Your search keyword '"Lynn RC"' showing total 1,084 results

151. Insights gained from single-cell analysis of chimeric antigen receptor T-cell immunotherapy in cancer.

Author

Tang, Lu, Huang, Zhong-Pei, Mei, Heng, and Hu, Yu

Subjects

CHIMERIC antigen receptors, ANTIGEN analysis, IMMUNOTHERAPY, T cells, TREATMENT effectiveness

Abstract

Advances in chimeric antigen receptor (CAR)-T cell therapy have significantly improved clinical outcomes of patients with relapsed or refractory hematologic malignancies. However, progress is still hindered as clinical benefit is only available for a fraction of patients. A lack of understanding of CAR-T cell behaviors in vivo at the single-cell level impedes their more extensive application in clinical practice. Mounting evidence suggests that single-cell sequencing techniques can help perfect the receptor design, guide gene-based T cell modification, and optimize the CAR-T manufacturing conditions, and all of them are essential for long-term immunosurveillance and more favorable clinical outcomes. The information generated by employing these methods also potentially informs our understanding of the numerous complex factors that dictate therapeutic efficacy and toxicities. In this review, we discuss the reasons why CAR-T immunotherapy fails in clinical practice and what this field has learned since the milestone of single-cell sequencing technologies. We further outline recent advances in the application of single-cell analyses in CAR-T immunotherapy. Specifically, we provide an overview of single-cell studies focusing on target antigens, CAR-transgene integration, and preclinical research and clinical applications, and then discuss how it will affect the future of CAR-T cell therapy. [ABSTRACT FROM AUTHOR]

Published

2023

152. A synthetic biology approach to engineering circuits in immune cells.

Author

Hoces, Daniel, Miguens Blanco, Jesús, and Hernández‐López, Rogelio A.

Subjects

BIOENGINEERING, SYNTHETIC biology, BIOLOGICAL systems, CYTOLOGY, SYNTHETIC receptors

Abstract

Summary: A synthetic circuit in a biological system involves the designed assembly of genetic elements, biomolecules, or cells to create a defined function. These circuits are central in synthetic biology, enabling the reprogramming of cellular behavior and the engineering of cells with customized responses. In cancer therapeutics, engineering T cells with circuits have the potential to overcome the challenges of current approaches, for example, by allowing specific recognition and killing of cancer cells. Recent advances also facilitate engineering integrated circuits for the controlled release of therapeutic molecules at specified locations, for example, in a solid tumor. In this review, we discuss recent strategies and applications of synthetic receptor circuits aimed at enhancing immune cell functions for cancer immunotherapy. We begin by introducing the concept of circuits in networks at the molecular and cellular scales and provide an analysis of the development and implementation of several synthetic circuits in T cells that have the goal to overcome current challenges in cancer immunotherapy. These include specific targeting of cancer cells, increased T‐cell proliferation, and persistence in the tumor microenvironment. By harnessing the power of synthetic biology, and the characteristics of certain circuit architectures, it is now possible to engineer a new generation of immune cells that recognize cancer cells, while minimizing off‐target toxicities. We specifically discuss T‐cell circuits for antigen density sensing. These circuits allow targeting of solid tumors that share antigens with normal tissues. Additionally, we explore designs for synthetic circuits that could control T‐cell differentiation or T‐cell fate as well as the concept of synthetic multicellular circuits that leverage cellular communication and division of labor to achieve improved therapeutic efficacy. As our understanding of cell biology expands and novel tools for genome, protein, and cell engineering are developed, we anticipate further innovative approaches to emerge in the design and engineering of circuits in immune cells. [ABSTRACT FROM AUTHOR]

Published

2023

153. Harnessing the power of artificial intelligence to advance cell therapy.

Author

Capponi, Sara and Daniels, Kyle G.

Subjects

CELLULAR therapy, ARTIFICIAL intelligence, MACHINE learning, PROTEIN structure prediction, DNA synthesis

Abstract

Summary: Cell therapies are powerful technologies in which human cells are reprogrammed for therapeutic applications such as killing cancer cells or replacing defective cells. The technologies underlying cell therapies are increasing in effectiveness and complexity, making rational engineering of cell therapies more difficult. Creating the next generation of cell therapies will require improved experimental approaches and predictive models. Artificial intelligence (AI) and machine learning (ML) methods have revolutionized several fields in biology including genome annotation, protein structure prediction, and enzyme design. In this review, we discuss the potential of combining experimental library screens and AI to build predictive models for the development of modular cell therapy technologies. Advances in DNA synthesis and high‐throughput screening techniques enable the construction and screening of libraries of modular cell therapy constructs. AI and ML models trained on this screening data can accelerate the development of cell therapies by generating predictive models, design rules, and improved designs. [ABSTRACT FROM AUTHOR]

Published

2023

154. Charging CAR by electrostatic power.

Author

Wang, Haopeng, Huang, Yuwei, and Xu, Chenqi

Subjects

T cell receptors, ANTIGEN receptors, SYNTHETIC receptors, CHIMERIC antigen receptors, TUMOR antigens

Abstract

Summary: Chimeric antigen receptor (CAR)‐T cell therapy has emerged as a promising approach for cancer treatment. CAR is a synthetic immune receptor that recognizes tumor antigen and activates T cells through multiple signaling pathways. However, the current CAR design is not as robust as T cell receptor (TCR), a natural antigen receptor with high sensitivity and efficiency. TCR signaling relies on specific molecular interactions, and thus electrostatic force, the major force of molecular interactions, play critical roles. Understanding how electrostatic charge regulates TCR/CAR signaling events will facilitate the development of next‐generation T cell therapies. This review summarizes recent findings on the roles of electrostatic interactions in both natural and synthetic immune receptor signaling, specifically that in CAR clustering and effector molecule recruitments, and highlights potential strategies for engineering CAR‐T cell therapy by leveraging charge‐based interactions. [ABSTRACT FROM AUTHOR]

Published

2023

155. Developing Strategies to Improve the Efficacy of CAR-T Therapy for Acute Myeloid Leukemia.

Author

Guo, Shujing, Gao, Xuejin, Sadhana, Mahara, Guo, Ruiting, Liu, Jile, Lu, Wenyi, and Zhao, Ming Feng

Abstract

Opinion statement: Acute myeloid leukemia (AML) is a fatal blood malignancy. With the development of immunotherapy, particularly chimeric antigen receptor T cells (CAR-T), the treatment of AML has undergone a significant change. Despite its advantages, CAR-T still faces a number of limitations and challenges while treating AML. Finding novel targets, altering the structure of CAR to increase efficacy while lowering side effects, and using double-target CAR and logic circuits are typical examples of key to answer these problems. With the advancement of gene editing technology, gene editing of tumor cells or normal cells to create therapeutic effects has grown in popularity. Additionally, the combination of multiple drugs is routinely used to address some of the obstacles and difficulties associated with CAR-T therapy. The review's primary goal was to summarize recent strategies and developments of CAR-T therapy for AML. [ABSTRACT FROM AUTHOR]

Published

2023

156. A case‐control survey study of environmental risk factors for primary hypoadrenocorticism in dogs.

Author

Treeful, Amy E., Searle, Kelly M., Carroll, Dana M., Yost, Kathleen J., Hedger, Anna L., and Friedenberg, Steven G.

Subjects

ENVIRONMENTAL risk, DOG breeds, DOGS, CONVENIENCE sampling (Statistics), CASE-control method, DOG bites

Abstract

Background: Primary hypoadrenocorticism in dogs is thought to be multifactorial with roles for both genetic and environmental factors. The contributions of environmental factors remain unexplored. Objective: Identify environmental and lifestyle exposures associated with primary hypoadrenocorticism in 2 dog breeds with high risk of developing the disease. Animals: Animals were not used in this study. Owners of Standard Poodles (STPDs) and Portuguese water dogs (POWDs) participated in a survey. Methods: Retrospective case‐control study. Dog owners were invited to participate in an online survey through convenience sampling. Questions regarded the demographics, health histories, and indoor/outdoor environments in which their dogs live and play. Responses for dogs with primary hypoadrenocorticism were compared to those without the disease using univariate and multivariate logistic regression models. Results: Five thousand forty‐seven responses (358 cases, 4689 controls) met initial inclusion criteria. Significant associations with modest effect size were found for community type, ingestion of canned food, and use of lawn fertilizer in some analysis models. Reproductive (spay/neuter) status exhibited the strongest association with high effect size across all models with adjusted odds ratio (OR) 2.5 (95% confidence interval [CI], 1.4‐4.5; P =.003) for spayed females and 6.0 (95% CI, 2.6‐13.9; P <.001) for neutered males. Conclusions and Clinical Importance: The large effect size for reproductive status reflects its high potential clinical relevance, whereas modest effect sizes for other environmental variables suggest lower potential clinical relevance. These findings are associations and do not necessarily imply causation. Before any actionable recommendations are warranted, additional evidence regarding biological mechanisms is needed. [ABSTRACT FROM AUTHOR]

Published

2023

157. Generation of functionally distinct T-cell populations by altering the viscoelasticity of their extracellular matrix.

Author

Adu-Berchie, Kwasi, Liu, Yutong, Zhang, David K. Y., Freedman, Benjamin R., Brockman, Joshua M., Vining, Kyle H., Nerger, Bryan A., Garmilla, Andrea, and Mooney, David J.

Published

2023

158. Tumor-derived autophagosome vaccines combined with immune adjuvants mediate antitumor immune responses via the neoantigen pathway.

Author

Jia YUAN, Yue CHANG, Yalan DAI, Yutong CHEN, Rongbin YUE, and Linjuan ZENG

Subjects

IMMUNOLOGICAL adjuvants, IMMUNE response, CANCER vaccines, TUMOR antigens, VACCINES, EXPERIMENTAL arthritis

Abstract

Vaccines composed of autophagosomes derived from tumor cells called DRibbles (DRiPs-containing blebs) are involved in the cross-presentation of tumor antigens, thus inducing cross-reactive T-cell responses against the tumor. Compared with traditional tumor lysate vaccines, autophagosome vaccines were found to be better sources of multiple tumor-associated antigens (TAAs) that activate antigen-specific T-cells. However, the involvement of tumor neoantigens in the immune responses of autophagosome vaccines remains unclear. The present study showed that exogenous autophagosome vaccines (DRibbles) combined with immune adjuvants (anti-OX40 antibody and ATP) can effectively activate functional T cells in vitro. Importantly, the combination of exogenous tumor-derived autophagosome vaccines and immune adjuvants was found to induce tumor regression in B16F10 and 4T1 tumor-bearing mice. The combination of autophagosome-enriched DRibbles with anti-OX40 antibody and ATP also exhibited optimal immune stimulation and antitumor efficiency in vivo. The effectiveness of exogenous DRibble vaccines was mainly due to their enhancement of tumor immunogenicity by increasing the presentation and release of tumor neoantigens. These findings suggest that this immunotherapeutic method may be effective in the treatment of cancer. [ABSTRACT FROM AUTHOR]

Published

2023

159. Secretion of 4-1BB Ligand Crosslinked to PD-1 Checkpoint Inhibitor Potentiates Chimeric Antigen Receptor T Cell Solid Tumor Efficacy.

Author

Dunn, Zachary S., Qu, Yun, MacMullan, Melanie, Chen, Xianhui, Cinay, Gunce, and Wang, Pin

Published

2023

160. Reprogramming T cell differentiation and exhaustion in CAR-T cell therapy.

Author

Bulliard, Yannick, Andersson, Borje S., Baysal, Mehmet A., Damiano, Jason, and Tsimberidou, Apostolia M.

Subjects

T cell differentiation, T-cell exhaustion, CELLULAR therapy, BIOENGINEERING, T cells

Abstract

T cell differentiation is a highly regulated, multi-step process necessary for the progressive establishment of effector functions, immunological memory, and long-term control of pathogens. In response to strong stimulation, as seen in severe or chronic infections or cancer, T cells acquire a state of hypo-responsiveness known as exhaustion, limiting their effector function. Recent advances in autologous chimeric antigen receptor (CAR)-T cell therapies have revolutionized the treatment of hematologic malignancies by taking advantage of the basic principles of T cell biology to engineer products that promote long-lasting T cell response. However, many patients' malignancies remain unresponsive to treatment or are prone to recur. Discoveries in T cell biology, including the identification of key regulators of differentiation and exhaustion, offer novel opportunities to have a durable impact on the fate of CAR-T cells after infusion. Such next-generation CAR-T cell therapies and their clinical implementation may result in the next leap forward in cancer treatment for selected patients. In this context, this review summarizes the foundational principles of T cell differentiation and exhaustion and describes how they can be utilized and targeted to further improve the design and efficacy of CAR-T cell therapies. [ABSTRACT FROM AUTHOR]

Published

2023

161. Phenotype and fate of liver-resident CD8 T cells during acute and chronic hepacivirus infection.

Author

Dravid, Piyush, Murthy, Satyapramod, Attia, Zayed, Cassady, Cole, Chandra, Rahul, Trivedi, Sheetal, Vyas, Ashish, Gridly, John, Holland, Brantley, Kumari, Anuradha, Grakoui, Arash, Cullen, John M., Walker, Christopher M., Sharma, Himanshu, and Kapoor, Amit

Subjects

T cells, HEPATITIS C, VIRAL nonstructural proteins, CYTOTOXIC T cells, CD8 antigen, T-cell exhaustion, T cell receptors

Abstract

Immune correlates of hepatitis C virus (HCV) clearance and control remain poorly defined due to the lack of an informative animal model. We recently described acute and chronic rodent HCV-like virus (RHV) infections in lab mice. Here, we developed MHC class I and class II tetramers to characterize the serial changes in RHV-specific CD8 and CD4 T cells during acute and chronic infection in C57BL/6J mice. RHV infection induced rapid expansion of T cells targeting viral structural and nonstructural proteins. After virus clearance, the virus-specific T cells transitioned from effectors to long-lived liver-resident memory T cells (TRM). The effector and memory CD8 and CD4 T cells primarily produced Th1 cytokines, IFN-γ, TNF-α, and IL2, upon ex vivo antigen stimulation, and their phenotype and transcriptome differed significantly between the liver and spleen. Rapid clearance of RHV reinfection coincided with the proliferation of virus-specific CD8 TRM cells in the liver. Chronic RHV infection was associated with the exhaustion of CD8 T cells (Tex) and the development of severe liver diseases. Interestingly, the virus-specific CD8 Tex cells continued proliferation in the liver despite the persistent high-titer viremia and retained partial antiviral functions, as evident from their ability to degranulate and produce IFN-γ upon ex vivo antigen stimulation. Thus, RHV infection in mice provides a unique model to study the function and fate of liver-resident T cells during acute and chronic hepatotropic infection. Author summary: Approximately 60–80% of humans fail to clear the hepatitis C virus infection, and the mechanism of HCV persistence and immune evasion remains elusive. T cells play an essential role in the control and clearance of HCV infection in humans and chimpanzees. Recently, we developed lab mouse and rat models for rodent HCV-like virus (RHV). Further development of these new rodent models is highly significant due to the lack of relevant animal models to study HCV immunity and pathogenesis. Here, we developed and used mouse MHC class I and class II tetramers to characterize the RHV-specific effector and memory T cells during acute and chronic RHV infection in immunocompetent lab mice. The control and clearance of primary and secondary RHV infection were associated with the expansion of liver-resident T cells expressing cytotoxic markers and antiviral cytokines. Chronic infection resulted in the exhaustion of T cells and the development of severe liver diseases. We defined the fundamental characteristics and unique transcriptome signature of liver-resident RHV-specific CD8 T cells during acute and chronic hepacivirus infection. Thus, our data and the newly developed mouse MHC class I and class II tetramers will allow the RHV mouse model to identify the liver-specific responses that shape the nature of liver-resident T cells and the divergent outcomes of hepacivirus infection and pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2023

162. Evolution by innovation as a driving force to improve TCR-T therapies.

Author

Schendel, Dolores J.

Subjects

T cell receptors, TECHNOLOGICAL innovations, CELLULAR therapy

Abstract

Adoptive cell therapies continually evolve through science-based innovation. Specialized innovations for TCR-T therapies are described here that are embedded in an End-to-End Platform for TCR-T Therapy Development which aims to provide solutions for key unmet patient needs by addressing challenges of TCR-T therapy, including selection of target antigens and suitable T cell receptors, generation of TCR-T therapies that provide long term, durable efficacy and safety and development of efficient and scalable production of patient-specific (personalized) TCR-T therapy for solid tumors. Multiple, combinable, innovative technologies are used in a systematic and sequential manner in the development of TCR-T therapies. One group of technologies encompasses product enhancements that enable TCR-T therapies to be safer, more specific and more effective. The second group of technologies addresses development optimization that supports discovery and development processes for TCR-T therapies to be performed more quickly, with higher quality and greater efficiency. Each module incorporates innovations layered onto basic technologies common to the field of immunology. An active approach of "evolution by innovation" supports the overall goal to develop best-in-class TCR-T therapies for treatment of patients with solid cancer. [ABSTRACT FROM AUTHOR]

Published

2023

163. Unusual herpetic reactivation in a young female following botox injection: a case report study.

Author

Amini-Salehi, Ehsan, Eslami, Narges, Tamimi, Amirhossein, Sedighi, Nasrin, Moghdam, Saman Soltani, Yaghubi-Kalurazi, Tofigh, Hassanipour, Soheil, Joukar, Farahnaz, Mansour-Ghanaei, Fariborz, and Eftekhari, Hojat

Subjects

BOTULINUM toxin, MEDICAL personnel, HERPES zoster, HERPES simplex, INJECTIONS, IMMUNOSUPPRESSIVE agents

Abstract

Background: Botox injections are commonly used for cosmetic and therapeutic purposes because they temporarily paralyze muscles, reduce wrinkles, and alleviate certain medical conditions. Although generally considered safe and effective, Botox injections may cause potential complications. While herpes reactivation is more commonly associated with immunosuppressive therapies, such as chemotherapy or corticosteroid use, its association with Botox injection is poorly documented. Case Presentation: A 33-year-old woman presented with progressive painful rashes and vesicles on her forehead, scalp, and right upper eyelid, accompanied by fever and malaise following a Botox injection to treat wrinkles. A positive Tzanck smear test result confirmed the diagnosis of herpes infection. The patient was treated with antiviral medication, and her symptoms gradually regressed over several days. Conclusions: Although herpes reactivation is more commonly associated with immunosuppressive therapies, few cases of herpes zoster and herpes simplex following Botox injection have been reported. The pathogenesis of herpes reactivation following Botox injection is unclear; however, it has been hypothesized that the Botox protein is a potent antigen that may activate the cellular immune system, making it easier for the virus to reactivate. Healthcare providers should be aware of this potential complication and consider it when evaluating patients who present with painful rashes following Botox injections. In addition, individuals who want to receive Botox injections should be informed of this complication. The diagnosis of herpetic infection should be made promptly, and antiviral therapy should be initiated to minimize the risk of complications. Further research is needed to better understand the pathogenesis and risk factors for herpes following Botox injection and to develop strategies for preventing and managing this complication. [ABSTRACT FROM AUTHOR]

Published

2023

164. Artificial Macrophage with Hierarchical Nanostructure for Biomimetic Reconstruction of Antitumor Immunity.

Author

Zhao, Henan, Liu, Renyu, Wang, Liqiang, Tang, Feiying, Chen, Wansong, and Liu, You-Nian

Subjects

MACROPHAGES, ARTIFICIAL cells, IMMUNITY, ANTIGEN presentation, TUMOR antigens, T cells, BIOMIMETIC materials

Abstract

Highlights: An artificial macrophage with hierarchical nanostructure (BaSO4@ZIF-8/TRF NMΦ) is constructed as an alternative to immunoactive macrophages. The Zn2+ chemical messenger as an "artificial cytokine" is released from the artificial macrophage to induce tumor anoikis and enhance immunogenicity. The artificial macrophage can efficiently capture tumor antigens for antigen presentation and T cell activation to fabricate long-term antitumor immunity, successfully mimicking the basic functions of natural immunoactive macrophage. Artificial cells are constructed from synthetic materials to imitate the biological functions of natural cells. By virtue of nanoengineering techniques, artificial cells with designed biomimetic functions provide alternatives to natural cells, showing vast potential for biomedical applications. Especially in cancer treatment, the deficiency of immunoactive macrophages results in tumor progression and immune resistance. To overcome the limitation, a BaSO4@ZIF-8/transferrin (TRF) nanomacrophage (NMΦ) is herein constructed as an alternative to immunoactive macrophages. Alike to natural immunoactive macrophages, NMΦ is stably retained in tumors through the specific affinity of TRF to tumor cells. Zn2+ as an "artificial cytokine" is then released from the ZIF-8 layer of NMΦ under tumor microenvironment. Similar as proinflammatory cytokines, Zn2+ can trigger cell anoikis to expose tumor antigens, which are selectively captured by the BaSO4 cavities. Therefore, the hierarchical nanostructure of NMΦs allows them to mediate immunogenic death of tumor cells and subsequent antigen capture for T cell activation to fabricate long-term antitumor immunity. As a proof-of-concept, the NMΦ mimics the biological functions of macrophage, including tumor residence, cytokine release, antigen capture and immune activation, which is hopeful to provide a paradigm for the design and biomedical applications of artificial cells. [ABSTRACT FROM AUTHOR]

Published

2023

165. Investigating potential immune mechanisms of trilaciclib administered prior to chemotherapy in patients with metastatic triple-negative breast cancer.

Author

Tan, Antoinette R., O'Shaughnessy, Joyce, Cao, Subing, Ahn, Sarah, and Yi, John S.

Abstract

Purpose: In a phase II trial in patients with metastatic triple-negative breast cancer (mTNBC; NCT02978716), administering trilaciclib prior to gemcitabine plus carboplatin (GCb) enhanced T-cell activation and improved overall survival versus GCb alone. The survival benefit was more pronounced in patients with higher immune-related gene expression. We assessed immune cell subsets and used molecular profiling to further elucidate effects on antitumor immunity. Methods: Patients with mTNBC and ≤ 2 prior chemotherapy regimens for locally recurrent TNBC or mTNBC were randomized 1:1:1 to GCb on days 1 and 8, trilaciclib prior to GCb on days 1 and 8, or trilaciclib alone on days 1 and 8, and prior to GCb on days 2 and 9. Gene expression, immune cell populations, and Tumor Inflammation Signature (TIS) scores were assessed in baseline tumor samples, with flow cytometric analysis and intracellular and surface cytokine staining used to assess immune cell populations and function. Results: After two cycles, the trilaciclib plus GCb group (n = 68) had fewer total T cells and significantly fewer CD8+ T cells and myeloid-derived suppressor cells compared with baseline, with enhanced T-cell effector function versus GCb alone. No significant differences were observed in patients who received GCb alone (n = 34). Of 58 patients in the trilaciclib plus GCb group with antitumor response data, 27 had an objective response. RNA sequencing revealed a trend toward higher baseline TIS scores among responders versus non‑responders. Conclusion: The results suggest that administering trilaciclib prior to GCb may modulate the composition and response of immune cell subsets to TNBC. [ABSTRACT FROM AUTHOR]

Published

2023

166. FLT3‐directed UniCAR T‐cell therapy of acute myeloid leukaemia.

Author

Peschke, J. C., Bergmann, R., Mehnert, M., Gonzalez Soto, K. E., Loureiro, L. R., Mitwasi, N., Kegler, A., Altmann, H., Wobus, M., Máthé, D., Szigeti, K., Feldmann, A., Bornhäuser, M., Bachmann, M., Fasslrinner, F., and Arndt, C.

Subjects

ACUTE myeloid leukemia, T cells, CHIMERIC antigen receptors, PROTEIN-tyrosine kinases

Abstract

Summary: Adaptor chimeric antigen receptor (CAR) T‐cell therapy offers solutions for improved safety and antigen escape, which represent main obstacles for the clinical translation of CAR T‐cell therapy in myeloid malignancies. The adaptor CAR T‐cell platform 'UniCAR' is currently under early clinical investigation. Recently, the first proof of concept of a well‐tolerated, rapidly switchable, CD123‐directed UniCAR T‐cell product treating patients with acute myeloid leukaemia (AML) was reported. Relapsed and refractory AML is prone to high plasticity under therapy pressure targeting one single tumour antigen. Thus, targeting of multiple tumour antigens seems to be required to achieve durable anti‐tumour responses, underlining the need to further design alternative AML‐specific target modules (TM) for the UniCAR platform. We here present the preclinical development of a novel FMS‐like tyrosine kinase 3 (FLT3)‐directed UniCAR T‐cell therapy, which is highly effective for in vitro killing of both AML cell lines and primary AML samples. Furthermore, we show in vivo functionality in a murine xenograft model. PET analyses further demonstrate a short serum half‐life of FLT3 TMs, which will enable a rapid on/off switch of UniCAR T cells. Overall, the presented preclinical data encourage the further development and clinical translation of FLT3‐specific UniCAR T cells for the therapy of AML. [ABSTRACT FROM AUTHOR]

Published

2023

167. Pre-clinical validation of a pan-cancer CAR-T cell immunotherapy targeting nfP2X7.

Author

Bandara, Veronika, Foeng, Jade, Gundsambuu, Batjargal, Norton, Todd S., Napoli, Silvana, McPeake, Dylan J., Tyllis, Timona S., Rohani-Rad, Elaheh, Abbott, Caitlin, Mills, Stuart J., Tan, Lih Y., Thompson, Emma J., Willet, Vasiliki M., Nikitaras, Victoria J., Zheng, Jieren, Comerford, Iain, Johnson, Adam, Coombs, Justin, Oehler, Martin K., and Ricciardelli, Carmela

Subjects

BREAST, CHIMERIC antigen receptors, IMMUNOTHERAPY, PURINERGIC receptors, CANCER cells, T cells

Abstract

Chimeric antigen receptor (CAR)-T cell immunotherapy is a novel treatment that genetically modifies the patients' own T cells to target and kill malignant cells. However, identification of tumour-specific antigens expressed on multiple solid cancer types, remains a major challenge. P2X purinoceptor 7 (P2X7) is a cell surface expressed ATP gated cation channel, and a dysfunctional version of P2X7, named nfP2X7, has been identified on cancer cells from multiple tissues, while being undetectable on healthy cells. We present a prototype -human CAR-T construct targeting nfP2X7 showing potential antigen-specific cytotoxicity against twelve solid cancer types (breast, prostate, lung, colorectal, brain and skin). In xenograft mouse models of breast and prostate cancer, CAR-T cells targeting nfP2X7 exhibit robust anti-tumour efficacy. These data indicate that nfP2X7 is a suitable immunotherapy target because of its broad expression on human tumours. CAR-T cells targeting nfP2X7 have potential as a wide-spectrum cancer immunotherapy for solid tumours in humans. The scarcity of targetable proteins broadly expressed on cancer cells, but not on healthy cells, is an obstacle for chimeric antigen receptor (CAR)-T cell therapy. Here the authors establish that a functionally impaired version of P2X purinoceptor 7, non-functional P2X7 (nfP2X7), fulfils these criteria, and demonstrate that CAR-T cells targeting nfP2X7 efficiently and selectively kill breast and prostate cancer cells in mouse models. [ABSTRACT FROM AUTHOR]

Published

2023

168. Cancer immunotherapies: advances and bottlenecks.

Author

Rui Rui, Liqun Zhou, and Shiming He

Subjects

IMMUNE checkpoint inhibitors, IMMUNOTHERAPY, CANCER vaccines, TUMOR microenvironment, IMMUNE system

Abstract

Immunotherapy has ushered in a new era in cancer treatment, and cancer immunotherapy continues to be rejuvenated. The clinical goal of cancer immunotherapy is to prime host immune system to provide passive or active immunity against malignant tumors. Tumor infiltrating leukocytes (TILs) play an immunomodulatory role in tumor microenvironment (TME) which is closely related to immune escape of tumor cells, thus influence tumor progress. Several cancer immunotherapies, include immune checkpoint inhibitors (ICIs), cancer vaccine, adoptive cell transfer (ACT), have shown great efficacy and promise. In this review, we will summarize the recent research advances in tumor immunotherapy, including the molecular mechanisms and clinical effects as well as limitations of immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2023

169. Preclinical and clinical trials of oncolytic vaccinia virus in cancer immunotherapy: a comprehensive review.

Author

Mengyuan Li, Minghuan Zhang, Qian Ye, Yunhua Liu, and Wenbin Qian

Subjects

VACCINIA, ONCOGENIC viruses, ONCOLYTIC virotherapy, CLINICAL trials, IMMUNOTHERAPY

Abstract

Oncolytic virotherapy has emerged as a promising treatment for human cancers owing to an ability to elicit curative effects via systemic administration. Tumor cells often create an unfavorable immunosuppressive microenvironment that degrade viral structures and impede viral replication; however, recent studies have established that viruses altered via genetic modifications can serve as effective oncolytic agents to combat hostile tumor environments. Specifically, oncolytic vaccinia virus (OVV) has gained popularity owing to its safety, potential for systemic delivery, and large gene insertion capacity. This review highlights current research on the use of engineered mutated viruses and gene-armed OVVs to reverse the tumor microenvironment and enhance antitumor activity in vitro and in vivo, and provides an overview of ongoing clinical trials and combination therapies. In addition, we discuss the potential benefits and drawbacks of OVV as a cancer therapy, and explore different perspectives in this field. [ABSTRACT FROM AUTHOR]

Published

2023

170. Multivalent adaptor proteins specifically target NK cells carrying a universal chimeric antigen receptor to ErbB2 (HER2)-expressing cancers.

Author

Pfeifer Serrahima, Jordi, Zhang, Congcong, Oberoi, Pranav, Bodden, Malena, Röder, Jasmin, Arndt, Claudia, Feldmann, Anja, Kiefer, Anne, Prüfer, Maren, Kühnel, Ines, Tonn, Torsten, Bachmann, Michael, and Wels, Winfried S.

Subjects

KILLER cells, CHIMERIC antigen receptors, ADAPTOR proteins, CELL surface antigens, CHIMERIC proteins, PROTEIN engineering, T cell receptors

Abstract

Chimeric antigen receptor (CAR)-engineered immune effector cells constitute a promising approach for adoptive cancer immunotherapy. Nevertheless, on-target/off-tumor toxicity and immune escape due to antigen loss represent considerable challenges. These may be overcome by adaptor CARs that are selectively triggered by bispecific molecules that crosslink the CAR with a tumor-associated surface antigen. Here, we generated NK cells carrying a first- or second-generation universal CAR (UniCAR) and redirected them to tumor cells with so-called target modules (TMs) which harbor an ErbB2 (HER2)-specific antibody domain for target cell binding and the E5B9 peptide recognized by the UniCAR. To investigate differential effects of the protein design on activity, we developed homodimeric TMs with one, two or three E5B9 peptides per monomer, and binding domains either directly linked or separated by an IgG4 Fc domain. The adaptor molecules were expressed as secreted proteins in Expi293F cells, purified from culture supernatants and their bispecific binding to UniCAR and ErbB2 was confirmed by flow cytometry. In cell killing experiments, all tested TMs redirected NK cell cytotoxicity selectively to ErbB2-positive tumor cells. Nevertheless, we found considerable differences in the extent of specific cell killing depending on TM design and CAR composition, with adaptor proteins carrying two or three E5B9 epitopes being more effective when combined with NK cells expressing the first-generation UniCAR, while the second-generation UniCAR was more active in the presence of TMs with one E5B9 sequence. These results may have important implications for the further development of optimized UniCAR and target module combinations for cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2023

171. Characterizing control of memory CD8 T cell differentiation by BTB-ZF transcription factor Zbtb20.

Author

Preiss, Nicholas K., Kamal, Yasmin, Wilkins, Owen M., Chenyang Li, Kolling IV, Fred W., Trask, Heidi W., Usherwood, Young-Kwang, Chao Cheng, Frost, Hildreth R., and Usherwood, Edward J.

Published

2023

172. Non‐coding RNAs in cancer immunotherapy: Predictive biomarkers and targets.

Author

Alahdal, Murad and Elkord, Eyad

Subjects

NON-coding RNA, T cell receptors, NON-small-cell lung carcinoma, BIOMARKERS, CHIMERIC antigen receptors

Abstract

Background: To date, standardising clinical predictive biomarkers for assessing the response to immunotherapy remains challenging due to variations in personal genetic signatures, tumour microenvironment complexities and epigenetic onco‐mechanisms. Main body: Early monitoring of key non‐coding RNA (ncRNA) biomarkers may help in predicting the clinical efficacy of cancer immunotherapy and come up with standard predictive ncRNA biomarkers. For instance, reduced miR‐125b‐5p level in the plasma of non‐small cell lung cancer patients treated with anti‐PD‐1 predicts a positive outcome. The level of miR‐153 in the plasma of colorectal cancer patients treated with chimeric antigen receptor T lymphocyte (CAR‐T) cell therapy may indicate the activation of T‐cell killing activity. miR‐148a‐3p and miR‐375 levels may forecast favourable responses to CAR‐T‐cell therapy in B‐cell acute lymphoblastic leukaemia. In cancer patients treated with the GPC3 peptide vaccine, serum levels of miR‐1228‐5p, miR‐193a‐5p and miR‐375‐3p were reported as predictive biomarkers of good response and improved overall survival. Therefore, there is a critical need for further studies to elaborate on the key ncRNA biomarkers that have the potential to predict early clinical responses to immunotherapy. Conclusion: This review summarises important predictive ncRNA biomarkers that were reported in cancer patients treated with different immunotherapeutic modalities, including monoclonal antibodies, small molecule inhibitors, cancer vaccines and CAR‐T cells. In addition, a concise discussion on forthcoming perspectives is provided, outlining technical approaches for the optimal utilisation of immunomodulatory ncRNA biomarkers as predictive tools and therapeutic targets. [ABSTRACT FROM AUTHOR]

Published

2023

173. Multiplexed transcriptomic profiling of the fate of human CAR T cells in vivo via genetic barcoding with shielded small nucleotides.

Author

Lu, Xiaoyin, Lofgren, Shane M., Zhao, Yuehui, and Mazur, Pawel K.

Published

2023

174. Advances in natural killer cell therapies for breast cancer.

Author

Kiaei, Seyedeh Zahra Fotook, Nouralishahi, Alireza, Ghasemirad, Mohammad, Barkhordar, Maryam, Ghaffari, Sasan, Kheradjoo, Hadis, Saleh, Mahshid, Mohammadzadehsaliani, Saman, and Molaeipour, Zahra

Subjects

BREAST, CELLULAR therapy, CANCER treatment, BREAST cancer, CANCER stem cells, KILLER cells, CHIMERIC antigen receptors, CETUXIMAB

Abstract

Breast cancer (BC) is the most common cause of cancer death in women. According to the American Cancer Society's yearly cancer statistics, BC constituted almost 15% of all the newly diagnosed cancer cases in 2022 for both sexes. Metastatic disease occurs in 30% of patients with BC. The currently available treatments fail to cure metastatic BC, and the average survival time for patients with metastatic BC is approximately 2 years. Developing a treatment method that terminates cancer stem cells without harming healthy cells is the primary objective of novel therapeutics. Adoptive cell therapy is a branch of cancer immunotherapy that utilizes the immune cells to attack cancer cells. Natural killer (NK) cells are an essential component of innate immunity and are critical in destroying tumor cells without prior stimulation with antigens. With the advent of chimeric antigen receptors (CARs), the autologous or allogeneic use of NK/CAR–NK cell therapy has raised new hopes for treating patients with cancer. Here, we describe recent developments in NK and CAR–NK cell immunotherapy, including the biology and function of NK cells, clinical trials, different sources of NK cells and their future perspectives on BC. [ABSTRACT FROM AUTHOR]

Published

2023

175. Supportive care for chimeric antigen receptor T-cell patients.

Author

Springell, Deborah, O'Reilly, Maeve, and Roddie, Claire

Published

2023

176. 4-1BB Targeting Immunotherapy: Mechanism, Antibodies, and Chimeric Antigen Receptor T.

Author

Shen, Xiaoling, Zhang, Rusong, Nie, Xiaojuan, Yang, Yanhua, Hua, Ye, and Lü, Peng

Published

2023

177. Genome Editing in Engineered T Cells for Cancer Immunotherapy.

Author

Bonini, Chiara, Chapuis, Aude G., Hudecek, Michael, Guedan, Sonia, Magnani, Chiara, and Qasim, Waseem

Published

2023

178. Massively parallel knock-in engineering of human T cells.

Author

Dai, Xiaoyun, Park, Jonathan J., Du, Yaying, Na, Zhenkun, Lam, Stanley Z., Chow, Ryan D., Renauer, Paul A., Gu, Jianlei, Xin, Shan, Chu, Zhiyuan, Liao, Cun, Clark, Paul, Zhao, Hongyu, Slavoff, Sarah, and Chen, Sidi

Abstract

The efficiency of targeted knock-in for cell therapeutic applications is generally low, and the scale is limited. In this study, we developed CLASH, a system that enables high-efficiency, high-throughput knock-in engineering. In CLASH, Cas12a/Cpf1 mRNA combined with pooled adeno-associated viruses mediate simultaneous gene editing and precise transgene knock-in using massively parallel homology-directed repair, thereby producing a pool of stably integrated mutant variants each with targeted gene editing. We applied this technology in primary human T cells and performed time-coursed CLASH experiments in blood cancer and solid tumor models using CD3, CD8 and CD4 T cells, enabling pooled generation and unbiased selection of favorable CAR-T variants. Emerging from CLASH experiments, a unique CRISPR RNA (crRNA) generates an exon3 skip mutant of PRDM1 in CAR-Ts, which leads to increased proliferation, stem-like properties, central memory and longevity in these cells, resulting in higher efficacy in vivo across multiple cancer models, including a solid tumor model. The versatility of CLASH makes it broadly applicable to diverse cellular and therapeutic engineering applications. Unbiased selection of CAR-T cells is achieved by massively parallel knock-in engineering. [ABSTRACT FROM AUTHOR]

Published

2023

179. Advances in manufacturing chimeric antigen receptor immune cell therapies.

Author

Ramamurthy A, Tommasi A, and Saha K

Subjects

Humans, Animals, Neoplasms therapy, Neoplasms immunology, Cell- and Tissue-Based Therapy methods, Gene Editing, T-Lymphocytes immunology, T-Lymphocytes metabolism, Receptors, Antigen, T-Cell genetics, Receptors, Antigen, T-Cell metabolism, Receptors, Chimeric Antigen genetics, Receptors, Chimeric Antigen metabolism, Receptors, Chimeric Antigen immunology, Immunotherapy, Adoptive methods, Immunotherapy, Adoptive adverse effects

Abstract

Biomedical research has witnessed significant strides in manufacturing chimeric antigen receptor T cell (CAR-T) therapies, marking a transformative era in cellular immunotherapy. Nevertheless, existing manufacturing methods for autologous cell therapies still pose several challenges related to cost, immune cell source, safety risks, and scalability. These challenges have motivated recent efforts to optimize process development and manufacturing for cell therapies using automated closed-system bioreactors and models created using artificial intelligence. Simultaneously, non-viral gene transfer methods like mRNA, CRISPR genome editing, and transposons are being applied to engineer T cells and other immune cells like macrophages and natural killer cells. Alternative sources of primary immune cells and stem cells are being developed to generate universal, allogeneic therapies, signaling a shift away from the current autologous paradigm. These multifaceted innovations in manufacturing underscore a collective effort to propel this therapeutic approach toward broader clinical adoption and improved patient outcomes in the evolving landscape of cancer treatment. Here, we review current CAR immune cell manufacturing strategies and highlight recent advancements in cell therapy scale-up, automation, process development, and engineering., (© 2024. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published

2024

180. Multiple small-dose infusions of G-CSF-mobilized haploidentical lymphocytes after autologous haematopoietic stem cell transplantation for acute myeloid leukaemia.

Author

Yang F, Ren Q, Zu Y, Gui R, Li Z, Wang J, Zhang Y, Yu F, Fang B, Fu Y, Wang Y, Liu Y, Zhang L, Zuo W, Li Y, Lin Q, Zhao H, Wang P, Zhang B, Huang Z, Song Y, and Zhou J

Subjects

Humans, Male, Female, Adult, Middle Aged, Retrospective Studies, Transplantation, Autologous, Adolescent, Hematopoietic Stem Cell Mobilization methods, Young Adult, Aged, Transplantation, Haploidentical methods, Leukemia, Myeloid, Acute therapy, Granulocyte Colony-Stimulating Factor administration & dosage, Hematopoietic Stem Cell Transplantation methods, Lymphocyte Transfusion

Abstract

This retrospective study analysed 106 acute myeloid leukaemia (AML) patients undergoing autologous haematopoietic stem cell transplantation (ASCT) to assess the impact of multiple small-dose infusions of granulocyte-colony-stimulating factor (G-CSF)-mobilized haploidentical lymphocytes as post-ASCT maintenance therapy. Among them, 50 patients received lymphocyte maintenance therapy, 21 received alternative maintenance therapy, and 35 received no maintenance therapy. Patients receiving lymphocyte maintenance therapy demonstrated significantly higher overall survival (OS) and disease-free survival (DFS) compared to those without maintenance therapy, with 4-year OS and DFS rates notably elevated. While there were no significant differences in recurrence rates among the three groups, lymphocyte maintenance therapy showcased particular benefits for intermediate-risk AML patients, yielding significantly higher OS and DFS rates and lower relapse rates compared to alternative maintenance therapy and no maintenance therapy. The study suggests that multiple small-dose infusions of G-CSF-mobilized haploidentical lymphocytes may offer promising outcomes for AML patients after ASCT, particularly for those classified as intermediate-risk. These findings underscore the potential efficacy of lymphocyte maintenance therapy in reducing disease relapse and improving long-term prognosis in this patient population., (© 2024 British Society for Haematology and John Wiley & Sons Ltd.)

Published

2024

181. Harnessing the tumor microenvironment to boost adoptive T cell therapy with engineered lymphocytes for solid tumors.

Author

Spiga M, Martini E, Maffia MC, Ciceri F, Ruggiero E, Potenza A, and Bonini C

Subjects

Humans, Animals, Receptors, Antigen, T-Cell metabolism, Receptors, Antigen, T-Cell genetics, Tumor Microenvironment immunology, Immunotherapy, Adoptive methods, Neoplasms therapy, Neoplasms immunology, T-Lymphocytes immunology, T-Lymphocytes metabolism, Receptors, Chimeric Antigen metabolism, Receptors, Chimeric Antigen genetics, Receptors, Chimeric Antigen immunology

Abstract

Adoptive cell therapy (ACT) using Chimeric Antigen Receptor (CAR) and T Cell Receptor (TCR) engineered T cells represents an innovative therapeutic approach for the treatment of hematological malignancies, yet its application for solid tumors is still suboptimal. The tumor microenvironment (TME) places several challenges to overcome for a satisfactory therapeutic effect, such as physical barriers (fibrotic capsule and stroma), and inhibitory signals impeding T cell function. Some of these obstacles can be faced by combining ACT with other anti-tumor approaches, such as chemo/radiotherapy and checkpoint inhibitors. On the other hand, cutting edge technological tools offer the opportunity to overcome and, in some cases, take advantage of TME intrinsic characteristics to boost ACT efficacy. These include: the exploitation of chemokine gradients and integrin expression for preferential T-cell homing and extravasation; metabolic changes that have direct or indirect effects on TCR-T and CAR-T cells by increasing antigen presentation and reshaping T cell phenotype; introduction of additional synthetic receptors on TCR-T and CAR-T cells with the aim of increasing T cells survival and fitness., (© 2024. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published

2024

182. Single-cell sequencing reveals the correlation of aggrephagy signaling and multiple myeloma immune microenvironment composition.

Author

Wang X, Feng Y, Wang F, Lin Z, Huang J, Li Q, Luo H, Liu X, Zhai X, Gao Q, Li L, Zhang Y, Wen J, Zhang L, Niu T, and Zheng Y

Subjects

Humans, Prognosis, Gene Expression Regulation, Neoplastic, Autophagy genetics, Autophagy immunology, Gene Expression Profiling methods, Biomarkers, Tumor genetics, Transcriptome, Multiple Myeloma genetics, Multiple Myeloma immunology, Tumor Microenvironment immunology, Tumor Microenvironment genetics, Single-Cell Analysis methods, Signal Transduction

Abstract

Aggrephagy, a type of autophagy, degrades the aggregation of misfolded protein in cells. However, the role of aggrephagy in multiple myeloma (MM) has not been fully demonstrated. In this study, we first investigated the correlation between aggrephagy signaling, MM immune microenvironment composition and disease prognosis. Single-cell RNA-seq data, including the expression profiles of 12,187 single cells from seven MM bone marrow (BM) and seven healthy BM samples, were analyzed by non-negative matrix factorization for 44 aggrephagy-related genes. Bulk RNA-seq cohorts from the Gene Expression Omnibus database were used to evaluate the prognostic value of aggrephagy-related immune cell subtypes and predict immune checkpoint blockade immunotherapeutic response in MM. Compared with healthy BM, MM BM exhibited different patterns of aggrephagy-related gene expression. In MM BM, macrophages, CD8 + T cells, B cells and natural killer cells could be grouped into four to nine aggrephagy-related subclusters. The signature of aggrephagy signaling molecule expression in the immune cells correlates with the patient's prognosis. Our investigation provides a novel view of aggrephagy signaling in MM tumor microenvironment cells, which might be a prognostic indicator and potential target for MM treatment., (© 2024 John Wiley & Sons Ltd.)

Published

2024

183. 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

Li Y, Hu GH, Xu LP, Zhang XH, Liu KY, Suo P, Wang Y, Cheng YF, and Huang XJ

Subjects

Humans, Child, Male, Female, Child, Preschool, Adolescent, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma therapy, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma mortality, Survival Rate, Precursor Cell Lymphoblastic Leukemia-Lymphoma therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma mortality, Receptors, Chimeric Antigen, Combined Modality Therapy, Hematopoietic Stem Cell Transplantation methods, Immunotherapy, Adoptive methods, Immunotherapy, Adoptive adverse effects, Philadelphia Chromosome

Abstract

Background: Philadelphia chromosome (Ph)-positive B-cell acute lymphoblastic leukemia (ALL) has a high complete remission (CR) rate, but relapse and prolonged measurable residual disease remain serious problems. We sought to describe the CR rate measurable residual disease negative rate and address the results and safety of pediatric patients who underwent after receiving chimeric antigen receptor (CAR) specific for CD19 (CAR-19) followed by hematopoietic stem cell transplantation (HSCT) for the treatment of Ph-positive ALL., Methods: A descriptive study was conducted at Peking University People's Hospital from September 2013 to January 2021. 13 patients with relapsed/refractory Ph-positive B-ALL who received CAR-T therapy followed by allo-HSCT were included. We concentrated on the overall patient survival and CR rate., Results: The median time between CAR-T therapy and allo-HSCT was 58 days. Among all the patients, the CR rate was 100%, the flow cytometry negativity rate was 84.62%, and the BCR-ABL negativity rate was 53.85% at 1 month after CAR-T infusion. All the patients achieved a major molecular response in 6 months after HSCT. After a median follow-up of 45 months, the 3-year OS rate was 66.7%, and the 3-year DFS rate was 61.5%. The 3-year OS rate of patients with BCR-ABL-positive pre-HSCT was significantly lower than that in the BCR-ABL-negative group (40.0% vs. 85.7%, P =0.042). Also, the same trend was observed for the 3-year DFS rate but did not differ significantly (40.0% vs. 75.0%, P =0.233)., Conclusions: CAR-T therapy followed by allo-HSCT can be a safe and effective treatment for Ph-positive B-ALL pediatric patients., Competing Interests: The authors declare no conflict of interest., (Copyright © 2024 Wolters Kluwer Health, Inc. All rights reserved.)

Published

2024

184. Immunosuppressive regulatory cells in cancer immunotherapy: restrain or modulate?

Author

Wu Y, Chen D, Gao Y, Xu Q, Zhou Y, Ni Z, and Na M

Subjects

Humans, Tumor Escape immunology, Drug Resistance, Neoplasm immunology, Animals, Immunosuppression Therapy, Neoplasms therapy, Neoplasms immunology, Immunotherapy methods, T-Lymphocytes, Regulatory immunology, Myeloid-Derived Suppressor Cells immunology

Abstract

Immunosuppressive regulatory cells (IRCs) play important roles in negatively regulating immune response, and are mainly divided into myeloid-derived suppressor cells (MDSCs) and regulatory T cells (Tregs). Large numbers of preclinical and clinical studies have shown that inhibition or reduction of IRCs could effectively elevate antitumor immune responses. However, several studies also reported that excessive inhibition of IRCs function is one of the main reasons causing the side effects of cancer immunotherapy. Therefore, the reasonable regulation of IRCs is crucial for improving the safety and efficiency of cancer immunotherapy. In this review, we summarised the recent research advances in the cancer immunotherapy by regulating the proportion of IRCs, and discussed the roles of IRCs in regulating tumour immune evasion and drug resistance to immunotherapies. Furthermore, we also discussed how to balance the potential opportunities and challenges of using IRCs to improve the safety of cancer immunotherapies., (© 2024. The Author(s) under exclusive licence to Japan Human Cell Society.)

Published

2024

185. Improved CAR-T cell activity associated with increased mitochondrial function primed by galactose.

Author

Gross G, Alkadieri S, Meir A, Itzhaki O, Aharoni-Tevet Y, Ben Yosef S, Zenab A, Shbiro L, Toren A, Yardeni T, and Jacoby E

Subjects

Animals, Mice, Humans, Receptors, Chimeric Antigen metabolism, Receptors, Chimeric Antigen immunology, Precursor Cell Lymphoblastic Leukemia-Lymphoma metabolism, Precursor Cell Lymphoblastic Leukemia-Lymphoma pathology, Antigens, CD19 metabolism, T-Lymphocytes metabolism, T-Lymphocytes immunology, Xenograft Model Antitumor Assays, Galactose metabolism, Mitochondria metabolism, Immunotherapy, Adoptive methods

Abstract

CD19 CAR-T cells have led to durable remissions in patients with refractory B-cell malignancies; nevertheless, most patients eventually relapse in the long term. Many interventions aimed at improving current products have been reported, with a subset of them focusing on a direct or indirect link to the metabolic state of the CAR-T cells. We assessed clinical products from an ongoing clinical trial utilizing CD19-28z CAR-T cells from patients with acute lymphoblastic leukemia. CAR-T clinical products leading to a complete response had significantly higher mitochondrial function (by oxygen consumption rate) irrespective of mitochondrial content. Next, we replaced the carbon source of the media from glucose to galactose to impact cellular metabolism. Galactose-containing media increased mitochondrial activity in CAR-T cells, and improved in in-vitro efficacy, without any consistent phenotypic change in memory profile. Finally, CAR-T cells produced in galactose-based glucose-free media resulted in increased mitochondrial activity. Using an in-vivo model of Nalm6 injected mice, galactose-primed CAR-T cells significantly improved leukemia-free survival compared to standard glucose-cultured CAR-T cells. Our results prove the significance of mitochondrial metabolism on CAR-T cell efficacy and suggest a translational pathway to improve clinical products., (© 2024. The Author(s), under exclusive licence to Springer Nature Limited.)

Published

2024

186. Programmable and multi-targeted CARs: a new breakthrough in cancer CAR-T cell therapy.

Author

Tahmasebi S, Elahi R, Khosh E, and Esmaeilzadeh A

Subjects

Humans, Immunotherapy, Adoptive, Neoplasms therapy, Receptors, Chimeric Antigen therapeutic use

Abstract

CAR-T cell therapy, as a novel immunotherapy approach, has indicated successful results in the treatment of hematological malignancies; however, distinct results have been achieved regarding solid tumors. Tumor immunosuppressive microenvironment has been identified as the most critical barrier in CAR-T cell therapy of solid tumors. Developing novel strategies to augment the safety and efficacy of CAR-T cells could be useful to overcome the solid tumor hurdles. Similar to other cancer treatments, CAR-T cell therapy can cause some side effects, which can disturb the healthy tissues. In the current review, we will discuss the practical breakthroughs in CAR-T cell therapy using the multi-targeted and programmable CARs instead of conventional types. These superior types of CAR-T cells have been developed to increase the function and safety of T cells in a controllable manner, which would diminish the incidence of relevant side effects. Moreover, we will describe the capability of these powerful CARs in targeting multiple tumor antigens, redirecting the CAR-T cells to specific target cells, incrementing the safety of CARs, and other advantages that lead to promising outcomes in cancer CAR-T cell therapy.

Published

2021

187. The screening, identification, design and clinical application of tumor-specific neoantigens for TCR-T cells.

Author

Li, Jiangping, Xiao, Zhiwen, Wang, Donghui, Jia, Lei, Nie, Shihong, Zeng, Xingda, and Hu, Wei

Subjects

CLINICAL medicine, MEDICAL screening, IMMUNE checkpoint proteins, CANCER vaccines, OVERALL survival

Abstract

Recent advances in neoantigen research have accelerated the development of tumor immunotherapies, including adoptive cell therapies (ACTs), cancer vaccines and antibody-based therapies, particularly for solid tumors. With the development of next-generation sequencing and bioinformatics technology, the rapid identification and prediction of tumor-specific antigens (TSAs) has become possible. Compared with tumor-associated antigens (TAAs), highly immunogenic TSAs provide new targets for personalized tumor immunotherapy and can be used as prospective indicators for predicting tumor patient survival, prognosis, and immune checkpoint blockade response. Here, the identification and characterization of neoantigens and the clinical application of neoantigen-based TCR-T immunotherapy strategies are summarized, and the current status, inherent challenges, and clinical translational potential of these strategies are discussed. Key points: 1) Established the computational process and platform of neoantigen prediction, and comprehensive prediction and screening of tumor specific neoantigens. 2) Rapid identification of neoantigen-specific TCRs for personalized engineered TCR-T cell therapy. 3) Classification and characteristics of tumor specific neoantigen-based therapy, and combined antitumor strategies. 4) The current status, inherent challenges, and clinical translational potential of TCR-T therapy. [ABSTRACT FROM AUTHOR]

Published

2023

188. A CD64/FcγRI-mediated mechanism hijacks PD-1 from PD-L1/2 interaction and enhances anti-PD-1 functional recovery of exhausted T cells.

Author

Joo, Victor, Petrovas, Constantinos, de Leval, Laurence, Noto, Alessandra, Obeid, Michel, Fenwick, Craig, and Pantaleo, Giuseppe

Subjects

T cells, PROGRAMMED cell death 1 receptors, T-cell exhaustion, T cell receptors, IMMUNE checkpoint inhibitors, CELL death, NEUROREHABILITATION, SECOND language acquisition

Abstract

Therapeutic monoclonal antibodies (mAb) targeting the immune checkpoint inhibitor programmed cell death protein 1 (PD-1) have achieved considerable clinical success in anti-cancer therapy through relieving T cell exhaustion. Blockade of PD-1 interaction with its ligands PD-L1 and PD-L2 is an important determinant in promoting the functional recovery of exhausted T cells. Here, we show that anti-PD-1 mAbs act through an alternative mechanism leading to the downregulation of PD-1 surface expression on memory CD4+ and CD8+ T cells. PD-1 receptor downregulation is a distinct process from receptor endocytosis and occurs in a CD14+ monocyte dependent manner with the CD64/Fcγ receptor I acting as the primary factor for this T cell extrinsic process. Importantly, downregulation of surface PD-1 strongly enhances antigen-specific functional recovery of exhausted PD-1+CD8+ T cells. Our study demonstrates a novel mechanism for reducing cell surface levels of PD-1 and limiting the inhibitory targeting by PD-L1/2 and thereby enhancing the efficacy of anti-PD-1 Ab in restoring T cell functionality. [ABSTRACT FROM AUTHOR]

Published

2023

189. Challenges and new technologies in adoptive cell therapy.

Author

Zhang, Pengchao, Zhang, Guizhong, and Wan, Xiaochun

Subjects

CELLULAR therapy, T cell receptors, CHIMERIC antigen receptors, TUMOR-infiltrating immune cells, CANCER treatment

Abstract

Adoptive cell therapies (ACTs) have existed for decades. From the initial infusion of tumor-infiltrating lymphocytes to the subsequent specific enhanced T cell receptor (TCR)-T and chimeric antigen receptor (CAR)-T cell therapies, many novel strategies for cancer treatment have been developed. Owing to its promising outcomes, CAR-T cell therapy has revolutionized the field of ACTs, particularly for hematologic malignancies. Despite these advances, CAR-T cell therapy still has limitations in both autologous and allogeneic settings, including practicality and toxicity issues. To overcome these challenges, researchers have focused on the application of CAR engineering technology to other types of immune cell engineering. Consequently, several new cell therapies based on CAR technology have been developed, including CAR-NK, CAR-macrophage, CAR-γδT, and CAR-NKT. In this review, we describe the development, advantages, and possible challenges of the aforementioned ACTs and discuss current strategies aimed at maximizing the therapeutic potential of ACTs. We also provide an overview of the various gene transduction strategies employed in immunotherapy given their importance in immune cell engineering. Furthermore, we discuss the possibility that strategies capable of creating a positive feedback immune circuit, as healthy immune systems do, could address the flaw of a single type of ACT, and thus serve as key players in future cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2023

190. Antitumor effect of neoantigen-reactive T cells combined with PD1 inhibitor therapy in mouse lung cancer.

Author

Qin, Huan, Hu, Haiyan, Liao, Ximing, Zhao, Pei, He, Wenjuan, Su, Xiaoping, Sun, Jiaxing, and Li, Qiang

Subjects

T cells, LUNG cancer, T cell receptors, IMMUNE checkpoint proteins, DENDRITIC cells, TUMOR growth

Abstract

Purpose: Neoantigens produced from mutations in tumors are important targets of T-cell-based immunotherapy and immune checkpoint blockade has been approved for treating multiple solid tumors. We investigated the potential benefit of adoptive neoantigen-reactive T (NRT) cells in combination with programmed cell death protein 1 inhibitor (anti-PD1) for treating lung cancer in a mouse model. Methods: NRT cells were prepared by co-culturing T cells and neoantigen-RNA vaccine-induced dendritic cells. Then, adoptive NRT cells in combination with anti-PD1 were administered to tumor-bearing mice. Pre- and post-therapy cytokine secretion, antitumor efficacy, and tumor microenvironment (TME) changes were determined both in vitro and in vivo. Results: We successfully generated NRT cells based on the 5 neoantigen epitopes identified in this study. NRT cells exhibited an enhanced cytotoxic phenotype in vitro and the combination therapy led to attenuated tumor growth. In addition, this combination strategy downregulated the expression of the inhibitory marker PD‐1 on tumor-infiltrating T cells and promoted the trafficking of tumor-specific T cells to the tumor sites. Conclusion: The adoptive transfer of NRT cells in association with anti-PD1 therapy can exert an antitumor effect on lung cancer, and is a feasible, effective, and novel immunotherapy regimen for treating solid tumors. [ABSTRACT FROM AUTHOR]

Published

2023

191. Get me out of here: Sphingosine 1‐phosphate signaling and T cell exit from tissues during an immune response.

Author

Hallisey, Victoria M. and Schwab, Susan R.

Subjects

T cells, IMMUNE response, SPHINGOSINE, CELL communication, LYMPHOID tissue

Abstract

Summary: During an immune response, the duration of T cell residence in lymphoid and non‐lymphoid tissues likely affects T cell activation, differentiation, and memory development. The factors that govern T cell transit through inflamed tissues remain incompletely understood, but one important determinant of T cell exit from tissues is sphingosine 1‐phosphate (S1P) signaling. In homeostasis, S1P levels are high in blood and lymph compared to lymphoid organs, and lymphocytes follow S1P gradients out of tissues into circulation using varying combinations of five G‐protein coupled S1P receptors. During an immune response, both the shape of S1P gradients and the expression of S1P receptors are dynamically regulated. Here we review what is known, and key questions that remain unanswered, about how S1P signaling is regulated in inflammation and in turn how S1P shapes immune responses. [ABSTRACT FROM AUTHOR]

Published

2023

192. Lenalidomide overcomes the resistance to third-generation CD19-CAR-T cell therapy in preclinical models of diffuse large B-cell lymphoma.

Author

Jin, Zhen, Xiang, Rufang, Qing, Kai, Li, Dan, Liu, Zhao, Li, Xiaoyang, Zhu, Hongming, Zhang, Yunxiang, Wang, Lining, Xue, Kai, Liu, Han, Xu, Zizhen, Wang, Yingxiao, and Li, Junmin

Subjects

DIFFUSE large B-cell lymphomas, B cells, LENALIDOMIDE, ANIMAL models in research, CELLULAR therapy, HEMATOLOGIC malignancies, PROGRAMMED cell death 1 receptors

Abstract

Purpose: Chimeric antigen receptor (CAR)-T cells against CD19 have been proven to be effective in treating B-cell hematological malignancies. However, the efficacy of this promising therapy is limited by many factors. Methods: In this study, the germinal center B-cell-like diffuse large B-cell lymphoma (GCB-DLBCL) cell line OCI-Ly1, and patient-derived xenografted (PDX) mice (CY-DLBCL) were used as the CAR-T cell-resistant model. Meanwhile, the activated B-cell-like (ABC) DLBCL cell line OCI-Ly3 and PDX mice (ZML-DLBCL) were defined as the CAR-T sensitive model. The enhancement of CAR-T cell function by lenalidomide (LEN) was examined in vitro and in vivo. Results: Lenalidomide effectively enhanced the function of third-generation CD19-CAR-T cells by polarizing CD8+ CAR-T cells to CD8 early-differentiated stage and Th1 type, reducing CAR-T cell exhaustion and improving cell expansion. It was further demonstrated that CAR-T cells combined with LEN substantially reduce the tumor burden and prolong the survival time in various DLBCL mouse models. LEN was also found to promote the infiltration of CD19-CAR-T cells into the tumor site by modulating the tumor microenvironment. Conclusion: In summary, the results of the present study suggest that LEN can improve the function of CD19-CAR-T cells, providing a basis for clinical trials using this combination therapy against DLBCL. [ABSTRACT FROM AUTHOR]

Published

2023

193. Cell Reprogramming Techniques: Contributions to Cancer Therapy.

Author

Guo, Tongtong and Wei, Qi

Subjects

CANCER treatment, INDUCED pluripotent stem cells, HEREDITY, PHENOTYPIC plasticity, CANCER cells

Abstract

The reprogramming of terminally differentiated cells over the past few years has become important for induced pluripotent stem cells (iPSCs) in the field of regenerative medicine and disease drug modeling. At the same time, iPSCs have also played an important role in human cancer research. iPSCs derived from cancer patients can be used to simulate the early progression of cancer, for drug testing, and to study the molecular mechanism of cancer occurrence. In recent years, with the application of cellular immunotherapy in cancer therapy, patient-derived iPSC-induced immune cells (T, natural killer, and macrophage cells) solve the problem of immune rejection and have higher immunogenicity, which greatly improves the therapeutic efficiency of immune cell therapy. With the continuous progress of cancer differentiation therapy, iPSC technology can reprogram cancer cells to a more primitive pluripotent undifferentiated state, and successfully reverse cancer cells to a benign phenotype by changing the epigenetic inheritance of cancer cells. This article reviews the recent progress of cell reprogramming technology in human cancer research, focuses on the application of reprogramming technology in cancer immunotherapy and the problems solved, and summarizes the malignant phenotype changes of cancer cells in the process of reprogramming and subsequent differentiation. [ABSTRACT FROM AUTHOR]

Published

2023

194. Tümör Hücre Yüzey Antijenleri.

Author

Pehlivan, Melek and Pirim, İbrahim

Abstract

Copyright of Journal of Tepecik Education & Research Hospital / İzmir Tepecik Eğitim ve Araştırma Hastanesi Dergisi is the property of Logos Medical Publishing and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

195. Targeting CXCL9/10/11–CXCR3 axis: an important component of tumor-promoting and antitumor immunity.

Author

Pan, Minjie, Wei, Xiaoshan, Xiang, Xuan, Liu, Yanhong, Zhou, Qiong, and Yang, Weibing

Abstract

Chemokines are chemotactic-competent molecules composed of a family of small cytokines, playing a key role in regulating tumor progression. The roles of chemokines in antitumor immune responses are of great interest. CXCL9, CXCL10, and CXCL11 are important members of chemokines. It has been widely investigated that these three chemokines can bind to their common receptor CXCR3 and regulate the differentiation, migration, and tumor infiltration of immune cells, directly or indirectly affecting tumor growth and metastasis. Here, we summarize the mechanism of how the CXCL9/10/11–CXCR3 axis affects the tumor microenvironment, and list the latest researches to find out how this axis predicts the prognosis of different cancers. In addition, immunotherapy improves the survival of tumor patients, but some patients show drug resistance. Studies have found that the regulation of CXCL9/10/11–CXCR3 on the tumor microenvironment is involved in the process of changing immunotherapy resistance. Here we also describe new approaches to restoring sensitivity to immune checkpoint inhibitors through the CXCL9/10/11–CXCR3 axis. [ABSTRACT FROM AUTHOR]

Published

2023

196. T‐cell exhaustion in CAR‐T‐cell therapy and strategies to overcome it.

Author

Yin, Xuechen, He, Lingfeng, and Guo, Zhigang

Subjects

T-cell exhaustion, CHIMERIC antigen receptors, CYTOTOXIC T cells, T cells, CANCER treatment

Abstract

Tumour immunotherapy has achieved good therapeutic effects in clinical practice and has received increased attention. Cytotoxic T cells undoubtedly play an important role in tumour immunotherapy. As a revolutionary tumour immunotherapy approach, chimeric antigen receptor T‐cell (CAR‐T‐cell) therapy has made breakthroughs in the treatment of haematological cancers. However, T cells are easily exhausted in vivo, especially after they enter solid tumours. The exhaustion of T cells can lead to poor results of CAR‐T‐cell therapy in the treatment of solid tumours. Here, we review the reasons for T‐cell exhaustion and how T‐cell exhaustion develops. We also review and discuss ways to improve CAR‐T‐cell therapy effects by regulating T‐cell exhaustion. [ABSTRACT FROM AUTHOR]

Published

2023

197. Macrophage's role in solid tumors: two edges of a sword.

Author

Jahandideh, Arian, Yarizadeh, Mahsa, Noei-Khesht Masjedi, Maryam, Fatehnejad, Mina, Jahandideh, Romina, Soheili, Roben, Eslami, Yeganeh, Zokaei, Maryam, Ahmadvand, Ardavan, Ghalamkarpour, Nogol, Kumar Pandey, Rajan, Nabi Afjadi, Mohsen, and payandeh, Zahra

Subjects

MACROPHAGES, CANCER cells, EXTRACELLULAR matrix, CHIMERIC antigen receptors, CELL proliferation

Abstract

The tumor microenvironment is overwhelmingly dictated by macrophages, intimately affiliated with tumors, exercising pivotal roles in multiple processes, including angiogenesis, extracellular matrix reconfiguration, cellular proliferation, metastasis, and immunosuppression. They further exhibit resilience to chemotherapy and immunotherapy via meticulous checkpoint blockades. When appropriately stimulated, macrophages can morph into a potent bidirectional component of the immune system, engulfing malignant cells and annihilating them with cytotoxic substances, thus rendering them intriguing candidates for therapeutic targets. As myelomonocytic cells relentlessly amass within tumor tissues, macrophages rise as prime contenders for cell therapy upon the development of chimeric antigen receptor effector cells. Given the significant incidence of macrophage infiltration correlated with an unfavorable prognosis and heightened resistance to chemotherapy in solid tumors, we delve into the intricate role of macrophages in cancer propagation and their promising potential in confronting four formidable cancer variants—namely, melanoma, colon, glioma, and breast cancers. [ABSTRACT FROM AUTHOR]

Published

2023

198. The potential of activator protein 1 (AP-1) in cancer targeted therapy.

Author

Dandan Song, Yan Lian, and Lin Zhang

Subjects

AP-1 transcription factor, CANCER treatment, SMALL molecules, DRUG resistance, ANTINEOPLASTIC agents

Abstract

Activator protein-1 (AP-1) is a transcription factor that consists of a diverse group of members including Jun, Fos, Maf, and ATF. AP-1 involves a number of processes such as proliferation, migration, and invasion in cells. Dysfunctional AP-1 activity is associated with cancer initiation, development, invasion, migration and drug resistance. Therefore, AP-1 is a potential target for cancer targeted therapy. Currently, some small molecule inhibitors targeting AP-1 have been developed and tested, showing some anticancer effects. However, AP-1 is complex and diverse in its structure and function, and different dimers may play different roles in different type of cancers. Therefore, more research is needed to reveal the specific mechanisms of AP-1 in cancer, and how to select appropriate inhibitors and treatment strategies. Ultimately, this review summarizes the potential of combination therapy for cancer. [ABSTRACT FROM AUTHOR]

Published

2023

199. GAS6-based CAR-T cells exhibit potent antitumor activity against pancreatic cancer.

Author

Fan, Jiawei, Yu, Ye, Yan, Lanzhen, Yuan, Yuncang, Sun, Bin, Yang, Dong, Liu, Nan, Guo, Jing, Zhang, Jie, and Zhao, Xudong

Subjects

PANCREATIC cancer, ANTINEOPLASTIC agents, PANCREATIC tumors, CANCER cells, CARCINOGENESIS, KINASES

Abstract

Background: The receptor tyrosine kinases TAM family (TYRO3, AXL, and MERTK) are highly expressed in multiple forms of cancer cells and tumor-associated macrophages and promote the development of cancers including pancreatic tumor. Targeting TAM receptors could be a promising therapeutic option. Methods: We designed a novel CAR based on the extracellular domain of growth arrest-specific protein 6 (GAS6), a natural ligand for all TAM members. The ability of CAR-T to kill pancreatic cancer cells is tested in vitro and in vivo, and the safety is evaluated in mice and nonhuman primate. Results: GAS6-CAR-T cells efficiently kill TAM-positive pancreatic cancer cell lines, gemcitabine-resistant cancer cells, and cancer stem-like cells in vitro. GAS6-CAR-T cells also significantly suppressed the growth of PANC1 xenografts and patient-derived xenografts in mice. Furthermore, these CAR-T cells did not induce obvious side effects in nonhuman primate or mice although the CAR was demonstrated to recognize mouse TAM. Conclusions: Our findings indicate that GAS6-CAR-T-cell therapy may be effective for pancreatic cancers with low toxicity. [ABSTRACT FROM AUTHOR]

Published

2023

200. Flubendazole inhibits PD-1 and suppresses melanoma growth in immunocompetent mice.

Author

Li, Yue, Wu, Ben, Hossain, Md Jakir, Quagliata, Lily, O'Meara, Connor, Wilkins, Marc R., Corley, Susan, and Khachigian, Levon M.

Subjects

PROGRAMMED cell death 1 receptors, IPILIMUMAB, T cell differentiation, IMMUNE checkpoint inhibitors, SMALL molecules, MELANOMA

Abstract

Background: Immune checkpoint inhibitor therapy has revolutionized the clinical management of a diverse range of cancer types, including advanced cutaneous melanoma. While immunotherapy targeting the PD-1/PD-L1 system has become standard of care, overall response rates remain unsatisfactory for most patients and there are no approved small molecule inhibitors of the PD-1/PD-L1 system. Flubendazole (FLU) is an anthelmintic that has been used to treat worm infections in humans and animals for decades. Methods: Here we tested the anti-cancer activity of systemically delivered FLU with suppression of PD-1 in immunocompetent mice. Results: In C57BL/6J mice bearing subcutaneous B16F10 melanoma, FLU reduced both tumor growth and PD-1 protein levels without affecting levels of PD-L1. FLU's suppression of PD-1 was accompanied by increased CD3+ T cell infiltration. Western blotting with extracts from human Jurkat T cells showed that FLU inhibited PD-1 protein expression, findings confirmed by flow cytometry. To gain mechanistic insights on FLU's ability to suppress PD-1 protein levels, we performed bulk RNA sequencing on extracts of Jurkat T cells exposed to the benzimidazole for 4 h. From a pool of 14,475 genes there were 1218 differentially-expressed genes; 687 with increased expression and 531 with decreased expression. Among the genes induced by FLU was the AP-1 family member, JUN and surprisingly, pdcd1. KEGG pathway analysis showed FLU up-regulated genes over-represented in multiple pathways (p < 0.01), the top hit being amoebiasis. FLU also affected the expression of genes in cancer-associated pathways, both through down-regulation and up-regulation. Gene set enrichment analysis revealed a large number of immunological signature gene sets correlated with FLU treatment, including gene sets associated with T cell differentiation, proliferation and function. The AP-1 inhibitor T5224 rescued PD-1 protein expression from inhibition by FLU. Conclusion: This study is the first to show that FLU can inhibit melanoma growth with PD-1 suppression in immunocompetent mice. [ABSTRACT FROM AUTHOR]

Published

2023