Your search keyword '"Lynn RC"' showing total 632 results

1. Oncolytic virus and CAR-T cell therapy in solid tumors.

Author

Ponterio, Eleonora, Haas, Tobias Longin, and De Maria, Ruggero

Subjects

ONCOLYTIC virotherapy, CHIMERIC antigen receptors, IMMUNE response, T cells, CANCER cells

Abstract

Adoptive immunotherapy with T cells, genetically modified to express a tumor-reactive chimeric antigen receptor (CAR), is an innovative and rapidly developing life-saving treatment for cancer patients without other therapeutic opportunities. CAR-T cell therapy has proven effective only in hematological malignancies. However, although by now only a few clinical trials had promising outcomes, we predict that CAR-T therapy will eventually become an established treatment for several solid tumors. Oncolytic viruses (OVs) can selectively replicate in and kill cancer cells without harming healthy cells. They can stimulate an immune response against the tumor, because OVs potentially stimulate adaptive immunity and innate components of the host immune system. Using CAR-T cells along with oncolytic viruses may enhance the efficacy of CAR-T cell therapy in destroying solid tumors by increasing the tumor penetrance of T cells and reducing the immune suppression by the tumor microenvironment. This review describes recent advances in the design of oncolytic viruses and CAR-T cells while providing an overview of the potential combination of oncolytic virotherapy with CAR-T cells for solid cancers. In this review, we will focus on the host-virus interaction in the tumor microenvironment to reverse local immunosuppression and to develop CAR-T cell effector function. [ABSTRACT FROM AUTHOR]

Published

2024

2. Evolving strategies to overcome barriers in CAR-T cell therapy for acute myeloid leukemia.

Author

Colonne, Chanukya K., Kimble, Erik L., and Turtle, Cameron J.

Published

2024

3. Emerging CART Therapies for Pediatric Acute Myeloid Leukemia.

Author

Ceolin, Valeria, Spadea, Manuela, Apolito, Vincenzo, Saglio, Francesco, and Fagioli, Franca

Published

2024

4. IL-10-expressing CAR T cells resist dysfunction and mediate durable clearance of solid tumors and metastases.

Author

Zhao, Yang, Chen, Jiangqing, Andreatta, Massimo, Feng, Bing, Xie, Yu-Qing, Wenes, Mathias, Wang, Yi, Gao, Min, Hu, Xiaomeng, Romero, Pedro, Carmona, Santiago, Sun, Jie, Guo, Yugang, and Tang, Li

Abstract

The success of chimeric antigen receptor (CAR) T cell therapy in treating several hematopoietic malignancies has been difficult to replicate in solid tumors, in part because of T cell exhaustion and eventually dysfunction. To counter T cell dysfunction in the tumor microenvironment, we metabolically armored CAR T cells by engineering them to secrete interleukin-10 (IL-10). We show that IL-10 CAR T cells preserve intact mitochondrial structure and function in the tumor microenvironment and increase oxidative phosphorylation in a mitochondrial pyruvate carrier-dependent manner. IL-10 secretion promoted proliferation and effector function of CAR T cells, leading to complete regression of established solid tumors and metastatic cancers across several cancer types in syngeneic and xenograft mouse models, including colon cancer, breast cancer, melanoma and pancreatic cancer. IL-10 CAR T cells also induced stem cell-like memory responses in lymphoid organs that imparted durable protection against tumor rechallenge. Our results establish a generalizable approach to counter CAR T cell dysfunction through metabolic armoring, leading to solid tumor eradication and long-lasting immune protection. CAR T cells engineered to express IL-10 eradicate solid tumors and metastases. [ABSTRACT FROM AUTHOR]

Published

2024

5. Advances in targeting tumor microenvironment for immunotherapy.

Author

Lugang Wang, Liubo Zhang, Zhen Zhang, Peng Wu, Yi Zhang, and Xinfeng Chen

Subjects

TREATMENT effectiveness, TUMOR microenvironment, METASTASIS, IMMUNE response, CANCER cells

Abstract

The tumor microenvironment (TME) provides essential conditions for the occurrence, invasion, and spread of cancer cells. Initial research has uncovered immunosuppressive properties of the TME, which include low oxygen levels (hypoxia), acidic conditions (low pH), increased interstitial pressure, heightened permeability of tumor vasculature, and an inflammatory microenvironment. The presence of various immunosuppressive components leads to immune evasion and affects immunotherapy efficacy. This indicates the potential value of targeting the TME in cancer immunotherapy. Therefore, TME remodeling has become an effective method for enhancing host immune responses against tumors. In this study, we elaborate on the characteristics and composition of the TME and how it weakens immune surveillance and summarize targeted therapeutic strategies for regulating the TME. [ABSTRACT FROM AUTHOR]

Published

2024

6. Transcriptional rewiring in CD8+ T cells: implications for CAR-T cell therapy against solid tumours.

Author

Srinivasan, Shamini, Armitage, Jesse, Nilsson, Jonas, and Waithman, Jason

Subjects

CHIMERIC antigen receptors, T-cell exhaustion, T cell differentiation, TRANSCRIPTION factors, T cells

Abstract

T cells engineered to express chimeric-antigen receptors (CAR-T cells) can effectively control relapsed and refractory haematological malignancies in the clinic. However, the successes of CAR-T cell therapy have not been recapitulated in solid tumours due to a range of barriers such as immunosuppression, poor infiltration, and tumour heterogeneity. Numerous strategies are being developed to overcome these barriers, which include improving culture conditions and manufacturing protocols, implementing novel CAR designs, and novel approaches to engineering the T cell phenotype. In this review, we describe the various emerging strategies to improve CAR T cell therapy for solid tumours. We specifically focus on new strategies to modulate cell function and fate that have precipitated from the growing knowledge of transcriptional circuits driving T cell differentiation, with the ultimate goal of driving more productive antitumour T cell immunity. Evidence shows that enrichment of particular phenotypic subsets of T cells in the initial cell product correlates to improved therapeutic responses and clinical outcomes. Furthermore, T cell exhaustion and poor persistence are major factors limiting therapeutic efficacy. The latest preclinical work shows that targeting specific master regulators and transcription factors can overcome these key barriers, resulting in superior T cell therapeutic products. This can be achieved by targeting key transcriptional circuits promoting memory-like phenotypes or sustaining key effector functions within the hostile tumour microenvironment. Additional discussion points include emerging considerations for the field such as (i) targeting permutations of transcription factors, (ii) transient expression systems, (iii) tissue specificity, and (iv) expanding this strategy beyond CAR-T cell therapy and cancer. [ABSTRACT FROM AUTHOR]

Published

2024

7. Trogocytosis in CAR immune cell therapy: a key mechanism of tumor immune escape.

Author

Chen, Yizhao, Xin, Qianling, Zhu, Mengjuan, Qiu, Jiaqi, Qiu, Ji, Li, Ruilin, and Tu, Jiajie

Subjects

KILLER cells, CHIMERIC antigen receptors, CELLULAR therapy, AUTOIMMUNE diseases, HEMATOLOGIC malignancies, T cells

Abstract

Immune cell therapy based on chimeric antigen receptor (CAR) technology platform has been greatly developed. The types of CAR immune cell therapy have expanded from T cells to innate immune cells such as NK cells and macrophages, and the diseases treated have expanded from hematological malignancies to non-tumor fields such as infectious diseases and autoimmune diseases. Among them, CAR-T and CAR-NK therapy have observed examples of rapid remission in approved clinical trials, but the efficacy is unstable and plagued by tumor resistance. Trogocytosis is a special phenomenon of intercellular molecular transfer that is common in the immune system and is achieved by recipient cells through acquisition and internalization of donor cell-derived molecules and mediates immune effects. Recently, a novel short-term drug resistance mechanism based on trogocytosis has been proposed, and the bidirectional molecular exchange between CAR immune cells and tumor cells triggered by trogocytosis partially explains the long-term relapse phenomenon after treatment with CAR immune cells. In this review, we summarize the research progress of trogocytosis in CAR immunotherapy, discuss the influencing factors of trogocytosis and its direct and indirect interference with CAR immune cells and emphasize that the interference of trogocytosis can further release the potential of CAR immune cell therapy. [ABSTRACT FROM AUTHOR]

Published

2024

8. Trogocytosis in CAR immune cell therapy: a key mechanism of tumor immune escape.

Author

Chen, Yizhao, Xin, Qianling, Zhu, Mengjuan, Qiu, Jiaqi, Qiu, Ji, Li, Ruilin, and Tu, Jiajie

Subjects

KILLER cells, CHIMERIC antigen receptors, CELLULAR therapy, AUTOIMMUNE diseases, HEMATOLOGIC malignancies, T cells

Abstract

Immune cell therapy based on chimeric antigen receptor (CAR) technology platform has been greatly developed. The types of CAR immune cell therapy have expanded from T cells to innate immune cells such as NK cells and macrophages, and the diseases treated have expanded from hematological malignancies to non-tumor fields such as infectious diseases and autoimmune diseases. Among them, CAR-T and CAR-NK therapy have observed examples of rapid remission in approved clinical trials, but the efficacy is unstable and plagued by tumor resistance. Trogocytosis is a special phenomenon of intercellular molecular transfer that is common in the immune system and is achieved by recipient cells through acquisition and internalization of donor cell-derived molecules and mediates immune effects. Recently, a novel short-term drug resistance mechanism based on trogocytosis has been proposed, and the bidirectional molecular exchange between CAR immune cells and tumor cells triggered by trogocytosis partially explains the long-term relapse phenomenon after treatment with CAR immune cells. In this review, we summarize the research progress of trogocytosis in CAR immunotherapy, discuss the influencing factors of trogocytosis and its direct and indirect interference with CAR immune cells and emphasize that the interference of trogocytosis can further release the potential of CAR immune cell therapy. [ABSTRACT FROM AUTHOR]

Published

2024

9. Revolutionizing the treatment for nasopharyngeal cancer: the impact, challenges and strategies of stem cell and genetically engineered cell therapies.

Author

Chin-King Looi, Ee-Mun Loo, Heng-Chee Lim, Yik-Ling Chew, Kok-Yong Chin, Shiau-Chuen Cheah, Bey Hing Goh, and Chun-Wai Mai

Subjects

CHIMERIC antigen receptors, CANCER relapse, TUMOR-infiltrating immune cells, STEM cells, T cells

Abstract

Nasopharyngeal carcinoma (NPC) is a distinct malignancy of the nasopharynx and is consistently associated with the Epstein-Barr virus (EBV) infection. Its unique anatomical location and complex aetiology often result in advancedstage disease at first diagnosis. While radiotherapy (RT) and chemotherapy have been the mainstays of treatment, they often fail to prevent tumour recurrence and metastasis, leading to high rates of treatment failure and mortality. Recent advancement in cell-based therapies, such as chimeric antigen receptor (CAR)-T cell therapy, have shown great promise in hematological malignancies and are now being investigated for NPC. However, challenges such as targeting specific tumour antigens, limited T cell persistence and proliferation, and managing treatment-related toxicities must be addressed. Extensive research is needed to enhance the effectiveness and safety of these therapies, paving the way for their integration into standard clinical practice for better management of NPC and a better quality of life for human health. [ABSTRACT FROM AUTHOR]

Published

2024

10. Application of novel CAR technologies to improve treatment of autoimmune disease.

Author

Cheever, Abigail, Kang, Chloe C., O'Neill, Kim L., and Weber, K. Scott

Subjects

REGULATORY T cells, CHIMERIC antigen receptors, SYSTEMIC lupus erythematosus, T cells, THERAPEUTICS, AUTOIMMUNE diseases

Abstract

Chimeric antigen receptor (CAR) T cell therapy has become an important treatment for hematological cancers, and its success has spurred research into CAR T cell therapies for other diseases, including solid tumor cancers and autoimmune diseases. Notably, the development of CAR-based treatments for autoimmune diseases has shown great progress recently. Clinical trials for anti-CD19 and anti-BCMA CAR T cells in treating severe B cell-mediated autoimmune diseases, like systemic lupus erythematosus (SLE), have shown lasting remission thus far. CAR T cells targeting autoreactive T cells are beginning clinical trials for treating T cell mediated autoimmune diseases. Chimeric autoantigen receptor (CAAR) T cells specifically target and eliminate only autoreactive B cells, and they have shown promise in treating mucosal pemphigus vulgaris and MuSK myasthenia gravis. Regulatory CAR T cells have also been developed, which show potential in altering autoimmune affected areas by creating a protective barrier as well as helping decrease inflammation. These new treatments are only the beginning of potential CAR T cell applications in treating autoimmune disease. Novel CAR technologies have been developed that increase the safety, potency, specificity, and efficacy of CAR T cell therapy. Applying these novel modifications to autoimmune CARs has the potential to enhance the efficacy and applicability of CAR therapies to autoimmune disease. This review will detail several recently developed CAR technologies and discuss how their application to autoimmune disease will improve this emerging field. These include logicgated CARs, soluble protein-secreting CARs, and modular CARs that enable CAR T cell therapies to be more specific, reach a wider span of target cells, be safer for patients, and give a more potent cytotoxic response. Applying these novel CAR technologies to the treatment of autoimmune diseases has the potential to revolutionize this growing application of CAR T cell therapies. [ABSTRACT FROM AUTHOR]

Published

2024

11. MEK inhibition prevents CAR-T cell exhaustion and differentiation via downregulation of c-Fos and JunB.

Author

Wang, Xiujian, Tao, Xiao, Chen, Pengjie, Jiang, Penglei, Li, Wenxiao, Chang, Hefeng, Wei, Cong, Lai, Xinyi, Zhang, Hao, Pan, Yihan, Ding, Lijuan, Liang, Zuyu, Cui, Jiazhen, Shao, Mi, Teng, Xinyi, Gu, Tianning, Wei, Jieping, Kong, Delin, Si, Xiaohui, and Han, Yingli

Published

2024

12. Advances in targeting tumor microenvironment for immunotherapy.

Author

Lugang Wang, Liubo Zhang, Zhen Zhang, Peng Wu, Yi Zhang, and Xinfeng Chen

Subjects

TREATMENT effectiveness, TUMOR microenvironment, METASTASIS, IMMUNE response, CANCER cells

Abstract

The tumor microenvironment (TME) provides essential conditions for the occurrence, invasion, and spread of cancer cells. Initial research has uncovered immunosuppressive properties of the TME, which include low oxygen levels (hypoxia), acidic conditions (low pH), increased interstitial pressure, heightened permeability of tumor vasculature, and an inflammatory microenvironment. The presence of various immunosuppressive components leads to immune evasion and affects immunotherapy efficacy. This indicates the potential value of targeting the TME in cancer immunotherapy. Therefore, TME remodeling has become an effective method for enhancing host immune responses against tumors. In this study, we elaborate on the characteristics and composition of the TME and how it weakens immune surveillance and summarize targeted therapeutic strategies for regulating the TME. [ABSTRACT FROM AUTHOR]

Published

2024

13. Transcriptional rewiring in CD8+ T cells: implications for CAR-T cell therapy against solid tumours.

Author

Srinivasan, Shamini, Armitage, Jesse, Nilsson, Jonas, and Waithman, Jason

Subjects

CHIMERIC antigen receptors, T-cell exhaustion, T cell differentiation, TRANSCRIPTION factors, T cells

Abstract

T cells engineered to express chimeric-antigen receptors (CAR-T cells) can effectively control relapsed and refractory haematological malignancies in the clinic. However, the successes of CAR-T cell therapy have not been recapitulated in solid tumours due to a range of barriers such as immunosuppression, poor infiltration, and tumour heterogeneity. Numerous strategies are being developed to overcome these barriers, which include improving culture conditions and manufacturing protocols, implementing novel CAR designs, and novel approaches to engineering the T cell phenotype. In this review, we describe the various emerging strategies to improve CAR T cell therapy for solid tumours. We specifically focus on new strategies to modulate cell function and fate that have precipitated from the growing knowledge of transcriptional circuits driving T cell differentiation, with the ultimate goal of driving more productive antitumour T cell immunity. Evidence shows that enrichment of particular phenotypic subsets of T cells in the initial cell product correlates to improved therapeutic responses and clinical outcomes. Furthermore, T cell exhaustion and poor persistence are major factors limiting therapeutic efficacy. The latest preclinical work shows that targeting specific master regulators and transcription factors can overcome these key barriers, resulting in superior T cell therapeutic products. This can be achieved by targeting key transcriptional circuits promoting memory-like phenotypes or sustaining key effector functions within the hostile tumour microenvironment. Additional discussion points include emerging considerations for the field such as (i) targeting permutations of transcription factors, (ii) transient expression systems, (iii) tissue specificity, and (iv) expanding this strategy beyond CAR-T cell therapy and cancer. [ABSTRACT FROM AUTHOR]

Published

2024

14. Transcriptional rewiring in CD8+ T cells: implications for CAR-T cell therapy against solid tumours.

Author

Srinivasan, Shamini, Armitage, Jesse, Nilsson, Jonas, and Waithman, Jason

Subjects

CHIMERIC antigen receptors, T-cell exhaustion, T cell differentiation, TRANSCRIPTION factors, T cells

Abstract

T cells engineered to express chimeric-antigen receptors (CAR-T cells) can effectively control relapsed and refractory haematological malignancies in the clinic. However, the successes of CAR-T cell therapy have not been recapitulated in solid tumours due to a range of barriers such as immunosuppression, poor infiltration, and tumour heterogeneity. Numerous strategies are being developed to overcome these barriers, which include improving culture conditions and manufacturing protocols, implementing novel CAR designs, and novel approaches to engineering the T cell phenotype. In this review, we describe the various emerging strategies to improve CAR T cell therapy for solid tumours. We specifically focus on new strategies to modulate cell function and fate that have precipitated from the growing knowledge of transcriptional circuits driving T cell differentiation, with the ultimate goal of driving more productive antitumour T cell immunity. Evidence shows that enrichment of particular phenotypic subsets of T cells in the initial cell product correlates to improved therapeutic responses and clinical outcomes. Furthermore, T cell exhaustion and poor persistence are major factors limiting therapeutic efficacy. The latest preclinical work shows that targeting specific master regulators and transcription factors can overcome these key barriers, resulting in superior T cell therapeutic products. This can be achieved by targeting key transcriptional circuits promoting memory-like phenotypes or sustaining key effector functions within the hostile tumour microenvironment. Additional discussion points include emerging considerations for the field such as (i) targeting permutations of transcription factors, (ii) transient expression systems, (iii) tissue specificity, and (iv) expanding this strategy beyond CAR-T cell therapy and cancer. [ABSTRACT FROM AUTHOR]

Published

2024

15. Microarray analysis points to LMNB1 and JUN as potential target genes for predicting metastasis promotion by etoposide in colorectal cancer.

Author

Liu, Jiafei, Yang, Hongjie, Li, Peng, Zhou, Yuanda, Zhang, Zhichun, Zeng, Qingsheng, Zhang, Xipeng, and Sun, Yi

Subjects

COLORECTAL cancer, GENE expression, GENE expression profiling, METASTASIS, CELL cycle

Abstract

Etoposide is a second-line chemotherapy agent widely used for metastatic colorectal cancer. However, we discovered that etoposide treatment induced greater motility potential in four colorectal cancer cell lines. Therefore, we used microarrays to test the mRNA of these cancer cell lines to investigate the mechanisms of etoposide promoting colorectal cancer metastasis. Differentially expressed genes (DEGs) were identified by comparing the gene expression profiles in samples from etoposide-treated cells and untreated cells in all four colorectal cancer cell lines. Next, these genes went through the Gene Set Enrichment Analysis (GSEA), Gene Ontology (GO) and the Kyoto Encyclopedia of Genes and Genomes (KEGG) Pathway analysis. Among the top 10 genes including the upregulated and downregulated, eight genes had close interaction according to the STRING database: FAS, HMMR, JUN, LMNB1, MLL3, PLK2, STAG1 and TBL1X. After etoposide treatment, the cell cycle, metabolism-related and senescence signaling pathways in the colorectal cancer cell lines were significantly downregulated, whereas necroptosis and oncogene pathways were significantly upregulated. We suggest that the differentially expressed genes LMNB1 and JUN are potential targets for predicting colorectal cancer metastasis. These results provide clinical guidance in chemotherapy, and offer direction for further research in the mechanism of colorectal cancer metastasis. [ABSTRACT FROM AUTHOR]

Published

2024

16. GLUT1 overexpression in CAR-T cells induces metabolic reprogramming and enhances potency.

Author

Guerrero, Justin A., Klysz, Dorota D., Chen, Yiyun, Malipatlolla, Meena, Lone, Jameel, Fowler, Carley, Stuani, Lucille, May, Audre, Bashti, Malek, Xu, Peng, Huang, Jing, Michael, Basil, Contrepois, Kévin, Dhingra, Shaurya, Fisher, Chris, Svensson, Katrin J., Davis, Kara L., Kasowski, Maya, Feldman, Steven A., and Sotillo, Elena

Subjects

T-cell exhaustion, METABOLIC reprogramming, GLUCOSE transporters, CELL physiology, REACTIVE oxygen species, T cells, GLYCOLYSIS

Abstract

The intensive nutrient requirements needed to sustain T cell activation and proliferation, combined with competition for nutrients within the tumor microenvironment, raise the prospect that glucose availability may limit CAR-T cell function. Here, we seek to test the hypothesis that stable overexpression (OE) of the glucose transporter GLUT1 in primary human CAR-T cells would improve their function and antitumor potency. We observe that GLUT1OE in CAR-T cells increases glucose consumption, glycolysis, glycolytic reserve, and oxidative phosphorylation, and these effects are associated with decreased T cell exhaustion and increased Th17 differentiation. GLUT1OE also induces broad metabolic reprogramming associated with increased glutathione-mediated resistance to reactive oxygen species, and increased inosine accumulation. When challenged with tumors, GLUT1OE CAR-T cells secrete more proinflammatory cytokines and show enhanced cytotoxicity in vitro, and demonstrate superior tumor control and persistence in mouse models. Our collective findings support a paradigm wherein glucose availability is rate limiting for effector CAR-T cell function and demonstrate that enhancing glucose availability via GLUT1OE could augment antitumor immune function. T cell activation is a process that requires extra nutrients, which could be difficult to source from the tumor microenvironment in competition with tumor cells. Here authors increase the metabolic fitness of CAR-T cells by stable overexpression of the glucose transporter GLUT1, which allows them to increase their glucose intake and enhances their antitumour function. [ABSTRACT FROM AUTHOR]

Published

2024

17. Sliding-attention transformer neural architecture for predicting T cell receptor–antigen–human leucocyte antigen binding.

Author

Feng, Ziyan, Chen, Jingyang, Hai, Youlong, Pang, Xuelian, Zheng, Kun, Xie, Chenglong, Zhang, Xiujuan, Li, Shengqing, Zhang, Chengjuan, Liu, Kangdong, Zhu, Lili, Hu, Xiaoyong, Li, Shiliang, Zhang, Jie, Zhang, Kai, and Li, Honglin

Published

2024

18. A Primer on Chimeric Antigen Receptor T-cell Therapy-related Toxicities for the Intensivist.

Author

Ong, Shin Yeu and Baird, John H.

Subjects

CYTOKINE release syndrome, INTENSIVE care patients, CHIMERIC antigen receptors, ADVERSE health care events, CRITICAL care medicine

Abstract

Chimeric antigen receptor (CAR) T-cell therapy is an innovative treatment approach that has shown remarkable efficacy against several hematologic malignancies. However, its use can be associated with unique and sometimes severe toxicities that require admission to intensive care unit in 30% of patients, and intensivists should be aware of immune-mediated toxicities of CAR T-cell therapy and management of adverse events. We will review available literature on current diagnostic criteria and therapeutic strategies for mitigating these most common toxicities associated with CAR T-cell therapy including cytokine release syndrome (CRS) and immune effector cell-associated neurotoxicity syndrome (ICANS) in the post-infusion period. The authors will also review other toxicities associated with CAR T-cell therapy including cytopenias, acquired immunocompromised states, and infections, and discuss the available literature on best supportive care and prophylaxis recommendations. Critical care medicine specialists play a crucial role in the management of patients undergoing CAR T-cell therapies. With the expanding use of these products in increasing numbers of treating centers, intensivists' roles as part of the multidisciplinary team caring for these patients will have an outsized impact on the continued success of these promising therapies. [ABSTRACT FROM AUTHOR]

Published

2024

19. ReCARving the future: bridging CAR T-cell therapy gaps with synthetic biology, engineering, and economic insights.

Author

Ali, Alaa and DiPersio, John F.

Subjects

CHIMERIC antigen receptors, SYNTHETIC biology, GENOME editing, T cells, CANCER treatment

Abstract

Chimeric antigen receptor (CAR) T-cell therapy has revolutionized the treatment of hematologic malignancies, offering remarkable remission rates in otherwise refractory conditions. However, its expansion into broader oncological applications faces significant hurdles, including limited efficacy in solid tumors, safety concerns related to toxicity, and logistical challenges in manufacturing and scalability. This review critically examines the latest advancements aimed at overcoming these obstacles, highlighting innovations in CAR T-cell engineering, novel antigen targeting strategies, and improvements in delivery and persistence within the tumor microenvironment. We also discuss the development of allogeneic CAR T cells as off-the-shelf therapies, strategies to mitigate adverse effects, and the integration of CAR T cells with other therapeutic modalities. This comprehensive analysis underscores the synergistic potential of these strategies to enhance the safety, efficacy, and accessibility of CAR T-cell therapies, providing a forward-looking perspective on their evolutionary trajectory in cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2024

20. Cross‐modal integration of bulk RNA‐seq and single‐cell RNA sequencing data to reveal T‐cell exhaustion in colorectal cancer.

Author

Xu, Mingcong, Zhang, Guorui, Cui, Ting, Liu, Jiaqi, Wang, Qiuyu, Shang, Desi, Yu, Tingting, Guo, Bingzhou, Huang, Jinjie, and Li, Chunquan

Subjects

FATIGUE (Physiology), DEEP learning, T cells, RNA sequencing, COLORECTAL cancer

Abstract

Colorectal cancer (CRC) is a relatively common malignancy clinically and the second leading cause of cancer‐related deaths. Recent studies have identified T‐cell exhaustion as playing a crucial role in the pathogenesis of CRC. A long‐standing challenge in the clinical management of CRC is to understand how T cells function during its progression and metastasis, and whether potential therapeutic targets for CRC treatment can be predicted through T cells. Here, we propose DeepTEX, a multi‐omics deep learning approach that integrates cross‐model data to investigate the heterogeneity of T‐cell exhaustion in CRC. DeepTEX uses a domain adaptation model to align the data distributions from two different modalities and applies a cross‐modal knowledge distillation model to predict the heterogeneity of T‐cell exhaustion across diverse patients, identifying key functional pathways and genes. DeepTEX offers valuable insights into the application of deep learning in multi‐omics, providing crucial data for exploring the stages of T‐cell exhaustion associated with CRC and relevant therapeutic targets. [ABSTRACT FROM AUTHOR]

Published

2024

21. Unlocking the potential of iPSC-derived immune cells: engineering iNK and iT cells for cutting-edge immunotherapy.

Author

Minggang Fang, Allen, Alexander, Chong Luo, and Finn, Jonathan D.

Subjects

DOUBLE-strand DNA breaks, INDUCED pluripotent stem cells, TECHNOLOGICAL innovations, GRAFT versus host disease, GENOME editing

Abstract

Induced pluripotent stem cells (iPSCs) have emerged as a revolutionary tool in cell therapies due to their ability to differentiate into various cell types, unlimited supply, and potential as off-the-shelf cell products. New advances in iPSCderived immune cells have generated potent iNK and iT cells which showed robust killing of cancer cells in animal models and clinical trials. With the advent of advanced genome editing technologies that enable the development of highly engineered cells, here we outline 12 strategies to engineer iPSCs to overcome limitations and challenges of current cell-based immunotherapies, including safety switches, stealth edits, avoiding graft-versus-host disease (GvHD), targeting, reduced lymphodepletion, efficient differentiation, increased in vivo persistence, stemness, metabolic fitness, homing/trafficking, and overcoming suppressive tumor microenvironment and stromal cell barrier. With the development of advanced genome editing techniques, it is now possible to insert large DNA sequences into precise genomic locations without the need for DNA double strand breaks, enabling the potential for multiplexed knock out and insertion. These technological breakthroughs have made it possible to engineer complex cell therapy products at unprecedented speed and efficiency. The combination of iPSC derived iNK, iT and advanced gene editing techniques provides new opportunities and could lead to a new era for next generation of cell immunotherapies. [ABSTRACT FROM AUTHOR]

Published

2024

22. IL-4 drives exhaustion of CD8+ CART cells.

Author

Stewart, Carli M., Siegler, Elizabeth L., Sakemura, R. Leo, Cox, Michelle J., Huynh, Truc, Kimball, Brooke, Mai, Long, Can, Ismail, Manriquez Roman, Claudia, Yun, Kun, Sirpilla, Olivia, Girsch, James H., Ogbodo, Ekene, Mohammed Ismail, Wazim, Gaspar-Maia, Alexandre, Budka, Justin, Kim, Jenny, Scholler, Nathalie, Mattie, Mike, and Filosto, Simone

Subjects

T-cell exhaustion, MANTLE cell lymphoma, CHIMERIC antigen receptors, FATIGUE (Physiology), CELLULAR therapy

Abstract

Durable response to chimeric antigen receptor T (CART) cell therapy remains limited in part due to CART cell exhaustion. Here, we investigate the regulation of CART cell exhaustion with three independent approaches including: a genome-wide CRISPR knockout screen using an in vitro model for exhaustion, RNA and ATAC sequencing on baseline and exhausted CART cells, and RNA and ATAC sequencing on pre-infusion CART cell products from responders and non-responders in the ZUMA-1 clinical trial. Each of these approaches identify interleukin (IL)-4 as a regulator of CART cell dysfunction. Further, IL-4-treated CD8+ CART cells develop signs of exhaustion independently of the presence of CD4+ CART cells. Conversely, IL-4 pathway editing or the combination of CART cells with an IL-4 monoclonal antibody improves antitumor efficacy and reduces signs of CART cell exhaustion in mantle cell lymphoma xenograft mouse models. Therefore, we identify both a role for IL-4 in inducing CART exhaustion and translatable approaches to improve CART cell therapy. The application and therapeutic success of CAR-T cell approaches are limited by the development of T cell exhaustion. Here, Stewart et al discover a role for IL-4 in driving CD8+ CAR-T cell exhaustion and demonstrate the improvement of CAR-T cell effectivity with interruption of IL-4 signalling. [ABSTRACT FROM AUTHOR]

Published

2024

23. Engineering potent chimeric antigen receptor T cells by programming signaling during T-cell activation.

Author

Li, Aileen W., Briones, Jessica D., Lu, Jia, Walker, Quinn, Martinez, Rowena, Hiraragi, Hajime, Boldajipour, Bijan A., Sundar, Purnima, Potluri, Shobha, Lee, Gary, Ali, Omar A., and Cheung, Alexander S.

Subjects

T cells, ANTIGEN receptors, CHIMERIC antigen receptors, CELL communication

Abstract

Programming cell signaling during T-cell activation represents a simple strategy for improving the potency of therapeutic T-cell products. Stim-R technology (Lyell Immunopharma) is a customizable, degradable synthetic cell biomimetic that emulates physiologic, cell-like presentation of signal molecules to control T-cell activation. A breadth of Stim-R formulations with different anti-CD3/anti-CD28 (αCD3/αCD28) antibody densities and stoichiometries were screened for their effects on multiple metrics of T-cell function. We identified an optimized formulation that produced receptor tyrosine kinase-like orphan receptor 1 (ROR1)-targeted chimeric antigen receptor (CAR) T cells with enhanced persistence and polyfunctionality in vitro, as assessed in repeat-stimulation assays, compared with a benchmark product generated using a conventional T-cell–activating reagent. In transcriptomic analyses, CAR T cells activated with Stim-R technology showed downregulation of exhaustion-associated gene sets and retained a unique subset of stem-like cells with effector-associated gene signatures following repeated exposure to tumor cells. Compared with the benchmark product, CAR T cells activated using the optimized Stim-R technology formulation exhibited higher peak expansion, prolonged persistence, and improved tumor control in a solid tumor xenograft model. Enhancing T-cell products with Stim-R technology during T-cell activation may help improve therapeutic efficacy against solid tumors. [ABSTRACT FROM AUTHOR]

Published

2024

24. Phenotypic and spatial heterogeneity of CD8+ tumour infiltrating lymphocytes.

Author

Sun, Yikan, Yinwang, Eloy, Wang, Shengdong, Wang, Zenan, Wang, Fangqian, Xue, Yucheng, Zhang, Wenkan, Zhao, Shenzhi, Mou, Haochen, Chen, Shixin, Jin, Lingxiao, Li, Binghao, and Ye, Zhaoming

Subjects

TUMOR-infiltrating immune cells, T cells, CANCER cells, CD8 antigen, IMMUNOTHERAPY

Abstract

CD8+ T cells are the workhorses executing adaptive anti-tumour response, and targets of various cancer immunotherapies. Latest advances have unearthed the sheer heterogeneity of CD8+ tumour infiltrating lymphocytes, and made it increasingly clear that the bulk of the endogenous and therapeutically induced tumour-suppressive momentum hinges on a particular selection of CD8+ T cells with advantageous attributes, namely the memory and stem-like exhausted subsets. A scrutiny of the contemporary perception of CD8+ T cells in cancer and the subgroups of interest along with the factors arbitrating their infiltration contextures, presented herein, may serve as the groundwork for future endeavours to probe further into the regulatory networks underlying their differentiation and migration, and optimise T cell-based immunotherapies accordingly. [ABSTRACT FROM AUTHOR]

Published

2024

25. Neoadjuvant immune checkpoint blockade in women with mismatch repair deficient endometrial cancer: a phase I study.

Author

Eerkens, Anneke L., Brummel, Koen, Vledder, Annegé, Paijens, Sterre T., Requesens, Marta, Loiero, Dominik, van Rooij, Nienke, Plat, Annechien, Haan, Floris-Jan, Klok, Patty, Yigit, Refika, Roelofsen, Thijs, de Lange, Natascha M., Klomp, Rie, Church, David, ter Elst, Arja, Wardenaar, René, Spierings, Diana, Foijer, Floris, and Koelzer, Viktor Hendrik

Subjects

PATHOLOGIC complete response, CANCER patients, MAGNETIC resonance imaging, IMMUNE checkpoint proteins, ENDOMETRIAL cancer

Abstract

Neoadjuvant immune checkpoint blockade (ICB) has shown unprecedented activity in mismatch repair deficient (MMRd) colorectal cancers, but its effectiveness in MMRd endometrial cancer (EC) remains unknown. In this investigator-driven, phase I, feasibility study (NCT04262089), 10 women with MMRd EC of any grade, planned for primary surgery, received two cycles of neoadjuvant pembrolizumab (200 mg IV) every three weeks. A pathologic response (primary objective) was observed in 5/10 patients, with 2 patients showing a major pathologic response. No patient achieved a complete pathologic response. A partial radiologic response (secondary objective) was observed in 3/10 patients, 5/10 patients had stable disease and 2/10 patients were non-evaluable on magnetic resonance imaging. All patients completed treatment without severe toxicity (exploratory objective). At median duration of follow-up of 22.5 months, two non-responders experienced disease recurrence. In-depth analysis of the loco-regional and systemic immune response (predefined exploratory objective) showed that monoclonal T cell expansion significantly correlated with treatment response. Tumour-draining lymph nodes displayed clonal overlap with intra-tumoural T cell expansion. All pre-specified endpoints, efficacy in terms of pathologic response as primary endpoint, radiologic response as secondary outcome and safety and tolerability as exploratory endpoint, were reached. Neoadjuvant ICB with pembrolizumab proved safe and induced pathologic, radiologic, and immunologic responses in MMRd EC, warranting further exploration of extended neoadjuvant treatment. Immune checkpoint blockade (ICB) has shown promising activity in patients with advanced endometrial cancer, however its potential in the context of loco-regional disease remains unclear. Here the authors report the results of a phase I trial of neoadjuvant pembrolizumab (anti-PD1) in patients with mismatch repair deficient resectable endometrial cancer. [ABSTRACT FROM AUTHOR]

Published

2024

26. Beckett Vintage Baseball Card: PRICE GUIDE.

Published

2024

27. Stem-like CD8+ T cells in cancer.

Author

Steiner, Chelsea, Denlinger, Nathan, Xiaopei Huang, and Yiping Yang

Subjects

T-cell exhaustion, T cells, IMMUNOLOGIC memory, CELL populations, IMMUNE checkpoint proteins

Abstract

Stem-like CD8+ T cells (TSL) are a subset of immune cells with superior persistence and antitumor immunity. They are TCF1+ PD-1+ and important for the expansion of tumor specific CD8+ T cells in response to checkpoint blockade immunotherapy. In acute infections, naïve CD8+ T cells differentiate into effector and memory CD8+ T cells; in cancer and chronic infections, persistent antigen stimulation can lead to T cell exhaustion. Recent studies have highlighted the dichotomy between late dysfunctional (or exhausted) T cells (TLD) that are TCF1-- PD-1+ and self-renewing TCF1+ PD-1+ TSL from which they derive. TCF1+ TSL cells are considered to have stem cell-like properties akin to memory T cell populations and can give rise to cytotoxic effector and transitory T cell phenotypes (TTE) which mediate tumor control. In this review, we will discuss recent advances made in research on the formation and expansion of TSL, as well as distinct niches required for their differentiation and maintenance in the setting of cancer. We will also discuss potential strategies to generate these cells, with clinical implications for stemness enhancement in vaccine design, immune checkpoint blockade (ICB), and adoptive T cell therapies. [ABSTRACT FROM AUTHOR]

Published

2024

28. Reshaping the tumor immune microenvironment to improve CAR-T cell-based cancer immunotherapy.

Author

Xia, Xueting, Yang, Zongxin, Lu, Qisi, Liu, Zhenyun, Wang, Lei, Du, Jinwen, Li, Yuhua, Yang, Dong-Hua, and Wu, Shaojie

Subjects

CHIMERIC antigen receptors, TUMOR microenvironment, TUMOR treatment, TREATMENT effectiveness, T cells

Abstract

In many hematologic malignancies, the adoptive transfer of chimeric antigen receptor (CAR) T cells has demonstrated notable success; nevertheless, further improvements are necessary to optimize treatment efficacy. Current CAR-T therapies are particularly discouraging for solid tumor treatment. The immunosuppressive microenvironment of tumors affects CAR-T cells, limiting the treatment's effectiveness and safety. Therefore, enhancing CAR-T cell infiltration capacity and resolving the immunosuppressive responses within the tumor microenvironment could boost the anti-tumor effect. Specific strategies include structurally altering CAR-T cells combined with targeted therapy, radiotherapy, or chemotherapy. Overall, monitoring the tumor microenvironment and the status of CAR-T cells is beneficial in further investigating the viability of such strategies and advancing CAR-T cell therapy. [ABSTRACT FROM AUTHOR]

Published

2024

29. ErbB- and MUC1-targeted CAR-T cell immunotherapy of oral squamous cell carcinoma.

Author

Summers, Saffron E., Salih, Vehid, and Foey, Andrew D.

Published

2024

30. Prdm1 positively regulates liver Group 1 ILCs cancer immune surveillance and preserves functional heterogeneity.

Author

Jitian He, Le Gao, Peiying Wang, Wing Keung Chan, Yiran Zheng, Yumo Zhang, Jiaman Sun, Xue Li, Jiming Wang, Xiao-Hong Li, Huaiyong Chen, Zhouxin Yang, and Youwei Wang

Published

2024

31. LIM-domain-only 4 (LMO4) enhances CD8+ T-cell stemness and tumor rejection by boosting IL-21-STAT3 signaling.

Author

Schelker, Roland C., Fioravanti, Jessica, Mastrogiovanni, Fabio, Baldwin, Jeremy G., Rana, Nisha, Li, Peng, Chen, Ping, Vadász, Timea, Spolski, Rosanne, Heuser-Loy, Christoph, Slavkovic-Lukic, Dragana, Noronha, Pedro, Damiano, Giuseppe, Raccosta, Laura, Maggioni, Daniela, Pullugula, Sree, Lin, Jian-Xin, Oh, Jangsuk, Grandinetti, Patrick, and Lecce, Mario

Published

2024

32. Multi-omics analysis reveals a feedback loop amplifying immune responses in acute graft-versus-host disease due to imbalanced gut microbiota and bile acid metabolism.

Author

Han, Lijie, Sun, Xianlei, Kong, Jingjing, Li, Jin, Feng, Kai, Bai, Yanliang, Wang, Xianjing, Zhu, Zhenhua, Yang, Fengyuan, Chen, Qingzhou, Zhang, Mengmeng, Yue, Baohong, Wang, Xiaoqian, Fu, Liyan, Chen, Yaoyao, Yang, Qiankun, Wang, Shuya, Xin, Qingxuan, Sun, Nannan, and Zhang, Danfeng

Subjects

HEMATOPOIETIC stem cell transplantation, GRAFT versus host disease, BILE acids, GUT microbiome, T cells

Abstract

Acute graft-versus-host disease (aGVHD) is primarily driven by allogeneic donor T cells associated with an altered composition of the host gut microbiome and its metabolites. The severity of aGVHD after allogeneic hematopoietic stem cell transplantation (allo-HSCT) is not solely determined by the host and donor characteristics; however, the underlying mechanisms remain unclear. Using single-cell RNA sequencing, we decoded the immune cell atlas of 12 patients who underwent allo-HSCT: six with aGVHD and six with non-aGVHD. We performed a fecal microbiota (16SrRNA sequencing) analysis to investigate the fecal bacterial composition of 82 patients: 30 with aGVHD and 52 with non-aGVHD. Fecal samples from these patients were analyzed for bile acid metabolism. Through multi-omic analysis, we identified a feedback loop involving "immune cell-gut microbes-bile acid metabolites" contributing to heightened immune responses in patients with aGVHD. The dysbiosis of the gut microbiota and disruption of bile acid metabolism contributed to an exaggerated interleukin-1 mediated immune response. Our findings suggest that resistin and defensins are crucial in mitigating against aGVHD. Therefore, a comprehensive multi-omic atlas incorporating immune cells, gut microbes, and bile acid metabolites was developed in this study and used to propose novel, non-immunosuppressive approaches to prevent aGVHD. [ABSTRACT FROM AUTHOR]

Published

2024

33. LILRB1-HLA-G axis defines a checkpoint driving natural killer cell exhaustion in tuberculosis.

Author

Wang, Jing, Chai, Qiyao, Lei, Zehui, Wang, Yiru, He, Jiehua, Ge, Pupu, Lu, Zhe, Qiang, Lihua, Zhao, Dongdong, Yu, Shanshan, Qiu, Changgen, Zhong, Yanzhao, Li, Bing-Xi, Zhang, Lingqiang, Pang, Yu, Gao, George Fu, and Liu, Cui Hua

Abstract

Chronic infections, including Mycobacterium tuberculosis (Mtb)-caused tuberculosis (TB), can induce host immune exhaustion. However, the key checkpoint molecules involved in this process and the underlying regulatory mechanisms remain largely undefined, which impede the application of checkpoint-based immunotherapy in infectious diseases. Here, through adopting time-of-flight mass cytometry and transcriptional profiling to systematically analyze natural killer (NK) cell surface receptors, we identify leukocyte immunoglobulin like receptor B1 (LILRB1) as a critical checkpoint receptor that defines a TB-associated cell subset (LILRB1+ NK cells) and drives NK cell exhaustion in TB. Mechanistically, Mtb-infected macrophages display high expression of human leukocyte antigen-G (HLA-G), which upregulates and activates LILRB1 on NK cells to impair their functions by inhibiting mitogen-activated protein kinase (MAPK) signaling via tyrosine phosphatases SHP1/2. Furthermore, LILRB1 blockade restores NK cell-dependent anti-Mtb immunity in immuno-humanized mice. Thus, LILRB1-HLA-G axis constitutes a NK cell immune checkpoint in TB and serves as a promising immunotherapy target. Synopsis: The immune inhibitory receptor leukocyte immunoglobulin like receptor B1 (LILRB1), which is upregulated and activated by human leukocyte antigen-G (HLA-G), drives natural killer (NK) cell exhaustion in tuberculosis (TB) patients, thus serving as a promising target for TB immunotherapy. The inhibitory receptor LILRB1 defines a TB-associated NK cell subset and drives NK cell exhaustion in TB patients. Mtb-infected macrophages display high expression of HLA-G, which upregulates and activates LILRB1 on NK cells in TB patients. LILRB1-HLA-G interaction drives NK cell exhaustion by inhibiting mitogen-activated protein kinase (MAPK) signaling via tyrosine phosphatases SHP1/2. LILRB1 checkpoint blockade unleashes host NK cell-dependent anti-TB immunity. The immune inhibitory receptor leukocyte immunoglobulin like receptor B1 (LILRB1), which is upregulated and activated by human leukocyte antigen-G (HLA-G), drives natural killer (NK) cell exhaustion in tuberculosis (TB) patients, thus serving as a promising target for TB immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2024

34. Advanced strategies in improving the immunotherapeutic effect of CAR‐T cell therapy.

Author

Wang, Minmin, Jia, Linzi, Dai, Xiangpeng, and Zhang, Xiaoling

Published

2024

35. 血液肿瘤微环境对 CAR-T 免疫疗法疗效及其不良反应的 影响的研究进展.

Author

廖彩凤, 赖胡榕, and 李剑

Published

2024

36. Tumor associated macrophages as key contributors and targets in current and future therapies for melanoma.

Author

Habib, Shabana, Osborn, Gabriel, Willsmore, Zena, Chew, Min Waye, Jakubow, Sophie, Fitzpatrick, Amanda, Wu, Yin, Sinha, Khushboo, Lloyd-Hughes, Hawys, Geh, Jenny L. C., MacKenzie-Ross, Alastair D, Whittaker, Sean, Sanz-Moreno, Victoria, Lacy, Katie E., Karagiannis, Sophia N, and Adams, Rebecca

Subjects

MACROPHAGES, CANCER cells, TUMOR microenvironment, IMMUNE response, IMMUNE system, MELANOMA

Abstract

Despite the success of immunotherapies for melanoma in recent years, there remains a significant proportion of patients who do not yet derive benefit from available treatments. Immunotherapies currently licensed for clinical use target the adaptive immune system, focussing on Tcell interactions and functions. However, the most prevalent immune cells within the tumor microenvironment (TME) of melanoma are macrophages, a diverse immune cell subset displaying high plasticity, to which no current therapies are yet directly targeted. Macrophages have been shown not only to activate the adaptive immune response, and enhance cancer cell killing, but, when influenced by factors within the TME of melanoma, these cells also promote melanoma tumorigenesis and metastasis. We present a review of the most up-to-date literatureavailable on PubMed, focussing on studies from within the last 10 years. We also include data from ongoing and recent clinical trials targeting macrophages in melanoma listed on clinicaltrials.gov. Understanding the multifaceted role of macrophages in melanoma, including their interactions with immune and cancer cells, the influence of current therapies on macrophage phenotype and functions and how macrophages could be targeted with novel treatment approaches, are all critical for improving outcomes for patients with melanoma. [ABSTRACT FROM AUTHOR]

Published

2024

37. Epigenome editing technologies for discovery and medicine.

Author

McCutcheon, Sean R., Rohm, Dahlia, Iglesias, Nahid, and Gersbach, Charles A.

Abstract

Epigenome editing has rapidly evolved in recent years, with diverse applications that include elucidating gene regulation mechanisms, annotating coding and noncoding genome functions and programming cell state and lineage specification. Importantly, given the ubiquitous role of epigenetics in complex phenotypes, epigenome editing has unique potential to impact a broad spectrum of diseases. By leveraging powerful DNA-targeting technologies, such as CRISPR, epigenome editing exploits the heritable and reversible mechanisms of epigenetics to alter gene expression without introducing DNA breaks, inducing DNA damage or relying on DNA repair pathways. Epigenome editing has versatile applications in biomedical research and disease treatment. [ABSTRACT FROM AUTHOR]

Published

2024

38. The investigation of oncolytic viruses in the field of cancer therapy.

Author

Zijun Yuan, Yinping Zhang, Xiang Wang, Xingyue Wang, Siqi Ren, Xinyu He, Jiahong Su, Anfu Zheng, Sipeng Guo, Yu Chen, Shuai Deng, Xu Wu, Mingxing Li, Fukuan Du, Yueshui Zhao, Jing Shen, Zechen Wang, and Zhangang Xiao

Subjects

CANCER treatment, ONCOGENIC viruses, IMMUNE checkpoint inhibitors, TUMOR treatment, COMBINED modality therapy

Abstract

Oncolytic viruses (OVs) have emerged as a potential strategy for tumor treatment due to their ability to selectively replicate in tumor cells, induce apoptosis, and stimulate immune responses. However, the therapeutic efficacy of single OVs is limited by the complexity and immunosuppressive nature of the tumor microenvironment (TME). To overcome these challenges, engineering OVs has become an important research direction. This review focuses on engineering methods and multi-modal combination therapies for OVs aimed at addressing delivery barriers, viral phagocytosis, and antiviral immunity in tumor therapy. The engineering approaches discussed include enhancing in vivo immune response, improving replication efficiency within the tumor cells, enhancing safety profiles, and improving targeting capabilities. In addition, this review describes the potential mechanisms of OVs combined with radiotherapy, chemotherapy, cell therapy and immune checkpoint inhibitors (ICIs), and summarizes the data of ongoing clinical trials. By continuously optimizing engineering strategies and combination therapy programs, we can achieve improved treatment outcomes and quality of life for cancer patients. [ABSTRACT FROM AUTHOR]

Published

2024

39. Interferon subverts an AHR–JUN axis to promote CXCL13+ T cells in lupus.

Author

Law, Calvin, Wacleche, Vanessa Sue, Cao, Ye, Pillai, Arundhati, Sowerby, John, Hancock, Brandon, Horisberger, Alice, Bracero, Sabrina, Skidanova, Viktoriya, Li, Zhihan, Adejoorin, Ifeoluwakiisi, Dillon, Eilish, Benque, Isaac J., Nunez, Diana Pena, Simmons, Daimon P., Keegan, Joshua, Chen, Lin, Baker, Tina, Brohawn, Phillip Z., and Al-Mossawi, Hussein

Abstract

Systemic lupus erythematosus (SLE) is prototypical autoimmune disease driven by pathological T cell–B cell interactions1,2. Expansion of T follicular helper (TFH) and T peripheral helper (TPH) cells, two T cell populations that provide help to B cells, is a prominent feature of SLE3,4. Human TFH and TPH cells characteristically produce high levels of the B cell chemoattractant CXCL13 (refs. 5,6), yet regulation of T cell CXCL13 production and the relationship between CXCL13+ T cells and other T cell states remains unclear. Here, we identify an imbalance in CD4+ T cell phenotypes in patients with SLE, with expansion of PD-1+/ICOS+ CXCL13+ T cells and reduction of CD96hi IL-22+ T cells. Using CRISPR screens, we identify the aryl hydrocarbon receptor (AHR) as a potent negative regulator of CXCL13 production by human CD4+ T cells. Transcriptomic, epigenetic and functional studies demonstrate that AHR coordinates with AP-1 family member JUN to prevent CXCL13+ TPH/TFH cell differentiation and promote an IL-22+ phenotype. Type I interferon, a pathogenic driver of SLE7, opposes AHR and JUN to promote T cell production of CXCL13. These results place CXCL13+ TPH/TFH cells on a polarization axis opposite from T helper 22 (TH22) cells and reveal AHR, JUN and interferon as key regulators of these divergent T cell states.Insufficient AHR activation has been suggested in SLE, and augmenting AHR activation therapeutically may prevent CXCL13+ TPH/TFH differentiation and the subsequent recruitment of B cells and formation of lymphoid aggregates in inflamed tissues. [ABSTRACT FROM AUTHOR]

Published

2024

40. The impact of tertiary lymphoid structures on tumor prognosis and the immune microenvironment in non-small cell lung cancer.

Author

Weng, Yiming, Yuan, Jingping, Cui, Xue, Wang, Jinsong, Chen, Honglei, Xu, Li, Chen, Xinyi, Peng, Min, and Song, Qibin

Abstract

Non-small cell lung cancer (NSCLC) is a common malignancy whose prognosis and treatment outcome are influenced by many factors. Some studies have found that tertiary lymphoid structures (TLSs) in cancer may contribute to prognosis and the prediction of immunotherapy efficacy However, the combined role of TLSs in NSCLC remains unclear. We accessed The Cancer Genome Atlas (TCGA) and Gene Expression Omnibus (GEO) databases to obtain mRNA sequencing data and clinical information as the TCGA cohort, and used our own sample of 53 advanced NSCLC as a study cohort. The samples were divided into TLS+ and TLS- groups by pathological tissue sections. Patients of the TLS+ group had a better OS (p = 0.022), PFS (p = 0.042), and DSS (p = 0.004) in the TCGA cohort, and the results were confirmed by the study cohort (PFS, p = 0.012). Furthermore, our result showed that the count and size of TLSs are closely associated with the efficacy of immunotherapy. In addition, the TLS+ group was associated with better immune status and lower tumor mutation load. In the tumor microenvironment (TME), the expression levels of CD4+ T cells and CD8+ T cells of different phenotypes were associated with TLSs. Overall, TLSs are a strong predictor of survival and immunotherapeutic efficacy in advanced NSCLC, and T cell-rich TLSs suggest a more ordered and active immune response site, which aids in the decision-making and application of immunotherapy in the clinic. [ABSTRACT FROM AUTHOR]

Published

2024

41. Universal CAR 2.0 to overcome current limitations in CAR therapy.

Author

Schlegel, Lara Sophie, Werbrouck, Coralie, Boettcher, Michael, and Schlegel, Patrick

Subjects

CHIMERIC antigen receptors, EXPERIMENTAL automobiles, HEMATOLOGIC malignancies

Abstract

Chimeric antigen receptor (CAR) T cell therapy has effectively complemented the treatment of advanced relapsed and refractory hematological cancers. The remarkable achievements of CD19- and BCMA-CAR T therapies have raised high expectations within the fields of hematology and oncology. These groundbreaking successes are propelling a collective aspiration to extend the reach of CAR therapies beyond B-lineage malignancies. Advanced CAR technologies have created a momentum to surmount the limitations of conventional CAR concepts. Most importantly, innovations that enable combinatorial targeting to address target antigen heterogeneity, using versatile adapter CAR concepts in conjunction with recent transformative nextgeneration CAR design, offer the promise to overcome both the bottleneck associated with CAR manufacturing and patient-individualized treatment regimens. In this comprehensive review, we delineate the fundamental prerequisites, navigate through pivotal challenges, and elucidate strategic approaches, all aimed at paving the way for the future establishment of multitargeted immunotherapies using universal CAR technologies. [ABSTRACT FROM AUTHOR]

Published

2024

42. Synthetic Cells and Molecules in Cellular Immunotherapy.

Author

Haikun Lin, Chentao Li, Wanying Zhang, Boxiang Wu, Yanan Wang, Shimin Wang, Dongrui Wang, Xia Li, and He Huang

Published

2024

43. CAR-T Therapy Followed by Hematopoietic Stem Cell Transplantation Can Improve Survival in Children Relapsed/ Refractory Philadelphia Chromosome–positive B-cell Acute Lymphoblastic Leukemia.

Author

Yao Li, Guan-Hua Hu, Lan-Ping Xu, Xiao-Hui, Zhang Kai-Yan Liu, Pan Suo, Yu Wang, Yi-Fei Cheng, and Xiao-Jun Huang

Published

2024

44. T-cell exhaustion in multiple myeloma.

Author

Żyłka, Krzysztof, Kubicki, Tadeusz, Gil, Lidia, and Dytfeld, Dominik

Published

2024

45. Deciphering the tumor immune microenvironment from a multidimensional omics perspective: insight into next-generation CAR-T cell immunotherapy and beyond.

Author

Zhou, Zhaokai, Wang, Jiahui, Wang, Jiaojiao, Yang, Shuai, Wang, Ruizhi, Zhang, Ge, Li, Zhengrui, Shi, Run, Wang, Zhan, and Lu, Qiong

Subjects

TUMOR microenvironment, IMMUNOTHERAPY, CHIMERIC antigen receptors, TREATMENT effectiveness, TUMOR lysis syndrome

Abstract

Tumor immune microenvironment (TIME) consists of intra-tumor immunological components and plays a significant role in tumor initiation, progression, metastasis, and response to therapy. Chimeric antigen receptor (CAR)-T cell immunotherapy has revolutionized the cancer treatment paradigm. Although CAR-T cell immunotherapy has emerged as a successful treatment for hematologic malignancies, it remains a conundrum for solid tumors. The heterogeneity of TIME is responsible for poor outcomes in CAR-T cell immunotherapy against solid tumors. The advancement of highly sophisticated technology enhances our exploration in TIME from a multi-omics perspective. In the era of machine learning, multi-omics studies could reveal the characteristics of TIME and its immune resistance mechanism. Therefore, the clinical efficacy of CAR-T cell immunotherapy in solid tumors could be further improved with strategies that target unfavorable conditions in TIME. Herein, this review seeks to investigate the factors influencing TIME formation and propose strategies for improving the effectiveness of CAR-T cell immunotherapy through a multi-omics perspective, with the ultimate goal of developing personalized therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2024

46. CDK4/6 inhibition enhances T-cell immunotherapy on hepatocellular carcinoma cells by rejuvenating immunogenicity.

Author

Cai, Xiurong, Yin, Guo, Chen, Shuai, Tacke, Frank, Guillot, Adrien, and Liu, Hanyang

Abstract

Hepatocellular carcinoma (HCC) poses a significant clinical challenge, necessitating the integration of immunotherapeutic approaches. Palbociclib, a selective CDK4/6 inhibitor, has demonstrated promising efficacy in preclinical HCC models and is being evaluated as a novel therapeutic option in clinical trials. Additionally, CDK4/6 inhibition induces cellular senescence, potentially influencing the tumor microenvironment and immunogenicity of cancer cells. In this study, we conducted comprehensive bioinformatic analyses using diverse HCC transcriptome datasets, including bulk and single-cell RNA-sequencing data from public databases. We also utilized human and mouse HCC cells to investigate functional aspects. Primary T cells isolated from mouse blood were employed to assess T cell immunity against HCC cells. Results revealed that CD8+ T-cell infiltration correlates with improved outcomes in HCC patients with suppressed CDK4/6 expression. Moreover, CDK4/6 expression was associated with alterations in the immune landscape and immune checkpoint expression within the liver tumor microenvironment. Furthermore, we found that treatment with Palbociclib and Doxorubicin induces cellular senescence and a senescence-associated secretory phenotype in HCC cells. Notably, pretreatment with Palbociclib augmented T cell-mediated cytotoxicity against HCC cells, despite upregulation of PD-L1, surpassing the effects of Doxorubicin pretreatment. In conclusion, our study elucidates a novel mechanism by which CDK4/6 inhibition enhances T-cell-associated cancer elimination and proposes a potential therapeutic strategy to enhance T-cell immunotherapy on HCC. [ABSTRACT FROM AUTHOR]

Published

2024

47. Fully equipped CARs to address tumor heterogeneity, enhance safety, and improve the functionality of cellular immunotherapies.

Author

Alviano, Antonio Maria, Biondi, Marta, Grassenis, Erica, Biondi, Andrea, Serafini, Marta, and Tettamanti, Sarah

Subjects

CELL communication, CHIMERIC antigen receptors, T cells, IMMUNOTHERAPY, HEMATOLOGIC malignancies, AUTOMOBILES

Abstract

Although adoptive transfer of chimeric antigen receptor (CAR)-engineered T cells has achieved unprecedented response rates in patients with certain hematological malignancies, this therapeutic modality is still far from fulfilling its remarkable potential, especially in the context of solid cancers. Antigen escape variants, off-tumor destruction of healthy tissues expressing tumorassociated antigens (TAAs), poor CAR-T cell persistence, and the occurrence of functional exhaustion represent some of the most prominent hurdles that limit CAR-T cell ability to induce long-lasting remissions with a tolerable adverse effect profile. In this review, we summarize the main approaches that have been developed to face such bottlenecks, including the adapter CAR (AdCAR) system, Boolean-logic gating, epitope editing, the modulation of cell-intrinsic signaling pathways, and the incorporation of safety switches to precisely control CAR-T cell activation. We also discuss the most pressing issues pertaining to the selection of co-stimulatory domains, with a focus on strategies aimed at promoting CAR-T cell persistence and optimal antitumor functionality. [ABSTRACT FROM AUTHOR]

Published

2024

48. Engineered CD47 protects T cells for enhanced antitumour immunity.

Author

Yamada-Hunter, Sean A., Theruvath, Johanna, McIntosh, Brianna J., Freitas, Katherine A., Lin, Frank, Radosevich, Molly T., Leruste, Amaury, Dhingra, Shaurya, Martinez-Velez, Naiara, Xu, Peng, Huang, Jing, Delaidelli, Alberto, Desai, Moksha H., Good, Zinaida, Polak, Roel, May, Audre, Labanieh, Louai, Bjelajac, Jeremy, Murty, Tara, and Ehlinger, Zach

Abstract

Adoptively transferred T cells and agents designed to block the CD47–SIRPα axis are promising cancer therapeutics that activate distinct arms of the immune system1,2. Here we administered anti-CD47 antibodies in combination with adoptively transferred T cells with the goal of enhancing antitumour efficacy but observed abrogated therapeutic benefit due to rapid macrophage-mediated clearance of T cells expressing chimeric antigen receptors (CARs) or engineered T cell receptors. Anti-CD47-antibody-mediated CAR T cell clearance was potent and rapid enough to serve as an effective safety switch. To overcome this challenge, we engineered the CD47 variant CD47(Q31P) (47E), which engages SIRPα and provides a ‘don’t eat me’ signal that is not blocked by anti-CD47 antibodies. TCR or CAR T cells expressing 47E are resistant to clearance by macrophages after treatment with anti-CD47 antibodies, and mediate substantial, sustained macrophage recruitment to the tumour microenvironment. Although many of the recruited macrophages manifested an M2-like profile3, the combined therapy synergistically enhanced antitumour efficacy. Our study identifies macrophages as major regulators of T cell persistence and illustrates the fundamental challenge of combining T-cell-directed therapeutics with those designed to activate macrophages. It delivers a therapeutic approach that is capable of simultaneously harnessing the antitumour effects of T cells and macrophages, offering enhanced potency against solid tumours.Combination of TCR or CAR T cells expressing the engineered CD47 variant 47E with anti-CD47 antibody therapy results in synergistic antitumour efficacy due to T cell resistance to clearance by macrophages, while maintaining macrophage recruitment into the tumour microenvironment. [ABSTRACT FROM AUTHOR]

Published

2024

49. Mechanisms and management of CAR T toxicity.

Author

Ferreri, Christopher J. and Bhutani, Manisha

Subjects

CYTOKINE release syndrome, MANTLE cell lymphoma, CHIMERIC antigen receptors, MULTIPLE myeloma, FOLLICULAR lymphoma, IMMUNE reconstitution inflammatory syndrome, DIFFUSE large B-cell lymphomas

Abstract

Chimeric antigen receptor (CAR) T cell therapies have dramatically improved treatment outcomes for patients with relapsed or refractory B-cell acute lymphoblastic leukemia, large B-cell lymphoma, follicular lymphoma, mantle cell lymphoma, and multiple myeloma. Despite unprecedented efficacy, treatment with CAR T cell therapies can cause a multitude of adverse effects which require monitoring and management at specialized centers and contribute to morbidity and non-relapse mortality. Such toxicities include cytokine release syndrome, immune effector cell-associated neurotoxicity syndrome, neurotoxicity distinct from ICANS, immune effector cell-associated hemophagocytic lymphohistiocytosis-like syndrome, and immune effector cell-associated hematotoxicity that can lead to prolonged cytopenias and infectious complications. This review will discuss the current understanding of the underlying pathophysiologic mechanisms and provide guidelines for the grading and management of such toxicities. [ABSTRACT FROM AUTHOR]

Published

2024

50. Advances in research on factors affecting chimeric antigen receptor T‐cell efficacy.

Author

Zhou, Delian, Zhu, Xiaojian, and Xiao, Yi

Subjects

CHIMERIC antigen receptors, T cells, CANCER invasiveness, TUMOR microenvironment, CELL anatomy

Abstract

Chimeric antigen receptor T‐cell (CAR‐T) therapy is becoming an effective technique for the treatment of patients with relapsed/refractory hematologic malignancies. After analyzing patients with tumor progression and sustained remission after CAR‐T cell therapy, many factors were found to be associated with the efficacy of CAR‐T therapy. This paper reviews the factors affecting the effect of CAR‐T such as tumor characteristics, tumor microenvironment and immune function of patients, CAR‐T cell structure, construction method and in vivo expansion values, lymphodepletion chemotherapy, and previous treatment, and provides a preliminary outlook on the corresponding therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2024