Your search keyword '"T cell"' showing total 86,322 results

1. Self-reactivity of CD8 T-cell clones determines their differentiation status rather than their responsiveness in infections.

Author

Paprckova, Darina, Niederlova, Veronika, Moudra, Alena, Drobek, Ales, Pribikova, Michaela, Janusova, Sarka, Schober, Kilian, Neuwirth, Ales, Michalik, Juraj, Huranova, Martina, Horkova, Veronika, Cesnekova, Michaela, Simova, Michaela, Prochazka, Jan, Balounova, Jana, Busch, Dirk H., Sedlacek, Radislav, Schwarzer, Martin, and Stepanek, Ondrej

Subjects

MOLECULAR cloning, T cells, CD8 antigen, AUTOANTIGENS, BIOLOGY

Abstract

Mature T cells are selected for recognizing self-antigens with low to intermediate affinity in the thymus. Recently, the relative differences in selfreactivity among individual T-cell clones were appreciated as important factors regulating their fate and immune response, but the role of self-reactivity in Tcell biology is incompletely understood. We addressed the role of selfreactivity in T-cell diversity by generating an atlas of mouse peripheral CD8+ T cells, which revealed two unconventional populations of antigeninexperienced T cells. In the next step, we examined the steady-state phenotype of monoclonal T cells with various levels of self-reactivity. Highly self-reactive clones preferentially differentiate into antigen-inexperienced memory-like cells, but do not form a population expressing type I interferoninduced genes, showing that these two subsets have unrelated origins. The functional comparison of naïve monoclonal CD8+ T cells specific to the identical model antigen did not show any correlation between the level of self-reactivity and the magnitude of the immune response. [ABSTRACT FROM AUTHOR]

Published

2022

2. Spatiotemporal Reassortment of Th1 Migratory Receptors in Inflamed Skin

Author

Carter, Evan Moss

Subjects

Chemokine, Inflammation, Integrin, Migration, T cell, Tissue, Biology, Immunology

Abstract

CD4+ T helper (Th) cells search a vast tissue area to find sites of infection or inflammation. The distribution of Th cells in tissues is shaped by tissue architecture, chemotactic cues, adhesion molecules, and the location of antigen (Ag). How Th cells integrate these signals to optimize tissue entry, exploration, and correct positioning for delivery of effector function is poorly understood. To gain insight into the stages of Th cell migration, an optogenetic tool based on the photoconvertible Kaede protein was used to spatiotemporally mark or “timestamp” type 1 Th (Th1) cells in inflamed skin. The timestamp enabled analysis of Th1 cells that recently entered tissue, Th1s that spent >24 hours in tissue, and Th1s that exited to the draining lymph node. Flow cytometry analysis revealed distinct changes in surface chemokine receptors (CCRs), integrin receptors, and markers of costimulation and activation based on tissue dwell time. CCRs were upregulated in inflamed skin, with a surprising exception – the canonical Th1 CCR CXCR3 was rapidly lost upon tissue entry. In tissue, integrins were most upregulated after entry, and costimulatory receptors and activation markers were upregulated over time. Some of these changes occurred within 4 hours of tissue entry. Both non-Ag signals and encounters with cognate Ag influenced receptor expression. These data suggest that one set of proteins is utilized in tissue entry while another combination is used to traffick through the skin or remain in tissue. The spatiotemporal sequence uncovered by this work may point to novel therapeutic targets, which could be manipulated to enhance or regulate Th cell effector function in treatments for infection, inflammation, and cancer.

Published

2024

3. The human T‐cell receptor repertoire in health and disease and potential for omics integration.

Author

Watkins, Thomas S and Miles, John J

Subjects

*HUMAN genetics, *BIG data, *IMMUNE system, *HUMAN beings, *BIOLOGY

Abstract

The adaptive immune system arose 600 million years ago in a cold‐blooded fish. Over countless generations, our antecedents tuned the function of the T‐cell receptor (TCR). The TCR system is arguably the most complex known to science. The TCR evolved hypervariability to fight the hypervariability of pathogens and cancers that look to consume our resources. This review describes the genetics and architecture of the human TCR and highlights surprising new discoveries over the past years that have disproved very old dogmas. The standardization of TCR sequencing data is discussed in preparation for big data bioinformatics and predictive analysis. We next catalogue new signatures and phenomenon discovered by TCR next generation sequencing (NGS) in health and disease and work that remain to be done in this space. Finally, we discuss how TCR NGS can add to immunodiagnostics and integrate with other omics platforms for both a deeper understanding of TCR biology and its use in the clinical setting. [ABSTRACT FROM AUTHOR]

Published

2021

4. Investigating the Metabolic Landscape of T Cell Development from Hematopoietic Stem Cells In Vivo and In Vitro

Author

Sun, Victoria

Subjects

Biology, Developmental biology, Immunology, Hematopoietic Stem Cell, Metabolism, Organoid, T cell, Thymopoiesis, Thymus

Abstract

Normal T cell production from hematopoietic stem and progenitor cells (HSPCs) declines with age, causing the immune system to become less efficient at fighting illnesses ranging from infections to cancer. T cell development begins when HSPCs from the bone marrow circulate in the blood and home to an organ called the thymus. After populating the thymus, HSPCs are first directed to a T cell fate. In later stages, committed thymocytes advance through pivotal checkpoints to mature into different types of T cells with specialized functions that then egress from the thymus. Although the metabolism of peripheral and activated T cells has been extensively studied, metabolic changes during stem cell development into T cells are not well understood, especially in human thymus. In vitro models of T cell differentiation are promising tools to study T cell development, but how well they reflect in vivo metabolism remains unclear. Studying metabolic changes in vitro also faces several challenges due to limitations in current standard culture systems. Previously, our lab developed an in vitro 3D “Artificial Thymic Organoid” (ATO) model that generates functional human T cells from various stem cell sources. Our goal is to improve T cell production and ultimately advance T cell therapies that regenerate the immune system. Here, we adapt the ATO system to recapitulate thymic differentiation of murine HSPCs into mature T cells and overcome several limitations of previous in vitro systems.Next, we integrate transcriptomics and metabolic extracellular flux data from human and murine in vivo and in vitro thymocytes to define the metabolic signatures that distinguish T lineage commitment and T cell maturation stages in the thymus. We reveal that patterns of metabolic activity are remarkably well-conserved in human and murine species, and during in vitro T cell development. Glycolysis and oxidative phosphorylation are drastically reduced at the developmental stage during which thymocytes are completing T cell receptor (TCR) rearrangement. Using an in vitro mouse knockout model of the recombinase activating gene Rag-1, we demonstrate that metabolic activity persistently decreases at the same stage even in the absence of TCR rearrangement. Thus, our results identify critical metabolic transitions that are highly conserved between species as well as in vivo and in vitro T cell development. Future studies in the lab would study the impact of perturbing metabolic pathways on T cell development, particularly in the context of aging.

Published

2021

5. Altered pre-existing SARS-CoV-2-specific T cell responses in elderly individuals

Author

Mitsuo Kina, Hiroki Ishikawa, Osamu Tamai, Sakura Toguchi, Masatake Miyagi, Tomoari Mori, Kentaro Tamaki, Hiroaki Tomori, Mio Miyagi, Naoyuki Taira, Koichi Oshiro, and Mary Collins

Subjects

viruses, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), T cell, fungi, Viral membrane, Biology, Asymptomatic, Article, Nucleoprotein, medicine.anatomical_structure, Interferon, Immunology, medicine, biology.protein, Risk factor, medicine.symptom, Antibody, medicine.drug

Abstract

Pre-existing SARS-CoV-2-specific T cells, but not antibodies, have been detected in some unexposed individuals. This may account for some of the diversity in clinical outcomes ranging from asymptomatic infection to severe COVID-19. Although age is a risk factor for COVID-19, how age affects SARS-CoV-2-specific T cell responses remains unknown. We found that some pre-existing T cell responses to specific SARS-CoV-2 proteins, Spike (S) and Nucleoprotein (N), were significantly lower in elderly donors (>70 years old) who were seronegative for S than in young donors. However, substantial pre-existing T cell responses to the viral membrane (M) protein were detected in some elderly donors. These responses likely compensate for loss of T cell responses specific to S and N. In contrast, young and elderly donors exhibited comparable T cell responses to S, N, and M proteins after infection with SARS-CoV-2. M-specific responses were mediated by CD4 T cells producing interferon-γ in both seronegative and seropositive individuals. T cells in seronegative elderly donors responded to various M-derived peptides, while the response after SARS-CoV-2 infection was apparently focused on a single peptide. These data suggest that diversity of target antigen repertoire for pre-existing SARS-CoV-2-specific T cells declines with age, but the magnitude of pre-existing T cell responses is maintained by T cells reactive to specific viral proteins such as M. A better understanding of the role of pre-existing SARS-CoV-2-specific T cells that are less susceptible to age-related loss may contribute to development of more effective vaccines for elderly people.

Published

2022

6. Genome 3D structure regulation of Immune cell development and activation

Author

He, Zhaoren

Subjects

Biology, Bioinformatics, B cell, enhancer, Genome architecture, HiC, Neutrophils, T cell

Abstract

Each type of cell in the immune system performs critical function to protect the body and maintain health. In the past few decades, the development and activation of T, B and NK cells have been thoroughly studied. However, it’s only until recently that we developed high throughput technology to study how genome folding structure is regulated in the immune cell development process. Here, I exploited the new techniques to study the development of B cell, T cell, and the activation process of neutrophils.In B cell activation, the transition from the follicular B to the plasma cell stage is orchestrated by an ensemble of transcriptional regulators. We examined how changes in expression patterns of key developmental regulators relate to alterations in nuclear positioning and found that gene activation at the onset of plasma cell development was concomitant with a gain in euchromatic character for an ensemble of genomic regions that dictate plasma cell fate, including the Prdm1 and Atf4 loci. We found that to permit the onset of plasma cell development the Ebf1 locus repositioned to peri-centromeric heterochromatin. Plasma cell differentiation was also associated with increased inter-chromosomal associations concurrent with alterations in gene expression and co-localization of Prdm1, Xbp1 and Atf4 transcripts in nuclear bodies. These data indicate that Ebf1 enforces the follicular B cell fate and that the onset of plasma cell fate is orchestrated by elaborate changes in compartmentalization and inter-chromosomal associations. In T cell differentiation, it is well known that Bcl11b specifies T cell fate. Here, we show that in developing T cells, the Bcl11b enhancer repositioned from the lamina to the nuclear interior. Our identified a non-coding RNA named ThymoD (thymocyte differentiation factor) controls the re-localization of Bcl11b enhancers. ThymoD transcription promoted demethylation at CTCF bound sites and activated cohesin-dependent looping to reposition the Bcl11b enhancer from the lamina to the nuclear interior and to juxtapose the Bcl11b enhancer and promoter into a single-loop domain. These large-scale changes in nuclear architecture were associated with the deposition of activating epigenetic marks across the loop domain, plausibly facilitating phase separation. These finding indicate how noncoding transcription orchestrates chromatin folding and compartmentalization to direct with high precision enhancer-promoter communication. During neutrophil activation, the cell undergoes large-scale changes in nuclear morphology. We found that neutrophils rapidly (

Published

2020

7. The depths of PD-1 function within the tumor microenvironment beyond CD8+ T cells

Author

Grace Mallett, Stephanie Laba, and Shoba Amarnath

Subjects

0301 basic medicine, Cancer Research, medicine.medical_treatment, T cell, Programmed Cell Death 1 Receptor, chemical and pharmacologic phenomena, CD8-Positive T-Lymphocytes, Biology, 03 medical and health sciences, 0302 clinical medicine, Immune system, Neoplasms, Tumor Microenvironment, medicine, Humans, Cytotoxic T cell, Lymphocytes, Tumor microenvironment, Innate lymphoid cell, Immunotherapy, T helper cell, biochemical phenomena, metabolism, and nutrition, Immunity, Innate, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cancer research, bacteria, CD8

Abstract

Programmed cell death-1 (PD-1; CD279) is a cell surface receptor that is expressed in both innate and adaptive immune cells. The role of PD-1 in adaptive immune cells, specifically in CD8sup+/supT cells, has been thoroughly investigated but its significance in other immune cells is yet to be well established. This review will address the role of PD-1 based therapies in enhancing non-CD8sup+/supT cell immune responses within cancer. Specifically, the expression and function of PD-1 in non-CD8sup+/supimmune cell compartments such as CD4sup+/supT helper cell subsets, myeloid cells and innate lymphoid cells (ILCs) will be discussed. By understanding the immune cell specific function of PD-1 within tissue resident innate and adaptive immune cells, it will be possible to stratify patients for PD-1 based therapies for both immunogeneic and non-immunogeneic neoplastic disorders. With this knowledge from fundamental and translational studies, PD-1 based therapies can be utilized to enhance T cell independent immune responses in cancers.

Published

2022

8. Anticancer natural products targeting immune checkpoint protein network

Author

Do-Hee Kim, Pawan Kumar Raut, Kyung-Soo Chun, and Young-Joon Surh

Subjects

Biological Products, Cancer Research, biology, T cell, Lymphocyte, medicine.medical_treatment, Programmed Cell Death 1 Receptor, chemical and pharmacologic phenomena, Immunotherapy, Immune Checkpoint Proteins, B7-H1 Antigen, Immune checkpoint, medicine.anatomical_structure, Immune system, CTLA-4, Neoplasms, biology.protein, medicine, Cancer research, Humans, Immunologic Factors, Cytotoxic T cell, Antibody, Immune Checkpoint Inhibitors

Abstract

Normal cells express surface proteins that bind to immune checkpoint proteins on immune cells to turn them off, whereby the immune system does not attack normal healthy cells. Cancer cells can also utilize this same protective mechanism by expressing surface proteins associated with checkpoint proteins on immune cells to overcome the immune surveillance. Immunotherapy is making the best use of the body's own immune system to reinforce anti-tumor responses. The most generally used immunotherapy is the control of immune checkpoints including the cytotoxic T lymphocyte-associated molecule-4 (CTLA-4), programmed cell death receptor-1 (PD-1), or programmed cell death ligand-1 (PD-L1). In spite of the clinical effectiveness of these immune checkpoint inhibitors, the overall response rate still remains low. Therefore, there have been considerable efforts in searching for alternative immune checkpoint proteins that may work as new therapeutic targets for treatment of cancer. Recent studies have identified several additional novel immune checkpoint targets, including lymphocyte activation gene-3, T cell immunoglobulin and mucin-domain containing-3, T cell immunoglobulin and immunoreceptor tyrosine-based inhibition motif domain, V-domain Ig suppressor of T cell activation, B7 homolog 3 protein, B and T cell lymphocyte attenuator, and Inducible T-cell COStimulator. Natural compounds, especially those present in medicinal or dietary plants, have been investigated for their anti-tumor effects in various in vitro and in vivo models. Some phytochemicals exert anti-tumor activities based on immunoregulation, capable of blocking interaction between proteins involved in immune checkpoint signal transduction or regulation of their expression. Recently, synergistic anti-cancer effects of diverse phytochemicals with anti-PD-1/PD-L1 or anti-CTLA-4 monoclonal antibody drugs have been continuously reported. Considering an increasing attention to noteworthy therapeutic effects of immune checkpoint inhibitors in the cancer therapy, this review focuses on regulatory effects of selected phytochemicals on immune checkpoint protein network and their combinational effectiveness with immune checkpoint inhibitors targeting tumor cells.

Published

2022

9. Overexpression of Nuclear Enriched Autosomal Transcript 1 Facilitates Cell Proliferation, Migration Invasion, and Suppresses Apoptosis in Endometrial Cancer by Targeting MicroRNA-202-3p/T Cell Immunoglobulin and Mucin Domain 4 Axis

Author

Caiyan Xu, Jianjun Zhai, and Yujing Fu

Subjects

0301 basic medicine, Cancer Research, T cell, Immunoglobulins, Apoptosis, Biology, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Cell Line, Tumor, microRNA, medicine, Humans, Radiology, Nuclear Medicine and imaging, Cell Proliferation, Pharmacology, Cell growth, Endometrial cancer, Mucin, Membrane Proteins, General Medicine, medicine.disease, Long non-coding RNA, Endometrial Neoplasms, MicroRNAs, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Female, RNA, Long Noncoding, Antibody

Abstract

Background: Endometrial cancer (EC) is an intractable gynecological cancer with increasing incidence and mortality worldwide. Accumulating studies indicated that long noncoding RNA nuclear enriched...

Published

2022

10. FYN and CD247: Key Genes for Septic Shock Based on Bioinformatics and Meta-Analysis

Author

Qian Miao, Yingchun Hu, Lin Hu, Yue Jiang, Ye Tian, and Tingyan Zhou

Subjects

Septic shock, T cell, Organic Chemistry, CD247, General Medicine, Biology, medicine.disease, Bioinformatics, Computer Science Applications, Sepsis, Systemic inflammatory response syndrome, FYN, medicine.anatomical_structure, Drug Discovery, medicine, Gene, Survival analysis

Abstract

Background:Septic shock is sepsis accompanied by hemodynamic instability and high clinical mortality.Material and Methods:GSE95233, GSE57065, GSE131761 gene-expression profiles of healthy control subjects and septic shock patients were downloaded from the Gene-Expression Omnibus (GEO) database, and differences of expression profiles and their intersection were analysed using GEO2R. Function and pathway enrichment analysis was performed on common differentially expressed genes (DEG), and key genes for septic shock were screened using a protein-protein interaction network created with STRING. Also, data from the GEO database were used for survival analysis for key genes, and a meta-analysis was used to explore expression trends of core genes. Finally, high-throughput sequencing using the blood of a murine sepsis model was performed to analyse the expression of CD247 and FYN in mice.Results:A total of 539 DEGs were obtained (p < 0.05). Gene ontology analysis showed that key genes were enriched in functions, such as immune response and T cell activity, and DEGs were enriched in signal pathways, such as T cell receptors. FYN and CD247 are in the centre of the protein-protein interaction network, and survival analysis found that they are positively correlated with survival from sepsis. Further, meta-analysis results showed that FYN could be useful for the prognosis of patients, and CD247 might distinguish between sepsis and systemic inflammatory response syndrome patients. Finally, RNA sequencing using a mouse septic shock model showed low expression of CD247 and FYN in this model.Conclusion:FYN and CD247 are expected to become new biomarkers of septic shock.

Published

2022

11. Commercialized kits to assess T-cell responses against SARS-CoV-2 S peptides. A pilot study in health care workers

Author

Andrés Antón, Candela Fernández-Naval, Iria Arrese-Muñoz, Juliana Esperalba, Mónica Martínez-Gallo, Ricardo Pujol-Borrell, Victoria Cardona, Tomás Pumarola, Moises Labrador-Horrillo, Victor Sanda, and Manuel Hernández-González

Subjects

CBC, complete blood count, COVID-19 Vaccines, BNT162b2-mRNA-COVID-19-vaccine, Coronavirus disease 2019 (COVID-19), Ensayos de liberación Interferon-gamma, Health Personnel, T-Lymphocytes, T cell, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Concordance, CLIA, chemiluminescence immunoassays, Pilot Projects, Cell mediated immunity, Antibodies, Viral, Immune system, Vacuna BNT162b2-mRNA-COVID-19, HCWs, health care workers, S, spike protein, Interferon-gamma-release-assays, ELISA, enzyme linked immunosorbent assay, Humans, Medicine, biology, SARS-CoV-2, business.industry, COVID-19, General Medicine, N, nucleocapsid protein, Vaccination, Specific antibody, IGRA, interferon-gamma-release-assays, medicine.anatomical_structure, Immunology, biology.protein, Original Article, Antibody, Peptides, business, Inmunidad Mediada por Células

Abstract

It is crucial to assess the levels of protection generated by natural infection or SARS-CoV-2 vaccines, mainly in individuals professionally exposed and in vulnerable groups. Measuring T-cell responses may complement antibody tests currently in use as correlates of protection. Our aim was to assess the feasibility of a validated assay of T-cell responses.Twenty health-care-workers (HCW) were included. Antibody test to SARS-CoV-2 N and S-proteins in parallel with a commercially available whole-blood-interferon-gamma-release-assay (IGRA) to S-peptides and two detection methods, CLIA and ELISA were determined.IGRA test detected T-cell responses in naturally exposed and vaccinated HCW already after first vaccination dose. The correlation by the two detection methods was very high (Whole-blood-IGRA-tests amenable to automation and constitutes a promising additional tool for measuring the state of the immune response to SARS-CoV-2; they are applicable to large number of samples and may become a valuable correlate of protection to COVID-19, particularly for vulnerable groups at risk of being re-exposed to infection, as are health-care-workers.Es fundamental evaluar los niveles de protección inmune en infectados o tras la vacunación frente a SARS-CoV-2. La cuantificación de la respuesta inmune celular T puede complementar la determinación de anticuerpos. Evaluamos la viabilidad de un ensayo comercial validado de respuesta celular T específica frente a SARS-CoV-2.Se incluyeron veinte trabajadores sanitarios (TS). Medimos anticuerpos contra las proteínas N y S de SARS-CoV-2 y realizamos el ensayo de liberación de interferón-gamma (IFNγ) en sangre completa (IGRA) frente a péptidos de la proteína S. IFNγ se determinó mediante dos métodos de detección: CLIA y ELISA.IGRA detectó respuesta celular T en TS tanto infectados como vacunados. La correlación de los dos métodos de detección de IFNγ fue muy alta (R 0,8) y la sensibilidad y la especificidad variaron entre 100 y 86% y 100-73% respectivamente. Hubo una concordancia muy alta entre los niveles de anticuerpos específicos y el ensayo IGRA aunque la correlación cuantitativa fue relativamente baja. En el grupo de infectados, una dosis de vacuna fue suficiente para alcanzar el «plateau» de respuesta inmune. IGRA fue claramente positivo en un profesional vacunado inmunosuprimido que presentaba anticuerpos contra la proteína S negativos.IGRA frente a péptidos de la proteína-S es susceptible de automatización y constituye una herramienta prometedora para medir la respuesta inmune celular frente a SARS-CoV-2; es aplicable a un gran número de muestras y puede servir para valorar la protección, particularmente en los grupos vulnerables en riesgo de volver a exponerse a la infección, como los TS.

Published

2022

12. Studying the biology of cytotoxic T lymphocytes in vivo with a fluorescent granzyme B-mTFP knock-in mouse

Author

Per Olof Berggren, Fritz Benseler, Christiane Harenberg, Claudia Schirra, Keerthana Ravichandran, Hsin Fang Chang, Elmar Krause, Praneeth Chitirala, Jens Rettig, Midhat H. Abdulreda, Paloma Martzloff, Trese Leinders-Zufall, and Nils Brose

Subjects

0301 basic medicine, Mouse, QH301-705.5, medicine.medical_treatment, T cell, Science, Green Fluorescent Proteins, Mice, Transgenic, Biology, cytotoxic granules, cytotoxic T lymphocytes, Granzymes, General Biochemistry, Genetics and Molecular Biology, Immunological synapse, GZMB, Mice, 03 medical and health sciences, Immunology and Inflammation, 0302 clinical medicine, In vivo, STED microscopy, medicine, Animals, Cytotoxic T cell, two-photon microscopy, Biology (General), General Immunology and Microbiology, General Neuroscience, immune synapse, General Medicine, Immunotherapy, Fusion protein, Tools and Resources, Cell biology, Granzyme B, 030104 developmental biology, medicine.anatomical_structure, Medicine, exocytosis, 030217 neurology & neurosurgery, T-Lymphocytes, Cytotoxic

Abstract

Understanding T cell function in vivo is of key importance for basic and translational immunology alike. To study T cells in vivo, we developed a new knock-in mouse line, which expresses a fusion protein of granzyme B, a key component of cytotoxic granules involved in T cell-mediated target cell-killing, and monomeric teal fluorescent protein from the endogenous Gzmb locus. Homozygous knock-ins, which are viable and fertile, have cytotoxic T lymphocytes with endogeneously fluorescent cytotoxic granules but wild-type-like killing capacity. Expression of the fluorescent fusion protein allows quantitative analyses of cytotoxic granule maturation, transport and fusion in vitro with super-resolution imaging techniques, and two-photon microscopy in living knock-ins enables the visualization of tissue rejection through individual target cell-killing events in vivo. Thus, the new mouse line is an ideal tool to study cytotoxic T lymphocyte biology and to optimize personalized immunotherapy in cancer treatment., eLife digest Cytotoxic, or killer, T cells are a key part of the immune system. They carry a lethal mixture of toxic chemicals, stored in packages called cytotoxic granules. Killer T cells inject the contents of these granules into infected, cancerous or otherwise foreign cells, forcing them to safely self-destruct. In test tubes, T cells are highly efficient serial killers, moving from one infected cell to the next at high speed. But, inside the body, their killing rate slows down. Researchers think that this has something to do with how killer T cells interact with other immune cells, but the details remain unclear. To get to grips with how killer T cells work in their natural environment, researchers need a way to follow them inside the body. One approach could be to use genetic engineering to attach a fluorescent tag to a protein found inside killer T cells. That tag then acts as a beacon, lighting the cells up and allowing researchers to track their movements. Tagging a protein inside the cytotoxic granules would allow close monitoring of T cells as they encounter, recognize and kill their targets. But fluorescent tags are bulky, and they can stop certain proteins from working as they should. To find out whether it is possible to track killer T cells with fluorescent tags, Chitirala, Chang et al. developed a new type of genetically modified mouse. The modification added a teal-colored tag to a protein inside the granules of the killer T cells. Chitirala, Chang et al. then used a combination of microscopy techniques inside and outside of the body to find out if the T cells still worked. This analysis showed that, not only were the tagged T cells able to kill diseased cells as normal, the tags made it possible to watch it happening in real time. Super-resolution microscopy outside of the body allowed Chitirala, Chang et al. to watch the killer T cells release their toxic granule content. It was also possible to follow individual T cells as they moved into, and destroyed, foreign tissue that had been transplanted inside the mice. These new mice provide a tool to understand how killer T cells really work. They could allow study not only of the cells themselves, but also their interactions with other immune cells inside the body. This could help to answer open questions in T cell research, such as why T cells seem to be so much more efficient at killing in test tubes than they are inside the body. Understanding this better could support the development of new treatments for viruses and cancer.

Published

2023

13. A high throughput bispecific antibody discovery pipeline

Author

Ci Ren, Xiaoming Chen, Per Niklas Hedde, Weian Zhao, George Wu, Jan Zimak, Qiwei Fu, Audrey W. Fung, Jonathan Chong, Aude I. Segaliny, Rodrigo Rivera, Yonglei Shang, Jayapriya Jayaraman, Ryan Luxon, Xiaoya Ma, and Xianzhi Jiang

Subjects

Bispecific antibody, Sequence analysis, T cell, Pipeline (computing), T-Lymphocytes, Medicine (miscellaneous), Computational biology, Biology, General Biochemistry, Genetics and Molecular Biology, Antibodies, Vaccine Related, Clinical Research, medicine, 2.1 Biological and endogenous factors, Aetiology, Throughput (business), Sequence (medicine), High-Throughput Screening Assays, medicine.anatomical_structure, 5.1 Pharmaceuticals, Blinatumomab, Bispecific, Immunization, Immunotherapy, Generic health relevance, Single-Cell Analysis, Development of treatments and therapeutic interventions, General Agricultural and Biological Sciences, Function (biology), medicine.drug, Biotechnology

Abstract

Bispecific antibodies (BsAbs) represent an emerging class of immunotherapy but inefficiency in the current BsAb discovery paradigm has limited their broad clinical availability. Here we report a high throughput, agnostic, single-cell-based BsAb functional screening pipeline, comprising molecular and cell engineering for efficient generation of BsAb library cells, followed by functional interrogation at the single-cell level to identify and sort positive clones and downstream sequence identification with single-cell PCR and sequencing and functionality characterization. Using a CD19xCD3 bispecific T cell engager (BiTE) as a model system, we demonstrate that our single cell platform possesses a high throughput screening efficiency of up to one and half million variant library cells per run and can isolate rare functional clones at low abundance of 0.008%. Using a complex CD19xCD3 BiTE-expressing cell library with approximately 22,300 unique variants comprising combinatorially varied scFvs, connecting linkers and VL/VH orientations, we have identified 98 unique clones including extremely rare ones (∼ 0.001% abundance). We also discovered BiTEs that exhibit novel properties contradictory to conventional wisdom, including harboring rigid scFv connecting peptide linkers yet with in vitro cytotoxicity comparable to that of clinically approved Blinatumomab. Through sequencing analyses on sorted BiTE clones, we discovered multiple design variable preferences for functionality including the CD19VL-VH– CD3VH-VL and CD19VH-VL–CD3VH-VL arrangements being the most favored orientation. Sequence analysis further interrogated the sequence composition of the CDRH3 domain in scFvs and identified amino acid residues conserved for function. We expect our single cell platform to not only significantly increase the development speed of high quality of new BsAb therapeutics for cancer and other disorders, but also enable identifying generalizable design principles for new BsAbs and other immunotherapeutics based on an in-depth understanding of the inter-relationships between sequence, structure, and function.

Published

2023

14. Characterization of a novel bispecific antibody targeting tissue factor-positive tumors with T cell engagement

Author

Jie Chen, Yuexian Zhou, Lei Wang, Lei Han, Huifang Zong, Rui Sun, Xiaodong Xiao, Yunsheng Yuan, Yueqing Xie, Zhidi Pan, Hua Jiang, Huili Lu, Baohong Zhang, and Jianwei Zhu

Subjects

biology, Chemistry, medicine.medical_treatment, T cell, CD3, T-cell receptor, Immunotherapy, Peripheral blood mononuclear cell, Tissue factor, medicine.anatomical_structure, Antigen, Tumor progression, medicine, Cancer research, biology.protein, General Pharmacology, Toxicology and Pharmaceutics

Abstract

T cell engaged bispecific antibody (TCB) is an effective immunotherapy for cancer treatment. Through co-targeting CD3 and tumor-associated antigen (TAA), TCB can redirect CD3+ T cells to eliminate tumor cells regardless of the specificity of T cell receptor. Tissue factor (TF) is a TAA that involved in tumor progression. Here, we designed and characterized a novel TCB targeting TF (TF-TCB) for the treatment of TF-positive tumors. In vitro, robust T cell activation, tumor cell lysis and T cell proliferation were induced by TF-TCB. The tumor cell lysis activity was dependent upon both CD3 and TF binding moieties of the TF-TCB, and was related to TF expression level of tumor cells. In vivo, in both tumor cell/human peripheral blood mononuclear cells (PBMC) co-grafting model and established tumor models with poor T cell infiltration, tumor growth was strongly inhibited by TF-TCB. T cell infiltration into tumors was induced during the treatment. Furthermore, efficacy of TF-TCB was further improved by combination with immune checkpoint inhibitors. For the first time, our results validated the feasibility of using TF as a target for TCB and highlighted the potential for TF-TCB to demonstrate efficacy in solid tumor treatment.

Published

2022

15. Adenosine Deaminase 1 Overexpression Enhances the Antitumor Efficacy of Chimeric Antigen Receptor-Engineered T Cells

Author

Melanie A. MacMullan, Yun Qu, Fangheng Hu, Gunce E. Cinay, Pin Wang, Zachary S. Dunn, Xianhui Chen, Hsuan-Yao Wang, and Jiangyue Liu

Subjects

Adenosine, Adenosine Deaminase, T-Lymphocytes, T cell, Receptors, Antigen, T-Cell, Immunotherapy, Adoptive, Cell therapy, Mice, Immune system, Adenosine deaminase, immune system diseases, Albumins, Cell Line, Tumor, Genetics, medicine, Animals, Humans, cvg, Molecular Biology, Research Articles, Receptors, Chimeric Antigen, biology, Armored car, Chemistry, cvg.computer_videogame, hemic and immune systems, Xenograft Model Antitumor Assays, Chimeric antigen receptor, medicine.anatomical_structure, Cancer cell, Cancer research, biology.protein, Molecular Medicine, Collagen, medicine.drug

Abstract

Chimeric antigen receptor (CAR) T cell therapy mediates unprecedented benefit in certain leukemias and lymphomas, but has yet to achieve similar success in combating solid tumors. A substantial body of work indicates that the accumulation of adenosine in the solid tumor microenvironment (TME) plays a crucial role in abrogating immunotherapies. Adenosine deaminase 1 (ADA) catabolizes adenosine into inosine and is indispensable for a functional immune system. We have, for the first time, engineered CAR T cells to overexpress ADA. To potentially improve the pharmacokinetic profile of ADA, we have modified the overexpressed ADA in two ways, through the incorporation of a (1) albumin-binding domain or (2) collagen-binding domain. ADA and modified ADA were successfully expressed by CAR T cells and augmented CAR T cell exhaustion resistance. In a preclinical engineered ovarian carcinoma xenograft model, ADA and collagen-binding ADA overexpression significantly enhanced CAR T cell expansion, tumor tissue infiltration, tumor growth control, and overall survival, whereas albumin-binding ADA overexpression did not. Furthermore, in a syngeneic colon cancer solid tumor model, the overexpression of mouse ADA by cancer cells significantly reduced tumor burden and remodeled the TME to favor antitumor immunity. The overexpression of ADA for enhanced cell therapy is a safe, straightforward, reproducible genetic modification that can be utilized in current CAR T cell constructs to result in an armored CAR T product with superior therapeutic potential.

Published

2022

16. Modulating Oncolytic Adenovirus Immunotherapy by Driving Two Axes of the Immune System by Expressing 4-1BBL and CD40L

Author

Brian J. Parrett, Michael A. Barry, Jack R. Hemsath, Michael J. Hansen, Brady Zell, and Shao-Chia Lu

Subjects

Oncolytic adenovirus, T cell, medicine.medical_treatment, CD40 Ligand, Melanoma, Experimental, chemical and pharmacologic phenomena, CD8-Positive T-Lymphocytes, Adenoviridae, Mice, Immune system, Antigen, Cell Line, Tumor, Genetics, medicine, Animals, Molecular Biology, CD40, biology, Immunotherapy, Oncolytic virus, Oncolytic Viruses, 4-1BB Ligand, medicine.anatomical_structure, Cancer cell, biology.protein, Cancer research, Molecular Medicine

Abstract

Oncolytic viruses can have utility for direct killing of cancer cells but may also serve to activate the immune system against cancer cells. While viruses alone can serve as immune stimulators, there is great interest in arming oncolytic viruses with the genes for immune stimulatory proteins to amplify their effects. In this work, we have tested the efficacy of a conditionally-replicating adenoviruses (CRAds) with and without selected immunostimulatory payloads in an immune competent mouse model of melanoma. Empty CRAd657 was compared to the same vector expressing mouse CD40L or mouse 4-1BBL. When CRAd657-m4-1BBL and CRAd657-mCD40L were injected into B16-hCAR murine melanoma tumors, both single vectors delayed tumor growth and prolong survival when compared to empty CRAd657. However, combined injection of both CRAd-4-1BBL and CRAd-CD40L mediated significantly better control of tumor growth. All of the payloads increased immune cell infiltration into tumors and notably reduced expression of PD-1 exhaustion marker on T cells. However, recruitment of CD8+ T cells was higher with 4-1BBL alone while CD40L expression induced more CD4+ T cell infiltration. Notably, the combination of CRAd657-4-1BBL and CRAd657-CD40L induced higher anti-TRP-2 tumor-associated antigen T cell responses than empty or single gene vectors. This combination also caused depigmentation in areas adjacent to the tumor sites in more animals. These data indicate that driving two axes of the immune system with combined immune stimulatory payloads can lead to improved anti-cancer immune responses and better tumor control in an immune competent model of cancer.

Published

2022

17. Mutant IDH Inhibits IFNγ–TET2 Signaling to Promote Immunoevasion and Tumor Maintenance in Cholangiocarcinoma

Author

Emily Kessler, Rodrigo Saad-Berreta, Hongwu Zheng, Vikram Deshpande, Krishna S. Tummala, Brandon Nicolay, William Shen, Ramzi Adil, Meng-Ju Wu, Juan Dubrot, Lipika Goyal, Vajira Weeresekara, Amaya Pankaj, Mathias Heikenwalder, Tong Wang, Mirian Fernandez-Vaquero, María García-Beccaria, Ting-Yu Wei, Kira E Olander, Sebastien Ronseaux, Vindhya Vijay, Qibiao Wu, Yuanli Zhen, Christine Hudson, Nabeel Bardeesy, Lei Shi, Rahul M. Kohli, Meiqi Luo, Yi Sun, Russell W. Jenkins, Robert T. Manguso, Cristina R. Ferrone, and Joshua Merritt

Subjects

T cell, Dioxygenases, Cholangiocarcinoma, Interferon-gamma, Mice, Immune system, Interferon, medicine, Animals, Humans, CTLA-4 Antigen, Receptor, biology, Chemistry, Isocitrate Dehydrogenase, Immune checkpoint, DNA-Binding Proteins, Bile Ducts, Intrahepatic, medicine.anatomical_structure, Isocitrate dehydrogenase, Bile Duct Neoplasms, Oncology, Mutation, Cancer research, biology.protein, Demethylase, CD8, medicine.drug

Abstract

Isocitrate dehydrogenase 1 mutations (mIDH1) are common in cholangiocarcinoma. (R)-2-hydroxyglutarate generated by the mIDH1 enzyme inhibits multiple α-ketoglutarate–dependent enzymes, altering epigenetics and metabolism. Here, by developing mIDH1-driven genetically engineered mouse models, we show that mIDH1 supports cholangiocarcinoma tumor maintenance through an immunoevasion program centered on dual (R)-2-hydroxyglutarate–mediated mechanisms: suppression of CD8+ T-cell activity and tumor cell–autonomous inactivation of TET2 DNA demethylase. Pharmacologic mIDH1 inhibition stimulates CD8+ T-cell recruitment and interferon γ (IFNγ) expression and promotes TET2-dependent induction of IFNγ response genes in tumor cells. CD8+ T-cell depletion or tumor cell–specific ablation of TET2 or IFNγ receptor 1 causes treatment resistance. Whereas immune-checkpoint activation limits mIDH1 inhibitor efficacy, CTLA4 blockade overcomes immunosuppression, providing therapeutic synergy. The findings in this mouse model of cholangiocarcinoma demonstrate that immune function and the IFNγ–TET2 axis are essential for response to mIDH1 inhibition and suggest a novel strategy for potentiating efficacy. Significance: Mutant IDH1 inhibition stimulates cytotoxic T-cell function and derepression of the DNA demethylating enzyme TET2, which is required for tumor cells to respond to IFNγ. The discovery of mechanisms of treatment efficacy and the identification of synergy by combined CTLA4 blockade provide the foundation for new therapeutic strategies. See related commentary by Zhu and Kwong, p. 604. This article is highlighted in the In This Issue feature, p. 587

Published

2022

18. Dual JAK2/Aurora kinase A inhibition prevents human skin graft rejection by allo-inactivation and ILC2-mediated tissue repair

Author

Megan J. Riddle, Nicholas J Lawrence, Jakub Tolar, Sang Y Yun, Heather E. Stefanski, Bruce R. Blazar, Kelly Walton, Michael A. Linden, Elizabeth M. Sagatys, Jane Yuet Ching Hui, Jongphil Kim, Yan Xing, Harshani Lawrence, Brian C. Betts, John V. Kiluk, Marie C. Lee, Said M. Sebti, Kirsti Walker, Joseph Pidala, Jordan Reff, Claudio Anasetti, and Brent H. Koehn

Subjects

Graft Rejection, T cell, Article, Mice, Immune system, Animals, Humans, Transplantation, Homologous, Immunology and Allergy, Medicine, Pharmacology (medical), STAT5, Aurora Kinase A, Transplantation, Innate immune system, biology, business.industry, Innate lymphoid cell, GATA3, Janus Kinase 2, Immunity, Innate, Mice, Inbred C57BL, medicine.anatomical_structure, biology.protein, Cancer research, Th17 Cells, business

Abstract

Prevention of allograft rejection often requires lifelong immune suppression, risking broad impairment of host immunity. Nonselective inhibition of host T cell function increases recipient risk of opportunistic infections and secondary malignancies. Here we demonstrate that AJI-100, a dual inhibitor of JAK2 and Aurora kinase A, ameliorates skin graft rejection by human T cells and provides durable allo-inactivation. AJI-100 significantly reduces the frequency of skin-homing CLA(+) donor T cells, limiting allograft invasion and tissue destruction by T effectors. AJI-100 also suppresses pathogenic Th1 and Th17 cells in the spleen yet spares beneficial regulatory T cells (Tregs). We show dual JAK2/Aurora kinase A blockade enhances human type 2 innate lymphoid cell (ILC2) responses, which are capable of tissue repair. ILC2 differentiation mediated by GATA3 requires STAT5 phosphorylation (pSTAT5) but is opposed by STAT3. Further, we demonstrate that Aurora kinase A activation correlates with low pSTAT5 in ILC2s. Importantly, AJI-100 maintains pSTAT5 levels in ILC2s by blocking Aurora kinase A and reduces interference by STAT3. Therefore, combined JAK2/Aurora kinase A inhibition is an innovative strategy to merge immune suppression with tissue repair after transplantation.

Published

2022

19. Evolution of SARS-CoV-2 immune responses in nursing home residents following full dose of the Comirnaty® COVID-19 vaccine

Author

Ignacio Torres, David Navarro, Paula Amat, María José Remigia, Juan Alberola, Estela Giménez, María José Beltrán, Eliseo Albert, Pilar Botija, Dixie Huntley, Beatriz Olea, María Jesús Alcaraz, and Celia Rodado

Subjects

Microbiology (medical), medicine.diagnostic_test, biology, Coronavirus disease 2019 (COVID-19), business.industry, T cell, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Flow cytometry, Vaccination, Infectious Diseases, medicine.anatomical_structure, Immune system, Immunology, medicine, biology.protein, Antibody, business, CD8

Abstract

ObjectivesThere is scarce information as to the durability of immune responses elicited by the Comirnaty® COVID-19 vaccine in nursing home residents. Here, we assessed SARS-CoV-2-Spike (S)-targeted antibody and functional T cell responses at around 6 months after complete vaccination.MethodsThe sample comprised 46 residents (34 females; age, 60-100 years), of whom 10 had COVID-19 prior to vaccination. Baseline (median of 17.5 days after vaccination) and follow-up (median, 195 days) plasma specimens were available for quantitation of SARS-CoV-2-S antibodies and enumeration of SARS-CoV-2-S-reactive IFN-γ CD4+ and CD8+ T cells by flow cytometry.ResultsIn total, 44/45 participants had detectable SARS-CoV-2-S antibodies at follow-up. Overall, antibody levels were found to decrease (median, 4.8 fold). Antibodies waning was more frequent (P+ T cells were detected in 33/46 and 24/46 at baseline and follow-up, respectively. The figures for CD4+ T cell counterparts were 12/46 and 30/46. Detectable SARS-CoV-2 IFN-γ CD8+ and CD4+ T cell responses at follow-up were more common in recovered (8/10 and 7/10, respectively) than in naïve residents (9/36 and 25/36, respectively). For those with detectable responses at both time points, SARS-CoV-2-S IFN-γ CD8+ T cell frequencies decreased significantly (P=0.001) over time whereas the opposite (P=0.01) was observed in CD4+ T cells.ConclusionAlmost all residents displayed detectable SARS-CoV-2-S-reactive antibodies and T cell responses, respectively, by around 6 months after complete vaccination with Comirnaty® COVID-19 vaccine, albeit generally waning in magnitude over time.

Published

2022

20. Enhancing CAR T function with the engineered secretion of C. perfringens neuraminidase

Author

Joseph S. Durgin, Zev A. Binder, Vijay Bhoj, Michael C. Milone, Donald M. O'Rourke, Radhika Thokala, Saba Ghassemi, Roddy S. O’Connor, Lexus R. Johnson, John Leferovich, and Edward Z Song

Subjects

Adoptive cell transfer, Clostridium perfringens, T cell, Antigens, CD19, Cell, Neuraminidase, Immunotherapy, Adoptive, Immune system, Cell Line, Tumor, Drug Discovery, Genetics, medicine, Humans, Molecular Biology, Pharmacology, Receptors, Chimeric Antigen, biology, Effector, Chemistry, Xenograft Model Antitumor Assays, Immune checkpoint, Cell biology, Cytolysis, medicine.anatomical_structure, biology.protein, Molecular Medicine

Abstract

Prior to adoptive transfer, CAR T cells are activated, lentivirally infected with CAR transgenes, and expanded over 9 to 11 days. An unintended consequence of this process is the progressive differentiation of CAR T cells over time in culture. Differentiated T cells engraft poorly, which limits their ability to persist and provide sustained tumor control in hematologic as well as solid tumors. Solid tumors include other barriers to CAR T cell therapies, including immune and metabolic checkpoints that suppress effector function and durability. Sialic acids are ubiquitous surface molecules with known immune checkpoint functions. The enzyme C. perfringens neuraminidase (CpNA) removes sialic acid residues from target cells, with good activity at physiologic conditions. In combination with galactose oxidase (GO), NA has been found to stimulate T cell mitogenesis and cytotoxicity in vitro. Here we determine whether CpNA alone and in combination with GO promotes CAR T cell antitumor efficacy. We show that CpNA restrains CAR T cell differentiation during ex vivo culture, giving rise to progeny with enhanced therapeutic potential. CAR T cells expressing CpNA have superior effector function and cytotoxicity in vitro. In a Nalm-6 xenograft model of leukemia, CAR T cells expressing CpNA show enhanced antitumor efficacy. Arming CAR T cells with CpNA also enhanced tumor control in xenograft models of glioblastoma as well as a syngeneic model of melanoma. Given our findings, we hypothesize that charge repulsion via surface glycans is a regulatory parameter influencing differentiation. As T cells engage target cells within tumors and undergo constitutive activation through their CARs, critical thresholds of negative charge may impede cell-cell interactions underlying synapse formation and cytolysis. Removing the dense pool of negative cell-surface charge with CpNA is an effective approach to limit CAR T cell differentiation and enhance overall persistence and efficacy.

Published

2022

21. Dynamic SARS-CoV-2-specific B-cell and T-cell responses following immunization with an inactivated COVID-19 vaccine

Author

Minxin Mao, Yue Yang, Yali Xiong, Ming Li, Han Shen, Jun Ni, Yuxin Chen, Chao Wu, Xin Tong, Shengxia Yin, Rui Huang, Jie Pan, Yawen Wan, Yue Tao, and Xiaomin Yan

Subjects

Microbiology (medical), COVID-19 Vaccines, T cell, Adaptive responses, T cells, Booster dose, Inactivated virus vaccine, CD8-Positive T-Lymphocytes, Virus, Neutralization, Immune system, Humans, Medicine, Prospective Studies, B cell, B cells, biology, SARS-CoV-2, business.industry, Vaccination, COVID-19, General Medicine, Infectious Diseases, medicine.anatomical_structure, Immunization, Immunology, biology.protein, Original Article, Antibody, business, CD8

Abstract

OBJECTIVE The dynamic adaptive immune responses elicited by the inactivated virus vaccine, CoronaVac, remain elusive. METHODS In a prospective cohort of 100 SARS-CoV-2 naïve healthcare professionals who received two doses of CoronaVac, we analyzed SARS-CoV-2-specific humoral and cellular responses at four different timepoints, including before vaccination (T1), 2 weeks after the first dose (T2), 2 weeks after the booster dose (T3), and 8-10 weeks post the booster dose (T4). SARS-CoV-2-specific antibodies, serum neutralizing activities, peripheral B cells, CD4+ and CD8+ T cells, and their memory subsets were simultaneously measured in this cohort. RESULTS SARS-CoV-2 Spike-specific IgG responses reached the peak (geometric mean titer [GMT] 54827, 30969-97065) after two doses and rapidly declined (GMT 502, 212-1190) at T4, whereas suboptimal IgA responses were detected (GMT 5, 2-9). Spike-specific circulating B cells (0.60%, 0.46-0.73% of total B cells) and memory B cells (1.18%, 0.92-1.44% of total memory B cells) were effectively induced at T3 and sustained over time (0.33%, 0.23-0.43%; 0.87%, 0.05-1.67%, respectively). SARS-CoV-2-specific circulating CD4+ T cells (0.57%, 0.47-0.66%) and CD8+ T cells (1.29%, 1.04-1.54%) were detected at T3. At T4, 0.78% (0.43-1.20%) of memory CD4+ T cells and 0.68% (0.29-1.30%) of memory CD8+ T cells were identified as SARS-CoV-2 specific, while 0.62% (0.51-0.75%) of CD4+ T cells and 0.47% (0.38-0.58%) of CD8+ T cells were SARS-CoV-2 specific terminally differentiated effector memory cells. Furthermore, age and interval between doses affected the magnitude of CoronaVac induced immune responses. SARS-CoV-2 memory CD4+ T cells was strongly associated with both RBD-specific memory B cells (r=0.87, p, Graphical abstract Image 1

Published

2022

22. Engineered extracellular vesicles for concurrent Anti-PDL1 immunotherapy and chemotherapy

Author

Lixue Wang, Chuandong Zhu, Yiqiu Xia, Wenjun Mao, Guosheng Wang, Yundi Chen, Ming-feng Zheng, Ethan J. Blumenthal, and Yuan Wan

Subjects

QH301-705.5, medicine.drug_class, medicine.medical_treatment, T cell, Cell, Biomedical Engineering, Monoclonal antibody, PD-1/PD-L1, Article, Biomaterials, Immune checkpoint inhibitors, medicine, Biology (General), Cytotoxicity, CRISPR/Cas9, Materials of engineering and construction. Mechanics of materials, biology, Chemistry, Immunotherapy, Extracellular vesicles, medicine.anatomical_structure, Apoptosis, Drug delivery, PARP inhibitor, TA401-492, Cancer research, biology.protein, Antibody, Biotechnology

Abstract

Immune checkpoint inhibitors (ICI) targeting PD-1/PD-L1 have been approved for the treatment of a variety of cancers. However, the efficacy of antibody-based ICIs could be further improved by mitigating anti-drug antibodies, proteolytic cleavage, and on-target off-tumor toxicity. One strategy for accomplishing this is through the use of extracellular vesicles (EVs), cell derived submicron vesicles with many unique properties. We constructed an engineered MDA-MB-231 cell line for harvesting EVs. This was accomplished by overexpressing a high-affinity variant human PD-1 protein (havPD-1), while simultaneously knocking out intrinsic PD-L1 and beta-2 microglobulin. The engineered havPD-1 EVs reduced PD-L1 overexpressing cancer cell proliferation and induced cellular apoptosis. Moreover, the EVs were shown to efficiently block PD-L1 mediated T cell suppression. Meanwhile antibody-dependent cellular cytotoxicity and complement-dependent cytotoxicity were not observed. The havPD-1 EVs treatment resulted in robust anti-tumor activity in both preventative co-implantation and therapeutic xenograft tumor models reconstituted with human T cells. The efficacy of the havPD-1 EVs was shown to be comparable to clinical anti-PD1 monoclonal antibodies. Additionally, loading the havPD-1 EVs with a potent PARP inhibitor was shown to further augment treatment efficacy. In brief, the engineered universal EVs harboring havPD-1 proteins can be used for cancer concurrent immunotherapy and chemotherapy., Graphical abstract Universal extracellular vesicles as immune checkpoint inhibitors and chemotherapeutics nanocarriers for cancer combination therapy.Image 1, Highlights • It is the first attempt to develop extracellular vesicles (EV) as direct agents for immune checkpoint therapy. • The HLA-I knock-out EVs could be off-the-self universal donors for EV-based therapy. • The EV-based concurrent immunotherapy and chemotherapy can significantly improve treatment efficacy.

Published

2022

23. Characterization of Immunophenotypic Aberrancies with Respect to Common Fusion Transcripts in B-Cell Precursor Acute Lymphoblastic Leukemia: A Report of 986 Indian Patients

Author

Ashish Kumar, Dikshat Gopal Gupta, Alka Khadwal, Jogeshwar Binota, Pankaj Malhotra, Parveen Bose, Preeti Sonam, Shano Naseem, Palak Rana, Man Updesh Singh Sachdeva, Subhash Varma, Amita Trehan, Minakshi Gupta, and Neelam Varma

Subjects

Adult, Male, Myeloid, Lineage (genetic), Oncogene Proteins, Fusion, T cell, CD33, India, Immunophenotyping, Cohort Studies, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, hemic and lymphatic diseases, Humans, Medicine, Child, B cell, biology, business.industry, CD117, Hematology, medicine.anatomical_structure, Fusion transcript, Acute Disease, Cancer research, biology.protein, Female, business

Abstract

Objective Based upon the immunophenotype, acute lymphoblastic leukaemia (ALL) can be categorized into B or T cell lineage (B-cell ALL or T-cell ALL). B-cell precursor ALL (BCP-ALL) cases show various genetic/molecular abnormalities and varying frequencies of chimeric fusion transcripts in BCP-ALL cases are reported from different parts of the world. We studied the immunophenotypic aberrancy profiles of a large number of BCP-ALL cases with respect to various common chimeric fusion transcripts. Materials and methods Flowcytometric Immunophenotyping and Multiplex RT-PCR assay were performed in 986 BCP-ALL cases. Results Among 986 BCP-ALL cases, the incidence of various fusion transcripts was 38.36% in adult cases and 20.68% in pediatric cases. Adult BCP-ALL cases harbouring t(9;22)(BCR-ABL1) fusion transcripts and having expression of aberrant myeloid markers, were significantly older at presentation (age, p=0.0218) and had male preponderance (male, p=0.0246), as compared to those without aberrant myeloid expression. In pediatric cases expressing t(12;21)(ETV6-RUNX1) chimeric fusion transcript, aberrant expression of CD13 was observed in 39.13%, CD33 in 36.95% and CD117 in 8.69% patients respectively. Pediatric BCP-ALL cases harbouring ETV6-RUNX1 fusion transcript and having expression of aberrant myeloid markers were not significantly different as compared to those without, with respect to their demographic and clinico-hematological characteristics (p=0.5955). Aberrant myeloid markers were rarely/never expressed in pediatric and adult BCP-ALL patients harbouring t(4;11)(KTM2A-AF4) and t(1;19)(TCF3-PBX1) fusion transcripts. Conclusion Aberrant myeloid markers were frequently expressed among BCP-ALL patients harbouring t(9;22)(BCR-ABL1) and t(12;21)(ETV6-RUNX1) fusion transcripts. However BCP-ALL patients harbouring t(4;11)(KTM2A-AF4) and t(1;19)(TCF3-PBX1) fusion transcripts rarely/ never expressed aberrant myeloid markers. Aberrant myeloid CD markers can be used in predicting chimeric fusion transcripts at baseline, so as to plan desirable TKI therapy in BCP-ALL cases with specific chimeric fusion transcripts. This study delineates the relationship of chimeric fusion transcripts with the aberrant expression of myeloid markers in a large cohort of BCP-ALL cases.

Published

2022

24. Asxl1 loss cooperates with oncogenic Nras in mice to reprogram the immune microenvironment and drive leukemic transformation

Author

Ross L. Levine, Jing Zhang, Fabao Liu, Alexis Vedder, Xin Gao, Sergey Nikolaev, Mrinal M. Patnaik, Abhishek A. Mangaonkar, Yun Zhou, Kalyan Vara Ganesh Nadiminti, Anthony M. Hunter, Terra L. Lasho, Wei Xu, Evan Flietner, Erik A. Ranheim, Xiaona You, Ruiqi Liao, Klaus Geissler, Eric Padron, Nathalie Droin, Guangyao Kong, Moritz Binder, Eric Solary, Maria E. Balasis, Christy Finke, Britta Will, Omar Abdel-Wahab, Adhithi Rajagopalan, Zhi Wen, and David T. Yang

Subjects

Neuroblastoma RAS viral oncogene homolog, Myeloid, T cell, Immunology, Biology, Biochemistry, GTP Phosphohydrolases, Mice, TIGIT, hemic and lymphatic diseases, Tumor Microenvironment, medicine, Animals, Humans, Monomeric GTP-Binding Proteins, Myeloid Neoplasia, Membrane Proteins, Myeloid leukemia, Leukemia, Myelomonocytic, Chronic, Cell Biology, Hematology, medicine.disease, Immune checkpoint, Repressor Proteins, Disease Models, Animal, Leukemia, Myeloid, Acute, Leukemia, Phenotype, medicine.anatomical_structure, Mutation, Cancer research, CD80, Signal Transduction

Abstract

Mutations in chromatin regulator ASXL1 are frequently identified in myeloid malignancies, in particular ∼40% of patients with chronic myelomonocytic leukemia (CMML). ASXL1 mutations are associated with poor prognosis in CMML and significantly co-occur with NRAS mutations. Here, we show that concurrent ASXL1 and NRAS mutations defined a population of CMML patients who had shorter leukemia-free survival than those with ASXL1 mutation only. Corroborating this human data, Asxl1−/− accelerated CMML progression and promoted CMML transformation to acute myeloid leukemia (AML) in NrasG12D/+ mice. NrasG12D/+;Asxl1−/− (NA) leukemia cells displayed hyperactivation of MEK/ERK signaling, increased global levels of H3K27ac, upregulation of Flt3. Moreover, we find that NA-AML cells overexpressed all the major inhibitory immune checkpoint ligands: programmed death-ligand 1 (PD-L1)/PD-L2, CD155, and CD80/CD86. Among them, overexpression of PD-L1 and CD86 correlated with upregulation of AP-1 transcription factors (TFs) in NA-AML cells. An AP-1 inhibitor or short hairpin RNAs against AP-1 TF Jun decreased PD-L1 and CD86 expression in NA-AML cells. Once NA-AML cells were transplanted into syngeneic recipients, NA-derived T cells were not detectable. Host-derived wild-type T cells overexpressed programmed cell death protein 1 (PD-1) and T-cell immunoreceptor with immunoglobulin and ITIM domains (TIGIT) receptors, leading to a predominant exhausted T-cell phenotype. Combined inhibition of MEK and BET resulted in downregulation of Flt3 and AP-1 expression, partial restoration of the immune microenvironment, enhancement of CD8 T-cell cytotoxicity, and prolonged survival in NA-AML mice. Our study suggests that combined targeted therapy and immunotherapy may be beneficial for treating secondary AML with concurrent ASXL1 and NRAS mutations.

Published

2022

25. Pembrolizumab for B-cell lymphomas relapsing after or refractory to CD19-directed CAR T-cell therapy

Author

Simon F. Lacey, Stephen J. Schuster, Elise A. Chong, Sunita D. Nasta, Jakub Svoboda, Marco Ruella, Siddharth Bhattacharyya, E. John Wherry, Cécile Alanio, and Daniel J. Landsburg

Subjects

Adult, Male, Oncology, medicine.medical_specialty, Lymphoma, B-Cell, T cell, Antigens, CD19, Immunology, Pembrolizumab, Neutropenia, Antibodies, Monoclonal, Humanized, Immunotherapy, Adoptive, Biochemistry, CD19, Antineoplastic Agents, Immunological, Refractory, Antigen, Internal medicine, medicine, Humans, Prospective Studies, Adverse effect, B cell, Aged, Salvage Therapy, Receptors, Chimeric Antigen, biology, business.industry, Cell Biology, Hematology, Middle Aged, Prognosis, medicine.disease, medicine.anatomical_structure, biology.protein, Female, Blood Commentary, Neoplasm Recurrence, Local, business, Follow-Up Studies

Abstract

CD19-directed chimeric antigen receptor–modified (CAR T) T cells achieve durable remissions in about 30% to 40% of relapsed/refractory large B-cell lymphomas. T-cell exhaustion and/or an immunosuppressive tumor microenvironment may contribute to CAR T-cell failure. Pembrolizumab, an anti-PD1 immune checkpoint inhibitor, may reverse T-cell exhaustion after CAR T-cell therapy. We treated 12 patients with B-cell lymphomas who were either refractory to (n = 9) or relapsed after (n = 3) CD19-directed CAR T-cell (4-1BB–costimulated) therapy with pembrolizumab 200 mg IV every 3 weeks. Median time from CAR T-cell infusion to first pembrolizumab dose was 3.3 months (range, 0.4-42.8 months). Pembrolizumab was well tolerated, and the only grade ≥3 adverse events related to pembrolizumab were neutropenia (n = 3; 25%). Best overall response rate after pembrolizumab was 25% (3 of 12 patients; 1 complete response; 2 partial responses). One (8%) patient had stable disease; thus, 4 of 12 (33%) patients had clinical benefit. After pembrolizumab, 4 patients with clinical benefit had an increase in percentage of CAR T cells by mass cytometry by time of flight (CyTOF); 3 of 4 of these patients also had increases in CAR19 transgene levels by quantitative polymerase chain reaction. Deep immune profiling using CyTOF revealed increased CAR T-cell activation and proliferation and less T-cell exhaustion in clinical responders. Together, PD1 blockade with pembrolizumab after CD19-directed CAR T-cell therapy appears safe and may achieve clinical responses in some patients with B-cell lymphomas refractory to or relapsed after CAR T-cell therapy. This trial was registered at www.clinicaltrials.gove as #NCT02650999.

Published

2022

26. Local and Systemic T Cell Immunity in Fighting Pig Viral and Bacterial Infections

Author

Wilhelm Gerner, Selma Schmidt, and Kerstin H. Mair

Subjects

General Veterinary, biology, Swine, T-Lymphocytes, T cell, Porcine Reproductive and Respiratory Syndrome, Bacterial Infections, biology.organism_classification, Porcine reproductive and respiratory syndrome virus, Acquired immune system, African Swine Fever Virus, Virology, African swine fever virus, Virus, medicine.anatomical_structure, Orthomyxoviridae Infections, Antigen, Classical swine fever, Genetics, medicine, Animals, Porcine respiratory and reproductive syndrome virus, Animal Science and Zoology, CD8, Biotechnology

Abstract

T cells are an essential component of the adaptive immune system. Over the last 15 years, a constantly growing toolbox with which to study T cell biology in pigs has allowed detailed investigations on these cells in various viral and bacterial infections. This review provides an overview on porcine CD4, CD8, and γδ T cells and the current knowledge on the differentiation of these cells following antigen encounter. Where available, the responses of these cells to viral infections like porcine reproductive and respiratory syndrome virus, classical swine fever virus, swine influenza A virus, and African swine fever virus are outlined. In addition, knowledge on the porcine T cell response to bacterial infections like Actinobacillus pleuropneumoniae and Salmonella Typhimurium is reviewed. For CD4 T cells, the response to the outlined infections is reflected toward the Th1/Th2/Th17/Tfh/Treg paradigm for functional differentiation. Expected final online publication date for the Annual Review of Animal Biosciences, Volume 10 is February 2022. Please see http://www.annualreviews.org/page/journal/pubdates for revised estimates.

Published

2022

27. Extrafollicular PD-1highCXCR5–CD4+ T cells participate in local immunoglobulin production in nasal polyps

Author

Hong-Xia Ding, Bo Liao, Jia Song, Zhi-Chao Wang, Zheng Liu, Nan Wang, Cai-Ling Chen, Yin Yao, Cui-Lian Guo, Di Yu, Yang Yang, Zhe-Zheng Wang, and Xue-Li Li

Subjects

biology, medicine.diagnostic_test, Chemistry, T cell, Immunology, Germinal center, respiratory system, Immunoglobulin E, Molecular biology, Flow cytometry, medicine.anatomical_structure, CTLA-4, biology.protein, medicine, Immunology and Allergy, Antibody, CXCL13, CC chemokine receptors

Abstract

Background Local immunoglobulin hyperproduction is observed in nasal polyps (NPs) with and without ectopic lymphoid tissues (eLTs). Objective Our aim was to identify the T-cell subsets involved in local immunoglobulin production independent of eLTs in NPs. Methods The localization, abundance, and phenotype of CD4+ T-cell subsets were studied by immunofluorescence, flow cytometry, and single-cell RNA sequencing. Purified nasal T-cell subsets were cultured with autologous peripheral naive B cells to explore their function. Programmed death ligand 1 and programmed death ligand 2 expression in NPs was investigated by immunofluorescence staining and flow cytometry. Results Accumulation of PD-1highCXCR5–CD4+ T cells outside lymphoid aggregates was found in NPs. Nasal PD-1highCXCR5–CD4+ T cells were characterized by a unique phenotype that was related to B-cell help and tissue residency and distinct from PD-1–/intCXCR5– and CXCR5+ CD4+ T cells in NPs as well as PD-1highCXCR5highCD4+ follicular helper T cells in tonsils. Compared with the frequencies of PD-1highCXCR5–CD4+ T cells and their IFN-γ+, IL-17A+, and IL-21+ subsets in the control inferior turbinate tissues, the frequencies of these cells and their subsets were increased in both eosinophilic and noneosinophilic NPs, whereas the frequencies of the IL-4+ and IL-4+IL-21+ subsets were increased only in eosinophilic NPs. Nasal PD-1highCXCR5–CD4+ T cells induced immunoglobulin production from B cells in a potency comparable to that induced by tonsillar follicular helper T cells. PD-1highCXCR5–CD4+ T-cell frequencies were correlated with IgE levels in eosinophilic NPs. PD-L1 and PD-L2 suppressed the function of PD-1highCXCR5–CD4+ T cells, and their levels were reduced in NPs. PD-1highCXCR5–CD4+ T-cell abundance was associated with the postsurgical relapse of NPs. Conclusion PD-1highCXCR5–CD4+ T cells participate in local immunoglobulin production independent of eLTs in NPs.

Published

2022

28. Prolonged severe acute respiratory syndrome coronavirus 2 persistence, attenuated immunologic response, and viral evolution in a solid organ transplant patient

Author

Marlena V. Habal, Lihong Liu, Brian E. Scully, Jayesh Shah, Lawrence J Purpura, Anne-Catrin Uhlemann, Medini K. Annavajhala, Benjamin A. Miko, Marcus R. Pereira, Nicola Medrano, Michelle Chang, Michael T. Yin, Hiroshi Mohri, Justin C Laracy, Anyelina Cantos, David D. Ho, and Moriya Tsuji

Subjects

Transplantation, biology, business.industry, viruses, medicine.medical_treatment, T cell, Cytokine, medicine.anatomical_structure, Immune system, Viral replication, Viral evolution, Immunology, medicine, biology.protein, Immunology and Allergy, Pharmacology (medical), Antibody, business, Neutralizing antibody, Viral load

Abstract

Unlike immunocompetent hosts, the duration of viral persistence after infection with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) can be prolonged in immunosuppressed patients. Here, we present a case of viral persistence for over 19 weeks in a patient with a history of solid organ transplant and explore the clinical, virologic, and immunologic course. Our patient still demonstrated viral persistence at 138 days with low polymerase chain reaction cycle threshold values and evidence of continuing viral sequence evolution indicative of ongoing virus replication. These findings have important implications for infection prevention and control recommendations in immunosuppressed patients. Immune response, including neutralizing antibody titers, T cell activity, and cytokine levels, peaked around days 44-72 after diagnosis. Anti-S trimer antibodies were low at all time points, and T cell response was attenuated by day 119. As immune response waned and viral load increased, increased genetic diversity emerged, suggesting a mechanism for the development of viral variants.

Published

2022

29. Exploiting T cell signaling to optimize engineered T cell therapies

Author

Lianjun Shen, Chenqi Xu, Haopeng Wang, Xinxin Wang, and Xianming Song

Subjects

Cancer Research, Receptors, Chimeric Antigen, T-Lymphocytes, T cell, Cell, T-cell receptor, Biology, Immunotherapy, Adoptive, Chimeric antigen receptor, Cell biology, Chimera (genetics), medicine.anatomical_structure, Immune system, Oncology, Antigen, Neoplasms, medicine, Humans, Receptor, Signal Transduction

Abstract

Engineered T cell therapies, mainly chimeric antigen receptor (CAR)-T and T cell receptor (TCR)-T, have become the new frontier of cancer treatment. CAR-T and TCR-T therapies differ in many aspects, including cell persistence and toxicity, leading to different therapeutic outcomes. Both TCR and CAR recognize antigens and trigger T cell mediated antitumor response, but they have distinct molecular structures and signaling properties. TCR represents one of the most complex receptors, while CAR is a single-chain chimera integrating modules from multiple immune receptors. Understanding the mechanisms underlying the strengths and limitations of both systems can pave the way for the development of next-generation T cell therapy. This review synthesizes recent findings on TCR and CAR signaling and highlights the potential strategies of T cell engineering by signaling refinement.

Published

2022

30. Interleukin-33 Reinvigorates Antiviral Function of Viral-Specific CD8+ T Cells in Chronic Hepatitis B Virus Infection

Author

Tao Yu, Jing Yu, Xiaoju Shi, and Chao Li

Subjects

Granzyme B production, Hepatitis B virus, T cell, Immunology, Interleukin, Biology, medicine.disease_cause, Virology, Interleukin 33, medicine.anatomical_structure, Antigen, medicine, Molecular Medicine, Cytotoxic T cell, CD8

Abstract

Restoration of exhausted hepatitis B virus (HBV)-specific CD8+ T cells is one of the important strategies for inhibition of viral replication. The role of interleukin (IL)-33 to recovery of CD8+ T cell activity is not fully elucidated. We investigated the effect of IL-33 on viral-specific CD8+ T cell responses in chronic hepatitis B (CHB) patients in vitro by both phenotypic and functional analysis. Plasma IL-33 was downregulated in CHB patients, while effective antiviral therapy rescued IL-33 expression. There was no significant difference of IL-33 receptor mRNA relative level in CD8+ T cells between CHB patients and controls. IL-33 induced the proliferation of HBV-specific CD8+ T cells, and reduced programmed death-1 expression on HBV-specific CD8+ T cells. IL-33 promoted the direct cytolytic activity of CD8+ T cells against HepG2.2.15 cells through boosting perforin and granzyme B production. Furthermore, IL-33 administration increased HBV-specific CD8+ T cell-mediated HBV replication and HBV antigen secretion mainly via enhancement of interferon-γ and tumor necrosis factor-α. IL-33 reinvigorated antiviral activity of HBV-specific CD8+ T cells, revealing that IL-33 might contribute to viral clearance in persistent HBV infection.

Published

2022

31. Epigenetic networks driving T cell identity and plasticity during immunosenescence

Author

Beatriz Suarez-Alvarez, Carlos López-Larrea, Maria Laura Saiz, and Ramon M. Rodriguez

Subjects

Epigenomics, Immunosenescence, T-Lymphocytes, animal diseases, T cell, Identity (social science), chemical and pharmacologic phenomena, biochemical phenomena, metabolism, and nutrition, Biology, Epigenesis, Genetic, Immune system, medicine.anatomical_structure, Genetics, medicine, bacteria, Epigenetics, Neuroscience

Abstract

The aging process is associated with the accumulation of epigenetic alterations in immune cells, although the origin of these changes is not clear. Understanding this epigenetic drift in the immune system can provide essential information about the progression of the aging process and the immune history of each individual.

Published

2022

32. Targeting transforming growth factor-β2 by antisense oligodeoxynucleotide accelerates T cell-mediated tumor rejection in a humanized mouse model of triple-negative breast cancer

Author

Hyeong-Jin Ji, Sang-Kyung Shin, Jun-Eui Park, Jihye Koo, Tae Hun Kim, Kyung-Chul Choi, Hong Kyu Lee, Cho-Won Kim, and Yeon Hee Seong

Subjects

Cancer Research, T cell, Immunology, Triple Negative Breast Neoplasms, Biology, T-Lymphocytes, Regulatory, Oligodeoxyribonucleotides, Antisense, Mice, Transforming Growth Factor beta2, Text mining, medicine, Animals, Humans, Immunology and Allergy, Triple-negative breast cancer, Antisense oligodeoxynucleotides, business.industry, Disease Models, Animal, medicine.anatomical_structure, Oncology, Tumor rejection, Humanized mouse, Cancer research, Leukocytes, Mononuclear, business, Transforming growth factor

Abstract

Background: Transforming growth factor (TGF-β) pathway mediates suppression of anti-tumor immunity, and is associated with poor prognosis in triple-negative breast cancer (TNBC). Methods: In this study, we generated a humanized animal model by transplanting human peripheral blood mononuclear cells into immunodeficient mice followed by inoculation of MDA-MB-231 cells, and subsequently analyzed the role of TGF-β2 in the interaction between human T cells and human tumor cells. Results: Following reconstitution of the human immune system, inhibition of TGF-β signaling by TGF-β2 antisense oligodeoxynucleotide (TASO) resulted in accelerated tumor growth inhibition. TGF-β2 inhibition also resulted in downregulation of peripheral Foxp3+ regulatory T cells (Treg), whereas no effect was seen in the expression of CD8+ cytotoxic T cells. Analysis of the TASO-treated mice serum revealed elevated levels of human IFN-γ and reduced levels of human IL-10 and TGF-β2. Moreover, TGF-β2 inhibition resulted in increased CD8+ T cell infiltration, whereas the reduced infiltration of Tregs into the tumor partly resulted from decreased expression of CCL22. Decreased intra-tumoral Tregs facilitated the activation of cytotoxic T cells, associated with increased granzyme B expression. Conclusion: These results indicate that TASO potentiated T-cell mediated antitumor immunity, and it is proposed that TGF-β2 may be a promising target in the immunotherapeutic strategy of TNBC.

Published

2022

33. Alterations in T-Cell Transcription Factors and Cytokine Gene Expression in Late-Onset Alzheimer’s Disease

Author

Mina Makvand, Arezoo Campbell, Seyed Kazem Malakouti, Leila Kamalzadeh, Ghasem Ahangari, and Masoud Neshan

Subjects

Male, T cell, Late onset, GATA3 Transcription Factor, Disease, Biology, Interferon-gamma, Alzheimer Disease, medicine, Humans, Cytokine genes, RNA, Messenger, Age of Onset, Transcription factor, Aged, Aged, 80 and over, Tumor Necrosis Factor-alpha, General Neuroscience, General Medicine, Psychiatry and Mental health, Clinical Psychology, medicine.anatomical_structure, Gene Expression Regulation, Case-Control Studies, Immunology, Leukocytes, Mononuclear, Th17 Cells, Female, Geriatrics and Gerontology, T-Box Domain Proteins

Abstract

Background: Late-onset Alzheimer’s disease (LOAD) is associated with many environmental and genetic factors. The effect of systemic inflammation on the pathogenesis of neurodegenerative diseases such as AD has been strongly suggested. T helper cells (Th) are one of the important components of the immune system and can easily infiltrate the brain in pathological conditions. The development of each Th-subset depends on the production of unique cytokines and their main regulator. Objective: This study aimed to compare the mRNA levels of Th-related genes derived from peripheral blood mononuclear cells of LOAD patients with control. Also, the identification of the most important Th1/Th2 genes and downstream pathways that may be involved in the pathogenesis of AD was followed by computational approaches. Methods: This study involved 30 patients with LOAD and 30 non-demented controls. The relative expression of T-cell cytokines (IFN-γ, TNF-α, IL-4, and IL-5) and transcription factors (T-bet and GATA-3) were assessed using Real-time PCR. Additionally, protein-protein interaction (PPI) was investigated by gene network construction. Results: A significant decrease at T-bet, IFN-γ, TNF-α, and GATA-3 mRNA levels was detected in the LOAD group, compared to the controls. However, there was no significant difference in IL-4 or IL-5 mRNA levels. Network analysis revealed a list of the highly connected protein (hubs) related to mitogen-activated protein kinase (MAPK) signaling and Th17 cell differentiation pathways. Conclusion: The findings point to a molecular dysregulation in Th-related genes, which can promising in the early diagnosis or targeted interventions of AD. Furthermore, the PPI analysis showed that upstream off-target stimulation may involve MAPK cascade activation and Th17 axis induction.

Published

2022

34. Immunomodulation and RNA interference alter hepatitis B virus–specific CD8 T‐cell recognition of infected HepG2‐NTCP

Author

Adrian Kuipery, Aman Mehrotra, Harry L.A. Janssen, Jordan J. Feld, Adam J. Gehring, and Juan Diego Sanchez Vasquez

Subjects

Hepatitis B virus, HBsAg, T cell, Antigen presentation, CD8-Positive T-Lymphocytes, Biology, medicine.disease_cause, Immunomodulation, Hepatitis B, Chronic, Immune system, Antigen, medicine, Humans, Cytotoxic T cell, Tenofovir, Hepatology, virus diseases, Virology, digestive system diseases, HBcAg, medicine.anatomical_structure, Toll-Like Receptor 7, Toll-Like Receptor 8, Culture Media, Conditioned, Interferon Type I, RNA Interference

Abstract

BACKGROUND & AIMS CD8 T cells are essential in controlling Hepatitis B virus (HBV) infection. Viral control is dependent on efficient recognition of HBV-infected hepatocytes by CD8 T cells, which can induce direct lysis of infected hepatocytes. In addition, CD8 T cells produce IFN-γ, which mediates non-cytopathic viral clearance. Innate immunomodulators and HBV-targeted RNA interference (RNAi) are being developed to treat chronic hepatitis B, but may modify HBV antigen presentation and impact CD8 T cell recognition, in addition to their primary mechanisms of action. APPROACH & RESULTS HBV infected HepG2-NTCP were treated with tenofovir disoproxil fumarate (TDF), Toll-like receptor (TLR) 7/8 agonists, TLR7/8 conditioned media (CM) collected from immune cells, or RNAi using short-interfering RNAs (siRNAs). The effect of these treatments on antigen presentation was measured through co-culture with CD8 T cells recognizing HLA-A0201 restricted epitopes, HBc18-27 or HBs183-191. Cytokine profiles of TLR7/8 CM was measured using cytometric bead array. TDF reduced viral replication, but not CD8 T cell recognition of infected cells. Direct exposure of infected HepG2-NTCP to TLR7/8 agonists had no impact on T cell recognition. Exposure of infected HepG2-NTCP to TLR7/8 CM enhanced HBV-specific CD8 T cell recognition through type 1 interferon (IFN) and IFN-γ dependent mechanisms. RNAi rapidly suppressed HBV DNA, HBV Core antigen (HBcAg), and HBV S antigen (HBsAg) expression, impairing recognition by HBV-specific CD8 T cells. CONCLUSIONS Immunomodulation, and RNAi, but not nucleos(t)ide analogues, alter recognition of infected HepG2-NTCP by HBV-specific CD8 T cells. Understanding these changes will inform combination treatments for CHB.

Published

2022

35. APOBEC Mutagenesis Inhibits Breast Cancer Growth through Induction of T cell–Mediated Antitumor Immune Responses

Author

Elizabeth A Mendes, Sarah C. Van Alsten, Jeremy Force, Brock McKinney, Ashley V. DiMarco, Kouros Owzar, Jichun Xie, Nina Marie G. Garcia, Melissa A. Troester, Xiaodi Qin, Brent A. Hanks, and James V. Alvarez

Subjects

APOBEC, Cancer Research, T-Lymphocytes, medicine.medical_treatment, T cell, Immunology, Mice, Nude, Breast Neoplasms, Biology, Article, Mice, Breast cancer, Immune system, Antigens, Neoplasm, Cell Line, Tumor, Tumor Microenvironment, medicine, Animals, Humans, APOBEC Deaminases, Mice, Inbred BALB C, Mammary tumor, Immunogenicity, Cancer, Immunotherapy, medicine.disease, Xenograft Model Antitumor Assays, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Mutagenesis, Mutation, Cancer research, Female

Abstract

The APOBEC family of cytidine deaminases is one of the most common endogenous sources of mutations in human cancer. Genomic studies of tumors have found that APOBEC mutational signatures are enriched in the HER2 subtype of breast cancer and are associated with immunotherapy response in diverse cancer types. However, the direct consequences of APOBEC mutagenesis on the tumor immune microenvironment have not been thoroughly investigated. To address this, we developed syngeneic murine mammary tumor models with inducible expression of APOBEC3B. We found that APOBEC activity induced antitumor adaptive immune responses and CD4+ T cell–mediated, antigen-specific tumor growth inhibition. Although polyclonal APOBEC tumors had a moderate growth defect, clonal APOBEC tumors were almost completely rejected, suggesting that APOBEC-mediated genetic heterogeneity limits antitumor adaptive immune responses. Consistent with the observed immune infiltration in APOBEC tumors, APOBEC activity sensitized HER2-driven breast tumors to anti–CTLA-4 checkpoint inhibition and led to a complete response to combination anti–CTLA-4 and anti-HER2 therapy. In human breast cancers, the relationship between APOBEC mutagenesis and immunogenicity varied by breast cancer subtype and the frequency of subclonal mutations. This work provides a mechanistic basis for the sensitivity of APOBEC tumors to checkpoint inhibitors and suggests a rationale for using APOBEC mutational signatures and clonality as biomarkers predicting immunotherapy response in HER2-positive (HER2+) breast cancers.

Published

2022

36. Stereotypic Expansion of T Regulatory and Th17 Cells during Infancy Is Disrupted by HIV Exposure and Gut Epithelial Damage

Author

Susan Holmes, Katie Lennard, Catherine A. Blish, Agano Kiravu, Clive M. Gray, Heather B. Jaspan, Berenice Alinde, Melanie S.S. Seabrook, and Sonwabile Dzanibe

Subjects

T cell, Immunology, CCR4, hemic and immune systems, chemical and pharmacologic phenomena, Biology, Article, CCL20, medicine.anatomical_structure, Immune system, In utero, Cord blood, medicine, Immunology and Allergy, CCL17, Homing (hematopoietic)

Abstract

Few studies have investigated immune cell ontogeny throughout the neonatal and early pediatric period, when there is often increased vulnerability to infections. In this study, we evaluated the dynamics of two critical T cell populations, T regulatory (Treg) cells and Th17 cells, over the first 36 wk of human life. First, we observed distinct CD4+ T cells phenotypes between cord blood and peripheral blood, collected within 12 h of birth, showing that cord blood is not a surrogate for newborn blood. Second, both Treg and Th17 cells expanded in a synchronous fashion over 36 wk of life. However, comparing infants exposed to HIV in utero, but remaining uninfected, with HIV-unexposed uninfected control infants, there was a lower frequency of peripheral blood Treg cells at birth, resulting in a delayed expansion, and then declining again at 36 wk. Focusing on birth events, we found that Treg cells coexpressing CCR4 and α4β7 inversely correlated with plasma concentrations of CCL17 (the ligand for CCR4) and intestinal fatty acid binding protein, IL-7, and CCL20. This was in contrast with Th17 cells, which showed a positive association with these plasma analytes. Thus, despite the stereotypic expansion of both cell subsets over the first few months of life, there was a disruption in the balance of Th17 to Treg cells at birth likely being a result of gut damage and homing of newborn Treg cells from the blood circulation to the gut.

Published

2022

37. Humoral response to the BBIBP-CorV vaccine over time in healthcare workers with or without exposure to SARS-CoV-2

Author

Victoria Ramos, Maria M.E. de Bracco, Roberto Gabriel Pozner, Georgina Wigdorovitz, Luis A. Castillo, Matias Javier Pereson, Natalia Aloisi, Ana Colado, Maria Noel Badano, Irene Angélica Keitelman, Patricia Baré, Juan Manuel Ortiz Wilczynski, Florencia Sabbione, Roberto Chuit, and S. Fink

Subjects

Adult, Male, COVID-19 Vaccines, T cell, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Health Personnel, T-Lymphocytes, Immunology, Antibodies, Viral, Article, Persistence (computer science), BBIBP-CorV, medicine, Humans, Humoral response, Seroconversion, Molecular Biology, Aged, Aged, 80 and over, B-Lymphocytes, biology, Multivariable linear regression, business.industry, SARS-CoV-2, SARS-CoV-2 infection, Vaccination, Antibody titer, COVID-19, Middle Aged, Anti-spike antibodies, medicine.anatomical_structure, Vaccines, Inactivated, biology.protein, Female, Antibody, business

Abstract

SARS-CoV-2-specific humoral response was analyzed over time in a group of healthcare workers with or without exposure to SARS-CoV-2, who underwent vaccination with BBIBP-CorV (Sinopharm) vaccine in Argentina.Seroconversion rates in unexposed subjects after the first and second doses were 40% and 100%, respectively, showing a significant increase in antibody concentrations from dose 1 to dose 2 (pThe highest antibody concentrations were found in younger subjects and women, remaining significantly associated in a multivariable linear regression model (p=0.005).A single dose of the BBIBP-CorV vaccine induced a strong antibody response in individuals with prior SARS-CoV-2infection, while a second dose did not increase this response. A sharp increase in antibody concentrations was observed following SARS-CoV-2 infection in those participants who became infected after the first and second doses (p=0.008).Individuals with SARS-CoV-2 exposure prior to vaccination showed significantly higher anti-spike IgG antibody levels, at all-time points, than those not exposed (ppOverall, our results showed a trend towards lower antibody concentrations over time following BBIBP-CorV vaccination. Sex and age seem to influence the magnitude of the humoral response in unexposed subjects while the combination of exposure to SARS-CoV-2 plus vaccination, whatever the sequence of the events was, produced a sharp increase in antibody levels.Evaluation of the humoral responses over time and the analysis of the induction and persistence of memory B and T cell responses, are needed to assess long-term immune protection induced by BBIBP-CorV vaccine.

Published

2022

38. CCL5/CCR5 axis in human diseases and related treatments

Author

Zhen Zeng, Tianxia Lan, Yuquan Wei, and Xiawei Wei

Subjects

Medicine (General), Chemokine, Genetic enhancement, T cell, Translational research, Inflammation, Review Article, QH426-470, Biochemistry, CCL5, R5-920, Immune system, Genetics, Medicine, Molecular Biology, Genetics (clinical), Cancer, biology, business.industry, virus diseases, Cell Biology, CCL5/CCR5, medicine.anatomical_structure, Immunology, biology.protein, Therapy, Signal transduction, medicine.symptom, Infection, business

Abstract

To defense harmful stimuli or maintain the immune homeostasis, the body produces and recruits a superfamily of cytokines such as interleukins, interferons, chemokines etc. Among them, chemokines act as crucial regulators in defense systems. CCL5/CCR5 combination is known for facilitating inflammatory responses, as well as inducing the adhesion and migration of different T cell subsets in immune responses. In addition, recent studies have shown that the interaction between CCL5 and CCR5 is involved in various pathological processes including inflammation, chronic diseases, cancers as well as the infection of COVID-19. This review focuses on how CCL5/CCR5 axis participates in the pathological processes of different diseases and their relevant signaling pathways for the regulation of the axis. Moreover, we highlighted the gene therapy and chemotherapy studies for treating CCR5-related diseases, including the ongoing clinical trials. The barriers and perspectives for future application and translational research were also summarized.

Published

2022

39. FGFR3 Destabilizes PD-L1 via NEDD4 to Control T-cell–Mediated Bladder Cancer Immune Surveillance

Author

Yue Li, Xin Jiang, Wushan Li, Ganyu Wang, Weiqiang Jing, Zhiwei Cui, Gaozhong Xiong, Benkang Shi, Shouzhen Chen, and Bo Han

Subjects

musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, T cell, medicine.medical_treatment, NEDD4, B7-H1 Antigen, Targeted therapy, Mice, Cell Line, Tumor, PD-L1, Tumor Microenvironment, medicine, Animals, Humans, Receptor, Fibroblast Growth Factor, Type 3, Immunologic Surveillance, Bladder cancer, biology, Chemistry, High-Throughput Nucleotide Sequencing, Membrane Proteins, Immunotherapy, medicine.disease, Ubiquitin ligase, Disease Models, Animal, stomatognathic diseases, medicine.anatomical_structure, Urinary Bladder Neoplasms, Oncology, biology.protein, Cancer research, Intercellular Signaling Peptides and Proteins, Female, CD8

Abstract

Fibroblast growth factor receptor 3 (FGFR3) is frequently activated by mutation or overexpression, and it is a validated therapeutic target in urothelial carcinoma (UC) of the bladder. However, the role and detailed molecular mechanism of FGFR3 in the immune microenvironment of bladder cancer remain largely unknown. Here, we demonstrate that inhibition of FGFR3 in FGFR3-activated bladder cancer elevates PD-L1 protein levels by affecting its ubiquitination, thereby inhibiting the antitumor activity of CD8+ T cells. Tissue microarray analysis in human UC showed an inverse correlation between FGFR3 and PD-L1. Furthermore, NEDD4, an E3 ubiquitin ligase of the NEDD4 family of proteins, was phosphorylated by FGFR3 activation and served as a regulator of PD-L1 ubiquitination. Mechanistically, NEDD4 interacted with PD-L1 and catalyzed Lys48 (K48)-linked polyubiquitination of PD-L1. In mice bearing NEDD4 knockout bladder cancer, CD8+ T-cell infiltration and antitumor activity were significantly inhibited due to PD-L1 upregulation in bladder cancer cells. Furthermore, multiple FGFR3-activated tumor-bearing mouse models suggested that attenuated CD8+ T-cell–mediated antitumor efficacy following FGFR3-targeted therapy could be rescued by a combination with anti-PD-1 immunotherapy, which leads to effective tumor suppression. This study establishes a key molecular link between targeted therapy and immune surveillance and identifies NEDD4 as a crucial E3 ubiquitin ligase that targets PD-L1 for degradation in FGFR3-activated bladder cancer. These findings may potentially be exploited for combination therapies in UC of the bladder and possibly other malignancies with activated FGFR3. Significance: NEDD4 links two important molecules associated with targeted therapy and immune surveillance, providing mechanistic rationale and preclinical support for immuno-targeted combination therapy for FGFR3-activated bladder cancer.

Published

2022

40. An efficient single-cell based method for linking human T cell phenotype to T cell receptor sequence and specificity

Author

Julia Puchan, Christian E. Busse, Sandro Hoffmann, Benjamin Mordmüller, Rebecca Hundsdorfer, Ilka Wahl, Peter G. Kremsner, Hedda Wardemann, and Stephen L. Hoffman

Subjects

Adult, CD4-Positive T-Lymphocytes, Male, Receptors, Antigen, T-Cell, alpha-beta, T cell, Immunology, T-cell receptor, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], Computational biology, CD8-Positive T-Lymphocytes, Biology, Phenotype, Immune system, medicine.anatomical_structure, Gene duplication, Expression cloning, medicine, Humans, Immunology and Allergy, Female, Single-Cell Analysis, Gene, CD8

Abstract

Contains fulltext : 248576.pdf (Publisher’s version ) (Open Access) Single-cell antigen-receptor gene amplification and sequencing platforms have been used to characterize T cell receptor (TCR) repertoires but typically fail to generate paired full-length gene products for direct expression cloning and do not enable linking this data to cell phenotype information. To overcome these limitations, we established a high-throughput platform for the quantitative and qualitative analysis of human TCR repertoires that provides insights into the clonal and functional composition of human CD4(+) and CD8(+) αβ T cells at the molecular and cellular level. The strategy is a powerful tool to qualitatively assess differences between antigen receptors of phenotypically defined αβ T cell subsets, e.g. in immune responses to cancer, vaccination, or infection, and in autoimmune diseases.

Published

2022

41. Mycobacterium tuberculosis latency-associated antigen Rv1733c SLP improves the accuracy of differential diagnosis of active tuberculosis and latent tuberculosis infection

Author

Lifan Zhang, Huimin Ma, Shijun Wan, Yueqiu Zhang, Mengqiu Gao, Xiaoqing Liu, and Peng Lyu

Subjects

Interleukin 2, Tuberculosis, T cell, Mycobacterium tuberculosis, Diagnosis, Differential, Immune system, Antigen, Latent Tuberculosis, medicine, Humans, Antigens, Bacterial, biology, Latent tuberculosis, business.industry, General Medicine, biology.organism_classification, medicine.disease, bacterial infections and mycoses, medicine.anatomical_structure, Immunology, Leukocytes, Mononuclear, Medicine, FluoroSpot, business, medicine.drug

Abstract

Background:. Differential diagnosis of active tuberculosis (ATB) and latent tuberculosis infection (LTBI) has been a challenge for clinicians in high TB burden countries. The purpose of this study was to improve the accuracy of differential diagnosis of ATB and LTBI by using fluorescent immunospot (FluoroSpot) assay to detect specific Th1 cell immune responses. The novel mycobacterium tuberculosis (MTB) latency-associated antigens Rv1733c and synthetic long peptides derived from Rv1733c (Rv1733c SLP) were used based on virulence factors early secreting antigen target-6 (ESAT-6) and culture filtrate protein-10 (CFP-10). Methods:. Fifty-seven ATB cases, including 20 pathogen-confirmed ATB and 37 clinically diagnosed ATB, and 36 LTBI cases, were enrolled between January and December 2017. FluoroSpot assay was used to detect the interferon γ (IFN-γ) and interleukin 2 (IL-2) secreted by the specific T cells after being stimulated with MTB virulence factors ESAT-6 and CFP-10, MTB latency-associated antigens Rv1733c and Rv1733c SLP. The receiver operating characteristic (ROC) curve was used to define the best cutoff value of latency-associated antigens in the use of differentiating ATB and LTBI. The sensitivity, specificity, predictive value, and likelihood ratio of ESAT-6 and CFP-10-FluoroSpot combined with latency-associated antigen in the differential diagnosis of ATB and LTBI were also calculated. Results:. Following the stimulation with Rv1733c and Rv1733c SLP, the frequency of single IL-2-secreting T cells stimulated by Rv1733c SLP had the largest area under the ROC curve, which was 0.766. With a cutoff value of 1 (spot-forming cells [SFCs]/2.5 × 105 peripheral blood mononuclear cells) for frequency, the sensitivity and specificity of distinguishing ATB from LTBI were 72.2% and 73.7%, respectively. ESAT-6 and CFP-10-FluoroSpot detected the frequency and proportion of single IFN-γ-secreting T cells; the sensitivity and specificity of distinguishing ATB from LTBI were 82.5% and 66.7%, respectively. Combined with the frequency of single IL-2-secreting T cells stimulated by Rv1733c SLP on the basis of ESAT-6 and CFP-10-FluoroSpot, the sensitivity and specificity increased to 84.2% and 83.3%, respectively. Conclusion:. Rv1733c SLP, combined with ESAT-6 and CFP-10, might be used as a candidate antigen for T cell-based tuberculosis diagnostic tests to differentiate ATB from LTBI.

Published

2022

42. B-cell to T-cell ratio as a novel indicator in flow cytometry in the diagnosis of thyroid lymphoma

Author

Miyoko Higuchi, Mitsuyoshi Hirokawa, Seiji Kuma, Aki Tanaka, Akira Miyauchi, Naoki Yamao, Risa Kanematsu, Toshitetsu Hayashi, and Ayana Suzuki

Subjects

Pathology, medicine.medical_specialty, Lymphoma, T-Lymphocytes, Endocrinology, Diabetes and Metabolism, T cell, Thyroid Gland, Immunoglobulin light chain, CD19, Immunophenotyping, Flow cytometry, Endocrinology, Thyroid lymphoma, Humans, Medicine, B cell, Retrospective Studies, biology, medicine.diagnostic_test, business.industry, Thyroid, Flow Cytometry, medicine.disease, medicine.anatomical_structure, biology.protein, business

Abstract

Preoperative flow cytometry is recommended to prove the monoclonality and confirm the diagnosis of thyroid lymphoma. However, lymphoma cases without light chain restriction may also have monoclonality. The aim of our study was to identify a novel marker for thyroid lymphomas using aspirated materials for flow cytometry. We retrospectively analyzed 26 patients with primary thyroid lymphomas and 16 patients with benign lymphoproliferative lesions. The materials for flow cytometry were obtained by fine-needle aspiration cytology using a 22-gauge needle under ultrasound guidance. Light chain restriction was defined as a κ to λ ratio of less than 0.5 or more than 3.0. According to the light chain-positive rate, 25% or less and more than 25% were classified as the low and high light chain-positive rate groups, respectively. B-cell predominance was defined as a CD19 to CD4 ratio (B- to T-cell ratio) of more than 2.0. B-cell predominance was more frequently observed in lymphomas (88.5%) than in benign lymphoproliferative lesions (25.0%; p < 0.001). Light chain restriction based on the κ/λ ratio was detected in 69.2% of lymphomas, but not in benign lymphoproliferative lesions. Among lymphomas belonging to the low light chain-positive rate group, 88.9% did not exhibit light chain restriction and B-cell predominance was present. In contrast, benign lymphoproliferative lesions with B-cell predominance were not detected in the low light chain-positive rate group. B-cell predominance was a useful indicator for diagnosing thyroid lymphoma in the low light chain-positive rate group without light chain restriction.

Published

2022

43. Single-cell atlas of splenocytes reveals a critical role of a novel plasma cell‒specific marker Hspa13 in antibody class-switching recombination and somatic hypermutation

Author

Yaqi Xu, Shan Zhou, Gencheng Han, Youdi He, Gaizhi Zhu, Renxi Wang, Bing Zhai, Xiaoling Liu, Wenting Su, and Xiaoqian Wang

Subjects

Transcription, Genetic, T cell, Antigens, CD19, Immunology, Somatic hypermutation, Biology, Plasma cell, Antibodies, Mice, Th2 Cells, medicine, Animals, HSP70 Heat-Shock Proteins, Molecular Biology, Gene Rearrangement, Mice, Knockout, Recombination, Genetic, Sheep, breakpoint cluster region, Germinal center, Cell Differentiation, EBI3, Germinal Center, Cell biology, medicine.anatomical_structure, Immunoglobulin class switching, biology.protein, Somatic Hypermutation, Immunoglobulin, Antibody, Biomarkers

Abstract

Our previous study had shown that member 13 (Hspa13) of heat shock protein family A (Hsp70) promotes plasma cell (PC) production and antibody secretion. To further explore Hspa13 expression and function, we combined single-cell RNA-sequencing and antigen receptor lineage (BCR) analysis to characterize sheep red cell‒primed splenocytes. The single-cell transcriptional profiles revealed that Hspa13 is specifically and highly expressed in PCs. These results suggest that Hspa13 is a novel PC-specific marker. In terms of its function, we found that the CD19cre-mediated conditional knock-out (cKO) of Hspa13 reduced the expression of Ebi3 and IL-10 in PCs. Ebi3 and IL-10 are important factors in IL-4‒secreting type 2 helper T cell (Th2) activation and differentiation. As expected, we found that the Hspa13 cKO reduced IL‒4-expressing follicular helper T (Tfh2) cells. Finally, the single-cell antigen receptor analysis demonstrated that the Hspa13 cKO reduced the Aicda-mediated antibody class-switching recombination (CSR) and somatic hypermutation (SHM) in germinal centers (GCs) B cells. Altogether, the single-cell atlas of splenocytes revealed a critical indirect role for the novel PC-specific marker Hspa13 in CSR and SHM in GC B cells by promoting Ebi3 and IL-10 expression in PCs to induce IL-4-expressing Tfh2 cells. Further exploration of Hspa13 expression and function will provide valuable clues for how to use Hspa13 in the treatment of autoimmune diseases.

Published

2022

44. Cooperating minimalist nanovaccine with PD-1 blockade for effective and feasible cancer immunotherapy

Author

Xinghan Wu, Xiaoming Cui, Xiuwen Guan, Weifen Zhang, Liping Zhao, Mingxia Jiang, Jinlong Ma, and Yuhan Zhang

Subjects

Medicine (General), Science (General), medicine.medical_treatment, T cell, Programmed Cell Death 1 Receptor, Protamine, Cancer immunotherapy, Cancer Vaccines, Mice, Q1-390, R5-920, Antigen, Neoplasms, CpG, PD-1, Animals, Medicine, ComputingMethodologies_COMPUTERGRAPHICS, Multidisciplinary, biology, business.industry, Immunotherapy, Blockade, Mice, Inbred C57BL, Ovalbumin, Nanovaccine, medicine.anatomical_structure, OVA, biology.protein, Cancer research, Nanoparticles, Antibody, business, Adjuvant

Abstract

Graphical abstract, Highlights • Facile antigen/adjuvant co-loaded nanovaccine made by convenient green preparation. • The immunological activity of the antigen and adjuvant was maximally preserved. • The minimalist nanovaccine had excellent stability and antitumor immune activation. • Nanovaccine combined with PD-1 antibody synergistically enhanced therapy outcome. • Good practicability for expanding clinical translation and personalized therapy., Introduction Tumor vaccine has been a research boom for cancer immunotherapy, while its therapeutic outcome is severely depressed by the vulnerable in vivo delivery efficiency. Moreover, tumor immune escape is also another intractable issue, which has badly whittled down the therapeutic efficiency. Objectives Our study aims to solve the above dilemmas by cooperating minimalist nanovaccine with PD-1 blockade for effective and feasible cancer immunotherapy. Methods The minimalist antigen and adjuvant co-delivery nanovaccine was developed by employing natural polycationic protamine (PRT) to carry the electronegative ovalbumin (OVA) antigen and unmethylated Cytosine-phosphorothioate-Guanine (CpG) adjuvant via convenient chemical bench-free “green” preparation without chemical-synthesis and no organic solvent was required, which could preserve the immunological activities of the antigens and adjuvants. On that basis, PD-1 antibody (aPD-1) was utilized to block the tumor immune escape and cooperate with the nanovaccine by maintaining the tumoricidal-activity of the vaccine-induced T cells. Results Benefited from the polycationic PRT, the facile PRT/CpG/OVA nanovaccine displayed satisfactory delivery performance, involving enhanced cellular uptake in dendritic cells (DCs), realizable endosomal escape and promoted stimulation for DCs’ maturation. These features would be helpful for the antitumor immunotherapeutic efficiency of the nanovaccine. Furthermore, the cooperation of the nanovaccine with aPD-1 synergistically improved the immunotherapy outcome, profiting by the cooperation of the “T cell induction” competency of the nanovaccine and the “T cell maintenance” function of the aPD-1. Conclusion This study will provide new concepts for the design and construction of facile nanovaccines, and contribute valuable scientific basis for cancer immunotherapy.

Published

2022

45. Nuclear Factor of Activated T Cells and Tolerance

Author

F. Macian

Subjects

Cytosol, medicine.anatomical_structure, Regulatory T cell, T cell, cardiovascular system, medicine, FOXP3, NFAT, Biology, Signal transduction, Transcription factor, Calcium signaling, Cell biology

Abstract

The nuclear factor of activated T cells (NFAT) transcription factors control a wide range of processes in T cells that determine the fate and functions of different T cell populations. The capacity of NFAT to regulate different programs of gene expression is determined by its ability to cooperate with multiple transcription factors and, therefore, integrate calcium signaling, which mediates NFAT activation and shuttling from the cytosol to the nucleus, with other signaling pathways that are engaged under specific conditions and induce the activation of distinct NFAT partners. This article will explore how, by forming specific transcriptional complexes, NFAT regulates events that are responsible for the establishment of T cell tolerance.

Published

2023

46. The Potential of T Cell Immunoglobulin and Mucin-Domain Containing-3 (Tim-3) in Designing Novel Immunotherapy for Bladder Cancer

Author

Seyed Ali Momeni, Masoumeh Kourosh-Arami, Laleh Sharifi, Saied Bokaie, Parizad Bavandpour, Monireh Mohsenzadegan, Mohammad Reza Nowroozi, and Erfan Amini

Subjects

medicine.drug_class, T-Lymphocytes, Endocrinology, Diabetes and Metabolism, T cell, medicine.medical_treatment, Monoclonal antibody, Immunity, medicine, Humans, Immunology and Allergy, Hepatitis A Virus Cellular Receptor 2, Innate immune system, Bladder cancer, biology, business.industry, Mucin, Mucins, Antibodies, Monoclonal, Immunotherapy, medicine.disease, medicine.anatomical_structure, Urinary Bladder Neoplasms, biology.protein, Cancer research, Antibody, business

Abstract

Targeting inhibitory receptors on T cells in the tumor sites can promote effective anti-tumor immunity in bladder cancer. Unfortunately, the main dilemma is that a large number of patients remain refractory to CTLA-4, PD-1, and PD-L1 blockade therapies. T-cell immunoglobulin and mucin domain 3 (Tim-3) is an inhibitory receptor expressed on T cells and innate immune cells. Both in vivo and in vitro data from patients with advanced cancers support the role of Tim-3 inhibition in satisfactory anti-tumor immunity. In bladder cancer, the expression level of Tim-3 significantly increases with advanced pathological grade and T stage. Therefore, rationality implies that designing novel monoclonal antibodies reactive with Tim-3 alone or in combination with other checkpoint inhibitors may indicate a favorable response in bladder cancer. Here, we aimed to investigate the possibility of targeting Tim-3 as a novel anti-cancer treatment for bladder cancer.

Published

2021

47. Expression, prognosis value, and immune infiltration of lncRNA ASB16-AS1 identified by pan-cancer analysis

Author

Xiao-dong Wang, Linyong Wu, Yun He, Jin-shu Pang, Yujia Zhao, Hong Yang, Yu-Ji Chen, and Wei Liao

Subjects

Carcinoma, Hepatocellular, T cell, Cell, Pan-cancer, Bioengineering, Biology, Applied Microbiology and Biotechnology, Long non-coding RNA ASB16-AS1, Immune system, Cell Movement, Cell Line, Tumor, Neoplasms, medicine, Humans, Molecular characteristics, Neoplasm Invasiveness, Cell Proliferation, Proportional Hazards Models, Oncogene, Liver Neoplasms, Reproducibility of Results, Cancer, Microsatellite instability, General Medicine, Prognosis, medicine.disease, Up-Regulation, Immune infiltration, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Tumor progression, Multivariate Analysis, Cancer research, RNA, Long Noncoding, Transcriptome, TP248.13-248.65, CD8, Research Article, Research Paper, Biotechnology

Abstract

Long-chain non-coding RNA ASB16-AS1 has been proven to be an oncogene for many cancer types. However, the relationship between ASB16-AS1 and immunity is still under studied. This study aims to explore the expression and prognostic potential of ASB16-AS1, and to visualize the relationship between ASB16-AS1 expression and immune infiltration in pan-cancer. We clarified ASB16-AS1 expression patterns in pan-cancer and its relationship with prognosis through multi-platform and multi-database sources (TCGA, GEO, GTEx, ArrayExpress, and SRA), and verified the function of ASB16-AS1 in liver hepatocellular carcinoma (LIHC). Then, a variety of immune cell content evaluation methods were used to mutually verify the correlation between ASB16-AS1 and immune infiltration. Finally, the relationships between ASB16-AS1 and some molecular characteristics (immune checkpoints, tumor mutation burden, microsatellite instability, oncogenic signaling pathways) were further explored. In terms of comprehensive analysis, compared with non-tumor tissues, ASB16-AS1 was highly expressed in tumor tissues, and indicated the value of poor prognosis in multiple cancer types. Functional assays, such as CCK8 assay, transwell assay and wound scratch assay, verified that high ASB16-AS1 expression promoted tumor progression in LIHC. ASB16-AS1 was positively correlated with B cells, T cell CD4+ and T cell CD8+ in most cancer types, and negatively correlated with macrophages, dendritic cells and neutrophils in some cancer types, especially in neutrophils. In addition, there were different interaction modes between ASB16-AS1 and molecular features, such as the relationship with oncogenic signaling pathways, showing that the high ASB16-AS1 expression was related to alterations in oncogenic signaling pathways. Our study emphasizes that ASB16-AS1 is a potential pan-cancer prognostic marker, whichs is associated with the immune infiltration in multiple cancer types.

Published

2021

48. Infectious sporozoite challenge modulates radiation attenuated sporozoite vaccine–induced memory CD8 + T cells for better survival characteristics

Author

Manoj Patidar, Naveen Yadav, Hardik Patel, Sarat K. Dalai, and Rajesh Parmar

Subjects

T cell, Immunology, Biology, medicine.disease, Microbiology, medicine.anatomical_structure, Immunization, Annexin, Virology, CX3CR1, medicine, Cytotoxic T cell, Malaria, Homeostasis, CD8

Abstract

Radiation attenuated sporozoite (RAS), a whole parasite vaccine approach provides sterile protection against malaria. However, RAS immunization does not confer protection for long, and that has been correlated with the waning parasite-induced memory CD8+ T cell responses. Interestingly, an intermittent infectious (wild-type) sporozoite challenge to the RAS vaccinated mice lengthened the protection period from 6 to 18 months. Herein, we have studied the changes that infectious sporozoite brought in RAS-induced memory CD8+ T cells for conferring lengthened protection. We observed that the infectious sporozoite challenge has boosted the frequency of foreign antigen-experienced memory CD8+ T cells. In those CD8+ T cells, it has reduced the Annexin-V reactivity, raised Bcl-2 expression, and also more cells undergone homeostatic proliferation (Ki-67+ ). It has also scaled down the frequency of Nur77 and CX3CR1 high expressing cells in those memory CD8+ T cell populations which we further correlated with better survival signals. This article is protected by copyright. All rights reserved.

Published

2021

49. Invariant NKT Cells Promote the Development of Highly Cytotoxic Multipotent CXCR3+CCR4+CD8+ T Cells That Mediate Rapid Hepatocyte Allograft Rejection

Author

Jing Han, Madison M Hart, Ginny L. Bumgardner, Robert T. Warren, Chelsea M Peterson, Bryce A Ringwald, Sachi R Chaudhari, Mahmoud Abdel-Rasoul, and Jason M. Zimmerer

Subjects

Graft Rejection, Adoptive cell transfer, T cell, Immunology, CD8-Positive T-Lymphocytes, Article, Mice, Immune system, medicine, Animals, Immunology and Allergy, Cytotoxic T cell, Mice, Knockout, biology, Chemistry, Allografts, Natural killer T cell, Liver Transplantation, Mice, Inbred C57BL, medicine.anatomical_structure, Perforin, Granzyme, Hepatocytes, Cancer research, biology.protein, Natural Killer T-Cells, CD8

Abstract

Hepatocyte transplant represents a treatment for metabolic disorders but is limited by immunogenicity. Our prior work identified the critical role of CD8+ T cells, with or without CD4+ T cell help, in mediating hepatocyte rejection. In this study, we evaluated the influence of invariant NKT (iNKT) cells, uniquely abundant in the liver, upon CD8-mediated immune responses in the presence and absence of CD4+ T cells. To investigate this, C57BL/6 (wild-type) and iNKT-deficient Jα18 knockout mice (cohorts CD4 depleted) were transplanted with allogeneic hepatocytes. Recipients were evaluated for alloprimed CD8+ T cell subset composition, allocytotoxicity, and hepatocyte rejection. We found that CD8-mediated allocytotoxicity was significantly decreased in iNKT-deficient recipients and was restored by adoptive transfer of iNKT cells. In the absence of both iNKT cells and CD4+ T cells, CD8-mediated allocytotoxicity and hepatocyte rejection was abrogated. iNKT cells enhance the proportion of a novel subset of multipotent, alloprimed CXCR3+CCR4+CD8+ cytolytic T cells that develop after hepatocyte transplant and are abundant in the liver. Alloprimed CXCR3+CCR4+CD8+ T cells express cytotoxic effector molecules (perforin/granzyme and Fas ligand) and are distinguished from alloprimed CXCR3+CCR4−CD8+ T cells by a higher proportion of cells expressing TNF-α and IFN-γ. Furthermore, alloprimed CXCR3+CCR4+CD8+ T cells mediate higher allocytotoxicity and more rapid allograft rejection. Our data demonstrate the important role of iNKT cells in promoting the development of highly cytotoxic, multipotent CXCR3+CCR4+CD8+ T cells that mediate rapid rejection of allogeneic hepatocytes engrafted in the liver. Targeting iNKT cells may be an efficacious therapy to prevent rejection of intrahepatic cellular transplants.

Published

2021

50. Effect of Clonally Expanded <scp> PD‐1 high CXCR5 </scp> – <scp>CD4</scp> + Peripheral T Helper Cells on B Cell Differentiation in the Joints of Patients With Antinuclear Antibody–Positive Juvenile Idiopathic Arthritis

Author

Hermann J. Girschick, Henner Morbach, Julia Klaussner, Johannes Dirks, Stephan Hackenberg, Jonas Fischer, Gabriele Haase, Annette Holl-Wieden, and Christine Hofmann

Subjects

musculoskeletal diseases, medicine.medical_treatment, T cell, Cellular differentiation, Immunology, T-cell receptor, CD11c, Biology, Molecular biology, CXCR5, medicine.anatomical_structure, Cytokine, Rheumatology, medicine, Immunology and Allergy, Synovial fluid, B cell

Abstract

Objectives Antinuclear antibody (ANA) positive Juvenile Idiopathic Arthritis (JIA) is characterized by synovial B cell hyperactivity, but the precise role of CD4+ T cells in promoting local B cell activation is unknown. The objective of this study is to unravel the phenotype and function of synovial CD4+ T cells that promote the aberrant B cell activation in JIA. Methods Flow cytometric analysis was performed to compare the phenotype and cytokine pattern of synovial fluid (SF) PD-1hi CD4+ T cells with tonsil TFH cells. TCRVB next generation sequencing was applied to analyze T cell subsets for signs of clonal expansion. The functional impact of these T cell subsets on B cells was dissected in in vitro co-cultures. Results Multidimensional flow-cytometric analysis revealed the expansion of IL-21 and IFN-γ co-expressing PD-1hi CXCR5- HLA-DR+ CD4+ T cells that accumulate in the joints of ANA+ JIA patients. These T cells exhibited signs of clonal expansion with restricted TCR clonotypes. Phenotypically they resembled peripheral T helper (TPH ) cells with an extrafollicular chemokine receptor pattern and high T-bet and Blimp-1 but low Bcl-6 expression. SF TPH cells particularly skewed B cell differentiation towards a CD21lo/- CD11c+ phenotype by provision of IL-21 and IFN-γ in vitro and correlated with the appearance of SF CD21lo/- CD11c+ CD27- IgM- double-negative B cells (BDN ) in situ. Conclusion Clonally expanded CD4+ TPH cells accumulate in the joints of ANA+ JIA patients and particularly promote CD21lo/- CD11c+ BDN cell differentiation The expansion of TPH and BDN cells might reflect the autoimmune response present in the joints of ANA+ JIA patients.

Published

2021