Your search keyword '"Abounader, Roger"' showing total 29 results

1. Regulation of c-Met-dependent gene expression by PTEN.

Author

Abounader, Roger, Reznik, Thomas, Colantuoni, Carlo, Martinez-Murillo, Francisco, Rosen, Eliot M, and Laterra, John

Subjects

*REGULATION of cell growth, *HEMATOPOIETIC growth factors, *GENE expression, *CYTOKINES, *ASTROCYTES, *HEPATOCYTE growth factor

Abstract

Receptor tyrosine kinases (RTK) and the tumor suppressor PTEN co-regulate oncogenic cell signaling pathways. How these interactions influence gene transcription is inadequately understood. We used expression microarrays to investigate the effects of PTEN on gene expression changes caused by activating c-Met in human glioblastoma cells. c-Met activation by scatter factor/hepatocyte growth factor (SF/HGF) altered the expression of 27-fold more genes in PTEN-null U-373MG cells than in PTEN homozygous primary normal human astrocytes (523 vs 19 genes). Restoring wt-PTEN in U-373MG cells dramatically altered patterns of c-Met regulated gene expression. This effect was varied depending on the specific gene in question. PTEN reduced the number of c-Met regulated transcripts from 931 to 502, decreased the relative number of genes upregulated by c-Met from 46 to 25%, and increased the relative number of downregulated genes from 54 to 75%. PTEN and c-Met co-regulated many genes involved in cell growth regulation such as oncogenes, growth factors, transcription factors, and constituents of the ubiquitin pathway. c-Met activation in PTEN-null (but not PTEN reconstituted) cells led to upregulation of the EGFR agonist TGFaand subsequently to EGFR activation. Using PTEN mutants, we found that PTEN's transcriptional effects were either lipid-phosphatase dependent, protein-phosphatase dependent, or phosphatase-independent. These results show that PTEN has critical and mechanistically complex effects on RTK-regulated gene transcription. These findings expand our understanding of tumor promoter/suppressor inter-relationships and downstream transcriptional effects of PTEN loss and c-Met overexpression in malignant gliomas.Oncogene (2004) 23, 9173-9182. doi:10.1038/sj.onc.1208146 Published online 1 November 2004 [ABSTRACT FROM AUTHOR]

Published

2004

2. Effect of DMTI knockdown on iron, cadmium, and lead uptake in Caco-2 cells.

Author

Bannon, Desmond I., Abounader, Roger, Lees, Peter J., and Bressler, Joseph P.

Subjects

*METALS in the body, *BIOLOGICAL transport, *FROG physiology

Abstract

DMT1 (divalent metal transporter 1) is a hydrogen-coupled divalent metal transporter with a substrate preference for iron, although the protein when expressed in frog oocytes transports a broad range of metals, including the toxic metals cadmium and lead. Wild-type Caco-2 cells displayed saturable transport of lead and iron that was stimulated by acid. Cadmium and manganese inhibited transport of iron, but zinc and lead did not. The involvement of DMT1 in the transport of toxic metals was examined by establishing clonal DMT1 knockdown and control Caco-2 cell lines. Knockdown cell lines displayed much lower levels of DMT1 mRNA and a smaller V[sub max] for iron uptake compared with control cell lines. One clone was further characterized and found to display an ∼50% reduction in uptake of iron across a pH range from 5.5 to 7.4. Uptake for cadmium also decreased 50% across the same pH range, but uptake for lead did not. These results show that DMT1 is important in iron and cadmium transport in Caco-2 cells but that lead enters these cells through an independent hydrogen-driven mechanism. [ABSTRACT FROM AUTHOR]

Published

2003

3. Reversion of human glioblastoma malignancy by U1 small nuclear RNA/ribozyme targeting of scatter factor/hepatocyte growth factor and c-met expression.

Author

Abounader, Roger, Ranganathan, Srikanth, Lal, Bachchu, Fielding, Kevin, Book, Adam, Dietz, Hal, Burger, Peter, Laterra, John, Abounader, R, Ranganathan, S, Lal, B, Fielding, K, Book, A, Dietz, H, Burger, P, and Laterra, J

Subjects

*HEPATOCYTE growth factor, *GLIOBLASTOMA multiforme

Abstract

Background: Expression of scatter factor (SF), also known as hepatocyte growth factor (HGF), and its receptor, c-met, is often associated with malignant progression of human tumors, including gliomas. Overexpression of SF/HGF in experimental gliomas enhances tumorigenicity and tumor-associated angiogenesis (i.e., growth of new blood vessels). However, the role of endogenous SF/HGF or c-met expression in the malignant progression of gliomas has not been examined directly. In this study, we tested the hypothesis that human glioblastomas can be SF/HGF-c-met dependent and that a reduction in endogenous SF/HGF or c-met expression can lead to inhibition of tumor growth and tumorigenicity.Methods: Expression of the SF/HGF and c-met genes was inhibited by transfecting glioblastoma cells with chimeric transgenes consisting of U1 small nuclear RNA, a hammerhead ribozyme, and antisense sequences. The effects of reduced SF/HGF and c-met expression on 1) SF/HGF-dependent induction of immediate early genes (c-fos and c-jun), indicative of signal transduction; 2) anchorage-independent colony formation (clonogenicity), an in vitro correlate of solid tumor malignancy; and 3) intracranial tumor formation in immunodeficient mice were quantified. Statistical tests were two-sided.Results: Introduction of the transgenes into glioblastoma cells reduced expression of the SF/HGF and c-met genes to as little as 2% of control cell levels. Reduction in c-met expression specifically inhibited SF/HGF-dependent signal transduction (P<.01). Inhibition of SF/HGF or c-met expression in glioblastoma cells possessing an SF/HGF-c-met autocrine loop reduced tumor cell clonogenicity (P =.005 for SF/HGF and P=.009 for c-met) and substantially inhibited tumorigenicity (P<.0001) and tumor growth in vivo (P<.0001).Conclusions: To our knowledge, this is the first successful inhibition of SF/HGF and c-met expression in a tumor model directly demonstrating a role for endogenous SF/HGF and c-met in human glioblastoma. Our results suggest that targeting the SF/HGF-c-met signaling pathway may be an important approach in controlling tumor progression. [ABSTRACT FROM AUTHOR]

Published

1999

4. Parallel changes of blood flow and heterogeneity of...

Author

Vogel, Johannes and Abounader, Roger

Subjects

*BLOOD plasma, *CEREBRAL circulation, *ANALYTICAL chemistry, RAT anatomy

Abstract

Investigates the heterogeneity of capillary plasma perfusion during lowered cerebral blood flow induced by hypocapnia in male Sprague-Dawley rats brains. Techniques used in experiment; What findings indicated; Reference to respiratory alkalosis, microcirculation and microvascular flow.

Published

1996

5. Activities of Some Medicinal Plants on the Proliferation and Invasion of Brain Tumor Cell Lines.

Author

Ngulde, Saidu I., Sandabe, Umar K., Abounader, Roger, Zhang, Ying, and Hussaini, Isa M.

Subjects

*CELL lines, *BRAIN tumors, *PLANT invasions, *MEDICINAL plants, *POLY(ADP-ribose) polymerase, *HEPATOTOXICOLOGY

Abstract

Cancer is a debilitating disease that is on the increase in both developed and developing countries. Anticancer drugs are often expensive, have narrow spectrum of activities, and are associated with toxicities and side effects such as myelosuppression, immunosuppression, gastrointestinal disturbance, alopecia, skin toxicity, and hepatotoxicity. Plants have been the major source of anticancer drugs both in orthodox and traditional medicine. Many of the plants claimed by the traditional medicine practitioners (TMPs) to be effective in the treatment of cancer are yet to be evaluated scientifically. In this work, five medicinal plants used by TMPs in Borno State, Nigeria, were tested against two brain tumor cell lines. Ethanol extracts of Securidaca longepedunculata, Andira inermis subsp. rooseveltii, Annona senegalensis, Carissa edulis, and Parinari polyandra were used. U87 and U231 brain tumor cell lines were used for proliferation assay, U251 cell line was used for the invasion assay in collagen V coated inserts, and U87 cell line was used for the western blot detection of cleaved Poly-ADP-Ribose-Polymerase (PARP). The result revealed that all tested extracts significantly (p < 0.05) inhibited the proliferation of U87 and U231 cell lines with the respective IC50 values ranging between 8 and 20 μg/ml for S. longepedunculata and 100 and 90 μg/ml for P. polyandra. The five extracts significantly (p < 0.05) inhibited the invasion of U251 cell line at the concentration of 10 μg/ml (S. longepedunculata), 20 μg/ml (A. inermis), 50 μg/ml (A. senegalensis), 50 μg/ml (C. edulis), and 50 μg/ml (P. polyandra). Securidaca longepedunculata extract induced the cleavage of PARP. It was concluded that these medicinal plants have antiproliferative and anti-invasive activities and possess good prospects as source of anticancer agents especially S. longepedunculata which induced apoptosis in U87 cell line. [ABSTRACT FROM AUTHOR]

Published

2020

6. Cryptic lncRNA-encoded ORFs: A hidden source of regulatory proteins.

Author

Dutta, Anindya, Hui Li, and Abounader, Roger

Abstract

A majority of the human genome is transcribed into noncoding RNAs, of which long noncoding RNAs (lncRNAs) form a large and heterogeneous fraction. While lncRNAs are mostly noncoding, recent evidence suggests that cryptic translation within some lncRNAs may produce proteins with important regulatory functions. In this issue of the JCI, Zheng, Wei, and colleagues used an integrative functional genomic strategy to systematically identify cryptic lncRNA-encoded ORFs that play a role in estrogen receptor-positive (ER+) breast cancer (BC). They identified 758 cryptic lncRNA-encoded ORFs undergoing active translation, of which 28 had potential functional and clinical relevance in ER+ BC. The LINC00992-encoded polypeptide GT3-INCP was upregulated in ER+ BC and drove tumor growth. GT3-INCP was regulated by estrogen and the ER and acted via the transcription factor GATA3 to regulate BC susceptibility and risk genes. These findings discern a largely unexplored class of molecules and have implications for many pathologies, including cancer. [ABSTRACT FROM AUTHOR]

Published

2023

7. Ethanol Extract of Securidaca longipedunculata Induces Apoptosis in Brain Tumor (U87) Cells.

Author

Ngulde, Saidu I., Sandabe, Umar K., Abounader, Roger, Dawson, Thomas K., Zhang, Ying, Iliya, Ibrahim, and Hussaini, Isa M.

Subjects

*CELL proliferation, *APOPTOSIS, *BARK, *BRAIN tumors, *CELL lines, *CHROMATOGRAPHIC analysis, *FLOW cytometry, *MEDICINAL plants, *PLANT roots, *TRANSFERASES, *WESTERN immunoblotting, *PLANT extracts, *CELL survival, *IN vitro studies

Abstract

Incidence of cancer is estimated to be on the increase and current anticancer drugs are characterized by narrow margin of safety and side effects. There is the need to explore new drugs especially from plants since plants serve as major source of drugs. Securidaca longipedunculata Fresen plant is called the mother of all medicines in northern Nigeria and is used traditionally in the treatment of cancers by most traditional medicine practitioners in the region. This study is aimed at evaluating the anticancer activity of the plant extract using U87 brain tumor cell line. Ethanol extract of its root bark was prepared and fractionated by silica gel column chromatography. In vitro activity of the extract and fractions were assessed on the viability of U87 malignant brain tumor cell line by using hemacytometer, annexin V-PE and 7AAD flow cytometry and western blot detection of Poly-ADP-Ribose-Polymerase (PARP) cleavage. The results showed that the extract significantly (p<0.01) inhibited proliferation of U87 cell line with IC50 of 20.535 μg/ml. Apoptosis was induced by the extract (41.53 ± 10.33%) and the polar fraction (47.3 ± 2.7%) via cleavage of PARP. It was concluded that the ethanol extract of S. longipedunculata root bark inhibited proliferation of U87 cell line and induced apoptosis by cleavage of PARP, thus supporting folkloric use of the plant in the management of cancers. [ABSTRACT FROM AUTHOR]

Published

2019

8. miR-3174 Is a New Tumor Suppressor MicroRNA That Inhibits Several Tumor-Promoting Genes in Glioblastoma.

Author

Hanif, Farina, Zhang, Ying, Dube, Collin, Gibert Jr., Myron K., Saha, Shekhar, Hudson, Kadie, Marcinkiewicz, Pawel, Kefas, Benjamin, Guessous, Fadila, and Abounader, Roger

Subjects

*TUMOR suppressor genes, *INTRACRANIAL tumors, *GLIOBLASTOMA multiforme, *BRAIN tumors, *MICRORNA, *GENES

Abstract

microRNAs (miRNAs) play an important role in the pathology of glioblastoma (GBM), which is the most malignant and most common primary malignant brain tumor. miRNAs can target multiple genes simultaneously and are considered as potential therapeutic agents or targets. This study aimed to determine the role of miR-3174 in the pathobiology of GBM using both in vitro and in vivo approaches. This is the first study deciphering the role of miR-3174 in GBM. We studied the expression of miR-3174 and found it to be downregulated in a panel of GBM cell lines, GSCs and tissues relative to astrocytes and normal brain tissue. This finding led us to hypothesize that miR-3174 has a tumor-suppressive role in GBM. Exogenous expression of miR-3174 inhibited GBM cell growth and invasion, and hampered the neurosphere formation ability of GSCs. miR-3174 downregulated the expression of multiple tumor-promoting genes including CD44, MDM2, RHOA, PLAU and CDK6. Further, overexpression of miR-3174 reduced tumor volume in nude mice with intracranial xenografts. Immuno-histochemical study of brain sections with intracranial tumor xenografts revealed the pro-apoptotic and anti-proliferative activity of miR-3174. In conclusion, we demonstrated that miR-3174 has a tumor-suppressive role in GBM and could be exploited for therapeutic purposes. [ABSTRACT FROM AUTHOR]

Published

2023

9. Transcribed Ultraconserved Regions in Cancer.

Author

Gibert Jr., Myron K., Sarkar, Aditya, Chagari, Bilhan, Roig-Laboy, Christian, Saha, Shekhar, Bednarek, Sylwia, Kefas, Benjamin, Hanif, Farina, Hudson, Kadie, Dube, Collin, Zhang, Ying, and Abounader, Roger

Subjects

*LINCRNA, *DNA

Abstract

Transcribed ultraconserved regions are putative lncRNA molecules that are transcribed from DNA that is 100% conserved in human, mouse, and rat genomes. This is notable, as lncRNAs are typically poorly conserved. TUCRs remain very understudied in many diseases, including cancer. In this review, we summarize the current literature on TUCRs in cancer with respect to expression deregulation, functional roles, mechanisms of action, and clinical perspectives. [ABSTRACT FROM AUTHOR]

Published

2022

10. MicroRNA 3928 Suppresses Glioblastoma through Downregulation of Several Oncogenes and Upregulation of p53.

Author

Mulcahy, Elizabeth Q. X., Zhang, Ying, Colόn, Rossymar R., Cain, Shelby R., Gibert Jr., Myron K., Dube, Collin J., Hafner, Markus, and Abounader, Roger

Subjects

*GLIOBLASTOMA multiforme, *MICRORNA, *BRAIN tumors, *DOWNREGULATION, *CELL growth, *ONCOGENES

Abstract

Glioblastoma (GBM) is the most frequent and lethal primary malignant brain tumor. Despite decades of research, therapeutic advances that significantly prolong life are non-existent. In recent years, microRNAs (miRNAs) have been a focus of study in the pathobiology of cancer because of their ability to simultaneously regulate multiple genes. The aim of this study was to determine the functional and mechanistic effects of miR-3928 in GBM both in vitro and in vivo. To the best of our knowledge, this is the first article investigating the role of miR-3928 in GBM. We measured endogenous miR-3928 expression levels in a panel of patient-derived GBM tissue samples and cell lines. We found that GBM tissue samples and cell lines express lower levels of miR-3928 than normal brain cortex and astrocytes, respectively. Therefore, we hypothesized that miR-3928 is a tumor suppressive microRNA. We verified this hypothesis by showing that exogenous expression of miR-3928 has a strong inhibitory effect on both cell growth and invasiveness of GBM cells. Stable ex vivo overexpression of miR-3928 in GBM cells led to a reduction in tumor size in nude mice xenografts. We identified many targets (MDM2, CD44, DDX3X, HMGA2, CCND1, BRAF, ATOH8, and BMI1) of miR-3928. Interestingly, inhibition of the oncogene MDM2 also led to an upregulation of wild-type p53 expression and phosphorylation. In conclusion, we find that miR-3928, through the downregulation of several oncogenes and upregulation and activation of wild-type p53, is a strong tumor suppressor in GBM. Furthermore, the fact that miR-3928 can target many important dysregulated proteins in GBM suggests it might be a "master" regulatory microRNA that could be therapeutically exploited. [ABSTRACT FROM AUTHOR]

Published

2022

11. Signaling pathways in medulloblastoma.

Author

Guessous, Fadila, Yunqing Li, and Abounader, Roger

Subjects

*MEDULLOBLASTOMA, *CEREBELLAR tumors, *GLIOMAS, *TUMORS, *BRAIN tumors

Abstract

Medulloblastoma is the most common brain tumor of childhood. Multiple signaling pathways have been associated with medulloblastoma formation and growth. These include the developmental pathways Hedgehog, (Hh) Notch, and Wnt as well as the receptor tyrosine kinases (RTK) c-Met, erbB2, IGF-R and TrkC, and the oncoprotein Myc. Here we review the involvement of these pathways in medulloblastoma malignancy with a focus on their mode of deregulation, prognostic value, functional effects, cellular and molecular mechanisms of action, and implications for therapy. J. Cell. Physiol. 217: 577–583, 2008. © 2008 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2008

12. The tumor-suppressive long noncoding RNA DRAIC inhibits protein translation and induces autophagy by activating AMPK.

Author

Saha, Shekhar, Ying Zhang, Wilson, Briana, Abounader, Roger, and Dutta, Anindya

Subjects

*LINCRNA, *AUTOPHAGY, *CASTRATION-resistant prostate cancer, *PROTEINS, *PROTEIN kinases, *NF-kappa B

Abstract

Long noncoding RNAs (lncRNAs) are long RNA transcripts that do not code for proteins and have been shown to play a major role in cellular processes through diverse mechanisms. DRAIC, a lncRNA that is downregulated in castration-resistant advanced prostate cancer, inhibits the NF-kB pathway by inhibiting the IKBa kinase. Decreased DRAIC expression predicted poor patient outcome in gliomas and seven other cancers. We now report that DRAIC suppresses invasion, migration, colony formation and xenograft growth of glioblastoma-derived cell lines. DRAIC activates AMP-activated protein kinase (AMPK) by downregulating the NF-kB target gene GLUT1, and thus represses mTOR, leading to downstream effects, such as a decrease in protein translation and increase in autophagy. DRAIC, therefore, has an effect on multiple signal transduction pathways that are important for oncogenesis, namely, the NF-kB pathway and AMPK-mTOR-S6K/ULK1 pathway. The regulation of NF-kB, protein translation and autophagy by the same lncRNA explains the tumor-suppressive role of DRAIC in different cancers and reinforces the importance of lncRNAs as emerging regulators of signal transduction pathways. [ABSTRACT FROM AUTHOR]

Published

2021

13. HGF/MET Signaling in Malignant Brain Tumors.

Author

Mulcahy, Elizabeth Qian Xu, Colόn, Rossymar Rivera, and Abounader, Roger

Subjects

*BRAIN tumors, *CANCER, *HEPATOCYTE growth factor, *SOFT tissue injuries, CENTRAL nervous system tumors

Abstract

Hepatocyte growth factor (HGF) ligand and its receptor tyrosine kinase (RTK) mesenchymal-epithelial transition factor (MET) are important regulators of cellular processes such as proliferation, motility, angiogenesis, and tissue regeneration. In healthy adult somatic cells, this ligand and receptor pair is expressed at low levels and has little activity except when tissue injuries arise. In cancer cells, HGF/MET are often overexpressed, and this overexpression is found to correlate with tumorigenesis, metastasis, and poorer overall prognosis. This review focuses on the signaling of these molecules in the context of malignant brain tumors. RTK signaling pathways are among the most common and universally dysregulated pathways in gliomas. We focus on the role of HGF/MET in the following primary malignant brain tumors: astrocytomas, glioblastomas, oligodendrogliomas, ependymomas, and embryonal central nervous system tumors (including medulloblastomas and others). Brain metastasis, as well as current advances in targeted therapies, are also discussed. [ABSTRACT FROM AUTHOR]

Published

2020

14. Role and Therapeutic Targeting of the HGF/MET Pathway in Glioblastoma.

Author

Cruickshanks, Nichola, Ying Zhang, Fang Yuan, Pahuski, Mary, Gibert, Myron, and Abounader, Roger

Abstract

Glioblastoma (GBM) is a lethal brain tumor with dismal prognosis. Current therapeutic options, consisting of surgery, chemotherapy and radiation, have only served to marginally increase patient survival. Receptor tyrosine kinases (RTKs) are dysregulated in approximately 90% of GBM; attributed to this, research has focused on inhibiting RTKs as a novel and effective therapy for GBM. Overexpression of RTK mesenchymal epithelial transition (MET), and its ligand, hepatocyte growth factor (HGF), in GBM highlights a promising new therapeutic target. This review will discuss the role of MET in cell cycle regulation, cell proliferation, evasion of apoptosis, cell migration and invasion, angiogenesis and therapeutic resistance in GBM. It will also discuss the modes of deregulation of HGF/MET and their regulation by microRNAs. As the HGF/MET pathway is a vital regulator of multiple pro-survival pathways, efforts and strategies for its exploitation for GBM therapy are also described. [ABSTRACT FROM AUTHOR]

Published

2017

15. Targetable T-type Calcium Channels Drive Glioblastoma.

Author

Ying Zhang, Cruickshanks, Nichola, Fang Yuan, Baomin Wang, Pahuski, Mary, Wulfkuhle, Julia, Gallagher, Isela, Koeppel, Alexander F., Hatef, Sarah, Papanicolas, Christopher, Jeongwu Lee, Bar, Eli E., Schiff, David, Turner, Stephen D., Petricoin, Emanuel F., Gray, Lloyd S., and Abounader, Roger

Subjects

*GLIOBLASTOMA multiforme treatment, *GLIOBLASTOMA multiforme, *CALCIUM channels, *MIBEFRADIL (Drug), *CANCER invasiveness, *TARGETED drug delivery, *PROGNOSIS

Abstract

Glioblastoma (GBM) stem-like cells (GSC) promote tumor initiation, progression, and therapeutic resistance. Here, we show how GSCs can be targeted by the FDA-approved drug mibefradil, which inhibits the T-type calcium channel Cav3.2. This calcium channel was highly expressed in human GBM specimens and enriched in GSCs. Analyses of the The Cancer Genome Atlas and REMBRANDT databases confirmed upregulation of Cav3.2 in a subset of tumors and showed that overexpression associated with worse prognosis. Mibefradil treatment or RNAi-mediated attenuation of Cav3.2 was sufficient to inhibit the growth, survival, and stemness of GSCs and also sensitized them to temozolomide chemotherapy. Proteomic and transcriptomic analyses revealed that Cav3.2 inhibition altered cancer signaling pathways and gene transcription. Cav3.2 inhibition suppressed GSC growth in part by inhibiting prosurvival AKT/mTOR pathways and stimulating proapoptotic survivin and BAX pathways. Furthermore, Cav3.2 inhibition decreased expression of oncogenes (PDGFA, PDGFB, and TGFB1) and increased expression of tumor suppressor genes (TNFRSF14 and HSD17B14). Oral administration of mibefradil inhibited growth of GSC-derived GBM murine xenografts, prolonged host survival, and sensitized tumors to temozolomide treatment. Our results offer a comprehensive characterization of Cav3.2 in GBM tumors and GSCs and provide a preclinical proof of concept for repurposing mibefradil as a mechanism-based treatment strategy for GBM. [ABSTRACT FROM AUTHOR]

Published

2017

16. Expression of lncRNAs in Low-Grade Gliomas and Glioblastoma Multiforme: An In Silico Analysis.

Author

Reon, Brian J., Anaya, Jordan, Zhang, Ying, Mandell, James, Purow, Benjamin, Abounader, Roger, and Dutta, Anindya

Subjects

*GLIOMAS, *GLIOBLASTOMA multiforme, *NON-coding RNA, *SOMATIC mutation, *SURVIVAL analysis (Biometry), *GENE expression, *GENETICS

Abstract

Background: Each year, over 16,000 patients die from malignant brain cancer in the US. Long noncoding RNAs (lncRNAs) have recently been shown to play critical roles in regulating neurogenesis and brain tumor progression. To better understand the role of lncRNAs in brain cancer, we performed a global analysis to identify and characterize all annotated and novel lncRNAs in both grade II and III gliomas as well as grade IV glioblastomas (glioblastoma multiforme [GBM]).Methods and Findings: We determined the expression of all lncRNAs in over 650 brain cancer and 70 normal brain tissue RNA sequencing datasets from The Cancer Genome Atlas (TCGA) and other publicly available datasets. We identified 611 induced and 677 repressed lncRNAs in glial tumors relative to normal brains. Hundreds of lncRNAs were specifically expressed in each of the three lower grade glioma (LGG) subtypes (IDH1/2 wt, IDH1/2 mut, and IDH1/2 mut 1p19q codeletion) and the four subtypes of GBMs (classical, mesenchymal, neural, and proneural). Overlap between the subtype-specific lncRNAs in GBMs and LGGs demonstrated similarities between mesenchymal GBMs and IDH1/2 wt LGGs, with 2-fold higher overlap than would be expected by random chance. Using a multivariate Cox regression survival model, we identified 584 and 282 lncRNAs that were associated with a poor and good prognosis, respectively, in GBM patients. We developed a survival algorithm for LGGs based on the expression of 64 lncRNAs that was associated with patient prognosis in a test set (hazard ratio [HR] = 2.168, 95% CI = 1.765-2.807, p < 0.001) and validation set (HR = 1.921, 95% CI = 1.333-2.767, p < 0.001) of patients from TCGA. The main limitations of this study are that further work is needed to investigate the clinical relevance of our findings, and that validation in an independent dataset is needed to determine the robustness of our survival algorithm.Conclusions: This work identifies a panel of lncRNAs that appear to be prognostic in gliomas and provides a critical resource for future studies examining the role of lncRNAs in brain cancers. [ABSTRACT FROM AUTHOR]

Published

2016

17. Combined PDGFR and HDAC Inhibition Overcomes PTEN Disruption in Chordoma.

Author

Lee, Dae-Hee, Zhang, Ying, Kassam, Amin B., Park, Myung-Jin, Gardner, Paul, Prevedello, Daniel, Henry, Stephanie, Horbinski, Craig, Beumer, Jan H., Tawbi, Hussein, Williams, Brian J., Shaffrey, Mark E., Egorin, Merrill J., Abounader, Roger, and Park, Deric M.

Subjects

*PLATELET-derived growth factor receptors, *HISTONE deacetylase, *PTEN protein, *CHORDOMA, *IMATINIB, *CANCER cell physiology

Abstract

Background: The majority of chordomas show activation of the platelet-derived growth factor receptor (PDGFR). Based on in vitro intertumoral variation in response to recombinant PDGF protein and PDGFR inhibition, and variable tumor response to imatinib, we hypothesized that chordomas resistant to PDGFR inhibition may possess downstream activation of the pathway. Methods: Molecular profiling was performed on 23 consecutive chordoma primary tissue specimens. Primary cultures established from 20 of the 23 specimens, and chordoma cell lines, UCH-1 and UCH-2, were used for in vitro experiments. Results: Loss of heterozygosity (LOH) at the phosphatase and tensin homolog (PTEN) locus was observed in 6 specimens (26%). PTEN disruption statistically correlated with increased Ki-67 proliferation index, an established marker of poor outcome for chordoma. Compared to wild type, PTEN deficient chordomas displayed increased proliferative rate, and responded less favorably to PDGFR inhibition. PTEN gene restoration abrogated this growth advantage. Chordomas are characterized by intratumoral hypoxia and local invasion, and histone deacetylase (HDAC) inhibitors are capable of attenuating both hypoxic signaling and cell migration. The combination of PDGFR and HDAC inhibition effectively disrupted growth and invasion of PTEN deficient chordoma cells. Conclusions: Loss of heterozygosity of the PTEN gene seen in a subset of chordomas is associated with aggressive in vitro behavior and strongly correlates with increased Ki-67 proliferative index. Combined inhibition of PDGFR and HDAC attenuates proliferation and invasion in chordoma cells deficient for PTEN. [ABSTRACT FROM AUTHOR]

Published

2015

18. Novel Anti-Apoptotic MicroRNAs 582-5p and 363 Promote Human Glioblastoma Stem Cell Survival via Direct Inhibition of Caspase 3, Caspase 9, and Bim.

Author

Floyd, Desiree Hunt, Zhang, Ying, Dey, Bijan K., Kefas, Benjamin, Breit, Hannah, Marks, Kaitlyn, Dutta, Anindya, Herold-Mende, Christel, Synowitz, Michael, Glass, Rainer, Abounader, Roger, and Purow, Benjamin W.

Subjects

*GLIOBLASTOMA multiforme, *CANCER stem cells, *MICRORNA, *BRAIN tumors, *APOPTOSIS, *CANCER relapse, *CASPASE inhibitors

Abstract

Glioblastoma is the most common and lethal primary brain tumor. Tumor initiation and recurrence are likely caused by a sub-population of glioblastoma stem cells, which may derive from mutated neural stem and precursor cells. Since CD133 is a stem cell marker for both normal brain and glioblastoma, and to better understand glioblastoma formation and recurrence, we looked for dys-regulated microRNAs in human CD133+ glioblastoma stem cells as opposed to CD133+ neural stem cells isolated from normal human brain. Using FACS sorting of low-passage cell samples followed by microRNA microarray analysis, we found 43 microRNAs that were dys-regulated in common in three separate CD133+ human glioblastomas compared to CD133+ normal neural stem cells. Among these were several microRNAs not previously associated with cancer. We then verified the microRNAs dys-regulated in glioblastoma using quantitative real time PCR and Taqman analysis of the original samples, as well as human GBM stem cell and established cell lines and many human specimens. We show that two candidate oncogenic microRNAs, miR-363 and miR-582-5p, can positively influence glioblastoma survival, as shown by forced expression of the microRNAs and their inhibitors followed by cell number assay, Caspase 3/7 assay, Annexin V apoptosis/fluorescence activated cell sorting, siRNA rescue of microRNA inhibitor treatment, as well as 3′UTR mutagenesis to show luciferase reporter rescue of the most successful targets. miR-582-5p and miR-363 are shown to directly target Caspase 3, Caspase 9, and Bim. [ABSTRACT FROM AUTHOR]

Published

2014

19. A New lncRNA, APTR, Associates with and Represses the CDKN1A/p21 Promoter by Recruiting Polycomb Proteins.

Author

Negishi, Masamitsu, Wongpalee, Somsakul P., Sarkar, Sukumar, Park, Jonghoon, Lee, Kyung Yong, Shibata, Yoshiyuki, Reon, Brian J., Abounader, Roger, Suzuki, Yutaka, Sugano, Sumio, and Dutta, Anindya

Subjects

*CYCLIN-dependent kinases, *PROMOTERS (Genetics), *POLYCOMB group proteins, *DNA damage, *CANCER invasiveness, *EPIGENETICS

Abstract

Long noncoding RNAs (lncRNAs) have emerged as a major regulator of cell physiology, but many of which have no known function. CDKN1A/p21 is an important inhibitor of the cell-cycle, regulator of the DNA damage response and effector of the tumor suppressor p53, playing a crucial role in tumor development and prevention. In order to identify a regulator for tumor progression, we performed an siRNA screen of human lncRNAs required for cell proliferation, and identified a novel lncRNA, APTR, that acts in trans to repress the CDKN1A/p21 promoter independent of p53 to promote cell proliferation. APTR associates with the promoter of CDKN1A/p21 and this association requires a complementary-Alu sequence encoded in APTR. A different module of APTR associates with and recruits the Polycomb repressive complex 2 (PRC2) to epigenetically repress the p21 promoter. A decrease in APTR is necessary for the induction of p21 after heat stress and DNA damage by doxorubicin, and the levels of APTR and p21 are anti-correlated in human glioblastomas. Our data identify a new regulator of the cell-cycle inhibitor CDKN1A/p21 that acts as a proliferative factor in cancer cell lines and in glioblastomas and demonstrate that Alu elements present in lncRNAs can contribute to targeting regulatory lncRNAs to promoters. [ABSTRACT FROM AUTHOR]

Published

2014

20. microRNA-148a Is a Prognostic oncomiR That Targets MIG6 and BIM to Regulate EGFR and Apoptosis in Glioblastoma.

Author

Jungeun Kim, Ying Zhang, Skalski, Michael, Hayes, Josie, Kefas, Benjamin, Schiff, David, Purow, Benjamin, Parsons, Sarah, Lawler, Sean, and Abounader, Roger

Subjects

*MICRORNA, *EPIDERMAL growth factor receptors, *PEPTIDE receptors, *APOPTOSIS, *GLIOBLASTOMA multiforme

Abstract

Great interest persists in useful prognostic and therapeutic targets in glioblastoma. In this study, we report the definition of miRNA (miR)-148a as a novel prognostic oncomiR in glioblastoma. miR-148a expression was elevated in human glioblastoma specimens, cell lines, and stem cells (GSC) compared with normal human brain and astrocytes. High levels were a risk indicator for glioblastoma patient survival. Functionally, miR-148a expression increased cell growth, survival, migration, and invasion in glioblastoma cells and GSCs and promoted GSC neurosphere formation. Two direct targets of miR-148a were identified, the EGF receptor (EGFR) regulator MIG6 and the apoptosis regulator BIM, which rescue experiments showed were essential to mediate the oncogenic activity of miR-148a. By inhibiting MIG6 expression, miR-148a reduced EGFR trafficking to Rab7-expressing compartments, which includes late endosomes and lysosomes. This process coincided with reduced degradation and elevated expression and activation of EGFR. Finally, inhibition of miR-148a strongly suppressed GSC and glioblastoma xenograft growth in vivo. Taken together, our findings provide a comprehensive analysis of the prognostic value and oncogenic function of miR-148a in glioblastoma, further defining it as a potential target for glioblastoma therapy. [ABSTRACT FROM AUTHOR]

Published

2014

21. MicroRNA-608 and MicroRNA-34a Regulate Chordoma Malignancy by Targeting EGFR, Bcl-xL and MET.

Author

Zhang, Ying, Schiff, David, Park, Deric, and Abounader, Roger

Subjects

*MICRORNA, *CHORDOMA, *GENE targeting, *MET receptor, *BCL genes, *CANCER genetics, *SPINAL cord cancer

Abstract

Chordomas are rare malignant tumors that originate from the notochord remnants and occur in the skull base, spine and sacrum. Due to a very limited understanding of the molecular pathogenesis of chordoma, there are no adjuvant and molecular therapies besides surgical resection and radiation therapy. microRNAs (miRNAs) are small noncoding regulatory RNA molecules with critical roles in cancer. The role of miRNAs in chordomas is mostly unknown. We uncover microRNA-608 (miR-608) and microRNA-34a (miR-34a) as novel tumor suppressive microRNAs that regulate malignancy in chordoma. We find that miR-608 and miR-34a expressions are downregulated in human chordoma cell lines and primary cells at least partially via alteration of their genes’ copy numbers. We identify the commonly deregulated oncogenes EGFR and Bcl-xL as direct targets of miR-608 and the receptor tyrosine kinase MET as direct target of miR-34a. We show that EGFR and MET activations promote chordoma cell proliferation and invasion and that pharmacological inhibition of EGFR and MET inhibits chordoma cell proliferation and survival. We demonstrate that restoration of miR-608 and miR-34a inhibits cell proliferation and invasion and induces apoptosis in chordoma cells. We find that miR-34a inversely correlates with MET expression and miR-608 inversely correlates with EGFR expression in chordoma cells. These findings demonstrate for the first time that miR-608 and miR-34a regulate chordoma malignancy by regulating EGFR, MET and Bcl-xL. [ABSTRACT FROM AUTHOR]

Published

2014

22. microRNA-34a promotes DNA damage and mitotic catastrophe.

Author

Kofman, Alexander V., Jungeun Kim, So Yeon Park, Dupart, Evan, Letson, Christopher, Yongde Bao, Kai Ding, Quan Chen, Schiff, David, Larner, James, and Abounader, Roger

Published

2013

23. A Novel PTEN/Mutant p53/ c-Myc/Bcl-XL Axis Mediates Context-Dependent Oncogenic Effects of PTEN with Implications for Cancer Prognosis and Therapy.

Author

Xiaoping Huang, Ying Zhang, Yaqiong Tang, Butler, Napoleon, Jungeun Kim, Guessous, Fadila, Schiff, David, Mandell, James, and Abounader, Roger

Subjects

*PTEN protein, *SUPPRESSORS of cytokine signaling, *GLIOBLASTOMA multiforme, *ONCOGENES, *CELL proliferation, *CANCER cells

Abstract

Phosphatase and tensin homolog located on chromosome 10 (PTEN) is one of the most frequently mutated tumor suppressors in human cancer including in glioblastoma. Here, we show that PTEN exerts unconventional oncogenic effects in glioblastoma through a novel PTEN/mutant p53/c-Myc/Bcl-XL molecular and functional axis. Using a wide array of molecular, genetic, and functional approaches, we demonstrate that PTEN enhances a transcriptional complex containing gain-of-function mutant p53, CBP, and NFY in human glioblastoma cells and tumor tissues. The mutant p53/CBP/NFY complex transcriptionally activates the oncogenes c-Myc and Bcl-XL, leading to increased cell proliferation, survival, invasion, and clonogenicity. Disruption of the mutant p53/c-Myc/Bcl-XL axis or mutant p53/CBP/ NFY complex reverses the transcriptional and oncogenic effects of PTEN and unmasks its tumor-suppressive function. Consistent with these data, we find that PTEN expression is associated with worse patient survival than PTEN loss in tumors harboring mutant p53 and that a small molecule modulator of p53 exerts greater antitumor effects in PTEN-expressing cancer cells. Altogether, our study describes a new signaling pathway that mediates contextdependent oncogenic/tumor-suppressive role of PTEN. The data also indicate that the combined mutational status of PTEN and p53 influences cancer prognosis and anticancer therapies that target PTEN and p53. [ABSTRACT FROM AUTHOR]

Published

2013

24. microRNA-34a is tumor suppressive in brain tumors and glioma stem cells.

Author

Guessous, Fadila, Ying Zhang, Kofman, Alexander, Catania, Alessia, Yunqing Li, Schiff, David, Purow, Benjamin, and Abounader, Roger

Published

2010

25. The Neuronal MicroRNA miR-326 Acts in a Feedback Loop with Notch and Has Therapeutic Potential against Brain Tumors.

Author

Kefas, Benjamin, Comeau, Laurey, Floyd, Desiree H., Seleverstov, Oleksandr, Godlewski, Jakub, Schmittgen, Tom, Jinmai Jiang, diPierro, Charles G., Yunqing Li, Chiocca, E. Antonio, Jeongwu Lee, Fine, Howard, Abounader, Roger, Lawler, Sean, and Purow, Benjamin

Subjects

*RNA, *NOTCH genes, *NOTCH proteins, *NERVOUS system, *BRAIN tumors, *GLIOMAS

Abstract

Little is known of microRNA interactions with cellular pathways. Few reports have associated microRNAs with the Notch pathway, which plays key roles in nervous system development and in brain tumors. We previously implicated the Notch pathway in gliomas, the most commonand aggressive brain tumors. While investigating Notch mediators, we noted microRNA-326 was upregulated following Notch-1 knockdown. This neuronally expressed microRNA was not only suppressed by Notch but also inhibited Notch proteins and activity, indicating a feedback loop. MicroRNA-326 was downregulated in gliomas via decreased expression of its host gene. Transfection of microRNA-326 into both established and stem cell-like glioma lines was cytotoxic, and rescue was obtained with Notch restoration. Furthermore, miR-326 transfection reduced glioma cell tumorigenicity in vivo. Additionally, we found microRNA-326 partially mediated the toxic effects of Notch knockdown. This work demonstrates a microRNA-326/Notch axis, shedding light on the biology of Notch and suggesting microRNA-326 delivery as a therapy. [ABSTRACT FROM AUTHOR]

Published

2009

26. Pediatric Oncology.

Author

Navid, Fariba, Lewis, Kristi, Abounader, Roger, Laterra, John, Khanna, Chand, and Helman, Lee

Subjects

*RHABDOMYOSARCOMA, *MET receptor, *PATHOLOGY

Abstract

Focuses on the association of factor receptor in decreased metastases in human rhabdomyosarcoma xenograft model. Significance of the pathway in malignant cellular processes; Role of Met overexpression in rhabdomyosarcoma; Use as a target in the setting of minimal residual disease.

Published

2001

27. BLBP Is Both a Marker for Poor Prognosis and a Potential Therapeutic Target in Paediatric Ependymoma.

Author

Sabnis, Durgagauri H., Liu, Jo-Fen, Simmonds, Lucy, Blackburn, Sophie, Grundy, Richard G., Kerr, Ian D., Coyle, Beth, and Abounader, Roger

Subjects

*LIPID analysis, *PROTEIN analysis, *CANCER invasiveness, *GLIOMAS, *CELL motility, *STEM cells, *DESCRIPTIVE statistics, *SURVIVAL analysis (Biometry), *TUMOR markers, *DRUG resistance in cancer cells, *CHILDREN

Abstract

Simple Summary: Ependymomas are the second most common paediatric brain tumour, and the 5-year survival rate remains no higher than 50%. Identifying new prognostic markers and targets for therapy in ependymoma is an important area of research. In this study, we demonstrate that brain lipid binding protein (BLBP, FABP7) is expressed in a sub-population of cells in ependymoma patient samples, consistent with it being a cancer stem cell marker. BLBP expression was associated with both significantly reduced event free survival and overall survival. BLBP can be functionally inhibited by PPAR antagonists, and we demonstrated that these antagonists can reduce ependymoma cell migration, invasion and chemo-resistance. The BLBP ligand docosohexanoic acid also attenuated these three hallmark characteristics of ependymomas, leading us to conclude that BLBP is not just a prognostic marker for poor ependymoma survival, but that it represents a druggable target in ependymoma therapy. Paediatric ependymomas are aggressive, treatment-resistant tumours with a tendency towards relapse, consistent with a sub-population of therapy-resistant cancer stem cells. These cells are believed to derive from brain lipid binding protein (BLBP)-expressing radial glia, hence we proposed that BLBP may be a marker for ependymoma therapy resistance. BLBP protein expression correlated with reduced overall survival (OS) in patients from two trials (CNS9204, a chemotherapy-led infant trial—5 y OS 45% vs. 80%, p = 0.011—and CNS9904, a radiotherapy-led trial—OS 38% vs. 85%, p = 0.002). All ependymoma cell lines examined by qRT-PCR expressed BLBP, with expression elevated in stem cell-enriched neurospheres. Modulation of BLBP function in 2D and 3D assays, using either peroxisome proliferator activated receptor (PPAR) antagonists or BLBP's fatty acid substrate docosahexaneoic acid (DHA), potentiated chemotherapy response and reduced cell migration and invasion in ependymoma cell lines. BLBP is therefore an independent predictor of poor survival in paediatric ependymoma, and treatment with PPAR antagonists or DHA may represent effective novel therapies, preventing chemotherapy resistance and invasion in paediatric ependymoma patients. [ABSTRACT FROM AUTHOR]

Published

2021

28. Noncoding RNAs in Glioblastoma: Emerging Biological Concepts and Potential Therapeutic Implications.

Author

Shahzad, Uswa, Krumholtz, Stacey, Rutka, James T., Das, Sunit, Kögel, Donat, Herold-Mende, Christel, Linder, Benedikt, and Abounader, Roger

Subjects

*GLIOMA treatment, *RNA physiology, *DISEASE progression, *PHENOMENOLOGICAL biology, *NEOVASCULARIZATION, *GLIOMAS, *RNA, *APOPTOSIS, *MOLECULAR biology, *CELL motility, *CELL survival, *CELL proliferation

Abstract

Simple Summary: Since the completion of the Human Genome Project, noncoding RNAs (ncRNAs) have emerged as an important class of genetic regulators. Several classes of ncRNAs, which include microRNAs (miRNAs), long noncoding RNAs (lncRNAs), circular RNAs (circRNAs), and piwi-interacting RNAs (piRNAs), have been shown to play important roles in controlling developmental and disease processes. In this article, we discuss the potential roles of ncRNAs in regulating glioblastoma (GBM) formation and progression as well as potential strategies to exploit the diagnostic and therapeutic potential of ncRNAs in GBM. Noncoding RNAs (ncRNAs) have emerged as a novel class of genomic regulators, ushering in a new era in molecular biology. With the advent of advanced genetic sequencing technology, several different classes of ncRNAs have been uncovered, including microRNAs (miRNAs), long noncoding RNAs (lncRNAs), circular RNAs (circRNAs), and piwi-interacting RNAs (piRNAs), which have been linked to many important developmental and disease processes and are being pursued as clinical and therapeutic targets. Molecular phenotyping studies of glioblastoma (GBM), the most common and lethal cancer of the adult brain, revealed that several ncRNAs are frequently dysregulated in its pathogenesis. Additionally, ncRNAs regulate many important aspects of glioma biology including tumour cell proliferation, migration, invasion, apoptosis, angiogenesis, and self-renewal. Here, we present an overview of the biogenesis of the different classes of ncRNAs, discuss their biological roles, as well as their relevance to gliomagenesis. We conclude by discussing potential approaches to therapeutically target the ncRNAs in clinic. [ABSTRACT FROM AUTHOR]

Published

2021

29. The p53 Pathway in Glioblastoma.

Author

Zhang, Ying, Dube, Collin, Gibert, Myron, Cruickshanks, Nichola, Wang, Baomin, Coughlan, Maeve, Yang, Yanzhi, Setiady, Initha, Deveau, Ciana, Saoud, Karim, Grello, Cassandra, Oxford, Madison, Yuan, Fang, and Abounader, Roger

Subjects

*GLIOMA treatment, *GLIOMAS, *CELL proliferation, *TUMOR suppressor genes, *APOPTOSIS, *CANCER patients, *CANCER invasiveness, *CELL lines, *CELL motility, *CELLULAR signal transduction, *GENE expression, *GENETIC mutation, *NEOVASCULARIZATION inhibitors, *TRANSCRIPTION factors, *TUMOR markers, *MICRORNA, *GAIN-of-function mutations, *PROGNOSIS, *GENETICS

Abstract

The tumor suppressor and transcription factor p53 plays critical roles in tumor prevention by orchestrating a wide variety of cellular responses, including damaged cell apoptosis, maintenance of genomic stability, inhibition of angiogenesis, and regulation of cell metabolism and tumor microenvironment. TP53 is one of the most commonly deregulated genes in cancer. The p53-ARF-MDM2 pathway is deregulated in 84% of glioblastoma (GBM) patients and 94% of GBM cell lines. Deregulated p53 pathway components have been implicated in GBM cell invasion, migration, proliferation, evasion of apoptosis, and cancer cell stemness. These pathway components are also regulated by various microRNAs and long non-coding RNAs. TP53 mutations in GBM are mostly point mutations that lead to a high expression of a gain of function (GOF) oncogenic variants of the p53 protein. These relatively understudied GOF p53 mutants promote GBM malignancy, possibly by acting as transcription factors on a set of genes other than those regulated by wild type p53. Their expression correlates with worse prognosis, highlighting their potential importance as markers and targets for GBM therapy. Understanding mutant p53 functions led to the development of novel approaches to restore p53 activity or promote mutant p53 degradation for future GBM therapies. [ABSTRACT FROM AUTHOR]

Published

2018