Your search keyword '"immunotherapy"' showing total 64,436 results

1. Soluble immune checkpoint factors reflect exhaustion of antitumor immunity and response to PD-1 blockade.

Author

Kurosaki, Takashi, Togashi, Yosuke, Fukuoka, Kazuya, Goto, Megumi, Chiba, Yasutaka, Tomida, Shuta, Ota, Takayo, Haratani, Koji, Takahama, Takayuki, Tanizaki, Junko, Yoshida, Takeshi, Iwasa, Tsutomu, Tanaka, Kaoru, Takeda, Masayuki, Hirano, Tomoko, Yoshida, Hironori, Ozasa, Hiroaki, Sakamori, Yuichi, Sakai, Kazuko, Higuchi, Keiko, Uga, Hitoshi, Suminaka, Chihiro, Hirai, Toyohiro, Nishio, Kazuto, Nakagawa, Kazuhiko, Honjo, Tasuku, Hayashi, Hidetoshi, Chamoto, Kenji, and Hatae, Ryusuke

Subjects

Immunotherapy, Lung cancer, Oncology, T cells, Humans, B7-H1 Antigen, Carcinoma, Non-Small-Cell Lung, Immunologic Factors, Lung Neoplasms, Programmed Cell Death 1 Receptor, Immune Checkpoint Inhibitors

Abstract

BACKGROUNDPrecise stratification of patients with non-small cell lung cancer (NSCLC) is needed for appropriate application of PD-1/PD-L1 blockade therapy.METHODSWe measured soluble forms of the immune-checkpoint molecules PD-L1, PD-1, and CTLA-4 in plasma of patients with advanced NSCLC before PD-1/PD-L1 blockade. A prospective biomarker-finding trial (cohort A) included 50 previously treated patients who received nivolumab. A retrospective observational study was performed for patients treated with any PD-1/PD-L1 blockade therapy (cohorts B and C), cytotoxic chemotherapy (cohort D), or targeted therapy (cohort E). Plasma samples from all patients were assayed for soluble immune-checkpoint molecules with a highly sensitive chemiluminescence-based assay.RESULTSNonresponsiveness to PD-1/PD-L1 blockade therapy was associated with higher concentrations of these soluble immune factors among patients with immune-reactive (hot) tumors. Such an association was not apparent for patients treated with cytotoxic chemotherapy or targeted therapy. Integrative analysis of tumor size, PD-L1 expression in tumor tissue (tPD-L1), and gene expression in tumor tissue and peripheral CD8+ T cells revealed that high concentrations of the 3 soluble immune factors were associated with hyper or terminal exhaustion of antitumor immunity. The combination of soluble PD-L1 (sPD-L1) and sCTLA-4 efficiently discriminated responsiveness to PD-1/PD-L1 blockade among patients with immune-reactive tumors.CONCLUSIONCombinations of soluble immune factors might be able to identify patients unlikely to respond to PD-1/PD-L1 blockade as a result of terminal exhaustion of antitumor immunity. Our data suggest that such a combination better predicts, along with tPD-L1, for the response of patients with NSCLC.TRIAL REGISTRATIONUMIN000019674.FUNDINGThis study was funded by Ono Pharmaceutical Co. Ltd. and Sysmex Corporation.

Published

2024

2. Checkpoint inhibitor therapy: Immune-related adverse event management.

Author

DAVIS, LORI, CASSELBURY, MARY BETH, and WILSON, SHARON

Subjects

*PREVENTION of drug side effects, *PATIENT education, *CONTINUING education units, *DRUG side effects, *IMMUNE system, *INFORMATION resources, *IMMUNE checkpoint inhibitors, *TUMORS, *MEDICAL needs assessment, *PHARMACODYNAMICS

Abstract

Treatment with immune checkpoint inhibitors for cancer is associated with a high prevalence of multiple immune-related toxicities. Immune-related adverse events (irAEs) can occur anytime during treatment and up to 3 months after treatment. This article discusses checkpoint inhibitor therapy and describes the implementation of a patient education program focused on recognizing immunotherapy irAEs and their toxicities. [ABSTRACT FROM AUTHOR]

Published

2024

3. Current Management Practices for Endometrial Cancer (EC) in the UK: A National Healthcare Professional Survey (KNOW-EC).

Author

George, A., Herbertson, R.A., Stillie, A., McCormack, S., Drean, A.M., Wesselbaum, A., Hudson, E., Miles, T., Ryan, N.A.J., Maxwell, H., Le Treust, L., and McCormack, M.

Subjects

*MEDICAL protocols, *NURSES, *HEALTH services accessibility, *OCCUPATIONAL adaptation, *CANCER patient medical care, *INTERVIEWING, *IMMUNOTHERAPY, *ONCOLOGY, *DESCRIPTIVE statistics, *TUMOR markers, *ENDOMETRIAL tumors, *ONCOLOGY nursing, *FEMALE reproductive organ tumors, *TELEPHONES, *ONCOLOGISTS, *PATIENT aftercare

Abstract

The clinical landscape for endometrial cancer in the UK is evolving to include new management guidelines and targeted treatment options. An understanding of current treatment and management practices in the UK will help services plan and adapt to upcoming changes. The purpose of this survey was to understand current and anticipated real-world practices for endometrial cancer care in the UK and potential areas for optimisation. Telephone interviews were conducted in November/December 2021 with UK-based healthcare professionals involved in endometrial cancer management. Questions were aligned with the British Gynaecological Cancer Society/European Society for Medical Oncology recommendations, covering the pathway from diagnosis and treatment to follow-up. A total of 63 healthcare professionals (HCPs) involved in the management of patients with endometrial cancer participated in telephone interviews. The results highlighted variations in management and treatment practices for endometrial cancer and suggest that current UK practice appears to diverge from national and international guidance in some instances. While somatic mismatch repair deficiency testing was used by 89.7% of respondents as mainstream testing, the survey highlighted a lack of access to other key molecular biomarker tests, such as polymerase epsilon (POLE) sequencing (used by only 9.8% of HCPs at the time of the survey). The results highlighted several perceived practical barriers to the swift adoption of new therapeutic options, including funding access, limited staff, treatment-related resources, staff education, and support. Our findings support the need for better access to biomarkers that could enable more effective and targeted treatments. • This survey describes the recent UK treatment landscape for endometrial cancer. • Respondents reported a wide degree in variation in practice across the UK. • There is a lack of access to certain molecular biomarker tests e.g., POLE tests. • Practical barriers may prevent swift adoption of new therapeutic options. • Areas for optimisation include additional education on immunotherapy treatment. [ABSTRACT FROM AUTHOR]

Published

2024

4. Immune Checkpoint Inhibitor Therapy for Kidney Transplant Recipients - A Review of Potential Complications and Management Strategies.

Author

Barbir, Elena Bianca, Abdulmoneim, Samer, Dudek, Arkadiusz Z., and Kukla, Aleksandra

Subjects

*IMMUNE checkpoint inhibitors, *KIDNEY transplantation, *GRAFT rejection, *THERAPEUTICS, *METASTASIS, *SKIN cancer

Abstract

Immune checkpoint inhibitor (ICI) therapy has enabled a paradigm shift in Oncology, with the treatment of metastatic cancer in certain tumor types becoming akin to the treatment of chronic disease. Kidney transplant recipients (KTR) are at increased risk of developing cancer compared to the general population. Historically, KTR were excluded from ICI clinical trials due to concern for allograft rejection and decreased anti-tumor efficacy. While early post-marketing data revealed an allograft rejection risk of 40%-50%, 2 recent small prospective trials have demonstrated lower rates of rejection of 0%-12%, suggesting that maintenance immunosuppression modification prior to ICI start modulates rejection risk. Moreover, objective response rates induced by ICI for the treatment of advanced or metastatic skin cancer, the most common malignancy in KTR, have been comparable to those achieved by immune intact patients. Non-invasive biomarkers may have a role in risk-stratifying patients before starting ICI, and monitoring for rejection, though allograft biopsy is required to confirm diagnosis. This clinically focused review summarizes current knowledge on complications of ICI use in KTR, including their mechanism, risk mitigation strategies, non-invasive biomarker use, approaches to treatment of rejection, and suggestions for future directions in research. [ABSTRACT FROM AUTHOR]

Published

2024

5. Stimuli‐Responsive Nanocarriers as Active Enhancers of Antitumoral Immunotherapy.

Author

Parra‐Nieto, Jorge, de Carcer, Iñigo Aguirre, García del Cid, María Amor, Jimenez‐Falcao, Sandra, Gónzalez‐Larre, Javier, and Baeza, Alejandro

Subjects

IMMUNOLOGIC memory, CANCER invasiveness, IMMUNE response, IMMUNE system, NANOCARRIERS

Abstract

In recent years, the understanding of the role of the immune system in tumor progression and metastasis is paving the way for the development of antitumoral strategies based on the delivery of immunotherapeutic agents. The engineering of stimuli‐responsive nanocarriers able to release their payload in a controlled manner being able to boost potent and sustained immune responses against tumors has provided a powerful tool to eradicate tumors with extreme precision. Paramount advantages to trigger the immune system against tumors are the high selectivity and memory effect of immune response, which allows not only to eradicate primary and metastatic malignancies but also to avoid their relapse. In this review, the recent advances carried out in the development of smart nanocarriers for immunotherapy are presented. [ABSTRACT FROM AUTHOR]

Published

2024

6. Combining mathematical modeling, in vitro data and clinical target expression to support bispecific antibody binding affinity selection: a case example with FAP-4-1BBL.

Author

Sanchez, Javier, Claus, Christina, McIntyre, Christine, Tanos, Tamara, Boehnke, Axel, Friberg, Lena E., Jönsson, Siv, and Frances, Nicolas

Subjects

BISPECIFIC antibodies, T cell receptors, CELL receptors, COLON cancer, FIBROBLASTS

Abstract

The majority of bispecific costimulatory antibodies in cancer immunotherapy are capable of exerting tumor-specific T-cell activation by simultaneously engaging both tumor-associated targets and costimulatory receptors expressed by T cells. The amount of trimeric complex formed when the bispecific antibody is bound simultaneously to the T cell receptor and the tumor-associated target follows a bell-shaped curve with increasing bispecific antibody exposure/dose. The shape of the curve is determined by the binding affinities of the bispecific antibody to its two targets and target expression. Here, using the case example of FAP-4-1BBL, a fibroblast activation protein alpha (FAP)-directed 4-1BB (CD137) costimulator, the impact of FAP-binding affinity on trimeric complex formation and pharmacology was explored using mathematical modeling and simulation. We quantified (1) the minimum number of target receptors per cell required to achieve pharmacological effect, (2) the expected coverage of the patient population for 19 different solid tumor indications, and (3) the range of pharmacologically active exposures as a function of FAP-binding affinity. A 10-fold increase in FAPbinding affinity (from a dissociation constant [KD] of 0.7 nM-0.07 nM) was predicted to reduce the number of FAP receptors needed to achieve 90% of the maximum pharmacological effect from 13,400 to 4,000. Also, the number of patients with colon cancer that would achieve 90% of the maximum effect would increase from 6% to 39%. In this work, a workflow to select binding affinities for bispecific antibodies that integrates preclinical in vitro data, mathematical modeling and simulation, and knowledge on target expression in the patient population, is provided. The early implementation of this approach can increase the probability of success with cancer immunotherapy in clinical development. [ABSTRACT FROM AUTHOR]

Published

2024

7. Out-of-hours admissions in patients treated with immune checkpoint inhibitors and their primary management with steroids.

Author

Awan, Sidra, Bharucha, Pooja, Steventon, Luke, Simpson, Helen, AHMAD, Tanya, Benafif, Sarah, Shaw, Heather, and Chambers, Pinkie

Subjects

*PREVENTION of drug side effects, *STEROID drugs, *PATIENT education, *DRUG side effects, *PATIENTS, *HOSPITAL admission & discharge, *IMMUNOTHERAPY, *RETROSPECTIVE studies, *TERTIARY care, *DESCRIPTIVE statistics, *IMMUNE checkpoint inhibitors, *LONGITUDINAL method, *MEDICAL records, *ACQUISITION of data, *ELECTRONIC health records, *LENGTH of stay in hospitals, *DEXAMETHASONE

Abstract

Introduction: The incidence of immune-related adverse events (irAEs) from immune checkpoint inhibitors (ICI) is well described. However, the impact on emergency care services is not. This study investigated the incidence of irAEs out-of-hours, and the management used to mitigate symptoms and side effects. Methods: This retrospective cohort study reviewed all emergency presentations triaged by the acute oncology team between December 2021 and June 2022, between 5 pm and 9 am. Patients were identified from triage audit sheets and remaining data points were retrieved from electronic health records. Inclusion criteria included all adult patients admitted on an ICI at one tertiary centre. Results: In 7 months, 970 patients called the acute oncology helpline 11% (n = 109) of patients were on an ICI treatment. After clinical review, 78% (n = 70) resulted in hospital admissions, with length of stay cumulating to 496 bed days. 56% (n = 39) of patients delayed reporting symptoms, ranging between 12 hours and 10 days from symptom onset to seeking support. 49% (n = 34) patients received steroids to manage suspected irAEs. Dexamethasone was the most common steroid used in 71% (n = 24) of patients, and variation was found in prescribed doses. Conclusions: These results underline the urgent need to address patient and staff education on adverse effects related to ICI. Patients require a comprehensive understanding of the symptoms and importance of prompt reporting. Staff education on recognition and treatment management is needed to reduce variation in practice. Further research is needed to identify barriers in symptom reporting and focus on realtime reporting to reduce the out-of-hours burden on services. [ABSTRACT FROM AUTHOR]

Published

2024

8. Grover's disease in oncologic patients: clinicopathologic features and systematic review.

Author

Paolino, Giovanni, Brunetti, Antonio P., Guida, Stefania, Rizzo, Nathalie, Mercuri, Santo R., and Rongioletti, Franco

Subjects

*CANCER chemotherapy, *BULLOUS pemphigoid, *ACUTE myeloid leukemia, *DRUG eruptions, *BLOOD diseases, *CUTANEOUS T-cell lymphoma, *RENAL cell carcinoma

Abstract

This article discusses Grover's disease (GD) in oncologic patients and provides a systematic review of relevant literature. GD is a skin condition whose pathogenesis is not fully understood, but recent evidence suggests it may involve an overexpression of interleukin 4 (IL-4). The association between GD and malignancies, as well as between GD and systemic oncologic treatments, has been sporadically reported. The review includes 31 patients with GD, with the most strongly associated malignancies being metastatic melanoma and hematologic malignancies. Immunotherapy was the most common observed oncologic treatment. The article also discusses the histological features, comorbidities, and treatment options for GD. [Extracted from the article]

Published

2024

9. MCMC Methods for Parameter Estimation in ODE Systems for CAR-T Cell Cancer Therapy.

Author

Antonini, Elia, Mu, Gang, Sansaloni-Pastor, Sara, Varma, Vishal, and Kabak, Ryme

Subjects

*STATISTICAL models, *HEMATOLOGIC malignancies, *T cells, *PREDICTION models, *CYTOKINE release syndrome, *GENETIC engineering, *CELL proliferation, *PROBABILITY theory, *CELLULAR therapy, *TREATMENT effectiveness, *DATA analysis software, *ALGORITHMS, *EVALUATION

Abstract

Simple Summary: Chimeric antigen receptor (CAR)-T cell therapy is a promising treatment for highly resistant blood cancers, using genetically modified T cells from the patient or a donor. While CAR-T therapy has been successful in pre-clinical and clinical stages for cancer treatment, it also presents challenges, including cytokine release syndrome. To improve the efficacy and reduce side effects, there is a need to better understand CAR-T cell behavior. We aimed to develop a mathematical framework that describes CAR-T behavior using ordinary differential equations (ODEs) and Bayesian parameter estimation (using advanced algorithms including Metropolis–Hastings, DEMetropolis, and DEMetropolisZ). This model will help to understand CAR-T behavior and, by extension, help to improve the effectiveness and efficacy of therapy in a clinical setting. Chimeric antigen receptor (CAR)-T cell therapy represents a breakthrough in treating resistant hematologic cancers. It is based on genetically modifying T cells transferred from the patient or a donor. Although its implementation has increased over the last few years, CAR-T has many challenges to be addressed, for instance, the associated severe toxicities, such as cytokine release syndrome. To model CAR-T cell dynamics, focusing on their proliferation and cytotoxic activity, we developed a mathematical framework using ordinary differential equations (ODEs) with Bayesian parameter estimation. Bayesian statistics were used to estimate model parameters through Monte Carlo integration, Bayesian inference, and Markov chain Monte Carlo (MCMC) methods. This paper explores MCMC methods, including the Metropolis–Hastings algorithm and DEMetropolis and DEMetropolisZ algorithms, which integrate differential evolution to enhance convergence rates. The theoretical findings and algorithms were validated using Python and Jupyter Notebooks. A real medical dataset of CAR-T cell therapy was analyzed, employing optimization algorithms to fit the mathematical model to the data, with the PyMC library facilitating Bayesian analysis. The results demonstrated that our model accurately captured the key dynamics of CAR-T cell therapy. This conclusion underscores the potential of parameter estimation to improve the understanding and effectiveness of CAR-T cell therapy in clinical settings. [ABSTRACT FROM AUTHOR]

Published

2024

10. Pembrolizumab induced type 1 diabetes mellitus in a patient with metastatic melanoma and literature review on steroids as a treatment option.

Author

Greene, Adina, Penner, Scott, Kunesh, Jacqueline, Altaf, Amal, McGrade, William, and Niu, Jiaxin

Subjects

*STEROID drugs, *INSULIN therapy, *THERAPEUTIC use of monoclonal antibodies, *TYPE 1 diabetes, *MELANOMA, *IMMUNOTHERAPY, *TREATMENT effectiveness, *MONOCLONAL antibodies, *METASTASIS, *IMMUNE checkpoint inhibitors

Abstract

Objective: We report a case of a 77-year-old male with metastatic melanoma who developed immune-checkpoint-inhibitor (ICI) induced type 1 diabetes mellitus (T1DM) after seven months of pembrolizumab treatment and required life-long insulin use. This prompted a literature review of best practice guidelines for long-term management of checkpoint-inhibitor induced T1DM including oral steroids as a treatment option similar to other ICI adverse effects. Data Sources and Summary: A literature search on PubMed was conducted to evaluate the efficacy of steroid treatment ICI-induced T1DM in any cancer type. Search terms consisted of "ipilimumab" OR "nivolumab" OR & "pembrolizumab" OR "immune checkpoint" AND "diabetes" OR "type 1 diabetes" AND "cancer" OR "melanoma" OR "carcinoma OR "sarcoma". Inclusion criteria were case reports published after 2015 in which the patient was diagnosed with ICI-induced T1DM or diabetic ketoacidosis where oral steroids were part of the treatment. Exclusion criteria included oral steroids not used as a treatment modality for T1DM, multiple endocrine comorbidities, no response recorded, and previous history of T1DM. 284 abstracts were found with these search terms of which 33 full-text articles were concluded to be eligible and screened and from which 8 records were included. From these 8 articles, there were 12 cases included. Conclusion: This literature search suggests that ICI-induced T1DM cannot be reversed by steroids and that insulin must be used permanently for treatment management. [ABSTRACT FROM AUTHOR]

Published

2024

11. The evolving landscape of tissue‐agnostic therapies in precision oncology.

Author

Subbiah, Vivek, Gouda, Mohamed A., Ryll, Bettina, Burris, Howard A., and Kurzrock, Razelle

Subjects

THERAPEUTIC use of antineoplastic agents, TUMOR genetics, GENOMICS, IMMUNOTHERAPY, IMMUNOGLOBULINS, TUMOR markers, ONCOLOGY, IMMUNE checkpoint inhibitors, TUMORS, INDIVIDUALIZED medicine, GENETIC mutation, GENETICS, CELL receptors

Abstract

Tumor‐agnostic therapies represent a paradigm shift in oncology by altering the traditional means of characterizing tumors based on their origin or location. Instead, they zero in on specific genetic anomalies responsible for fueling malignant growth. The watershed moment for tumor‐agnostic therapies arrived in 2017, with the US Food and Drug Administration's historic approval of pembrolizumab, an immune checkpoint inhibitor. This milestone marked the marriage of genomics and immunology fields, as an immunotherapeutic agent gained approval based on genomic biomarkers, specifically, microsatellite instability‐high or mismatch repair deficiency (dMMR). Subsequently, the approval of NTRK inhibitors, designed to combat NTRK gene fusions prevalent in various tumor types, including pediatric cancers and adult solid tumors, further underscored the potential of tumor‐agnostic therapies. The US Food and Drug Administration approvals of targeted therapies (BRAF V600E, RET fusion), immunotherapies (tumor mutational burden ≥10 mutations per megabase, dMMR) and an antibody‐drug conjugate (Her2‐positive–immunohistochemistry 3+ expression) with pan‐cancer efficacy have continued, offering newfound hope to patients grappling with advanced solid tumors that harbor particular biomarkers. In this comprehensive review, the authors delve into the expansive landscape of tissue‐agnostic targets and drugs, shedding light on the rationale underpinning this approach, the hurdles it faces, presently approved therapies, voices from the patient advocacy perspective, and the tantalizing prospects on the horizon. This is a welcome advance in oncology that transcends the boundaries of histology and location to provide personalized options. [ABSTRACT FROM AUTHOR]

Published

2024

12. A Comprehensive Revision of Radiation Immunotherapy and the Abscopal Effect in Central Nervous System Metastases: Reassessing the Frontier

Author

Júlia Moscardini-Martelli, Alejandro Rodríguez-Camacho, Jorge Alejandro Torres-Ríos, Juan Marcos Meraz-Soto, José Guillermo Flores-Vázquez, Laura Crystell Hernández-Sánchez, Francisco Javier Lozano-Ruiz, Federico Maldonado-Magos, Dharely Cid-Sánchez, Christian Haydeé Flores-Balcázar, Miguel Ángel Celis-López, Guillermo Axayacatl Gutiérrez-Aceves, Fabiola Flores-Vázquez, and Sergio Moreno-Jiménez

Subjects

abscopal effect, immunotherapy, radiotherapy, radiosurgery, oncology, metastasis, Biology (General), QH301-705.5

Abstract

Seventy years ago, Robin Mole introduced the concept of the abscopal effect to describe a rare phenomenon. This occurs when local radiation triggers an immune-mediated reduction in tumors outside the treated area but within the same organism. Observing this effect has been linked to improved overall and progression-free survival in patients who experience it. While the abscopal effect was once considered rare, it is now being observed more frequently due to the combination of radiation with immunotherapy. As a result, more researchers are exploring this study area, which shows promise for excellent results. This review focuses explicitly on the immunological implications of activating the abscopal effect through ionizing radiation in the central nervous system and explores the potentially involved immunological pathways.

Published

2024

13. The use of viruses in anti-cancer therapies – new achievements and challenges

Author

Małgorzata Grudnik, Katarzyna Grudnik, Maciej Słomian, Monika Prokurat, Karolina Lau, and Katarzyna Kryszczyszyn-Musialik

Subjects

oncolytic viruses, cancer, immunotherapy, oncology, medicine, Pharmacy and materia medica, RS1-441, Dentistry, RK1-715

Abstract

Viruses are gaining pivotal significance in innovative therapeutic strategies, underscoring their growing role in the field of oncology. The utilization of oncolytic viruses for the selective recognition and effective elimination of cancerous cells has captured the interest of scientists for many years. Due to the unique features of their application, such as greater patient comfort compared to the use of conventional therapies alone, a positive response of the body to treatment, and improved patient survival rates, virus-based therapies may become a pivotal pillar of modern oncology in future, particularly when integrated into combination therapies. It is assumed that further research into the specifics of viruses and their interactions will enable the development of more precise and effective immunotherapies targeted at cancers. However, considering the dynamic nature of these strategies, simultaneous rigorous monitoring of the potential hazards associated with virus application is imperative to ensure patient safety and further advancements in oncology. This review focuses on the analysis of virus application in cancer therapy and the emerging challenges related to clinical studies, placing particular emphasis on their specificity, versatility, and the direction in which modern forms of therapy are heading.

Published

2024

14. Therapeutic antibodies in oncology: an immunopharmacological overview.

Author

Toledo-Stuardo, Karen, Ribeiro, Carolina H., González-Herrera, Fabiola, Matthies, Douglas J., Le Roy, María Soledad, Dietz-Vargas, Claudio, Latorre, Yesenia, Campos, Ivo, Guerra, Yuneisy, Tello, Samantha, Vásquez-Sáez, Valeria, Novoa, Pedro, Fehring, Nicolás, González, Mauricio, Rodríguez-Siza, Jose, Vásquez, Gonzalo, Méndez, Pamela, Altamirano, Claudia, and Molina, María Carmen

Subjects

*ANTIBODY-dependent cell cytotoxicity, *IMMUNOGLOBULIN G, *IMMUNE response, *BIOTECHNOLOGY, *ANTIBODY-drug conjugates, *ONCOLOGY

Abstract

The biotechnological development of monoclonal antibodies and their immunotherapeutic use in oncology have grown exponentially in the last decade, becoming the first-line therapy for some types of cancer. Their mechanism of action is based on the ability to regulate the immune system or by interacting with targets that are either overexpressed in tumor cells, released into the extracellular milieu or involved in processes that favor tumor growth. In addition, the intrinsic characteristics of each subclass of antibodies provide specific effector functions against the tumor by activating antibody-dependent cellular cytotoxicity, complement-dependent cytotoxicity, and antibody-dependent cellular phagocytosis, among other mechanisms. The rational design and engineering of monoclonal antibodies have improved their pharmacokinetic and pharmacodynamic features, thus optimizing the therapeutic regimens administered to cancer patients and improving their clinical outcomes. The selection of the immunoglobulin G subclass, modifications to its crystallizable region (Fc), and conjugation of radioactive substances or antineoplastic drugs may all improve the antitumor effects of therapeutic antibodies. This review aims to provide insights into the immunological and pharmacological aspects of therapeutic antibodies used in oncology, with a rational approach at molecular modifications that can be introduced into these biological tools, improving their efficacy in the treatment of cancer. [ABSTRACT FROM AUTHOR]

Published

2024

15. Immunotherapy and liver cancer research trends and the 100 most cited articles: A bibliometric analysis.

Author

Kong, Yang, Wang, Yizhi, Yang, Qifan, and Ye, Song

Subjects

*BIBLIOMETRICS, *LIVER cancer, *ONCOLYTIC virotherapy, *LIVER analysis, *TUMOR microenvironment

Abstract

Bibliometric analysis of liver cancer research, particularly in immunotherapy, reveals crucial insights. The US leads in liver cancer mortality but ranks fifth globally. Scopus database analysis identified 2,349 papers, with the top 100 ranging from 127 to 4,959 citations. Notably, “Microenvironmental Regulation of Tumours Progression and Metastasis” in the Journal of Nature Medicine garnered the highest citations. Journals like the Journal of Hepatology, Hepatology, and Nature Reports Clinical Oncology contributed significantly. Understanding molecular mechanisms and prognostic indicators is paramount for advancing combination therapies.For better patient outcomes, research trends in liver cancer immunotherapy point to improved treatment protocols, knowledge of the tumor microenvironment, combining therapies, predicting disease course, international cooperation, sophisticated surgical techniques, early detection, oncolytic virotherapy, and patient-centered care. This research underscores immunotherapy’s pivotal role and encourages further exploration, offering valuable insights into liver cancer treatment trends. [ABSTRACT FROM AUTHOR]

Published

2024

16. Impact of fatigue on quality of life in oncology patients treated with immunotherapy.

Author

Olaru, Diana

Subjects

*FATIGUE (Physiology), *INFLAMMATION, *QUALITY of life, *LONGEVITY, *CANCER patients, *CANCER fatigue

Abstract

Fatigue is one of the most common side effects of immunotherapy, affecting 78-96% of patients. The mechanism is not fully understood, but may relate to the pro-inflammatory state induced by immunotherapy. Compared to chemotherapy, immunotherapy has less impact on quality of life and allows patients to maintain satisfactory quality of life for longer. However, fatigue can still significantly affect patients' physical capabilities and ability to participate in enjoyable activities. Guidelines recommend assessing fatigue and quality of life from diagnosis and throughout treatment. Multiple validated tools exist to measure fatigue objectively. Management approaches include both pharmacological and non-pharmacological methods. Exercise, particularly aerobic and yoga, appears to be one of the most effective non-pharmacological interventions for improving fatigue and quality of life. Overall, while immunotherapy-related fatigue impacts quality of life, it seems to do so to a lesser degree than other cancer treatments. More research is needed on optimal management strategies. [ABSTRACT FROM AUTHOR]

Published

2024

17. Toxicity-Induced Discontinuation of Immune Checkpoint Inhibitors in Metastatic Urothelial Cancer: 6-Year Experience from a Specialized Uro-Oncology Center.

Author

Rodler, Severin, Aydogdu, Can, Brinkmann, Isabel, Berg, Elena, Kopliku, Rega, Götz, Melanie, Ivanova, Troya, Tamalunas, Alexander, Schulz, Gerald B., Heinemann, Volker, Stief, Christian G., and Casuscelli, Jozefina

Subjects

*CANCER chemotherapy, *UROLOGY, *CANCER treatment, *DRUG toxicity, *COLITIS, *MEDICAL specialties & specialists, *DRUG side effects, *HEPATITIS, *URINARY organs, *TERMINATION of treatment, *MYCOPLASMA pneumoniae infections, *ONCOLOGY, *CANCER patients, *RETROSPECTIVE studies, *DISEASE remission, *IMMUNE checkpoint inhibitors, *MEDICAL records, *ACQUISITION of data, *GASTRITIS, *SPECIALTY hospitals, *IMMUNITY

Abstract

Simple Summary: This study analyzed patients with metastatic bladder cancer. A total of 108 patients received immunotherapy, but 11 had to stop their immunotherapy because of adverse events to the therapy. Despite stopping the therapy, the treatment effect could be seen for a longer time, and many patients did not have to start therapy again. This study helps us to understand what happens when patients have to stop immunotherapy due to adverse events and what to do next regarding cancer therapy for those patients. Immune checkpoint inhibitor (ICI) therapies have been established as the standard-of-care in various uro-oncological cancers. Immune-related adverse events (irAEs) are frequent, but their degree rarely leads to the discontinuation of immunotherapies. Unplanned permanent treatment discontinuation may negatively impact the outcomes of patients, but there are emerging data about a positive correlation between emergence of severe irAEs and therapeutic cancer responses. In this study, a retrospective analysis of patients treated for urothelial carcinoma (UC) with ICI-based immunotherapy was conducted. irAEs were classified according to the Common Terminology Criteria for Adverse Events (CTCAEs) and radiological responses according to the Response Evaluation Criteria In Solid Tumors (RECISTs). Out of 108 patients with metastatic urothelial cancer that underwent immunotherapy, 11 experienced a severe irAE that required permanent discontinuation of ICI therapy. The most frequent irAEs leading to discontinuation were hepatitis (n = 4), pneumonitis (n = 2), and gastritis or colitis (n = 2). Prior to discontinuation (R1), the radiological best response was complete remission (CR) in three patients, partial response (PR) in six, and stable disease (SD) in wo patients. After the discontinuation of ICI therapy (R2), the best responses were CR in six, PR in three, and SD in two patients. Following discontinuation, the majority of these patients showed a sustained treatment response, despite not receiving any cancer-specific treatment. The median time of response after discontinuation of ICI therapy was 26.0 (5.2–55.8) months. We propose accurate counseling and close follow-ups of patients following their discontinuation of ICI therapy due to irAEs, as responses can be durable and deep, and many patients do not require immediate subsequent therapies, even in urothelial cancer. More data are required to find predictors of the length of response to appropriately counsel patients. [ABSTRACT FROM AUTHOR]

Published

2024

18. Multi-Cohort Transcriptomic Profiling of Medical Gas Plasma-Treated Cancers Reveals the Role of Immunogenic Cell Death.

Author

Gkantaras, Antonios, Kotzamanidis, Charalampos, Kyriakidis, Konstantinos, Farmaki, Evangelia, Makedou, Kali, Tzimagiorgis, Georgios, Bekeschus, Sander, and Malousi, Andigoni

Subjects

*PROSTATE physiology, *COLD (Temperature), *RESEARCH funding, *PLASMA gases, *IMMUNOTHERAPY, *CELLULAR immunity, *OXIDATIVE stress, *DESCRIPTIVE statistics, *LONGITUDINAL method, *ATMOSPHERIC pressure, *CELL culture, *GENE expression profiling, *CELL death, *LUNG tumors, *TUMORS, *CYTOKINES, *INTERLEUKINS

Abstract

Simple Summary: Medical gas plasma is a new modality in cancer treatment showing favorable results in preclinical and clinical trials; however, the cascade of molecular events underlying selective killing of cancer cells has not been fully elucidated. This study examines the hypothesis that cell death induced by gas plasma is mediated by a universal molecular mechanism. Using high-throughput data from eight transcriptomic studies on patient-derived prostate cultures, melanoma, breast, lymphoma, and lung cancer cells, we implemented two computational methodologies for re-analysis of single cohorts as well as meta-analysis of multi-cohort gene expression data. The results provide converging insights into the induction of immunogenic cell death in human tumors, reinforcing the potential of plasma treatment as an emerging immunotherapeutic approach in oncology. The therapeutic potential of cold physical gas plasma operated at atmospheric pressure in oncology has been thoroughly demonstrated in numerous preclinical studies. The cytotoxic effect on malignant cells has been attributed mainly to biologically active plasma-generated compounds, namely, reactive oxygen and nitrogen species. The intracellular accumulation of reactive oxygen and nitrogen species interferes strongly with the antioxidant defense system of malignant cells, activating multiple signaling cascades and inevitably leading to oxidative stress-induced cell death. This study aims to determine whether plasma-induced cancer cell death operates through a universal molecular mechanism that is independent of the cancer cell type. Using whole transcriptome data, we sought to investigate the activation mechanism of plasma-treated samples in patient-derived prostate cell cultures, melanoma, breast, lymphoma, and lung cancer cells. The results from the standardized single-cohort gene expression analysis and parallel multi-cohort meta-analysis strongly indicate that plasma treatment globally induces cancer cell death through immune-mediated mechanisms, such as interleukin signaling, Toll-like receptor cascades, and MyD88 activation leading to pro-inflammatory cytokine release and tumor antigen presentation. [ABSTRACT FROM AUTHOR]

Published

2024

19. Assessing the Performance of Alternative Methods for Estimating Long-Term Survival Benefit of Immuno-oncology Therapies.

Author

Monnickendam, Giles

Subjects

*TECHNOLOGY assessment, *SURVIVAL analysis (Biometry), *SURVIVAL rate, *IMMUNE checkpoint inhibitors, *MEDICAL technology, *PARAMETRIC modeling, *EXTRAPOLATION

Abstract

This study aimed to determine the accuracy and consistency of established methods of extrapolating mean survival for immuno-oncology (IO) therapies, the extent of any systematic biases in estimating long-term clinical benefit, what influences the magnitude of any bias, and the potential implications for health technology assessment. A targeted literature search was conducted to identify published long-term follow-up from clinical trials of immune-checkpoint inhibitors. Earlier published results were identified and Kaplan-Meier estimates for short- and long-term follow-up were digitized and converted to pseudo–individual patient data using an established algorithm. Six standard parametric, 5 flexible parametric, and 2 mixture-cure models (MCMs) were used to extrapolate long-term survival. Mean and restricted mean survival time (RMST) were estimated and compared between short- and long-term follow-up. Predicted RMST from extrapolation of early data underestimated observed RMST in long-term follow-up for 184 of 271 extrapolations. All models except the MCMs frequently underestimated observed RMST. Mean survival estimates increased with longer follow-up in 196 of 270 extrapolations. The increase exceeded 20% in 122 extrapolations. Log-logistic and log-normal models showed the smallest change with additional follow-up. MCM performance varied substantially with functional form. Standard and flexible parametric models frequently underestimate mean survival for IO treatments. Log-logistic and log-normal models may be the most pragmatic and parsimonious solutions for estimating IO mean survival from immature data. Flexible parametric models may be preferred when the data used in health technology assessment are more mature. MCMs fitted to immature data produce unreliable results and are not recommended. • Treatment with immune-checkpoint inhibitors can result in a proportion of patients achieving durable response, generating a long tail to the survival distribution. Conventional extrapolation methods applied to short-term data may not perform well in estimating mean survival in these circumstances. • Both standard parametric and spline-based flexible parametric models (FPMs) tend to underestimate survival benefit for immuno-oncology therapies. Performance seems to worsen as the proportion of durable responders increases. More flexible models perform better than restrictive models, but with some risk of overfitting to short-term data. Mixture-cure models fitted to early data cuts produce unreliable results and may substantially overestimate mean survival. • Log-logistic and log-normal models may be the most pragmatic and parsimonious solutions for estimating mean survival from short-term data when the proportion of durable responders is expected to be low. FPMs using odds or normal scale may be better options when the data used in health technology assessment are more mature. When the expected proportion of durable responders is high, neither standard nor FPMs are expected to perform well and methods integrating external information should be considered. [ABSTRACT FROM AUTHOR]

Published

2024

20. Neurological autoimmunity in melanoma patients: a comparison between those exposed and non-exposed to immune checkpoint inhibitors.

Author

Vilaseca, Andreu, Farina, Antonio, Villagrán-García, Macarena, Pegat, Antoine, Benaiteau, Marie, Ciano-Petersen, Nicolás Lundahl, Do, Le-Duy, Rogemond, Véronique, Gonçalves, David, Psimaras, Dimitri, Birzu, Cristina, Honnorat, Jérôme, and Joubert, Bastien

Subjects

*PARANEOPLASTIC syndromes, *IMMUNE checkpoint inhibitors, *AUTOIMMUNE diseases, *IPILIMUMAB, *AUTOIMMUNITY, *CENTRAL nervous system, *MELANOMA, *NEUROLOGICAL disorders

Abstract

Background: The clinical spectrum of melanoma-associated neurological autoimmunity, whether melanoma-associated paraneoplastic neurological syndromes (PNS) or induced by immune checkpoint inhibitors (ICI), is not well characterized. We aim to describe the clinical spectrum of melanoma-associated neurological autoimmunity. Methods: A systematic review of the literature combined with patients from French databases of paraneoplastic neurological syndromes was conducted. All melanoma patients with a possible immune-mediated neurologic syndrome were included and classified according to whether they had previously been exposed to ICI (ICI-neurotoxicity) or not (ICI-naïve) at first neurological symptoms. Results: Seventy ICI-naïve (literature: n = 61) and 241 ICI-neurotoxicity patients (literature: n = 180) were identified. Neuromuscular manifestations predominated in both groups, but peripheral neuropathies were more frequent in ICI-neurotoxicity patients (39.4% vs 21.4%, p = 0.005) whereas myositis was more frequent in ICI-naïve patients (42.9% vs 18.7%, p < 0.001). ICI-naïve patients had also more frequent central nervous system (CNS) involvement (35.7% vs 23.7%, p = 0.045), classical paraneoplastic syndrome (25.7% vs 5.8%, p < 0.001), and more frequently positive for anti-neuron antibodies (24/32, 75.0% vs 38/90, 42.2%, p = 0.001). Although more ICI-neurotoxicity patients died during the acute phase (22/202, 10.9% vs 1/51, 2.0%, p = 0.047), mostly myositis patients (14/22, 63.6%), mortality during follow-up was higher in ICI-naïve patients (58.5% vs 29.8%, p < 0.001). There was no significant difference in the frequency of life independence (mRS ≤ 2) in the surviving patients in both groups (95.5% vs 91.0%, p = 0.437). Conclusions: Melanoma-associated PNS appear remarkably rare. The clinical similarities observed in neurological autoimmunity between ICI-treated and ICI-naïve patients, characterized predominantly by demyelinating polyradiculoneuropathy and myositis, suggest a potential prior immunization against melanoma antigens contributing to ICI-related neurotoxicity. [ABSTRACT FROM AUTHOR]

Published

2024

21. Associations between dermatologic immune-related adverse event morphologies and systemic immunomodulatory/immunosuppressive treatment: A large retrospective cohort study.

Author

Reardon, Rachel M., Perlman, Katherine L., Asdourian, Maria S., Shah, Nishi, Jacoby, Ted V., Thompson, Leah L., Reynolds, Kerry L., Semenov, Yevgeniy R., and Chen, Steven T.

Published

2024

22. Editorial: Application of multi-omics analysis in thoracic cancer immunotherapy

Author

Jindong Xie, Tingting Cai, Attila Szöllősi, Yuan Li, and Hailin Tang

Subjects

multi-omics, thoracic cancer, immunotherapy, oncology, tumor microenvironment, Immunologic diseases. Allergy, RC581-607

Published

2024

23. Stimuli‐Responsive Nanocarriers as Active Enhancers of Antitumoral Immunotherapy

Author

Jorge Parra‐Nieto, Iñigo Aguirre deCarcer, María Amor García del Cid, Sandra Jimenez‐Falcao, Javier Gónzalez‐Larre, and Alejandro Baeza

Subjects

drug release, immunotherapy, nanomedicine, oncology, stimuli‐responsive, Physics, QC1-999, Technology

Abstract

Abstract In recent years, the understanding of the role of the immune system in tumor progression and metastasis is paving the way for the development of antitumoral strategies based on the delivery of immunotherapeutic agents. The engineering of stimuli‐responsive nanocarriers able to release their payload in a controlled manner being able to boost potent and sustained immune responses against tumors has provided a powerful tool to eradicate tumors with extreme precision. Paramount advantages to trigger the immune system against tumors are the high selectivity and memory effect of immune response, which allows not only to eradicate primary and metastatic malignancies but also to avoid their relapse. In this review, the recent advances carried out in the development of smart nanocarriers for immunotherapy are presented.

Published

2024

24. The latest treatment of colorectal cancer - a review paper

Author

Anna Wojtkiewicz, Magda Piekarska, Zuzanna Kudas, Krzysztof Szerej, Mateusz Górka, and Weronika Stec

Subjects

colorectal cancer, immunotherapy, oncology, crc, latest treatment of colorectal cancer, nutrition in colorectal cancer, Sports, GV557-1198.995, Sports medicine, RC1200-1245

Abstract

The review article discusses the latest therapeutic approaches in the treatment of colorectal cancer (CRC), with a particular focus on metastatic disease. Despite advancements in standard treatments such as surgery, chemotherapy, and targeted therapies, the prognosis for patients with metastatic CRC remains poor, with five-year survival rates still low. The article examines the potential of immunotherapy, including PD-1 inhibitors like dostarlimab, which have shown promising results in treating selected patient groups. Additionally, the role of the ketogenic diet and probiotics as supportive strategies in CRC treatment is discussed, highlighting their potential to influence cancer metabolism and improve therapeutic outcomes. The article also addresses the development of nanotechnology-based therapies, such as PEGylated PLGA nanoparticles and sphingomyelin nanosystems, which may enhance drug delivery precision, thereby improving treatment efficacy and minimizing side effects. The conclusion emphasizes the need for further research into these innovative therapies and their integration with existing treatment protocols to improve survival and quality of life for CRC patients.

Published

2024

25. Immune Checkpoint Inhibitor Therapy for Kidney Transplant Recipients – A Review of Potential Complications and Management Strategies

Author

Elena Bianca Barbir, Samer Abdulmoneim, Arkadiusz Z. Dudek, and Aleksandra Kukla

Subjects

immunology, rejection risk, oncology, kidney transplant, biomarkers, immunotherapy, Specialties of internal medicine, RC581-951

Abstract

Immune checkpoint inhibitor (ICI) therapy has enabled a paradigm shift in Oncology, with the treatment of metastatic cancer in certain tumor types becoming akin to the treatment of chronic disease. Kidney transplant recipients (KTR) are at increased risk of developing cancer compared to the general population. Historically, KTR were excluded from ICI clinical trials due to concern for allograft rejection and decreased anti-tumor efficacy. While early post-marketing data revealed an allograft rejection risk of 40%–50%, 2 recent small prospective trials have demonstrated lower rates of rejection of 0%–12%, suggesting that maintenance immunosuppression modification prior to ICI start modulates rejection risk. Moreover, objective response rates induced by ICI for the treatment of advanced or metastatic skin cancer, the most common malignancy in KTR, have been comparable to those achieved by immune intact patients. Non-invasive biomarkers may have a role in risk-stratifying patients before starting ICI, and monitoring for rejection, though allograft biopsy is required to confirm diagnosis. This clinically focused review summarizes current knowledge on complications of ICI use in KTR, including their mechanism, risk mitigation strategies, non-invasive biomarker use, approaches to treatment of rejection, and suggestions for future directions in research.

Published

2024

26. Combining mathematical modeling, in vitro data and clinical target expression to support bispecific antibody binding affinity selection: a case example with FAP-4-1BBL

Author

Javier Sanchez, Christina Claus, Christine McIntyre, Tamara Tanos, Axel Boehnke, Lena E. Friberg, Siv Jönsson, and Nicolas Frances

Subjects

immunotherapy, bispecific antibody, modeling, simulation, binding affinity, oncology, Therapeutics. Pharmacology, RM1-950

Abstract

The majority of bispecific costimulatory antibodies in cancer immunotherapy are capable of exerting tumor-specific T-cell activation by simultaneously engaging both tumor-associated targets and costimulatory receptors expressed by T cells. The amount of trimeric complex formed when the bispecific antibody is bound simultaneously to the T cell receptor and the tumor-associated target follows a bell-shaped curve with increasing bispecific antibody exposure/dose. The shape of the curve is determined by the binding affinities of the bispecific antibody to its two targets and target expression. Here, using the case example of FAP-4-1BBL, a fibroblast activation protein alpha (FAP)-directed 4-1BB (CD137) costimulator, the impact of FAP-binding affinity on trimeric complex formation and pharmacology was explored using mathematical modeling and simulation. We quantified (1) the minimum number of target receptors per cell required to achieve pharmacological effect, (2) the expected coverage of the patient population for 19 different solid tumor indications, and (3) the range of pharmacologically active exposures as a function of FAP-binding affinity. A 10-fold increase in FAP-binding affinity (from a dissociation constant [KD] of 0.7 nM–0.07 nM) was predicted to reduce the number of FAP receptors needed to achieve 90% of the maximum pharmacological effect from 13,400 to 4,000. Also, the number of patients with colon cancer that would achieve 90% of the maximum effect would increase from 6% to 39%. In this work, a workflow to select binding affinities for bispecific antibodies that integrates preclinical in vitro data, mathematical modeling and simulation, and knowledge on target expression in the patient population, is provided. The early implementation of this approach can increase the probability of success with cancer immunotherapy in clinical development.

Published

2024

27. Molecular Therapy: Oncology

Subjects

cancer biology, immunotherapy, cancer, oncology, molecular therapy, gene therapy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Published

2024

28. Editorial: Application of multi-omics analysis in thoracic cancer immunotherapy.

Author

Xie, Jindong, Cai, Tingting, Szöllősi, Attila, Li, Yuan, and Tang, Hailin

Published

2024

29. Molecular Markers in Melanoma Progression: A Study on the Expression of miRNA Gene Subtypes in Tumoral vs. Benign Nevi

Author

Mihaela Prodan, Sergiu Costescu, Ahmed Elagez, Sorina Maria Denisa Laitin, Vlad Bloanca, Zorin Crainiceanu, Edward Seclaman, Ana-Olivia Toma, Roxana Manuela Fericean, George Puenea, and Gabriel Veniamin Cozma

Subjects

melanoma, microRNA, immunotherapy, biomarkers, oncology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

This study investigates the differential expression of miRNA gene subtypes in tumoral versus benign nevi in individuals with melanoma, aiming to identify clinically significant correlations that could serve as reliable markers for assessing tumor stage and progression. Conducted between 2019 and 2022, this descriptive, quantitative observational research analyzed 90 formalin-fixed paraffin-embedded (FFPE) samples from the Pius Brinzeu County Emergency Clinical Hospital, Timisoara, including 45 samples of advanced-stage melanoma and 45 samples of pigmented nevi. miRNA purification and analysis were performed using the miRNeasy Kit and the Human Cancer PathwayFinder miScript miRNA PCR Array, with statistical analysis (including logistic regression) to determine associations with cancer staging, such as high Breslow index risk, number of mitoses, and vascular invasion. After the analysis and comparison of 180 miRNA gene subtypes, we selected 10 of the most upregulated and 10 most downregulated genes. The results revealed that hsa-miR-133b, hsa-miR-335-5p, hsa-miR-200a-3p, and hsa-miR-885-5p were significantly upregulated in melanoma samples, with fold changes ranging from 1.09 to 1.12. Conversely, hsa-miR-451a and hsa-miR-29b-3p showed notable downregulation in melanoma, with fold changes of 0.90 and 0.92, respectively. Additionally, logistic regression analysis identified hsa-miR-29b-3p (OR = 2.51) and hsa-miR-200a-3p (OR = 2.10) as significantly associated with an increased risk of a high Breslow index, while hsa-miR-127-3p and hsa-miR-451a were associated with a reduced risk. Conclusively, this study underscores the significant alterations in miRNA expression in melanoma compared to benign nevi and highlights the potential of specific miRNAs as biomarkers for melanoma progression. The identification of miRNAs with significant associations to melanoma characteristics suggests their utility in developing non-invasive, cost-effective diagnostic tools and in guiding therapeutic decisions, potentially improving patient outcomes in melanoma management.

Published

2024

30. A Review of the Current Approach and Treatment Landscape for Stage III Non-Small Cell Lung Cancer.

Author

Sridhar, Arthi, Khan, Hina, Yohannan, Binoy, Chan, Kok Hoe, Kataria, Nilansh, and Jafri, Syed Hasan

Subjects

*NON-small-cell lung carcinoma, *DISEASE management

Abstract

The therapeutic landscape of the management of stage III non-small cell lung cancer (NSCLC) has drastically evolved with the incorporation of immunotherapy and targeted therapy. Stage III NSCLC accounts for one-third of the cases and the treatment strategy of these locally advanced presentations are diverse, ranging from surgical to non-surgical options; with the incorporation of chemo-immunotherapy, radiation, and targeted therapies wherever applicable. The staging of this disease has also changed, and it is essential to have a strong multidisciplinary approach to do justice to patient care. In this article, we aim to navigate the nuanced approaches in the diagnosis and treatment of stage III NSCLC and expand on the evolution of the management of this disease. [ABSTRACT FROM AUTHOR]

Published

2024

31. Molecular Markers in Melanoma Progression: A Study on the Expression of miRNA Gene Subtypes in Tumoral vs. Benign Nevi.

Author

Prodan, Mihaela, Costescu, Sergiu, Elagez, Ahmed, Laitin, Sorina Maria Denisa, Bloanca, Vlad, Crainiceanu, Zorin, Seclaman, Edward, Toma, Ana-Olivia, Fericean, Roxana Manuela, Puenea, George, and Cozma, Gabriel Veniamin

Subjects

*GENE expression, *MELANOMA, *LOGISTIC regression analysis, *NEVUS, *TUMOR classification

Abstract

This study investigates the differential expression of miRNA gene subtypes in tumoral versus benign nevi in individuals with melanoma, aiming to identify clinically significant correlations that could serve as reliable markers for assessing tumor stage and progression. Conducted between 2019 and 2022, this descriptive, quantitative observational research analyzed 90 formalin-fixed paraffin-embedded (FFPE) samples from the Pius Brinzeu County Emergency Clinical Hospital, Timisoara, including 45 samples of advanced-stage melanoma and 45 samples of pigmented nevi. miRNA purification and analysis were performed using the miRNeasy Kit and the Human Cancer PathwayFinder miScript miRNA PCR Array, with statistical analysis (including logistic regression) to determine associations with cancer staging, such as high Breslow index risk, number of mitoses, and vascular invasion. After the analysis and comparison of 180 miRNA gene subtypes, we selected 10 of the most upregulated and 10 most downregulated genes. The results revealed that hsa-miR-133b, hsa-miR-335-5p, hsa-miR-200a-3p, and hsa-miR-885-5p were significantly upregulated in melanoma samples, with fold changes ranging from 1.09 to 1.12. Conversely, hsa-miR-451a and hsa-miR-29b-3p showed notable downregulation in melanoma, with fold changes of 0.90 and 0.92, respectively. Additionally, logistic regression analysis identified hsa-miR-29b-3p (OR = 2.51) and hsa-miR-200a-3p (OR = 2.10) as significantly associated with an increased risk of a high Breslow index, while hsa-miR-127-3p and hsa-miR-451a were associated with a reduced risk. Conclusively, this study underscores the significant alterations in miRNA expression in melanoma compared to benign nevi and highlights the potential of specific miRNAs as biomarkers for melanoma progression. The identification of miRNAs with significant associations to melanoma characteristics suggests their utility in developing non-invasive, cost-effective diagnostic tools and in guiding therapeutic decisions, potentially improving patient outcomes in melanoma management. [ABSTRACT FROM AUTHOR]

Published

2024

32. 2024 Trending Now in Cancer Care: Part 1.

Author

Marino, Monique J. and Radwan, Rachel

Subjects

TUMOR prevention, CANCER treatment, COMMUNITY support, PSYCHOLOGICAL resilience, EMPLOYEE retention, EMPLOYEE orientation, INTERPROFESSIONAL relations, T cells, MEDICAL personnel, PSYCHOLOGICAL burnout, SOCIAL determinants of health, MENTAL health, CANCER patient medical care, MEDICAL care, IMMUNOTHERAPY, PRIMARY health care, WORK environment, LGBTQ+ people, CONFERENCES & conventions, ONCOLOGY, JOB satisfaction, PATIENT-centered care, EMPLOYEE recruitment, LABOR demand, CLINICAL competence, CONTINUING education, HEALTH education, CANCER patient psychology, ADVERSE health care events, SPECIALTY hospitals, COVID-19 pandemic, CELL receptors, PATIENT participation, COMMUNITY-based social services, LABOR supply, PSYCHOSOCIAL factors, SEXUAL health

Published

2024

33. Comparison of Large Language Models in Answering Immuno-Oncology Questions: A Cross-Sectional Study.

Author

Iannantuono, Giovanni Maria, Bracken-Clarke, Dara, Karzai, Fatima, Choo-Wosoba, Hyoyoung, Gulley, James L, and Floudas, Charalampos S

Subjects

ARTIFICIAL intelligence tests, LANGUAGE & languages, CROSS-sectional method, RESEARCH funding, PHILOSOPHY of education, IMMUNOTHERAPY, MEDICAL coding software, FISHER exact test, SAMPLE size (Statistics), RESEARCH evaluation, READABILITY (Literary style), ONCOLOGY, CANCER patients, EDUCATIONAL tests & measurements, DESCRIPTIVE statistics, COMPARATIVE studies, DATA analysis software

Abstract

Background The capability of large language models (LLMs) to understand and generate human-readable text has prompted the investigation of their potential as educational and management tools for patients with cancer and healthcare providers. Materials and Methods We conducted a cross-sectional study aimed at evaluating the ability of ChatGPT-4, ChatGPT-3.5, and Google Bard to answer questions related to 4 domains of immuno-oncology (Mechanisms, Indications, Toxicities, and Prognosis). We generated 60 open-ended questions (15 for each section). Questions were manually submitted to LLMs, and responses were collected on June 30, 2023. Two reviewers evaluated the answers independently. Results ChatGPT-4 and ChatGPT-3.5 answered all questions, whereas Google Bard answered only 53.3% (P  < .0001). The number of questions with reproducible answers was higher for ChatGPT-4 (95%) and ChatGPT3.5 (88.3%) than for Google Bard (50%) (P  < .0001). In terms of accuracy, the number of answers deemed fully correct were 75.4%, 58.5%, and 43.8% for ChatGPT-4, ChatGPT-3.5, and Google Bard, respectively (P  = .03). Furthermore, the number of responses deemed highly relevant was 71.9%, 77.4%, and 43.8% for ChatGPT-4, ChatGPT-3.5, and Google Bard, respectively (P  = .04). Regarding readability, the number of highly readable was higher for ChatGPT-4 and ChatGPT-3.5 (98.1%) and (100%) compared to Google Bard (87.5%) (P  = .02). Conclusion ChatGPT-4 and ChatGPT-3.5 are potentially powerful tools in immuno-oncology, whereas Google Bard demonstrated relatively poorer performance. However, the risk of inaccuracy or incompleteness in the responses was evident in all 3 LLMs, highlighting the importance of expert-driven verification of the outputs returned by these technologies. [ABSTRACT FROM AUTHOR]

Published

2024

34. Harnessing the cGAS-STING pathway to potentiate radiation therapy: current approaches and future directions.

Author

Colangelo, Nicholas W., Gerber, Naamit K., Vatner, Ralph E., and Cooper, Benjamin T.

Subjects

RADIOTHERAPY, IONIZING radiation, NUCLEAR DNA, MITOCHONDRIAL DNA, TUMOR microenvironment

Abstract

In this review, we cover the current understanding of how radiation therapy, which uses ionizing radiation to kill cancer cells, mediates an anti-tumor immune response through the cGAS-STING pathway, and how STING agonists might potentiate this. We examine how cGAS-STING signaling mediates the release of inflammatory cytokines in response to nuclear and mitochondrial DNA entering the cytoplasm. The significance of this in the context of cancer is explored, such as in response to cell-damaging therapies and genomic instability. The contribution of the immune and non-immune cells in the tumor microenvironment is considered. This review also discusses the burgeoning understanding of STING signaling that is independent of inflammatory cytokine release and the various mechanisms by which cancer cells can evade STING signaling. We review the available data on how ionizing radiation stimulates cGAS-STING signaling as well as how STING agonists may potentiate the anti-tumor immune response induced by ionizing radiation. There is also discussion of how novel radiation modalities may affect cGASSTING signaling. We conclude with a discussion of ongoing and planned clinical trials combining radiation therapy with STING agonists, and provide insights to consider when planning future clinical trials combining these treatments. [ABSTRACT FROM AUTHOR]

Published

2024

35. Drug Cost Avoidance Resulting from Participation in Clinical Trials: A 10-Year Retrospective Analysis of Cancer Patients with Solid Tumors.

Author

Carreras, Maria-Josep, Renedo-Miró, Berta, Valdivia, Carolina, Tomás-Guillén, Elena, Farriols, Anna, Mañós, Laura, Vidal, Jana, Alcalde, María, De la Paz, Isabel, Jiménez-Lozano, Inés, Palacio-Lacambra, Maria-Eugenia, Sabaté, Nuria, Felip, Enriqueta, Garralda, Elena, Garau, Margarita, Gorgas, Maria-Queralt, Monterde, Josep, and Tabernero, Josep

Subjects

*THERAPEUTIC use of antineoplastic agents, *COST control, *CLINICAL trials, *IMMUNOTHERAPY, *TERTIARY care, *RETROSPECTIVE studies, *ONCOLOGY, *DESCRIPTIVE statistics, *TUMORS, *CANCER patient psychology, *MEDICAL care costs

Abstract

Simple Summary: In the present framework of constraints on healthcare budgets, an assessment of costs of antineoplastic drugs is a crucial step in contributing to the sustainability of public-payer systems. This study evaluated the characteristics of cancer clinical trials and potential drug cost avoidance in a large population of adult cancer patients with solid tumors enrolled in clinical trials over a 10-year period (2010–2019). These trials were conducted at the Medical Oncology Department of Vall d'Hebron University Hospital in Barcelona (Spain), one of the largest tertiary care centers in the country. Based on the data of 2930 clinical trials with 10,488 participants, it was found that the total cost of antineoplastic drugs supplied by sponsors in the clinical trials setting was EUR 107,306,084, with a potential cost savings of EUR 92,662,609. Participation in sponsored clinical trials in which drugs are provided free of charge yields considerable cost savings, with benefits in clinical strategies to reduce drug expenditures. The objective of this single-center retrospective study was to describe the clinical characteristics of adult patients with solid tumors enrolled in cancer clinical trials over a 10-year period (2010–2019) and to assess drug cost avoidance (DCA) associated with sponsors' contributions. The sponsors' contribution to pharmaceutical expenditure was calculated according to the actual price (for each year) of pharmaceutical specialties that the Vall d'Hebron University Hospital (HUVH) would have had to bear in the absence of sponsorship. A total of 2930 clinical trials were conducted with 10,488 participants. There were 140 trials in 2010 and 459 in 2019 (228% increase). Clinical trials of high complexity phase I and basket trials accounted for 34.3% of all trials. There has been a large variation in the pattern of clinical research over the study period, whereas, in 2010, targeted therapy accounted for 79.4% of expenditure and cytotoxic drugs for 20.6%; in 2019, immunotherapy accounted for 68.4%, targeted therapy for 24.4%, and cytotoxic drugs for only 7.1%. A total of four hundred twenty-one different antineoplastic agents were used, the variability of which increased from forty-seven agents in 2010, with only seven of them accounting for 92.8% of the overall pharmaceutical expenditure) to three hundred seventeen different antineoplastic agents in 2019, with thirty-three of them accounting for 90.6% of the overall expenditure. The overall expenditure on antineoplastic drugs in clinical care patients not included in clinical trials was EUR 120,396,096. The total cost of antineoplastic drugs supplied by sponsors in a clinical trial setting was EUR 107,306,084, with a potential DCA of EUR 92,662,609. Overall, clinical trials provide not only the best context for the progress of clinical research and healthcare but also create opportunities for reducing cancer care costs. [ABSTRACT FROM AUTHOR]

Published

2024

36. Analysis of physical and biological delivery systems for DNA cancer vaccines and their translation to clinical development.

Author

Oelkrug, Christopher

Subjects

*DNA vaccines, *CANCER vaccines, *BIOLOGICAL systems, *IMMUNOLOGIC memory, *VACCINES, *CD8 antigen

Abstract

DNA cancer vaccines as an approach in tumor immunotherapy are still being investigated in preclinical and clinical settings. Nevertheless, only a small number of clinical studies have been published so far and are still active. The investigated vaccines show a relatively stable expression in in-vitro transfected cells and may be favorable for developing an immunologic memory in patients. Therefore, DNA vaccines could be suitable as a prophylactic or therapeutic approach against cancer. Due to the low efficiency of these vaccines, the administration technique plays an important role in the vaccine design and its efficacy. These DNA cancer vaccine delivery systems include physical, biological, and non-biological techniques. Although the pre-clinical studies show promising results in the application of the different delivery systems, further studies in clinical trials have not yet been successfully proven. [ABSTRACT FROM AUTHOR]

Published

2024

37. Therapeutically targeting the unique disease landscape of pediatric high-grade gliomas.

Author

Fernando, Dasun, Ahmed, Afsar U., and Williams, Bryan R. G.

Subjects

CENTRAL nervous system tumors, GLIOMAS, YOUNG adults, CENTRAL nervous system, OVERALL survival, DISEASE management

Abstract

Pediatric high-grade gliomas (pHGG) are a rare yet devastating malignancy of the central nervous system's glial support cells, affecting children, adolescents, and young adults. Tumors of the central nervous system account for the leading cause of pediatric mortality of which high-grade gliomas present a significantly grim prognosis. While the past few decades have seen many pediatric cancers experiencing significant improvements in overall survival, the prospect of survival for patients diagnosed with pHGGs has conversely remained unchanged. This can be attributed in part to tumor heterogeneity and the existence of the bloodbrain barrier. Advances in discovery research have substantiated the existence of unique subgroups of pHGGs displaying alternate responses to different therapeutics and varying degrees of overall survival. This highlights a necessity to approach discovery research and clinical management of the disease in an alternative subtype-dependent manner. This review covers traditional approaches to the therapeutic management of pHGGs, limitations of such methods and emerging alternatives. Novel mutations which predominate the pHGG landscape are highlighted and the therapeutic potential of targeting them in a subtype specific manner discussed. Collectively, this provides an insight into issues in need of transformative progress which arise during the management of pHGGs. [ABSTRACT FROM AUTHOR]

Published

2024

38. Safety and Efficacy of IL-12 Plasmid DNA Transfection into Pig Skin: Supportive Data for Human Clinical Trials on Gene Therapy and Vaccination.

Author

Lampreht Tratar, Ursa, Jesenko, Tanja, Omerzel, Masa, Seliskar, Alenka, Stupan, Urban, Djokic, Mihajlo, Sredensek, Jerneja, Trotovsek, Blaz, Sersa, Gregor, and Cemazar, Maja

Subjects

*GENE therapy, *CLINICAL trials, *DNA vaccines, *GENE transfection, *SWINE, *GENETIC transformation, *BLOOD testing

Abstract

Gene electrotransfer (GET) of plasmids encoding interleukin 12 (IL-12) has already been used for the treatment of various types of tumors in human oncology and as an adjuvant in DNA vaccines. In recent years, we have developed a plasmid encoding human IL-12 (phIL12) that is currently in a phase I clinical study. The aim was to confirm the results of a non-clinical study in mice on pharmacokinetic characteristics and safety in a porcine model that better resembled human skin. The GET of phIL12 in the skin was performed on nine pigs using different concentrations of plasmid phIL12 and invasive (needle) or noninvasive (plate) types of electrodes. The results of our study demonstrate that the GET of phIL-12 with needle electrodes induced the highest expression of IL-12 at the protein level on day 7 after the procedure. The plasmid was distributed to all tested organs; however, its amount decreased over time and was at a minimum 28 days after GET. Based on plasmid copy number and expression results, together with blood analysis, we showed that IL-12 GET is safe in a porcine animal model. Furthermore, we demonstrated that pigs are a valuable model for human gene therapy safety studies. [ABSTRACT FROM AUTHOR]

Published

2024

39. Regulating diagnosis—Molecular and regulatory sub‐stratifications of lung cancer treatment.

Author

Hauge, Amalie Martinus

Subjects

*TREATMENT of lung tumors, *HEALTH services accessibility, *MEDICAL care use, *IMMUNOTHERAPY, *LUNG tumors, *ACQUISITION of data, *SOCIOLOGY, *INDIVIDUALIZED medicine, *MOLECULAR diagnosis, *MEDICAL care costs

Abstract

The sociology of diagnosis has shown that diagnosis not only serves to label the underlying cause of disease but also to provide access to services and resources. Elaborating on this double‐affordance of diagnosis, this article examines how precision medicine reconfigures diagnosis as a label and as a process in regulatory and clinical settings. Reporting from an ethnographic case study of the introduction of immunotherapy for lung cancer, the paper unfolds the uncertainties involved in dissecting diagnosis into layers and examines the efforts and negotiations it takes to enable these layers to work both as clinical entities and regulative entities with the purpose of delineating access to treatment. I suggest that the work of subdividing diseases into molecularly defined categories for the purpose of delineating treatment‐eligible populations can be labelled 'diagnostic sub‐stratification' and argue that it is pertinent to understand the political capacity of this strategy. Diagnostic sub‐stratification involves a push of diagnosis from the clinic 'up' into the regulatory system and 'out' into the laboratories, obscuring who is accountable for the diagnostic categories employed to define patients' treatment access. [ABSTRACT FROM AUTHOR]

Published

2024

40. CD24 blockade promotes anti‐tumor immunity in oral squamous cell carcinoma.

Author

Zou, Ke‐Long, Lan, Zhou, Cui, Hao, Zhao, Yu‐Yue, Wang, Wei‐Ming, and Yu, Guang‐Tao

Subjects

*FLOW cytometry, *MOUTH tumors, *HOMOGRAFTS, *IN vivo studies, *ANIMAL experimentation, *IMMUNOHISTOCHEMISTRY, *WESTERN immunoblotting, *ANTINEOPLASTIC agents, *MACROPHAGES, *IMMUNITY, *CELL proliferation, *RESEARCH funding, *MEMBRANE proteins, *ANTIGENS, *SQUAMOUS cell carcinoma, *MICE

Abstract

Objectives: Our study elucidates the prognostic role of cluster of differentiation (CD) 24 expression in oral squamous cell carcinoma (OSCC) and determines whether targeting CD24 enhances the anti‐tumor immune response by inhibiting tumor‐associated macrophages (TAMs). Materials and Methods: The expression of CD24 and CD68 was analyzed immunohistochemically via tissue microarrays constructed using 56 cohorts of patients with OSCC and 20 control specimens. Further, CD24 was inhibited in an allograft squamous cell carcinoma (SCC) related mouse model with CD24mAb to determine the tumor volume and weight. Changes in immune cells such as TAMs and T cells in the tumor microenvironment (TME) were analyzed by Flow cytometry. The expression of CD4, CD8, and Ki67 was analyzed via immunohistochemistry. The inhibition of CD24 was confirmed by Western blot and immunohistochemistry. Results: CD24 was overexpressed in OSCC. High expression of CD24 indicated poor survival in patients with OSCC (p = 0.0334). CD24 expression was significantly correlated with CD68 (p = 0.0424). The inhibition of CD24 delayed tumor growth in vivo. A decrease in TAMs number and an increase in T cell number were confirmed, while the ability of tumor proliferation was impaired. Conclusion: Targeting CD24 could enhance anti‐tumor immune response by inhibiting TAMs. [ABSTRACT FROM AUTHOR]

Published

2024

41. Use of a topical Janus kinase inhibitor in immune checkpoint inhibitor-induced eczematous reaction: a case report.

Author

Powers, Camille M., Verma, Hannah, Orloff, Jeremy, Piontkowski, Austin J., Tiersten, Amy, Lamb, Angela, and Gulati, Nicholas

Subjects

*IMMUNE checkpoint inhibitors, *KINASE inhibitors, *ATOPIC dermatitis, *RUXOLITINIB, *CANCER treatment

Abstract

In this report, we describe the case of a 28-year-old female with bilateral breast cancer in the setting of a BRCA1 mutation, who presented to dermatology with an eczematous reaction, ultimately diagnosed as a cutaneous immune-related adverse event (cirAE) secondary to an immune checkpoint inhibitor (ICI), pembrolizumab. Our case report highlights a novel therapeutic option for an eczematous cirAE: the topical JAK 1/2 inhibitor, ruxolitinib. CirAEs can occur in up to 55% of patients on ICIs, a class of medications seeing rapidly increasing use in cancer therapy, and prior research has demonstrated that ICI-induced dermatitis may involve different pathways than traditionally observed in their spontaneous counterparts. Specifically, marked Th1 skewing is noted in ICI-induced dermatitis, as opposed to a predominant Th2 response which typically characterizes spontaneous atopic dermatitis. To our knowledge, this is the first case report in the literature discussing use of a topical JAK inhibitor, ruxolitinib, in the treatment of topical steroid-refractory cirAEs. Furthermore, as topical JAK inhibitors are thought to not carry the risks of systemic JAK inhibitors, including malignancy, ruxolitinib cream is a promising therapeutic option for this challenging patient population. [ABSTRACT FROM AUTHOR]

Published

2024

42. ESMO Gastrointestinal Oncology

Subjects

oncology, gastrointestinal cancers, cancer diagnostics, immunotherapy, epidemiology, cancer prevention, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Published

2024

43. A case of biopsy‐proven acute interstitial nephritis following atezolizumab‐bevacizumab treatment of advanced unresectable hepatocellular carcinoma

Author

Reema Patel, Omar Elghawy, Amanda Gibbs, Srishti Gupta, and Varinder Kaur

Subjects

atezolizumab, hepatocellular carcinoma, immune related adverse event, immunotherapy, oncology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background The advent of immune checkpoint inhibitors (ICIs) represented a significant breakthrough in cancer therapy. Recently, the combined use of atezolizumab and bevacizumab was approved as first‐line treatment for unresectable hepatocellular carcinoma (HCC). Exposure to a novel and diverse spectrum of immune‐related adverse events (irAEs) has increased with the growing utilization of ICIs, however, a comprehensive understanding surrounding newer agents is still lacking. The incidence of kidney toxicities is rare but rising, often underreported due to the lack of confirmatory biopsies. Here, we present a rare case of biopsy‐proven acute interstitial nephritis (AIN) following atezolizumab‐bevacizumab treatment of advanced unresectable HCC. Case An 84‐year‐old male with T4N0M0 hepatocellular carcinoma was admitted after cycle 5 of atezolizumab due to decreased urine output and dysuria with a serum creatine of 4.7 mg/dL compared to a baseline of 1.3 mg/dL. To confirm the diagnosis of possible intrinsic renal injury, an ultrasound‐guided non‐focal biopsy of the left kidney was performed, revealing AIN. Potential exacerbatory medications, such as proton‐pump inhibitors, were discontinued. The patient was discharged on oral steroids with improvement in serum creatinine. Before completing the steroid taper, the patient developed pneumocystis pneumonia and eventually transitioned to hospice care. Conclusion This case highlights the valuable role renal biopsy can play in accurately capturing irAEs and guiding appropriate management in the setting of ICI‐induced AKI. It also exemplifies important considerations for steroid treatment of irAEs in the setting of comorbidities, such as diabetes.

Published

2024

44. CBFA2T3-GLIS2 model of pediatric acute megakaryoblastic leukemia identifies FOLR1 as a CAR T cell target

Author

Le, Quy, Hadland, Brandon, Smith, Jenny L, Leonti, Amanda, Huang, Benjamin J, Ries, Rhonda, Hylkema, Tiffany A, Castro, Sommer, Tang, Thao T, McKay, Cyd N, Perkins, LaKeisha, Pardo, Laura, Sarthy, Jay, Beckman, Amy K, Williams, Robin, Idemmili, Rhonda, Furlan, Scott, Ishida, Takashi, Call, Lindsey, Srivastava, Shivani, Loeb, Anisha M, Milano, Filippo, Imren, Suzan, Morris, Shelli M, Pakiam, Fiona, Olson, James M, Loken, Michael R, Brodersen, Lisa Eidenschink, Riddell, Stanley R, Tarlock, Katherine, Bernstein, Irwin D, Loeb, Keith R, and Meshinchi, Soheil

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Pediatric Research Initiative, Pediatric, Cancer, Genetics, Pediatric Cancer, Stem Cell Research, Stem Cell Research - Nonembryonic - Human, Stem Cell Research - Nonembryonic - Non-Human, Biotechnology, Hematology, Rare Diseases, Childhood Leukemia, Orphan Drug, 2.1 Biological and endogenous factors, Aetiology, Animals, Child, Child, Preschool, Humans, Infant, Disease Models, Animal, Folate Receptor 1, Immunotherapy, Adoptive, Leukemia, Megakaryoblastic, Acute, Oncogene Proteins, Fusion, T-Lymphocytes, Transcriptome, Xenograft Model Antitumor Assays, Cancer immunotherapy, Leukemias, Oncogenes, Oncology, Therapeutics, Medical and Health Sciences, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

The CBFA2T3-GLIS2 (C/G) fusion is a product of a cryptic translocation primarily seen in infants and early childhood and is associated with dismal outcome. Here, we demonstrate that the expression of the C/G oncogenic fusion protein promotes the transformation of human cord blood hematopoietic stem and progenitor cells (CB HSPCs) in an endothelial cell coculture system that recapitulates the transcriptome, morphology, and immunophenotype of C/G acute myeloid leukemia (AML) and induces highly aggressive leukemia in xenograft models. Interrogating the transcriptome of C/G-CB cells and primary C/G AML identified a library of C/G-fusion-specific genes that are potential targets for therapy. We developed chimeric antigen receptor (CAR) T cells directed against one of the targets, folate receptor α (FOLR1), and demonstrated their preclinical efficacy against C/G AML using in vitro and xenograft models. FOLR1 is also expressed in renal and pulmonary epithelium, raising concerns for toxicity that must be addressed for the clinical application of this therapy. Our findings underscore the role of the endothelial niche in promoting leukemic transformation of C/G-transduced CB HSPCs. Furthermore, this work has broad implications for studies of leukemogenesis applicable to a variety of oncogenic fusion-driven pediatric leukemias, providing a robust and tractable model system to characterize the molecular mechanisms of leukemogenesis and identify biomarkers for disease diagnosis and targets for therapy.

Published

2022

45. Acidosis-mediated increase in IFN-γ-induced PD-L1 expression on cancer cells as an immune escape mechanism in solid tumors

Author

Philipp Knopf, Dimitri Stowbur, Sabrina H. L. Hoffmann, Natalie Hermann, Andreas Maurer, Valentina Bucher, Marilena Poxleitner, Bredi Tako, Dominik Sonanini, Balaji Krishnamachary, Sanhita Sinharay, Birgit Fehrenbacher, Irene Gonzalez-Menendez, Felix Reckmann, David Bomze, Lukas Flatz, Daniela Kramer, Martin Schaller, Stephan Forchhammer, Zaver M. Bhujwalla, Leticia Quintanilla-Martinez, Klaus Schulze-Osthoff, Mark D. Pagel, Marieke F. Fransen, Martin Röcken, André F. Martins, Bernd J. Pichler, Kamran Ghoreschi, and Manfred Kneilling

Subjects

Modulators of tumor microenvironment, Immune checkpoint inhibitors, Drug resistance mechanisms in immunotherapy, pH modulation of the tumor microenvironment, Immunotherapy, Oncology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Immune checkpoint inhibitors have revolutionized cancer therapy, yet the efficacy of these treatments is often limited by the heterogeneous and hypoxic tumor microenvironment (TME) of solid tumors. In the TME, programmed death-ligand 1 (PD-L1) expression on cancer cells is mainly regulated by Interferon-gamma (IFN-γ), which induces T cell exhaustion and enables tumor immune evasion. In this study, we demonstrate that acidosis, a common characteristic of solid tumors, significantly increases IFN-γ-induced PD-L1 expression on aggressive cancer cells, thus promoting immune escape. Using preclinical models, we found that acidosis enhances the genomic expression and phosphorylation of signal transducer and activator of transcription 1 (STAT1), and the translation of STAT1 mRNA by eukaryotic initiation factor 4F (elF4F), resulting in an increased PD-L1 expression. We observed this effect in murine and human anti-PD-L1-responsive tumor cell lines, but not in anti-PD-L1-nonresponsive tumor cell lines. In vivo studies fully validated our in vitro findings and revealed that neutralizing the acidic extracellular tumor pH by sodium bicarbonate treatment suppresses IFN-γ-induced PD-L1 expression and promotes immune cell infiltration in responsive tumors and thus reduces tumor growth. However, this effect was not observed in anti-PD-L1-nonresponsive tumors. In vivo experiments in tumor-bearing IFN-γ−/− mice validated the dependency on immune cell-derived IFN-γ for acidosis-mediated cancer cell PD-L1 induction and tumor immune escape. Thus, acidosis and IFN-γ-induced elevation of PD-L1 expression on cancer cells represent a previously unknown immune escape mechanism that may serve as a novel biomarker for anti-PD-L1/PD-1 treatment response. These findings have important implications for the development of new strategies to enhance the efficacy of immunotherapy in cancer patients.

Published

2023

46. Quality of biomarker defined subgroups in FDA approvals of PD-1/PD-L1 inhibitors 2014 to 2020.

Author

Kim, Myung S, Xu, Alexander, Haslam, Alyson, and Prasad, Vinay

Subjects

Humans, Neoplasms, Drug Approval, United States Food and Drug Administration, United States, Programmed Cell Death 1 Receptor, B7-H1 Antigen, Immune Checkpoint Inhibitors, PD-L1, biomarker, clinical trial design, immunotherapy, oncology, subgroup analysis, Clinical Trials and Supportive Activities, Clinical Research, Cancer, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Good Health and Well Being, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

PD-L1 expression is associated with differential response in cancers treated with checkpoint inhibitors. Clinical trials for Food and Drug Administration (FDA) approvals of programmed death receptor-1 (PD-1)/programmed death ligand-1 (PD-L1) inhibitors include limited subgroup analyses based on PD-L1 expression. We aimed to define the characteristics of PD-L1 defined subgroups of clinical trials leading to FDA approvals for new indications of PD-1/PD-L1 inhibitors. FDA approvals for PD-1/PD-L1 inhibitors from January 2014 to December 2020 were identified and the clinical trials leading to each drug approval were reviewed. We collected key variables from publicly available information on FDA website and peer-reviewed publications of clinical trials. We assessed regulatory characteristics (approval date, approved drug[s], cancer type, line of therapy and biomarker-restricted approval criteria) of each approval. Clinical trials leading to approvals were reviewed for trial design (RCT vs single arm study, primary endpoint) and PD-L1 defined subgroup design (no subgroup analysis, single threshold 2-group analysis, nested subgroups and adjacent subgroups). We then compared regulatory and trials characteristics (trial design, primary endpoint and biomarker approval criteria) between studies with nested and adjacent subgroups. There were 60 approvals for PD-1/PD-L1 inhibitors between January 2014 and December 2020. Twelve of 60 (20%) did not include any PD-L1 subgroups. Twenty-five of 60 (42%) approvals reported only two subgroups, 14 (23%) included adjacent subgroups and 9 (15%) had nested subgroups. Twenty-five of 60 trials (42%) are single arm studies. Comparison of characteristics between trials with nested subgroup design and adjacent subgroup design did not show differences. We conclude that approvals for new indications of PD-1/PD-L1 inhibitors are based on studies that do not include comprehensive reporting of outcomes by PD-L1 biomarker subgroups.

Published

2022

47. The Prognostic Role of [18F]FDG PET/CT in Patients with Advanced Cutaneous Squamous Cell Carcinoma Submitted to Cemiplimab Immunotherapy: A Single-Center Retrospective Study.

Author

Filippi, Luca, Proietti, Ilaria, Petrozza, Vincenzo, Potenza, Concetta, Bagni, Oreste, and Schillaci, Orazio

Subjects

*THERAPEUTIC use of monoclonal antibodies, *THERAPEUTIC use of antineoplastic agents, *POSITRON emission tomography computed tomography, *RETROSPECTIVE studies, *ACQUISITION of data, *TREATMENT effectiveness, *CANCER patients, *RADIOPHARMACEUTICALS, *MEDICAL records, *KAPLAN-Meier estimator, *DEOXY sugars, *SQUAMOUS cell carcinoma, *IMMUNOTHERAPY, *PROPORTIONAL hazards models, *GLYCOLYSIS

Abstract

Background: Baseline 2-deoxy-2[18F]fluoro-d-glucose ([18F]FDG) positron emission tomography (PET)-derived parameters and 12-week metabolic response were investigated as prognostic factors in advanced cutaneous squamous cell carcinoma (cSCC) submitted to cemiplimab immunotherapy. Materials and Methods: Clinical records of 25 cSCC patients receiving cemiplimab, submitted to [18F]FDG positron emission tomography/computed tomography (PET/CT) at baseline and after ∼12 weeks, were retrospectively reviewed. The Kaplan–Meier (KM) method was applied to analyze differences in event-free survival (EFS), and Cox regression analysis was employed to identify the prognostic factors. Results: At the 12-week PET/CT evaluation, 16 patients (64%) were classified as responders (complete or partial response) and 9 (36%) as nonresponders ("unconfirmed progressive metabolic disease") according to immune PET Response Criteria in Solid Tumors (iPERCIST). By KM analysis, baseline metabolic tumor volume (MTV) and total lesion glycolysis (TLG) significantly correlated with the EFS (p < 0.05). Furthermore, the KM analysis showed that the lack of metabolic response at 12 weeks was associated with meaningfully shorter EFS (7.2 ± 1 months in nonresponders vs. 20.3 ± 2.3 months in responders). In Cox multivariate analysis, metabolic response at 12 weeks remained the only predictor of the EFS (p < 0.05). Conclusions: Baseline tumor load (i.e., MTV and TLG) and metabolic response at 12 weeks may have a prognostic impact in cSCC patients treated with cemiplimab. [ABSTRACT FROM AUTHOR]

Published

2024

48. Insights of Clinical Significance From 109 695 Solid Tumor Tissue-Based Comprehensive Genomic Profiles.

Author

Heilmann, Andreas M, Riess, Jonathan W, McLaughlin-Drubin, Margaret, Huang, Richard S P, Hjulstrom, Meghann, Creeden, James, Alexander, Brian M, and Erlich, Rachel L

Subjects

TUMOR diagnosis, TUMOR treatment, TISSUE analysis, CLINICAL pathology, SCIENTIFIC observation, GENETIC mutation, SEQUENCE analysis, ONCOGENES, CARCINOGENESIS, RETROSPECTIVE studies, ACQUISITION of data, INDIVIDUALIZED medicine, MEDICAL protocols, CANCER patients, GENOMICS, GENE expression profiling, DECISION making, DIAGNOSIS, MEDICAL records, RESEARCH funding, DECISION making in clinical medicine, TUMOR markers, TUMORS, IMMUNOTHERAPY

Abstract

Background FoundationOneCDx is approved in the US and Japan as a companion diagnostic test to identify patients with cancer who may benefit from treatment with 30 drug therapies in the US and 23 in Japan. Tumor profiling with FoundationOneCDx also detects genomic findings with evidence of clinical significance that may inform clinical care decisions beyond companion diagnostic claims. This observational study reports the breadth and impact of clinical decision insights from FoundationOneCDx solid tumor profiles. Materials and Methods Consecutive test result reports for patients with solid tumor diagnoses (n  = 109 695) were retrospectively analyzed for clinically significant predictive, prognostic, and diagnostic genomic alterations and signatures, determined in accordance with professional guidelines. Interventional clinical trials with targeted therapies or immune checkpoint inhibitors were matched to tumor profiles based on evidence that the genomic finding may be an actionable, investigational, or hypothetical target in the patient's tumor type. Results In 14 predefined cancer types (80.7% of analyzed solid tumors), predictive, prognostic, and diagnostic markers were reported in 47.6%, 13.2%, and 4.5% of samples, respectively, accounting for a total of 51.2% of tumor profiles. Pan-cancer predictive markers of tumor mutational burden (TMB) of 10 or more mutations per megabase, high microsatellite instability (MSI), or NTRK1/2/3 fusions were observed in 15.6%, 2.0%, and 0.1% of solid tumors, respectively. Most solid tumor profiles (89.2%) had genomic results that could theoretically inform decisions on the selection of immunotherapy and targeted therapy clinical trials. Conclusion For this real-world population of patients with FoundationOneCDx solid tumor profiles in the routine course of clinical care, clinically significant findings were reported for approximately half of patients with genomic results. [ABSTRACT FROM AUTHOR]

Published

2024

49. Anorektales Melanom.

Author

Neeff, Hannes Philipp

Abstract

Copyright of Colo-Proctology is the property of Springer Nature 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

2024

50. Recent advances in the treatment for gynecologic oncology.

Author

Li, Lei and Lang, Jinghe

Subjects

THERAPEUTIC use of antineoplastic agents, OVARIAN tumors, GYNECOLOGY, CONFERENCES & conventions, ANTINEOPLASTIC agents, ONCOLOGY, IMMUNOTHERAPY, ENZYME inhibitors, PHARMACODYNAMICS

Abstract

This commentary summarized the most important findings in the first half 2023 year based on Society of Gynecologic Oncology (SGO) annual meeting and publications in crucial journals. This commentary provided a comprehensive overview of notable developments in the field of gynecologic oncology throughout the first half of 2023, drawing insights from the Society of Gynecologic Oncology (SGO) Annual Meeting and pivotal publications in esteemed journals. The discourse delved into the forefront of molecular mechanisms, emphasizing critical themes such as homologous recombination repair deficiency, mismatch repair, immune checkpoint blockades, and anti-angiogenesis in various cancers. Specific attention was given to advancements in targeted and immunotherapeutic modalities, notably examining the efficacy and safety profiles of poly (ADP-Ribose) polymerase inhibitors (PARPi) in ovarian cancer. Conclusively, the commentary underscored the transformative impact of molecularly guided therapies, marking them as pivotal in addressing refractory conditions and set the stage for heightened expectations in future advancements. PARP inhibitors have become the standard maintenance treatment for ovarian cancer. Among the first six articles, two (SOLO1 and PAOLA-1) summarized evidence supporting the improvement of overall survival with PARP inhibitors in maintenance therapy, while the NOVA study reported no benefit in overall survival. The first, fourth, and sixth articles discussed the feasibility of PARP inhibitors, immune checkpoint inhibitors used alone or in combination in neoadjuvant therapy (post-chemotherapy surgery). The latter two articles focused on the application of PD-1 (immune checkpoint inhibitors) in locally advanced cervical cancer, demonstrating enhanced efficacy. Currently, immune checkpoint inhibitors are commonly used in advanced cervical and endometrial cancers due to their status as hot tumors. Their use, either alone or in combination with anti-angiogenic drugs, has shown better outcomes in recurrent and advanced refractory endometrial and cervical cancers compared to traditional chemotherapy. A study from Huashan Hospital discussed the effectiveness of immune checkpoint inhibitors combined with anti-angiogenic therapy in recurrent cervical cancer, although there might be a typo as the initial mention was about endometrial cancer. The following article discussed late-stage endometrial cancer, finding no difference in survival between chemotherapy and chemotherapy combined with radiation. Subsequent articles highlighted the superiority of immune checkpoint inhibitors combined with chemotherapy in treating recurrent endometrial cancer, as well as the efficacy of immune checkpoint inhibitors combined with anti-angiogenic therapy in endometrial cancer. The final article focused on the therapeutic effect of HER2-positive ADC class drugs in uterine cancer sarcoma. [ABSTRACT FROM AUTHOR]

Published

2024