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102. Mining the plasma-proteome associated genes in patients with gastro-esophageal cancers for biomarker discovery

Author

Fang-Xiang Wu, Shahid Ahmed, Hongyu Guo, Adnan Zaidi, Andrew Freywald, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, and Lynn Dwernychuk

Subjects
0301 basic medicine, Proteomics, Support Vector Machine, Esophageal Neoplasms, Proteome, Science, Gene Expression, Computational biology, Biology, Article, 03 medical and health sciences, Plasma, 0302 clinical medicine, Text mining, Stomach Neoplasms, Databases, Genetic, medicine, Cancer genomics, Biomarkers, Tumor, Humans, In patient, Gene Regulatory Networks, Biomarker discovery, Gene, Early Detection of Cancer, Cancer, Multidisciplinary, Receiver operating characteristic, business.industry, Gene Expression Profiling, Area under the curve, Reproducibility of Results, medicine.disease, Gene Expression Regulation, Neoplastic, MicroRNAs, 030104 developmental biology, ROC Curve, 030220 oncology & carcinogenesis, Medicine, Neoplasm Recurrence, Local, business, Transcriptome
Abstract

Gastro-esophageal (GE) cancers are one of the major causes of cancer-related death in the world. There is a need for novel biomarkers in the management of GE cancers, to yield predictive response to the available therapies. Our study aims to identify leading genes that are differentially regulated in patients with these cancers. We explored the expression data for those genes whose protein products can be detected in the plasma using the Cancer Genome Atlas to identify leading genes that are differentially regulated in patients with GE cancers. Our work predicted several candidates as potential biomarkers for distinct stages of GE cancers, including previously identified CST1, INHBA, STMN1, whose expression correlated with cancer recurrence, or resistance to adjuvant therapies or surgery. To define the predictive accuracy of these genes as possible biomarkers, we constructed a co-expression network and performed complex network analysis to measure the importance of the genes in terms of a ratio of closeness centrality (RCC). Furthermore, to measure the significance of these differentially regulated genes, we constructed an SVM classifier using machine learning approach and verified these genes by using receiver operator characteristic (ROC) curve as an evaluation metric. The area under the curve measure was > 0.9 for both the overexpressed and downregulated genes suggesting the potential use and reliability of these candidates as biomarkers. In summary, we identified leading differentially expressed genes in GE cancers that can be detected in the plasma proteome. These genes have potential to become diagnostic and therapeutic biomarkers for early detection of cancer, recurrence following surgery and for development of targeted treatment.

Published
2021

105. Dancing with the dead: Eph receptors and their kinase-null partners

Author

Truitt, Luke and Freywald, Andrew

Subjects
Research, Protein kinases -- Research, Tyrosine -- Research, Tyrosine metabolism -- Research, Membrane proteins -- Research
Abstract

Introduction Receptor tyrosine kinases (RTKs) are cell membrane proteins acting upon ligand stimulation as initiation points for cytoplasmic signaling cascades that balance multiple biological responses at both cellular and physiological [...], Eph receptor tyrosine kinases and their ligands, ephrins, are membrane proteins coordinating a wide range of biological functions both in developing embryos and in adult multicellular organisms. Numerous studies have implicated Eph receptors in the induction of opposing responses, including cell adhesion or repulsion, support or inhibition of cell proliferation and cell migration, and progression or suppression of multiple malignancies. Similar to other receptor tyrosine kinases, Eph receptors rely on their ability to catalyze tyrosine phosphorylation for signal transduction. Interestingly, however, Eph receptors also actively utilize three kinase-deficient receptor tyrosine kinases, EphB6, EphA10, and Ryk, in their signaling network. The accumulating evidence suggests that the unusual flexibility of the Eph family, allowing it to initiate antagonistic responses, might be partially explained by the influence of the kinase-dead participants and that the exact outcome of an Eph-mediated action is likely to be defined by the balance between the signaling of catalytically potent and catalytically null receptors. We discuss in this minireview the emerging functions of the kinase-dead EphB6, EphA10, and Ryk receptors both in normal biological responses and in malignancy, and analyze currently available information related to the molecular mechanisms of their action in the context of the Eph family. Key words: receptor tyrosine kinase, Eph family, EphB6, EphA10, Ryk. Les recepteurs Eph a activite tyrosine kinase et leurs ligands, les ephrines, sont des proteines membranaires qui coordonnent un large spectre de fonctions biologiques chez les organismes multicellulaires, tant chez l'embryon en developpement que chez l'adulte. Plusieurs etudes ont implique les recepteurs Eph dans l'induction de reponses opposees, notamment l'adherence et la repulsion cellulaires, la promotion et l'inhibition de la proliferation cellulaire et la migration cellulaire, et la progression et la suppression de plusieurs types de tumeurs malignes. Tout comme les autres recepteurs a activite tyrosine kinase, les recepteurs Eph dependent de leur capacite a catalyser la phosphorylation de residus tyrosine pour remission de signaux. Fait irteressant, trois recepteurs depourvus d'activite tyrosine kinase, EphB6, EphA10 et Ryk, sont activement exploites dans le reseau signaletique. De plus en plus de preuvesconfirment la flexibilite inhabituelle de la famille Eph qui lui permet d'initier des reponses opposees, ce qui pourrait s'expliquer en partie par l'influence des membres depourvus d'activite kinase. Le resultat precis d'une activite initiee par Eph est vraisemblablement defini par la balance de la signalisation des recepteurs catalytiquement actifs et inactifs impliques. Nous discutons dans cette minisynthese des fonctions emergentes des recepteurs depourvus d'activite kinase EphB6, EphA10 et Ryk, dans les reponses biologiques normales et malignes, et nous analysons les informations actuellement disponibles sur les mecanismes moleculaires de leur action dans le contexte de la famille Eph. Mots-cles: recepteur a activite tyrosine kinase, famille Eph, EphB6, EphA10, Ryk. [Traduit par la Redaction]

Published
2011
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107. The EphB6 receptor is overexpressed in pediatric T cell acute lymphoblastic leukemia and increases its sensitivity to doxorubicin treatment

Author

Frederick S. Vizeacoumar, Behzad M. Toosi, Andrew Freywald, Emily J McEwen, Franco J. Vizeacoumar, Amr M. El Zawily, and Tanya Freywald

Subjects
0301 basic medicine, Drug, media_common.quotation_subject, T cell, Lymphoblastic Leukemia, Receptor, EphB6, lcsh:Medicine, Drug resistance, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Article, 03 medical and health sciences, 0302 clinical medicine, EPHB6, medicine, Animals, Humans, Doxorubicin, Receptor, Child, lcsh:Science, Protein kinase B, media_common, Multidisciplinary, Antibiotics, Antineoplastic, business.industry, lcsh:R, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, Heterografts, lcsh:Q, business, medicine.drug
Abstract

While impressive improvements have been achieved in T-ALL therapy, current treatment approaches fail in approximately 25% of patients and these patients have limited treatment options. Another significant group of patients is being overtreated, which causes long-lasting side effects. Identification of molecules controlling drug resistance in T-ALL is crucial for treatment optimisation in both scenarios. We report here the EphB6 receptor is frequently overexpressed in T-ALL. Remarkably, our observations indicate that EphB6 acts in T-ALL cells to enhance sensitivity to a DNA-damaging drug, doxorubicin, as interruption of EphB6 activity interferes with the efficiency of doxorubicin-induced eradication of T-ALL cells in cell culture and in xenograft animals. This effect relies on the protection of Akt kinase signaling, while Akt inhibition combined with doxorubicin application produces synergistic effects on the elimination of EphB6-deficient T-ALL cells. These data imply that EphB6 suppresses T-ALL resistance by interfering with Akt activity. Our observations highlight a novel role for EphB6 in reducing drug resistance of T-ALL and suggest that doxorubicin treatment should produce better results if personalised based on EphB6 levels. If successfully verified in clinical studies, this approach should improve outcomes for T-ALL patients resistant to current therapies and for patients, who are being overtreated.

Published
2017
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108. Hygiene management for long-term ventilated persons in the home health care setting: a scoping review

Author

Isabel Hoeppchen, Carola Walter, Stefanie Berger, Anna Brandauer, Nicole Freywald, Patrick Kutschar, Katharina Maria Lex, Annemarie Strobl, and Irmela Gnass

Subjects
Methicillin-Resistant Staphylococcus aureus, Infection Control, Health Policy, Germany, Humans, Hygiene, Home Care Services
Abstract

Background Evidence and recommendations for hygiene management in home mechanical ventilation (HMV) are rare. In Germany, few regionally limited studies show poor hygiene management or a lack of its implementation. This scoping review of international literature identified the evidence in hygiene management for ventilated patients in the home care setting which has to be implemented for infection prevention and control. Methods A review of international literature was conducted in CINAHL, PubMed and Web of Science. The search focused on four key domains: HMV, hygiene management, home care setting, and methicillin-resistant Staphylococcus aureus (MRSA). Data of included studies were extracted using a data charting sheet. Extracted data were assigned to the categories (1) study description, (2) setting and participants, and (3) hygiene management. Results From 1,718 reviewed articles, n = 8 studies met inclusion criteria. All included studies had a quantitative study design. The approaches were heterogeneous due to different settings, study populations and types of ventilation performed. Regarding aspects of hygiene management, most evidence was found for infectious critical activities (n = 5), quality management for hygiene (n = 4), and training and education (n = 4). This review identified research gaps concerning kitchen hygiene, relatives and visitors of HMV patients, and waste management (n = 0). Discussion Overall evidence was rather scarce. Consequently, this review could not answer all underlying research questions. No evidence was found for measures in hygiene management relating to ventilated patients’ relatives. Evidence for kitchen hygiene, waste management and interaction with relatives is available for inpatient care settings. However, this may not be transferable to outpatient care. Binding legal requirements and audits may help regulate the implementation of HMV hygiene measures. Conclusion Infection control programmes included qualified personnel, hygiene plans, and standards for MRSA and multidrug-resistant organisms (MDRO). The appropriateness of hygiene management measures for outpatient care is the basis for their application in practice.

Published
2021

110. Preface

Author

Behzad M. Toosi, Andrew Freywald, and Franco J. Vizeacoumar

Published
2021
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111. Computational Prediction of Chemical Tools for Identification and Validation of Synthetic Lethal Interaction Networks

Author

Eric W. Price, Christopher P. Phenix, Ran Cao, Frederick S. Vizeacoumar, Franco J. Vizeacoumar, Andrew Freywald, Kalpana Kalyanasundaram Bhanumathy, and Omar Abuhussein

Subjects
Virtual screening, chemistry.chemical_compound, chemistry, Computer science, Chromosome instability, In silico, Synthetic rescue, Identification (biology), Synthetic lethality, Computational biology, Chemical space, Chemical library
Abstract

Cancer is one of the leading causes of death and chromosomal instability (CIN) is a hallmark feature of cancer. CIN, a source of genetic variation in either altered chromosome number or structure contributes to tumor heterogeneity and has become a hot topic in recent years prominently for its role in therapeutic responses. Synthetic lethality and synthetic rescue based approaches, for example, advancing CRISPR-Cas9 platform, are emerging as a powerful strategy to identify new potential targets to selectively eradicate cancer cells. Unfortunately, only few of them are further explored therapeutically due to the difficulty in linking these targets to small molecules for pharmacological intervention. This, however, can be alleviated by the efforts to bring chemical, bioactivity, and genomic data together, as well as established computational approaches. In this chapter, we will discuss some of these advances, including established databases and in silico target-ligand prediction, with the aim to navigate through the synthetically available chemical space to the biologically targetable landscape, and eventually, to the chemical modeling of synthetic lethality and synthetic rescue interactions, that are of great clinical and pharmaceutical relevance and significance.

Published
2021
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113. Th cells promote CTL survival and memory via acquired pMHC-I and endogenous IL-2 and CD40L signaling and by modulating apoptosis-controlling pathways.

Author

Channakeshava Sokke Umeshappa, Yufeng Xie, Shulin Xu, Roopa Hebbandi Nanjundappa, Andrew Freywald, Yulin Deng, Hong Ma, and Jim Xiang

Subjects
Medicine, Science
Abstract

Involvement of CD4(+) helper T (Th) cells is crucial for CD8(+) cytotoxic T lymphocyte (CTL)-mediated immunity. However, CD4(+) Th's signals that govern CTL survival and functional memory are still not completely understood. In this study, we assessed the role of CD4(+) Th cells with acquired antigen-presenting machineries in determining CTL fates. We utilized an adoptive co-transfer into CD4(+) T cell-sufficient or -deficient mice of OTI CTLs and OTII Th cells or Th cells with various gene deficiencies pre-stimulated in vitro by ovalbumin (OVA)-pulsed dendritic cell (DCova). CTL survival was kinetically assessed in these mice using FITC-anti-CD8 and PE-H-2K(b)/OVA257-264 tetramer staining by flow cytometry. We show that by acting via endogenous CD40L and IL-2, and acquired peptide-MHC-I (pMHC-I) complex signaling, CD4(+) Th cells enhance survival of transferred effector CTLs and their differentiation into the functional memory CTLs capable of protecting against highly-metastasizing tumor challenge. Moreover, RT-PCR, flow cytometry and Western blot analysis demonstrate that increased survival of CD4(+) Th cell-helped CTLs is matched with enhanced Akt1/NF-κB activation, down-regulation of TRAIL, and altered expression profiles with up-regulation of prosurvival (Bcl-2) and down-regulation of proapoptotic (Bcl-10, Casp-3, Casp-4, Casp-7) molecules. Taken together, our results reveal a previously unexplored mechanistic role for CD4(+) Th cells in programming CTL survival and memory recall responses. This knowledge could also aid in the development of efficient adoptive CTL cancer therapy.

Published
2013
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114. Characterization of Leading Dysregulated Plasma-Proteome Associated Genes in Patients with Gastro-Esophageal Cancers

Author

Frederick S. Vizeacoumar, Adnan Zaidi, Andrew Freywald, Franco J. Vizeacoumar, Lynn Dwernychuk, and Shahid Ahmed

Subjects
business.industry, Gastro, Proteome, Cancer research, Medicine, In patient, business, Gene
Abstract

Background: Gastro-esophageal cancers are one of the major causes of cancer-related death in the world. There is a need for novel biomarkers in the management of gastro-esophageal cancers to identify new therapeutic targets and to yield predictive response to the available therapies. Our study aims to identify leading genes that are dysregulated (upregulated or downregulated) in patients with gastro-esophageal cancers.Methods: We examined gene expression data for those genes whose protein products can be detected in the plasma in 600 independent tumor samples and 46 matching normal tissue samples using the Cancer Genome Atlas (TCGA) to identify leading genes that are dysregulated in patients with gastro-esophageal cancers. Non-parametric Mann-Whitney-U test was used to evaluate differential expression of genes using a cut-off of P< 0.05.Results: The comparison between tumors sample and healthy tissue showed BIRC5 (p=2.61 E-08), APOC2 (p=3.23E-08), CENPF (p=4.38E-08), STMN1 (p=5.74E-08), and HNRPC (p=8.21E-08) were the leading genes significantly overexpressed in esophageal cancer whereas CST1 (p=3.97 E-21), INHBA (p=9.22E-20), ACAN (p=1.08E-19), HSP90AB1 (p=2.62E-19), and HSPD1 (p=3.91E-19) were the leading genes that were overexpressed in stomach cancer. Conversely, C16orf89 (9.78E-08), AR (1.01E-07), CKB (1.17E-07), ADH1B (1.79E-07), and NCAM1 (2.15E-07) were the leading gene that were significantly downregulated in esophageal cancer whereas GPX3 (1.65E-19), CLEC3B (5.70E-19), CFD (5.68E-18), GSN (4.5IE-17), and CCL14 (1.12E-16) were significantly downregulated in stomach cancer. Furthermore, Stage-based examination showed stage-specific differential expression of various genes as well as stage-wise increasing or decreasing up-regulation or down-regulation of selected genes, respectively. Conclusions: The present study identified leading upregulated and downregulated genes in gastro-esophageal cancers that can be detected in the plasma proteome. These genes have potential to become diagnostic and therapeutic biomarkers for early detection of cancer, recurrence following surgery and for development of targeted-treatment.

Published
2020
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115. Protein Tyrosine Kinases: Their Roles and Their Targeting in Leukemia

Author

Vincenzo Giambra, Andrew Freywald, Franco J. Vizeacoumar, Amrutha Balagopal, Frederick S. Vizeacoumar, and Kalpana Kalyanasundaram Bhanumathy

Subjects
0301 basic medicine, Non-receptor tyrosine kinase, Cancer Research, therapeutic antibodies, Review, lcsh:RC254-282, Receptor tyrosine kinase, 03 medical and health sciences, 0302 clinical medicine, Protein phosphorylation, DDR1, AXL receptor tyrosine kinase, biology, small molecule inhibitor, protein kinase, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, non-receptor tyrosine kinase, leukaemia, Cancer research, biology.protein, receptor tyrosine kinase, Phosphorylation, Tyrosine kinase, Proto-oncogene tyrosine-protein kinase Src
Abstract

Simple Summary Protein phosphorylation is a key regulatory mechanism that controls a wide variety of cellular responses. This process is catalysed by the members of the protein kinase superfamily that are classified into two main families based on their ability to phosphorylate either tyrosine or serine and threonine residues in their substrates. Massive research efforts have been invested in dissecting the functions of tyrosine kinases, revealing their importance in the initiation and progression of human malignancies. Based on these investigations, numerous tyrosine kinase inhibitors have been included in clinical protocols and proved to be effective in targeted therapies for various haematological malignancies. In this review, we provide insights into the role of tyrosine kinases in leukaemia and discuss their targeting for therapeutic purposes with the currently available inhibitory compounds. Abstract Protein kinases constitute a large group of enzymes catalysing protein phosphorylation and controlling multiple signalling events. The human protein kinase superfamily consists of 518 members and represents a complicated system with intricate internal and external interactions. Protein kinases are classified into two main families based on the ability to phosphorylate either tyrosine or serine and threonine residues. Among the 90 tyrosine kinase genes, 58 are receptor types classified into 20 groups and 32 are of the nonreceptor types distributed into 10 groups. Tyrosine kinases execute their biological functions by controlling a variety of cellular responses, such as cell division, metabolism, migration, cell–cell and cell matrix adhesion, cell survival and apoptosis. Over the last 30 years, a major focus of research has been directed towards cancer-associated tyrosine kinases owing to their critical contributions to the development and aggressiveness of human malignancies through the pathological effects on cell behaviour. Leukaemia represents a heterogeneous group of haematological malignancies, characterised by an uncontrolled proliferation of undifferentiated hematopoietic cells or leukaemia blasts, mostly derived from bone marrow. They are usually classified as chronic or acute, depending on the rates of their progression, as well as myeloid or lymphoblastic, according to the type of blood cells involved. Overall, these malignancies are relatively common amongst both children and adults. In malignant haematopoiesis, multiple tyrosine kinases of both receptor and nonreceptor types, including AXL receptor tyrosine kinase (AXL), Discoidin domain receptor 1 (DDR1), Vascular endothelial growth factor receptor (VEGFR), Fibroblast growth factor receptor (FGFR), Mesenchymal–epithelial transition factor (MET), proto-oncogene c-Src (SRC), Spleen tyrosine kinase (SYK) and pro-oncogenic Abelson tyrosine-protein kinase 1 (ABL1) mutants, are implicated in the pathogenesis and drug resistance of practically all types of leukaemia. The role of ABL1 kinase mutants and their therapeutic inhibitors have been extensively analysed in scientific literature, and therefore, in this review, we provide insights into the impact and mechanism of action of other tyrosine kinases involved in the development and progression of human leukaemia and discuss the currently available and emerging treatment options based on targeting these molecules.

Published
2020

117. Transgene IL-21-Engineered T Cell-Based Vaccine Potently Converts CTL Exhaustion via the Activation of the mTORC1 Pathway in Chronic Infection

Author

Jim Xiang, Suresh K. Tikoo, Aizhang Xu, Xueying Zhang, Andrew Freywald, Changyu Zheng, and Rajni Chibbar

Subjects
business.industry, Transgene, T cell, respiratory system, Virus, CTL, Chronic infection, medicine.anatomical_structure, Immunity, Immunology, Medicine, Cytotoxic T cell, business, T-cell vaccine
Abstract

CD8+ cytotoxic T lymphocyte (CTL) exhaustion is one of the major obstacles for the effectiveness of virus control in chronic infectious diseases. We previously generated novel ovalbumin (OVA)-specific 41BBL-expressing OVA-TEXO and human immunodeficiency virus (HIV-1) Gag-specific Gag-TEXO vaccines, inducing therapeutic immunity in wild-type C57BL/6 (B6) mice, and converting CTL exhaustion in recombinant OVA-specific adenovirus AdVOVA-infected B6 (AdVOVA-B6) mice with chronic infection. IL-21 cytokine plays an important role in controlling chronic infections. Therefore, in this study, we constructed recombinant transgene IL-21-expressing AdVIL-21, and generated IL-21-expressing OVA-TEXO/IL-21 and Gag-TEXO/IL21 vaccines, or control vaccines (OVA-TEXO/Null and Gag-TEXO/Null) by infecting OVA-TEXO and Gag-TEXO cells with AdVIL-21 or the control AdVNull, lacking transgene, and assessed their effects in B6 or AdVOVA-B6 mice. We demonstrate that both OVA-TEXO/IL-21 and control OVA-TEXO/Null vaccines are capable of converting CTL exhaustion in chronic infection. However, the OVA-TEXO/IL-21 vaccine more efficiently rescues exhausted CTLs by increasing stronger CTL proliferation and effector cytokine IFN-γ expression than the control OVA-TEXO/Null vaccine in AdVOVA-B6 mice with chronic infection, though both vaccines stimulated comparable OVA-specific CTL responses and protective immunity against OVA-expressing BL6-10OVA melanoma lung metastasis in wild-type B6 mice. In vivo, the OVA-TEXO/IL-21-stimulated CTLs more efficiently up-regulate phosphorylation of mTORC1-controlled EIF4E and expression of mTORC1- regulated T-bet molecule than the control OVA-TEXO/Null-stimulated ones. Importantly, the Gag-TEXO/IL21 vaccine induces stronger Gag-specific therapeutic immunity against established Gag-expressing BL6-10Gag melanoma lung metastases than the control Gag-TEXO/Null vaccine in chronic infection. Therefore, this study should have a strong impact on developing new therapeutic vaccines for patients with chronic infections.

Published
2019
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118. CD154 and IL-2 signaling of CD4+ T cells play a critical role in multiple phases of CD8+ CTL responses following adenovirus vaccination.

Author

Channakeshava Sokke Umeshappa, Roopa Hebbandi Nanjundappa, Yufeng Xie, Andrew Freywald, Yulin Deng, Hong Ma, and Jim Xiang

Subjects
Medicine, Science
Abstract

Adenoviral (AdV) vectors represent most commonly utilized viral vaccines in clinical studies. While the role of CD8(+) cytotoxic T lymphocyte (CTL) responses in mediating AdV-induced protection is well understood, the involvement of CD4(+) T cell-provided signals in the development of functional CD8(+) CTL responses remain unclear. To explore CD4(+) T helper signals required for AdVova-stimulated CTL responses, we established an adoptive transfer system by transferring CD4(+) T cells derived from various knock out and transgenic mice into wild-type and/or CD4-deficient animals, followed by immunizing with recombinant ovalbumin (OVA)-expressing AdVova vector. Without CD4(+) T help, both primary and memory CTL responses were greatly reduced in this model, and were associated with increased PD-1 expression. The provision of OVA-specific CD4(+) T help in CD4(+) T cell-deficient mice restored AdVova-induced primary CTL responses, and supported survival and recall responses of AdVova-stimulated memory CTLs. These effects were specifically mediated by CD4(+) T cell-produced IL-2 and CD154 signals. Adoptive transfer of "helped" or "unhelped" effector and memory CTLs into naïve CD4(+) T cell-deficient or -sufficient mice also revealed an additional role for polyclonal CD4(+) T cell environment in the survival of AdVova-stimulated CTLs, partially explaining the extension of CTL contraction phase. Finally, during recall responses, CD4(+) T cell environment, particularly involving memory CD4(+) T cells, greatly enhanced expansion of memory CTLs. Collectively, our data strongly suggest a critical role for CD4(+) T help in multiple phases of AdV-stimulated CTL responses, and could partially explain certain failures in AdV-based immunization trials targeting malignant tumors and chronic diseases that are often associated with compromised CD4(+) T cell population and function.

Published
2012
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119. Molecular characterization of an MLL1 fusion and its role in chromosomal instability

Author

Sreejit Parameswaran, Keith Bonham, Hui Li, Darrell D. Mousseau, Kalpana Kalyanasundaram Bhanumathy, M. F. Islam, Frederick S. Vizeacoumar, Chelsea E. Cunningham, Peter C. Stirling, Maruti Uppalapati, Behzad M. Toosi, Yuliang Wu, Andrew Freywald, Franco J. Vizeacoumar, and Fujun Qin

Subjects
0301 basic medicine, Cancer Research, chromosomal rearrangement, chromosomal instability, Oncogene Proteins, Fusion, Carcinogenesis, Recombinant Fusion Proteins, Cell Cycle Proteins, Chromosomal rearrangement, lcsh:RC254-282, Models, Biological, 03 medical and health sciences, Chimera (genetics), 0302 clinical medicine, Cancer stem cell, Chromosome instability, tumor heterogeneity, Genetics, medicine, Biomarkers, Tumor, Humans, Gene Regulatory Networks, Oncogene Fusion, Research Articles, biology, Base Sequence, CD44, Nuclear Proteins, RNA-Binding Proteins, General Medicine, DOT1L, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, HCT116 Cells, Fusion protein, 3. Good health, Clone Cells, Leukemia, 030104 developmental biology, Phenotype, Oncology, mitotic checkpoint, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Molecular Medicine, fusion proteins, Myeloid-Lymphoid Leukemia Protein, Research Article
Abstract

Chromosomal rearrangements involving the mixed-lineage leukemia (MLL1) gene are common in a unique group of acute leukemias, with more than 100 fusion partners in this malignancy alone. However, do these fusions occur or have a role in solid tumors? We performed extensive network analyses of MLL1-fusion partners in patient datasets, revealing that multiple MLL1-fusion partners exhibited significant interactions with the androgen-receptor signaling pathway. Further exploration of tumor sequence data from TCGA predicts the presence of MLL1 fusions with truncated SET domain in prostate tumors. To investigate the physiological relevance of MLL1 fusions in solid tumors, we engineered a truncated version of MLL1 by fusing it with one of its known fusion partners, ZC3H13, to use as a model system. Functional characterization with cell-based assays revealed that MLL1-ZC3H13 fusion induced chromosomal instability, affected mitotic progression, and enhanced tumorsphere formation. The MLL1-ZC3H13 chimera consistently increased the expression of a cancer stem cell marker (CD44); in addition, we detected potential collateral lethality between DOT1L and MLL1 fusions. Our work reveals that MLL1 fusions are likely prevalent in solid tumors and exhibit a potential pro-tumorigenic role.

Published
2018

125. The intrinsically kinase-inactive EPHB6 receptor predisposes cancer cells to DR5-induced apoptosis by promoting mitochondrial fragmentation

Author

Vijaya Indukuri, Amr M. El Zawily, Andrew Freywald, Franco J. Vizeacoumar, Behzad M. Toosi, Scot C. Leary, and Tanya Freywald

Subjects
Dynamins, 0301 basic medicine, MAP Kinase Signaling System, Apoptosis, Triple Negative Breast Neoplasms, DRP1, Receptor tyrosine kinase, GTP Phosphohydrolases, Mitochondrial Proteins, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, EPHB6, Humans, cancer, Medicine, DR5, Receptors, Eph Family, biology, Kinase, business.industry, Erythropoietin-producing hepatocellular (Eph) receptor, Cancer, Organelle fission, medicine.disease, mitochondrial dynamics, Mitochondria, 3. Good health, Receptors, TNF-Related Apoptosis-Inducing Ligand, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer cell, Immunology, biology.protein, Cancer research, business, Microtubule-Associated Proteins, Research Paper
Abstract

// Amr M. El Zawily 1, 2 , Behzad M. Toosi 1 , Tanya Freywald 3 , Vijaya V. Indukuri 4 , Franco J. Vizeacoumar 1, 3 , Scot C. Leary 4 , Andrew Freywald 1 1 Department of Pathology and Laboratory Medicine, College of Medicine, University of Saskatchewan, Royal University Hospital, Saskatoon, SK, S7N 0W8, Canada 2 Faculty of Science, Damanhour University, Damanhour, 22516, Egypt 3 Cancer Research, Saskatchewan Cancer Agency, Saskatoon, SK, S7N 5E5, Canada 4 Department of Biochemistry, College of Medicine, University of Saskatchewan, Saskatoon, SK, S7N 5E5, Canada Correspondence to: Andrew Freywald, email: andrew.freywald@usask.ca Scot C. Leary, email: scot.leary@usask.ca Keywords: EPHB6, DRP1, mitochondrial dynamics, cancer, DR5 Received: August 19, 2016 Accepted: October 12, 2016 Published: October 24, 2016 ABSTRACT Death Receptor 5 (DR5) is a promising target for cancer therapy due to its ability to selectively induce apoptosis in cancer cells. However, the therapeutic usefulness of DR5 agonists is currently limited by the frequent resistance of malignant tumours to its activation. The identification of molecular mechanisms that determine outcomes of DR5 action is therefore crucial for improving the efficiency of DR5-activating reagents in cancer treatment. Here, we provide evidence that an intrinsically kinase-inactive member of the Eph group of receptor tyrosine kinases, EPHB6, induces marked fragmentation of the mitochondrial network in breast cancer cells of triple-negative origin, lacking expression of the estrogen, progesterone and HER2 receptors. Remarkably, this response renders cancer cells more susceptible to DR5-mediated apoptosis. EPHB6 action in mitochondrial fragmentation proved to depend on its ability to activate the ERK-DRP1 pathway, which increases the frequency of organelle fission. Moreover, DRP1 activity is also essential to the EPHB6-mediated pro-apoptotic response that we observe in the context of DR5 activation. These findings provide the first description of a member of the receptor tyrosine kinase family capable of producing a pro-apoptotic effect through the activation of ERK-DRP1 signaling and subsequent mitochondrial fragmentation. Our observations are of potential practical importance, as they imply that DR5-activating therapeutic approaches should be applied in a more personalized manner to primarily treat EPHB6-expressing tumours. Finally, our findings also suggest that the EPHB6 receptor itself may represent a promising target for cancer therapy, since EPHB6 and DR5 co-activation should support more efficient elimination of cancer cells.

Published
2016
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126. Targeting synthetic lethality between the SRC kinase and the EPHB6 receptor may benefit cancer treatment

Author

Yue Li, Courtney Gerger, Behzad M. Toosi, Frederick S. Vizeacoumar, Rani Kanthan, Amr M. El Zawily, Darrell D. Mousseau, Kalpana Kalyanasundaram Bhanumathy, James M. Paul, Tanya Freywald, Deborah H. Anderson, Franco J. Vizeacoumar, Zhaolei Zhang, and Andrew Freywald

Subjects
0301 basic medicine, Gerontology, Oncology, Indoles, Pyridines, Triple Negative Breast Neoplasms, Synthetic lethality, Mice, SCID, Receptor tyrosine kinase, chemistry.chemical_compound, Mice, 0302 clinical medicine, Mice, Inbred NOD, genetic interaction, Acetamides, EPHB6, Medicine, RNA, Small Interfering, Sulfonamides, biology, Cell Death, Immunohistochemistry, 3. Good health, Gene Expression Regulation, Neoplastic, src-Family Kinases, SU6656, 030220 oncology & carcinogenesis, SRC kinase, Female, Proto-oncogene tyrosine-protein kinase Src, Research Paper, medicine.medical_specialty, Morpholines, Breast Neoplasms, 03 medical and health sciences, Breast cancer, breast cancer, Internal medicine, Cell Line, Tumor, Animals, Humans, Fluorescent Dyes, Receptors, Eph Family, business.industry, Gene Expression Profiling, Cell Membrane, Cancer, medicine.disease, Xenograft Model Antitumor Assays, synthetic lethality, 030104 developmental biology, chemistry, Cancer cell, biology.protein, business, Synthetic Lethal Mutations, Genome-Wide Association Study
Abstract

// James M. Paul 1, * , Behzad Toosi 2, * , Frederick S. Vizeacoumar 2, * , Kalpana Kalyanasundaram Bhanumathy 2 , Yue Li 3, 4, 5 , Courtney Gerger 2 , Amr El Zawily 2, 6 , Tanya Freywald 7 , Deborah H. Anderson 7 , Darrell Mousseau 8 , Rani Kanthan 2 , Zhaolei Zhang 3, 4 , Franco J. Vizeacoumar 2, 7 , Andrew Freywald 2 1 Department of Biochemistry, University of Saskatchewan, Saskatoon, SK, S7N 5E5, Canada 2 Department of Pathology and Laboratory Medicine, College of Medicine, University of Saskatchewan, Royal University Hospital, Saskatoon, SK, S7N 0W8, Canada 3 Department of Computer Science, University of Toronto, Toronto, ON, M5S 3G4, Canada 4 The Donnelly Centre, University of Toronto, Toronto, ON, M5S 3E1, Canada 5 Present address: Computer Science and Artificial Intelligence Laboratory, Massachusetts Institute of Technology, Cambridge, MA, 02139, USA 6 Faculty of Science, Damanhour University, Damanhour, 22516, Egypt 7 Cancer Research, Saskatchewan Cancer Agency, Saskatoon, SK, S7N 5E5, Canada 8 Cell Signaling Laboratory, Neuroscience Cluster, University of Saskatchewan, Saskatoon, SK, S7N 5E5, Canada * These authors contributed equally to this work Correspondence to: Franco J. Vizeacoumar, email: franco.vizeacoumar@usask.ca Andrew Freywald, email: andrew.freywald@usask.ca Keywords: breast cancer, genetic interaction, synthetic lethality, EPHB6, SRC kinase Received: April 22, 2016 Accepted: June 17, 2016 Published: July 13, 2016 ABSTRACT Application of tumor genome sequencing has identified numerous loss-of-function alterations in cancer cells. While these alterations are difficult to target using direct interventions, they may be attacked with the help of the synthetic lethality (SL) approach. In this approach, inhibition of one gene causes lethality only when another gene is also completely or partially inactivated. The EPHB6 receptor tyrosine kinase has been shown to have anti-malignant properties and to be downregulated in multiple cancers, which makes it a very attractive target for SL applications. In our work, we used a genome-wide SL screen combined with expression and interaction network analyses, and identified the SRC kinase as a SL partner of EPHB6 in triple-negative breast cancer (TNBC) cells. Our experiments also reveal that this SL interaction can be targeted by small molecule SRC inhibitors, SU6656 and KX2-391, and can be used to improve elimination of human TNBC tumors in a xenograft model. Our observations are of potential practical importance, since TNBC is an aggressive heterogeneous malignancy with a very high rate of patient mortality due to the lack of targeted therapies, and our work indicates that FDA-approved SRC inhibitors may potentially be used in a personalized manner for treating patients with EPHB6-deficient TNBC. Our findings are also of a general interest, as EPHB6 is downregulated in multiple malignancies and our data serve as a proof of principle that EPHB6 deficiency may be targeted by small molecule inhibitors in the SL approach.

Published
2016

127. Promoter analysis of the gene encoding the [beta]-subunit of the rat amiloride-sensitive epithelial sodium channel

Author

Bremner, Harry Robert, Freywald, Tanya, O'Brodovich, Hugh M., and Otulakowski, Gail

Subjects
Physiology -- Research, Sodium channels -- Genetic aspects, Gene expression -- Research, Biological sciences
Abstract

Promoter analysis of the gene encoding the [beta]-subunit of the rat amiloride-sensitive epithelial sodium channel. Am J Physiol Lung Cell Mol Physiol 282: L124-L134, 2002.--The amiloride-sensitive epithelial [Na.sup.+] channel (ENaC), found in the apical membrane of [Na.sup.+]-absorptive epithelia, is made up of three differentially regulated subunits: [alpha], [beta] and [gamma]. We undertook a study of the 5'-end of the gene encoding the [beta]-ENaC subunit in the rat. 5'-Rapid amplification of cDNA ends and RNase protection assays indicated multiple transcription start sites over a 50-bp region. Sequencing 1.3 kb of the 5'-flanking DNA revealed putative binding sites for PEA3, Sp1, activator protein (AP)-1 and Oct-1 but neither a TATA box nor consensus sites for steroid hormone receptor binding. Transient transfections of reporter constructs driven by [beta]-ENaC 5'- flanking DNA in the representative epithelial cell lines Madin-Darby canine kidney, MLE-15, and Caco-2 revealed a negative element present between positions - 424 and - 311 that affected basal transcription rates. Gel shift assays showed protein-DNA binding activity of an AP-1 consensus site in this region; however, mutation of the AP-1 site did not abrogate the repressive activity of the region in transient transfections. Deletion of two clusters of Sp1 consensus binding sites between -1 and -51 bp and between -169 and -211 bp indicated that the proximal cluster was essential to basal promoter activity in transfected cell lines. In a comparison of these data with those in published studies on [alpha]- and [gamma]-ENaC promoters, the [beta]- and [gamma]-subunit promoters appear to be more similar to each other than to the [alpha]-promoter. ion transport; Sp1; transcription; gene expression

Published
2002

132. The CINs of Polo-Like Kinase 1 in Cancer

Author

Cunningham, Chelsea E., primary, MacAuley, Mackenzie J., additional, Vizeacoumar, Frederick S., additional, Abuhussein, Omar, additional, Freywald, Andrew, additional, and Vizeacoumar, Franco J., additional

Published
2020
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133. Heterologous human/rat HER2-specific exosome-targeted T cell vaccine stimulates potent humoral and CTL responses leading to enhanced circumvention of HER2 tolerance in double transgenic HLA-A2/HER2 mice

Author

Aizhang Xu, Yufeng Xie, Shahid Ahmeqd, Jim Xiang, Andrew Freywald, Changyu Zheng, Amer Sami, Rajni Chibbar, and Jie Wu

Subjects
Cytotoxicity, Immunologic, 0301 basic medicine, Receptor, ErbB-2, Recombinant Fusion Proteins, T-Lymphocytes, Transgene, Genetic Vectors, Heterologous, Breast Neoplasms, Mice, Transgenic, Exosomes, Cancer Vaccines, Cell Line, Viral vector, DNA vaccination, Mice, 03 medical and health sciences, 0302 clinical medicine, Gene Order, HLA-A2 Antigen, Immune Tolerance, Animals, Humans, skin and connective tissue diseases, neoplasms, Immunity, Cellular, General Veterinary, General Immunology and Microbiology, biology, Chemistry, Public Health, Environmental and Occupational Health, Transfection, Xenograft Model Antitumor Assays, Molecular biology, Immunity, Humoral, Rats, Disease Models, Animal, 030104 developmental biology, Infectious Diseases, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, Female, Antibody, Immunologic Memory, T-cell vaccine, CD8
Abstract

DNA vaccines composed of heterologous human HER2 and rat neu sequences induce stronger antibody response and protective antitumor immunity than either HER2 or neu DNA vaccines in transgenic mice. We previously developed HER2-specific exosome-targeted T-cell vaccine HER2-T EXO capable of stimulating HER2-specific CD8 + T-cell responses, but only leading to partial protective immunity in double-transgenic HLA-A2/HER2 mice with self-immune tolerance to HER2. Here, we constructed an adenoviral vector AdV HuRt expressing HuRt fusion protein composed of NH 2 -HER2 1-407 (Hu) and COOH-neu 408-690 (Rt) fragments, and developed a heterologous human/rat HER2-specific exosome-targeted T-cell vaccine HuRt-T EXO using polyclonal CD4 + T-cells uptaking exosomes released by AdV HuRt -transfected dendritic cells. We found that the HuRt-T EXO vaccine stimulates enhanced CD4 + T-cell responses leading to increased induction of HER2-specific antibody (∼70 µg/ml) compared to that (∼40 µg/ml) triggered by the homologous HER2-T EXO vaccine. By using PE-H-2K d /HER2 23-71 tetramer, we determined that HuRt-T EXO stimulates stronger HER2-specific CD8 + T-cell responses eradicating 90% of HER2-specific target cells, while HER2-T EXO -induced CD8 + T-cell responses only eliminating 53% targets. Furthermore, HuRt-T EXO , but not HER2-T EXO vaccination, is capable of suppressing early stage-established HER2-expressing 4T1 HER2 breast cancer in its lung metastasis or subcutaneous form in BALB/c mice, and of completely protecting transgenic HLA-A2/HER2 mice from growth of HLA-A2/HER2-expressing BL6-10 A2/HER2 melanoma. HuRt-T EXO -stimulated HER2-specific CD8 + T-cells not only are cytolytic to trastuzumab-resistant HLA-A2/HER2-expressing BT474/A2 breast tumor cells in vitro but also eradicates pre-established BT474/A2 tumors in athymic nude mice. Therefore, our novel heterologous human/rat HER2-specific T-cell vaccine HuRt-T EXO, circumventing HER2 tolerance, may provide a new therapeutic alternative for patients with trastuzumab-resistant HER2 + breast tumor.

Published
2018
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134. Simulated microgravity inhibits cell focal adhesions leading to reduced melanoma cell proliferation and metastasis via FAK/RhoA-regulated mTORC1 and AMPK pathways

Author

Yulin Deng, Tuo Zhao, Qin Zhao, Cuihong Fan, Jun Zhang, Xin Tan, Jim Xiang, Harald Genth, Andrew Freywald, and Aizhang Xu

Subjects
0301 basic medicine, RHOA, Integrin, lcsh:Medicine, RAC1, CDC42, mTORC1, AMP-Activated Protein Kinases, Mechanistic Target of Rapamycin Complex 1, Article, Focal adhesion, Mice, 03 medical and health sciences, 0302 clinical medicine, stomatognathic system, Cell Line, Tumor, Animals, Neoplasm Metastasis, lcsh:Science, Melanoma, Cytoskeleton, Weightlessness Simulation, Cell Proliferation, Focal Adhesions, Multidisciplinary, biology, Cell growth, Chemistry, lcsh:R, AMPK, NAD, Mitochondria, Cell biology, Enzyme Activation, 030104 developmental biology, Focal Adhesion Kinase 1, 030220 oncology & carcinogenesis, biology.protein, lcsh:Q, rhoA GTP-Binding Protein, Glycolysis, Signal Transduction
Abstract

Simulated microgravity (SMG) was reported to affect tumor cell proliferation and metastasis. However, the underlying mechanism is elusive. In this study, we demonstrate that clinostat-modelled SMG reduces BL6-10 melanoma cell proliferation, adhesion and invasiveness in vitro and decreases tumor lung metastasis in vivo. It down-regulates metastasis-related integrin α6β4, MMP9 and Met72 molecules. SMG significantly reduces formation of focal adhesions and activation of focal adhesion kinase (FAK) and Rho family proteins (RhoA, Rac1 and Cdc42) and of mTORC1 kinase, but activates AMPK and ULK1 kinases. We demonstrate that SMG inhibits NADH induction and glycolysis, but induces mitochondrial biogenesis. Interestingly, administration of a RhoA activator, the cytotoxic necrotizing factor-1 (CNF1) effectively converts SMG-triggered alterations and effects on mitochondria biogenesis or glycolysis. CNF1 also converts the SMG-altered cell proliferation and tumor metastasis. In contrast, mTORC inhibitor, rapamycin, produces opposite responses and mimics SMG-induced effects in cells at normal gravity. Taken together, our observations indicate that SMG inhibits focal adhesions, leading to inhibition of signaling FAK and RhoA, and the mTORC1 pathway, which results in activation of the AMPK pathway and reduced melanoma cell proliferation and metastasis. Overall, our findings shed a new light on effects of microgravity on cell biology and human health.

Published
2018
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135. CD8+ memory T-cell inflation renders compromised CD4+ T-cell-dependent CD8+ T-cell immunity via naïve T-cell anergy

Author

Xu A, Freywald A, Xie Y, Li Z, and Xiang J

Subjects
T cell anergy, lcsh:Immunologic diseases. Allergy, Lymphopenia, memory T cell inflation, defective immunity, lcsh:RC581-607, T cell proliferation
Abstract

Aizhang Xu,1,2 Andrew Freywald,3 Yufeng Xie,4 Zejun Li,5 Jim Xiang1,2 1Cancer Research Cluster, Saskatchewan Cancer Agency, 2Department of Oncology, 3Department of Pathology, University of Saskatchewan, Saskatoon, SK, Canada; 4Department of Oncology, First Affiliated Hospital, Soochow University, Suzhou, 5Shanghai Veterinary Research Institute, Shanghai, China Abstract: Whether inflation of CD8+ memory T (mT) cells, which is often derived from repeated prime-boost vaccinations or chronic viral infections in the elderly, would affect late CD8+ T-cell immunity is a long-standing paradox. We have previously established an animal model with mT-cell inflation by transferring ConA-stimulated monoclonal CD8+ T cells derived from Ova-specific T-cell-receptor transgenic OTI mice into irradiation-induced lymphopenic B6 mice. In this study, we also established another two animal models with mT-cell inflation by transferring, 1) ConA-stimulated monoclonal CD8+ T cells derived from lymphocytic choriomeningitis virus glycoprotein-specific T-cell-receptor transgenic P14 mice, and 2) ConA-stimulated polyclonal CD8+ T cells derived from B6.1 mice into B6 mice with irradiation-induced lymphopenia. We vaccinated these mice with recombinant Ova-expressing Listeria monocytogenes and Ova-pulsed dendritic cells, which stimulated CD4+ T cell-independent and CD4+ T-cell-dependent CD8+ T-cell responses, respectively, and assessed Ova-specific CD8+ T-cell responses by flow cytometry. We found that Ova-specific CD8+ T-cell responses derived from the latter but not the former vaccination were significantly reduced in mice with CD8+ mT-cell inflation compared to wild-type B6 mice. We determined that naïve CD8+ T cells purified from splenocytes of mice with mT-cell inflation had defects in cell proliferation upon stimulation in vitro and in vivo and upregulated T-cell anergy-associated Itch and GRAIL molecules. Taken together, our data reveal that CD8+ mT-cell inflation renders compromised CD4+ T-cell-dependent CD8+ T-cell immunity via naïve T-cell anergy, and thus show promise for the design of efficient vaccines for elderly patients with CD8+ mT-cell inflation. Keywords: lymphopenia, memory T-cell inflation, defective immunity, T-cell proliferation, T-cell anergy

Published
2017

136. CD8+ memory T-cell inflation renders compromised CD4+ T-cell-dependent CD8+ T-cell immunity via naïve T-cell anergy

Author

Zejun Li, Jim Xiang, Yufeng Xie, Aizhang Xu, and Andrew Freywald

Subjects
Naive T cell, Immunology, Biology, Lymphocytic choriomeningitis, medicine.disease, medicine.anatomical_structure, Immunity, Monoclonal, medicine, Splenocyte, Immunology and Allergy, Cytotoxic T cell, Memory T cell, CD8
Abstract

Whether inflation of CD8+ memory T (mT) cells, which is often derived from repeated prime-boost vaccinations or chronic viral infections in the elderly, would affect late CD8+ T-cell immunity is a long-standing paradox. We have previously established an animal model with mT-cell inflation by transferring ConA-stimulated monoclonal CD8+ T cells derived from Ova-specific T-cell-receptor transgenic OTI mice into irradiation-induced lymphopenic B6 mice. In this study, we also established another two animal models with mT-cell inflation by transferring, 1) ConA-stimulated monoclonal CD8+ T cells derived from lymphocytic choriomeningitis virus glycoprotein-specific T-cell-receptor transgenic P14 mice, and 2) ConA-stimulated polyclonal CD8+ T cells derived from B6.1 mice into B6 mice with irradiation-induced lymphopenia. We vaccinated these mice with recombinant Ova-expressing Listeria monocytogenes and Ova-pulsed dendritic cells, which stimulated CD4+ T cell-independent and CD4+ T-cell-dependent CD8+ T-cell responses, respectively, and assessed Ova-specific CD8+ T-cell responses by flow cytometry. We found that Ova-specific CD8+ T-cell responses derived from the latter but not the former vaccination were significantly reduced in mice with CD8+ mT-cell inflation compared to wild-type B6 mice. We determined that naive CD8+ T cells purified from splenocytes of mice with mT-cell inflation had defects in cell proliferation upon stimulation in vitro and in vivo and upregulated T-cell anergy-associated Itch and GRAIL molecules. Taken together, our data reveal that CD8+ mT-cell inflation renders compromised CD4+ T-cell-dependent CD8+ T-cell immunity via naive T-cell anergy, and thus show promise for the design of efficient vaccines for elderly patients with CD8+ mT-cell inflation.

Published
2017
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137. Differential expression of HNF1A and HNF1A‐AS1 in colon cancer cells.

Author

Sepehri, Zahra, Banerjee, Archana, Vizeacoumar, Frederick S., Freywald, Andrew, Vizeacoumar, Franco J., Dolinsky, Vernon W., and Davie, James R.

Subjects
COLON cancer, HEPATOCYTE nuclear factors, LINCRNA, CANCER cells, ANTISENSE RNA, HOMEOBOX genes
Abstract

The human hepatocyte nuclear factor 1 homeobox A (HNF1A) gene loci express the protein‐coding HNF1A transcript and a long non‐coding RNA in the anti‐sense (HNF1A‐AS1) direction. HNF1A‐AS1 is expressed in numerous types of cancers and poor clinical outcomes such as higher mortality rates, greater metastatic capacity, and poor prognosis of the disease are the results of this expression. In this study, we determined the epigenetic features of the HNF1A gene loci, and expression and cellular localization of HNF1A‐AS1 RNA, HNF1A RNA, and HNF1A protein in colorectal cancer (HT‐29, HTC116, RKO, and SW480) and normal colon epithelial (CCD841) cells. The HT‐29 HNF1A gene had active histone marks (H3K4me3, H3K27ac) and DNase 1 accessible sites at the promoter regions of the HNF1A and HNF1A‐AS1 genes. These epigenetic marks were not observed in the other colorectal cancer cells or in the normal colon epithelial cells. Consistent with the active gene epigenetic signature of the HNF1A gene in HT‐29 cells, HNF1A protein, and HNF1A/HNF1A‐AS1 transcripts were detected in HT‐29 cells but poorly, if at all observed, in the other cell types. In HT‐29 cells, HNF1A‐AS1 localized to the nucleus and was found to bind to the enhancer of zeste homolog 2 (EZH2, a member of PRC2 complex) and potentially form RNA–DNA triplexes with DNase 1 accessible sites in the HT‐29 genome. These activities of HNF1A‐AS1 may contribute to the oncogenic properties of this long non‐coding RNA. [ABSTRACT FROM AUTHOR]

Published
2022
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139. Schmerz und Depression als zentrale Einflussfaktoren auf die gesundheitsbezogene Lebensqualität bei AltenheimbewohnerInnen

Author

Brandauer, Anna, Berger, Stefanie, Freywald, Nicole, Gnass, Irmela, Kutschar, Patrick, Seidenspinner, Denise, and Osterbrink, Jürgen

Subjects
ddc: 610, 610 Medical sciences, Medicine
Abstract

Hintergrund: AltenheimbewohnerInnen (AHB) sind häufig von chronischen Erkrankungen und Komorbiditäten betroffen, welche für die Betroffenen große Einschränkungen bedeuten. Insbesondere Schmerz hat eine hohe, weiterhin steigende Prävalenz von mehr als 50%. Dieser wurde[zum vollständigen Text gelangen Sie über die oben angegebene URL], 18. Deutscher Kongress für Versorgungsforschung (DKVF)

Published
2019
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141. Nursing Education Intervention Effects on Pain Intensity of Nursing Home Residents with Different Levels of Cognitive Impairment: A Cluster-Randomized Controlled Trial

Author

Kutschar,P, Berger,S, Brandauer,A, Freywald,N, Osterbrink,J, Seidenspinner,D, Gnass,I, Kutschar,P, Berger,S, Brandauer,A, Freywald,N, Osterbrink,J, Seidenspinner,D, and Gnass,I

Abstract

P Kutschar,1 S Berger,1 A Brandauer,1 N Freywald,1 J Osterbrink,1,2 D Seidenspinner,3 I Gnass1 1Institute of Nursing Science and Practice, Paracelsus Medical University, Salzburg, Austria; 2Brooks College of Health, University of North Florida, Jacksonville, FL, USA; 3Nursing Science and Practice Development, University Hospital of Munich-Großhadern (LMU), Munich, GermanyCorrespondence: P KutscharInstitute of Nursing Science and Practice, Paracelsus Medical University, Strubergasse 21, Salzburg 5020, AustriaTel +43 662 80 344Email patrick.kutschar@pmu.ac.atPurpose: Pain management in nursing homes is challenging and pain prevalence remains high. The objective of this study was to improve the pain situation of nursing home residents following a nursing-related educational intervention within a cluster-randomized controlled trial (2016– 2018).Participants: Clusters were nursing homes from one nursing home operator in Bavaria, Germany. Nursing home residents who were permanently registered in the facilities, at least 60 years of age, and who themselves or their legal guardians provided informed consent were included.Intervention: In addition to the implementation of pain nurses and pain care assistants, staff of the intervention group received an educational intervention in pain management, containing classroom (quality circles) and web-based training for nurses.Methods: Based on the Mini-Mental State Examination (MMSE), residents were either interviewed (MMSE 10– 30) using self-report instruments or observed (MMSE 0– 9) by proxy assessment. The primary outcome in residents able to self-report was maximum pain intensity according to Brief Pain Inventory (BPI); in those not able to self-report treatment-relevant pain above cut-off (≥ 2) on the Pain Assessment in Advanced Dementia (PAINAD).Results: Out of 20 randomly selected clusters, 9 nursing homes from the control, and 6 nursing homes from the intervention group particip

Published
2020

142. Hygiene management for long-term ventilated persons in the home health care setting: a scoping review.

Author

Hoeppchen, Isabel, Walter, Carola, Berger, Stefanie, Brandauer, Anna, Freywald, Nicole, Kutschar, Patrick, Lex, Katharina Maria, Strobl, Annemarie, and Gnass, Irmela

Subjects
HOME care services, HYGIENE, INFECTION prevention, METHICILLIN-resistant staphylococcus aureus, MULTIDRUG resistance
Abstract

Background: Evidence and recommendations for hygiene management in home mechanical ventilation (HMV) are rare. In Germany, few regionally limited studies show poor hygiene management or a lack of its implementation. This scoping review of international literature identified the evidence in hygiene management for ventilated patients in the home care setting which has to be implemented for infection prevention and control.Methods: A review of international literature was conducted in CINAHL, PubMed and Web of Science. The search focused on four key domains: HMV, hygiene management, home care setting, and methicillin-resistant Staphylococcus aureus (MRSA). Data of included studies were extracted using a data charting sheet. Extracted data were assigned to the categories (1) study description, (2) setting and participants, and (3) hygiene management.Results: From 1,718 reviewed articles, n = 8 studies met inclusion criteria. All included studies had a quantitative study design. The approaches were heterogeneous due to different settings, study populations and types of ventilation performed. Regarding aspects of hygiene management, most evidence was found for infectious critical activities (n = 5), quality management for hygiene (n = 4), and training and education (n = 4). This review identified research gaps concerning kitchen hygiene, relatives and visitors of HMV patients, and waste management (n = 0).Discussion: Overall evidence was rather scarce. Consequently, this review could not answer all underlying research questions. No evidence was found for measures in hygiene management relating to ventilated patients' relatives. Evidence for kitchen hygiene, waste management and interaction with relatives is available for inpatient care settings. However, this may not be transferable to outpatient care. Binding legal requirements and audits may help regulate the implementation of HMV hygiene measures.Conclusion: Infection control programmes included qualified personnel, hygiene plans, and standards for MRSA and multidrug-resistant organisms (MDRO). The appropriateness of hygiene management measures for outpatient care is the basis for their application in practice. [ABSTRACT FROM AUTHOR]

Published
2022
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143. CD40 agonist converting CTL exhaustion via the activation of the mTORC1 pathway enhances PD-1 antagonist action in rescuing exhausted CTLs in chronic infection

Author

Jianqing Xu, Aizhang Xu, Jim Xiang, Andrew Freywald, Rong Wang, Kristoffor Stewart, Changyu Zheng, and Suresh K. Tikoo

Subjects
0301 basic medicine, Agonist, medicine.drug_class, Programmed Cell Death 1 Receptor, Biophysics, chemical and pharmacologic phenomena, Mechanistic Target of Rapamycin Complex 1, Infections, Lymphocyte Activation, Biochemistry, Mice, 03 medical and health sciences, medicine, Animals, Cytotoxic T cell, CD40 Antigens, Molecular Biology, Cells, Cultured, Diphtheria toxin, CD40, biology, TOR Serine-Threonine Kinases, Antagonist, Antibodies, Monoclonal, hemic and immune systems, Cell Biology, Chronic infection, CTL, 030104 developmental biology, Multiprotein Complexes, Chronic Disease, Immunology, biology.protein, CD8, Signal Transduction, T-Lymphocytes, Cytotoxic
Abstract

Expansion of PD-1-expressing CD8+ cytotoxic T lymphocytes (CTLs) and associated CTL exhaustion are chief issues for ineffective virus-elimination in chronic infectious diseases. PD-1 blockade using antagonistic anti-PD-L1 antibodies results in a moderate conversion of CTL exhaustion. We previously demonstrated that CD40L signaling of ovalbumin (OVA)-specific vaccine, OVA-Texo, converts CTL exhaustion via the activation of the mTORC1 pathway in OVA-expressing adenovirus (AdVova)-infected B6 mice showing CTL inflation and exhaustion. Here, we developed AdVova-infected B6 and transgenic CD11c-DTR (termed AdVova-B6 and AdVova-CD11c-DTR) mice with chronic infection, and assessed a potential effect of CD40 agonist on the conversion of CTL exhaustion and on a potential enhancement of PD-1 antagonist action in rescuing exhausted CTLs in our chronic infection models. We demonstrate that a single dose of anti-CD40 alone can effectively convert CTL exhaustion by activating the mTORC1 pathway, leading to CTL proliferation, up-regulation of an effector-cytokine IFN-γ and the cytolytic effect in AdVova-B6 mice. Using anti-CD4 antibody and diphtheria toxin (DT) to deplete CD4+ T-cells and dendritic cells (DCs), we discovered that the CD40 agonist-induced conversion in AdVova-B6 and AdVova-CD11c-DTR mice is dependent upon host CD4+ T-cell and DC involvements. Moreover, CD40 agonist significantly enhances PD-1 antagonist effectiveness in rescuing exhausted CTLs in chronic infection. Taken together, our data demonstrate the importance of CD40 signaling in the conversion of CTL exhaustion and its ability to enhance PD-1 antagonist action in rescuing exhausted CTLs in chronic infection. Therefore, our findings may positively impact the design of new therapeutic strategies for chronic infectious diseases.

Published
2017
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144. Enhanced suppression of polyclonal CD8+25+ regulatory T cells via exosomal arming of antigen-specific peptide/MHC complexes

Author

Rajni Chibbar, Khawaja Ashfaque Ahmed, Chuan-Yong Mu, Jim Xiang, Xueshu Zhang, Aizhang Xu, Xueqin Pang, Lu Wang, Yehan Zhu, Jianan Huang, and Andrew Freywald

Subjects
0301 basic medicine, CD86, Clonal anergy, T cell, Immunology, Priming (immunology), hemic and immune systems, chemical and pharmacologic phenomena, Cell Biology, Dendritic cell, Biology, Cell biology, 03 medical and health sciences, CTL, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, medicine, Immunology and Allergy, Cytotoxic T cell, CD80, 030215 immunology
Abstract

Compared with CD4+25+ regulatory T cells (Tregs), the mechanisms for natural, polyclonal CD8+25+ Treg immune suppression have been significantly less studied. We previously showed that polyclonal T cells can acquire antigen-specific targeting activity through arming with exosomal peptide-MHC (pMHC). In this study, we assessed the suppressive effect of CD8+25+ Tregs or CD8+25+ Tregs armed with ovalbumin (OVA)-specific exosomes on other immune cells and OVA-specific dendritic cell (DCOVA)-stimulated antitumor immunity. We demonstrate that CD8+25+ Tregs inhibit T cell proliferation in vitro in a cell contact-dependent fashion but independent of the expression of immunosuppressive IL-10, TGF-β, and CTLA-4. CD8+25+ Tregs anergize naïve T cells upon stimulation by up-regulating T cell anergy-associated Egr2 and down-regulating IL-2 production. Tregs also anergize DCs by preventing DC maturation through the down-regulation of Iab, CD80, CD86, and inflammatory cytokines, leading to defects in T cell stimulation. Moreover, CD8+25+ Tregs inhibit CTLs through inducing CTL death via perforin-mediated apoptosis and through reducing effector CTL cytotoxic activity via down-regulating CTL perforin-production and degranulation. In addition, we show that CD8+25+ Tregs suppress DCOVA-stimulated CTL responses in priming and effector phases and inhibit immunity against OVA-expressing CCLOVA lung cancer. Remarkably, polyclonal CD8+25+ Tregs armed with OVA-specific exosomal pMHC class-II (pMHC-II), or pMHC class-I (pMHC-I) complexes exert their enhanced inhibition of CTL responses in the priming and the effector phases, respectively. Taken together, our investigation reveals that assigning antigen specificity to nonspecific polyclonal CD8+25+ Tregs for enhanced immune suppression can be achieved through exosomal pMHC arming. This principle may have a great effect on Treg-mediated immunotherapy of autoimmune diseases.

Published
2017
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145. An integrated computational and experimental study uncovers FUT9 as a metabolic driver of colorectal cancer

Author

Sreejit Parameswaran, Tanya Freywald, Nir Gonen, Chelsea E. Cunningham, Keren Yizhak, Emily J McEwen, Franco J. Vizeacoumar, Eytan Ruppin, Kalpana Kalyanasundaram Bhanumathy, Behzad M. Toosi, Frederick S. Vizeacoumar, Andrew Freywald, and Noam Auslander

Subjects
0301 basic medicine, Colorectal cancer, Carcinogenesis, tumor suppressor, Mice, SCID, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Article, FUT9, 03 medical and health sciences, Mice, Inbred NOD, oncogene, Cell Line, Tumor, medicine, Gene silencing, Animals, Humans, Genes, Tumor Suppressor, Neoplasm Invasiveness, Transcription factor, genome‐scale metabolic modeling, Cancer, Gene knockdown, General Immunology and Microbiology, Oncogene, biology, Applied Mathematics, CD44, Computational Biology, Genomics, Articles, medicine.disease, Fucosyltransferases, Disease Models, Animal, 030104 developmental biology, Metabolism, Computational Theory and Mathematics, colon cancer, Gene Knockdown Techniques, Genome-Scale & Integrative Biology, biology.protein, Cancer research, Neoplastic Stem Cells, General Agricultural and Biological Sciences, Colorectal Neoplasms, Algorithms, Information Systems
Abstract

Metabolic alterations play an important role in cancer and yet, few metabolic cancer driver genes are known. Here we perform a combined genomic and metabolic modeling analysis searching for metabolic drivers of colorectal cancer. Our analysis predicts FUT9, which catalyzes the biosynthesis of Ley glycolipids, as a driver of advanced‐stage colon cancer. Experimental testing reveals FUT9's complex dual role; while its knockdown enhances proliferation and migration in monolayers, it suppresses colon cancer cells expansion in tumorspheres and inhibits tumor development in a mouse xenograft models. These results suggest that FUT9's inhibition may attenuate tumor‐initiating cells (TICs) that are known to dominate tumorspheres and early tumor growth, but promote bulk tumor cells. In agreement, we find that FUT9 silencing decreases the expression of the colorectal cancer TIC marker CD44 and the level of the OCT4 transcription factor, which is known to support cancer stemness. Beyond its current application, this work presents a novel genomic and metabolic modeling computational approach that can facilitate the systematic discovery of metabolic driver genes in other types of cancer.

Published
2017

150. TLR9 agonist enhances radiofrequency ablation-induced CTL responses, leading to the potent inhibition of primary tumor growth and lung metastasis

Author

Jim Xiang, Zhaoying Fu, Jingying Yuan, Lifeng Zhang, Bing Zhang, Michael A. J. Moser, Rajni Chibbar, Wenjun Zhang, Fatma Babikr, Andrew Freywald, and Aizhang Xu

Subjects
0301 basic medicine, Cytotoxicity, Immunologic, Hot Temperature, Immunology, chemical and pharmacologic phenomena, CD8-Positive T-Lymphocytes, Article, Metastasis, 03 medical and health sciences, Mice, Necrosis, 0302 clinical medicine, Adjuvants, Immunologic, Antigens, Neoplasm, Cell Line, Tumor, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Humans, Neoplasm Metastasis, Lung, Radiofrequency Ablation, CD40, biology, Chemistry, TLR9, hemic and immune systems, Dendritic Cells, medicine.disease, Primary tumor, Mice, Inbred C57BL, CTL, 030104 developmental biology, Infectious Diseases, Toll-Like Receptor 9, Cancer research, biology.protein, Tumor necrosis factor alpha, CD80, Dinucleoside Phosphates, Neoplasm Transplantation, 030215 immunology
Abstract

Radiofrequency ablation (RFA) is the most common approach to thermal ablation for cancer therapy. Unfortunately, its efficacy is limited by incomplete ablation, and further optimization of RFA is required. Here, we demonstrate that incubation at 65 °C triggers more EG7 tumor cell death by necrosis than treatment at 45 °C, and the 65 °C-treated cells are more effective at inducing antigen-specific CD8(+) cytotoxic T lymphocyte (CTL) responses after injection in mice than the 45 °C-treated ones. Dendritic cells (DCs) that phagocytose 65 °C-treated EG7 cells become mature with upregulated MHCII and CD80 expression and are capable of efficiently inducing effector CTLs in mouse tumor models. RFA (65 °C) therapy of EG7 tumors induces large areas of tumor necrosis and stimulates CTL responses. This leads to complete regression of small (~100 mm(3)) tumors but fails to suppress the growth of larger (~350 mm(3)) tumors. The administration of the Toll-like receptor-9 (TLR9) agonist unmethylated cytosine-phosphorothioate-guanine oligonucleotide (CpG) to DCs phagocytosing 65 °C-treated EG7 cells enhances the expression of MHCII and CD40 on DCs as well as DC-induced stimulation of CTL responses. Importantly, the intratumoral administration of CpG following RFA also increases the frequencies of tumor-associated immunogenic CD11b(−)CD11c(+)CD103(+) DC2 and CD11b(+)F4/80(+)MHCII(+) M1 macrophages and increases CD4(+) and CD8(+) T-cell tumor infiltration, leading to enhanced CD4(+) T cell-dependent CTL responses and potent inhibition of primary RFA-treated or distant untreated tumor growth as well as tumor lung metastasis in mice bearing larger tumors. Overall, our data indicate that CpG administration, which enhances RFA-induced CTL responses and ultimately potentiates the inhibition of primary tumor growth and lung metastasis, is a promising strategy for improving RFA treatment, which may assist in optimizing this important cancer therapy.

Published
2018

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