Your search keyword '"neu"' showing total 31 results

1. Rank ectopic expression in the presence of Neu and MMTV oncogenes alters mammary epithelial cell populations and their tumorigenic potential.

Author

Cordero, Alex, Santamaría, Patricia G., and González-Suárez, Eva

Abstract

Determination of the mammary epithelial cell that serves as the cell of origin for breast cancer is key to understand tumor heterogeneity and clinical management. In this study, we aimed to decipher whether Rank expression in the presence of PyMT and Neu oncogenes might affect the cell of origin of mammary gland tumors. We observed that Rank expression in PyMT+/− and Neu+/− mammary glands alters the basal and luminal mammary cell populations already in preneoplasic tissue, which may interfere with the tumor cell of origin restricting their tumorigenesis ability upon transplantation assays. In spite of this, Rank expression eventually promotes tumor aggressiveness once tumorigenesis is established. [ABSTRACT FROM AUTHOR]

Published

2023

2. Neu Perspectives, Therapies, and Challenges for Metastatic HER2-Positive Breast Cancer.

Author

Salkeni, Mohamad Adham, Rizvi, Wajeeha, Hein, Kyaw, and Higa, Gerald M

Subjects

HER2 positive breast cancer, METASTATIC breast cancer, PROGNOSIS, BREAST cancer, DISEASE relapse, PROGRESSIVE supranuclear palsy

Abstract

Even though gene amplification or protein overexpression occurs in approximately one-fifth of all breast cancers, the discovery of HER2 has, nevertheless, had profound implications for the disease. Indeed, the characterization of the receptor resulted in a number of significant advances. Structurally, unique features provided avenues for the development of numerous compounds with target-specificity; molecularly, biological constructs revealed a highly complex, internal signal transduction pathway with regulatory effects on tumor proliferation, survival, and perhaps, even resistance; and clinically, disease outcomes manifested its predictive and prognostic value. Yet despite the receptor's utility, the beneficial effects are diminished by tumor recurrence after neo- or adjuvant therapy as well as losses resulting from the inability to cure patients with metastatic disease. What these observations suggest is that while tumor response may be partially linked to uncoupling cell surface message reception and nuclear gene expression, as well as recruitment of the innate immune system, disease progression and/or resistance may involve a reprogrammable signaling mainframe that elicits alternative growth and survival signals. This review attempts to meld current perceptions related to HER2-positive metastatic breast cancer with particular attention to current biological insights and therapeutic challenges. [ABSTRACT FROM AUTHOR]

Published

2021

3. Test gest (TEGEST) k rychlému vyšetření epizodické paměti u mírné kognitivní poruchy.

Author

Bartoš, A.

Abstract

Copyright of Česká a Slovenská Neurologie a Neurochirurgie is the property of Czech Medical Association of JE Purkyne and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2018

4. 强心益气方联合瑞舒伐他汀治疗急性心肌梗死的疗效及对患者血清相关指标的影响

Author

曹甜甜, 张巍, 张云, 王鑫, and 刘洁

Abstract

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

Published

2017

5. 强心益气方联合瑞舒伐他汀治疗急性心肌梗死的疗效及对患者血清相关指标的影响

Author

曹甜甜, 张巍, 张云, 王鑫, and 刘洁

Abstract

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

Published

2017

6. The glucose transporter GLUT1 is required for ErbB2-induced mammary tumorigenesis.

Author

Wellberg, Elizabeth A., Johnson, Stevi, Finlay-Schultz, Jessica, Lewis, Andrew S., Terrell, Kristina L., Sartorius, Carol A., Abel, E. Dale, Muller, William J., and Anderson, Steven M.

Subjects

GLUCOSE transporter genetics, POLYOMAVIRUS diseases, ANTIGEN analysis, LABORATORY mice, DIAGNOSIS, THERAPEUTICS, GLUCOSE metabolism, ANIMALS, BIOLOGICAL models, BREAST tumors, CARRIER proteins, CELL lines, CELL physiology, CELL receptors, GENETIC techniques, MICE, RESEARCH funding, DISEASE progression, KAPLAN-Meier estimator, NEOPLASTIC cell transformation, METABOLISM

Abstract

Background: Altered tumor cell metabolism is an emerging hallmark of cancer; however, the precise role for glucose in tumor initiation is not known. GLUT1 (SLC2A1) is expressed in breast cancer cells and is likely responsible for avid glucose uptake observed in established tumors. We have shown that GLUT1 was necessary for xenograft tumor formation from primary mammary cells transformed with the polyomavirus middle-T antigen but that it was not necessary for growth after tumors had formed in vivo, suggesting a differential requirement for glucose depending on the stage of tumorigenesis.Methods: To determine whether GLUT1 is required early during mammary tumorigenesis, we crossed MMTV-NIC mice, which express activated HER2/NEU/ERBB2 and Cre recombinase, to Slc2a1 Flox/Flox (GLUT1Flox/Flox) mice to generate NIC-GLUT1+/+, NIC-GLUT1Flox/+, and NIC-GLUT1Flox/Flox mice. In addition, we evaluated effects of glucose restriction or GLUT1 inhibition on transformation in MCF10A-ERBB2 breast epithelial cells in three-dimensional culture. Finally, we utilized global gene expression profiling data of primary human breast tumors to determine the relationship between SLC2A1 and stage of tumorigenesis.Results: All of the NIC-GLUT1+/+ mice developed tumors in less than 200 days. In contrast, only 1 NIC-GLUT1Flox/Flox mouse and 1 NIC-GLUT1Flox/+ mouse developed mammary tumors, even after 18 months. Mammary gland development was not disrupted in NIC mice lacking GLUT1; however, epithelial content of mature glands was reduced compared to NIC-GLUT1Flox/+ mice. In MCF10A-ERBB2 cells, glucose restriction or GLUT1 inhibition blocked transformation induced by activated ERBB2 through reduced cell proliferation. In human breast cancers, SLC2A1 was higher in ductal carcinoma in situ compared to the normal breast, but lower in invasive versus in situ lesions, suggesting the requirement for GLUT1 decreases as tumors progress.Conclusions: This study demonstrates a strict requirement for GLUT1 in the early stages of mammary tumorigenesis in vitro and in vivo. While metabolic adaptation has emerged as a hallmark of cancer, our data indicate that early tumor cells rely heavily on glucose and highlight the potential for glucose restriction as a breast cancer preventive strategy. [ABSTRACT FROM AUTHOR]

Published

2016

7. Mutant p53 - heat shock response oncogenic cooperation: a new mechanism of cancer cell survival.

Author

Alexandrova, Evguenia M. and Marchenko, Natalia D.

Subjects

TUMOR suppressor genes, TUMOR suppressor proteins, APOPTOSIS

Abstract

The main tumor suppressor function of p53 as a "guardian of the genome" is to respond to cellular stress by transcriptional activation of apoptosis, growth arrest, or senescence in damaged cells. Not surprisingly, mutations in the p53 gene are the most frequent genetic alteration in human cancers. Importantly, mutant p53 (mutp53) proteins not only lose their wild-type tumor suppressor activity but also can actively promote tumor development. Two main mechanisms accounting for mutp53 proto-oncogenic activity are inhibition of the wild-type p53 in a dominant-negative fashion and gain of additional oncogenic activities known as gain-of-function (GOF). Here, we discuss a novel mechanism of mutp53 GOF, which relies on its oncogenic cooperation with the heat shock machinery. This coordinated adaptive mechanism renders cancer cells more resistant to proteotoxic stress and provides both, a strong survival advantage to cancer cells and a promising means for therapeutic intervention. [ABSTRACT FROM AUTHOR]

Published

2015

8. C-erbB2/HER2 in Human Gliomas, Medulloblastomas, and Meningiomas: A Minireview.

Author

Waage, Ingunn Syversen, Vreim, Ingeborg, and Torp, Sverre Helge

Subjects

BRAIN tumor diagnosis, GLIOMAS, TUMOR markers, IMMUNOHISTOCHEMISTRY, GENE expression, GROWTH factors

Abstract

C-erbB2/HER2 serves as an important prognostic and predictive biomarker in various human tumors, especially in breast cancer, whereas its role in human intracranial tumors is more uncertain. We therefore performed a search in PubMed to get an update. This literature review comprises immunohistochemical studies on the clinical significance of c-erbB2/HER2 overexpression in gliomas, medulloblastomas, and meningiomas. In general, the findings were discrepant with regard to correlations between overexpression, tumor grade, and prognosis. Use of various antibodies may be a contributing factor to these discrepancies. Standardization of the immunohistochemical procedures is a relevant topic for discussion. [ABSTRACT FROM PUBLISHER]

Published

2013

9. Grb7 and Filamin-a associate and are colocalized to cell membrane ruffles upon EGF stimulation.

Author

Paudyal, Prakash, Shrestha, Sanjay, Madanayake, Thushara, Shuster, Charles B., Rohrschneider, Larry R., Rowland, Aaron, and Lyons, Barbara A.

Abstract

Grb7 is an adaptor molecule mediating signal transduction from multiple cell surface receptors to diverse downstream pathways. Grb7, along with Grb10 and Grb14, make up the Grb7 protein family. This protein family has been shown to be overexpressed in certain cancers and cancer cell lines. Grb7 and a receptor tyrosine kinase, ErbB2, are overexpressed in 20-30% of breast cancers. Grb7 overexpression has been linked to enhanced cell migration and metastasis, although the participants in these pathways have not been fully determined. In this study, we report the Grb7 protein interacts with Filamin-a, an actin-crosslinking component of the cell cytoskeleton. Additionally, we have demonstrated the interaction between Grb7 and Flna is specific to the RA-PH domains of Grb7, and the immunoglobulin-like repeat 16-19 domains of Flna. We demonstrate that full-length Grb7 and Flna interact in the mammalian cellular environment, as well as in vitro. Immunofluorescent microscopy shows potential colocalization of Grb7 and Flna in membrane ruffles upon epidermal growth factor stimulation. These studies are amongst the first to establish a clear connection between Grb7 signaling and cytoskeletal remodeling. [ABSTRACT FROM AUTHOR]

Published

2013

10. Dimerization in the Grb7 Protein.

Author

Peterson, Tabitha A., Benallie, Renee L., Bradford, Andrew M., Pias, Sally C., Yazzie, Jaron, Lor, Siamee N., Haulsee, Zachary M., Park, Chad K., Johnson, Dennis L., Rohrschneider, Larry R., Spuches, Anne, and Lyons, Barbara A.

Abstract

In previous studies, we showed that the tyrosine phosphorylation state of growth factor receptor-bound protein 7 (Grb7) affects its ability to bind to the transcription regulator FHL2 and the cortactin-interacting protein, human HS-1-associated protein-1. Here, we present results describing the importance of dimerization in the Grb7-Src homology 2 (SH2) domain in terms of its structural integrity and the ability to bind phosphorylated tyrosine peptide ligands. A tyrosine phosphorylation-mimic mutant (Y80E-Grb7-SH2) is largely dimerization deficient and binds a tyrosine-phosphorylated peptide representative of the receptor tyrosine kinase (RTK) erbB2 with differing thermodynamic characteristics than the wild-type SH2 domain. Another dimerization-deficient mutant (F99R-Grb7-SH2) binds the phosphorylated erbB2 peptide with similarly changed thermodynamic characteristics. Both Y80E-Grb7-SH2 and F99R-Grb7-SH2 are structured by circular dichroism measurements but show reduced thermal stability relative to the wild type-Grb7-SH2 domain as measured by circular dichroism and nuclear magnetic resonance. It is well known that the dimerization state of RTKs (as binding partners to adaptor proteins such as Grb7) plays an important role in their regulation. Here, we propose the phosphorylation state of Grb7-SH2 domain tyrosine residues could control Grb7 dimerization, and dimerization may be an important regulatory step in Grb7 binding to RTKs such as erbB2. In this manner, additional dimerization-dependent regulation could occur downstream of the membrane-bound kinase in RTK-mediated signaling pathways. Copyright © 2012 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2012

11. Grb7 binds to Hax-1 and undergoes an intramolecular domain association that offers a model for Grb7 regulation.

Author

Siamakpour-Reihani, Sharareh, Peterson, Tabitha A., Bradford, Andrew M., Argiros, Haroula J., Haas, Laura Lowell, Lor, Siamee N., Haulsee, Zachary M., Spuches, Anne M., Johnson, Dennis L., Rohrschneider, Larry R., Shuster, Charles Brad, and Lyons, Barbara A.

Subjects

CELL migration, FOCAL adhesion kinase, HOMOLOGY (Biology), MOLECULAR recognition, MOLECULAR biology

Abstract

The article discusses a study which identified the interaction partners of Grb7 adaptor protein potentially involved in focal adhesion kinase (FAK)/Grb7-mediated cell migration. It clarifies the role of the Grb7-Ras Associating (RA) and -Pleckstrin Homology (PH) domains in this protein and explores the phosphorylation state of Grb7 necessary for, or during, binding interactions. It also proposes a Grb7autoinhibitory mechanism based upon the results.

Published

2011

12. A meta-analysis on the association of HER-2 overexpression with prognosis in human osteosarcoma.

Author

LI, Y. G. and GENG, X.

Subjects

OSTEOSARCOMA, HER2 protein, TUMOR proteins, GENE expression, META-analysis

Abstract

LI Y.G. & GENG X. (2010) European Journal of Cancer Care 19, 313–316 A meta-analysis on the association of HER-2 overexpression with prognosis in human osteosarcoma Various studies examining the relationship between HER-2 overexpression and clinical outcome in patients with osteosarcoma have yielded inconclusive results. The purpose of the current study was to evaluate the relation of HER-2 status with clinical outcome in osteosarcoma. We conducted a meta-analysis of five studies that evaluated the relation between HER-2 status and 2-year survival. DerSimonian-Laird random effects analysis was used to estimate the effects of HER-2 overexpression on 2-year survival. The combined relative risk in patients with osteosarcoma for 2-year survival was 1.26 (95% confidence interval, 0.50–3.14; P = 0.63). HER-2-positive status tended to be associated with a worse 2-year survival, but the overall results were not formally statistically significant. An unfavourable prognostic effect of HER-2 overexpression in osteosarcoma was evident from the meta-analysis. However, because several studies were excluded by the current eligibility criteria, caution is needed in interpreting the results. [ABSTRACT FROM AUTHOR]

Published

2010

13. Myeloid-derived suppressor cells in mammary tumor progression in FVB Neu transgenic mice.

Author

Abe, Fuminori, Dafferner, Alicia J., Donkor, Moses, Westphal, Sherry N., Scholar, Eric M., Solheim, Joyce C., Singh, Rakesh K., Hoke, Traci A., and Talmadge, James E.

Subjects

MOUSE mammary tumor virus, TRANSGENIC mice, SUPPRESSOR cells, REVERSE transcriptase polymerase chain reaction, FLOW cytometry, SPLEEN

Abstract

Female mice transgenic for the rat proto-oncogene c-erb-B2, under control of the mouse mammary tumor virus (MMTV) promoter (neuN), spontaneously develop metastatic mammary carcinomas. The development of these mammary tumors is associated with increased number of GR-1+CD11b+ myeloid derived suppressor cells (MDSCs) in the peripheral blood (PB), spleen and tumor. We report a complex relationship between tumor growth, MDSCs and immune regulatory molecules in non-mutated neu transgenic mice on a FVB background (FVB-neuN). The first and second tumors in FVB-neuN mice develop at a median of 265 (147–579) and 329 (161–523) days, respectively, resulting in a median survival time (MST) of 432 (201 to >500) days. During tumor growth, significantly increased number of MDSCs is observed in the PB and spleen, as well as, in infiltrating the mammary tumors. Our results demonstrate a direct correlation between tumor size and the number of MDSCs infiltrating the tumor and an inverse relationship between the frequency of CD4+ T-cells and MDSCs in the spleen. Quantitative reverse transcription-polymerase chain reaction (qRT-PCR) assessment of enzyme and cytokine transcript levels in the spleen, tumor, tumor-infiltrating non-parenchymal cells (NPCs) and mammary glands revealed a significant increase in transcript levels from grossly normal mammary glands and tumor-infiltrating NPCs during tumor progression. Tumor NPCs, as compared to spleen cells from wild-type (w/t) mice, expressed significantly higher levels of arginase-1 (ARG-1), nitric oxide synthase (NOS-2), vascular endothelial growth factor (VEGF-A) and significantly lower levels of interferon (IFN)-γ, interleukin (IL)-2 and fms-like tyrosine kinase-3 ligand (Flt3L) transcript levels. Transcript levels in the spleens of tumor-bearing (TB) mice also differed from normal mice, although to a lesser extent than transcript levels from tumor-infiltrating NPCs. Furthermore, both spleen cells and NPCs from TB mice, but not control mice, suppressed alloantigen responses by syngeneic control spleen cells. Correlative studies revealed that the number of MDSCs in the spleen was directly associated with granulocyte colony stimulating factor (G-CSF) transcript levels in the spleen; while the number of MDSCs in the tumors was directly correlated with splenic granulocyte macrophage stimulating factor (GM-CSF) transcript levels, tumor volume and tumor cell number. Together our results support a role for MDSCs in tumor initiation and progressive, T-cell depression and loss of function provide evidence which support multiple mechanisms of MDSC expansion in a site-dependent manner. [ABSTRACT FROM AUTHOR]

Published

2010

14. Her-2 DNA versus cell vaccine: immunogenicity and anti-tumor activity.

Author

Whittington, Paula J., Radkevich-Brown, Olga, Jacob, Jennifer B., Jones, Richard F., Weise, Amy M., and Wei-Zen Wei

Subjects

DNA vaccines, CANCER treatment, VACCINATION, CLINICAL trials, IMMUNE response

Abstract

Direct comparison and ranking of vaccine formulations in pre-clinical studies will expedite the identification of cancer vaccines for clinical trials. Two human ErbB-2 (Her-2) vaccines, naked DNA and whole cell vaccine, were tested side-by-side in wild type and Her-2 transgenic mice. Both vaccines can induce humoral and cellular immunity to the entire repertoire of Her-2 epitopes. Mice were electro-vaccinated i.m. with a mixture of pGM-CSF and pE2TM, the latter encodes Her-2 extracellular and transmembrane domains. Alternatively, mice were injected i.p. with human ovarian cancer SKOV3 cells that have amplified Her-2. In wild type mice, comparable levels of Her-2 antibodies (Ab) were induced by these two vaccines. However, T cell immunity and protection against Her-2+ tumors were superior in DNA vaccinated mice. In BALB Her-2 transgenic (Tg) mice, which were tolerant to Her-2, DNA and cell vaccines were administered after regulatory T cells (Treg) were removed by anti-CD25 mAb. Again, comparable levels of Her-2 Ab were induced, but DNA vaccines rendered greater anti-tumor activity. In B6xDR3 Her-2 Tg mice that expressed the autoimmune prone HLA-DR3 allele, higher levels of Her-2 Ab were induced by SKOV3 cell than by Her-2 DNA. But anti-tumor activity was still more profound in DNA vaccinated mice. Therefore, Her-2 DNA vaccine induced greater anti-tumor immunity than cell vaccine, whether mice were tolerant to Her-2 or susceptible to autoimmunity. Through such side-by-side comparisons in appropriate pre-clinical test systems, the more effective vaccine formulations will emerge as candidates for clinical trials. [ABSTRACT FROM AUTHOR]

Published

2009

15. Tiam1-deficiency impairs mammary tumor formation in MMTV-c- neu but not in MMTV-c- myc mice.

Author

Strumane, K., Rygiel, T., van der Valk, M., and Collard, J. G.

Subjects

CYTOSKELETAL proteins, NUCLEOTIDES, NUCLEIC acids, INTERFERON inducers, G proteins

Abstract

Rho-like small GTPases, including RhoA, Rac1 and Cdc42, are crucial for the regulation of a large variety of biological processes such as the cytoskeletal organization and gene transcription. The activities of Rho GTPases are predominantly controlled by guanine nucleotide exchange factors (GEFs), which activate GTPases by catalyzing the exchange of bound GDP for GTP. Earlier, we have identified the Tiam1 gene as an invasion-inducing gene that encodes a specific activator (GEF) of the Rac GTPase. We found that Tiam1-mediated Rac signaling functions in various aspects of tumorigenicity including the formation and progression of Ras-induced skin tumors and Wnt-induced intestinal tumors. Here, we further distinguish the oncogenic pathways that depend on Tiam1 signaling in the mammary gland. We crossed Tiam1 knockout mice with MMTV-c- myc and MMTV-c- neu transgenic mice, in which the expression of both oncogenes is targeted to the mammary gland leading to mammary tumorigenesis. We found Tiam1 important for Neu-induced tumor formation and progression but not for Myc-induced tumors. Tiam1-deficiency delayed Neu-induced tumor initiation and reduced metastasis but had no effect on the growth of the MMTV-c- neu tumors. Our data indicate that the Rac activator Tiam1 contributes to tumorigenicity induced by specific oncogenic signaling pathways only. [ABSTRACT FROM AUTHOR]

Published

2009

16. Association between HER-2 over-expression and prognosis in human osteosarcoma: a meta-analysis.

Author

Li, Yueguo and Zhang, Ning

Abstract

Various studies examining the relationship between HER-2 over-expression and the response to chemotherapy and clinical outcome in patients with osteosarcoma have yielded inconclusive results. The purpose of the current study was to evaluate the relation of HER-2 status with the response to chemotherapy and clinical outcome in osteosarcoma. We conducted a meta-analysis of 6 studies that evaluated the correlation between HER-2 status and histologic response to chemotherapy and 2-year survival. Data were synthesized in summary receiver operating characteristic curves and with summary likelihood ratios (LRs) and relative risk. The quantitative synthesis showed that HER-2 status is not a prognostic factor for the response to chemotherapy. The positive LR was 1.27 (95% confidence interval, 0.91∼1.77), and the negative LR was 0.68 (95% confidence interval, 0.38∼1.22). There was no significant between-study heterogeneity. HER2-positive status tended to be associated with a worse 2-year survival, but the overall results were not formally statistically significant. HER-2 status is not associated with the histologic response to chemotherapy in patients with osteosarcoma, whereas HER-2 positive patients may be associated with decreased survival. [ABSTRACT FROM AUTHOR]

Published

2008

17. Neu-mediated phosphorylation of protein tyrosine phosphatase epsilon is critical for activation of Src in mammary tumor cells.

Author

Berman-Golan, D. and Elson, A.

Subjects

PROTEIN-tyrosine phosphatase, CANCER cells, MORPHOLOGY, PHENOTYPES, PHOSPHORYLATION

Abstract

The receptor-type protein tyrosine phosphatase epsilon (RPTPɛ) activates c-Src in mammary tumor cells induced in vivo by Neu. Tumor cells lacking RPTPɛ exhibit reduced c-Src activity, appear less transformed morphologically and proliferate slower in vitro and in vivo. Expression of Src rescues most of these phenotypes, indicating that c-Src activity is important for maintaining the transformed phenotype. However, the molecular mechanisms that control activation of c-Src by RPTPɛ are unknown. We show that Neu induces phosphorylation of RPTPɛ exclusively at its C-terminal Y695, and that this phosphorylation is required for activation of c-Src by RPTPɛ. Phosphorylation of RPTPɛ does not affect its activity toward another substrate, the voltage-gated potassium channel Kv2.1, suggesting that phosphorylation directs RPTPɛ activity toward c-Src. Phosphorylation of RPTPɛ reduces its dimerization at the cell membrane, although this does not affect its activity significantly. RPTPɛ is subject to strong auto- and trans-dephosphorylation, suggesting that dephosphorylation limits the activation of c-Src downstream of Neu. We conclude that an Neu-RPTPɛ-Src signaling pathway exists in mammary tumor cells, in which phosphorylation of RPTPɛ by Neu directs RPTPɛ to activate c-Src. Reversible phosphorylation of RPTPɛ at Y695 may thus function as a ‘molecular switch’, which affects the substrate specificity of the phosphatase.Oncogene (2007) 26, 7028–7037; doi:10.1038/sj.onc.1210505; published online 7 May 2007 [ABSTRACT FROM AUTHOR]

Published

2007

18. The oncogene HER2: its signaling and transforming functions and its role in human cancer pathogenesis.

Author

Moasser, M. M.

Subjects

CANCER, CARCINOGENESIS, EPIDERMAL growth factor, ONCOGENES, CANCER genes

Abstract

The year 2007 marks exactly two decades since Human Epidermal Growth Factor Receptor-2 (HER2) was functionally implicated in the pathogenesis of human breast cancer. This finding established the HER2 oncogene hypothesis for the development of some human cancers. The subsequent two decades have brought about an explosion of information about the biology of HER2 and the HER family. An abundance of experimental evidence now solidly supports the HER2 oncogene hypothesis and etiologically links amplification of the HER2 gene locus with human cancer pathogenesis. The molecular mechanisms underlying HER2 tumorigenesis appear to be complex and a unified mechanistic model of HER2-induced transformation has not emerged. Numerous hypotheses implicating diverse transforming pathways have been proposed and are individually supported by experimental models and HER2 may indeed induce cell transformation through multiple mechanisms. Here I review the evidence supporting the oncogenic function of HER2, the mechanisms that are felt to mediate its oncogenic functions, and the evidence that links the experimental evidence with human cancer pathogenesis.Oncogene (2007) 26, 6469–6487; doi:10.1038/sj.onc.1210477; published online 30 April 2007 [ABSTRACT FROM AUTHOR]

Published

2007

19. Fatty acid synthase inhibitors are chemopreventive for mammary cancer in neu-N transgenic mice.

Author

Alli, Patricia M., Pinn, Michael L., Jaffee, Elizabeth M., McFadden, Jill M., and Kuhajda, Francis P.

Subjects

FATTY acids, CHEMOPREVENTION, XENOGRAFTS, TRANSGENIC mice, TUMORS, CANCER

Abstract

High levels of fatty acid synthase (FAS) have been found in cancer precursor lesions of the colon, stomach, esophagus, oral cavity, prostate, and breast. Inhibition of FAS with C75 has led to a significant antitumor effect in both human breast and prostate cancer xenografts. Recently, HER2/neu, which has also been identified in preneoplastic breast lesions, has been shown to regulate FAS expression through the PI3K/Akt signal transduction pathway rendering them susceptible to FAS inhibition. Utilizing the neu-N transgenic mouse model of mammary cancer, weekly treatment of the neu-N mice with C75 (30?mg/kg) for 10 weeks significantly delayed tumor progression. Only 20%of the C75-treated transgenic mice developed mammary carcinoma by 220 days, compared to 50%in the vehicle control animals. Two C75-treated animals never developed mammary cancer. Analysis of mammary tissue following 10 weeks of C75 treatment revealed a significant delay in mammary maturation as manifested by a reduction of the number and caliber of mammary ducts and budding epithelial structures. Apoptotic changes were increased, DNA synthesis was decreased, and the expressions of FAS, neu, Akt, phospho-Akt, and p21waf1 were all decreased when compared to vehicle controls and FVB/N mice. Importantly, these effects were restricted to the breast epithelial cells that overexpressed neu, not involving other normal duct structures in the skin, liver, or kidney. C247, an FAS inhibitor chemically distinct from C75, significantly delayed mammary maturation similar to C75. Thus, pharmacological inhibition of FAS affects the expression of key oncogenes involved in both cancer development and maintenance of the malignant phenotype. Moreover, these data identify FAS as a potential novel drug target for breast cancer chemoprevention.Oncogene (2005) 24, 39-46. doi:10.1038/sj.onc.1208174 Published online 18 October 2004 [ABSTRACT FROM AUTHOR]

Published

2005

20. Activated Neu/ErbB-2 Induces Expression of the Vascular Endothelial Growth Factor Gene by Functional Activation of the Transcription Factor Sp 1.

Author

Finkenzeller, Günter, Weindel, Karin, Zimmermann, Wolfgang, Westin, Gunnar, and Marmé, Dieter

Abstract

The neu(c- erbB-2 or HER2) proto-oncogene which encodes a receptor protein homologous to the epidermal growth factor receptor is overexpressed in 20%–30% of human breast and ovarian cancers. Oncogenic activation of Neu can also occur through multiple molecular mechanisms, including a point mutation in the transmembrane domain, deletion of the extracellular domain and short in-frame deletions of 7–12 amino acids in the extracellular region proximal to the transmembrane domain. Because of the highly vascularized phenotype of breast and ovarian cancers and the contribution of the Neu receptor to the development and progression of these tumors, we investigated the effect of Neu on the expression of the tumor angiogenesis factor VEGF. Expression of various activated Neu receptors but not wild-type Neu in Rat-1 cells, leads to increased VEGF expression on mRNA as well as on protein level. This effect is mediated by transcriptional activation of the VEGF promoter via a cluster of Sp 1 binding sites. Molecular analysis of the activation mechanism of Sp 1 revealed that neither the VEGF promoter binding activity of Sp 1 nor the expression of Sp 1 is affected by Neu transformation of the cells. Instead, functional Neu-induced transactivation of Sp 1 was observed by using a GAL4-based transactivation assay. These results demonstrate that functional changes of the transcription factor Sp 1 mediates a Neu-signaling cascade leading to VEGF promoter activation. [ABSTRACT FROM AUTHOR]

Published

2004

21. Contrasting effects of VEGF gene disruption in embryonic stem cell-derived versus oncogene-induced tumors.

Author

Viloria-Petit, Alicia, Miquerol, Lucile, Yu, Joanne L., Gertsenstein, Marina, Sheehan, Capucine, May, Linda, Henkin, Jack, Lobe, Corrinne, Nagy, Andras, Skerbel, Robert, and Rak, Janusz

Subjects

GENE targeting, GENETIC engineering, VASCULAR endothelial growth factors, CYTOKINES, IMMUNOREGULATION, EPITHELIUM

Abstract

Previous gene targeting studies have implicated an indispensable role of vascular endothelial growth factor (VEGF) in tumor angiogenesis, particularly in tumors of embryonal or endocrine origin. In contrast, we report here that transformation of VEGF-deficient adult fibroblasts (MDF528) with ras or neu oncogenes gives rise to highly tumorigenic and angiogenic fibro-sarcomas. These aggressive VEGF-null tumors (S28ras, S28neu) originated from VEGF-/- embryonic stem cells, which themselves were tumorigenically deficient. We also report that VEGF production by tumor stroma has a modest rote in oncogene-driven tumor angiogenesis. Both ras and neu oncogenes down-regulated at least two endogenous inhibitors of angiogenesis [pigment epithelium derived factor (PEDF) and thrombospondin 1 (TSP-1)]. This is functionally important as administration of an antiangiogenic TSP-1 peptide (ABT-526) markedly inhibited growth of VEGF-/- tumors, with some ingress of pericytes. These results provide the first definitive genetic demonstration of the dispensability of tumor cell-derived VEGF in certain cases of 'adult' tumor angiogenesis, and thus highlight the importance of considering VEGF-independent as welt as VEGF- dependent pathways when attempting to block this process pharmacologically. [ABSTRACT FROM AUTHOR]

Published

2003

22. Transfection of the c-erbB2/neu gene upregulates the expression of sialyl Lewis X, α1,3-fucosyltransferase VII, and metastatic potential in a human hepatocarcinoma cell line.

Author

Liu, Fei, Qi, Hui-Ling, Zhang, Ying, Zhang, Xia-Ying, and Chen, Hui-Li

Subjects

ONCOGENES, METASTASIS, LIVER cells, DISEASES

Abstract

The pCMV4 plasmid containing the cancer-promoting gene, c-erbB2/neu, was cotransfected into the human hepatocarcinoma cell line 7721 with the pcDNA3 vector, which contains the ‘neo’ selectable marker. Several clones showing stable expression of c-erbB2/neu were established and characterized by determination of c-erbB2/neu mRNA and its encoded protein p185. Expression of Lewis antigens and α1,3-fucosyltransferases and the biological behavior of 7721 cells after c-erbB2/neu transfection were studied using mock cells transfected with the vectors pCMV4 and pcDNA3 as controls. SLex expression on the surface of mock cells was high, whereas expression of SDLex, Lex and SLea was absent or negligible. This is compatible with the abundant expression of α1,3-fucosyltransferase VII, very low expression of αfucosyltransferase III/VI, and almost absent expression of α1,3-fucosyltransferase IV in the mock cells. After transfection of c-erbB2/neu, expression of SLex and α1,3-fucosyltransferase VII were simultaneously elevated, but that of αfucosyltransferase III/VI was not altered. The expression of both SLex and α1,3-fucosyltransferase VII correlated positively with the expression of c-erbB2/neu in different clones, being highest in clone 13, medium in clone 6, and lowest in clone 7. In addition, the adhesion of 7721 cells to human umbilical vein endothelial cells (HUVECs) or P-selectin, as well as cell migration and invasion, were increased in c-erbB2/neu-transfected cells. These increases also correlated positively with the expression intensities of c-erbB2/neu, SLex and α1,3-fucosyltransferase VII in the different clones, whereas cell adhesion to fibronectin correlated negatively with these variables. mAbs to SLex (KM93) and SDLex (FH6) significantly and slightly, respectively, abolished cell adhesion to HUVECs or P-selectin and cell migration and invasion. mAbs to SDLex and SLea did not suppress cell adhesion to HUVECs nor inhibit cell migration and invasion. Transfection of α1,3-fucosyltransferase VII cDNA into 7721 cells showed similar results to transfection of c-erbB2/neu, and the increased adhesion to HUVECs, cell migration, and invasion were also inhibited significantly by KM93 and slightly by FH6. These results indicate that expression of α1,3-fucosyltransferase VII and its specific product, SLex, and their capacity for cell adhesion, migration and invasion are closely related. Therefore, the c-erbB2/neu gene is proposed to be a metastasis-promoting gene, and its effects are at least partially mediated by the increased expression of α1,3-fucosyltransferase VII and SLex. [ABSTRACT FROM AUTHOR]

Published

2001

23. The neu-protein and breast cancer.

Author

Potter, Christian and Schelfhout, Anne-Marie

Abstract

The neu-protein is overexpressed in about 20% of invasive duct cell carcinomas of the breast. The only reliable sign for neu-overexpression by immunohistochemistry is membrane staining. Its overexpression is correlated with decreased overall survival and disease free survival due to increased metastatic activity of neu-overexpressing tumour cells. This increased metastatic potential is a consequence of the motility enhancing activity of the neu-protein, which is exclusively expressed on pseudopodia, and to a lesser extent of its growth stimulating effect. From a clinical point of view, the assessment of neu-overexpression in breast cancer might become a useful tool in the future treatment of patients by chemotherapy, since patients whose tumour shows neu-overexpression benefit from higher doses of chemotherapy. The molecule plays a key role in the pathogenesis of Paget's disease of the breast. A chemotactic factor which is secreted by epidermal keratinocytes attracts the Paget cells to spread into the epidermis and acts via the neu-protein. In ductal carcinoma in situ, the combination of neu-overexpression and large cell type is highly correlated with extent of disease and therefore neu-overexpression might be a predictive marker for recurrence of disease after tumour resection. [ABSTRACT FROM AUTHOR]

Published

1995

24. Age- and dose-dependent transplacental carcinogenesis by N-nitrosoethylurea in Syrian golden hamsters.

Author

Diwan, Bhalchandra, Rehm, Sabine, and Rice, Jerry

Abstract

Syrian golden hamsters have a very short period (15 days) of gestation. The implantation of the balstocyst occurs on day 5, embryogenesis proceeds very rapidly thereafter and neural tube closure is completed by day 9. In the present study the effects of two different doses of N-nitrosoethylurea (NEU) administered at various stages of gestation were quantitatively evaluated in Syrian golden hamsters. NEU at either 0.2 or 0.5 mmol/kg was administered transplacentally as a single i.p. injection to pregnant hamsters on gestation days 7, 8, 9, 10, 11, 12, 13, or 14. The incidence, latency period and multiplicity of tumors varied with the dose of NEU and the stage of development at the time of NEU administration. Although tumors of the peripheral nervous system predominated, a variety of other tumors, including melanomas and visceral tumors of epithelial and mesenchymal origin, were also observed in hamster offspring exposed transplacentally to NEU. Sensitivity to transplacental carcinogenesis was maximal during late gestation and very low before day 9. [ABSTRACT FROM AUTHOR]

Published

1996

25. The neu oncogene product in serum and tissue of patients with metastatic gastrointestinal carcinomas.

Author

Vogel, W., Kath, R., Kosmehl, H., Olschowsky, E., and Höffken, K.

Abstract

We report on our experience investigating the serum levels of the soluble domain of p185 and the neu protein expression in the corresponding tumour tissue in patients with advanced gastrointestinal carcinomas. The study included 32 patients who were treated with palliative chemotherapy. The serum levels of the neu protein were investigated by immunosorbent assay techniques. We used the alkaline phosphatase/anti-(alkaline phosphatase) method for investigating the corresponding tumour tissue immunohistochemically. Increased serum neu protein levels were found in 8 of 22 (36%) patients with colorectal carcinomas and in 2 patients with advanced abdominal adenocarcinoma of unknown primary. All other patients with advanced gastrointestinal cancers were serum- neu-protein-negative. All serum- neu-protein-positive patients with colorectal carcinomas showed also an elevated neu protein expression. The extent of serum neu protein expression corresponded to the clinical course and the tumour marker CA 19-9. The serum neu protein may be useful for monitoring patients with advanced colorectal carcinomas, particularly in cases of immunohistochemical neu-protein-positive primary tumours. [ABSTRACT FROM AUTHOR]

Published

1996

26. Humoral and cellular responses raised against the human HER2 oncoprotein are cross-reactive with the homologous product of the neu proto-oncogene, but do not protect rats against B104 tumors expressing mutated neu.

Author

Taylor, Peter, Gerder, Marlene, Moros, Zoila, and Feldmann, Marc

Abstract

The neu proto-oncogene encodes a plasma membrane protein belonging to the epidermal growth factor receptor family. The cell line B104, derived from a BDIX rat neuroblastoma, carries a point mutation in neu, and forms a tumor when injected into these rats. The human homologue of the neu oncogene (here called HER2) is overexpressed in certain types of cancer. Rats were immunized with HER2 protein (HER2) to investigate a possible cross-reaction between the homologous proteins which could protect them against subsequent inoculation with B104. Specific antibody in the serum was measured by cell-based enzyme-linked immunosorbent assay and fluorescence immunocytochemistry, and delayed-type hypersensitivity by an ear assay. Sera from animals immunized with the HER2 extracellular domain (HER2-ECD) reacted with both HER2- and neu-expressing cells. In the ear assay, a significant cellular response to both HER2-ECD ( P <0.05) and neu protein ( P <0.001) was observed in HER2-ECD-immunized rats. However, the growth of B104 tumors in rats was not affected by preimmunization with HER2-ECD. The results indicate that an autoreactive immune response to neu was induced by immunization with HER2-ECD, but was too weak to affect the growth of the neu-bearing tumor. [ABSTRACT FROM AUTHOR]

Published

1996

27. Activation of Mauthner neurons during prey capture.

Author

Canfield, J. and Rose, G.

Abstract

The Mauthner (M-) cells, a bilateral pair of medullary neurons in fish, initiate the characteristic 'C-start' predatory escape response of teleosts. Similar movements have been described during hatching, social interactions, and feeding. M-cell firing, however, has not been correlated directly with these other behaviors. The objective of this study was to determine whether the M-cell, in addition to escape, plays a role in feeding. [ABSTRACT FROM AUTHOR]

Published

1993

28. Transcriptional Regulation of Type I Receptor Tyrosine Kinases in the Mammary Gland.

Author

Bates, Nicholas and Hurst, Helen

Abstract

The transcriptional regulation of the human EGFR3 and ERBB2 genes has been extensively studied, particularly in the context of their overexpression in breast cancer. Here we summarize published work detailing the transcription factors which interact with the promoters of these and the rat ERBB2 homologue, neu, genes and discuss their possible relevance to gene activation in cancer. In addition we review the biologically significant molecules which modulate expression of these genes and discuss the nuclear factors involved in mediating these responses. We also describe novel therapies which may result from these studies and highlight directions for future research into the control of expression of the EGFR and ERBB2 genes in the normal mammary gland and in breast cancer. [ABSTRACT FROM AUTHOR]

Published

1997

29. When All Colonies Are Blue.

Published

2005

30. Application of the AMeX method to the evaluation of HER-2 status in breast carcinomas: Comparison with the results of HercepTest.

Author

Mizogami, Masayo, Sakurai, Shinji, Kikuchi, Midori, Ohta, Kenichi, Sakurai, Tatsuo, Tanaka, Akira, and Saito, Ken

Subjects

MONOCLONAL antibodies, HER2 protein, BREAST cancer

Abstract

The recent development of the recombinant humanized monoclonal antibody against HER-2 oncoprotein requires a simple and accurate method for the evaluation of HER-2 status in patients with breast cancers. We here report that the evaluation of the HER-2 status is improved by the use of the acetone-methanol-xylene (AMeX) method. Compared with an ordinary test of HercepTest, 25 out of 63 cases (39.7%) were scored upwards by the AMeX method. In addition, the HER-2 gene amplification was easily estimated by fluorescence in situ hybridization (FISH) using the AMeX method. Thus, the AMeX method is likely to provide more improved data about the HER-2 status in breast carcinoma specimens. [ABSTRACT FROM AUTHOR]

Published

2003

31. Anti-HER2/Neu passive-aggressive immunotherapy.

Author

Mortenson, Eric D and Fu, Yang-Xin

Subjects

TRASTUZUMAB, IMMUNOTHERAPY, CD4 antigen, ONCOGENES, CELL communication, ANTINEOPLASTIC agents, DRUG efficacy, THERAPEUTICS

Abstract

Preclinical studies have established that CD8+T cells are necessary for efficient immunotherapeutic regimens targetingv-erb-b2avian erythroblastic leukemia viral oncogene homolog 2 (ERBB2, best known as HER2/Neu). Recently, we extended upon these findings by demonstrating that anti-HER2/Neu therapy also requires CD4+T cells and CD40/CD40L signaling within the tumor microenvironment. Our results add to mounting evidence demonstrating that adaptive immunity is crucial to the efficacy of conventional and targeted anticancer chemotherapeutics. [ABSTRACT FROM PUBLISHER]

Published

2014