mechanisms that govern biology of memory CD8 T cells.

Published

2018

169. Cheating the Hunger Games; Mechanisms Controlling Clonal Diversity of CD8 Effector and Memory Populations

Author

Inga Kavazović, Bojan Polić, and Felix M. Wensveen

Subjects

immunity, CD8 T cell, affinity, memory, T cell receptor, differentiation, Immunologic diseases. Allergy, RC581-607

Abstract

Effector and memory CD8 T cells have an intrinsic difference in the way they must approach antigen; effector cells need to address the pathogen at hand and therefore favor outgrowth of only high-affinity clones. In contrast, the memory pool benefits from greater clonal diversity to recognize and eliminate pathogens with mutations in their immunogenic epitopes. Effector and memory fates are ultimately the result of the same three signals that control T cell activation; T cell receptor (TCR) engagement together with co-stimulation and cytokines. Great progress has been made in our understanding of the transcriptional programs that drive effector or memory differentiation. However, how these two different programs result from the same initial cues is still a matter of debate. An emerging image is that not only the classical three signals determine T cell differentiation, but also the ability of cells to access these signals relative to that of other activated clones. Inter-clonal competition is therefore not only a selective force, but also a mediator of CD8 T cell fate. How this is regulated on a transcriptional level, especially in the context of a selective “hunger game” based on antigen-affinity in which only cells of high-affinity are supposed to survive, is still poorly defined. In this review, we discuss recent literature that illustrates how antigen-affinity dependent inter-clonal competition shapes effector and memory populations in an environment of antigen affinity-driven selection. We argue that fine-tuning of TCR signal intensity presents an attractive target for regulating the scope of CD8 T cell vaccines.

Published

2018

170. A Subset of CXCR5+CD8+ T Cells in the Germinal Centers From Human Tonsils and Lymph Nodes Help B Cells Produce Immunoglobulins

Author

Juan Shen, Xi Luo, Qiongli Wu, Jun Huang, Guanying Xiao, Liantang Wang, Binyan Yang, Huabin Li, and Changyou Wu

Subjects

CD8 T cell, C-X-C chemokine receptor type 5, Follicular, B cell, Tfh-like cell, Immunologic diseases. Allergy, RC581-607

Abstract

Recent studies indicated that CXCR5+CD8+ T cells in lymph nodes could eradicate virus-infected target cells. However, in the current study we found that a subset of CXCR5+CD8+ T cells in the germinal centers from human tonsils or lymph nodes are predominately memory cells that express CD45RO and CD27. The involvement of CXCR5+CD8+ T cells in humoral immune responses is suggested by their localization in B cell follicles and by the concomitant expression of costimulatory molecules, including CD40L and ICOS after activation. In addition, CXCR5+CD8+ memory T cells produced significantly higher levels of IL-21, IFN-γ, and IL-4 at mRNA and protein levels compared to CXCR5−CD8+ memory T cells, but IL-21-expressing CXCR5+CD8+ T cells did not express Granzyme B and perforin. When cocultured with sorted B cells, sorted CXCR5+CD8+ T cells promoted the production of antibodies compared to sorted CXCR5−CD8+ T cells. However, fixed CD8+ T cells failed to help B cells and the neutralyzing antibodies against IL-21 or CD40L inhibited the promoting effects of sorted CXCR5+CD8+ T cells on B cells for the production of antibodies. Finally, we found that in the germinal centers of lymph nodes from HIV-infected patients contained more CXCR5+CD8+ T cells compared to normal lymph nodes. Due to their versatile functional capacities, CXCR5+CD8+ T cells are promising candidate cells for immune therapies, particularly when CD4+ T cell help are limited.

Published

2018

171. PD-1 Expression on Mycobacterium tuberculosis-Specific CD4 T Cells Is Associated With Bacterial Load in Human Tuberculosis

Author

Cheryl L. Day, Deborah A. Abrahams, Rubina Bunjun, Lynnett Stone, Marwou de Kock, Gerhard Walzl, Robert J. Wilkinson, Wendy A. Burgers, and Willem A. Hanekom

Subjects

CD4 T cell, CD8 T cell, tuberculosis, PD-1, IFN-γ, proliferation, Immunologic diseases. Allergy, RC581-607

Abstract

Persistent antigen stimulation in chronic infections has been associated with antigen-specific T cell dysfunction and upregulation of inhibitory receptors, including programmed cell death protein 1 (PD-1). Pulmonary tuberculosis (TB) disease is characterized by high levels of Mycobacterium tuberculosis (Mtb), yet the relationship between bacterial load, PD-1 expression, and Mtb-specific T cell function in human TB has not been well-defined. Using peripheral blood samples from adults with LTBI and with pulmonary TB disease, we tested the hypothesis that PD-1 expression is associated with bacterial load and functional capacity of Mtb-specific T cell responses. We found that PD-1 was expressed at significantly higher levels on Th1 cytokine-producing Mtb-specific CD4 T cells from patients with smear-positive TB, compared with smear-negative TB and LTBI, which decreased after completion of anti-TB treatment. By contrast, expression of PD-1 on Mtb-specific CD8 T cells was significantly lower than on Mtb-specific CD4 T cells and did not differ by Mtb infection and disease status. In vitro stimulation of PBMC with Mtb antigens demonstrated that PD-1 is induced on proliferating Mtb-specific CD4 T cells and that Th1 cytokine production capacity is preferentially maintained within PD-1+ proliferating CD4 T cells, compared with proliferating Mtb-specific CD4 T cells that lack PD-1 expression. Together, these data indicate that expression of PD-1 on Mtb-specific CD4 T cells is indicative of mycobacterial antigen exposure and identifies a population of effector cells with Th1 cytokine production capacity. These studies provide novel insights into the role of the PD-1 pathway in regulating CD4 and CD8 T cell responses in Mtb infection and provide rationale for future studies to evaluate PD-1 expression on antigen-specific CD4 T cells as a potential biomarker for bacterial load and treatment response in human TB.

Published

2018

172. The CD8 T Cell Response to Respiratory Virus Infections

Author

Megan E. Schmidt and Steven M. Varga

Subjects

CD8 T cell, memory T cell, respiratory virus, respiratory syncytial virus, influenza A virus, human metapneumovirus, Immunologic diseases. Allergy, RC581-607

Abstract

Humans are highly susceptible to infection with respiratory viruses including respiratory syncytial virus (RSV), influenza virus, human metapneumovirus, rhinovirus, coronavirus, and parainfluenza virus. While some viruses simply cause symptoms of the common cold, many respiratory viruses induce severe bronchiolitis, pneumonia, and even death following infection. Despite the immense clinical burden, the majority of the most common pulmonary viruses lack long-lasting efficacious vaccines. Nearly all current vaccination strategies are designed to elicit broadly neutralizing antibodies, which prevent severe disease following a subsequent infection. However, the mucosal antibody response to many respiratory viruses is not long-lasting and declines with age. CD8 T cells are critical for mediating clearance following many acute viral infections in the lung. In addition, memory CD8 T cells are capable of providing protection against secondary infections. Therefore, the combined induction of virus-specific CD8 T cells and antibodies may provide optimal protective immunity. Herein, we review the current literature on CD8 T cell responses induced by respiratory virus infections. Additionally, we explore how this knowledge could be utilized in the development of future vaccines against respiratory viruses, with a special emphasis on RSV vaccination.

Published

2018

173. Decisions on the Road to Memory

Author

Amsen, Derk, Backer, Ronald A., Helbig, Christina, Katsikis, Peter D., editor, Schoenberger, Stephen P., editor, and Pulendran, Bali, editor

Published

2013

174. Role of tumor-intrinsic calcineurin in shaping the tumor microenvironment and regulating the cytotoxic T cell response

Author

VALACHE, MIHAI, Valache, M, and GRANUCCI, FRANCESCA

Subjects

NFAT, CD8 T cell, Cellule T CD8, Calcineurin, MED/04 - PATOLOGIA GENERALE, Tumori freddi, Immunoterapia, Immunotherapy, Calcineurina, Cold tumor

Abstract

La calcineurina (Cn) è una Serina/Treonina-fosfatasi responsabile della defosforilazione di una numerosa serie di substrati tra cui il fattore trascrizionale NFAT. L’asse calcineurina-NFAT è noto essere in grado di regolare molteplici processi tumorigenici quali proliferazione, sopravvivenza, transizione epitelio-mesenchimale e metastatizzazione e pertanto si presenta come ottimo bersaglio per lo studio dei meccanismi di tumorigenesi. In particolare, è stato studiato il ruolo dell’asse calcineurina-NFAT nei tumori “freddi”, in quanto refrattari alle immunoterapie moderne. Pertanto bersagliare questo asse potrebbe offrire nuove opportunità terapeutiche. Per gli studi sono state utilizzate delle linee cellulari tumorali murine geneticamente modificate per avere un blocco costitutivo dell’interazione tra calcineurina ed NFAT. L’inibizione farmacologica dell’attività enzimatica della calcineurina con farmaci quali Ciclosporina A e Tacrolimus è noto causare un effetto citostatico. È stato dunque verificato che il blocco dell’interazione calcineurina-NFAT non impattasse la crescita ed il ciclo cellulare, che avrebbe potuto introdurre un ulteriore bias nel modello. Per verificare gli effetti globali di questo blocco dell’interazione Cn-NFAT sullo stato delle cellule coltivate in 2D ed in 3D è stato effettuato un sequenziamento degli RNA in bulk. Dall’analisi dei dati sono emerse come alterate diverse vie di segnalazione cellulare, a seconda delle condizioni di coltura, ed in particolare la via della transizione epitelio-mesenchimale, le vie infiammatorie e le vie coinvolte nella fosforilazione ossidativa. Essendo noto il ruolo di NFAT nella regolazione del microambiente tumorale, sono stati anche indagati gli effetti dell’inibizione dell’asse Cn-NFAT in vivo, in modelli murini di tumori sottocutanei. Sorprendentemente, è stato osservato un aumento dell’infiltrato intratumorale di cellule T CD8+. Un’ulteriore analisi dei dati di sequenziamento dell’RNA ha evidenziato come i tumori in cui l’asse Cn-NFAT è inibito presentano una maggiore produzione di citochine e chemochine con funzione chemoattraente per le cellule T CD8+. Questo aumento è stato ulteriormente confermato anche in vitro tramite qRT-PCR. Inoltre, l’inibizione di queste citochine in vivo ha annullato l’incremento nel reclutamento delle cellule T CD8+ nei tumori in cui manca l’interazione Cn-NFAT. Il ruolo antitumorale delle cellule CD8+ è ampiamente noto. Nel nostro modello tuttavia il semplice reclutamento di queste cellule non ha determinato cambiamenti nella crescita. Per chiarire meglio questo aspetto è stato indagato lo stato di esaurimento di queste cellule. È stato pertanto osservato che i tumori in cui l’asse Cn-NFAT è inibito presentano un maggior numero di cellule T CD8+ esaurite definite “progenitor exhausted”, che possono dunque essere riattivate tramite immunoterapia. Pertanto la somministrazione di un inibitore degli immunocheckpoint è risultata in una diminuzione notevole della crescita tumorale. Per corroborare questi risultati nell’uomo sono stati analizzati dei dati pubblici di trascrittomica, che hanno evidenziato una correlazione positiva tra l’espressione di fattori chemotattici per le cellule T CD8+ e la sopravvivenza dei pazienti. Insieme questi risultati indicano che l’inibizione intratumorale dell’asse calcineurina-NFAT può rappresentare una nuova strategia terapeutica che può affiancare in maniera sinergica le attuali immunoterapie. Calcineurin is a serine-threonine phosphatase that can dephosphorylate a large number of substrates, among which there is the transcription factor NFAT. My research activity has focused on investigating the role of calcineurin (Cn) in “cold” tumors, and in particular the role of the Cn-NFAT axis. This axis is known to play various protumorigenic roles in tumors and its modulation could prove beneficial towards the development of novel therapies, since cold tumors are notoriously refractory to immunotherapy. We employed genetically engineered tumor cell lines to study the impact of a constitutive inhibition of the Cn-NFAT interaction both in vitro and in vivo. We investigated the impact that this inhibition has in vitro by confirming that there is no cytostatic effect that could confound ulterior results and no alterations in the cell cycle. We also confirmed that growth wasn’t altered in vivo. We performed an RNA sequencing on cells cultivated both in 2D and in 3d in order to determine the global expression variations that this inhibition induced in our cell line models. Based on the data analysis we identified several pathways that were altered based on the specific cultivation techniques we used. From this we could infer that the Cn-NFAT axis plays a role in several cell processes such as epithelial-to-mesenchymal transition and also oxidative phosphorylation. Since NFAT is known to contribute to the tumor microenvironment, we investigated whether there are any alterations in the immune infiltrate in vivo. Surprisingly we found that in our model there was an enhanced recruitment of CD8+ T cells. Further analysis of the RNAseq data revealed that the impairment of the Cn-NFAT axis induced an increased production of T cell chemotactic factors such as cytokines and chemokines. Indeed, the inhibition of these pathways in vivo abrogated the T cell recruitment. We then sought to understand why this increase in the CD8+ T cell infiltrate did not result in alterations in cancer growth and hypothesized that the tumors employ active strategies of immunosuppression. We therefore analyzed the exhaustion state of the infiltrating T cells and observed an increase in the “progenitor exhausted” populations, suggesting that their activation status can be modulated by immunotherapy. Indeed, the administration of an immune checkpoint blockade greatly diminished tumor growth. To corroborate these data in humans, we analyzed publicly available databases of transcriptomic data and indeed found a correlation between the expression of T cell chemotactic factors and patient survival. Overall, our data suggest that the inhibition of the Cn-NFAT axis can enhance existing immunotherapies.

Published

2023

175. Host Factors That Influence Coxsackievirus B3 Replication and Pathogenensis

Author

Dhalech, Adeeba Haroon

Subjects

CD8 T cell, Testosterone, Gut bacteria, Sex difference, Coxsackievirus B3

Abstract

Indiana University-Purdue University Indianapolis (IUPUI), Enteric viruses are infectious human pathogens that initiate infection in the gastrointestinal tract. They follow a fecal-oral route of transmission and are spread by contamination of food, water, or contact between individuals. Furthermore, enteric viruses also cause significant morbidity, mortality, and economic burdens yearly. Coxsackievirus (CV) is commonly isolated among enteric viruses and is an etiological agent of hand, foot, and mouth disease, hemorrhagic conjunctivitis, and myocarditis. The virus predominantly infects infants and young children and accounts for 11% of the fatality rate in neonates. Despite CV’s impact on human health, there are no treatments or vaccines for CV infections. Using a mouse model to study a key CV, Coxsackievirus B3 (CVB3), our laboratory has found two critical factors that impact CVB3 replication and pathogenesis. First, we have demonstrated that intestinal bacteria enhance intestinal CVB3 replication. We found that certain specific bacteria (Salmonella enterica) and its cell wall components, like lipopolysaccharides (LPS), enhanced CVB3 stability and infectivity in vitro. Additionally, we found that particular constituents of LPS are required for stability to occur. These data suggest that specific bacteria may be integral in maintaining CVB3 infectivity in the intestine. Besides virus-microbiome interaction, CVB3 is also impacted by sex hormones. Using castrated mice models, we observed a sex bias to CVB3 infection, with male mice succumbing to CVB3-induced disease at an increased rate compared to female mice. Our data suggest that testosterone, a predominant male sex hormone, enhanced CVB3 intestinal replication and viral dissemination to organs in male and female mice, but lethality only in male mice. Moreover, testosterone also affected the immune response by reducing the activation of the CD8+ T cells. CD8+ T cells are required to clear the viral infection and are integral in vaccine development. In contrast, we found an enhanced CD8+ T cell response in female mice to CVB3 infection, suggesting a sex-dependent T cell response that may underlie the sex bias in disease. Overall, these data represent an essential advancement in the CV field and will help develop future therapeutics and aid in vaccine design to limit CV infections.

Published

2023

176. DNAJB1-PRKACA fusion neoantigens elicit rare endogenous T cell responses that potentiate cell therapy for fibrolamellar carcinoma.

Author

Kirk AM, Crawford JC, Chou CH, Guy C, Pandey K, Kozlik T, Shah RK, Chung S, Nguyen P, Zhang X, Wang J, Bell M, Mettelman RC, Allen EK, Pogorelyy MV, Kim H, Minervina AA, Awad W, Bajracharya R, White T, Long D Jr, Gordon B, Morrison M, Glazer ES, Murphy AJ, Jiang Y, Fitzpatrick EA, Yarchoan M, Sethupathy P, Croft NP, Purcell AW, Federico SM, Stewart E, Gottschalk S, Zamora AE, DeRenzo C, Strome SE, and Thomas PG

Subjects

Humans, Receptors, Antigen, T-Cell genetics, T-Lymphocytes pathology, Cell- and Tissue-Based Therapy, HSP40 Heat-Shock Proteins genetics, Cyclic AMP-Dependent Protein Kinase Catalytic Subunits genetics, Carcinoma, Hepatocellular genetics, Carcinoma, Hepatocellular therapy, Carcinoma, Hepatocellular pathology

Abstract

Fibrolamellar carcinoma (FLC) is a liver tumor with a high mortality burden and few treatment options. A promising therapeutic vulnerability in FLC is its driver mutation, a conserved DNAJB1-PRKACA gene fusion that could be an ideal target neoantigen for immunotherapy. In this study, we aim to define endogenous CD8 T cell responses to this fusion in FLC patients and evaluate fusion-specific T cell receptors (TCRs) for use in cellular immunotherapies. We observe that fusion-specific CD8 T cells are rare and that FLC patient TCR repertoires lack large clusters of related TCR sequences characteristic of potent antigen-specific responses, potentially explaining why endogenous immune responses are insufficient to clear FLC tumors. Nevertheless, we define two functional fusion-specific TCRs, one of which has strong anti-tumor activity in vivo. Together, our results provide insights into the fragmented nature of neoantigen-specific repertoires in humans and indicate routes for clinical development of successful immunotherapies for FLC., Competing Interests: Declaration of interests J.C.C., A.M.K., A.E.Z., S.E.S., and P.G.T. have a patent application for TCRs for treating FLC. J.C.C. has additional patent applications in the field of immunotherapy. A.W.P. is a member of the scientific advisory board (SAB) of Bioinformatics Solutions Inc. (Canada), shareholder and SAB member of Evaxion Biotech (Denmark), consultant for Grey Wolf Therapeutics (UK), and cofounder of Resseptor Therapeutics (Melbourne). S.G. is a co-inventor on patent applications in the fields of cell/gene therapy for cancer, consultant of TESSA Therapeutics, member of the Data and Safety Monitoring Board of Immatics, and SAB member of Be Biopharma and has received honoraria from Tidal, Catamaran Bio, and Sanofi within the last 2 years. S.E.S. is a cofounder, stockholder, and paid consultant for Gliknik Inc., serves on the SAB and holds stock options for Virion Inc., and receives royalties from the Mayo Clinic for licensed IP surrounding manipulation of the PD-1:PD-L1 pathway for cancer treatment. P.G.T. is on the SAB of Immunoscape and Shennon Bio, received personal fees and research support from Elevate Bio, and consulted for 10×, Illumina, Pfizer, Cytoagents, and JNJ., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

177. The cellular microenvironment regulates CX3CR1 expression on CD8 + T cells and the maintenance of CX3CR1 + CD8 + T cells.

Author

Pokharel J, Shryki I, Zwijnenburg AJ, Sandu I, Krumm L, Bekiari C, Avramov V, Heinbäck R, Lysell J, Eidsmo L, Harris HE, and Gerlach C

Subjects

Cellular Microenvironment, Receptors, Antigen, T-Cell metabolism, CX3C Chemokine Receptor 1 metabolism, CD8-Positive T-Lymphocytes metabolism, Receptors, Chemokine genetics

Abstract

Expression levels of the chemokine receptor CX3CR1 serve as high-resolution marker delineating functionally distinct antigen-experienced T-cell states. The factors that influence CX3CR1 expression in T cells are, however, incompletely understood. Here, we show that in vitro priming of naïve CD8 + T cells failed to robustly induce CX3CR1, which highlights the shortcomings of in vitro priming settings in recapitulating in vivo T-cell differentiation. Nevertheless, in vivo generated memory CD8 + T cells maintained CX3CR1 expression during culture. This allowed us to investigate whether T-cell receptor ligation, cell death, and CX3CL1 binding influence CX3CR1 expression. T-cell receptor stimulation led to downregulation of CX3CR1. Without stimulation, CX3CR1 + CD8 + T cells had a selective survival disadvantage, which was enhanced by factors released from necrotic but not apoptotic cells. Exposure to CX3CL1 did not rescue their survival and resulted in a dose-dependent loss of CX3CR1 surface expression. At physiological concentrations of CX3CL1, CX3CR1 surface expression was only minimally reduced, which did not hamper the interpretability of T-cell differentiation states delineated by CX3CR1. Our data further support the broad utility of CX3CR1 surface levels as T-cell differentiation marker and identify factors that influence CX3CR1 expression and the maintenance of CX3CR1 expressing CD8 + T cells., (© 2023 The Authors. European Journal of Immunology published by Wiley-VCH GmbH.)

Published

2024

178. Senescence blurs the line between innate and adaptive immune cells.

Author

Quinn, Kylie M and Linterman, Michelle A

Subjects

*IMMUNOSENESCENCE, *CELLULAR aging, *KILLER cells, *CYTOTOXIC T cells, *MITOGEN-activated protein kinases, *CELLS

Abstract

Keywords: CD8 T cell; immunosenescence; leishmania; NK cell; NKG2D; sestrin EN CD8 T cell immunosenescence leishmania NK cell NKG2D sestrin 431 433 3 07/03/20 20200701 NES 200701 In Covre I et al. i and Pereira I et al i ., the authors demonstrate the parallels between senescent NK cells and senescent CD8 T cells, and formalise the mechanism by which senescent CD8 T cells become more NK cell-like, through the action of sestrins. Given that these senescence features are shared across NK cells and CD8 SP + sp T cells and they emerge at the same time across these populations, it is very likely that a common mechanism could drive senescence in each cell type. Finally, while sestrins mediate senescence and NK cell-like functions in CD8 SP + sp T cell, the mechanism that underpins senescence in NK cells is unclear. [Extracted from the article]

Published

2020

179. A Critical Role of IL-21-Induced BATF in Sustaining CD8-T-Cell-Mediated Chronic Viral Control

Author

Gang Xin, David M. Schauder, Begoña Lainez, Jason S. Weinstein, Zhengxi Dai, Yuhong Chen, Enric Esplugues, Renren Wen, Demin Wang, Ian A. Parish, Allan J. Zajac, Joe Craft, and Weiguo Cui

Subjects

IL-21, BATF, STAT3, IRF4, Blimp-1, CD8 T cell, LCMV, Biology (General), QH301-705.5

Abstract

Control of chronic viral infections by CD8 T cells is critically dependent on CD4 help. In particular, helper-derived IL-21 plays a key role in sustaining the CD8 T cell response; however, the molecular pathways by which IL-21 sustains CD8 T cell immunity remain unclear. We demonstrate that IL-21 causes a phenotypic switch of transcription factor expression in CD8 T cells during chronic viral infection characterized by sustained BATF expression. Importantly, BATF expression during chronic infection is both required for optimal CD8 T cell persistence and anti-viral effector function and sufficient to rescue “unhelped” CD8 T cells. Mechanistically, BATF sustains the response by cooperating with IRF4, an antigen-induced transcription factor that is also critically required for CD8 T cell maintenance, to preserve Blimp-1 expression and thereby sustain CD8 T cell effector function. Collectively, these data suggest that CD4 T cells “help” the CD8 response during chronic infection via IL-21-induced BATF expression.

Published

2015

180. Harnessing CD8+ T Cells Under HIV Antiretroviral Therapy.

Author

Warren, Joanna A., Clutton, Genevieve, and Goonetilleke, Nilu

Subjects

CD8 antigen, T cells, ANTIRETROVIRAL agents, HIV, IMMUNOSENESCENCE

Abstract

Antiretroviral therapy (ART) has transformed HIV from a fatal disease to a chronic condition. In recent years there has been considerable interest in strategies to enable HIV-infected individuals to cease ART without viral rebound, either by purging all cells infected harboring replication-competent virus (HIV eradication), or by boosting immune responses to allow durable suppression of virus without rebound (HIV remission). Both of these approaches may need to harness HIV-specific CD8+ T cells to eliminate infected cells and/or prevent viral spread. In untreated infection, both HIV-specific and total CD8+ T cells are dysfunctional. Here, we review our current understanding of both global and HIV-specific CD8+ T cell immunity in HIV-infected individuals with durably suppressed viral load under ART, and its implications for HIV cure, eradication or remission. Overall, the literature indicates significant normalization of global T cell parameters, including CD4/8 ratio, activation status, and telomere length. Global characteristics of CD8+ T cells from HIV+ART+ individuals align more closely with those of HIV-seronegative individuals than of viremic HIV-infected individuals. However, markers of senescence remain elevated, leading to the hypothesis that immune aging is accelerated in HIV-infected individuals on ART. This phenomenon could have implications for attempts to prime de novo , or boost existing HIV-specific CD8+ T cell responses. A major challenge for both HIV cure and remission strategies is to elicit HIV-specific CD8+ T cell responses superior to that elicited by natural infection in terms of response kinetics, magnitude, breadth, viral suppressive capacity, and tissue localization. Addressing these issues will be critical to the success of HIV cure and remission attempts. [ABSTRACT FROM AUTHOR]

Published

2019

181. The Transcription Factor TCF1 Preserves the Effector Function of Exhausted CD8 T Cells During Chronic Viral Infection.

Author

Wang, Yifei, Hu, Jianjun, Li, Yiding, Xiao, Minglu, Wang, Haoqiang, Tian, Qin, Li, Zhirong, Tang, Jianfang, Hu, Li, Tan, Yan, Zhou, Xinyuan, He, Ran, Wu, Yuzhang, Ye, Lilin, Yin, Zhinan, Huang, Qizhao, and Xu, Lifan

Subjects

TRANSCRIPTION factors, CD8 antigen, CELLULAR immunity, T cells, VIRUS diseases, CHRONIC diseases

Abstract

The long-term persistence of viral antigens drives virus-specific CD8 T cell exhaustion during chronic viral infection. Yet exhausted, CD8 T cells are still endowed with certain levels of effector function, by which they can keep viral replication in check in chronic infection. However, the regulatory factors involved in regulating the effector function of exhausted CD8 T cell are largely unknown. Using mouse model of chronic LCMV infection, we found that the deletion of transcription factor TCF-1 in LCMV-specific exhausted CD8 T cells led to the profound reduction in cytokine production and degranulation. Conversely, ectopic expression of TCF-1 or using agonist to activate TCF-1 activities promotes the effector function of exhausted CD8 T cells. Mechanistically, TCF-1 fuels the functionalities of exhausted CD8 T cells by promoting the expression of an array of key effector function-associated transcription regulators, including Foxo1, Zeb2, Id3, and Eomes. These results collectively indicate that targeting TCF-1 mediated transcriptional pathway may represent a promising immunotherapy strategy against chronic viral infections by reinvigorating the effector function of exhausted virus-specific CD8 T cells. [ABSTRACT FROM AUTHOR]

Published

2019

182. Specific T-cell receptor gene transfer enhances immune response: A potential therapeutic strategy for the control of human cytomegalovirus infection in immunocompromised patients.

Author

Zhang, Runan, Zhang, Yanyue, Hu, Jianhua, Wu, Wei, Chen, Xiaoming, Lu, Zhongjie, Yang, Rong, Huang, Yaping, and Fan, Jun

Subjects

*GENETIC transformation, *T-cell receptor genes, *IMMUNOCOMPROMISED patients, *HUMAN cytomegalovirus diseases, *HUMAN cytomegalovirus

Abstract

Highlights • VSTs could be generated by transfer of TCR genes into PBMCs from donors and patients. • The generation of functional T cells varied among transduction of different PBMCs. • TCR gene transfer is a potential therapeutic strategy for HCMV controlling. Abstract Human cytomegalovirus (HCMV) infection is a leading cause of morbidity and mortality in immunocompromised patients, but no specific therapeutic strategy is effective clinically, despite recent achievements. HCMV-specific T-cell therapy was thought to be helpful for the management of HCMV infection. To conduct a deep exploration, we investigated the possibility of engineering peripheral blood mononuclear cells (PBMCs) from immunocompetent and immunocompromised subjects with specific T-cell receptor (TCR) genes. CD8-positive T cells that specifically bind to NLV pentamers could be generated by transferring TCR genes to PBMCs from immunocompetent and immunocompromised subjects. The generation of functional T cells varied among transduction of different PBMCs. The numbers of IFN-γ-secreting T cells increased significantly in immunocompetent and immunodeficient PBMCs, but were unchanged in immune-reconstituted PBMCs. TCR gene transfer is a potential therapeutic strategy for controlling HCMV infection in immunocompromised patients. The transfer of TCR genes into immunocompetent and immunodeficient PBMCs would be more meaningful in response to HCMV infection than would the transfer into immune-reconstituted PBMCs. [ABSTRACT FROM AUTHOR]

Published

2019

183. Chimeric antigen receptor (CAR) T cells targeting a pathogenic MHC class II:peptide complex modulate the progression of autoimmune diabetes.

Author

Zhang, Li, Sosinowski, Tomasz, Cox, Aaron R., Cepeda, Joseph Ray, Sekhar, Nitin S., Hartig, Sean M., Miao, Dongmei, Yu, Liping, Pietropaolo, Massimo, and Davidson, Howard W.

Abstract

Abstract A primary initiating epitope in the NOD mouse model of Type 1 Diabetes (T1D) lies between residues 9 and 23 of the insulin B chain. The B:9-23 peptide can bind to the NOD MHC class II molecule (I-Ag7) in multiple registers, but only one, (register 3, R3), creates complexes able to stimulate the majority of pathogenic B:9-23-specific CD4+ T cells. Previously we generated a monoclonal antibody (mAb287) that targets this critical I-Ag7-B:9-23(R3) complex. When given weekly to pre-diabetic mice at either early or late stages of disease, mAb287 was able to delay or prevent T1D in the treated animals. Although the precise mechanism of action of mAb287 remains unclear, we hypothesized that it may involve deletion of antigen presenting cells (APCs) bearing the pathogenic IAg7-B:9-23(R3) complexes, and that this process might be rendered more efficient by re-directing cytotoxic T cells using a mAb287 chimeric antigen receptor (287-CAR). As anticipated, 287-CAR T cells secreted IFN-γ in response to stimulation by I-Ag7-B:9-23(R3) complexes expressed on artificial APCs, but not I-Ag7 loaded with other peptides, and killed the presenting cells in vitro. A single infusion of 287-CAR CD8+ T cells to young (5 week old) NOD mice significantly delayed the onset of overt hyperglycemia compared to untreated animals (p = 0.022). None of the 287-CAR CD8+ T cell treated mice developed diabetes before 18 weeks of age, while 29% of control-CAR T cell treated mice (p = 0.044) and 52% of the un-treated mice (p = 0.0001) had developed T1D by this time. However, the protection provided by 287-CAR CD8+ T cells declined with time, and no significant difference in overall incidence by 30 weeks between the 3 groups was observed. Mechanistic studies indicated that the adoptively transferred 287-CAR T cells selectively homed to pancreatic lymph nodes, and in some animals could persist for at least 1–2 weeks post-transfer, but were essentially undetectable 10–15 weeks later. Our study demonstrates that CAR T cells specific for a pathogenic MHC class II:peptide complex can be effective in vivo , but that a single infusion of the current iteration can only delay, but not prevent, the development of T1D. Future studies should therefore be directed towards optimizing strategies designed to improve the longevity of the transferred cells. Highlights • Anti-[I-Ag7/insulin B:9-23 (register 3)] redirected CD8 T cells kill APCs expressing their target antigens. • The re-directed T cells selectively accumulate in organs where their target ligands are presented. • A single infusion of these CAR T cells suppresses the formation of insulin autoantibodies and delays T1D in young NOD mice. [ABSTRACT FROM AUTHOR]

Published

2019

184. Engineering T cell response to cancer antigens by choice of focal therapeutic conditions.

Author

Shao, Qi, O'Flanagan, Stephen, Lam, Tiffany, Roy, Priyatanu, Pelaez, Francisco, Burbach, Brandon J, Azarin, Samira M, Shimizu, Yoji, and Bischof, John C

Published

2019

185. Cheating the Hunger Games; Mechanisms Controlling Clonal Diversity of CD8 Effector and Memory Populations.

Author

Kavazović, Inga, Polić, Bojan, and Wensveen, Felix M.

Abstract

Effector and memory CD8 T cells have an intrinsic difference in the way they must approach antigen; effector cells need to address the pathogen at hand and therefore favor outgrowth of only high-affinity clones. In contrast, the memory pool benefits from greater clonal diversity to recognize and eliminate pathogens with mutations in their immunogenic epitopes. Effector and memory fates are ultimately the result of the same three signals that control T cell activation; T cell receptor (TCR) engagement together with co-stimulation and cytokines. Great progress has been made in our understanding of the transcriptional programs that drive effector or memory differentiation. However, how these two different programs result from the same initial cues is still a matter of debate. An emerging image is that not only the classical three signals determine T cell differentiation, but also the ability of cells to access these signals relative to that of other activated clones. Inter-clonal competition is therefore not only a selective force, but also a mediator of CD8 T cell fate. How this is regulated on a transcriptional level, especially in the context of a selective "hunger game" based on antigen-affinity in which only cells of high-affinity are supposed to survive, is still poorly defined. In this review, we discuss recent literature that illustrates how antigen-affinity dependent inter-clonal competition shapes effector and memory populations in an environment of antigen affinity-driven selection. We argue that fine-tuning of TCR signal intensity presents an attractive target for regulating the scope of CD8 T cell vaccines. [ABSTRACT FROM AUTHOR]

Published

2018

186. Defining Memory CD8 T Cell.

Author

Martin, Matthew D. and Badovinac, Vladimir P.

Abstract

CD8 T cells comprising the memory pool display considerable heterogeneity, with individual cells differing in phenotype and function. This review will focus on our current understanding of heterogeneity within the antigen-specific memory CD8 T cell compartment and classifications of memory CD8 T cell subsets with defined and discrete functionalities. Recent data suggest that phenotype and/or function of numerically stable circulatory memory CD8 T cells are defined by the age of memory CD8 T cell (or time after initial antigen-encounter). In addition, history of antigen stimulations has a profound effect on memory CD8 T cell populations, suggesting that repeated infections (or vaccination) have the capacity to further shape the memory CD8 T cell pool. Finally, genetic background of hosts and history of exposure to diverse microorganisms likely contribute to the observed heterogeneity in the memory CD8 T cell compartment. Extending our tool box and exploring alternative mouse models (i.e., "dirty" and/or outbred mice) to encompass and better model diversity observed in humans will remain an important goal for the near future that will likely shed new light into the mechanisms that govern biology of memory CD8 T cells. [ABSTRACT FROM AUTHOR]

Published

2018

187. A MULTISCALE MODEL OF THE CD8 T CELL IMMUNE RESPONSE STRUCTURED BY INTRACELLULAR CONTENT.

Author

Barbarroux, Loïc, Michel, Philippe, Adimy, Mostafa, and Crauste, Fabien

Subjects

T cells, CD8 antigen, IMMUNE response, CELL-mediated cytotoxicity, CELL proliferation

Abstract

During the primary CD8 T cell immune response, CD8 T cells undergo proliferation and continuous differentiation, acquiring cytotoxic abilities to address the infection and generate an immune memory. At the end of the response, the remaining CD8 T cells are antigen-specific memory cells that will respond stronger and faster in case they are presented this very same antigen again. We propose a nonlinear multiscale mathematical model of the CD8 T cell immune response describing dynamics of two inter-connected physical scales. At the intracellular scale, the level of expression of key proteins involved in proliferation, death, and differentiation of CD8 T cells is modeled by a delay differential system whose dynamics define maturation velocities of CD8 T cells. At the population scale, the amount of CD8 T cells is represented by a discrete density and cell fate depends on their intracellular content. We introduce the model, then show essential mathematical properties (existence, uniqueness, positivity) of solutions and analyse their asymptotic behavior based on the behavior of the intracellular regulatory network. We numerically illustrate the model's ability to qualitatively reproduce both primary and secondary responses, providing a preliminary tool for investigating the generation of long-lived CD8 memory T cells and vaccine design. [ABSTRACT FROM AUTHOR]

Published

2018

188. 2D Kinetic Analysis of TCR and CD8 Coreceptor for LCMV GP33 Epitopes.

Author

Kolawole, Elizabeth M., Andargachew, Rakieb, Liu, Baoyu, Jacobs, Jesica R., and Evavold, Brian D.

Abstract

The LCMV GP33 CD8 epitope has long been one of the most widely used antigens in viral immunology. Of note, almost all of the in vitro analyses of CD8 T cell responses to this epitope make use of an altered peptide ligand (APL) in which the cysteine from the original 9-mer peptide (KAVYNFAT C) is substituted by a methionine at position 41 (KAVYNFAT M). In addition, it is possible that the antigen processed during natural LCMV infection is an 11-mer peptide (KAVYNFAT CGI) rather than the widely used 9-mer. Although previous affinity measurements using purified proteins for these antigen variants revealed minimal differences, we applied highly sensitive two dimensional (2D) biophysical based techniques to further dissect TCR interaction with these closely related GP33 variants. The kinetic analyses of affinity provided by the 2D micropipette adhesion frequency assay (2D-MP) and bond lifetime under force analyzed using a biomembrane force probe (BFP) revealed significant differences between 41M, 41C and the 11-mer 41CGI antigen. We found a hierarchy in 2D affinity as 41M peptide displayed augmented TCR 2D affinity compared to 41C and 41CGI. These differences were also maintained in the presence of CD8 coreceptor and when analysis of total TCR:pMHC and CD8:pMHC bonds were considered. Moreover, the three ligands displayed dramatic differences in the bond lifetimes generated under force, in particular the 41CGI variant with the lowest 2D affinity demonstrated a 15-fold synergistic contribution of the CD8 coreceptor to overall bond lifetime. Our analyses emphasize the sensitivity of single cell and single bond 2D kinetic measurements in distinguishing between related agonist peptides. [ABSTRACT FROM AUTHOR]

Published

2018

189. Exhaustion and Inflation at Antipodes of T Cell Responses to Chronic Virus Infection.

Author

Cicin-Sain, Luka and Arens, Ramon

Subjects

*VIRUS diseases, *T cells, *CD8 antigen, *VIRAL replication, *VIRAL antigens, *VIRAL genes

Abstract

Viruses that have coevolved with their host establish chronic infections that are well tolerated by the host. Other viruses, that are partly adapted to their host, may induce chronic infections where persistent replication and viral antigen expression occur. The former induce highly functional and resilient CD8 T cell responses called memory inflation. The latter induce dysfunctional and exhausted responses. The reasons compelling T cell responses towards inflationary or exhausted responses are only partly understood. In this review we compare the two conditions and describe mechanistic similarities and differences. We also provide a list of potential reasons why exhaustion or inflation occur in different virus infections. We propose that T cell-mediated transcriptional repression of viral gene expression provides a critical feature of inflation that allows peaceful virus and host coexistence. The virus is controlled, but its genome is not eradicated. If this mechanism is not available, as in the case of RNA viruses, the virus and the host are compelled to an arms race. If virus proliferation and spread proceed uncontrolled for too long, T cells are forced to strike a balance between viral control and tissue destruction, losing antiviral potency and facilitating virus persistence. [ABSTRACT FROM AUTHOR]

Published

2018

190. Long-Term Persistence of Exhausted CD8 T Cells in Chronic Infection Is Regulated by MicroRNA-155.

Author

Stelekati, Erietta, Chen, Zeyu, Manne, Sasikanth, Kurachi, Makoto, Ali, Mohammed-Alkhatim, Lewy, Keith, Cai, Zhangying, Nzingha, Kito, McLane, Laura M., Hope, Jennifer L., Fike, Adam J., Katsikis, Peter D., and Wherry, E. John

Abstract

Summary Persistent viral infections and tumors drive development of exhausted T (T EX ) cells. In these settings, T EX cells establish an important host-pathogen or host-tumor stalemate. However, T EX cells erode over time, leading to loss of pathogen or cancer containment. We identified microRNA (miR)-155 as a key regulator of sustained T EX cell responses during chronic lymphocytic choriomeningitis virus (LCMV) infection. Genetic deficiency of miR-155 ablated CD8 T cell responses during chronic infection. Conversely, enhanced miR-155 expression promoted expansion and long-term persistence of T EX cells. However, rather than strictly antagonizing exhaustion, miR-155 promoted a terminal T EX cell subset. Transcriptional profiling identified coordinated control of cell signaling and transcription factor pathways, including the key AP-1 family member Fosl2. Overexpression of Fosl2 reversed the miR-155 effects, identifying a link between miR-155 and the AP-1 transcriptional program in regulating T EX cells. Thus, we identify a mechanism of miR-155 regulation of T EX cells and a key role for Fosl2 in T cell exhaustion. [ABSTRACT FROM AUTHOR]

Published

2018

191. Anti-HBV response to toll-like receptor 7 agonist GS-9620 is associated with intrahepatic aggregates of T cells and B cells.

Author

Li, Li, Barry, Vivian, Daffis, Stephane, Niu, Congrong, Huntzicker, Erik, French, Dorothy M., Mikaelian, Igor, Lanford, Robert E., IVDelaney, William E., and Fletcher, Simon P.

Subjects

*T cell receptors, *CELL receptors, *TOLL-like receptors, *T-cell receptor genes, *B cells, *ANTIGEN receptors, *DISEASES

Abstract

Background & Aims GS-9620, an oral agonist of toll-like receptor 7, is in clinical development for the treatment of chronic hepatitis B (CHB). GS-9620 was previously shown to induce prolonged suppression of serum viral DNA and antigens in the chimpanzee and woodchuck models of CHB. Herein, we investigated the immunomodulatory mechanisms underlying these antiviral effects. Methods Archived liver biopsies and paired peripheral blood mononuclear cell samples from a previous chimpanzee study were analyzed by RNA sequencing, quantitative reverse transcription PCR, immunohistochemistry (IHC) and in situ hybridization (ISH). Results GS-9620 treatment of CHB chimpanzees induced an intrahepatic transcriptional profile significantly enriched with genes associated with hepatitis B virus (HBV) clearance in acutely infected chimpanzees. Type I and II interferon, CD8 + T cell and B cell transcriptional signatures were associated with treatment response, together with evidence of hepatocyte death and liver regeneration. IHC and ISH confirmed an increase in intrahepatic CD8 + T cell and B cell numbers during treatment, and revealed that GS-9620 transiently induced aggregates predominantly comprised of CD8 + T cells and B cells in portal regions. There were no follicular dendritic cells or IgG-positive cells in these lymphoid aggregates and very few CD11b + myeloid cells. There was no change in intrahepatic natural killer cell number during GS-9620 treatment. Conclusion The antiviral response to GS-9620 treatment in CHB chimpanzees was associated with an intrahepatic interferon response and formation of lymphoid aggregates in the liver. Our data indicate these intrahepatic structures are not fully differentiated follicles containing germinal center reactions. However, the temporal correlation between development of these T and B cell aggregates and the antiviral response to treatment suggests they play a role in promoting an effective immune response against HBV. Lay summary New therapies to treat chronic hepatitis B (CHB) are urgently needed. In this study we performed a retrospective analysis of liver and blood samples from a chimpanzee model of CHB to help understand how GS-9620, a drug in clinical trials, suppressed hepatitis B virus (HBV). We found that the antiviral response to GS-9620 was associated with accumulation of immune cells in the liver that can either kill cells infected with HBV or can produce antibodies that may prevent HBV from infecting new liver cells. These findings have important implications for how GS-9620 may be used in patients and may also help guide the development of new therapies to treat chronic HBV infection. [ABSTRACT FROM AUTHOR]

Published

2018

192. Combined sublethal irradiation and agonist anti-CD40 enhance donor T cell accumulation and control of autochthonous murine pancreatic tumors.

Author

Ward-Kavanagh, Lindsay K., Kokolus, Kathleen M., Cooper, Timothy K., Lukacher, Aron E., and Schell, Todd D.

Subjects

*CD40 antigen, *T cells, *IMMUNOSUPPRESSION, *PANCREATIC cancer treatment, *CANCER immunotherapy, *IRRADIATION

Abstract

Tumor-reactive T lymphocytes can promote the regression of established tumors. However, their efficacy is often limited by immunosuppressive mechanisms that block T cell accumulation or function. ACT provides the opportunity to ameliorate immune suppression prior to transfer of tumor-reactive T cells to improve the therapeutic benefit. We evaluated the combination of lymphodepleting whole body irradiation (WBI) and agonist anti-CD40 (αCD40) antibody on control of established autochthonous murine neuroendocrine pancreatic tumors following the transfer of naïve tumor-specific CD8 T cells. Sublethal WBI had little impact on disease outcome but did promote T cell persistence in the lymphoid organs. Host conditioning with αCD40, an approach known to enhance APC function and T cell expansion, transiently increased donor T cell accumulation in the lymphoid organs and pancreas, but failed to control tumor progression. In contrast, combined WBI and αCD40 prolonged T cell proliferation and dramatically enhanced accumulation of donor T cells in both the lymphoid organs and pancreas. This dual conditioning approach also promoted high levels of inflammation in the pancreas and tumor, induced histological regression of established tumors, and extended the lifespan of treated mice. Prolonged survival was entirely dependent upon adoptive transfer, but only partially dependent upon IFNγ production by donor T cells. Our results identify the novel combination of two clinically relevant host conditioning approaches that synergize to overcome immune suppression and drive strong tumor-specific T cell accumulation within well-established tumors. [ABSTRACT FROM AUTHOR]

Published

2018

193. Risk of autoimmune diseases in patients with RASopathies: systematic study of humoral and cellular immunity

Author

Maria Siano, Pietro Strisciuglio, Valentina Pinna, Serena Cabaro, F. Di Candia, S. Sestito, D. Melis, D. De Brasi, Maria Alessio, Vittoria D'Esposito, Stefano Pagano, Pietro Formisano, Marco Tartaglia, Daniela Concolino, V. Marchetti, Giuseppe Perruolo, A. De Luca, Siano, M A, Marchetti, V, Pagano, S, Di Candia, F, Alessio, M, De Brasi, D, De Luca, A, Pinna, V, Sestito, S, Concolino, D, Tartaglia, M, Strisciuglio, P, D'Esposito, V, Cabaro, S, Perruolo, G, Formisano, P, and Melis, D

Subjects

medicine.medical_specialty, Cellular immunity, Inflammatory cytokine, Antigens, CD19, Autoimmunity, CD8 T cells, RASopathy, medicine.disease_cause, Autoimmune Disease, Gastroenterology, Autoimmune Diseases, Immune system, Psoriasis, Internal medicine, medicine, Humans, Pharmacology (medical), Genetics (clinical), Autoimmune disease, Immunity, Cellular, biology, business.industry, Research, Autoantibody, General Medicine, medicine.disease, Inflammatory cytokines, CD8 T cell, biology.protein, Medicine, Antibody, business, Human

Abstract

Background Abnormalities of the immune system are rarely reported in patients affected by RASopathies. Aim of the current study was to investigate the prevalence of immune system dysfunction in a cohort of patients affected by RASopathies. Study design A group of 69 patients was enrolled: 60 at the Federico II University, Naples, 7 at University Magna Graecia of Catanzaro, 2 at “Scuola Medica Salernitana”, Salerno. An age- and sex-matched control group was also enrolled. Autoimmune disorders were investigated according to international consensus criteria. Immune framework was also evaluated by immunoglobulin levels, CD3, CD4, CD8, CD19, CD56 lymphocyte subpopulations, autoantibodies levels and panel of inflammatory molecules, in both patients and controls. Results Frequent upper respiratory tract infections were recorded in 2 patients; pneumonia, psoriasis and alopecia in single patients. Low IgA levels were detected in 8/44 patients (18.18%), low CD8 T cells in 13/35 patients (37.14%). Anti-tg and anti-TPO antibodies were detected in 3/24 patients (12.5%), anti r-TSH in 2 cases (8.33%), all in euthyroidism. Serum IgA and CD8 levels were significantly lower in patients than in controls (p 0.00685; p 0.000656 respectively). All tested patients showed increased inflammatory molecules compared to controls. These findings may anticipate the detection of overt autoimmune disease. Conclusions Patients affected by RASopathies are at risk to develop autoimmune disorders. Routine screening for autoimmunity is recommended in patients with RASopathy.

Published

2021

194. Comparative analysis of the DNA methylation landscape in CD4, CD8, and B memory lineages

Author

Ze Zhang, Rondi Butler, Devin C. Koestler, Shelby Bell-Glenn, Gayathri Warrier, Annette M. Molinaro, Brock C. Christensen, John K. Wiencke, Karl T. Kelsey, and Lucas A. Salas

Subjects

CD4-Positive T-Lymphocytes, 1.1 Normal biological development and functioning, Clinical Sciences, Central memory cell, CD8-Positive T-Lymphocytes, Paediatrics and Reproductive Medicine, Genetic, Underpinning research, Genetics, Humans, Immune response, Molecular Biology, Genetics (clinical), B cell, DNA methylation, Immune activation, Inflammatory and immune system, Human Genome, Cell Differentiation, CD4 T cell, TEMRA, CD8 T cell, Immunologic Memory, Developmental Biology, Epigenesis, Effector memory cell

Abstract

Background There is considerable evidence that epigenetic mechanisms and DNA methylation are critical drivers of immune cell lineage differentiation and activation. However, there has been limited coordinated investigation of common epigenetic pathways among cell lineages. Further, it remains unclear if long-lived memory cell subtypes differentiate distinctly by cell lineages. Results We used the Illumina EPIC array to investigate the consistency of DNA methylation in B cell, CD4 T, and CD8 T naïve and memory cells states. In the process of naïve to memory activation across the three lineages, we identify considerable shared epigenetic regulation at the DNA level for immune memory generation. Further, in central to effector memory differentiation, our analyses revealed specific CpG dinucleotides and genes in CD4 T and CD8 T cells with DNA methylation changes. Finally, we identified unique DNA methylation patterns in terminally differentiated effector memory (TEMRA) CD8 T cells compared to other CD8 T memory cell subtypes. Conclusions Our data suggest that epigenetic alterations are widespread and essential in generating human lymphocyte memory. Unique profiles are involved in methylation changes that accompany memory genesis in the three subtypes of lymphocytes.

Published

2022

195. Identification and characterization of antigen specific t cells from healthy donors for cancer immunotherapy

Author

Martínez Enríquez, Laura Camila, Parra López, Carlos Alberto, Inmunología y Medicina Traslacional, Martinez Enriquez, Laura Camila [0000-0003-0799-942X], and Martínez Enríquez, Laura Camila [0001705413]

Subjects

Neoantigens, inmunogenicidad, tetrámero, Prevención del cáncer, 616 - Enfermedades [610 - Medicina y salud], healthy donor, donantes sanos, Sistema Inmunológico, Neoantígenos, CD8 T cell, Immune System, Immugenicity, Linfocitos T CD8, Cancer Prevention, Sistemas de cultivo

Abstract

ilustraciones, diagramas, gráficas. tablas La inmunoterapia basada en neoantígenos permite estimular el sistema inmune del paciente con cáncer al inducir una respuesta antitumoral dirigida mediada por Linfocitos T (LT). Los neoantígenos son generados por mutaciones somáticas en el ADN que producen cambios en la secuencia de aminoácidos y que son exclusivas de las células tumorales. La selección de neoantígenos inmunogénicos se realiza por medio de herramientas in-silico que predicen la afinidad y tiempo de unión del neoantígeno a la molécula de HLA, luego estos son evaluados en sistemas de cultivo in-vitro con las células de los pacientes, sin embargo, la frecuencia reportada de respuestas a neoantígenos es aún baja. Por lo tanto, este estudio planteó dos acercamientos diferentes para identificar y caracterizar neoantígenos inmunogénicos. Por un lado, se propuso la implementación de sistemas de cultivo con células de donantes sanos para evaluar la inmunogenicidad de los neoantígenos de manera in-vitro. Por otra parte, se propuso el uso del docking y la dinámica molecular para identificar características moleculares asociadas a la inmunogenicidad de los neoantígenos. Para el primer enfoque se utilizaron células mononucleares de sangre periférica (PBMCs) de donantes sanos HLA-A*02:01. Se evaluaron cuatro tipos de cultivos diferentes, manteniendo el uso de las citoquinas IL-21, IL-15 e IL-7 pero modificando las células de partida: i) PBMCs totales, ii) cocultivo acelerado con células dendríticas a partir de PBMCs, iii) cocultivo de células dendríticas in-situ (DCs in-situ) con LT CD8+ vírgenes enriquecidos y iv) cocultivo de células dendríticas por adherencia de monocitos (moDCs) con LT CD8+ vírgenes enriquecidos. Los neoantígenos restringidos a HLA-A*02:01 fueron seleccionados a partir de una búsqueda en la literatura y se evaluaron en forma de pool. El reconocimiento de los LT CD8+ a neoantígenos se evaluó mediante la producción de las citoquinas IFN-γ y TNF-a y por la marcación de tetrámeros. Como resultados se pudo observar que es necesaria la presencia de células presentadoras profesionales, como lo son las DC, y un enriquecimiento de los LT CD8 vírgenes, pues fue en este cultivo que se logró detectar, aunque en baja proporción, LT específicos contra los neoantígenos. No obstante, estos resultados solo se observaron en 2 de 4 donantes evaluados, lo cual indica que es necesario realizar ensayos adicionales para poder determinar que este sistema de cultivo es el indicado. Para el segundo enfoque se realizó una prueba de concepto con dos neoantígenos (uno inmunogénico y otro no inmunogénico) para evaluar el uso del docking y la dinámica molecular como herramientas de tamizaje para la identificación de neoantígenos inmunogénicos, permitiendo determinar que un neoantígeno inmunogénico debe formar un complejo péptido-MHC estable en el tiempo. Este estudio demuestra la alta complejidad que representa el uso de células de donantes sanos y de las herramientas computacionales de docking y dinámica molecular, sin embargo, estos dos enfoques son prometedores ya que no solo permitirían mejorar la selección de neoantígenos inmunogénicos sino también tienen el potencial de identificar TCR específicos contra estos antígenos con fines de terapia adoptiva celular basada en modificación del TCR. (Texto tomado de la fuente) Immunotherapy based on neoantigens allows to stimulate the immune system of cancer patients by inducing a directed antitumor response mediated by T cells. Neoantigens are generated by somatic mutations in DNA that produce changes in the amino acid sequence and are exclusive to tumor cells. The selection of immunogenic neoantigens to predict the affinity and binding of the neoantigen to the HLA is performed in silico and then evaluated with in vitro culture assays with patient cells, however, the reported frequency of responses to neoantigens is low. Therefore, this study proposed two different approaches to identify and characterize immunogenic neoantigens. On the one hand, the implementation of culture systems with cells from healthy donors to evaluate the immunogenicity of neoantigens in vitro. On the other hand, the use of docking and molecular dynamics to identify in silico molecular characteristics associated with the immunogenicity of neoantigens. To evaluate the first approach, peripheral blood mononuclear cells (PBMCs) from healthy HLA-A*02:01 donors were used as a model. HLA-A*02:01-restricted neoantigens were selected from a literature search and evaluated as a pool. Four different types of cultures were evaluated, maintaining the use of the cytokines IL-21, IL-15 and IL-7 but modifying the starting cells: i) total PBMCs, ii) accelerated co-culture with dendritic cells (acDCs) from PBMCs and iii ) co-culture of dendritic cells in situ with Naïve CD8+ T cells and iv) co-culture of monocyte derived dendritic cells with Naïve CD8+ T cells. Recognition of CD8+ T cells to neoantigens was assessed by cytokine production and by tetramer labeling. It was possible to observe that the presence of professional antigen presenting cells, such as DCs, and an enrichment of Naïve CD8+ T cells is necessary to detect, although in low proportion, specific LTs against neoantigens. However, these results were only observed in 2 of 4 donors evaluated, which indicates that additional tests are necessary to determine if this culture system work. For the second approach, a proof of concept was carried out with two neoantigens (one immunogenic and one non-immunogenic) to evaluate the use of docking and molecular dynamics as screening tools for the identification of immunogenic neoantigens, allowing to determine that an immunogenic neoantigen should form a peptide-MHC complex stable over time. This study demonstrates the high complexity of using healthy donor cells and tools such as molecular dynamics and docking, however, these two approaches are promising since they would not only allow to improve the selection of immunogenic neoantigens but also the identification of TCRs specific to neoantigens for adoptive cell therapy with cell modification of the TCR Maestría Magíster en Inmunología Vacunas contra el cáncer

Published

2022

196. Design of an Epitope-Based Vaccine Ensemble for Animal Trypanosomiasis by Computational Methods

Author

Lucas Michel-Todó, Pascal Bigey, Pedro A Reche, María-Jesus Pinazo, Joaquim Gascón, and Julio Alonso-Padilla

Subjects

african animal trypanosomiasis, epitope-based vaccine, b-cell epitopes, cd4 t cell, cd8 t cell, pdna, string-of-beads, Medicine

Abstract

African animal trypanosomiasis is caused by vector-transmitted parasites of the genus Trypanosoma. T. congolense and T. brucei brucei are predominant in Africa; T. evansi and T. vivax in America and Asia. They have in common an extracellular lifestyle and livestock tropism, which provokes huge economic losses in regions where vectors are endemic. There are licensed drugs to treat the infections, but adherence to treatment is poor and appearance of resistances common. Therefore, the availability of a prophylactic vaccine would represent a major breakthrough towards the management and control of the disease. Selection of the most appropriate antigens for its development is a bottleneck step, especially considering the limited resources allocated. Herein we propose a vaccine strategy based on multiple epitopes from multiple antigens to counteract the parasites´ biological complexity. Epitopes were identified by computer-assisted genome-wide screenings, considering sequence conservation criteria, antigens annotation and sub-cellular localization, high binding affinity to antigen presenting molecules, and lack of cross-reactivity to proteins in cattle and other breeding species. We ultimately provide 31 B-cell, 8 CD4 T-cell, and 15 CD8 T-cell epitope sequences from 30 distinct antigens for the prospective design of a genetic ensemble vaccine against the four trypanosome species responsible for African animal trypanosomiasis.

Published

2020

197. Memory CD8 + T cells exhibit tissue imprinting and non‐stable exposure‐dependent reactivation characteristics following blood‐stage Plasmodium berghei ANKA infections

Author

Leo A. H. Zeef, Jenna J Godfrey, Antonn J Cheeseman, Ana Villegas-Mendez, Michael J. Haley, Rebecca S. Dookie, Patrick Strangward, Kevin N. Couper, and Tovah N. Shaw

Subjects

Effector, brain, CD69, Immunology, Spleen, Biology, biology.organism_classification, immune memory, Phenotype, Cell biology, medicine.anatomical_structure, CD8 T cell, parasitic diseases, medicine, biology.protein, Immunology and Allergy, Cytotoxic T cell, cerebral malaria, Plasmodium berghei, Antibody, CD8

Abstract

Experimental cerebral malaria (ECM) is a severe complication of Plasmodium berghei ANKA (PbA) infection in mice, characterized by CD8+ T-cell accumulation within the brain. Whilst the dynamics of CD8+ T-cell activation and migration during extant primary PbA infection have been extensively researched, the fate of the parasite-specific CD8+ T cells upon resolution of ECM is not understood. In this study, we show that memory OT-I cells persist systemically within the spleen, lung and brain following recovery from ECM after primary PbA-OVA infection. Whereas memory OT-I cells within the spleen and lung exhibited canonical central memory (Tcm) and effector memory (Tem) phenotypes, respectively, memory OT-I cells within the brain post-PbA-OVA infection displayed an enriched CD69+CD103− profile and expressed low levels of T-bet. OT-I cells within the brain were excluded from short-term intravascular antibody labelling but were targeted effectively by longer-term systemically administered antibodies. Thus, the memory OT-I cells were extravascular within the brain post-ECM but were potentially not resident memory cells. Importantly, whilst memory OT-I cells exhibited strong reactivation during secondary PbA-OVA infection, preventing activation of new primary effector T cells, they had dampened reactivation during a fourth PbA-OVA infection. Overall, our results demonstrate that memory CD8+ T cells are systemically distributed but exhibit a unique phenotype within the brain post-ECM, and that their reactivation characteristics are shaped by infection history. Our results raise important questions regarding the role of distinct memory CD8+ T-cell populations within the brain and other tissues during repeat Plasmodium infections.

Published

2021

198. Signals for antigen-independent differentiation of memory CD8+ T cells

Author

Eliza Mari Kwesi-Maliepaard, Fred van Leeuwen, and Heinz Jacobs

Subjects

Innate memory, Stimulation, Review, Virtual memory, Biology, CD8-Positive T-Lymphocytes, Epigenesis, Genetic, Cellular and Molecular Neuroscience, Antigen, Cytotoxic T cell, Animals, Humans, Epigenetics, Antigens, Molecular Biology, Pharmacology, Antigen-inexperienced memory, Cell Biology, Phenotype, Immunity, Innate, CD8 T cell, Molecular Medicine, CD8+ T cell, Neuroscience, Immunologic Memory, CD8

Abstract

Conventional CD8+ memory T cells develop upon stimulation with foreign antigen and provide increased protection upon re-challenge. Over the past two decades, new subsets of CD8+ T cells have been identified that acquire memory features independently of antigen exposure. These antigen-inexperienced memory T cells (TAIM) are described under several names including innate memory, virtual memory, and memory phenotype. TAIM cells exhibit characteristics of conventional or true memory cells, including antigen-specific responses. In addition, they show responsiveness to innate stimuli and have been suggested to provide additional levels of protection toward infections and cancer. Here, we discuss the current understanding of TAIM cells, focusing on extrinsic and intrinsic molecular conditions that favor their development, their molecular definitions and immunological properties, as well as their transcriptional and epigenetic regulation.

Published

2021

199. This title is unavailable for guests, please login to see more information.

Author

WAKAMIYA, Takahito, KUBO, Terufumi, YAMASHITA, Shimpei, KOHJIMOTO, Yasuo, TORIGOE, Toshihiko, HARA, Isao, WAKAMIYA, Takahito, KUBO, Terufumi, YAMASHITA, Shimpei, KOHJIMOTO, Yasuo, TORIGOE, Toshihiko, and HARA, Isao

Abstract

Although several biomarkers have been identified to predict prognosis in renal cell carcinoma (RCC), there are no evidence-based biomarkers to predict the response to immune checkpoint inhibitors. In this study, we focused on lymphocytes and tumor cells in the tumor microenvironment and investigated whether immunostaining scoring could predict the best overall response. We evaluated 32 patients with metastatic RCC (mRCC) who were treated with nivolumab monotherapy between August 2016 and July 2020. We performed immunostaining for CD8 T cells, TIA-1, PD-L1, and HLA class 1 in RCC tissues and assigned a score with a maximum of 4 points each, which we defined as histological score. The best overall response of nivolumab was observed in 4 patients (12.5%) with complete response (CR), 10 patients (31.3%) with partial response (PR), 5 patients (15.6%) with stable disease (SD), and 13 patients (40.6%) with progressive disease (PD). There was no significant difference in patient background between the CR＋PR＋SD group (19 patients) and the PD group (13 patients), but CD8 T cells were significantly higher and TIA-1 positive cells tended to be higher in the CR＋PR＋SD group (CD8 T cell : p＝0.03, TIA-1 : p＝0.07, PD-L1 : p＝0.67, HLA class 1 : p＝1.00). In univariate analysis, histological score ≥3 tended to contribute to the best overall response of nivolumab (p＝0.05). There was no significant difference in overall survival or cancer-specific survival after nivolumab administration between the two groups of patients with histological score ≥3 and those with histological score ＜3. In conclusion, immunostaining scoring based on CD8 T cells may be able to predict the efficacy of single-agent nivolumab in patients with mRCC.

Published

2022

200. The impact of CD160 deficiency on alloreactive CD8 T cell responses and allograft rejection

Author

Universidad de Sevilla. Departamento de Medicina, Río, María Luisa del, Nguyen, Tuan H., Tesson, Laurent, Heslan, Jean Marie, Gutiérrez-Adán, Alfonso, Fernández-González, Raúl, Pérez Simón, José Antonio, Rodríguez-Barbosa, José Ignacio, Universidad de Sevilla. Departamento de Medicina, Río, María Luisa del, Nguyen, Tuan H., Tesson, Laurent, Heslan, Jean Marie, Gutiérrez-Adán, Alfonso, Fernández-González, Raúl, Pérez Simón, José Antonio, and Rodríguez-Barbosa, José Ignacio

Abstract

CD160 is a member of the immunoglobulin superfamily with a pattern of expression mainly restricted to cytotoxic cells. To assess the functional relevance of the HVEM/CD160 signaling pathway in allogeneic cytotoxic responses, exon 2 of the CD160 gene was targeted by CRISPR/Cas9 to generate CD160 deficient mice. Next, we evaluated the impact of CD160 deficiency in the course of an alloreactive response. To that aim, parental donor WT (wild-type) or CD160 KO (knock-out) T cells were adoptively transferred into non-irradiated semiallogeneic F1 recipients, in which donor alloreactive CD160 KO CD4 T cells and CD8 T cells clonally expanded less vigorously than in WT T cell counterparts. This differential proliferative response rate at the early phase of T cell expansion influenced the course of CD8 T cell differentiation and the composition of the effector T cell pool that led to a significant decreased of the memory precursor effector cells (MPECs) / short-lived effector cells (SLECs) ratio in CD160 KO CD8 T cells compared to WT CD8 T cells. Despite these differences in T cell proliferation and differentiation, allogeneic MHC class I mismatched (bm1) skin allograft survival in CD160 KO recipients was comparable to that of WT recipients. However, the administration of CTLA-4.Ig showed an enhanced survival trend of bm1 skin allografts in CD160 KO with respect to WT recipients. Finally, CD160 deficient NK cells were as proficient as CD160 WT NK cells in rejecting allogeneic cellular allografts or MHC class I deficient tumor cells. CD160 may represent a CD28 alternative costimulatory molecule for the modulation of allogeneic CD8 T cell responses either in combination with costimulation blockade or by direct targeting of alloreactive CD8 T cells that upregulate CD160 expression in response to alloantigen stimulation.

Published

2022