Your search keyword '"Tyrosine kinase inhibitors"' showing total 3 results

1. Immunotherapy, Tumor Microenvironment and Survival Signaling.

Author

Golubovskaya, Vita and Golubovskaya, Vita

Subjects

Clinical & internal medicine, Medicine, Autophagy, BCMA, CAR T cell, CAR macrophage, CAR-T, CAR-T cells, CD11, CD18, CD19, CD37, DCLK1, angiogenesis, antigen loss, breast cancer, cancer, cancer immunotherapy, cancer metabolism, cancer nanomedicine, cancer stem cells, cancer vaccines, cardiotoxicity, cell therapy, cell-cell contact, check point inhibitors, checkpoint, chemotherapy, chimeric antigen receptor, chimeric antigen receptors, clonogenicity, colorectal cancer, combination therapy, crosstalk, dendritic cells, electroporation, hypoxia, immune checkpoint inhibitor, immune checkpoint inhibitors, immune escape, immunogenic cell death, immunometabolism, immunomodulation, immunomodulators, immunotherapeutic agent, immunotherapies, immunotherapy, lentiviral transduction, lentivirus, leukemia cells, lung metastasis, lymphoma, lytic peptides, macrophages, melanoma, miRNA, microenvironment, mitochondria, mitochondrial transfer, myeloid-derived suppressor cells, n/a, nanoparticles, oncolytic viral therapy, pathogenesis, pediatric solid tumors, personalized medicine, programmed cell death 1 ligand 1, programmed cell death protein 1, regulatory T cells, resistance, risk factors, solid tumors, targeted therapy, targeted treatment, triple-negative breast cancer, tuft cells, tumor, tumor antigen, tumor antigens, tumor immune evasion, tumor microenvironment, tumor stem cells, tumor stroma, tunneling nanotubes, tyrosine kinase inhibitors, β2 integrins

Abstract

Summary: The book is based on the Cancers journal Special Issue entitled "Immunotherapy, Tumor Microenvironment and Survival Signaling", and focuses on important problems concerning tumors and tumor microenvironment interactions, as well as novel immunotherapies such as CAR-T cell therapy. Immunotherapies have recently shown remarkable results in the treatment of cancer patients. However, there are still many questions that remain to be solved in regards to more effective therapies, such as the tumor heterogeneous profile, tumor microenvironment, and tumor survival epigenetic and genetic pathways, all of which make patients resistant to the presently available treatments for cancer. This book demonstrates different approaches to overcome the challenges faced by immunotherapies due to suppressive tumor microenvironments. This book includes 18 papers that can be divided into three chapters: 1. novel immunotherapies; 2. targeting tumor microenvironment and novel approaches; 3. targeting tumors and tumor microenvironment in different types of cancer.

2. Protein Kinase Inhibitors.

Author

Hoda, Daanish and Daud, Adil

Abstract

Over the last few decades, scientists have begun to unravel the molecular basis of cancer. This understanding has led to many new treatment targets. New compounds designed to specifically inhibit these targets offer great promise. Trastuzumab, imatinib, sorafenib and sunitinib are all examples of targeted inhibitors that have significantly advanced the treatment of certain malignancies. Since then there has been development of many new agents. In this chapter, we discuss the available small molecule signal transduction modulators and their affect on cancer. [ABSTRACT FROM AUTHOR]

Published

2011

3. Present and potential future adjuvant issues in high-grade astrocytic glioma treatment.

Author

Lefranc, F., Rynkowski, M., DeWitte, O., and Kiss, R.

Abstract

Despite major advances in the management of malignant gliomas of which glioblastomas represent the ultimate grade of malignancy, they remain characterized by dismal prognoses. Glioblastoma patients have a median survival expectancy of only 14 months on the current standard treatment of surgical resection to the extent feasible, followed by adjuvant radiotherapy plus temozolomide, given concomitantly with and after radiotherapy. Malignant gliomas are associated with such dismal prognoses because glioma cells can actively migrate through the narrow extra-cellular spaces in the brain, often travelling relatively long distances, making them elusive targets for effective surgical management. Clinical and experimental data have demonstrated that invasive malignant glioma cells show a decrease in their proliferation rates and a relative resistance to apoptosis (type I programmed cell death) as compared to the highly cellular centre of the tumor, and this may contribute to their resistance to conventional pro-apoptotic chemotherapy and radiotherapy. Resistance to apoptosis results from changes at the genomic, transcriptional and post-transcriptional level of proteins, protein kinases and their transcriptional factor effectors. The PTEN/PI3K/Akt/mTOR/NF-ΚB and the Ras/Raf/MEK/ERK signaling cascades play critical roles in the regulation of gene expression and prevention of apoptosis. Components of these pathways are mutated or aberrantly expressed in human cancer, notably glioblastomas. Monoclonal antibodies and low molecular-weight kinase inhibitors of these pathways are the most common classes of agents in targeted cancer treatment. However, most clinical trials of these agents as monotherapies have failed to demonstrate survival benefit. Despite resistance to apoptosis being closely linked to tumorigenesis, tumor cells can still be induced to die by non-apoptotic mechanisms such as necrosis, senescence, autophagy (type II programmed cell death) and mitotic catastrophe. Temozolomide brings significant therapeutic benefits in glioblastoma treatment. Part of temozolomide cytotoxic activity is exerted through pro-autophagic processes and also through the induction of late apoptosis. Autophagy, type II programmed cell death, represents an alternative mechanism to overcome, at least partly, the dramatic resistance of many cancers to pro-apoptotic-related therapies. Another way to potentially overcome apoptosis resistance is to decrease the migration of malignant glioma cells in the brain, which then should restore a level of sensitivity to pro-apoptotic drugs. Recent series of studies have supported the concept that malignant gliomas might be seen as an orchestration of cross-talks between cancer cells, microenvironment, vasculature and cancer stem cells. The present chapter focuses on (i) the major signaling pathways making glioblastomas resistant to apoptosis, (ii) the signaling pathways distinctly activated by pro-autophagic drugs as compared to pro-apoptotic ones, (iii) autophagic cell death as an alternative to combat malignant gliomas, (iv) the major scientific data already obtained by researchers to prove that temozolomide is actually a pro-autophagic and pro-apoptotic drug, (v) the molecular and cellular therapies and local drug delivery which could be used to complement conventional treatments, and a review of some of the currently ongoing clinical trials, (vi) the fact that reducing the levels of malignant glioma cell motility can restore pro-apoptotic drug sensitivity, (vii) the observation that inhibiting the sodium pump activity reduces both glioma cell proliferation and migration, (viii) the brain tumor stem cells as a target to complement conventional treatment. [ABSTRACT FROM AUTHOR]

Published

2009