Your search keyword '"Jane Barraclough"' showing total 15 results

1. Increases in c-Yes Expression Level and Activity Promote Motility But Not Proliferation of Human Colorectal Carcinoma Cells

Author

Jane Barraclough, Cassandra Hodgkinson, Alison Hogg, Caroline Dive, and Arkadiusz Welman

Subjects

c-Yes, c-Src, colon cancer, proliferation, motility, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Increases in the levels and/or activity of nonreceptor tyrosine kinases c-Src and c-Yes are often associated with colorectal carcinogenesis. The physiological consequences of increased c-Yes activity during the early and late stages of tumorigenesis, in addition to the degree of redundancy between c-Yes and c-Src in colorectal cancer cells, remain elusive. To study the consequences of increases in c-Yes levels and activity in later stages of colorectal carcinogenesis, we developed human colorectal cancer cell lines in which c-Yes levels and activity can be inducibly increased by a tightly controlled expression of wild-type c-Yes or by constitutively active mutants of c-Yes, c-YesY537F, c-YesΔr6aa. c-Yes induction resulted in increased cell motility but did not promote proliferation either in vitro or in vivo. These results suggest that in later stages of colorectal carcinogenesis, elevations in cYes levels/activity may promote cancer spread and metastasis rather than tumor growth.

Published

2007

2. Increases in c-Src Expression Level and Activity Do Not Promote the Growth of Human Colorectal Carcinoma Cells In Vitro and In Vivo

Author

Arkadiusz Welman, Christopher Cawthome, Lourdes Ponce-Perez, Jane Barraclough, Sarah Danson, Stephen Murray, Jeff Cummings, Terry D. Allen, and Caroline Dive

Subjects

c-Src, colon cancer, proliferation, cell death, Tet On, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The levels and activity of c-Src in colorectal cancer cells increase steadily during the course of colorectal carcinogenesis and are most highly elevated in advanced metastatic disease. However, the effects of increases in c-Src activity on the proliferation of colorectal cancer cells during early and late stages of tumorigenesis remain elusive. To study the consequences of increases in c-Src levels and activity on the growth of colorectal cancer cells in later stages of colorectal carcinogenesis, we developed human colorectal cancer cell lines in which c-Src levels and activity could be inducibly increased by a tightly controlled expression of wild-type c-Src or of the constitutively active mutant of c-Src, c-SrcY527F. Src induction activated multiple signaling pathways (often associated with a proliferative response) but promoted neither cell proliferation in vitro nor tumor growth in a xenograft model in vivo. These results indicate that, in more advanced stages of colorectal carcinogenesis, increases in c-Src levels and activity are likely to have functions other than the direct promotion of tumor growth.

Published

2006

3. Supplementary Figure 3 from Cyclin E2 Overexpression Is Associated with Endocrine Resistance but not Insensitivity to CDK2 Inhibition in Human Breast Cancer Cells

Author

Elizabeth A. Musgrove, Cristin G. Print, Robert L. Sutherland, Rob I. Nicholson, Julia M. Gee, Lance D. Miller, Michael A. Black, Christine S. Lee, Jane Barraclough, Andrew Stone, Marijke N. Boersma, Anita Muthukaruppan, Jian Kang, C. Marcelo Sergio, and C. Elizabeth Caldon

Abstract

PDF file, 41KB, Supplementary Figure 3: Effect of overexpression of cyclins E1 and E2 on antiestrogen-induced growth arrest. T-47D cells overexpressing cyclin E1, cyclin E2 or vector control were treated with fulvestrant or vehicle. Densitometry of Western blots of cell lysates collected after 24h (A) or 48h (B) fulvestrant treatment. Loading was corrected using β-actin levels. Data represent mean � SEM of quadruplicate experiments.

Published

2023

4. Data from Cyclin E2 Overexpression Is Associated with Endocrine Resistance but not Insensitivity to CDK2 Inhibition in Human Breast Cancer Cells

Author

Elizabeth A. Musgrove, Cristin G. Print, Robert L. Sutherland, Rob I. Nicholson, Julia M. Gee, Lance D. Miller, Michael A. Black, Christine S. Lee, Jane Barraclough, Andrew Stone, Marijke N. Boersma, Anita Muthukaruppan, Jian Kang, C. Marcelo Sergio, and C. Elizabeth Caldon

Abstract

Cyclin E2, but not cyclin E1, is included in several gene signatures that predict disease progression in either tamoxifen-resistant or metastatic breast cancer. We therefore examined the role of cyclin E2 in antiestrogen resistance in vitro and its potential for therapeutic targeting through cyclin-dependent kinase (CDK) inhibition. High expression of CCNE2, but not CCNE1, was characteristic of the luminal B and HER2 subtypes of breast cancer and was strongly predictive of shorter distant metastasis-free survival following endocrine therapy. After antiestrogen treatment of MCF-7 breast cancer cells, cyclin E2 mRNA and protein were downregulated and cyclin E2–CDK2 activity decreased. However, this regulation was lost in tamoxifen-resistant (MCF-7 TAMR) cells, which overexpressed cyclin E2. Expression of either cyclin E1 or E2 in T-47D breast cancer cells conferred acute antiestrogen resistance, suggesting that cyclin E overexpression contributes to the antiestrogen resistance of tamoxifen-resistant cells. Ectopic expression of cyclin E1 or E2 also reduced sensitivity to CDK4, but not CDK2, inhibition. Proliferation of tamoxifen-resistant cells was inhibited by RNAi-mediated knockdown of cyclin E1, cyclin E2, or CDK2. Furthermore, CDK2 inhibition of E-cyclin overexpressing cells and tamoxifen-resistant cells restored sensitivity to tamoxifen or CDK4 inhibition. Cyclin E2 overexpression is therefore a potential mechanism of resistance to both endocrine therapy and CDK4 inhibition. CDK2 inhibitors hold promise as a component of combination therapies in endocrine-resistant disease as they effectively inhibit cyclin E1 and E2 overexpressing cells and enhance the efficacy of other therapeutics. Mol Cancer Ther; 11(7); 1488–99. ©2012 AACR.

Published

2023

5. Supplementary Methods, Figure Legends and Tables 1 - 2 from Cyclin E2 Overexpression Is Associated with Endocrine Resistance but not Insensitivity to CDK2 Inhibition in Human Breast Cancer Cells

Author

Elizabeth A. Musgrove, Cristin G. Print, Robert L. Sutherland, Rob I. Nicholson, Julia M. Gee, Lance D. Miller, Michael A. Black, Christine S. Lee, Jane Barraclough, Andrew Stone, Marijke N. Boersma, Anita Muthukaruppan, Jian Kang, C. Marcelo Sergio, and C. Elizabeth Caldon

Abstract

PDF file, 56KB.

Published

2023

6. Supplementary Figure 1 from Cyclin E2 Overexpression Is Associated with Endocrine Resistance but not Insensitivity to CDK2 Inhibition in Human Breast Cancer Cells

Author

Elizabeth A. Musgrove, Cristin G. Print, Robert L. Sutherland, Rob I. Nicholson, Julia M. Gee, Lance D. Miller, Michael A. Black, Christine S. Lee, Jane Barraclough, Andrew Stone, Marijke N. Boersma, Anita Muthukaruppan, Jian Kang, C. Marcelo Sergio, and C. Elizabeth Caldon

Abstract

PDF file, 929KB, Supplementary Figure 1: Cyclin E2 association with breast cancer subtype, grade, and outcome. A: Relationship between a second cyclin E2 probeset and breast cancer subtype, or histological grade. Box: upper and lower quartiles; dividing line: median. B: Relative expression of cyclin E1 and a second cyclin E2 probeset in individual tumours in breast cancer subtypes. C: Kaplan-Meier survival analysis of distant metastasis-free survival from ER-positive patients treated with endocrine therapy (n=287) and untreated ER-negative patients (n=106), using a 70% cutoff between high and low expression.

Published

2023

7. Supplementary Figure 2 from Cyclin E2 Overexpression Is Associated with Endocrine Resistance but not Insensitivity to CDK2 Inhibition in Human Breast Cancer Cells

Author

Elizabeth A. Musgrove, Cristin G. Print, Robert L. Sutherland, Rob I. Nicholson, Julia M. Gee, Lance D. Miller, Michael A. Black, Christine S. Lee, Jane Barraclough, Andrew Stone, Marijke N. Boersma, Anita Muthukaruppan, Jian Kang, C. Marcelo Sergio, and C. Elizabeth Caldon

Abstract

PDF file, 78KB, Supplementary Figure 2: Deregulation of cyclin E in tamoxifen-resistant cells. MCF-7C and TAMR cells were treated with vehicle, OH-Tam (100 nM) or fulvestrant (10 nM). A: S phase percentage derived from flow cytometry of propidium iodide-stained cells. B: Densitometry of Western blots using GAPDH as a loading control. Data represent the mean � range of duplicate experiments.

Published

2023

8. Cyclin E2 Overexpression Is Associated with Endocrine Resistance but not Insensitivity to CDK2 Inhibition in Human Breast Cancer Cells

Author

Crispin G. Print, Robert Ian Nicholson, Christine Lee, Robert L. Sutherland, Andrew Stone, Michael A. Black, Jian Kang, C. Elizabeth Caldon, Lance D. Miller, Anita Muthukaruppan, C. Marcelo Sergio, Julia Margaret Wendy Gee, Marikje N. Boersma, Elizabeth A. Musgrove, and Jane Barraclough

Subjects

Cancer Research, Cyclin E, Cyclin D, Cyclin B, Gene Expression, Breast Neoplasms, Estrogen Receptor Modulators, Cyclin-dependent kinase, Cell Line, Tumor, Cyclins, Humans, skin and connective tissue diseases, Protein Kinase Inhibitors, Cell Proliferation, Neoplasm Staging, Cyclin, Oncogene Proteins, biology, Gene Expression Profiling, Cyclin-Dependent Kinase 2, Cell biology, Cyclin E1, Cyclin E2, Oncology, Drug Resistance, Neoplasm, biology.protein, Cancer research, Female, Cyclin A2, Signal Transduction

Abstract

Cyclin E2, but not cyclin E1, is included in several gene signatures that predict disease progression in either tamoxifen-resistant or metastatic breast cancer. We therefore examined the role of cyclin E2 in antiestrogen resistance in vitro and its potential for therapeutic targeting through cyclin-dependent kinase (CDK) inhibition. High expression of CCNE2, but not CCNE1, was characteristic of the luminal B and HER2 subtypes of breast cancer and was strongly predictive of shorter distant metastasis-free survival following endocrine therapy. After antiestrogen treatment of MCF-7 breast cancer cells, cyclin E2 mRNA and protein were downregulated and cyclin E2–CDK2 activity decreased. However, this regulation was lost in tamoxifen-resistant (MCF-7 TAMR) cells, which overexpressed cyclin E2. Expression of either cyclin E1 or E2 in T-47D breast cancer cells conferred acute antiestrogen resistance, suggesting that cyclin E overexpression contributes to the antiestrogen resistance of tamoxifen-resistant cells. Ectopic expression of cyclin E1 or E2 also reduced sensitivity to CDK4, but not CDK2, inhibition. Proliferation of tamoxifen-resistant cells was inhibited by RNAi-mediated knockdown of cyclin E1, cyclin E2, or CDK2. Furthermore, CDK2 inhibition of E-cyclin overexpressing cells and tamoxifen-resistant cells restored sensitivity to tamoxifen or CDK4 inhibition. Cyclin E2 overexpression is therefore a potential mechanism of resistance to both endocrine therapy and CDK4 inhibition. CDK2 inhibitors hold promise as a component of combination therapies in endocrine-resistant disease as they effectively inhibit cyclin E1 and E2 overexpressing cells and enhance the efficacy of other therapeutics. Mol Cancer Ther; 11(7); 1488–99. ©2012 AACR.

Published

2012

9. Generation of cells expressing improved doxycycline-regulated reverse transcriptional transactivator rtTA2S-M2

Author

Jane Barraclough, Arkadiusz Welman, and Caroline Dive

Subjects

Regulation of gene expression, Cell signaling, Electroporation, Transfection, Computational biology, Biology, Flow Cytometry, General Biochemistry, Genetics and Molecular Biology, Cell Line, Internal ribosome entry site, Transduction (genetics), Gene Expression Regulation, Cell culture, Doxycycline, Gene expression, Trans-Activators, Humans, Genetic Engineering, Plasmids

Abstract

Tet-on cell lines engineered to stably express doxycycline (Dox)-regulated reverse transcriptional transactivator (rtTA) have many applications in biomedical research and biotechnology. Unfortunately, construction and maintenance of such cells often proves to be costly, labor intensive and ineffective. Moreover, the Tet-on clones generated using standard methodology were often unstable and frequently displayed significantly changed physiological properties compared with their parental cells. Here we describe an optimized protocol for generation of Tet-on cells. The protocol is based on the use of a recently developed pN1p beta actin-rtTA2S-M2-IRES-EGFP vector (where IRES is an internal ribosome entry site) and permits relatively inexpensive construction of many Tet-on clones with essentially 100% efficiency. The method is well suited for 'difficult' cell lines displaying genetic instability and high levels of epigenetic silencing. The constructed Tet-on cells remain stable with time in the absence of any selection agents, are easy to monitor and preserve the characteristics of parental cells. The protocol can be completed in 2 months.

Published

2006

10. Construction and characterization of multiple human colon cancer cell lines for inducibly regulated gene expression

Author

Gareth J. Griffiths, Jane Barraclough, Arkadiusz Welman, Christopher Cawthorne, Judith C. Williams, Ian J. Stratford, Caroline Dive, Nigel K Smith, and Rachel L. Cowen

Subjects

Regulation of gene expression, Oncogene, Blotting, Western, Cytomegalovirus, Cell Biology, Biology, Cell cycle, Biochemistry, Molecular biology, Green fluorescent protein, Gene Expression Regulation, Neoplastic, Transactivation, Cell culture, In vivo, Cell Line, Tumor, Doxycycline, Gene expression, Humans, Electrophoresis, Polyacrylamide Gel, Transgenes, Promoter Regions, Genetic, Molecular Biology, Plasmids, Subcellular Fractions

Abstract

Validation of targets for cancer drug discovery requires robust experimental models. Systems based on inducible gene expression are well suited to this purpose but are difficult to establish in several epithelial cell types. Using the recently discovered transcriptional transactivator (rtTA2S-M2), we developed a strategy for fast and efficient generation of Tet On cells. Multiple clones of HCT116, SW480, and HT29 human colon cancer cells for doxycycline-regulated gene expression were constructed that constitutively express green fluorescent protein (GFP) for selection/maintenance purposes. The cell lines displayed good fold inducibility (49-124xHCT116; 178-621xSW480; 261-787xHT29) and minimal leakiness after transient transfection with a luciferase reporter or with vectors driving inducible expression of red fluorescent protein (dsRed2), constitutively active c-Src or dominant negative K-Ras4B. The clones preserved their transformed phenotype as demonstrated by comparing their properties to respective wild type cells, in terms of growth in vitro and in vivo (as tumor xenografts), cell cycle traverse, and sensitivity to drugs used in chemotherapy. These engineered cell lines enabled tightly controlled inducible gene expression both in vitro and in vivo, and proved well suited for construction of double-stable cell lines inducibly expressing a protein of interest. As such they represent a useful research tool for example, to dissect oncogene function(s) in colon cancer. Supplementary material for this article be found at http://www.mrw.interscience.wiley.com/suppmat/0730-2312/suppmat/94/suppmat_welman.doc.

Published

2005

11. Cyclin D as a therapeutic target in cancer

Author

C. Elizabeth Caldon, Elizabeth A. Musgrove, Andrew Stone, Jane Barraclough, and Robert L. Sutherland

Subjects

Polymorphism, Genetic, biology, business.industry, Applied Mathematics, General Mathematics, Cyclin D, Cyclin A, Cyclin B, Oncogenes, Cyclin D1, Cyclin-dependent kinase, Neoplasms, biology.protein, Cancer research, Medicine, Humans, Cyclin-dependent kinase 6, business, Cyclin A2, Cyclin

Abstract

Cyclin D1, and to a lesser extent the other D-type cyclins, is frequently deregulated in cancer and is a biomarker of cancer phenotype and disease progression. The ability of these cyclins to activate the cyclin-dependent kinases (CDKs) CDK4 and CDK6 is the most extensively documented mechanism for their oncogenic actions and provides an attractive therapeutic target. Is this an effective means of targeting the cyclin D oncogenes, and how might the patient subgroups that are most likely to benefit be identified?

Published

2011

12. Difluoro analogue of UCS15A triggers activation of exogenously expressed c-Src in HCT 116 human colorectal carcinoma cells

Author

Arkadiusz Welman, Sally Freeman, Christopher Cawthorne, Caroline Dive, Richard A. Bryce, Jane Barraclough, and Noor Atatreh

Subjects

Conformational change, Protein Conformation, Enzyme Activators, Biology, Models, Biological, SH3 domain, Cell Line, Tumor, Drug Discovery, Humans, Computer Simulation, Kinase activity, Pharmacology, Src homology domain, Molecular Structure, Activator (genetics), Effector, Carcinoma, General Medicine, Fluorine, Molecular biology, Enzyme Activation, src-Family Kinases, Benzaldehydes, Colorectal Neoplasms, Tyrosine kinase, o-Phthalaldehyde, Proto-oncogene tyrosine-protein kinase Src

Abstract

UCS 15A, an antibiotic produced by Streptomyces sp., has been reported to specifically disrupt SH3 domain-mediated interactions in eukaryotic cells. Interestingly, in the case of the non-receptor tyrosine kinase Src, UCS15A was effective in suppressing the SH3 domain-mediated intermolecular rather than intramolecular interactions, and thus prevented Src interactions with certain downstream effectors without affecting Src kinase activity. Here the synthesis of a novel difluoro analogue of UCS15A is described. The effects of this compound (8) on Src activity were tested in HCT 116 colorectal carcinoma cells engineered for inducible expression of c-Src. The presence of compound (8) resulted in the increased activity of the induced c-Src implicating that (8) acts as a c-Src activator in vivo. These observations are supported by computer modelling studies which suggest that the aldehyde group of (8) may covalently bind to a lysine residue in the SH2-kinase linker region situated in the proximity of the SH3 domain, which could promote a conformational change resulting in increased Src activity.

Published

2007

13. Increases in c-Yes Expression Level and Activity Promote Motility But Not Proliferation of Human Colorectal Carcinoma Cells

Author

Alison Hogg, Caroline Dive, Cassandra L Hodgkinson, Jane Barraclough, and Arkadiusz Welman

Subjects

Cancer Research, c-Yes, Colorectal cancer, proliferation, Recombinant Fusion Proteins, c-Src, Motility, Adenocarcinoma, Biology, Mouse model of colorectal and intestinal cancer, medicine.disease_cause, lcsh:RC254-282, Metastasis, Mice, Cell Movement, Cell Line, Tumor, Cell Adhesion, medicine, Animals, Humans, Proto-Oncogene Proteins c-yes, Cancer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Neoplasm Proteins, src-Family Kinases, colon cancer, motility, Doxycycline, Enzyme Induction, Immunology, Cancer research, Female, Colorectal Neoplasms, Carcinogenesis, human activities, Tyrosine kinase, Cell Division, Neoplasm Transplantation, Research Article

Abstract

Increases in the levels and/or activity of nonreceptor tyrosine kinases c-Src and c-Yes are often associated with colorectal carcinogenesis. The physiological consequences of increased c-Yes activity during the early and late stages of tumorigenesis, in addition to the degree of redundancy between c-Yes and c-Src in colorectal cancer cells, remain elusive. To study the consequences of increases in c-Yes levels and activity in later stages of colorectal carcinogenesis, we developed human colorectal cancer cell lines in which c-Yes levels and activity can be inducibly increased by a tightly controlled expression of wild-type c-Yes or by constitutively active mutants of c-Yes, c-YesY537F, c-YesΔr6aa. c-Yes induction resulted in increased cell motility but did not promote proliferation either in vitro or in vivo . These results suggest that in later stages of colorectal carcinogenesis, elevations in cYes levels/activity may promote cancer spread and metastasis rather than tumor growth.

Published

2007

14. Increases in c-Src Expression Level and Activity Do Not Promote the Growth of Human Colorectal Carcinoma Cells In Vitro and In Vivo

Author

Caroline Dive, Jane Barraclough, Terence D Allen, Stephen M Murray, Jeffrey Cummings, Lourdes Ponce-Perez, Christopher Cawthorne, Arkadiusz Welman, and Sarah Danson

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Programmed cell death, Colorectal cancer, Cell growth, proliferation, c-Src, Mouse model of colorectal and intestinal cancer, Biology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, medicine.disease_cause, lcsh:RC254-282, cell death, colon cancer, Cell culture, Internal medicine, Tet On, medicine, Cancer research, Signal transduction, Carcinogenesis, Proto-oncogene tyrosine-protein kinase Src

Abstract

The levels and activity of c-Src in colorectal cancer cells increase steadily during the course of colorectal carcinogenesis and are most highly elevated in advanced metastatic disease. However, the effects of increases in c-Src activity on the proliferation of colorectal cancer cells during early and late stages of tumorigenesis remain elusive. To study the consequences of increases in c-Src levels and activity on the growth of colorectal cancer cells in later stages of colorectal carcinogenesis, we developed human colorectal cancer cell lines in which c-Src levels and activity could be inducibly increased by a tightly controlled expression of wild-type c-Src or of the constitutively active mutant of c-Src, c-SrcY527F. Src induction activated multiple signaling pathways (often associated with a proliferative response) but promoted neither cell proliferation in vitro nor tumor growth in a xenograft model in vivo. These results indicate that, in more advanced stages of colorectal carcinogenesis, increases in c-Src levels and activity are likely to have functions other than the direct promotion of tumor growth.

Published

2006

15. Construction and characterization of multiple human colon cancer cell lines for inducibly regulated gene expressionArkadiusz Welman and Christopher Cawthorne have contributed equally to this study.

Author

Arkadiusz Welman, Christopher Cawthorne, Jane Barraclough, Nigel Smith, Gareth J. Griffiths, Rachel L. Cowen, Judith C. Williams, Ian J. Stratford, and Caroline Dive

Published

2005