Your search keyword '"Munro, Alison F."' showing total 5 results

1. A conformation selective mode of inhibiting SRC improves drug efficacy and tolerability

Author

University of Edinburgh, Ministerio de Ciencia, Innovación y Universidades (España), European Commission, CSIC - Centro de Investigaciones Biológicas Margarita Salas (CIB), Universidad de Granada, Wellcome Trust, Lietha, Daniel [0000-0002-6133-6486], Webb, Emily R. [0000-0001-9339-4544], Li, Xue-Feng [0000-0003-2612-0310], Muir, Morwenna [0000-0001-5835-3886], Luque-Ortega, Juan Román [0000-0003-3206-7480], Beetham, Henry [0000-0002-8446-2485], Schoenherr, Christina [0000-0002-0983-6168], Arends, Mark J. [0000-0002-6826-8770], Frame, Margaret C. [0000-0001-5882-1942], Carragher, Neil O. [0000-0001-5541-9747], Unciti-Broceta, Asier [0000-0003-1029-2855], Temps, Caroline, Lietha, Daniel, Webb, Emily R., Li, Xue-Feng, Dawson, John C., Muir, Morwenna, Macleod, Kenneth G., Valero, Teresa, Munro, Alison F., Contreras-Montoya, Rafael, Luque-Ortega, Juan Román, Fraser, Craig, Beetham, Henry, Schoenherr, Christina, Lopalco, Maria, Arends, Mark J., Frame, Margaret C., Qian, Bin-Zhi, Brunton, Valerie G., Carragher, Neil O., Unciti-Broceta, Asier, University of Edinburgh, Ministerio de Ciencia, Innovación y Universidades (España), European Commission, CSIC - Centro de Investigaciones Biológicas Margarita Salas (CIB), Universidad de Granada, Wellcome Trust, Lietha, Daniel [0000-0002-6133-6486], Webb, Emily R. [0000-0001-9339-4544], Li, Xue-Feng [0000-0003-2612-0310], Muir, Morwenna [0000-0001-5835-3886], Luque-Ortega, Juan Román [0000-0003-3206-7480], Beetham, Henry [0000-0002-8446-2485], Schoenherr, Christina [0000-0002-0983-6168], Arends, Mark J. [0000-0002-6826-8770], Frame, Margaret C. [0000-0001-5882-1942], Carragher, Neil O. [0000-0001-5541-9747], Unciti-Broceta, Asier [0000-0003-1029-2855], Temps, Caroline, Lietha, Daniel, Webb, Emily R., Li, Xue-Feng, Dawson, John C., Muir, Morwenna, Macleod, Kenneth G., Valero, Teresa, Munro, Alison F., Contreras-Montoya, Rafael, Luque-Ortega, Juan Román, Fraser, Craig, Beetham, Henry, Schoenherr, Christina, Lopalco, Maria, Arends, Mark J., Frame, Margaret C., Qian, Bin-Zhi, Brunton, Valerie G., Carragher, Neil O., and Unciti-Broceta, Asier

Abstract

Despite the approval of several multikinase inhibitors that target SRC and the overwhelming evidence of the role of SRC in the progression and resistance mechanisms of many solid malignancies, inhibition of its kinase activity has thus far failed to improve patient outcomes. Here we report the small molecule eCF506 locks SRC in its native inactive conformation, thereby inhibiting both enzymatic and scaffolding functions that prevent phosphorylation and complex formation with its partner FAK. This unprecedented mechanism of action resulted in highly potent and selective pathway inhibition, in culture and in vivo. Treatment with eCF506 resulted in increased antitumor efficacy and tolerability in syngeneic murine cancer models, demonstrating significant therapeutic advantages over existing SRC/ABL inhibitors. Therefore, this novel mode of inhibiting SRC could lead to improved treatment of SRC-associated disorders.

Published

2021

2. A four gene signature predicts benefit from anthracyclines: evidence from the BR9601 and MA.5 clinical trials.

Author

Spears, Melanie, Spears, Melanie, Yousif, Fouad, Lyttle, Nicola, Boutros, Paul C, Munro, Alison F, Twelves, Chris, Pritchard, Kathleen I, Levine, Mark N, Shepherd, Lois, Bartlett, John MS, Spears, Melanie, Spears, Melanie, Yousif, Fouad, Lyttle, Nicola, Boutros, Paul C, Munro, Alison F, Twelves, Chris, Pritchard, Kathleen I, Levine, Mark N, Shepherd, Lois, and Bartlett, John MS

Abstract

Chromosome instability (CIN) in solid tumours results in multiple numerical and structural chromosomal aberrations and is associated with poor prognosis in multiple tumour types. Recent evidence demonstrated CEP17 duplication, a CIN marker, is a predictive marker of anthracycline benefit. An analysis of the BR9601 and MA.5 clinical trials was performed to test the role of existing CIN gene expression signatures as predictive markers of anthracycline sensitivity in breast cancer. Univariate analysis demonstrated, high CIN25 expression score was associated with improved distant relapse free survival (DRFS) (HR: 0.74, 95% CI 0.54-0.99, p = 0.046). High tumour CIN70 and CIN25 scores were associated with aggressive clinicopathological phenotype and increased sensitivity to anthracycline therapy compared to low CIN scores. However, in a prospectively planned multivariate analysis only pathological grade, nodal status and tumour size were significant predictors of outcome for CIN25/CIN70. A limited gene signature was generated, patients with low tumour CIN4 scores benefited from anthracycline treatment significantly more than those with high CIN4 scores (HR 0.37, 95% CI 0.20-0.56, p = 0.001). In multivariate analyses the treatment by marker interaction for CIN4/anthracyclines demonstrated hazard ratio of 0.35 (95% CI 0.15-0.80, p = 0.012) for DRFS. This data shows CIN4 is independent predictor of anthracycline benefit for DRFS in breast cancer.

Published

2015

3. A four gene signature predicts benefit from anthracyclines: evidence from the BR9601 and MA.5 clinical trials.

Author

Spears, Melanie, Spears, Melanie, Yousif, Fouad, Lyttle, Nicola, Boutros, Paul C, Munro, Alison F, Twelves, Chris, Pritchard, Kathleen I, Levine, Mark N, Shepherd, Lois, Bartlett, John MS, Spears, Melanie, Spears, Melanie, Yousif, Fouad, Lyttle, Nicola, Boutros, Paul C, Munro, Alison F, Twelves, Chris, Pritchard, Kathleen I, Levine, Mark N, Shepherd, Lois, and Bartlett, John MS

Abstract

Chromosome instability (CIN) in solid tumours results in multiple numerical and structural chromosomal aberrations and is associated with poor prognosis in multiple tumour types. Recent evidence demonstrated CEP17 duplication, a CIN marker, is a predictive marker of anthracycline benefit. An analysis of the BR9601 and MA.5 clinical trials was performed to test the role of existing CIN gene expression signatures as predictive markers of anthracycline sensitivity in breast cancer. Univariate analysis demonstrated, high CIN25 expression score was associated with improved distant relapse free survival (DRFS) (HR: 0.74, 95% CI 0.54-0.99, p = 0.046). High tumour CIN70 and CIN25 scores were associated with aggressive clinicopathological phenotype and increased sensitivity to anthracycline therapy compared to low CIN scores. However, in a prospectively planned multivariate analysis only pathological grade, nodal status and tumour size were significant predictors of outcome for CIN25/CIN70. A limited gene signature was generated, patients with low tumour CIN4 scores benefited from anthracycline treatment significantly more than those with high CIN4 scores (HR 0.37, 95% CI 0.20-0.56, p = 0.001). In multivariate analyses the treatment by marker interaction for CIN4/anthracyclines demonstrated hazard ratio of 0.35 (95% CI 0.15-0.80, p = 0.012) for DRFS. This data shows CIN4 is independent predictor of anthracycline benefit for DRFS in breast cancer.

Published

2015

4. Is TIMP-1 immunoreactivity alone or in combination with other markers a predictor of benefit from anthracyclines in the BR9601 adjuvant breast cancer chemotherapy trial?

Author

Munro, Alison F., Bartels, Annette, Balslev, Eva, Twelves, Christopher J., Cameron, David A, Brünner, Nils, Bartlett, John Ms, Munro, Alison F., Bartels, Annette, Balslev, Eva, Twelves, Christopher J., Cameron, David A, Brünner, Nils, and Bartlett, John Ms

Abstract

INTRODUCTION: Predictive cancer biomarkers to guide the right treatment to the right patient at the right time are strongly needed. The purpose of the present study was to validate prior results that tissue inhibitor of metalloproteinase 1 (TIMP-1) alone or in combination with either HER2 or TOP2A copy number can be used to predict benefit from epirubicin (E) containing chemotherapy compared with cyclophosphamide, methotrexate and fluorouracil (CMF) treatment. METHODS: For the purpose of this study, formalin fixed paraffin embedded tumor tissue from women recruited into the BR9601 clinical trial, which randomized patients to E-CMF versus CMF, were analyzed for TIMP-1 immunoreactivity. Using previously collected data for HER2 amplification and TOP2A gene aberrations, we defined patients as "anthracycline non-responsive", that is, 2T (TIMP-1 immunoreactive and TOP2A normal) and HT (TIMP-1 immunoreactive and HER2 negative) and anthracycline responsive (all other cases). RESULTS: In total, 288 tumors were available for TIMP-1 analysis with (183/274) 66.8%, and (181/274) 66.0% being classed as 2T and HT responsive, respectively. TIMP-1 was neither associated with patient prognosis (relapse free survival or overall survival) nor with a differential effect of E-CMF and CMF. Also, TIMP-1 did not add to the predictive value of HER2, TOP2A gene aberrations, or to Ki67 immunoreactivity. CONCLUSION: This study could not confirm the predictive value of TIMP-1 immunoreactivity in patients randomized to receive E-CMF versus CMF as adjuvant treatment for primary breast cancer.

Published

2013

5. Is TIMP-1 immunoreactivity alone or in combination with other markers a predictor of benefit from anthracyclines in the BR9601 adjuvant breast cancer chemotherapy trial?

Author

Munro, Alison F., Bartels, Annette, Balslev, Eva, Twelves, Christopher J., Cameron, David A, Brünner, Nils, Bartlett, John Ms, Munro, Alison F., Bartels, Annette, Balslev, Eva, Twelves, Christopher J., Cameron, David A, Brünner, Nils, and Bartlett, John Ms

Abstract

INTRODUCTION: Predictive cancer biomarkers to guide the right treatment to the right patient at the right time are strongly needed. The purpose of the present study was to validate prior results that tissue inhibitor of metalloproteinase 1 (TIMP-1) alone or in combination with either HER2 or TOP2A copy number can be used to predict benefit from epirubicin (E) containing chemotherapy compared with cyclophosphamide, methotrexate and fluorouracil (CMF) treatment. METHODS: For the purpose of this study, formalin fixed paraffin embedded tumor tissue from women recruited into the BR9601 clinical trial, which randomized patients to E-CMF versus CMF, were analyzed for TIMP-1 immunoreactivity. Using previously collected data for HER2 amplification and TOP2A gene aberrations, we defined patients as "anthracycline non-responsive", that is, 2T (TIMP-1 immunoreactive and TOP2A normal) and HT (TIMP-1 immunoreactive and HER2 negative) and anthracycline responsive (all other cases). RESULTS: In total, 288 tumors were available for TIMP-1 analysis with (183/274) 66.8%, and (181/274) 66.0% being classed as 2T and HT responsive, respectively. TIMP-1 was neither associated with patient prognosis (relapse free survival or overall survival) nor with a differential effect of E-CMF and CMF. Also, TIMP-1 did not add to the predictive value of HER2, TOP2A gene aberrations, or to Ki67 immunoreactivity. CONCLUSION: This study could not confirm the predictive value of TIMP-1 immunoreactivity in patients randomized to receive E-CMF versus CMF as adjuvant treatment for primary breast cancer.

Published

2013