Showing total 168 results

1. Role of microbes in colorectal cancer therapy: Cross-talk between the microbiome and tumor microenvironment.

Author

Cong Xia, Yantao Cai, Shuangyi Ren, and Chenglai Xia

Subjects

COLORECTAL cancer, TUMOR microenvironment, KILLER cells, CYTOTOXIC T cells, T helper cells, CANCER treatment, HUMAN microbiota

Abstract

The human gut microbiota is associated with the development and progression of colorectal cancer, and manipulation of the gut microbiota is a novel strategy for the prevention and treatment of colorectal cancer. Some bacteria have antitumor activity against colorectal cancer, where specific bacteria can improve the tumor microenvironment, activate immune cells including dendritic cells, helper T cells, natural killer cells, and cytotoxic T cells, and upregulate the secretion of pro-tumor immune cytokines such as interleukin-2 and interferon. In this paper, we summarize some bacteria with potential benefits in colorectal cancer and describe their roles in the tumor microenvironment, demonstrate the application of gut microbes in combination with immunosuppressive agents, and provide suggestions for further experimental studies and clinical practice applications. [ABSTRACT FROM AUTHOR]

Published

2022

2. PD-1/PD-L1 inhibitors for advanced or metastatic cervical cancer: From bench to bed.

Author

Weijia Huang, Jiewei Liu, Kai Xu, Huilin Chen, and Ce Bian

Subjects

PROGRAMMED cell death 1 receptors, PROGRAMMED death-ligand 1, CERVICAL cancer, CYTOTOXIC T cells, METASTASIS, CETUXIMAB, MOVEMENT disorders, PRECANCEROUS conditions

Abstract

Advanced or metastatic cervical cancer has a poor prognosis, and the 5-year overall survival is <5% with conventional radiotherapy and chemotherapy. Immunotherapy, particularly immune checkpoint inhibitors (ICIs), achieved initial success in advanced solid tumors, while their efficacy and safety in advanced or metastatic cervical cancer remains to be explored. Previous studies found high-risk HPV infection and elevated PD-L1 expression in cervical precancerous lesions and squamous cell carcinoma. Meanwhile, elevated PD-L1 expression, high cytotoxic T lymphocyte infiltration, and abnormal cytotoxic T lymphocyte function might benefit inflammation infiltration for ICIs in the tumor microenvironment. Patients with HPV infection, squamous cell carcinoma, advanced stage, large tumor size, poor differentiation, metastatic disease, history of multiple childbirth and abortion, or a previous history of receiving chemotherapy might be associated with positive PD-L1 expression. Although there is no correlation between PD-L1 expression and prognosis using conventional radiotherapy, patients with high PD-L1 expression have a poorer prognosis. Several clinical studies demonstrate preliminary safety and efficacy for PD-1/PD-L1 inhibitors, and the exploration of combination strategies such as immunotherapy combined with chemotherapy, radiotherapy, anti-angiogenesis therapy, or dual ICIs is ongoing. This paper systematically reviews PD-L1 expression patterns and their relationship with prognosis, along with reported and ongoing clinical trials of PD-1/PD-L1 inhibitors in cervical cancer to clarify the prospect of ICIs for cervical cancer from bench to bed. [ABSTRACT FROM AUTHOR]

Published

2022

3. Current status of immunotherapy for non-small cell lung cancer.

Author

Tao Yang, Yilin Xiong, Yufei Zeng, Yan Wang, Jing Zeng, Jie Liu, Shangfu Xu, and Li-Sheng Li

Subjects

BISPECIFIC antibodies, NON-small-cell lung carcinoma, IMMUNE checkpoint inhibitors, MONOCLONAL antibodies, IMMUNOTHERAPY, ANTIBODY-drug conjugates, T cell receptors, CYTOTOXIC T cells

Abstract

Nowadays, lung cancer is still the deadliest oncological disease in the world. Among them, non-small cell lung cancer (NSCLC) accounts for 80%~85% of all lung cancers, and its 5-year survival rate is less than 15%, making the situation critical. In the past decades, despite some clinical advances in conventional treatments, the overall survival rate of NSCLC is still not optimistic due to its unique physiological conditions and the frequent occurrence of tumor escape. In recent years, immunotherapy has become a new hot spot in lung cancer research, including antibody therapy and cell therapy, which have been developed and utilized one after another, especially immune checkpoint inhibitor (ICI). These approaches have effectively improved the overall survival rate and objective response rate of NSCLC patients by enhancing the immune capacity of the body and targeting tumor cells more effectively, which is more specific and less toxic compared with conventional chemotherapy, and providing more strategies for NSCLC treatment. In this paper, we reviewed the relevant targets, clinical progress and adverse reaction in monoclonal antibodies, antibody-drug conjugates, ICI, bispecific antibodies, T-cell receptor engineered T cell therapy (TCR-T), Chimeric antigen receptor T-cell immunotherapy (CAR-T), and also report on their combination therapy from the immune-related background to provide better NSCLC treatment and prospective. [ABSTRACT FROM AUTHOR]

Published

2022

4. Autoimmunity and Cancer—Two Sides of the Same Coin.

Author

Sakowska, Justyna, Arcimowicz, Łukasz, Jankowiak, Martyna, Papak, Ines, Markiewicz, Aleksandra, Dziubek, Katarzyna, Kurkowiak, Małgorzata, Kote, Sachin, Kaźmierczak-Siedlecka, Karolina, Połom, Karol, Marek-Trzonkowska, Natalia, and Trzonkowski, Piotr

Subjects

PROGRAMMED cell death 1 receptors, AUTOIMMUNITY, CYTOTOXIC T cells, IMMUNOLOGICAL tolerance, B cells, AUTOIMMUNE diseases

Abstract

Autoimmune disease results from the immune response against self-antigens, while cancer develops when the immune system does not respond to malignant cells. Thus, for years, autoimmunity and cancer have been considered as two separate fields of research that do not have a lot in common. However, the discovery of immune checkpoints and the development of anti-cancer drugs targeting PD-1 (programmed cell death receptor 1) and CTLA-4 (cytotoxic T lymphocyte antigen 4) pathways proved that studying autoimmune diseases can be extremely helpful in the development of novel anti-cancer drugs. Therefore, autoimmunity and cancer seem to be just two sides of the same coin. In the current review, we broadly discuss how various regulatory cell populations, effector molecules, genetic predisposition, and environmental factors contribute to the loss of self-tolerance in autoimmunity or tolerance induction to cancer. With the current paper, we also aim to convince the readers that the pathways involved in cancer and autoimmune disease development consist of similar molecular players working in opposite directions. Therefore, a deep understanding of the two sides of immune tolerance is crucial for the proper designing of novel and selective immunotherapies. [ABSTRACT FROM AUTHOR]

Published

2022

5. The Antifibrotic and the Anticarcinogenic Activity of Capsaicin in Hot Chili Pepper in Relation to Oral Submucous Fibrosis.

Author

Huang, Zoufang, Sharma, Mohit, Dave, Aparna, Yang, Yuqi, Chen, Zhe-Sheng, and Radhakrishnan, Raghu

Subjects

ORAL submucous fibrosis, HOT peppers, REGULATORY T cells, CYTOTOXIC T cells, CAPSAICIN, INTRACELLULAR calcium

Abstract

A burning sensation on eating spicy foods purportedly supports the role of capsaicin, an active component of chili peppers, in the etiology of oral submucous fibrosis (OSF). Although the mast cell mediators and activated P2X receptors induce a constant burning sensation through an ATP-dependent mechanism, it is the activation of the transient receptor potential vanilloid 1 (TRPV-1) receptor by capsaicin that aggravates it. The molecular basis for the burning pain in OSF is thus attributable to the activation of TRPV1. There is overwhelming evidence that confirms capsaicin has more of a protective role in attenuating fibrosis and is potentially therapeutic in reversing conditions linked to collagen accumulation. The activation of TRPV-1 by capsaicin increases intracellular calcium ([Ca2+]i), upregulates AMP-activated protein kinase (AMPK) and Sirtuin-1 (SIRT-1), to enrich endothelium-dependent vasodilation via endothelial nitric oxide synthase (eNOS). The induction of vasodilation induces antifibrotic effects by alleviating hypoxia. The antifibrotic effects of capsaicin are mediated through the upregulation of antioxidant enzymes, downregulation of inflammatory genes and suppression of new collagen fibril formation. Capsaicin also demonstrates an anticarcinogenic effect by upregulating the cytotoxic T cells and downregulating regulatory T cells through the inhibition of angiogenesis and promotion of apoptosis. Judicious administration of capsaicin with an appropriate delivery mechanism may have therapeutic benefits in reducing pain sensation, rendering antifibrotic effects, and preventing the malignant transformation of OSF. This paper provides an overview of the molecular basis of capsaicin and its therapeutic application as an antifibrotic and anticarcinogenic agent for the treatment of OSF. [ABSTRACT FROM AUTHOR]

Published

2022

6. Treatment Advances in EBV Related Lymphoproliferative Diseases.

Author

Lv, Kebing, Yin, Ting, Yu, Min, Chen, Zhiwei, Zhou, Yulan, and Li, Fei

Subjects

LYMPHOPROLIFERATIVE disorders, KILLER cells, CYTOTOXIC T cells, HODGKIN'S disease, T-cell lymphoma, CUTANEOUS T-cell lymphoma, PERIPHERAL nerve tumors

Abstract

Epstein Barr virus (EBV) can affect 90% of the human population. It can invade B lymphocytes, T lymphocytes and natural killer cells of the host and remain in the host for life. The long latency and reactivation of EBV can cause malignant transformation, leading to various lymphoproliferative diseases (LPDs), including EBV-related B-cell lymphoproliferative diseases (EBV-B-LPDs) (for example, Burkitt lymphoma (BL), classic Hodgkin's lymphoma (cHL), and posttransplantation and HIV-related lymphoproliferative diseases) and EBV-related T-cell lymphoproliferative diseases (EBV-T/NK-LPDs) (for example, extranodal nasal type natural killer/T-cell lymphoma (ENKTCL), aggressive NK cell leukaemia (ANKL), and peripheral T-cell lymphoma, not otherwise specified (PTCL-NOS). EBV-LPDs are heterogeneous with different clinical features and prognoses. The treatment of EBV-LPDs is usually similar to that of EBV-negative lymphoma with the same histology and can include chemotherapy, radiotherapy, and hematopoietic stem cell transplant (HSCT). However, problems such as serious toxicity and drug resistance worsen the survival prognosis of patients. EBV expresses a variety of viral and lytic proteins that regulate cell cycle and death processes and promote the survival of tumour cells. Based on these characteristics, a series of treatment strategies for EBV in related malignant tumours have been developed, such as monoclonal antibodies, immune checkpoint inhibitors, cytotoxic T lymphocytes (CTLs) and epigenetic therapy. These new individualized therapies can produce highly specific killing effects on tumour cells, and nontumour cells can be protected from toxicity. This paper will focus on the latest progress in the treatment of EBV-LPDs based on pathological mechanisms. [ABSTRACT FROM AUTHOR]

Published

2022

7. Application of Artificial Intelligence Modeling Technology Based on Fluid Biopsy to Diagnose Alzheimer's Disease.

Author

Sh, Yuan, Liu, Benliang, Zhang, Jianhu, Zhou, Ying, Hu, Zhiyuan, and Zhang, Xiuli

Subjects

ALZHEIMER'S disease, ARTIFICIAL intelligence, DIAGNOSIS, CYTOTOXIC T cells, ARTIFICIAL neural networks

Abstract

Background: There are no obvious clinical signs and symptoms in the early stages of Alzheimer's disease (AD), and most patients usually have mild cognitive impairment (MCI) before diagnosis. Therefore, early diagnosis of AD is very critical. This paper mainly discusses the blood biomarkers of AD patients and uses machine learning methods to study the changes of blood transcriptome during the development of AD and to search for potential blood biomarkers for AD. Methods: Individualized blood mRNA expression data of 711 patients were downloaded from the GEO database, including the control group (CON) (238 patients), MCI (189 patients), and AD (284 patients). Firstly, we analyzed the subcellular localization, protein types and enrichment pathways of the differentially expressed mRNAs in each group, and established an artificial intelligence individualized diagnostic model. Furthermore, the XCell tool was used to analyze the blood mRNA expression data and obtain blood cell composition and quantitative data. Ratio characteristics were established for mRNA and XCell data. Feature engineering operations such as collinearity and importance analysis were performed on all features to obtain the best feature solicitation. Finally, four machine learning algorithms, including linear support vector machine (SVM), Adaboost, random forest and artificial neural network, were used to model the optimal feature combinations and evaluate their classification performance in the test set. Results: Through feature engineering screening, the best feature collection was obtained. Moreover, the artificial intelligence individualized diagnosis model established based on this method achieved a classification accuracy of 91.59% in the test set. The area under curve (AUC) of CON, MCI, and AD were 0.9746, 0.9536, and 0.9807, respectively. Conclusion: The results of cell homeostasis analysis suggested that the homeostasis of Natural killer T cell (NKT) might be related to AD, and the homeostasis of Granulocyte macrophage progenitor (GMP) might be one of the reasons for AD. [ABSTRACT FROM AUTHOR]

Published

2021

8. PD-1/PD-L1 Checkpoint Inhibitors in Tumor Immunotherapy.

Author

Liu, Jinhua, Chen, Zichao, Li, Yaqun, Zhao, Wenjie, Wu, JiBiao, and Zhang, Zhen

Subjects

PROGRAMMED death-ligand 1, PROGRAMMED cell death 1 receptors, T cells, CYTOTOXIC T cells, IMMUNE checkpoint proteins, CANCER cells, INHIBITION of cellular proliferation, TREATMENT failure

Abstract

Programmed death protein 1 (PD1) is a common immunosuppressive member on the surface of T cells and plays an imperative part in downregulating the immune system and advancing self-tolerance. Its ligand programmed cell death ligand 1 (PDL1) is overexpressed on the surface of malignant tumor cells, where it binds to PD1, inhibits the proliferation of PD1-positive cells, and participates in the immune evasion of tumors leading to treatment failure. The PD1/PDL1-based pathway is of great value in immunotherapy of cancer and has become an important immune checkpoint in recent years, so understanding the mechanism of PD1/PDL1 action is of great significance for combined immunotherapy and patient prognosis. The inhibitors of PD1/PDL1 have shown clinical efficacy in many tumors, for example, blockade of PD1 or PDL1 with specific antibodies enhances T cell responses and mediates antitumor activity. However, some patients are prone to develop drug resistance, resulting in poor treatment outcomes, which is rooted in the insensitivity of patients to targeted inhibitors. In this paper, we reviewed the mechanism and application of PD1/PDL1 checkpoint inhibitors in tumor immunotherapy. We hope that in the future, promising combination therapy regimens can be developed to allow immunotherapeutic tools to play an important role in tumor treatment. We also discuss the safety issues of immunotherapy and further reflect on the effectiveness of the treatment and the side effects it brings. [ABSTRACT FROM AUTHOR]

Published

2021

9. Regulatory CD4+ T cells redirected against pathogenic CD8+ T cells protect NOD mice from development of autoimmune diabetes.

Author

Kakabadse, Dimitri, Dawei Chen, Fishman, Sigal, Weinstein-Marom, Hadas, Davies, Joanne, Li Wen, Gross, Gideon, and Wong, F. Susan

Subjects

REGULATORY T cells, CYTOTOXIC T cells, T cells, T cell receptors, TYPE 1 diabetes

Abstract

Introduction: In this study, we report a novel therapeutic approach redirecting antigen-specific CD4+ T cells recognizing a hybrid insulin peptide (BDC2.5 T cell receptor (TCR) transgenic CD4+ T cells) to attract and suppress islet-specific CD8+ T cells T cells in the non-obese diabetic (NOD) mouse model, and prevent the development of autoimmune diabetes. Methods: Purified BDC2.5 CD4+ T cells were induced to differentiate into regulatory T cells (Tregs). The Tregs were then electroporated with mRNA encoding chimeric human β2 microglobulin (hβ 2m) covalently linked to insulin B chain amino acids 15-23 (designated INS-eTreg) or islet-specific glucose-6- phosphatase related protein (IGRP) peptide 206-214 (designated IGRP-eTreg). Immunoregulatory functions of these engineered regulatory T cells (eTregs) were tested by in vitro assays and in vivo co-transfer experiments with β-cell-antigen-specific CD8+ T cells in NOD.Scid mice or by adoptive transfer into young, pre-diabetic NOD mice. Results: These eTregs were phenotyped by flow cytometry, and shown to have high expression of FoxP3, as well as other markers of Treg function, including IL- 10. They suppressed polyclonal CD4+ T cells and antigen-specific CD8+ T cells (recognizing insulin or IGRP), decreasing proliferation and increasing exhaustion and regulatory markers in vitro. In vivo, eTregs reduced diabetes development in co-transfer experiments with pathogenic antigen-specific CD8+ T cells (INS- CD8+ or IGRP-CD8+ cells) into NOD.Scid mice. Finally, when the eTreg were injected into young NOD mice, they reduced insulitis and prevented spontaneous diabetes in the recipient mice. Conclusion: Our results suggest a novel therapeutic strategy to protect NOD mice by targeting antigen-specific cytotoxic CD8+ T cells, using redirected antigen-specific CD4+ Treg cells, to suppress autoimmune diabetes. This may suggest an innovative therapy for protection of people at risk of development of type 1 diabetes. [ABSTRACT FROM AUTHOR]

Published

2024

10. Thymic development of human natural killer T cells: recent advances and implications for immunotherapy.

Author

Pellicci, Daniel G., Tavakolinia, Naeimeh, Perriman, Louis, Berzins, Stuart P., and Menne, Christopher

Subjects

CYTOTOXIC T cells, KILLER cells, T cells, HUMAN body, IMMUNOTHERAPY

Abstract

Invariant natural killer T (iNKT) cells are a subset of lipid-reactive, unconventional T cells that have anti-tumor properties that make them a promising target for cancer immunotherapy. Recent studies have deciphered the developmental pathway of human MAIT and Vγ9Vδ2 γδ-T cells as well as murine iNKT cells, yet our understanding of human NKT cell development is limited. Here, we provide an update in our understanding of how NKT cells develop in the human body and how knowledge regarding their development could enhance human treatments by targeting these cells. [ABSTRACT FROM AUTHOR]

Published

2024

11. An in silico Model of T Cell Infiltration Dynamics Based on an Advanced in vitro System to Enhance Preclinical Decision Making in Cancer Immunotherapy.

Author

Lewin, Thomas D., Avignon, Blandine, Tovaglieri, Alessio, Cabon, Lauriane, Gjorevski, Nikolche, and Hutchinson, Lucy G.

Subjects

T cells, DECISION making, EPITHELIUM, IMMUNOTHERAPY, TUMOR microenvironment, CYTOTOXIC T cells, CHEMOTAXIS, EPITHELIAL cells

Abstract

Cancer immunotherapy often involves the use of engineered molecules to selectively bind and activate T cells located within tumour tissue. Fundamental to the success of such treatments is the presence or recruitment of T cells localised within the tumour microenvironment. Advanced organ-on-a-chip systems provide an in vitro setting in which to investigate how novel molecules influence the spatiotemporal dynamics of T cell infiltration into tissue, both in the context of anti-tumour efficacy and off-tumour toxicity. While highly promising, the complexity of these systems is such that mathematical modelling plays a crucial role in the quantitative evaluation of experimental results and maximising the mechanistic insight derived. We develop a mechanistic, mathematical model of a novel microphysiological in vitro platform that recapitulates T cell infiltration into epithelial tissue, which may be normal or transformed. The mathematical model describes the spatiotemporal dynamics of infiltrating T cells in response to chemotactic cytokine signalling. We integrate the model with dynamic imaging data to optimise key model parameters. The mathematical model demonstrates a good fit to the observed experimental data and accurately describes the distribution of infiltrating T cells. This model is designed to complement the in vitro system; with the potential to elucidate complex biological mechanisms, including the mode of action of novel therapies and the drivers of safety events, and, ultimately, improve the efficacy-safety profile of T cell-targeted cancer immunotherapies. [ABSTRACT FROM AUTHOR]

Published

2022

12. Bariatric-induced microbiome changes alter MASLD development in association with changes in the innate immune system.

Author

Shera, Simer, Katzka, William, Yang, Julianne C., Chang, Candace, Arias-Jayo, Nerea, Lagishetty, Venu, Balioukova, Anna, Yijun Chen, Dutson, Erik, Zhaoping Li, Mayer, Emeran A., Pisegna, Joseph R., Sanmiguel, Claudia, Pawar, Shrey, Zhang, David, Leitman, Madelaine, Hernandez, Laura, Jacobs, Jonathan P., and Dong, Tien S.

Subjects

CYTOTOXIC T cells, KILLER cells, BARIATRIC surgery, SLEEVE gastrectomy, WEIGHT gain, WEIGHT loss

Abstract

Introduction: Metabolic dysfunction-associated steatotic liver disease (MASLD) affects nearly 25% of the population and is the leading cause for liver-related mortality. Bariatric surgery is a well-known treatment for MASLD and obesity. Understanding the fundamental mechanisms by which bariatric surgery can alter MASLD can lead to new avenues of therapy and research. Previous studies have identified the microbiome's role in bariatric surgery and in inflammatory immune cell populations. The host innate immune system modulates hepatic inflammation and fibrosis, and thus the progression of MASLD. The precise role of immune cell types in the pathogenesis of MASLD remains an active area of investigation. The aim of this study was to understand the interplay between microbiota composition post-bariatric surgery and the immune system in MASLD. Methods: Eighteen morbidly obese females undergoing sleeve gastrectomy were followed pre-and post-surgery. Stool from four patients, showing resolved MASLD post-surgery with sustained weight loss, was transplanted into antibiotic treated mice. Mice received pre-or post-surgery stool and were fed a standard or high-fat diet. Bodyweight, food intake, and physiological parameters were tracked weekly. Metabolic parameters were measured post-study termination. Results: The human study revealed that bariatric surgery led to significant weight loss (p > 0.05), decreased inflammatory markers, and improved glucose levels six months post-surgery. Patients with weight loss of 20% or more showed distinct changes in blood metabolites and gut microbiome composition, notably an increase in Bacteroides. The mouse model confirmed surgery-induced microbiome changes to be a major factor in the reduction of markers and attenuation of MASLD progression. Mice receiving post-surgery fecal transplants had significantly less weight gain and liver steatosis compared to pre-surgery recipients. There was also a significant decrease in inflammatory cytokines interferon gamma, interleukin 2, interleukin 15, and mig. This was accompanied by alterations in liver immunophenotype, including an increase in natural killer T cells and reduction of Kupfer cells in the post-surgery transplant group. Discussion: Our findings suggest surgery induced microbial changes significantly reduce inflammatory markers and fatty liver progression. The results indicate a potential causal link between the microbiome and the host immune system, possibly mediated through modulation of liver NKT and Kupffer cells. [ABSTRACT FROM AUTHOR]

Published

2024

13. Traversing the bench to bedside journey for iNKT cell therapies.

Author

O'Neal, Julie, Mavers, Melissa, Jayasinghe, Reyka G., and DiPersio, John F.

Subjects

GRAFT versus host disease, KILLER cells, CYTOTOXIC T cells, CHIMERIC antigen receptors, HEMATOPOIETIC stem cells

Abstract

Invariant natural killer T (iNKT) cells are immune cells that harness properties of both the innate and adaptive immune system and exert multiple functions critical for the control of various diseases. Prevention of graft-versus-host disease (GVHD) by iNKT cells has been demonstrated in mouse models and in correlative human studies in which high iNKT cell content in the donor graft is associated with reduced GVHD in the setting of allogeneic hematopoietic stem cell transplants. This suggests that approaches to increase the number of iNKT cells in the setting of an allogeneic transplant may reduce GVHD. iNKT cells can also induce cytolysis of tumor cells, and murine experiments demonstrate that activating iNKT cells in vivo or treating mice with ex vivo expanded iNKT cells can reduce tumor burden. More recently, research has focused on testing anti-tumor efficacy of iNKT cells genetically modified to express a chimeric antigen receptor (CAR) protein (CAR-iNKT) cells to enhance iNKT cell tumor killing. Further, several of these approaches are now being tested in clinical trials, with strong safety signals demonstrated, though efficacy remains to be established following these early phase clinical trials. Here we review the progress in the field relating to role of iNKT cells in GVHD prevention and anti- cancer efficacy. Although the iNKT field is progressing at an exciting rate, there is much to learn regarding iNKT cell subset immunophenotype and functional relationships, optimal ex vivo expansion approaches, ideal treatment protocols, need for cytokine support, and rejection risk of iNKT cells in the allogeneic setting. [ABSTRACT FROM AUTHOR]

Published

2024

14. Single-cell analysis of human PBMCs in healthy and type 2 diabetes populations: dysregulated immune networks in type 2 diabetes unveiled through single-cell profiling.

Author

Doeon Gu, Jinyeong Lim, Kyung Yeon Han, In-Ho Seo, Jae Hwan Jee, Soo Jin Cho, Yoon Ho Choi, Sung Chul Choi, Jang Hyun Koh, Jin-Young Lee, Mira Kang, Dong-Hyuk Jung, and Woong-Yang Park

Subjects

TYPE 2 diabetes, MONONUCLEAR leukocytes, B cells, T cells, CYTOTOXIC T cells, B cell differentiation, IMMUNOLOGIC memory, CLONE cells

Abstract

Abnormalities in glucose metabolism that precede the onset of type 2 diabetes (T2D) activate immune cells, leading to elevated inflammatory factors and chronic inflammation. However, no single-cell RNA sequencing (scRNA-seq) studies have characterized the properties and networks of individual immune cells in T2D. Here, we analyzed peripheral blood mononuclear cells (PBMCs) from non-diabetes and T2D patients by scRNA-seq. We found that CD14 monocytes in T2D patients were in a pro-inflammatory state and intermediate monocytes expressed more MHC class II genes. In T2D patients, cytotoxic CD4 T cells, effector memory CD8 T cells, and gd T cells have increased cytotoxicity and clonal expansion. B cells were characterized by increased differentiation into intermediate B cells, plasma cells, and isotype class switching with increased expression of soluble antibody genes. These results suggest that monocytes, T cells, and B cells could interact to induce chronic inflammation in T2D patients with pro-inflammatory characteristics. [ABSTRACT FROM AUTHOR]

Published

2024

15. Graft-versus-tumor effect of post-transplant cyclophosphamide-based allogeneic hematopoietic cell transplantation.

Author

Hirohisa Nakamae

Subjects

HEMATOPOIETIC stem cell transplantation, KILLER cells, CYTOTOXIC T cells, IMMUNE reconstitution inflammatory syndrome, GRAFT versus host disease, TREATMENT effectiveness

Abstract

Post-transplant cyclophosphamide (PTCy) is becoming the standard prophylaxis for graft-versus-host disease (GVHD) in HLA-haploidentical allogeneic hematopoietic cell transplantation (allo-HCT) and in HLA-matched allo-HCT. Immune reconstitution in the post-transplant setting may influence the graftversus- tumor (GVT) effect because PTCy has a profound effect on T cell and natural killer cell functions and their reconstitution after allo-HCT. However, many recent studies have shown that the incidence of relapse after allo-HCT with PTCy is comparable to that after conventional allo-HCT. To further improve the outcomes, it is critical to establish a strategy to maintain or effectively induce the GVT effect when using PTCy as a platform for GVHD prophylaxis. However, there is a paucity of studies focusing on the GVT effect in allo-HCT with PTCy. Therefore, focusing on this issue may lead to the establishment of more appropriate strategies to improve transplantation outcomes without exacerbating GVHD, including novel therapies involving cell modification. [ABSTRACT FROM AUTHOR]

Published

2024

16. Combination of JAK inhibitor and immune checkpoint inhibitor in clinical trials: a breakthrough.

Author

Shiqing Dong and Zhongnan Ma

Subjects

LIFE sciences, DRUG side effects, REGULATORY T cells, CYTOTOXIC T cells, IMMUNE checkpoint inhibitors, OVARIAN cancer, AUTOIMMUNE diseases

Abstract

The article discusses the combination of Janus kinase (JAK) inhibitors and immune checkpoint inhibitors in clinical trials, showing promising results in treating Hodgkin lymphoma and non-small cell lung cancer. The combination therapy aims to enhance antitumor immunity by reversing T-cell exhaustion, modulating the tumor microenvironment, and enhancing antigen presentation. Challenges such as safety, patient selection, dosing, and resistance mechanisms need to be addressed for the full potential of this therapy. While the studies provide encouraging results, further research is needed to apply this approach to a wider range of cancer types and explore combination with other emerging therapies. [Extracted from the article]

Published

2024

17. Combination of JAK inhibitor and immune checkpoint inhibitor in clinical trials: a breakthrough.

Author

Shiqing Dong and Zhongnan Ma

Subjects

LIFE sciences, DRUG side effects, REGULATORY T cells, CYTOTOXIC T cells, IMMUNE checkpoint inhibitors, OVARIAN cancer, AUTOIMMUNE diseases

Abstract

The article discusses the combination of Janus kinase (JAK) inhibitors and immune checkpoint inhibitors in clinical trials as a breakthrough in cancer treatment. The combination therapy has shown improved clinical responses in patients with Hodgkin lymphoma and non-small cell lung cancer. By enhancing T-cell activity and reducing immune resistance, the combination therapy has demonstrated promising results in preclinical and clinical studies. However, challenges related to safety, patient selection, dosing, and resistance mechanisms need to be addressed for the full potential of this therapy to be realized. [Extracted from the article]

Published

2024

18. Editorial: Community series in the role of CD1- and MR1-restricted T cells in immunity and disease, volume II.

Author

Kazuya Iwabuchi and Van Kaer, Luc

Subjects

CYTOTOXIC T cells, KILLER cells, CELL physiology, TISSUE physiology, T cell receptors

Abstract

This document is a summary of a collection of articles from the journal Frontiers in Immunology, focusing on the role of CD1- and MR1-restricted T cells in immunity and disease. The articles discuss various topics, including the repertoire of lipids associated with CD1 isoforms, the mechanisms of iNKT cell recognition of glycolipid antigens, and the heterogeneity of iNKT cells in different tissues. They also explore the potential of NKT cells as targets for immune therapies in inflammatory bowel disease and obesity-associated tissue inflammation. The articles provide insights into the functions and regulation of these T cell subsets and highlight their potential for the development of new immunotherapies. [Extracted from the article]

Published

2024

19. T‐ and B‐cell therapy in solid organ transplantation: current evidence and future expectations.

Author

Pilat, Nina, Lefsihane, Katia, Brouard, Sophie, Kotsch, Katja, Falk, Christine, Steiner, Romy, Thaunat, Olivier, Fusil, Floriane, Montserrat, Nuria, Amarelli, Cristiano, and Casiraghi, Federica

Subjects

THERAPEUTICS, TRANSPLANTATION of organs, tissues, etc., CYTOTOXIC T cells, B cells, REGULATORY T cells, PSYCHONEUROIMMUNOLOGY

Abstract

Summary: Cell therapy has emerged as an attractive therapeutic option in organ transplantation. During the last decade, the therapeutic potency of Treg immunotherapy has been shown in various preclinical animal models and safety was demonstrated in first clinical trials. However, there are still critical open questions regarding specificity, survival, and migration to the target tissue so the best Treg population for infusion into patients is still under debate. Recent advances in CAR technology hold the promise for Treg‐functional superiority. Another exciting strategy is the generation of B‐cell antibody receptor (BAR) Treg/cytotoxic T cells to specifically regulate or deplete alloreactive memory B cells. Finally, B cells are also capable of immune regulation, making them promising candidates for immunomodulatory therapeutic strategies. This article summarizes available literature on cell‐based innovative therapeutic approaches aiming at modulating alloimmune response for transplantation. Crucial areas of investigation that need a joined effort of the transplant community for moving the field toward successful achievement of tolerance are highlighted. [ABSTRACT FROM AUTHOR]

Published

2021

20. The C1q and gC1qR axis as a novel checkpoint inhibitor in cancer.

Author

Ghebrehiwet, Berhane, Zaniewski, Michal, Fernandez, Audrey, DiGiovanni, Mathew, Reyes, Tiana N., Ping Ji, Savitt, Anne G., Williams, Jennie L., Seeliger, Markus A., and Peerschke, Ellinor I. B.

Subjects

CYTOTOXIC T cells, CYTOLOGY, CANCER cell proliferation, CANCER cells, IPILIMUMAB, ECULIZUMAB, T cells

Abstract

Understanding at the molecular level of the cell biology of tumors has led to significant treatment advances in the past. Despite such advances however, development of therapy resistance and tumor recurrence are still unresolved major challenges. This therefore underscores the need to identify novel tumor targets and develop corresponding therapies to supplement existing biologic and cytotoxic approaches so that a deeper and more sustained treatment responses could be achieved. The complement system is emerging as a potential novel target for cancer therapy. Data accumulated to date show that complement proteins, and in particular C1q and its receptors cC1qR/CR and gC1qR/p33/HABP1, are overexpressed in most cancer cells and together are involved not only in shaping the inflammatory tumor microenvironment, but also in the regulation of angiogenesis, metastasis, and cell proliferation. In addition to the soluble form of C1q that is found in plasma, the C1q molecule is also found anchored on the cell membrane of monocytes, macrophages, dendritic cells, and cancer cells, via a 22aa long leader peptide found only in the A-chain. This orientation leaves its 6 globular heads exposed outwardly and thus available for high affinity binding to a wide range of molecular ligands that enhance tumor cell survival, migration, and proliferation. Similarly, the gC1qR molecule is not only overexpressed in most cancer types but is also released into the microenvironment where it has been shown to be associated with cancer cell proliferation and metastasis by activation of the complement and kinin systems. Co-culture of either T cells or cancer cells with purified C1q or anti-gC1qR has been shown to induce an anti-proliferative response. It is therefore postulated that in the tumor microenvironment, the interaction between C1q expressing cancer cells and gC1qR bearing cytotoxic T cells results in T cell suppression in a manner akin to the PD-L1 and PD-1 interaction. [ABSTRACT FROM AUTHOR]

Published

2024

21. Extracellular vesicle-mediated communication between CD8+ cytotoxic T cells and tumor cells.

Author

Zeyu Huang, Xuehui Liu, Qinghao Guo, Yihang Zhou, Linlin Shi, Qingjin Cai, Shupei Tang, Qin Ouyang, and Ji Zheng

Subjects

CYTOTOXIC T cells, T cells, EXTRACELLULAR vesicles, CELL physiology, TUMOR microenvironment

Abstract

Tumors pose a significant global public health challenge, resulting in numerous fatalities annually. CD8+ T cells play a crucial role in combating tumors; however, their effectiveness is compromised by the tumor itself and the tumor microenvironment (TME), resulting in reduced efficacy of immunotherapy. In this dynamic interplay, extracellular vesicles (EVs) have emerged as pivotal mediators, facilitating direct and indirect communication between tumors and CD8+ T cells. In this article, we provide an overview of how tumor-derived EVs directly regulate CD8+ T cell function by carrying bioactive molecules they carry internally and on their surface. Simultaneously, these EVs modulate the TME, indirectly influencing the efficiency of CD8+ T cell responses. Furthermore, EVs derived from CD8+ T cells exhibit a dual role: they promote tumor immune evasion while also enhancing antitumor activity. Finally, we briefly discuss current prevailing approaches that utilize functionalized EVs based on tumor-targeted therapy and tumor immunotherapy. These approaches aim to present novel perspectives for EV-based tumor treatment strategies, demonstrating potential for advancements in the field. [ABSTRACT FROM AUTHOR]

Published

2024

22. Single-cell RNA sequencing reveals Immune Education promotes T cell survival in mice subjected to the cecal ligation and puncture sepsis model.

Author

Ham, Steven D., Abraham, Mabel N., Deutschman, Clifford S., and Taylor, Matthew D.

Subjects

T cells, CYTOTOXIC T cells, RNA sequencing, CELL survival, IMMUNOLOGIC memory

Abstract

Background: Individual T cell responses vary significantly based on the microenvironment present at the time of immune response and on prior induced T cell memory. While the cecal ligation and puncture (CLP) model is the most commonly used murine sepsis model, the contribution of diverse T cell responses has not been explored. We defined T cell subset responses to CLP using single-cell RNA sequencing and examined the effects of prior induced T cell memory (Immune Education) on these responses. We hypothesized that Immune Education prior to CLP would alter T cell responses at the single cell level at a single, early post-CLP time point. Methods: Splenic T cells were isolated from C57BL/6 mice. Four cohorts were studied: Control, Immune-Educated, CLP, and Immune-Educated CLP. At age 8 weeks, Immune-Educated and Immune-Educated CLP mice received anti-CD3? antibody; Control and CLP mice were administered an isotype control. CLP (two punctures with a 22-gauge needle) was performed at 12-13 weeks of life. Mice were sacrificed at baseline or 24-hours post-CLP. Unsupervised clustering of the transcriptome library identified six distinct T cell subsets: quiescent naïve CD4+, primed naïve CD4+, memory CD4+, naïve CD8+, activated CD8+, and CD8+ cytotoxic T cell subsets. T cell subset specific gene set enrichment analysis and Hurdle analysis for differentially expressed genes (DEGs) were performed. Results: T cell responses to CLP were not uniform - subsets of activated and suppressed T cells were identified. Immune Education augmented specific T cell subsets and led to genomic signatures favoring T cell survival in unoperated and CLP mice. Additionally, the combination of Immune Education and CLP effected the expression of genes related to T cell activity in ways that differed from CLP alone. Validating our finding that IL7R pathway markers were upregulated in Immune-Educated CLP mice, we found that Immune Education increased T cell surface IL7R expression in post-CLP mice. Conclusion: Immune Education enhanced the expression of genes associated with T cell survival in unoperated and CLP mice. Induction of memory T cell compartments via Immune Education combined with CLP may increase the model's concordance to human sepsis. [ABSTRACT FROM AUTHOR]

Published

2024

23. Cytotoxic response of tumor-infiltrating lymphocytes of head and neck cancer slice cultures under mitochondrial dysfunction.

Author

Greier, Maria do Carmo, Runge, Annette, Dudas, Jozsef, Hartl, Roland, Santer, Matthias, Dejaco, Daniel, Steinbichler, Teresa Bernadette, Federspiel, Julia, Seifarth, Christof, Konschake, Marko, Sprung, Susanne, Sopper, Sieghart, Randhawa, Avneet, Mayr, Melissa, Hofauer, Benedikt Gabriel, and Riechelmann, Herbert

Subjects

HEAD & neck cancer, CYTOTOXIC T cells, TUMOR-infiltrating immune cells, CELL physiology, MITOCHONDRIA, METABOLIC reprogramming

Abstract

Background: Head and neck squamous cell carcinomas (HNSCC) are highly heterogeneous tumors. In the harsh tumor microenvironment (TME), metabolic reprogramming and mitochondrial dysfunction may lead to immunosuppressive phenotypes. Aerobic glycolysis is needed for the activation of cytotoxic T-cells and the absence of glucose may hamper the full effector functions of cytotoxic T-cells. To test the effect of mitochondrial dysfunction on cytotoxic T cell function, slice cultures (SC) of HNSCC cancer were cultivated under different metabolic conditions. Methods: Tumor samples from 21 patients with HNSCC were collected, from which, SC were established and cultivated under six different conditions. These conditions included high glucose, T cell stimulation, and temporarily induced mitochondrial dysfunction (MitoDys) using FCCP and oligomycin A with or without additional T cell stimulation, high glucose and finally, a control medium. Over three days of cultivation, sequential T cell stimulation and MitoDys treatments were performed. Supernatant was collected, and SC were fixed and embedded. Granzyme B was measured in the supernatant and in the SC via immunohistochemistry (IHC). Staining of PD1, CD8/Ki67, and cleavedcaspase3 (CC3) were performed in SC. Results: Hematoxylin eosin stains showed that overall SC quality remained stable over 3 days of cultivation. T cell stimulation, both alone and combined with MitoDys, led to significantly increased granzyme levels in SC and in supernatant. Apoptosis following T cell stimulation was observed in tumor and stroma. Mitochondrial dysfunction alone increased apoptosis in tumor cell aggregates. High glucose concentration alone had no impact on T cell activity and apoptosis. Apoptosis rates were significantly lower under conditions with high glucose and MitoDys (p=0.03). Conclusion: Stimulation of tumor-infiltrating lymphocytes in SC was feasible, which led to increased apoptosis in tumor cells. Induced mitochondrial dysfunction did not play a significant role in the activation and function of TILs in SC of HNSCC. Moreover, high glucose concentration did not promote cytotoxic T cell activity in HNSCC SC. [ABSTRACT FROM AUTHOR]

Published

2024

24. Dynamics of SARS-CoV-2 immunity after vaccination and breakthrough infection in rituximab-treated rheumatoid arthritis patients: a prospective cohort study.

Author

Kared, Hassen, Jyssum, Ingrid, Alirezaylavasani, Amin, Egner, Ingrid M., Trung The Tran, Tietze, Lisa, Lund, Katrine Persgård, Tveter, Anne Therese, Provan, Sella A., Ørbo, Hilde, Haavardsholm, Espen A., Vaage, John Torgils, Jørgensen, Kristin, Syversen, Silje Watterdal, Lund-Johansen, Fridtjof, Goll, Guro Løvik, and Munthe, Ludvig A.

Subjects

BREAKTHROUGH infections, CYTOTOXIC T cells, RHEUMATOID arthritis, IMMUNOLOGIC memory, IMMUNITY

Abstract

Background: SARS-CoV-2 vaccination in rheumatoid arthritis (RA) patients treated with B cell-depleting drugs induced limited seroconversion but robust cellular response. We aimed to document specific T and B cell immunity in response to vaccine booster doses and breakthrough infection (BTI). Methods: We included 76 RA patients treated with rituximab who received up to four SARS-CoV-2 vaccine doses or three doses plus BTI, in addition to vaccinated healthy donors (HD) and control patients treated with tumor necrosis factor inhibitor (TNFi). We quantified anti-SARS-CoV-2 receptor-binding domain (RBD) Spike IgG, anti-nucleocapsid (NC) IgG, 92 circulating inflammatory proteins, Spike-binding B cells, and Spike-specific T cells along with comprehensive high-dimensional phenotyping and functional assays. Findings: The time since the last rituximab infusion, persistent inflammation, and age were associated with the anti-SARS-CoV-2 RBD IgG seroconversion. The vaccine-elicited serological response was accompanied by an incomplete induction of peripheral Spike-specific memory B cells but occurred independently of T cell responses. Vaccine- and BTI-elicited cellular immunity was similar between RA and HD ex vivo in terms of frequency or phenotype of Spike-specific cytotoxic T cells and in vitro in terms of the functionality and differentiation profile of Spike-specific T cells. Interpretation: SARS-CoV-2 vaccination in RA can induce persistent effector T-cell responses that are reactivated by BTI. Paused rituximab medication allowed serological responses after a booster dose (D4), especially in RA with lower inflammation, enabling efficient humoral and cellular immunity after BTI, and contributed overall to the development of potential durable immunity. [ABSTRACT FROM AUTHOR]

Published

2024

25. Combined effects of exercise and immuno-chemotherapy treatments on tumor growth in MC38 colorectal cancer-bearing mice.

Author

Gouez, Manon, Rébillard, Amélie, Thomas, Amandine, Beaumel, Sabine, Matera, Eva-Laure, Gouraud, Etienne, Orfila, Luz, Martin, Brice, Pérol, Olivia, Chaveroux, Cédric, Chirico, Erica N., Dumontet, Charles, Fervers, Béatrice, and Pialoux, Vincent

Subjects

TUMOR growth, TUMOR treatment, CYTOTOXIC T cells, IMMUNE checkpoint inhibitors, TUMOR microenvironment

Abstract

Acute exercise induces transient modifications in the tumor microenvironment and has been linked to reduced tumor growth along with increased infiltration of immune cells within the tumor in mouse models. In this study, we aimed to evaluate the impact of acute exercise before treatment administration on tumor growth in a mice model of MC38 colorectal cancer receiving an immune checkpoint inhibitor (ICI) and chemotherapy. Six-week-old mice injected with colorectal cancer cells (MC38) were randomized in 4 groups: control (CTRL), immuno-chemotherapy (TRT), exercise (EXE) and combined intervention (TRT/ EXE). Both TRT and TRT-EXE received ICI: anti-PD1-1 (1 injection/week) and capecitabine + oxaliplatin (5 times a week) for 1 week (experimentation 1), 3 weeks (experimentation 2). TRT-EXE and EXE groups were submitted to 50 minutes of treadmill exercise before each treatment administration. Over the protocol duration, tumor size has been monitored daily. Tumor growth and microenvironment parameters were measured after the intervention on Day 7 (D7) and Day 16 (D16). From day 4 to day 7, tumor volumes decreased in the EXE/ TRT group while remaining stable in the TRT group (p=0.0213). From day 7 until day 16 tumor volume decreased with no significant difference between TRT and TRT/EXE. At D7 the TRT/EXE group exhibited a higher total infiltrate T cell (p=0.0118) and CD8+ cytotoxic T cell (p=0.0031). At D16, tumor marker of apoptosis, vascular integrity and inflammation were not significantly different between TRT and TRT/EXE. Our main result was that acute exercise before immuno-chemotherapy administration significantly decreased early-phase tumor growth (D0 to D4). Additionally, exercise led to immune cell infiltration changes during the first week after exercise, while no significant molecular alterations in the tumor were observed 3 weeks after exercise. [ABSTRACT FROM AUTHOR]

Published

2024

26. CXCR5+TIM-3-PD-1+ stem-like cytotoxic CD8+ T cells: elevated in chronic rhinosinusitis and associated with disease severity.

Author

Zhichen Liu, Zixuan Zhao, Huanxia Xie, Ning Lu, Jisheng Liu, and Qingqing Jiao

Subjects

CYTOTOXIC T cells, AUTOIMMUNE diseases, CHEMOKINE receptors, BLOOD cell count, T-cell exhaustion, T cells

Abstract

Background: Chronic rhinosinusitis (CRS) is a chronic inflammatory disease with an autoimmune background. Altered expression levels of T cell immunoglobulin and mucin-domain containing-3 (TIM-3), C-X-C chemokine receptor type 5 (CXCR5), and programmed cell death protein 1 (PD-1) are implicated in the progression of inflammatory and autoimmune diseases. Moreover, CXCR5+TIM-3-PD-1+ stem-like cytotoxic T cells function as memory stem cells during chronic disease processes and retain cytotoxicityrelated gene networks. Objectives: To explore the expressions of CXCR5, TIM-3, and PD-1 on T cells and their correlation with clinical parameters in CRS. Methods: Flow cytometry was used to assess the expressions and coexpressions of CXCR5, TIM-3, and PD-1 on T cells in the tissues of the paranasal sinus and peripheral blood of patients with CRS as well as healthy controls. Immunofluorescence was used to assess the co-localization of TIM-3, CXCR5, and PD-1 with T cells. The disease severity of our patients with CRS was evaluated using the Lund-Mackay score. A complete blood count was also performed for the patients with CRS. Results: Expression levels of CXCR5 and PD-1 on T cells were significantly increased in the nasal tissues of patients with CRS. Compared with those in healthy controls, patients with CRS had high percentages of CXCR5+TIM-3-PD-1+ CD8+ and CD4+ T cells in nasal tissues, while no significant difference was observed in peripheral blood levels. Patients with CRS had a higher density of nasal CXCR5+TIM-3-PD-1+ T cells than that in healthy controls. CXCR5+TIM-3-PD-1+ CD8+ T cell levels in the nasal polyps of patients with CRS were negatively correlated with the patients' Lund-Mackay scores. The levels of CXCR5+TIM-3-PD-1+ T cells in nasal tissues were also negatively associated with disease duration and positively associated with the chronic inflammatory state of CRS. Conclusions: The level of CXCR5+TIM-3-PD-1+ stem cell-like T cells, especially CXCR5+TIM-3-PD-1+ CD8+ T cells, is increased in CRS. Therefore, inducing CXCR5+TIM-3-PD-1+ T cell exhaustion may be an effective immunotherapy for CRS. [ABSTRACT FROM AUTHOR]

Published

2024

27. Delivery of Mycobacterium tuberculosis epitopes by Bordetella pertussis adenylate cyclase toxoid expands HLA-E-restricted cytotoxic CD8+ T cells.

Author

Badami, Giusto D., La Manna, Marco P., Di Carlo, Paola, Stanek, Ondrej, Linhartova, Irena, Caccamo, Nadia, Sebo, Peter, and Dieli, Francesco

Subjects

CYTOTOXIC T cells, ADENYLATE cyclase, MYCOBACTERIUM tuberculosis, BORDETELLA pertussis, BCG vaccines, EPITOPES

Abstract

Introduction: Tuberculosis (TB) remains the first cause of death from infection caused by a bacterial pathogen. Chemotherapy does not eradicate Mycobacterium tuberculosis (Mtb) fromhuman lungs, andthe pathogen causes a latent tuberculosis infectionthatcannotbepreventedbythecurrently availableBacilleCalmetteGuerin (BCG) vaccine, which is ineffective inthe prevention of pulmonary TBinadults. HLAE-restricted CD8+ T lymphocytes are essential players in protective immune responses against Mtb. Hence, expanding this population in vivo or ex vivo may be crucial for vaccination or immunotherapy against TB. Methods: The enzymatically inactive Bordetella pertussis adenylate cyclase (CyaA) toxoid is an effective tool for delivering peptide epitopes into the cytosol of antigen-presenting cells (APC) for presentation and stimulation of specific CD8+ T-cell responses. In this study, we have investigated the capacity of the CyaA toxoid to deliver Mtb epitopes known to bind HLA-E for the expansion of human CD8+ T cells in vitro. Results: Our results show that the CyaA-toxoid containing five HLA-E-restricted Mtb epitopes causes significant expansion of HLA-E-restricted antigen-specific CD8+ T cells, which produce IFN-g and exert significant cytotoxic activity towards peptide-pulsed macrophages. Discussion: HLA-E represents a promising platform for the development of new vaccines; our study indicates that the CyaA construct represents a suitable delivery system of the HLA-E-binding Mtb epitopes for ex vivo and in vitro expansion of HLA-E-restricted CD8+ T cells inducing a predominant Tc1 cytokine profile with a significant increase of IFN-γ production, for prophylactic and immunotherapeutic applications against Mtb. [ABSTRACT FROM AUTHOR]

Published

2023

28. Editorial: Host-Pathogen Interactions During Pneumococcal Infection.

Author

Yamaguchi, Masaya, Kinjo, Yuki, and Nizet, Victor

Subjects

MEDICAL sciences, ELASTASES, CYTOTOXIC T cells, INFECTION, LECTINS

Published

2021

29. Targeting of tumor cells by custom antigen transfer: a novel approach for immunotherapy of cancer.

Author

Nesi, Ilaria, Bella, Chiara Della, Taddei, Maria Letizia, Santi, Alice, Pranzini, Erica, Paoli, Paolo, D'Elios, Mario Milco, Ramazzotti, Matteo, Genovese, Massimo, Caselli, Anna, and Cirri, Paolo

Subjects

CYTOTOXIC T cells, MAJOR histocompatibility complex, GENETIC drift, IMMUNE system, IMMUNOTHERAPY, HUMAN carcinogenesis

Abstract

In the early stages of carcinogenesis, the transformed cells become "invisible" to the immune system. From this moment on, the evolution of the tumor depends essentially on the genotype of the primitive cancer cells and their subsequent genetic drift. The role of the immune system in blocking tumor progression from the earliest stages is largely underestimated because by the time tumors are clinically detectable, the immune system has already completely failed its task. Therefore, a clinical treatment capable of restoring the natural anti-tumor role of the immune system could prove to be the "ultimate weapon" against cancer. Herein, we propose a novel therapeutic approach for the treatment of solid cancer that exploits the capability of activated monocytes to transfer major histocompatibility complex I (MHC-I) molecules bound to antigenic peptides to cancer cells using microvesicles as cargo, making tumor cells target of a "natural" CD8+ T lymphocyte cytotoxic response. [ABSTRACT FROM AUTHOR]

Published

2023

30. Immunological analysis of hybrid neoantigen peptide encompassing class I/II neoepitope-pulsed dendritic cell vaccine.

Author

Shinji Morisaki, Hideya Onishi, Takafumi Morisaki, Makoto Kubo, Masayo Umebayashi, Hiroto Tanaka, Norihiro Koya, Shinichiro Nakagawa, Kenta Tsujimura, Sachiko Yoshimura, Poh Yin Yew, Kazuma Kiyotani, Yusuke Nakamura, Masafumi Nakamura, Takanari Kitazono, and Takashi Morisaki

Subjects

PEPTIDES, CYTOTOXIC T cells, DENDRITIC cells, T cell receptors, HLA histocompatibility antigens, T cells

Abstract

Neoantigens/ are tumor-specific antigens that evade central immune tolerance mechanisms in the thymus. Long-term tumor-specific cytotoxic T lymphocyte activity maintenance requires class II antigen-reactive CD4+ T cells. We had previously shown that intranodal vaccination with class I neoantigen peptidepulsed dendritic cells (DCs) induced a robust immune response in a subset of patients with metastatic cancer. The present study aimed to perform a detailed ex vivo analysis of immune responses in four patients receiving an intranodal hybrid human leukocyte antigen class II neoantigen peptide encompassing a class I neoantigen epitope (hybrid neoantigen)-pulsed DC vaccine. After vaccination, strong T-cell reactions against the hybrid class II peptide and the class I-binding neoantigen peptide were observed in all four patients. We found that hybrid class II neoantigen peptide-pulsed DCs stimulated CD4+ T cells via direct antigen presentation and CD8+ T cells via cross-presentation. Further, we demonstrated that hybrid class II peptides encompassing multiple class I neoantigen epitope-pulsed DCs could present multiple class I peptides to CD8+ T cells via cross-presentation. Our findings provide insight into the mechanisms underlying hybrid neoantigen-pulsed DC vaccine therapy and suggest future neoantigen vaccine design. [ABSTRACT FROM AUTHOR]

Published

2023

31. High CD8+ tumor-infiltrating lymphocytes indicate severe exhaustion and poor prognosis in angioimmunoblastic T-cell lymphoma.

Author

Qiqi Zhu, Yiming Yang, Xueqin Deng, Ningning Chao, Zihang Chen, Yunxia Ye, Wenyan Zhang, Weiping Liu, and Sha Zhao

Subjects

FATIGUE (Physiology), T-cell lymphoma, TUMOR-infiltrating immune cells, CYTOTOXIC T cells, CD8 antigen

Abstract

Background: Exhaustion of CD8+ tumor-infiltrating lymphocytes (TILs), characterized by the overexpression of immune checkpoints (IC), is a major impediment to anti-tumor immunity. However, the exhaustion status of CD8+TILs in angioimmunoblastic T cell lymphoma (AITL) remains unclear. Therefore, we aimed to elucidate the exhaustion status of CD8+TILs in AITL and its influence on prognosis. Methods: The correlation between CD8+TILs and IC expression in AITL was analyzed using single-cell RNA sequencing (n = 2), flow cytometry (n = 20), and RNA sequencing (n = 20). Biological changes related to CD8+TILs exhaustion at different cytotoxic T lymphocyte (CTL) levels (mean expression levels of CD8A, CD8B, GZMA, GZMB, and PRF1) in AITL were evaluated using RNA sequencing (n = 20) and further validated using the GEO dataset (n = 51). The impact of CD8 protein expression and CTL levels on patient prognosis was analyzed using flow cytometry and RNA sequencing, respectively. Results: Our findings demonstrated that the higher the infiltration of CD8+TILs, the higher was the proportion of exhausted CD8+TILs characterized by the overexpression of multiple IC. This was accompanied by extensive exhaustion- related biological changes, which suggested severe exhaustion in CD8+TILs and may be one of the main reasons for the poor prognosis of patients with high CD8+TILs and CTL. Conclusion: Our study comprehensively reveals the exhaustion status of CD8+TILs and their potential negative impact on AITL prognosis, which facilitates further mechanistic studies and is valuable for guiding immunotherapy strategies. [ABSTRACT FROM AUTHOR]

Published

2023

32. Induction of liver-resident memory T cells and protection at liver-stage malaria by mRNA-containing lipid nanoparticles.

Author

Sayuri Nakamae, Satoshi Miyagawa, Koki Ogawa, Mariko Kamiya, Mayumi Taniguchi, Akari Ono, Maho Kawaguchi, Teklemichael, Awet Alem, Jiun-Yu Jian, Tamasa Araki, Yukimi Katagami, Hidefumi Mukai, Takeshi Annoura, Katsuyuki Yui, Kenji Hirayama, Shigeru Kawakami, and Shusaku Mizukami

Subjects

IMMUNOLOGIC memory, CYTOTOXIC T cells, MALARIA, CIRCUMSPOROZOITE protein, LIVER cells

Abstract

Recent studies have suggested that CD8+ liver-resident memory T (TRM) cells are crucial in the protection against liver-stage malaria. We used liver-directed mRNA-containing lipid nanoparticles (mRNA-LNPs) to induce liver TRM cells in a murine model. Single-dose intravenous injections of ovalbumin mRNA-LNPs effectively induced antigen-specific cytotoxic T lymphocytes in a dose-dependent manner in the liver on day 7. TRM cells (CD8+ CD44hi CD62Llo CD69+ KLRG1-) were induced 5 weeks after immunization. To examine the protective efficacy, mice were intramuscularly immunized with two doses of circumsporozoite protein mRNA-LNPs at 3-week intervals and challenged with sporozoites of Plasmodium berghei ANKA. Sterile immunity was observed in some of the mice, and the other mice showed a delay in blood-stage development when compared with the control mice. mRNA-LNPs therefore induce memory CD8+ T cells that can protect against sporozoites during liver-stage malaria and may provide a basis for vaccines against the disease. [ABSTRACT FROM AUTHOR]

Published

2023

33. Dynamic evaluation of blood immune cells predictive of response to immune checkpoint inhibitors in NSCLC by multicolor spectrum flow cytometry.

Author

Weijie Ma, Sixi Wei, Siqi Long, Tian, Eddie C., McLaughlin, Bridget, Jaimes, Maria, Montoya, Dennis J., Viswanath, Varun R., Chien, Jeremy, Qianjun Zhang, Van Dyke, Jonathan E., Shuai Chen, and Tianhong Li

Subjects

IMMUNE checkpoint inhibitors, BLOOD cells, FLOW cytometry, MONONUCLEAR leukocytes, CYTOTOXIC T cells, IPILIMUMAB

Abstract

Introduction: Immune checkpoint inhibitors (ICIs) only benefit a subset of cancer patients, underlining the need for predictive biomarkers for patient selection. Given the limitations of tumor tissue availability, flow cytometry of peripheral blood mononuclear cells (PBMCs) is considered a noninvasive method for immune monitoring. This study explores the use of spectrum flow cytometry, which allows a more comprehensive analysis of a greater number of markers using fewer immune cells, to identify potential blood immune biomarkers and monitor ICI treatment in non-small-cell lung cancer (NSCLC) patients. Methods: PBMCs were collected from 14 non-small-cell lung cancer (NSCLC) patients before and after ICI treatment and 4 healthy human donors. Using spectrum flow cytometry, 24 immune cell markers were simultaneously monitored using only 1 million PBMCs. The results were also compared with those from clinical flow cytometry and bulk RNA sequencing analysis. Results: Our findings showed that the measurement of CD4+ and CD8+ T cells by spectrum flow cytometry matched well with those by clinical flow cytometry (Pearson R ranging from 0.75 to 0.95) and bulk RNA sequencing analysis (R=0.80, P=1.3 x 10-4). A lower frequency of CD4+ central memory cells before treatment was associated with a longer median progression-free survival (PFS) [Not reached (NR) vs. 5 months; hazard ratio (HR)=8.1, 95% confidence interval (CI) 1.5-42, P=0.01]. A higher frequency of CD4-CD8-double-negative (DN) T cells was associated with a longer PFS (NR vs. 4.45 months; HR=11.1, 95% CI 2.2-55.0, P=0.003). ICIs significantly changed the frequency of cytotoxic CD8+PD1+ T cells, DN T cells, CD16+CD56dim and CD16+CD56- natural killer (NK) cells, and CD14+HLDRhigh and CD11c+HLADR + monocytes. Of these immune cell subtypes, an increase in the frequency of CD16+CD56dim NK cells and CD14 +HLADRhigh monocytes after treatment compared to before treatment were associated with a longer PFS (NR vs. 5 months, HR=5.4, 95% CI 1.1-25.7, P=0.03; 7.8 vs. 3.8 months, HR=5.7, 95% CI 169 1.0-31.7, P=0.04), respectively. Conclusion: Our preliminary findings suggest that the use of multicolor spectrum flow cytometry helps identify potential blood immune biomarkers for ICI treatment, which warrants further validation. [ABSTRACT FROM AUTHOR]

Published

2023

34. Impaired thymic iNKT cell differentiation at early precursor stage in murine haploidentical bone marrow transplantation with GvHD.

Author

Weijia Zhao, Yujia Wang, Xinwei Zhang, Jie Hao, Kunshan Zhang, Xiaojun Huang, Yingjun Chang, Hounan Wu, Rong Jin, and Qing Ge

Subjects

BONE marrow transplantation, CELL differentiation, CYTOTOXIC T cells, GRAFT versus host disease, T cells

Abstract

Introduction: Early recovery of donor-derived invariant natural killer T (iNKT) cells are associated with reduced risk of graft-versus-host disease (GvHD) and overall survival. Patients with severe GvHD, however, had much slower iNKT cell reconstitution relative to conventional T cells. Methods: To characterize the delay of iNKT cell reconstitution and explore its possible causes, we used a haploidentical bone marrow transplantation (haplo-BMT) mouse model with GvHD. We found the delayed recovery of thymic and peripheral iNKT cell numbers with markedly decreased thymic NKT1 subset in GvHD mice. The defective generation of thymic iNKT precursors with egress capability contributed to the reduced peripheral iNKT cells in GvHD mice. We further identified intermediate NK1.1- NKT1 precursor subpopulations under steady-state conditions and found that the differentiation of these subpopulations was impaired in the thymi of GvHD mice. Detailed characterization of iNKT precursors and thymic microenvironment showed a close association of elevated TCR/co-stimulatory signaling provided by double positive thymocytes and macrophages with defective down-regulation of proliferation, metabolism, and NKT2 signature in iNKT precursor cells. Correspondingly, NKT2 but not NKT1 differentiation was favored in GvHD mice. Discussion: These data underline the important roles of TCR and co-stimulatory signaling in the differentiationof thymic iNKT subsets under transplantation conditions. [ABSTRACT FROM AUTHOR]

Published

2023

35. Impact of interval progression before autologous stem cell transplant in patients with multiple myeloma.

Author

Bao, Alicia, Qiuhong Zhao, Kudalkar, Ruchi, Rodriguez, Jose, Sharma, Nidhi, Bumma, Naresh, Devarakonda, Srinivas S., Khan, Abdullah M., Umyarova, Elvira, Rosko, Ashley E., Benson, Don, and Cottini, Francesca

Subjects

STEM cell transplantation, MULTIPLE myeloma, CYTOTOXIC T cells, KILLER cells, PATIENTS' attitudes

Abstract

In transplant-eligible patients who undergo upfront autologous stem cell transplant (ASCT) for multiple myeloma (MM), standard practice is to treat with six to eight cycles of induction therapy followed by high-dose chemotherapy with ASCT. A gap between the end of induction and the day of ASCT exists to allow stem cell mobilization and collection. Despite attempts to limit the length of this interval, we noticed that some patients experience interval progression (IP) of disease between the end of induction therapy and the day of ASCT. We analyzed 408 MM patients who underwent ASCT between 2011 and 2016. The median length of the interval between end of induction and ASCT was 38 days. We observed that 26% of patients in the entire cohort and 23.6% of patients who received induction with bortezomib-lenalidomide-dexamethasone (VRD) experienced IP. These patients deepened their responses with ASCT, independently of induction regimen. In the entire cohort, IP was significantly associated with shorter PFS in the univariable analysis (Hazard Ratio, HR = 1.37, P = 0.022) but not in the multivariable analysis (HR = 1.14, P = 0.44). However, analyzing only patients who received VRD as induction, progression-free survival (PFS) remained inferior in both the univariable (HR = 2.02; P = 0.002) and the multivariable analyses (HR = 1.96; P = 0.01). T cells and natural killer (NK) cells are increasingly studied targets of immunomodulatory therapy, as immune dysfunction is known to occur in patients with MM. Peripheral blood from 35 MM patients were analyzed. At time of ASCT, patients with IP had significantly increased percentages of CD3+CD8+CD57+ CD28- (P = 0.05) and CD3+CD4+LAG3+ (P = 0.0022) T-cells, as well as less CD56bright and CD56dim NK cells bearing activated markers such as CD69, NKG2D, and CD226. These data suggest that IP can impact the length of response to ASCT; therefore, further studies on the management of these patients are needed. [ABSTRACT FROM AUTHOR]

Published

2023

36. An optimized cultivation method for future in vivo application of γδ T cells.

Author

Bold, Anna, Gross, Heike, Holzmann, Elisabeth, Knop, Stefan, Hoeres, Timm, and Wilhelm, Martin

Subjects

T cells, ANTIBODY-dependent cell cytotoxicity, T cell receptors, GRAFT versus host reaction, MAJOR histocompatibility complex, CURRENT good manufacturing practices, CYTOTOXIC T cells

Abstract

γδ T cells, with their properties of both the innate and acquired immune systems, are suitable candidates for cellular immunotherapy in cancer. Because of their non-major histocompatibility complex (MHC) binding T cell receptor, allogenic transfer is feasible without relevant graft versus host reactions. In recent years, much experience has been gained with ex vivo expansion and stimulation of γδ T cells using bisphosphonates and Interleukin 2. Unfortunately, many current stimulation protocols are based on the use of xenogenic materials and other potentially hazardous supplements, which conflicts with basic principles of Good Manufacturing Practice (GMP). Adherence to the concept and current guidelines of GMP is state of the art for production of Advanced Therapy Medicinal Products (ATMP) like cell therapeutics and a necessity for clinical use under a regulatory perspective. In this study, we developed a new stimulation protocol that induces a marked increase of γδ T cell counts and allows for an easier transition from research to clinical applications with minimized regulatory workload. It reliably leads to a cell product with a purity of more than 90% γδ T cells and improved in vitro anti-tumor activity compared to our previous standard procedure. Furthermore, by investigating correlations between properties of unstimulated γδ T cells and proliferation rate as well as degranulation ability of stimulated γδ T cells, we can draw conclusions about suitable donors. Finally, we examined if expansion can be improved by pulsing zoledronate and/or using Interleukin 15 with or without Interleukin 2. Significant improvements can be achieved with respect to intrinsic and antibody-dependent cell-mediated cytotoxicity. Our results demonstrate that the stimulation protocol presented here leads to an improved γδ T cell product for future clinical applications. [ABSTRACT FROM AUTHOR]

Published

2023

37. Advances in attractive therapeutic approach for macrophage activation syndrome in COVID-19.

Author

Shunyao Chen, Cong Zhang, Deng Chen, Liming Dong, Teding Chang, and Zhao-Hui Tang

Subjects

THERAPEUTICS, COVID-19 pandemic, CONVALESCENT plasma, CYTOTOXIC T cells, BREAKTHROUGH infections, MACROPHAGE activation syndrome, AMNIOTIC fluid embolism

Abstract

Nowadays, people have relaxed their vigilance against COVID-19 due to its declining infection numbers and attenuated virulence. However, COVID-19 still needs to be concern due to its emerging variants, the relaxation of restrictions as well as breakthrough infections. During the period of the COVID-19 infection, the imbalanced and hyper-responsive immune system plays a critical role in its pathogenesis. Macrophage Activation Syndrome (MAS) is a fatal complication of immune system disease, which is caused by the excessive activation and proliferation of macrophages and cytotoxic T cells (CTL). COVID-19-related hyperinflammation shares common clinical features with the above MAS symptoms, such as hypercytokinemia, hyperferritinemia, and coagulopathy. In MAS, immune exhaustion or defective anti-viral responses leads to the inadequate cytolytic capacity of CTL which contributes to prolonged interaction between CTL, APCs and macrophages. It is possible that the same process also occurred in COVID-19 patients, and further led to a cytokine storm confined to the lungs. It is associated with the poor prognosis of severe patients such as multiple organ failure and even death. The main difference of cytokine storm is that in COVID-19 pneumonia is mainly the specific damage of the lung, while in MAS is easy to develop into a systemic. The attractive therapeutic approach to prevent MAS in COVID-19 mainly includes antiviral, antibiotics, convalescent plasma (CP) therapy and hemadsorption, extensive immunosuppressive agents, and cytokine-targeted therapies. Here, we discuss the role of the therapeutic approaches mentioned above in the two diseases. And we found that the treatment effect of the same therapeutic approach is different. [ABSTRACT FROM AUTHOR]

Published

2023

38. CD38 marks the exhausted CD8+ tissue-resident memory T cells in hepatocellular carcinoma.

Author

Reolo, Marie J. Y., Masayuki Otsuka, Seow, Justine Jia Wen, Joycelyn Lee, Yun Hua Lee, Nguyen, Phuong H. D., Chun Jye Lim, Wasser, Martin, Chua, Camillus, Lim, Tony K. H., Wei Qiang Leow, Chung, Alexander, Goh, Brian K. P., Chow, Pierce K. H., DasGupta, Ramanuj, Joe Poh Sheng Yeong, and Chew, Valerie

Subjects

IMMUNOLOGIC memory, MONONUCLEAR leukocytes, CD38 antigen, T-cell exhaustion, CYTOTOXIC T cells

Abstract

Introduction: Despite recent advances in immunotherapy for hepatocellular carcinoma (HCC), the overall modest response rate underscores the need for a better understanding of the tumor microenvironment (TME) of HCC. We have previously shown that CD38 is widely expressed on tumor-infiltrating leukocytes (TILs), predominantly on CD3+ T cells and monocytes. However, its specific role in the HCC TME remains unclear. Methods: In this current study, we used cytometry time-of-flight (CyTOF), bulk RNA sequencing on sorted T cells, and single-cell RNA (scRNA) sequencing to interrogate expression of CD38 and its correlation with T cell exhaustion in HCC samples. We also employed multiplex immunohistochemistry (mIHC) for validating our findings. Results: From CyTOF analysis, we compared the immune composition of CD38- expressing leukocytes in TILs, non-tumor tissue-infiltrating leukocytes (NIL), and peripheral blood mononuclear cells (PBMC). We identified CD8+ T cells as the dominant CD38-expressing TILs and found that CD38 expression was significantly higher in CD8+ TRM in TILs than in NILs. Furthermore, through transcriptomic analysis on sorted CD8+ TRM from HCC tumors, we observed a higher expression of CD38 along with T cell exhaustion genes, including PDCD1 and CTLA4, compared to the circulating memory CD8 T cells from PBMC. This was validated by scRNA sequencing that revealed co-expression of CD38 with PDCD1, CTLA4, and ITGAE (CD103) in T cells from HCC tumors. The protein co-expression of CD38 and PD-1 on CD8+ T cells was further demonstrated by mIHC on HCC FFPE tissues, marking CD38 as a T cell co-exhaustion marker in HCC. Lastly, the higher proportions of CD38+PD-1+ CD8+ T cells and CD38+PD-1+ TRM were significantly associated with the higher histopathological grades of HCC, indicating its role in the aggressiveness of the disease. Conclusion: Taken together, the concurrent expression of CD38 with exhaustion markers on CD8+ TRM underpins its role as a key marker of T cell exhaustion and a potential therapeutic target for restoring cytotoxic T cell function in HCC. [ABSTRACT FROM AUTHOR]

Published

2023

39. Editorial: The Past and the Future of Human Immunity Under Viral Evolutionary Pressure.

Author

Hurst, Tara Patricia and Magiorkinis, Gkikas

Subjects

RETROVIRUSES, IMMUNITY, CYTOTOXIC T cells, SIMIAN immunodeficiency virus, HIV seroconversion

Abstract

They submitted articles discussing the ongoing dynamics of co-existing with ancient endogenous retroviruses, as well as the pressures exerted by extant exogenous viruses such as influenza and human immunodeficiency virus (HIV-1). This highlights the adaptability of the immune response to viral infection but also how infection could alter gene expression to shift T cell phenotypes. The effect of immunity-virus interface at the population level was examined by Williams et al. where they present the perplexing phenomenon of a "pocket" of uninfected individuals in a connected network of recently HIV-1-infected individuals. [Extracted from the article]

Published

2019

40. Immunosuppressive cells in oncolytic virotherapy for glioma: challenges and solutions.

Author

Junfeng Liu, Piranlioglu, Raziye, Fei Ye, Kai Shu, Ting Lei, and Hiroshi Nakashima

Subjects

CYTOTOXIC T cells, ONCOLYTIC virotherapy, MYELOID-derived suppressor cells, GLIOMAS, MYELOID cells, T cells

Abstract

Glioblastoma is a highly aggressive form of brain cancer characterized by the abundance of myeloid lineage cells in the tumor microenvironment. Tumorassociated macrophages and microglia (TAM) and myeloid-derived suppressor cells (MDSCs), play a pivotal role in promoting immune suppression and tumor progression. Oncolytic viruses (OVs) are self-amplifying cytotoxic agents that can stimulate local anti-tumor immune responses and have the potential to suppress immunosuppressive myeloid cells and recruit tumor-infiltrating T lymphocytes (TILs) to the tumor site, leading to an adaptive immune response against tumors. However, the impact of OV therapy on the tumor-residentmyeloid population and the subsequent immune responses are not yet fully understood. This review provides an overview of how TAM and MDSC respond to different types of OVs, and combination therapeutics that target themyeloid population to promote antitumor immune responses in the glioma microenvironment. [ABSTRACT FROM AUTHOR]

Published

2023

41. Differences in the phenotypes and transcriptomic signatures of chimeric antigen receptor T lymphocytes manufactured via electroporation or lentiviral transfection.

Author

Anna Niu, Jintao Zou, Xuan Hu, Zhang Zhang, Lingyu Su, Jing Wang, Xing Lu, Wei Zhang, Wei Chen, and Xiaopeng Zhang

Subjects

T cell receptors, CHIMERIC antigen receptors, CYTOTOXIC T cells, GENE transfection, ELECTROPORATION

Abstract

Chimeric antigen receptor (CAR)-T cell therapy is an innovative treatment for CD19-expressing lymphomas. CAR-T cells are primarily manufactured via lentivirus transfection or transposon electroporation. While anti-tumor efficacy comparisons between the two methods have been conducted, there is a current dearth of studies investigating the phenotypes and transcriptome alterations induced in T cells by the two distinct manufacturing methods. Here, we established CAR-T signatures using fluorescent imaging, flow cytometry, and RNA-sequencing. A small fraction of CAR-T cells that were produced using the PiggyBac transposon (PB CAR-T cells) exhibited much higher expression of CAR than those produced using a lentivirus (Lenti CAR-T cells). PB and Lenti CAR-T cells containedmore cytotoxic T cell subsets than control T cells, and Lenti CAR-T cells presented a more pronounced memory phenotype. RNA-sequencing further revealed vast disparities between the two CAR-T cell groups, with PB CAR-T cells exhibiting greater upregulation of cytokines, chemokines, and their receptors. Intriguingly, PB CAR-T cells singularly expressed IL-9 and fewer cytokine release syndrome-associated cytokines when activated by target cells. In addition, PB CAR-T cells exerted faster in vitro cytotoxicity against CD19-expressing K562 cells but similar in vivo anti-tumor efficacy with Lenti CAR-T. Taken together, these data provide insights into the phenotypic alterations induced by lentiviral transfection or transposon electroporation and will attract more attention to the clinical influence of different manufacturing procedures. [ABSTRACT FROM AUTHOR]

Published

2023

42. Mechanisms of action of monoclonal antibodies in oncology integrated in IMGT/mAb-DB.

Author

Manso, Taciana, Kushwaha, Anjana, Abdollahi, Nika, Duroux, Patrice, Giudicelli, Véronique, and Kossida, Sofia

Subjects

MONOCLONAL antibodies, IMMUNE checkpoint proteins, AMINO acid sequence, CYTOTOXIC T cells, REGULATORY T cells

Abstract

Background: Cancer cells activate different immune checkpoint (IC) pathways in order to evade immunosurveillance. Immunotherapies involving ICs either block or stimulate these pathways and enhance the efficiency of the immune system to recognize and attack cancer cells. In this way, the development of monoclonal antibodies (mAbs) targeting ICs has significant success in cancer treatment. Recently, a systematic description of the mechanisms of action (MOA) of the mAbs has been introduced in IMGT/mAb-DB, the IMGT® database dedicated to mAbs for therapeutic applications. The characterization of these antibodies provides a comprehensive understanding of how mAbs work in cancer. Methods: In depth biocuration taking advantage of the abundant literature data as well as amino acid sequence analyses from mAbs managed in IMGT/2Dstructure-DB, the IMGT® protein database, allowed to define a standardized and consistent description of the MOA of mAbs targeting immune checkpoints in cancer therapy. Results: A fine description and a standardized graphical representation of the MOA of selected mAbs are integrated within IMGT/mAb-DB highlighting two main mechanisms in cancer immunotherapy, either Blocking or Agonist. In both cases, the mAbs enhance cytotoxic T lymphocyte (CTL)-mediated anti-tumor immune response (Immunostimulant effect) against tumor cells. On the one hand, mAbs targeting co-inhibitory receptors may have a functional Fc region to increase anti-tumor activity by effector properties that deplete Treg cells (Fceffector function effect) or may have limited FcgR binding to prevent Teff cells depletion and reduce adverse events. On the other hand, agonist mAbs targeting co-stimulatory receptors may bind to FcgRs, resulting in antibody crosslinking (FcgR crosslinking effect) and substantial agonism. Conclusion: In IMGT/mAb-DB, mAbs for cancer therapy are characterized by their chains, domains and sequence and by several therapeutic metadata, including their MOA. MOAs were recently included as a search criterion to query the database. IMGT® is continuing standardized work to describe the MOA of mAbs targeting additional immune checkpoints and novel molecules in cancer therapy, as well as expanding this study to other clinical domains. [ABSTRACT FROM AUTHOR]

Published

2023

43. Landscapes and mechanisms of CD8+ T cell exhaustion in gastrointestinal cancer.

Author

Jia-Tong Ding, Kang-Ping Yang, Hao-Nan Zhou, Ying-Feng Huang, Hui Li, and Zhen Zong

Subjects

T-cell exhaustion, GASTROINTESTINAL cancer, CYTOTOXIC T cells, T cells, STOMACH cancer

Abstract

CD8+ T cells, a cytotoxic T lymphocyte, are a key component of the tumor immune system, but they enter a hyporeactive T cell state in long-term chronic inflammation, and how to rescue this depleted state is a key direction of research. Current studies on CD8+ T cell exhaustion have found that the mechanisms responsible for their heterogeneity and differential kinetics may be closely related to transcription factors and epigenetic regulation, which may serve as biomarkers and potential immunotherapeutic targets to guide treatment. Although the importance of T cell exhaustion in tumor immunotherapy cannot be overstated, studies have pointed out that gastric cancer tissues have a better anti-tumor T cell composition compared to other cancer tissues, which may indicate that gastrointestinal cancers have more promising prospects for the development of precision-targeted immunotherapy. Therefore, the present study will focus on the mechanisms involved in the development of CD8+ T cell exhaustion, and then review the landscapes and mechanisms of T cell exhaustion in gastrointestinal cancer as well as clinical applications, which will provide a clear vision for the development of future immunotherapies. [ABSTRACT FROM AUTHOR]

Published

2023

44. Immunization with a novel mRNA vaccine, TGGT1_216200 mRNA-LNP, prolongs survival time in BALB/c mice against acute toxoplasmosis.

Author

Yizhuo Zhang, Dan Li, Yu Shen, Shiyu Li, Shaohong Lu, and Bin Zheng

Subjects

NF-kappa B, CYTOTOXIC T cells, HUMORAL immunity, INTERFERON regulatory factors, TH2 cells

Abstract

Toxoplasma gondii, a specialized intracellular parasite, causes a widespread zoonotic disease and is a severe threat to social and economic development. There is a lack of effective drugs and vaccines against T. gondii infection. Recently, mRNA vaccines have been rapidly developed, and their packaging materials and technologies are well established. In this study, TGGT1_216200 (TG_200), a novel molecule from T. gondii, was identified using bioinformatic screening analysis. TG_200 was purified and encapsulated with a lipid nanoparticle (LNP) to produce the TG_200 mRNA-LNP vaccine. The immune protection provided by the new vaccine and its mechanisms after immunizing BABL/C mice via intramuscular injection were investigated. There was a strong immune response when mice were vaccinated with TG_200 mRNA-LNP. Elevated levels of anti-T. gondii-specific immunoglobulin G (IgG), and a higher IgG2a-to-IgG1 ratio was observed. The levels of interleukin-12 (IL-12), interferon-γ (IFN-γ), IL-4, and IL-10 were also elevated. The result showed that the vaccine induced a mixture of Th1 and Th2 cells, and Th1-dominated humoral immune response. Significantly increased antigen-specific splenocyte proliferation was induced by TG_200 mRNA-LNP immunization. The vaccine could also induce T. gondii-specific cytotoxic T lymphocytes (CTLs). The expression levels of interferon regulatory factor 8 (IRF8), T-Box 21 (T-bet), and nuclear factor kappa B (NF-kB) were significantly elevated after TG_200 mRNA-LNP immunization. The levels of CD83, CD86, MHC-I, MHC-II, CD8, and CD4 molecules were also higher. The results indicated that TG_200 mRNA-LNP produced specific cellular and humoral immune responses. Most importantly, TG_200 mRNA-LNP immunized mice survived significantly longer (19.27 ± 3.438 days) than the control mice, which died within eight days after T. gondii challenge (P< 0.001). The protective effect of adoptive transfer was also assessed, and mice receiving serum and splenocytes from mice immunized with TG_200 mRNA-LNP showed improved survival rates of 9.70 ± 1.64 days and, 13.40 ± 2.32 days, respectively (P< 0.001). The results suggested that TG_200 mRNA-LNP is a safe and promising vaccine against T. gondii infection. [ABSTRACT FROM AUTHOR]

Published

2023

45. Three distinct mechanisms underlying human γδ T cell-mediated cytotoxicity against malignant pleural mesothelioma.

Author

Yasuhiro Umeyama, Hirokazu Taniguchi, Hiroshi Gyotoku, Hiroaki Senju, Hiromi Tomono, Shinnosuke Takemoto, Hiroyuki Yamaguchi, Tagod, Mohammed S. O., Masashi Iwasaki, Yoshimasa Tanaka, and Hiroshi Mukae

Subjects

T cell receptors, PLEURA cancer, MONONUCLEAR leukocytes, CELL-mediated cytotoxicity, KILLER cells, CYTOTOXIC T cells, T cells

Abstract

Introduction: Malignant pleural mesothelioma (MPM) is a rare and highly aggressive thoracic tumor with poor prognosis and limited therapeutic options. Although immune checkpoint inhibitors exhibit a promising effect in some patients with unresectable MPM in clinical trials, the majority of MPM patients show only modest response rates to the currently available treatments. It is thus imperative to develop novel and innovative therapeutic modalities for MPM, including immune effector cell-based therapies. Methods: gd T cells were expanded using tetrakis-pivaloyloxymethyl 2-(thiazole-2-ylamino) ethylidene-1,1-bisphosphonate (PTA) and interleukin-2, and the therapeutic potential of gd T cells was examined through analyzing cell surface markers and cellular cytotoxicity against MPM in vitro using a europium chelatebased time-resolved fluorescence assay system and a luciferase-based luminescence assay system. Results and discussion: We successfully expanded gd T cells from peripheral blood mononuclear cells of healthy donors and MPM patients.γd T cells expressed natural killer receptors such as NKG2D and DNAM-1 and exhibited a moderate level of cytotoxicity to MPM cells in the absence of antigens. The inclusion of PTA, (E)-4-hydroxy-3-methylbut-2-enyl diphosphate (HMBPP) or zoledronic acid (ZOL) induced a TCR-dependent cytotoxicity in γd T cells and secreted interferon-γ (IFN-γ). In addition, γd T cells expressing CD16 exhibited a significant level of cytotoxicity against MPM cells in the presence of an antiepidermal growth factor receptor (EGFR) mAb, at lower concentrations than in clinical settings, whereas a detectable level of IFN-g was not produced. Taken together, γd T cells showed cytotoxic activity against MPM in three distinct mechanisms through NK receptors, TCRs and CD16. Since major histocompatibility complex (MHC) molecules are not involved in the recognition, both autologous and allogeneic γd T cells could be used for the development of γd T cell-based adoptive immunotherapy for MPM. [ABSTRACT FROM AUTHOR]

Published

2023

46. Editorial: Bringing function to the forefront of cell therapy: how do we demonstrate potency?

Author

Fraser, Alasdair R., Curbishley, Stuart M., Roemhild, Andy, and Tsang, Kwong

Subjects

REGULATORY T cells, CYTOTOXIC T cells, HEMATOPOIETIC stem cells, KILLER cells, TUMOR-infiltrating immune cells

Abstract

This article, titled "Editorial: Bringing function to the forefront of cell therapy: how do we demonstrate potency?" discusses the importance of demonstrating the potency of cell-based therapies. These therapies include a range of cells, such as T cells, natural killer cells, mesenchymal stem cells, and endothelial cells, which are used in clinical immune therapies. The article emphasizes the need for appropriate assays to determine the efficacy of these therapies and highlights new approaches for in vitro testing and the use of surrogate markers. It also includes reviews on the use of cell therapies for cancer treatment and COVID-19, as well as original research on assessing the function and potency of different cell types. Overall, the article highlights the ongoing challenge of demonstrating potency in cell therapy and the importance of developing effective assays for characterizing these therapies. [Extracted from the article]

Published

2024

47. Syrian hamster as an ideal animal model for evaluation of cancer immunotherapy.

Author

Yangyang Jia, Yanru Wang, Dunmall, Louisa S. Chard, Lemoine, Nicholas R., Pengju Wang, and Yaohe Wang

Subjects

GOLDEN hamster, IMMUNE checkpoint inhibitors, ANIMAL models in research, IMMUNOTHERAPY, TUMOR treatment, CYTOTOXIC T cells, PROGRAMMED cell death 1 receptors

Abstract

Cancer immunotherapy (CIT) has emerged as an exciting new pillar of cancer treatment. Although benefits have been achieved in individual patients, the overall response rate is still not satisfactory. To address this, an ideal preclinical animal model for evaluating CIT is urgently needed. Syrian hamsters present similar features to humans with regard to their anatomy, physiology, and pathology. Notably, the histological features and pathological progression of tumors and the complexity of the tumor microenvironment are equivalent to the human scenario. This article reviews the current tumor models in Syrian hamster and the latest progress in their application to development of tumor treatments including immune checkpoint inhibitors, cytokines, adoptive cell therapy, cancer vaccines, and oncolytic viruses. This progress strongly advocates Syrian hamster as an ideal animal model for development and assessment of CIT for human cancer treatments. Additionally, the challenges of the Syrian hamster as an animal model for CIT are also discussed. [ABSTRACT FROM AUTHOR]

Published

2023

48. Cyclooxygenase-2-Prostaglandin E2 pathway: A key player in tumor-associated immune cells.

Author

Kaipeng Jin, Chao Qian, Jinti Lin, and Bing Liu

Subjects

KILLER cells, MYELOID-derived suppressor cells, ANTIGEN presenting cells, CYTOTOXIC T cells, PROSTAGLANDIN receptors

Abstract

Cyclooxygenases-2 (COX-2) and Prostaglandin E2 (PGE2), which are important inchronic inflammatory diseases, can increase tumor incidence and promote tumorgrowth and metastasis. PGE2 binds to various prostaglandin E receptors to activatespecific downstream signaling pathways such as PKA pathway, b-catenin pathway, NF-kB pathway and PI3K/AKT pathway, all of which play important roles inbiological and pathological behavior. Nonsteroidal anti-inflammatory drugs(NSAIDs), which play as COX-2 inhibitors, and EP antagonists are important inanti-tumor immune evasion. The COX-2-PGE2 pathway promotes tumor immuneevasion by regulating myeloid-derived suppressor cells, lymphocytes (CD8+ Tcells, CD4+ T cells and natural killer cells), and antigen presenting cells(macrophages and dendritic cells). Based on conventional treatment, theaddition of COX-2 inhibitors or EP antagonists may enhance immunotherapyresponse in anti-tumor immune escape. However, there are still a lot of challengesin cancer immunotherapy. In this review, we focus on how the COX-2-PGE2pathway affects tumor-associated immune cells. [ABSTRACT FROM AUTHOR]

Published

2023

49. The frequency of differentiated CD3+CD27-CD28- T cells predicts response to CART cell therapy in diffuse large B-cell lymphoma.

Author

Worel, Nina, Grabmeier-Pfistershammer, Katharina, Kratzer, Bernhard, Schlager, Martina, Tanzmann, Andreas, Rottal, Arno, Körmöczi, Ulrike, Porpaczy, Edit, Staber, Philipp B., Skrabs, Cathrin, Herkner, Harald, Gudipati, Venugopal, Huppa, Johannes B., Salzer, Benjamin, Lehner, Manfred, Saxenhuber, Nora, Friedberg, Eleonora, Wohlfarth, Philipp, Hopfinger, Georg, and Rabitsch, Werner

Subjects

DIFFUSE large B-cell lymphomas, T cells, CELLULAR therapy, B cell lymphoma, CYTOTOXIC T cells

Abstract

Background: Chimeric antigen receptor T (CART) cell therapy targeting the B cell specific differentiation antigen CD19 has shown clinical efficacy in a subset of relapsed/refractory (r/r) diffuse large B cell lymphoma (DLBCL) patients. Despite this heterogeneous response, blood pre-infusion biomarkers predicting responsiveness to CART cell therapy are currently understudied. Methods: Blood cell and serum markers, along with clinical data of DLBCL patients who were scheduled for CART cell therapy were evaluated to search for biomarkers predicting CART cell responsiveness. Findings: Compared to healthy controls (n=24), DLBCL patients (n=33) showed significant lymphopenia, due to low CD3+CD4+ T helper and CD3-CD56+ NK cell counts, while cytotoxic CD3+CD8+ T cell counts were similar. Although lymphopenic, DLBCL patients had significantly more activated HLA-DR+ (P=0.005) blood T cells and a higher frequency of differentiated CD3+CD27-CD28-(28.7 ± 19.0% versus 6.6 ± 5.8%; P<0.001) T cells. Twenty-six patients were infusedwithCART cells (median 81 days after leukapheresis) andwere analyzed for the overall response (OR) 3 months later. Univariate and multivariate regression analyses showed that low levels of differentiated CD3+CD27-CD28-T cells (23.3 ± 19.3% versus 35.1 ± 18.0%) were independently associated with OR. This association was even more pronounced when patients were stratified for complete remission (CR versus non-CR: 13.7 ± 11.7% versus 37.7 ± 17.4%, P=0.001). A cut-off value of ≤ 18% of CD3+CD27-CD28-T cells predicted CR at 12 months with high accuracy (P<0.001). In vitro, CD3+CD8+CD27-CD28-compared to CD3+CD8+CD27+CD28+ CART cells displayed similar CD19+ target cell-specific cytotoxicity, but were hypoproliferative and produced less cytotoxic cytokines (IFN-g and TNF-a). CD3+CD8+ T cells outperformed CD3+CD4+ T cells 3-to 6-fold in terms of their ability to kill CD19+ target cells. Interpretation: Low frequency of differentiated CD3+CD27-CD28-T cells at leukapheresis represents a novel pre-infusion blood biomarker predicting a favorable response to CART cell treatment in r/r DLBCL patients. [ABSTRACT FROM AUTHOR]

Published

2023

50. The antigen processing-associated transporter gene polymorphism: Role on gene and protein expression in HPV-infected pre-cancerous cervical lesion.

Author

Silva Medeiros, Fernanda, da Silva, Mauro César, da Silva, Neila Caroline Henrique, Gomes, Thailany Thays, Garcia Gomes, Renan, Albuquerque Paiva, Larissa, Oliveira dos Santos Gomes, Fabiana, Alves Peixoto, Christina, Valença Rygaard, Maria Carolina, Welkovic, Stefan, Bezerra Menezes, Maria Luiza, Donadi, Eduardo Antônio, and Lucena-Silva, Norma

Subjects

PRECANCEROUS conditions, GENE expression, GENETIC polymorphisms, CYTOTOXIC T cells, PROTEIN expression, T cells

Abstract

Human papillomavirus (HPV) is the major pathogen for cervical lesions. The evasion mechanism of the immune response and persistence of HPV infection can be influenced by polymorphisms (SNPs) in genes associated with transporter associated with antigen processing (TAP), which may change the peptide binding affinity or the TAP expression impacting the efficiency of peptide transport in the secretory pathway, and the presentation of peptides to cytotoxic T lymphocytes. This study aimed to evaluate the role of the TAP1 and TAP2 polymorphisms, TAP1, and TAP2 genes expressions, and protein levels in cervical cells presenting different degrees of pre-cancerous lesions in 296 immunocompetent women infected or not by HPV. TAP SNPs were genotyped by Sanger sequencing, and gene expression by real-time PCR. Aneuploidy was determined by DNA index using flow cytometry. TAP-1 and TAP-2 tissue expressions were evaluated by immunohistochemistry. The Asp697Gly SNP of TAP1 presented a risk for cellular aneuploidy (P=0.0244). HPV+ women had higher TAP-2 mRNA (P=0.0212) and protein (P<0.0001) levels. The TAP2D and TAP2E haplotypes were associated with the risk for aneuploidy and pre-cancerous lesions. In conclusion, nucleotide variability at the peptide binding region of peptide transporter genes, particularly of the TAP2 gene, may influence the HPV-peptide transportation from the cytosol to the endoplasmic reticulum, increasing the susceptibility to the development of high-grade cervical lesions. [ABSTRACT FROM AUTHOR]

Published

2022