Your search keyword '"Yamakawa, Y"' showing total 93 results

1. Sasaki H, Dai M, Auclair D, Fukai I, Kiriyama M, Yamakawa Y, Fujii Y, Chen LB. Serum level of the periostin, a homologue of an insect cell adhesion molecule, as a prognostic marker in nonsmall cell lung carcinomas.Cancer. 2001;92(4):843-8

Author

Robert A. Smith, David A. Rothenberger, Richard C. Wender, Bernard Levin, Marion R. Nadel, P. S. Schroy, G. E. Feldman, Sally W. Vernon, Graham A. Colditz, and Robert H. Fletcher

Subjects

Strategic planning, Oncology, Cancer Research, medicine.medical_specialty, Adenomatous polyps, Colorectal cancer, business.industry, General surgery, Early detection, Cancer, medicine.disease, Internal medicine, medicine, business

Published

2002

2. Role of Immune Cells in Brain Metastasis of Lung Cancer Cells and Neuron-Tumor Cell Interaction

Author

Noda, M., Seike, T., Fujita, K., Yamakawa, Y., Kido, M., and Iguchi, H.

Published

2011

3. Present Scenario and Future Landscape of Payloads for ADCs: Focus on DNA-Interacting Agents.

Author

Valsasina, Barbara, Orsini, Paolo, Terenghi, Chiara, and Ocana, Alberto

Subjects

PLASMA stability, DNA damage, CELL death, CHEMICAL structure, ANTHRACYCLINES, DNA topoisomerase I, MONOCLONAL antibodies

Abstract

ADCs have emerged as a promising class of therapeutics, combining the targeting specificity of monoclonal antibodies with the cytotoxic potency of small-molecule drugs. Although the majority of approved ADCs are still based on microtubule binder payloads, the recent success of topoisomerase I inhibitors has revitalized interest in the identification of novel agents overcoming present limitations in the field including narrow therapeutic window and chemoresistance. The success of DNA binders as payload for ADCs has been very limited, up to now, due, among other factors, to high hydrophobicity and planar chemical structures resulting in most cases in ADCs with a strong tendency to aggregate, poor plasma stability, and limited therapeutic index. Some of these molecules, however, continue to be of interest due to their favorable properties in terms of cytotoxic potency even in chemoresistant settings, bystander and immunogenic cell death effects, and known combinability with approved drugs. We critically evaluated several clinically tested ADCs containing DNA binders, focusing on payload physicochemical properties, cytotoxic potency, and obtained clinical results. Our analysis suggests that further exploration of certain chemical classes, specifically anthracyclines and duocarmycins, based on the optimization of physicochemical parameters, reduction of cytotoxic potency, and careful design of targeting molecules is warranted. This approach will possibly result in a novel generation of payloads overcoming the limitations of clinically validated ADCs. [ABSTRACT FROM AUTHOR]

Published

2024

4. Death-associated protein 3 in cancer--discrepant roles of DAP3 in tumours and molecular mechanisms.

Author

Hao Song, Huifang Liu, Xiufeng Wang, Yuteng Yang, Xiangkun Zhao, Jiang, Wen G., Laijian Sui, and Xicheng Song

Subjects

TUMOR growth, CARCINOGENESIS, DISEASE progression, DRUG resistance, CAUSES of death

Abstract

Cancer, ranks as the secondary cause of death, is a group of diseases that are characterized by uncontrolled tumor growth and distant metastasis, leading to increased mortality year-on-year. To date, targeted therapy to intercept the aberrant proliferation and invasion is crucial for clinical anticancer treatment, however, mutant expression of target genes often leads to drug resistance. Therefore, it is essential to identify more molecules that can be targeted to facilitate combined therapy. Previous studies showed that death associated protein 3 (DAP3) exerts a pivotal role in regulating apoptosis signaling of tumors, meanwhile, aberrant DAP3 expression is associated with the tumorigenesis and disease progression of various cancers. This review provides an overview of the molecule structure of DAP3 and the discrepant roles played by DAP3 in various types of tumors. Considering the molecular mechanism of DAP3-regulated cancer development, new potential treatment strategies might be developed in the future. [ABSTRACT FROM AUTHOR]

Published

2024

5. Apoptosis Inhibitor 5: A Multifaceted Regulator of Cell Fate.

Author

Abbas, Hafsia, Derkaoui, Dalia Kheira, Jeammet, Louise, Adicéam, Emilie, Tiollier, Jérôme, Sicard, Hélène, Braun, Thorsten, and Poyet, Jean-Luc

Subjects

PHENOMENOLOGICAL biology, APOPTOSIS, FIBROBLASTS

Abstract

Apoptosis, or programmed cell death, is a fundamental process that maintains tissue homeostasis, eliminates damaged or infected cells, and plays a crucial role in various biological phenomena. The deregulation of apoptosis is involved in many human diseases, including cancer. One of the emerging players in the intricate regulatory network of apoptosis is apoptosis inhibitor 5 (API5), also called AAC-11 (anti-apoptosis clone 11) or FIF (fibroblast growth factor-2 interacting factor). While it may not have yet the same level of notoriety as some other cancer-associated proteins, API5 has garnered increasing attention in the cancer field in recent years, as elevated API5 levels are often associated with aggressive tumor behavior, resistance to therapy, and poor patient prognosis. This review aims to shed light on the multifaceted functions and regulatory mechanisms of API5 in cell fate decisions as well as its interest as therapeutic target in cancer. [ABSTRACT FROM AUTHOR]

Published

2024

6. Ca 2+ Signaling and Src Functions in Tumor Cells.

Author

Villalobo, Antonio

Subjects

CALCIUM ions, CALMODULIN, CELL physiology, PROTEIN-tyrosine kinases, CELL communication, KINASES

Abstract

Signaling by calcium ion (Ca2+) plays a prominent role in cell physiology, and these mechanisms are frequently altered in tumor cells. In this review, we consider the interplay of Ca2+ signaling and the functions of the proto-oncogene non-receptor tyrosine kinase c-Src in tumor cells, and the viral oncogenic variant v-Src in transformed cells. Also, other members of the Src-family kinases are considered in this context. The role of Ca2+ in the cell is frequently mediated by Ca2+-binding proteins, where the Ca2+-sensor protein calmodulin (CaM) plays a prominent, essential role in many cellular signaling pathways. Thus, we cover the available information on the role and direct interaction of CaM with c-Src and v-Src in cancerous cells, the phosphorylation of CaM by v-Src/c-Src, and the actions of different CaM-regulated Ser/Thr-protein kinases and the CaM-dependent phosphatase calcineurin on v-Src/c-Src. Finally, we mention some clinical implications of these systems to identify mechanisms that could be targeted for the therapeutic treatment of human cancers. [ABSTRACT FROM AUTHOR]

Published

2023

7. Management of chronic myeloid leukaemia: current treatment options, challenges, and future strategies.

Author

Younes, Salma, Ismail, Mohamed A., Al-Jurf, Rana, Ziyada, Ayah, Nasrallah, Gheyath K., Abdulrouf, Palli Valapila, Nagy, Mohamed, Zayed, Hatem, Farrell, Thomas, Sorio, Claudio, Morsi, Hisham, Qoronfleh, M. Walid, and Al-Dewik, Nader I.

Subjects

CHRONIC myeloid leukemia, PROTEIN-tyrosine kinase inhibitors, CELLULAR signal transduction, SMALL molecules, CHRONIC leukemia

Abstract

Small molecule therapy is a critical component of targeted anticancer treatment, with tyrosine kinase inhibitors (TKIs) being the first compounds to treat the clonal Chronic Myelogenous Leukaemia (CML) translocation t (9;22) (q34; q11) effectively since 2001. TKIs, such as imatinib, have improved the 10-year survival rate of CML patients to 80%. They bind the BCR::ABL1 kinase and inhibit downstream signaling pathways. However, therapy failure may be seen in 20-25% of CML patients due to intolerance or inadequacy related to BCR::ABL1 dependent or independent mechanisms. This review aimed to summarize current treatment options involving TKIs, resistance mechanisms and the prospective approaches to overcome TKI resistance. We highlight BCR::ABL1-dependent mechanisms of TKI resistance by reviewing clinically-documented BCR::ABL1 mutations and their consequences for TKI binding. In addition, we summarize BCR::ABL1 independent pathways, including the relevance of drug efflux, dysregulation of microRNA, and the involvement of alternative signaling pathways. We also discuss future approaches, such as gene-editing techniques in the context of CML, as potential therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2023

8. The origin of brain malignancies at the blood–brain barrier.

Author

McDonald, Brennan, Barth, Kathrin, and Schmidt, Mirko H. H.

Subjects

BLOOD-brain barrier, BRAIN metastasis, BRAIN tumors, EXTRACELLULAR vesicles, SURVIVAL rate, GLIOMAS

Abstract

Despite improvements in extracranial therapy, survival rate for patients suffering from brain metastases remains very poor. This is coupled with the incidence of brain metastases continuing to rise. In this review, we focus on core contributions of the blood–brain barrier to the origin of brain metastases. We first provide an overview of the structure and function of the blood–brain barrier under physiological conditions. Next, we discuss the emerging idea of a pre-metastatic niche, namely that secreted factors and extracellular vesicles from a primary tumor site are able to travel through the circulation and prime the neurovasculature for metastatic invasion. We then consider the neurotropic mechanisms that circulating tumor cells possess or develop that facilitate disruption of the blood–brain barrier and survival in the brain's parenchyma. Finally, we compare and contrast brain metastases at the blood–brain barrier to the primary brain tumor, glioma, examining the process of vessel co-option that favors the survival and outgrowth of brain malignancies. [ABSTRACT FROM AUTHOR]

Published

2023

9. TENDENCIAS EMERGENTES DE INVESTIGACIÓN CIENTÍFICA SOBRE Dactylopius coccus Costa (HEMIPTERA: DACTYLOPIIDAE), ÁCIDO CARMÍNICO Y SUS DERIVADOS: UN ANÁLISIS BIBLIOMÉTRICO.

Author

Bravo-Vinaja, Angel and de Jesús Méndez-Gallegos, Santiago

Subjects

COCHINEAL insect, SCIENTIFIC literature, SOLAR cells, CANCER, BIBLIOMETRICS

Abstract

Copyright of Agricultura Sociedad y Desarrollo is the property of Colegio de Postgraduados and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

10. Therapeutic Drug Monitoring in Oncohematological Patients: A Fast and Accurate HPLC-UV Method for the Quantification of Nilotinib in Human Plasma and Its Clinical Application.

Author

Escudero-Ortiz, Vanesa, Rodríguez-Lucena, Francisco José, Estan-Cerezo, Gabriel, Mancheño-Maciá, Esther, Conesa-García, Venancio, García-Monsalve, Ana, Soriano-Irigaray, Leticia, and Navarro-Ruiz, Andrés

Subjects

NILOTINIB, DRUG monitoring, PATIENT monitoring, CHRONIC myeloid leukemia, CLINICAL medicine, PROTEIN-tyrosine kinase inhibitors

Abstract

Nilotinib, a second-generation tyrosine kinase inhibitor, has demonstrated clinical activity in chronic myeloid leukemia. As an exposure–response relationship has been observed for nilotinib, its therapeutic drug monitoring could be a valuable tool in clinical practice. Therefore, the aim of this study was to develop and validate a selective and precise high performance liquid chromatography–ultraviolet method for the measurement of nilotinib in plasma from patients with cancer. After protein precipitation extraction with acetonitrile, nilotinib and rilpivirine were separated using isocratic elution on a Tracer Excel 120 ODS C18 column using a mobile phase consisting of a mixture of potassium dihydrogen phosphate-buffered solution (pH 5.5; 0.037 M)–methanol–acetonitrile (45:45:10, v/v/v), pumped at a flow rate of 1.7 mL·min−1. A wavelength of 254 nm was selected for the quantification of the analyte and the internal standard (IS). The technique was validated following the guidelines for the validation of analytical methods of regulatory agencies (Food and Drug Administration (FDA) and the European Medicines Agency (EMA)). Linearity was established in a concentration range between 125 and 7000 ng/mL. The detection limit was 90 ng/mL, and the lower limit of quantification was 125 ng/mL. For all concentrations in the calibration curve, the intraday and interday coefficients of variation were less than 4.1%. Median recovery of nilotinib from plasma was ≥65.1% (±21.4%). The method described is sensitive, selective, reproducible, and rapid, and can be used for the accurate determination of nilotinib in human plasma for pharmacokinetics studies and for therapeutic drug monitoring (TDM) of nilotinib in routine clinical practice. [ABSTRACT FROM AUTHOR]

Published

2023

11. Extensive Molecular Dynamics Simulations Disclosed the Stability of mPGES‐1 Enzyme and the Structural Role of Glutathione (GSH) Cofactor.

Author

Di Micco, Simone, Lauro, Gianluigi, and Bifulco, Giuseppe

Subjects

MOLECULAR dynamics, ENZYME stability, SMALL molecules, CYTOSKELETAL proteins, GLUTATHIONE, PROTEIN structure

Abstract

A deep in silico investigation of various microsomal prostaglandin E2 synthase‐1 (mPGES‐1) protein systems is here reported using molecular dynamics (MD) simulations. Firstly, eight different proteins models (Models A−H) were built, starting from the active enzyme trimer system (Model A), namely that bound to three glutathione (GSH) cofactor molecules, and then gradually removing the GSHs (Models B−H), simulating each of them for 100 ns in explicit solvent. The analysis of the obtained data disclosed the structural role of GSH in the chemical architecture of mPGES‐1 enzyme, thus suggesting the unlikely displacement of this cofactor, in accordance with experimentally determined protein structures co‐complexed with small molecule inhibitors. Afterwards, Model A was submitted to microsecond‐scale molecular dynamics simulation (total simulation time=10 μs), in order to shed light about the dynamical behaviour of this enzyme at atomic level and to obtain further structural features and protein function information. We confirmed the structural stability of the enzyme machinery, observing a conformational rigidity of the protein, with a backbone RMSD of ∼3 Å along the simulation time, and highlighting the strong active contribution of GSH molecules due to their active role in packing the protein chains through a tight binding at monomer interfaces. Furthermore, the focused analysis on R73 residue disclosed its role in solvent exchange events, probably excluding its function as route for GSH to enter towards the endoplasmic reticulum membrane, in line with the recently reported function of cap domain residues F44‐D66 as gatekeeper for GSH entrance into catalytic site. [ABSTRACT FROM AUTHOR]

Published

2022

12. Neither soyfoods nor isoflavones warrant classification as endocrine disruptors: a technical review of the observational and clinical data.

Author

Messina, Mark, Mejia, Sonia Blanco, Cassidy, Aedin, Duncan, Alison, Kurzer, Mindy, Nagato, Chisato, Ronis, Martin, Rowland, Ian, Sievenpiper, John, and Barnes, Stephen

Abstract

Soybeans are a rich source of isoflavones, which are classified as phytoestrogens. Despite numerous proposed benefits, isoflavones are often classified as endocrine disruptors, based primarily on animal studies. However, there are ample human data regarding the health effects of isoflavones. We conducted a technical review, systematically searching Medline, EMBASE, and the Cochrane Library (from inception through January 2021). We included clinical studies, observational studies, and systematic reviews and meta-analyses (SRMA) that examined the relationship between soy and/or isoflavone intake and endocrine-related endpoints. 417 reports (229 observational studies, 157 clinical studies and 32 SRMAs) met our eligibility criteria. The available evidence indicates that isoflavone intake does not adversely affect thyroid function. Adverse effects are also not seen on breast or endometrial tissue or estrogen levels in women, or testosterone or estrogen levels, or sperm or semen parameters in men. Although menstrual cycle length may be slightly increased, ovulation is not prevented. Limited insight could be gained about possible impacts of in utero isoflavone exposure, but the existing data are reassuring. Adverse effects of isoflavone intake were not identified in children, but limited research has been conducted. After extensive review, the evidence does not support classifying isoflavones as endocrine disruptors. [ABSTRACT FROM AUTHOR]

Published

2022

13. Periostin: biology and function in cancer.

Author

Dorafshan, Shima, Razmi, Mahdieh, Safaei, Sadegh, Gentilin, Erica, Madjd, Zahra, and Ghods, Roya

Subjects

PERIOSTIN, TUMOR proteins, PERIODONTAL ligament, BIOLOGY, EPITHELIAL-mesenchymal transition

Abstract

Periostin (POSTN), a member of the matricellular protein family, is a secreted adhesion-related protein produced in the periosteum and periodontal ligaments. Matricellular proteins are a nonstructural family of extracellular matrix (ECM) proteins that regulate a wide range of biological processes in both normal and pathological conditions. Recent studies have demonstrated the key roles of these ECM proteins in the tumor microenvironment. Furthermore, periostin is an essential regulator of bone and tooth formation and maintenance, as well as cardiac development. Also, periostin interacts with multiple cell-surface receptors, especially integrins, and triggers signals that promote tumor growth. According to recent studies, these signals are implicated in cancer cell survival, epithelial-mesenchymal transition (EMT), invasion, and metastasis. In this review, we will summarize the most current data regarding periostin, its structure and isoforms, expressions, functions, and regulation in normal and cancerous tissues. Emphasis is placed on its association with cancer progression, and also future potential for periostin-targeted therapeutic approaches will be explored. [ABSTRACT FROM AUTHOR]

Published

2022

14. Day-to-Day Decision Making by Adolescents and Young Adults with Cancer.

Author

Pyke-Grimm, Kimberly A., Franck, Linda S., Halpern-Felsher, Bonnie, Goldsby, Robert E., and Rehm, Roberta S.

Subjects

SELF advocacy, RESEARCH methodology, INTERVIEWING, MENTAL health, TUMORS in children, QUALITATIVE research, SELF-efficacy, DECISION making in adolescence, DESCRIPTIVE statistics, COMMUNICATION, INTERPERSONAL relations, PARTICIPANT observation, HEALTH self-care

Abstract

Background: Adolescents and young adults (AYAs) with cancer must negotiate the transition between childhood and adulthood while dealing with a life-threatening illness. AYA involvement in decision making varies depending on the type of decision and when decisions occur during treatment, and evidence suggests that AYAs want to be involved in decision making. Objective: To explore involvement of AYAs with cancer in day-to-day decisions affected by their cancer and treatment. Methods: This qualitative study used interpretive focused ethnography within the sociologic tradition, informed by symbolic interactionism. Semi-structured interviews and informal participant observation took place at two quaternary pediatric oncology programs. Results: Thirty-one interviews were conducted with 16 AYAs ages 15 to 20 years. Major day to day decision-making categories identified included: (1) mental mindset, (2) self-care practices, (3) self-advocacy, and (4) negotiating relationships. Participants described how they came to grips with their illness early on and decided to fight their cancer. They described decisions they made to protect their health, how they advocated for themselves and decisions they made about relationships with family and friends. Conclusions: Through day-to-day decisions, participants managed the impact of cancer and its treatment on their daily lives. Research should focus on developing and implementing interventions to empower AYAs to participate in day-to-day decisions that will affect how they manage their cancer, its treatment and ultimately their outcomes. Implications for Practice: Healthcare providers can facilitate AYA's participation in day-to-day decision making through encouraging autonomy and self-efficacy by providing support and through effective communication. [ABSTRACT FROM AUTHOR]

Published

2022

15. Inositol 1,4,5-trisphosphate receptor type 1 autoantibody (ITPR1-IgG/anti-Sj)-associated autoimmune cerebellar ataxia, encephalitis and peripheral neuropathy: review of the literature.

Author

Jarius, Sven, Bräuninger, Stefan, Chung, Ha-Yeun, Geis, Christian, Haas, Jürgen, Komorowski, Lars, Wildemann, Brigitte, and Roth, Christian

Abstract

Background: In 2014, we first described novel autoantibodies to the inositol 1,4,5-trisphosphate receptor type 1 (ITPR1-IgG/anti-Sj) in patients with autoimmune cerebellar ataxia (ACA) in this journal. Here, we provide a review of the available literature on ITPR1-IgG/anti-Sj, covering clinical and paraclinical presentation, tumour association, serological findings, and immunopathogenesis.Methods: Review of the peer-reviewed and PubMed-listed English language literature on ITPR1-IgG/anti-Sj. In addition, we provide an illustrative report on a new patient with ITPR1-IgG-associated encephalitis with cognitive decline and psychosis.Results: So far, at least 31 patients with serum ITPR1-IgG/anti-Sj have been identified (clinical information available for 21). The most common manifestations were ACA, encephalopathy with seizures, myelopathy, and (radiculo)neuropathy, including autonomic neuropathy. In 45% of cases, an underlying tumour was present, making the condition a facultative paraneoplastic neurological disorder. The neurological syndrome preceded tumour diagnosis in all but one case. In most cases, immunotherapy had only moderate or no effect. The association of ITPR1-IgG/anti-Sj with manifestations other than ACA is corroborated by the case of a 48-year-old woman with high-titre ITPR1-IgG/anti-Sj antibodies and rapid cognitive decline, affecting memory, attention and executive function, and psychotic manifestations, including hallucinations, investigated here in detail. FDG-PET revealed right-temporal glucose hypermetabolism compatible with limbic encephalitis. Interestingly, ITPR1-IgG/anti-Sj mainly belonged to the IgG2 subclass in both serum and cerebrospinal fluid (CSF) in this and further patients, while it was predominantly IgG1 in other patients, including those with more severe outcome, and remained detectable over the entire course of disease. Immunotherapy with intravenous methylprednisolone, plasma exchange, and intravenous immunoglobulins, was repeatedly followed by partial or complete recovery. Long-term treatment with cyclophosphamide was paralleled by relative stabilization, although the patient noted clinical worsening at the end of each treatment cycle.Conclusions: The spectrum of neurological manifestations associated with ITPR1 autoimmunity is broader than initially thought. Immunotherapy may be effective in some cases. Studies evaluating the frequency of ITPR1-IgG/anti-Sj in patients with cognitive decline and/or psychosis of unknown aetiology are warranted. Tumour screening is essential in patients presenting with ITPR1-IgG/anti-Sj. [ABSTRACT FROM AUTHOR]

Published

2022

16. Estrogens, Cancer and Immunity.

Author

Orzołek, Izabela, Sobieraj, Jan, and Domagała-Kulawik, Joanna

Subjects

PUBLIC health surveillance, DENDRITIC cells, IMMUNE checkpoint inhibitors, ESTRADIOL, ESTROGEN, ANTINEOPLASTIC agents, IMMUNOSUPPRESSION, MACROPHAGES, LYMPHOCYTES, IMMUNITY, TUMORS

Abstract

Simple Summary: In this review, we present current knowledge of sex hormones in the process of development of malignant diseases. The impact of sex hormones on immune system is presented. A special account is devoted to estrogens and their role in modification of anticancer immune response. Sex hormones are included in many physiological and pathological pathways. Estrogens belong to steroid hormones active in female sex. Estradiol (E2) is the strongest female sex hormone and, with its receptors, contributes to oncogenesis, cancer progression and response to treatment. In recent years, a role of immunosurveillance and suppression of immune response in malignancy has been well defined, forming the basis for cancer immunotherapy. The interplay of sex hormones with cancer immunity, as well as the response to immune checkpoint inhibitors, is of interest. In this review, we investigate the impact of sex hormones on natural immune response with respect to main active elements in anticancer immune surveillance: dendritic cells, macrophages, lymphocytes and checkpoint molecules. We describe the main sex-dependent tumors and the contribution of estrogen in their progression, response to treatment and especially modulation of anticancer immune response. [ABSTRACT FROM AUTHOR]

Published

2022

17. External evaluation of population pharmacokinetic models of imatinib in adults diagnosed with chronic myeloid leukaemia.

Author

Corral Alaejos, Álvaro, Zarzuelo Castañeda, Aránzazu, Jiménez Cabrera, Silvia, Sánchez‐Guijo, Fermín, Otero, María José, and Pérez‐Blanco, Jonás Samuel

Subjects

NILOTINIB, CHRONIC myeloid leukemia, IMATINIB, DRUG monitoring, MYELOID leukemia, PHARMACOKINETICS

Abstract

Aims: Imatinib is considered the standard first‐line treatment in newly diagnosed patients with chronic‐phase myeloid leukaemia (CML). Several imatinib population pharmacokinetic (popPK) models have been developed. However, their predictive performance has not been well established when extrapolated to different populations. Therefore, this study aimed to perform an external evaluation of available imatinib popPK models developed mainly in adult patients, and to evaluate the improvement in individual model‐based predictions through Bayesian forecasting computed by each model at different treatment occasions. Methods: A literature review was conducted through PubMed and Scopus to identify popPK models. Therapeutic drug monitoring data collected in adult CML patients treated with imatinib was used for external evaluation, including prediction‐ and simulated‐based diagnostics together with Bayesian forecasting analysis. Results: Fourteen imatinib popPK studies were included for model‐performance evaluation. A total of 99 imatinib samples were collected from 48 adult CML patients undergoing imatinib treatment with a minimum of one plasma concentration measured at steady‐state between January 2016 and December 2020. The model proposed by Petain et al showed the best performance concerning prediction‐based diagnostics in the studied population. Bayesian forecasting demonstrated a significant improvement in predictive performance at the second visit. Inter‐occasion variability contributed to reducing bias and improving individual model‐based predictions. Conclusions: Imatinib popPK studies developed in Caucasian subjects including α1‐acid glycoprotein showed the best model performance in terms of overall bias and precision. Moreover, two imatinib samples from different visits appear sufficient to reach an adequate model‐based individual prediction performance trough Bayesian forecasting. [ABSTRACT FROM AUTHOR]

Published

2022

18. Thymic epithelial tumours in 51 dogs: Histopathologic and clinicopathologic findings.

Author

Yale, Andrew D., Priestnall, Simon L., Pittaway, Rachel, and Taylor, Angela J.

Subjects

MYASTHENIA gravis, CLINICAL pathology, DOGS, TUMORS, PROGNOSIS, SURVIVAL rate

Abstract

Canine thymic epithelial tumours (TET) are uncommon and little is known about their behaviour. Previous attempts at histologic classification have varied, and as such reliable prognostic information is unavailable. The aim of this retrospective multi‐institutional study was to evaluate cases of canine TETs, irrespective of subtype, in order to identify useful histopathologic and clinicopathologic prognostic factors. Cases were included if the tumour arose from the cranial mediastinum and a diagnosis of TET was made on the basis of histopathology. Fifty‐one dogs were included. In addition to clinicopathologic data, histology samples were reviewed for the following features: mitotic count, percentage of necrosis, presence of Hassall's corpuscles, lymphocytic infiltrate, cellular pleomorphism and vascular or capsular invasion. The median survival time for all dogs was 449 days. The 1‐ and 2‐year survival rate was 52.6% and 26.3% respectively. On multivariable analysis surgical excision of the thymic tumour was associated with significantly prolonged survival; the presence of metastasis, myasthenia gravis and moderate or marked cellular pleomorphism were associated with significantly reduced survival. Additional studies are needed to further evaluate prognostic factors to aid treatment recommendations. [ABSTRACT FROM AUTHOR]

Published

2022

19. Tumor Immune Microenvironment and Immunotherapy in Brain Metastasis From Non-Small Cell Lung Cancer.

Author

Wang, Yuchang, Chen, Rui, Wa, Yue, Ding, Shikuan, Yang, Yijian, Liao, Junbo, Tong, Lei, and Xiao, Gelei

Subjects

NON-small-cell lung carcinoma, BRAIN metastasis, TUMOR microenvironment, IMMUNE checkpoint inhibitors, CANCER patients

Abstract

Brain metastasis (BM), a devastating complication of advanced malignancy, has a high incidence in non-small cell lung cancer (NSCLC). As novel systemic treatment drugs and improved, more sensitive imaging investigations are performed, more patients will be diagnosed with BM. However, the main treatment methods face a high risk of complications at present. Therefore, based on immunotherapy of tumor immune microenvironment has been proposed. The development of NSCLC and its BM is closely related to the tumor microenvironment, the surrounding microenvironment where tumor cells live. In the event of BM, the metastatic tumor microenvironment in BM is composed of extracellular matrix, tissue-resident cells that change with tumor colonization and blood-derived immune cells. Immune-related cells and chemicals in the NSCLC brain metastasis microenvironment are targeted by BM immunotherapy, with immune checkpoint inhibition therapy being the most important. Blocking cancer immunosuppression by targeting immune checkpoints provides a suitable strategy for immunotherapy in patients with advanced cancers. In the past few years, several therapeutic advances in immunotherapy have changed the outlook for the treatment of BM from NSCLC. According to emerging evidence, immunotherapy plays an essential role in treating BM, with a more significant safety profile than others. This article discusses recent advances in the biology of BM from NSCLC, reviews novel mechanisms in diverse tumor metastatic stages, and emphasizes the role of the tumor immune microenvironment in metastasis. In addition, clinical advances in immunotherapy for this disease are mentioned. [ABSTRACT FROM AUTHOR]

Published

2022

20. The molecular structure and role of LECT2 or CHM‐II in arthritis, cancer, and other diseases.

Author

Zhu, Sipin, Bennett, Samuel, Li, Yihe, Liu, Mei, and Xu, Jiake

Subjects

MOLECULAR structure, VIRAL tropism, NON-alcoholic fatty liver disease, CELL receptors, CARTILAGE cells, CHEMOTACTIC factors, BONE cells, CHEMOTAXIS

Abstract

Leukocyte cell‐derived chemotaxin‐2 (LECT2 or LECT‐2), also called chondromodulin II (ChM‐II or CHM2) plays a versatile role in various tissues. It was first identified as a chemotactic factor to promote the migration of neutrophils. It was also reported as a hepatokine to regulate glucose metabolism, obesity, and nonalcoholic fatty liver disease. As a secreted factor, LECT2 binds to several cell surface receptors CD209a, Tie1, and Met to regulate inflammatory reaction, fibrogenesis, vascular invasion, and tumor metastasis in various cell types. As an intracellular molecule, it is associated with LECT2‐mediated amyloidosis, in which LECT2 misfolding results in insoluble fibrils in multiple tissues such as the kidney, liver, and lung. Recently, LECT2 was found to be associated with the development of rheumatoid arthritis and osteoarthritis, involving the dysregulation of osteoclasts, mesenchymal stem cells, osteoblasts, chondrocytes, and endothelial cells in the bone microenvironment. LECT2 is implicated in the development of cancers, such as hepatocellular carcinoma via MET‐mediated PTP1B/Raf1/ERK signaling pathways and is proposed as a biomarker. The mechanisms by which LECT2 regulates diverse pathogenic conditions in various tissues remain to be fully elucidated. Further research to understand the role of LECT2 in a tissue tropism‐dependent manner would facilitate the development of LECT2 as a biomarker for diagnosis and therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2022

21. Chemoenzymatic Synthesis of 9NHAc‐GD2 Antigen to Overcome the Hydrolytic Instability of O‐Acetylated‐GD2 for Anticancer Conjugate Vaccine Development.

Author

Wu, Xuanjun, Ye, Jinfeng, DeLaitsch, Andrew T., Rashidijahanabad, Zahra, Lang, Shuyao, Kakeshpour, Tayeb, Zhao, Yuetao, Ramadan, Sherif, Saavedra, Paulo Vilar, Yuzbasiyan‐Gurkan, Vilma, Kavunja, Herbert, Cao, Hongzhi, Gildersleeve, Jeffrey C., and Huang, Xuefei

Subjects

VACCINE development, ANTIGENS, IMMUNOGLOBULIN G, ACETAMIDE, IMMUNOGLOBULINS, CARBOHYDRATES

Abstract

Ganglioside GD2 is an attractive tumor‐associated carbohydrate antigen for anti‐cancer vaccine development. However, its low immunogenicity and the significant side effects observed with anti‐GD2 antibodies present significant obstacles for vaccines. To overcome these, a new GD2 derivative bearing an N‐acetamide (NHAc) at its non‐reducing end neuraminic acid (9NHAc‐GD2) has been designed to mimic the 9‐O‐acetylated‐GD2 (9OAc‐GD2), a GD2 based antigen with a restricted expression on tumor cells. 9NHAc‐GD2 was synthesized efficiently via a chemoenzymatic method and subsequently conjugated with a powerful carrier bacteriophage Qβ. Mouse immunization with the Qβ‐9NHAc‐GD2 conjugate elicited strong and long‐lasting IgG antibodies, which were highly selective toward 9NHAc‐GD2 with little cross‐recognition of GD2. Immunization of canines with Qβ‐9NHAc‐GD2 showed the construct was immunogenic in canines with little adverse effects, paving the way for future clinical translation to humans. [ABSTRACT FROM AUTHOR]

Published

2021

22. CD44 as a tumor biomarker and therapeutic target.

Author

Xu, Hanxiao, Niu, Mengke, Yuan, Xun, Wu, Kongming, and Liu, Aiguo

Subjects

BIOMARKERS, EPITHELIAL-mesenchymal transition, CANCER stem cells, HUMAN carcinogenesis, CANCER invasiveness, TUMOR markers

Abstract

CD44, a complex transmembrane glycoprotein, exists in multiple molecular forms, including the standard isoform CD44s and CD44 variant isoforms. CD44 participates in multiple physiological processes, and aberrant expression and dysregulation of CD44 contribute to tumor initiation and progression. CD44 represents a common biomarker of cancer stem cells, and promotes epithelial-mesenchymal transition. CD44 is involved in the regulation of diverse vital signaling pathways that modulate cancer proliferation, invasion, metastasis and therapy-resistance, and it is also modulated by a variety of molecules in cancer cells. In addition, CD44 can serve as an adverse prognostic marker among cancer population. The pleiotropic roles of CD44 in carcinoma potentially offering new molecular target for therapeutic intervention. Preclinical and clinical trials for evaluating the pharmacokinetics, efficacy and drug-related toxicity of CD44 monoclonal antibody have been carried out among tumors with CD44 expression. In this review, we focus on current data relevant to CD44, and outline CD44 structure, the regulation of CD44, functional properties of CD44 in carcinogenesis and cancer progression as well as the potential CD44-targeting therapy for cancer management. [ABSTRACT FROM AUTHOR]

Published

2020

23. Prognostic value of periostin in multiple solid cancers: A systematic review with meta‐analysis.

Author

Yang, Tao, Deng, Zhengdong, Pan, Zhongya, Qian, Yawei, Yao, Wei, and Wang, Jianming

Subjects

META-analysis, BREAST cancer prognosis, PROGRESSION-free survival, ODDS ratio, CANCER, LYMPH nodes, CONFIDENCE intervals

Abstract

Previous studies have shown that the expression of periostin (POSTN) is significantly correlated with prognosis in multiple solid cancers. However, the function of POSTN in tumorigenesis and its relationship with clinical outcomes have not been systematically summarized and analyzed. Thus, a meta‐analysis was performed to evaluate the prognostic pertinence of POSTN in solid cancer. We conducted a systematic search in the PubMed, EMBASE, Web of Science, and Cochrane library databases, and a total of 10 studies were used to assess the association of POSTN expression and patients' overall survival (OS) and disease‐free survival (DFS). The hazard ratio (HR) or odds ratio (OR) and their corresponding 95% confidence intervals (95% CIs) were further calculated to estimate the association between POSTN and relevant clinical parameters of solid cancer patients. The pooled results indicated that POSTN overexpression was associated with poor OS (HR = 2.35, 95% CI = 1.88–2.93, p < .00001) and DFS (HR = 2.70, 95% CI = 2.00–3.65, p < .00001) in a cohort of 993 patients with cancer. Subsequent analyses showed that the positive expression ratio of POSTN was evidently higher in cancer tissues than in normal tissues (OR = 7.44, 95% CI = 3.66–13.95, p < .00001). In addition, subgroup analysis showed that POSTN was related to microvascular invasion (OR = 5.09, 95% CI = 3.07–8.44, p < .00001), tumor differentiation (OR = 2.03, 95% CI = 1.41–2.91, p = .0001), and lymph node metastasis (OR = 3.05, 95% CI = 2.01–4.64, p < .00001). These data showed that POSTN could be a credible prognostic biomarker and a potential therapeutic target in human solid cancer. [ABSTRACT FROM AUTHOR]

Published

2020

24. miRNA signatures in childhood sarcomas and their clinical implications.

Author

Viera, G. M., Salomao, K. B., de Sousa, G. R., Baroni, M., Delsin, L. E. A., Pezuk, J. A., and Brassesco, M. S.

Abstract

Progresses in multimodal treatments have significantly improved the outcomes for childhood cancer. Nonetheless, for about one-third of patients with Ewing sarcoma, rhabdomyosarcoma, or osteosarcoma steady remission has remained intangible. Thus, new biomarkers to improve early diagnosis and the development of precision-targeted medicine remain imperative. Over the last decade, remarkable progress has been made in the basic understanding of miRNAs function and in interpreting the contribution of their dysregulation to cancer development and progression. On this basis, this review focuses on what has been learned about the pivotal roles of miRNAs in the regulation of key genes implicated in childhood sarcomas. [ABSTRACT FROM AUTHOR]

Published

2019

25. Thymoma appearing 9 years after the resection of squamous cell carcinoma of the lip: A case report of triple primary tumors and literature review.

Author

Maruyama, Nobuyuki, Sasaki, Takanobu, Arasaki, Akira, Matsuzaki, Akiko, Nakasone, Toshiyuki, Teruya, Takao, Matayoshi, Akira, Maruyama, Tessho, Karube, Kennosuke, Fujita, Jiro, Yoshimi, Naoki, Kuniyoshi, Yukio, and Nishihara, Kazuhide

Subjects

SQUAMOUS cell carcinoma, SECONDARY primary cancer, LITERATURE reviews, TUMORS, LIPS, THYMOMA

Abstract

The occurrence of second primary tumor (SPT)following malignancy treatment is common. In patients with head and neck (H&N) cancer, SPTs principally occur in the H&N region, lungs or esophagus. Therefore, patient follow-up after cancer treatment is important in order to detect recurrence, metastasis and new primary tumors. However, no standard guidelines on lifelong follow-up imaging are available. Herein, we report a patient who presented with three metachronous primary tumors-squamous cell carcinoma (SCC) of the tongue, SCC of the lip and type A thymoma. The third tumor was incidentally detected during follow-up using contrast-enhanced computed tomography (CT) 9 years following resection of the second tumor. To the best of our knowledge, this specific combination of metachronous tumors has not yet been reported. Based on the literature review, we observed that thymoma occurs following H&N cancer treatment. Therefore, to ensure that the presence of subsequent thymomas is not overlooked, we suggest regular lifelong follow-up using contrast-enhanced CT in patients who had previously been diagnosed with H&N cancer. The literature review revealed that thymomas occur in patients with H&N cancer and should be detected at the earliest convenience. [ABSTRACT FROM AUTHOR]

Published

2019

26. Unraveling 'The Cancer Genome Atlas' information on the role of SLC transporters in anticancer drug uptake.

Author

Al-Abdulla, Ruba, Perez-Silva, Laura, Abete, Lorena, Romero, Marta R., Briz, Oscar, and Marin, Jose J. G.

Subjects

ANTINEOPLASTIC agents, GENOMES, ATLASES, CELL membranes, MOLECULAR weights, RNA splicing

Abstract

Introduction: Anticancer chemotherapy often faces the problem of intrinsic or acquired drug refractoriness due in part to efficient mechanisms of defense present or developed, respectively, in cancer cells. Owing to their polarity and/or high molecular weight, many cytostatic agents cannot freely cross the plasma membrane by simple diffusion and hence depend on SLC proteins to enter cancer cells. The downregulation of these transporters and the appearance of either inactivating mutations or aberrant splicing, hamper the possibility of anticancer drugs to interact with their intracellular targets. Areas covered: In addition to specific literature, we have revised Gene database of the NCBI PubMed resources and information publicly available at NIH 'The Cancer Genome Atlas' (TCGA) (update November 2018) to evaluate the relationship between the profile of expression of SLC transporters playing a major role in the transportome and accounting for drug uptake, in healthy and tumor tissue, and their ability to recognize as substrate several antitumor drugs frequently used in the treatment of different types of cancer, which could affect the overall response to chemotherapy based on regimens including these drugs. Expert commentary: Changes in the transportome may affect the overall response to chemotherapy based on drugs taken up by SLC transporters. [ABSTRACT FROM AUTHOR]

Published

2019

27. A Fragrant Environment Containing α-Pinene Suppresses Tumor Growth in Mice by Modulating the Hypothalamus/ Sympathetic Nerve/Leptin Axis and Immune System.

Author

Masatoshi Kusuhara, Koji Maruyama, Hidee Ishii, Yoko Masuda, Kazutoshi Sakurai, Eiko Tamai, and Kenichi Urakami

Published

2019

28. Influence of transcriptional variants on metastasis.

Author

De Faria Poloni, Joice and Bonatto, Diego

Abstract

Cancer metastasis is defined as the dissemination of malignant cells from the primary tumor site, leading to colonization of distant organs and the establishment of a secondary tumor. Metastasis is frequently associated with chemoresistance and is the major cause of cancer-related mortality. Metastatic cells need to acquire the ability to resist to stresses provided by different environments, such as reactive oxygen species, shear stress, hemodynamic forces, stromal composition, and immune responses, to colonize other tissues. Hence, only a small population of cells has a metastasis-initiating potential. Several studies have revealed the misregulation of transcriptional variants during cancer progression, and many splice events can be used to distinguish between normal and tumoral tissue. These variants, which are abnormally expressed in malignant cells, contribute to an adaptive response of tumor cells and the success of the metastatic cascade, promoting an anomalous cell cycle, cellular adhesion, resistance to death, cell survival, migration and invasion. Understanding the different aspects of splicing regulation and the influence of transcriptional variants that control metastatic cells is critical for the development of therapeutic strategies. In this review, we describe how transcriptional variants contribute to metastatic competence and discuss how targeting specific isoforms may be a promising therapeutic strategy. [ABSTRACT FROM AUTHOR]

Published

2018

29. Variant isoforms of CD44 involves acquisition of chemoresistance to cisplatin and has potential as a novel indicator for identifying a cisplatin-resistant population in urothelial cancer.

Author

Hagiwara, Masayuki, Kikuchi, Eiji, Tanaka, Nobuyuki, Kosaka, Takeo, Mikami, Shuji, Saya, Hideyuki, and Oya, Mototsugu

Subjects

UROTHELIUM, CD44 antigen, CISPLATIN, CANCER chemotherapy, DRUG resistance in cancer cells, CANCER relapse, CANCER

Abstract

Background: Cisplatin is the most commonly used chemotherapeutic agent in the treatment of patients with metastatic and/or recurrent urothelial cancer. However, the effectiveness of these treatments is severely limited due to the development of cisplatin resistance. Cancer stem cells have been documented as one of the key hypotheses involved in chemoresistance. CD44v8-10 has been identified as one of the new cancer stem cells markers and was recently shown to enhance the antioxidant system by interaction with xCT, a subunit of the cystine transporter modulating intracellular glutathione synthesis. The aim of the present study was to investigate the clinical role of CD44v8-10 and the molecular mechanism underlying the acquisition of cisplatin resistance through CD44v8-10 in urothelial cancer.Methods: We analyzed the clinical significance of the immunohistochemical CD44v9 expression, which detects the immunogen of human CD44v8-10, in 77 urothelial cancer patients treated with cisplatin-based systemic chemotherapy for recurrence and/or metastasis. We then evaluated the biological role of CD44v8-10 in the acquisition of cisplatin resistance using the urothelial cancer cell lines, T24 and T24PR, which were generated to acquire resistance to cisplatin.Results: The 5-year cancer-specific survival rate was significantly lower in the CD44v9-positive group than in the CD44v9-negative group (P = 0.008). Multivariate analyses revealed that CD44v9 positivity was an independent risk factor of cancer-specific survival (P = 0.024, hazard ratio = 5.16) in urothelial cancer patients who had recurrence and/or metastasis and received cisplatin-based chemotherapy. The expression of CD44v8-10 and xCT was stronger in T24PR cells than in T24 cells. The amount of intracellular glutathione was significantly higher in T24PR cells than in T24 cells (p < 0.001), and intracellular reactive oxygen species production by cisplatin was lower in T24PR cells than in T24 cells. Furthermore, the knockdown of CD44v8-10 by siRNA led to the recovery of cisplatin sensitivity in T24PR cells.Conclusions: CD44v9 in tumor specimens has potential as a novel indicator for identifying a cisplatin-chemoresistant population among urothelial cancer patients. CD44v8-10 contributes to reactive oxygen species defenses, which are involved in chemoresistance, by promoting the function of xCT, which adjusts the synthesis of glutathione. [ABSTRACT FROM AUTHOR]

Published

2018

30. Apoplexy in Optochiasmatic Cavernous Hemangioma Causing Visual Diminution: A Case Report.

Author

Bansal, Sumit, Suri, Ashish, Suri, Vaishali, and Kakkar, Aanchal

Subjects

CEREBROVASCULAR disease diagnosis, HEMANGIOMAS, OPTIC chiasm, HISTOLOGY, PREOPERATIVE care, NEUROSURGERY, DIAGNOSIS, CANCER

Abstract

This report concerns a woman who presented with abrupt onset of monocular visual symptoms accompanied by an intense holocranial headache, diagnosed as optic chiasm apoplexy caused by a cavernous hemangioma of the optic chiasm. The surgical and histologic findings demonstrated a cavernous hemangioma. The lesion was removed completely without any noticeable bleeding. The preoperative visual deficit improved after surgery. [ABSTRACT FROM AUTHOR]

Published

2016

31. Robot-assisted versus laparoscopic rectal resection for cancer in a single surgeon's experience: a cost analysis covering the initial 50 robotic cases with the da Vinci Si.

Author

Morelli, Luca, Guadagni, Simone, Lorenzoni, Valentina, Di Franco, Gregorio, Cobuccio, Luigi, Palmeri, Matteo, Caprili, Giovanni, D'Isidoro, Cristiano, Moglia, Andrea, Ferrari, Vincenzo, Di Candio, Giulio, Mosca, Franco, and Turchetti, Giuseppe

Subjects

SURGICAL robots, PRIX Pictet, CARCINOGENS, CANCER, TUMORS

Abstract

Purpose: The aim of this study is to compare surgical parameters and the costs of robotic surgery with those of laparoscopic approach in rectal cancer based on a single surgeon's early robotic experience. Methods: Data from 25 laparoscopic (LapTME) and the first 50 robotic (RobTME) rectal resections performed at our institution by an experienced laparoscopic surgeon (>100 procedures) between 2009 and 2014 were retrospectively analyzed and compared. Patient demographic, procedure, and outcome data were gathered. Costs of the two procedures were collected, differentiated into fixed and variable costs, and analyzed against the robotic learning curve according to the cumulative sum (CUSUM) method. Results: Based on CUSUM analysis, RobTME group was divided into three phases (Rob1: 1-19; Rob2: 20-40; Rob3: 41-50). Overall median operative time (OT) was significantly lower in LapTME than in RobTME (270 vs 312.5 min, p = 0.006). A statistically significant change in OT by phase of robotic experience was detected in the RobTME group ( p = 0.010). Overall mean costs associated with LapTME procedures were significantly lower than with RobTME ( p < 0.001). Statistically significant reductions in variable and overall costs were found between robotic phases ( p < 0.009 for both). With fixed costs excluded, the difference between laparoscopic and Rob3 was no longer statistically significant. Conclusions: Our results suggest a significant optimization of robotic rectal surgery's costs with experience. Efforts to reduce the dominant fixed cost are recommended to maintain the sustainability of the system and benefit from the technical advantages offered by the robot. [ABSTRACT FROM AUTHOR]

Published

2016

32. Phosphatases and kinases regulating CDC25 activity in the cell cycle: clinical implications of CDC25 overexpression and potential treatment strategies.

Author

Sur, Swastika and Agrawal, Devendra

Abstract

Alterations in the cell-cycle regulatory genes result in uncontrolled cell proliferation leading to several disease conditions. Cyclin-dependent kinases (CDK) and their regulatory subunit, cyclins, are essential proteins in cell-cycle progression. The activity of CDK is regulated by a series of phosphorylation and dephosphorylation at different amino acid residues. Cell Division Cycle-25 (CDC25) plays an important role in transitions between cell-cycle phases by dephosphorylating and activating CDKs. CDC25B and CDC25C play a major role in G2/M progression, whereas CDC25A assists in G1/S transition. Different isomers of CDC25 expressions are upregulated in various clinicopathological situations. Overexpression of CDC25A deregulates G1/S and G2/M events, including the G2 checkpoint. CDC25B has oncogenic properties. Binding to the 14-3-3 proteins regulates the activity and localization of CDC25B. CDC25C is predominantly a nuclear protein in mammalian cells. At the G2/M transition, mitotic activation of CDC25C protein occurs by its dissociation from 14-3-3 proteins along with its phosphorylation at multiple sites within its N-terminal domain. In this article, we critically reviewed the biology of the activation/deactivation of CDC25 by kinases/phosphatases to maintain the level of CDK-cyclin activities and thus the genomic stability, clinical implications due to dysregulation of CDC25, and potential role of CDC25 inhibitors in diseases. [ABSTRACT FROM AUTHOR]

Published

2016

33. Microenvironment in metastasis: roadblocks and supportive niches.

Author

Pein, Maren and Oskarsson, Thordur

Subjects

METASTASIS, MOLECULAR physics, PATHOLOGY, CELLS, ORGANISMS

Abstract

In many cancers, malignant cells can spread from the primary tumor through blood circulation and initiate metastasis in secondary organs. Metastatic colonization may depend not only on inherent properties of cancer cells, but also on suitable microenvironments in distant sites. Increasing evidence suggests that the nature of the microenvironment may determine the fate of disseminated cancer cells, providing either hindrance or support for cancer cell propagation. This can result in strong selective pressure where the vast majority of cancer cells, invading a secondary organ, are either eliminated or maintained in a dormant state. The ability of cancer cells to fend off or circumvent anti-metastatic signals from the stroma and the capacity to manipulate the local microenvironment towards a supporting environment, a metastatic niche, may be essential for metastatic growth. The molecular interactions between cancer cells and the stroma are still enigmatic, but recent studies are beginning to reveal their nature. Here, we discuss the interactive relationship between metastatic cancer cells and host stroma, involving selection and adaptation of metastasis-initiating cells and host tissue remodeling. Understanding the dynamic and continuously evolving cross talk between metastatic cancer cells and the stroma may be crucial when developing cancer treatments. [ABSTRACT FROM AUTHOR]

Published

2015

34. Periostin Expression and Its Prognostic Value for Colorectal Cancer.

Author

Zewu Li, Xin Zhang, Yongmei Yang, Sanhui Yang, Zhaogang Dong, Lutao Du, Lili Wang, and Chuanxin Wang

Subjects

INTEGRINS, GROWTH factors, METASTASIS, CANCER, PERIOSTIN, PROTEIN expression, IMMUNOHISTOCHEMISTRY

Abstract

Integrin is important for cell growth, invasion and metastasis, which are frequently observed in malignant tumors. The periostin (POSTN) gene encodes the ligand for integrin, one of the key focal adhesion proteins contributing to the formation of a structural link between the extracellular matrix and integrins. High expression levels of the POSTN gene are correlated with numerous human malignancies. We examined POSTN protein in colorectal cancer specimens from 115 patients by strictly following up using immunohistochemistry. Cytoplasm immunohistochemical staining showed POSTN protein expression in colorectal cancers. The positive expression rate of POSTN protein (59.13%, 68/115) in colorectal cancers was significantly higher than that in adjacent normal colon mucosa (0.47%, 11/109). POSTN over-expression in colorectal cancers was positively correlated with tumor size, differentiation, lymph node metastasis, serosal invasion, clinical stage and five-year survival rates. Further analysis showed that patients with advanced stage colorectal cancer and high POSTN expression levels had lower survival rates than those with early stage colorectal cancer and low POSTN expression levels. Overall, our results showed that POSTN played an important role in the progression of colorectal cancers. [ABSTRACT FROM AUTHOR]

Published

2015

35. The Fairy Chemical Imidazole-4-carboxamide Inhibits the Expression of Axl, PD-L1, and PD-L2 and Improves Response to Cisplatin in Melanoma.

Author

Inoue, Chisa, Yasuma, Taro, D'Alessandro-Gabazza, Corina N., Toda, Masaaki, Fridman D'Alessandro, Valeria, Inoue, Ryo, Fujimoto, Hajime, Kobori, Hajime, Tharavecharak, Suphachai, Takeshita, Atsuro, Nishihama, Kota, Okano, Yuko, Wu, Jing, Kobayashi, Tetsu, Yano, Yutaka, Kawagishi, Hirokazu, and Gabazza, Esteban C.

Subjects

IMMUNE checkpoint proteins, PROGRAMMED death-ligand 1, FAIRIES, MELANOMA, ANTINEOPLASTIC agents

Abstract

The leading cause of death worldwide is cancer. Many reports have proved the beneficial effect of mushrooms in cancer. However, the precise mechanism is not completely clear. In the present study, we focused on the medicinal properties of biomolecules released by fairy ring-forming mushrooms. Fairy chemicals generally stimulate or inhibit the growth of surrounding vegetation. In the present study, we evaluated whether fairy chemicals (2-azahypoxanthine, 2-aza-8-oxohypoxanthine, and imidazole-4-carboxamide) exert anticancer activity by decreasing the expression of Axl and immune checkpoint molecules in melanoma cells. We used B16F10 melanoma cell lines and a melanoma xenograft model in the experiments. Treatment of melanoma xenograft with cisplatin combined with imidazole-4-carboxamide significantly decreased the tumor volume compared to untreated mice or mice treated cisplatin alone. In addition, mice treated with cisplatin and imidazole-4-carboxamide showed increased peritumoral infiltration of T cells compared to mice treated with cisplatin alone. In vitro studies showed that all fairy chemicals, including imidazole-4-carboxamide, inhibit the expression of immune checkpoint molecules and Axl compared to controls. Imidazole-4-carboxamide also significantly blocks the cisplatin-induced upregulation of PD-L1. These observations point to the fairy chemical imidazole-4-carboxamide as a promising coadjuvant therapy with cisplatin in patients with cancer. [ABSTRACT FROM AUTHOR]

Published

2022

36. Thymoma and the increased risk of developing extrathymic malignancies: a multicentre study†.

Author

Filosso, Pier Luigi, Galassi, Claudia, Ruffini, Enrico, Margaritora, Stefano, Bertolaccini, Luca, Casadio, Caterina, Anile, Marco, and Venuta, Federico

Subjects

THYMOMA, SURGICAL excision, MYASTHENIA gravis, AUTOIMMUNE diseases, TUMOR risk factors

Abstract

OBJECTIVES Although thymoma is considered a relatively indolent neoplasia, patients affected by this disease are at high risk of developing second tumours (STs). The aim of this study is to assess the risk of developing STs after surgical thymoma resection. METHODS A multicentre retrospective study of patients operated on for thymoma within five Italian Thoracic Surgery Institutions, between 2000 and 2011, was conducted. The overall STs number and incidence were calculated. The number of metachronous STs was compared with the expected cancer number (ECN) in an Italian population, and the standardized incidence ratio (SIR) and 95% confidence intervals were calculated. Potential variables of STs predictors were also evaluated. RESULTS There were 302 patients; myasthenia gravis (MG) was observed in 166 (55%) and other autoimmune syndromes in 49 of them. In 118 patients (39.1%), the Masaoka thymoma stage was greater than II and in 194, the WHO histological type ranged from B1 to C. Fifty STs were observed (28 metachronous, 4 synchronous and 18 detected before thymoma). The observed metachronous STs number was significantly higher than ECN. An increased risk of STs development was observed in advanced stage thymomas and in those with histological high grade. On the contrary, MG seems to be a protective factor in STs development. CONCLUSIONS Our study confirms the high risk of developing STs in patients with thymoma. Aggressive forms of thymoma are those in which this risk appears to be more evident. The central role of an intrinsic immune system alteration might be the key to interpret this phenomenon. [ABSTRACT FROM AUTHOR]

Published

2013

37. Paraneoplastic and non-paraneoplastic autoimmunity to neurons in the central nervous system.

Author

Melzer, Nico, Meuth, Sven, and Wiendl, Heinz

Subjects

PARANEOPLASTIC syndromes, AUTOIMMUNITY, CENTRAL nervous system, IMMUNOTHERAPY, ENCEPHALITIS, CYTOTOXIC T cells, NEUROTRANSMITTER receptors

Abstract

Autoimmune central nervous system (CNS) inflammation occurs both in a paraneoplastic and non-paraneoplastic context. In a widening spectrum of clinical disorders, the underlying adaptive (auto) immune response targets neurons with a divergent role for cellular and humoral disease mechanisms: (1) in encephalitis associated with antibodies to intracellular neuronal antigens, neuronal antigen-specific CD8 T cells seemingly account for irreversible progressive neuronal cell death and neurological decline with poor response to immunotherapy. However, a pathogenic effect of humoral immune mechanisms is also debated. (2) In encephalitis associated with antibodies to synaptic and extrasynaptic neuronal cell surface antigens, potentially reversible antibody-mediated disturbance of synaptic transmission and neuronal excitability occurs in the absence of excessive neuronal damage and accounts for a good response to immunotherapy. However, a pathogenic effect of cellular immune mechanisms is also debated. We provide an overview of entities, clinical hallmarks, imaging features, characteristic laboratory, electrophysiological, cerebrospinal fluid and neuropathological findings, cellular and molecular disease mechanisms as well as therapeutic options in these two broad categories of inflammatory CNS disorders. [ABSTRACT FROM AUTHOR]

Published

2013

38. Matricellular proteins: priming the tumour microenvironment for cancer development and metastasis.

Author

Wong, G S and Rustgi, A K

Subjects

PROTEINS, TUMORS, EXTRACELLULAR matrix proteins, EXTRACELLULAR matrix, CANCER

Abstract

Matricellular proteins have been classified as a family of non-structural matrix proteins capable of modulating a variety of biological processes within the extracellular matrix (ECM). These proteins are expressed dynamically and their cellular functions are highly dependent upon cues from the local environment. Recent studies have shown an increasing appreciation of the key roles these ECM proteins play within the tumour microenvironment. Induced by either tumour cells or tumour stromal components, matricellular proteins initiate downstream signalling events that lead to proliferation, invasion, matrix remodelling and dissemination to pre-metastatic niches in other organs. In this review, we summarise and discuss the current knowledge of the diverse roles these proteins play within the microenvironment that influences tumour progression and potential for future therapies targeting the tumour microenvironment. [ABSTRACT FROM AUTHOR]

Published

2013

39. Ubiquitin C-terminal hydrolase-L1 interacts with adhesion complexes and promotes cell migration, survival, and anchorage independent growth.

Author

Frisan, Teresa, Coppotelli, Giuseppe, Dryselius, Rikard, and Masucci, Mafia G.

Subjects

ADHERENS junctions, ANOIKIS, UBIQUITIN carboxy-terminal hydrolase, CANCER, CELL adhesion, FOCAL adhesion kinase

Abstract

Ubiquitin C-terminal hydrolase-L1 (UCH-L1) is a deubiquitinating enzyme of unknown function that is highly expressed in neurons and overexpressed in several human cancers. UCH-L1 has been implicated in the regulation of phenotypic properties associated with malignant cell growth but the underlying mechanisms have not been elucidated. By comparing cells expressing catalytically active or inactive versions of UCH-L1, we found that the active enzyme enhances cell adhesion, spreading, and migration; inhibits anoikis; and promotes anchorage independent growth. UCH-L1 accumulates at the motile edge of the cell membrane during the initial phases of adhesion, colocalizes with focal adhesion kinase (FAN), p120-catenin, and vinculin, and enhances the formation of focal adhesions, which correlates with enhanced FAK activation. The involvement of UCH-L1 in the regulation of focal adhesions and adherens junctions is supported by coimmunoprecipitation with key components of these complexes, including FAK, paxillin, p120- catenin, β-catenin, and vinculin. UCH-L1 stabilizes focal adhesion signaling in the absence of adhesion, as assessed by reduced caspase-dependent cleavage of FAK following cell detachment and sustained activity of the AKT signaling pathway. These findings offer new insights on the molecular interactions through which the deubiquitinating enzyme regulates the survival, proliferation, and metastatic potential of malignant cells. [ABSTRACT FROM AUTHOR]

Published

2012

40. HDAC inhibitor-based therapies: Can we interpret the code?

Author

New, Maria, Olzscha, Heidi, and La Thangue, Nicholas B.

Subjects

HISTONE deacetylase inhibitors, CANCER treatment, EPIGENETICS, TUMOR growth, CARCINOGENESIS, CHROMATIN, ONCOGENES, NEOVASCULARIZATION

Abstract

Abstract: Abnormal epigenetic control is a common early event in tumour progression, and aberrant acetylation in particular has been implicated in tumourigenesis. One of the most promising approaches towards drugs that modulate epigenetic processes has been seen in the development of inhibitors of histone deacetylases (HDACs). HDACs regulate the acetylation of histones in nucleosomes, which mediates changes in chromatin conformation, leading to regulation of gene expression. HDACs also regulate the acetylation status of a variety of other non-histone substrates, including key tumour suppressor proteins and oncogenes. Histone deacetylase inhibitors (HDIs) are potent anti-proliferative agents which modulate acetylation by targeting histone deacetylases. Interest is increasing in HDI-based therapies and so far, two HDIs, vorinostat (SAHA) and romidepsin (FK228), have been approved for treating cutaneous T-cell lymphoma (CTCL). Others are undergoing clinical trials. Treatment with HDIs prompts tumour cells to undergo apoptosis, and cell-based studies have shown a number of other outcomes to result from HDI treatment, including cell-cycle arrest, cell differentiation, anti-angiogenesis and autophagy. However, our understanding of the key pathways through which HDAC inhibitors affect tumour cell growth remains incomplete, which has hampered progress in identifying malignancies other than CTCL which are likely to respond to HDI treatment. [Copyright &y& Elsevier]

Published

2012

41. The IRF family of transcription factors: Inception, impact and implications in oncogenesis.

Author

Yanai, Hideyuki, Negishi, Hideo, and Taniguchi, Tadatsugu

Subjects

INTERFERON regulatory factors, TRANSCRIPTION factors, CARCINOGENESIS, IMMUNOLOGY, DISEASE susceptibility, CANCER treatment

Abstract

Members of the interferon-regulatory factor (IRF) proteins family were originally identified as transcriptional regulators of the Type I interferon system. Thanks to consistent advances made in our understanding of the immunobiology of innate receptors, it is now clear that several IRFs are critical for the elicitation of innate pattern recognition receptors, and- as a consequence-for adaptive immunity. In addition, IRFs have attracted great attentions as they modulate cellular responses that are involved in tumorigenesis. The regulation of oncogenesis by IRFs has important implications for understanding the host susceptibility to several Types of cancers, their progression, as well as the potential for therapeutic interventions. [ABSTRACT FROM AUTHOR]

Published

2012

42. Brain metastases: pathobiology and emerging targeted therapies.

Author

Preusser, Matthias, Capper, David, Ilhan-Mutlu, Aysegül, Berghoff, Anna, Birner, Peter, Bartsch, Rupert, Marosi, Christine, Zielinski, Christoph, Mehta, Minesh, Winkler, Frank, Wick, Wolfgang, and Deimling, Andreas

Subjects

BRAIN cancer, CANCER patients, THERAPEUTICS, MELANOMA, NEUROENDOCRINE tumors, CANCER invasiveness, LUNG cancer

Abstract

Brain metastases (BM) are common in cancer patients and are associated with high morbidity and poor prognosis, even after intensive multimodal therapy including resection, radiotherapy (stereotactic radiosurgery or whole brain radiotherapy) and chemotherapy. However, advances in the understanding of the pathobiology of BM and the development of molecular targeted agents hold promise for improved prophylaxis and therapy of BM. Here we provide a comprehensive review of the current concepts on mechanisms of the brain-metastatic cascade involving hematogenous dissemination of tumor cells, attachment to microvessel endothelial cells, extravasation into the brain, interaction with the local microenvironment, angiogenesis and intraparenchymal proliferation. Transendothelial migration depends on adhesion molecules such as integrins, selectins and chemokines. Tumor cells invade the brain by degrading extracellular matrix components using heparanase and matrix metalloproteinases. Astrocytes and microglial cells exert not only anti-, but also pro-neoplastic effects on brain-invading tumor cells. Some tumor types (e.g. melanoma) show prominent cooption of preexisting vasculature, while other tumor types (e.g. lung cancer) tend to show early angiogenesis after brain invasion. In this article we also critically summarize the data on currently studied targeted therapeutics in BM especially in the context of recent preclinical data. The most promising agents for BM patients include anti-angiogenic drugs, inhibitors of v-RAF murine sarcoma viral oncogene homolog B1 (BRAF) for BRAF V600E mutated melanoma and inhibitors of epithelial growth factor receptor for non-small cell lung cancer. Molecular analysis of the BRAF V600E status of melanoma BM using DNA-based methods or immunohistochemistry may soon enter the routine neuropathological practice. [ABSTRACT FROM AUTHOR]

Published

2012

43. Why does Jack, and not Jill, break his crown? Sex disparity in brain tumors.

Subjects

BRAIN tumors, SEX factors in disease, SEXUAL dimorphism, CANCER cells, CANCER

Abstract

The article presents a research review on how sex plays a fundamental role in brain tumor biology. It indicates that brain tumors do occur more frequently in males, when compared to females, irrespective of age, tumor histology, or region. The basis for this sex disparity is constituted by sexually dimorphic mechanisms that might control tumor cell biology, and immune and brain microenvironmental responses to cancer.

Published

2012

44. Periostin is up-regulated in high grade and highstage prostate cancer.

Author

Tischler, Verena, Fritzsche, Florian R., Wild, Peter J., Stephan, Carsten, Seifert, Hans-Helge, Riener, Marc-Oliver, Hermanns, Thomas, Mortezavi, Ashkan, Gerhardt, Josefine, Schraml, Peter, Jung, Klaus, Moch, Holger, Soltermann, Alex, and Kristiansen, Glen

Subjects

EPITHELIAL cells, CANCER, PROSTATE cancer, IMMUNOHISTOCHEMISTRY, COHORT analysis

Abstract

Background: Expression of periostin is an indicator of epithelial-mesenchymal transition in cancer but a detailed analysis of periostin expression in prostate cancer has not been conducted so far. Methods: Here, we evaluated periostin expression in prostate cancer cells and peritumoural stroma immunohistochemically in two independent prostate cancer cohorts, including a training cohort (n = 93) and a test cohort (n = 325). Metastatic prostate cancers (n = 20), hormone refractory prostate cancers (n = 19) and benign prostatic tissues (n = 38) were also analyzed. Results: In total, strong epithelial periostin expression was detectable in 142 of 418 (34.0%) of prostate carcinomas and in 11 of 38 benign prostate glands (28.9%). Increased periostin expression in carcinoma cells was significantly associated with high Gleason score (p < 0.01) and advanced tumour stage (p < 0.05) in the test cohort. Whereas periostin expression was weak or absent in the stroma around normal prostate glands, strong periostin expression in tumour stroma was found in most primary and metastatic prostate cancers. High stromal periostin expression was associated with higher Gleason scores (p < 0.001). There was a relationship between stromal periostin expression and shortened PSA relapse free survival times in the training cohort (p < 0.05). Conclusions: Our data indicate that periostin up-regulation is related to increased tumour aggressiveness in prostate cancer and might be a promising target for therapeutical interventions in primary and metastatic prostate cancer. [ABSTRACT FROM AUTHOR]

Published

2010

45. Modified Maximal Thymectomy for Thymic Epithelial Tumors: Predictors of Survival and Neurological Outcome in Patients with Thymomatous Myasthenia Gravis.

Author

Prokakis, Christos, Koletsis, Efstratios, Apostolakis, Efstratios, Zolota, Vasiliki, Chroni, Elisabeth, Baltayiannis, Nikolaos, Chatzimichalis, Antonios, and Dougenis, Dimitrios

Subjects

THYMECTOMY, EPITHELIAL cells, TUMORS, CANCER, RADIOTHERAPY

Abstract

Thymic epithelial tumors are characterized by slow growth and variable malignant behavior. We present our experience on the surgical management of these tumors. We conducted a retrospective analysis of patients with thymomas undergoing modified maximal thymectomy over a period of 16 years. Evaluated parameters included gender, age, Masaoka stage, WHO histology, R0 resection, myasthenia gravis, and adjuvant radiotherapy. In thymoma-associated myasthenia gravis, further analysis was made according the Osserman stage, the time from myasthenia diagnosis to thymectomy, and the steroid treatment. End points were survival for the total study group and achievement of complete stable remission (CSR) in patients with myasthenia gravis. The study group consisted of 15 male and 24 female patients. There was no perioperative mortality. Overall survival was 91.6% and 75.1% at 5 and 10 years. Univariate analysis identified the following predictors of survival: myasthenia ( P < 0.001), Masaoka stage ( P < 0.001), R0 resection ( P < 0.001), and WHO histology ( P = 0.007). Only the WHO histology was an independent predictor of survival in multivariate analysis ( P = 0.003). Myasthenia patients had CSR prediction of 51.9% and 75.9% at 10 and 15 years. Preoperative steroid treatment ( P = 0.007) and WHO histology ( P = 0.021) were independent predictors of CSR on multivariate analysis. Modified maximal thymectomy is safe and efficient in the treatment of thymomas. WHO histology is the prime determinant of tumor aggressiveness and patient survival. Paraneoplastic myasthenia gravis and its outcome after thymectomy is significantly correlated with the WHO classification subtypes; however, lower CSR rates are not necessarily associated with more aggressive histological subgroups. [ABSTRACT FROM AUTHOR]

Published

2009

46. The multifaceted role of periostin in tumorigenesis.

Author

Kai Ruan, Shideng Bao, and Gaoliang Ouyang

Subjects

CARCINOGENESIS, PERIOSTEUM, PERIODONTAL ligament, CANCER, METASTASIS

Abstract

Periostin, also called osteoblast-specific factor 2 (OSF-2), is a member of the fasciclin family and a disulfide-linked cell adhesion protein that has been shown to be expressed preferentially in the periosteum and periodontal ligaments, where it acts as a critical regulator of bone and tooth formation and maintenance. Furthermore, periostin plays an important role in cardiac development. Recent clinical evidence has also revealed that periostin is involved in the development of various tumors, such as breast, lung, colon, pancreatic, and ovarian cancers. Periostin interacts with multiple cell-surface receptors, most notably integrins, and signals mainly via the PI3-K/Akt and other pathways to promote cancer cell survival, epithelial–mesenchymal transition (EMT), invasion, and metastasis. In this review, aspects related to the function of periostin in tumorigenesis are summarized. [ABSTRACT FROM AUTHOR]

Published

2009

47. The regulation of cell proliferation by the papillomavirus early proteins.

Author

Hamid, N. Abdul, Brown, C., and Gaston, K.

Subjects

PAPILLOMAVIRUSES, CELL proliferation, ONCOGENES, CANCER, PROTEINS

Abstract

The human papillomavirus (HPV) E6 and E7 oncogenes have direct effects on host cell proliferation. The viral E2 protein regulates transcription of E6 and E7 and thereby has an indirect effect on cell proliferation. In HPV-induced tumours, misappropriate random integration of the viral genome into the host chromosome often leads to disruption of the E2 gene and the loss of E2 expression. This results in cessation of the virus life cycle and the deregulation of E6 and E7 and is an important step in tumourigenesis. However, prior to these integration events, E2 can interact directly with the E6 and E7 proteins and modulate their activities. E2 also interacts with a variety of host proteins, including the p53 tumour suppressor protein. Here we outline evidence that suggests a role for E2 in the regulation of cell proliferation, and we discuss the importance of this regulation in viral infection and cervical tumourigenesis. [ABSTRACT FROM AUTHOR]

Published

2009

48. Targeting histone deacetylases for the treatment of disease.

Author

Lawless, M. W., Norris, S., O'Byrne, K. J., and Gray, S. G.

Subjects

HISTONE deacetylase, THERAPEUTICS, INFLAMMATION, ENDOPLASMIC reticulum, CANCER treatment, LIVER cancer

Abstract

• Introduction • HATs/HDACs and the pro-inflammatory environment • HATs/HDACs and endoplasmic reticulum (ER) stress • The potential role of histone deacetylase inhibitors in the treatment of cancer - Non-small cell cancer (NSCLC) - In vitro evidence for targeting HDACs in NSCLC - Combinatorial therapies involving HDi in NSCLC - Hepatocellular carcinoma (HCC) - In vitro evidence for the use of HDi in liver cancer - Combinatorial treatments involving HDi in hepatoma • Potential role of histone deacetylase inhibitors in the treatment of diabetes - Disease models, knockouts and assays - Pancreatic islet protection using histone deacetylase inhibitors - Additional in vitro evidence - Stem cells, HDACs and histone deacetylase inhibitors • The potential role of histone deacetylase inhibitors in the treatment of neurodegenerative conditions - Neuronal traits are modulated by HDAC/REST complexes - E2F, HDACs and neuronal survival mechanisms - HDACs play important roles in stem cell neuronal differentiation • Histone deacetylase inhibitors - SAHA (vorinostat) - Phenylbutyrate - Valproic acid - AN-9 - CI-994 - Romidepsin - MS-275 - LBH589 (panobinostat) - MGC D0103 • Caveats - Do HDAC inhibitors target genes or help chaperone activity as their primary response? • Final comments The ‘histone code’ is a well-established hypothesis describing the idea that specific patterns of post-translational modifications to histones act like a molecular ‘code’ recognized and used by non-histone proteins to regulate specific chromatin functions. One modification, which has received significant attention, is that of histone acetylation. The enzymes that regulate this modification are described as lysine acetyltransferases or KATs, and histone deacetylases or HDACs. Due to their conserved catalytic domain HDACs have been actively targeted as a therapeutic target. The pro-inflammatory environment is increasingly being recognized as a critical element for both degenerative diseases and cancer. The present review will discuss the current knowledge surrounding the clinical potential and current development of histone deacetylases for the treatment of diseases for which a pro-inflammatory environment plays important roles, and the molecular mechanisms by which such inhibitors may play important functions in modulating the pro-inflammatory environment. [ABSTRACT FROM AUTHOR]

Published

2009

49. Toward the virtual screening of Cdc25A phosphatase inhibitors with the homology modeled protein structure.

Author

Hwangseo Park and Young Jeon

Subjects

PHOSPHATASES, CHEMICAL inhibitors, CANCER, HYDROGEN bonding, DRUGS

Abstract

Abstract  Cdc25 phosphatases have been considered as attractive drug targets for anticancer therapy due to the correlation of their overexpression with a wide variety of cancers. As a method for the discovery of novel inhibitors of Cdc25 phosphatases, we have evaluated the computer-aided drug design protocol involving the homology modeling of Cdc25A and virtual screening with the two docking tools: FlexX and the modified AutoDock program implementing the effects of ligand solvation in the scoring function. The homology modeling with the X-ray crystal structure of Cdc25B as a template provides a high-quality structure of Cdc25A that enables the structure-based inhibitor design. Of the two docking programs under consideration, AutoDock is found to be more accurate than FlexX in terms of scoring putative ligands. A detailed binding mode analysis of the known inhibitors shows that they can be stabilized in the active site of Cdc25A through the simultaneous establishment of the multiple hydrogen bonds and the hydrophobic interactions. The present study demonstrates the usefulness of the modified AutoDock program as a docking tool for virtual screening of new Cdc25 phosphatase inhibitors as well as for binding mode analysis to elucidate the activities of known inhibitors. Figure Structures and available IC50 values (in μM) of the twenty Cdc25 phosphatase inhibitors seeded in docking library [ABSTRACT FROM AUTHOR]

Published

2008

50. The IRF Family Transcription Factors in Immunity and Oncogenesis.

Author

Tamura, Tomohiko, Yanai, Hideyuki, Savitsky, David, and Taniguchi, Tadatsugu

Subjects

INTERFERONS, GENETIC transcription, CELL differentiation, HEMATOPOIESIS, GENETIC regulation, CELL cycle regulation, DISEASE susceptibility, CANCER

Abstract

The interferon regulatory factor (IRF) family, consisting of nine members in mammals, was identified in the late 1980s in the context of research into the type I interferon system. Subsequent studies over the past two decades have revealed the versatile and critical functions performed by this transcription factor family. Indeed, many IRF members play central roles in the cellular differentiation of hematopoietic cells and in the regulation of gene expression in response to pathogen-derived danger signals. In particular, the advances made in understanding the immunobiology of Toll-like and other pattern-recognition receptors have recently generated new momentum for the study of IRFs. Moreover, the role of several IRF family members in the regulation of the cell cycle and apoptosis has important implications for understanding susceptibility to and progression of several cancers. [ABSTRACT FROM AUTHOR]

Published

2008