Your search keyword '"Marta Guzman"' showing total 76 results

1. Interactions between BRD4S, LOXL2, and MED1 drive cell cycle transcription in triple‐negative breast cancer

Author

Laura Pascual‐Reguant, Queralt Serra‐Camprubí, Debayan Datta, Damiano Cianferoni, Savvas Kourtis, Antoni Gañez‐Zapater, Chiara Cannatá, Lorena Espinar, Jessica Querol, Laura García‐López, Sara Musa‐Afaneh, Maria Guirola, Anestis Gkanogiannis, Andrea Miró Canturri, Marta Guzman, Olga Rodríguez, Andrea Herencia‐Ropero, Joaquin Arribas, Violeta Serra, Luis Serrano, Tian V Tian, Sandra Peiró, and Sara Sdelci

Subjects

cell cycle, combinatorial therapy, gene expression, triple‐negative breast cancer, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Triple‐negative breast cancer (TNBC) often develops resistance to single‐agent treatment, which can be circumvented using targeted combinatorial approaches. Here, we demonstrate that the simultaneous inhibition of LOXL2 and BRD4 synergistically limits TNBC proliferation in vitro and in vivo. Mechanistically, LOXL2 interacts in the nucleus with the short isoform of BRD4 (BRD4S), MED1, and the cell cycle transcriptional regulator B‐MyB. These interactions sustain the formation of BRD4 and MED1 nuclear transcriptional foci and control cell cycle progression at the gene expression level. The pharmacological co‐inhibition of LOXL2 and BRD4 reduces BRD4 nuclear foci, BRD4‐MED1 colocalization, and the transcription of cell cycle genes, thus suppressing TNBC cell proliferation. Targeting the interaction between BRD4S and LOXL2 could be a starting point for the development of new anticancer strategies for the treatment of TNBC.

Published

2023

2. Data from MYC Inhibition Halts Metastatic Breast Cancer Progression by Blocking Growth, Invasion, and Seeding

Author

Laura Soucek, Jonathan R. Whitfield, Lars-Gunnar Larsson, Violeta Serra, Joaquín Arribas, Marta Guzman, Marta Escorihuela, Antonio Luque-García, Loay Mahmoud, Mohammad Alzrigat, Miguel Ángel Morcillo, Sergio López-Estévez, Jastrinjan Kaur, Virginia Castillo Cano, Sílvia Casacuberta-Serra, Génesis Martín-Fernández, Erika Serrano, Sandra Martínez-Martín, Laia Foradada, Mariano F. Zacarías-Fluck, Fabio Giuntini, Toni Jauset, Marie-Eve Beaulieu, and Daniel Massó-Vallés

Abstract

MYC's role in promoting tumorigenesis is beyond doubt, but its function in the metastatic process is still controversial. Omomyc is a MYC dominant negative that has shown potent antitumor activity in multiple cancer cell lines and mouse models, regardless of their tissue of origin or driver mutations, by impacting on several of the hallmarks of cancer. However, its therapeutic efficacy against metastasis has not been elucidated yet. Here we demonstrate for the first time that MYC inhibition by transgenic Omomyc is efficacious against all breast cancer molecular subtypes, including triple-negative breast cancer, where it displays potent antimetastatic properties both in vitro and in vivo. Importantly, pharmacologic treatment with the recombinantly produced Omomyc miniprotein, recently entering a clinical trial in solid tumors, recapitulates several key features of expression of the Omomyc transgene, confirming its clinical applicability to metastatic breast cancer, including advanced triple-negative breast cancer, a disease in urgent need of better therapeutic options.Significance:While MYC role in metastasis has been long controversial, this manuscript demonstrates that MYC inhibition by either transgenic expression or pharmacologic use of the recombinantly produced Omomyc miniprotein exerts antitumor and antimetastatic activity in breast cancer models in vitro and in vivo, suggesting its clinical applicability.

Published

2023

3. Supplementary Figure 3 from Antitumor Activity of the Hsp90 Inhibitor IPI-504 in HER2-Positive Trastuzumab-Resistant Breast Cancer

Author

José Baselga, Claudia Aura, José Jimenez, Ludmila Prudkin, Varenka Rodriguez, Kip A. West, Kelly L. Slocum, Alice R. Lim, Olga Rodriguez, Marta Guzman, Emmanuel Normant, Violeta Serra, and Maurizio Scaltriti

Abstract

Supplementary Figure 3 from Antitumor Activity of the Hsp90 Inhibitor IPI-504 in HER2-Positive Trastuzumab-Resistant Breast Cancer

Published

2023

4. Supplementary Figure 1 from Antitumor Activity of the Hsp90 Inhibitor IPI-504 in HER2-Positive Trastuzumab-Resistant Breast Cancer

Author

José Baselga, Claudia Aura, José Jimenez, Ludmila Prudkin, Varenka Rodriguez, Kip A. West, Kelly L. Slocum, Alice R. Lim, Olga Rodriguez, Marta Guzman, Emmanuel Normant, Violeta Serra, and Maurizio Scaltriti

Abstract

Supplementary Figure 1 from Antitumor Activity of the Hsp90 Inhibitor IPI-504 in HER2-Positive Trastuzumab-Resistant Breast Cancer

Published

2023

5. Supplementary Figure 2 from Antitumor Activity of the Hsp90 Inhibitor IPI-504 in HER2-Positive Trastuzumab-Resistant Breast Cancer

Author

José Baselga, Claudia Aura, José Jimenez, Ludmila Prudkin, Varenka Rodriguez, Kip A. West, Kelly L. Slocum, Alice R. Lim, Olga Rodriguez, Marta Guzman, Emmanuel Normant, Violeta Serra, and Maurizio Scaltriti

Abstract

Supplementary Figure 2 from Antitumor Activity of the Hsp90 Inhibitor IPI-504 in HER2-Positive Trastuzumab-Resistant Breast Cancer

Published

2023

6. Supplementary Figure Legends 1-3 from Antitumor Activity of the Hsp90 Inhibitor IPI-504 in HER2-Positive Trastuzumab-Resistant Breast Cancer

Author

José Baselga, Claudia Aura, José Jimenez, Ludmila Prudkin, Varenka Rodriguez, Kip A. West, Kelly L. Slocum, Alice R. Lim, Olga Rodriguez, Marta Guzman, Emmanuel Normant, Violeta Serra, and Maurizio Scaltriti

Abstract

Supplementary Figure Legends 1-3 from Antitumor Activity of the Hsp90 Inhibitor IPI-504 in HER2-Positive Trastuzumab-Resistant Breast Cancer

Published

2023

7. Supplementary Figure from Identification of a Molecularly-Defined Subset of Breast and Ovarian Cancer Models that Respond to WEE1 or ATR Inhibition, Overcoming PARP Inhibitor Resistance

Author

Mark J. O'Connor, Judith Balmaña, Cristina Cruz, Christopher J. Lord, Elaine Cadogan, Josep V. Forment, J. Carl Barrett, Gordon B. Mills, Carlos Caldas, Brian Dougherty, Susan Critchlow, Alan Lau, Cristina Saura, Javier Cortés, Joaquin Arribas, Judit Grueso, Olga Rodríguez, Marta Guzman, Albert Gris-Oliver, Alejandra Bruna, Ambar Ahmed, Paul W.G. Wijnhoven, Adina Hughes, Zena Wilson, Jenni Nikkilä, Krishna C. Bulusu, Stephen J. Pettitt, Aditi Gulati, Rachel Brough, Alba Llop-Guevara, Filippos Michopoulos, Joshua Armenia, Zhongwu Lai, Gemma N. Jones, Andrea Herencia-Ropero, Marta Palafox, Urszula M. Polanska, Marta Castroviejo-Bermejo, Anderson T. Wang, and Violeta Serra

Abstract

Supplementary Figure from Identification of a Molecularly-Defined Subset of Breast and Ovarian Cancer Models that Respond to WEE1 or ATR Inhibition, Overcoming PARP Inhibitor Resistance

Published

2023

8. Supplementary Data from Identification of a Molecularly-Defined Subset of Breast and Ovarian Cancer Models that Respond to WEE1 or ATR Inhibition, Overcoming PARP Inhibitor Resistance

Author

Mark J. O'Connor, Judith Balmaña, Cristina Cruz, Christopher J. Lord, Elaine Cadogan, Josep V. Forment, J. Carl Barrett, Gordon B. Mills, Carlos Caldas, Brian Dougherty, Susan Critchlow, Alan Lau, Cristina Saura, Javier Cortés, Joaquin Arribas, Judit Grueso, Olga Rodríguez, Marta Guzman, Albert Gris-Oliver, Alejandra Bruna, Ambar Ahmed, Paul W.G. Wijnhoven, Adina Hughes, Zena Wilson, Jenni Nikkilä, Krishna C. Bulusu, Stephen J. Pettitt, Aditi Gulati, Rachel Brough, Alba Llop-Guevara, Filippos Michopoulos, Joshua Armenia, Zhongwu Lai, Gemma N. Jones, Andrea Herencia-Ropero, Marta Palafox, Urszula M. Polanska, Marta Castroviejo-Bermejo, Anderson T. Wang, and Violeta Serra

Abstract

Supplementary Data from Identification of a Molecularly-Defined Subset of Breast and Ovarian Cancer Models that Respond to WEE1 or ATR Inhibition, Overcoming PARP Inhibitor Resistance

Published

2023

9. Data from Identification of a Molecularly-Defined Subset of Breast and Ovarian Cancer Models that Respond to WEE1 or ATR Inhibition, Overcoming PARP Inhibitor Resistance

Author

Mark J. O'Connor, Judith Balmaña, Cristina Cruz, Christopher J. Lord, Elaine Cadogan, Josep V. Forment, J. Carl Barrett, Gordon B. Mills, Carlos Caldas, Brian Dougherty, Susan Critchlow, Alan Lau, Cristina Saura, Javier Cortés, Joaquin Arribas, Judit Grueso, Olga Rodríguez, Marta Guzman, Albert Gris-Oliver, Alejandra Bruna, Ambar Ahmed, Paul W.G. Wijnhoven, Adina Hughes, Zena Wilson, Jenni Nikkilä, Krishna C. Bulusu, Stephen J. Pettitt, Aditi Gulati, Rachel Brough, Alba Llop-Guevara, Filippos Michopoulos, Joshua Armenia, Zhongwu Lai, Gemma N. Jones, Andrea Herencia-Ropero, Marta Palafox, Urszula M. Polanska, Marta Castroviejo-Bermejo, Anderson T. Wang, and Violeta Serra

Abstract

Purpose:PARP inhibitors (PARPi) induce synthetic lethality in homologous recombination repair (HRR)-deficient tumors and are used to treat breast, ovarian, pancreatic, and prostate cancers. Multiple PARPi resistance mechanisms exist, most resulting in restoration of HRR and protection of stalled replication forks. ATR inhibition was highlighted as a unique approach to reverse both aspects of resistance. Recently, however, a PARPi/WEE1 inhibitor (WEE1i) combination demonstrated enhanced antitumor activity associated with the induction of replication stress, suggesting another approach to tackling PARPi resistance.Experimental Design:We analyzed breast and ovarian patient-derived xenoimplant models resistant to PARPi to quantify WEE1i and ATR inhibitor (ATRi) responses as single agents and in combination with PARPi. Biomarker analysis was conducted at the genetic and protein level. Metabolite analysis by mass spectrometry and nucleoside rescue experiments ex vivo were also conducted in patient-derived models.Results:Although WEE1i response was linked to markers of replication stress, including STK11/RB1 and phospho-RPA, ATRi response associated with ATM mutation. When combined with olaparib, WEE1i could be differentiated from the ATRi/olaparib combination, providing distinct therapeutic strategies to overcome PARPi resistance by targeting the replication stress response. Mechanistically, WEE1i sensitivity was associated with shortage of the dNTP pool and a concomitant increase in replication stress.Conclusions:Targeting the replication stress response is a valid therapeutic option to overcome PARPi resistance including tumors without an underlying HRR deficiency. These preclinical insights are now being tested in several clinical trials where the PARPi is administered with either the WEE1i or the ATRi.

Published

2023

10. HighFGFR1–4mRNA Expression Levels Correlate with Response to Selective FGFR Inhibitors in Breast Cancer

Author

Fara Brasó-Maristany, Marta Guzman, Josep Tabernero, Mafalda Oliveira, Zighereda Ogbah, Judit Grueso, Maurizio Scaltriti, Mireia Parés, Aleix Prat, Oriol Casanovas, Elena Garralda, Jordi Rodon, Olga Rodriguez, Mònica Sánchez-Guixé, Cinta Hierro, Analia Azaro, Violeta Serra, Rodrigo Dienstmann, Paolo Nuciforo, Ana Vivancos, Cristina Saura, Erika Monelli, Mariona Graupera, Guillermo Villacampa, José Antonio Jiménez, and Cristina Viaplana

Subjects

CD31, Cancer Research, medicine.diagnostic_test, business.industry, Angiogenesis, Kinase, Fibroblast growth factor receptor 1, medicine.disease, Immunofluorescence, Metastatic breast cancer, Breast cancer, Oncology, Cancer research, Medicine, Immunohistochemistry, business

Abstract

Purpose:FGFR1 amplification (FGFR1amp) is recurrent in metastatic breast cancer (MBC) and is associated with resistance to endocrine therapy and CDK4/6 inhibitors (CDK4/6is). Multi-tyrosine kinase inhibitors (MTKIs) and selective pan-FGFR inhibitors (FGFRis) are being developed for FGFR1amp breast cancer. High-level FGFR amplification and protein expression by IHC have identified breast cancer responders to FGFRis or MTKIs, respectively.Experimental Design:Here, we used preclinical models and patient samples to identify predictive biomarkers to these drugs. We evaluated the antitumor activity of an FGFRi and an MTKI in a collection of 17 breast cancer patient–derived xenografts (PDXs) harboring amplification in FGFR1/2/3/4 and in 10 patients receiving either an FGFRi/MTKI. mRNA levels were measured on FFPE tumor samples using two commercial strategies. Proliferation and angiogenesis were evaluated by detecting Ki-67 and CD31 in viable areas by immunofluorescence.Results:High FGFR1–4 mRNA levels but not copy-number alteration (CNA) is associated with FGFRi response. Treatment with MTKIs showed higher response rates than with FGFRis (86% vs. 53%), regardless of the FGFR1–4 mRNA levels. FGFR-addicted PDXs exhibited an antiproliferative response to either FGFRis or MTKIs, and PDXs exclusively sensitive to MTKI exhibited an additional antiangiogenic response. Consistently, the clinical benefit of MTKIs was not associated with high FGFR1–4 mRNA levels and was observed in patients previously treated with antiangiogenic drugs.Conclusions:Tailored therapy with FGFRis in molecularly selected MBC based on high FGFR1–4 mRNA levels warrants prospective validation in patients with CDK4/6i-resistant luminal breast cancer and in patients with TNBC without targeted therapeutic options.

Published

2022

11. Supplementary Table 6 from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

XLS file 38K, Single-biomarker tumor growth inhibition projection

Published

2023

12. Supplementary Figure 2 from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

PDF file 155K, Principal component analysis (PCA) of the ten biomarkers provides a biomarker profile for each cell line

Published

2023

13. Supplementary Data from Clinical Benefit of Lapatinib-Based Therapy in Patients with Human Epidermal Growth Factor Receptor 2–Positive Breast Tumors Coexpressing the Truncated p95HER2 Receptor

Author

José Baselga, Neal Rosen, Joaquin Arribas, David Cameron, Charles Geyer, Henry Gomez, Maria Koehler, Robert Gagnon, Catherine Ellis, Josep Lluis Parra, Marta Guzman, Gertrudis Sánchez, Pier Davide Angelini, José Jimenez, Claudia Aura, Ludmila Prudkin, Sarat Chandarlapaty, and Maurizio Scaltriti

Abstract

Supplementary Data from Clinical Benefit of Lapatinib-Based Therapy in Patients with Human Epidermal Growth Factor Receptor 2–Positive Breast Tumors Coexpressing the Truncated p95HER2 Receptor

Published

2023

14. Supplementary Figure 1 from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

PDF file 285K, Biomarker validation by Western blot

Published

2023

15. Supplementary Figure 3 from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

PDF file 252K, In vivo pharmacodynamic IHC-based biomarker dose-response quantifications

Published

2023

16. Data from Clinical Benefit of Lapatinib-Based Therapy in Patients with Human Epidermal Growth Factor Receptor 2–Positive Breast Tumors Coexpressing the Truncated p95HER2 Receptor

Author

José Baselga, Neal Rosen, Joaquin Arribas, David Cameron, Charles Geyer, Henry Gomez, Maria Koehler, Robert Gagnon, Catherine Ellis, Josep Lluis Parra, Marta Guzman, Gertrudis Sánchez, Pier Davide Angelini, José Jimenez, Claudia Aura, Ludmila Prudkin, Sarat Chandarlapaty, and Maurizio Scaltriti

Abstract

Purpose: A subgroup of human epidermal growth factor receptor 2 (HER2)–overexpressing breast tumors coexpresses p95HER2, a truncated HER2 receptor that retains a highly functional HER2 kinase domain but lacks the extracellular domain and results in intrinsic trastuzumab resistance. We hypothesized that lapatinib, a HER2 tyrosine kinase inhibitor, would be active in these tumors. We have studied the correlation between p95HER2 expression and response to lapatinib, both in preclinical models and in the clinical setting.Experimental Design: Two different p95HER2 animal models were used for preclinical studies. Expression of p95HER2 was analyzed in HER2-overexpressing breast primary tumors from a first-line lapatinib monotherapy study (EGF20009) and a second-line lapatinib in combination with capecitabine study (EGF100151). p95HER2 expression was correlated with overall response rate (complete + partial response), clinical benefit rate (complete response + partial response + stable disease ≥24 wk), and progression-free survival using logistic regression and Cox proportional hazard models.Results: Lapatinib inhibited tumor growth and the HER2 downstream signaling of p95HER2-expressing tumors. A total of 68 and 156 tumors from studies EGF20009 and EGF100151 were evaluable, respectively, for p95HER2 detection. The percentage of p95HER2-positive patients was 20.5% in the EGF20009 study and 28.5% in the EGF100151 study. In both studies, there was no statistically significant difference in progression-free survival, clinical benefit rate, and overall response rate between p95HER2-positive and p95HER2-negative tumors.Conclusions: Lapatinib as a monotherapy or in combination with capecitabine seems to be equally effective in patients with p95HER2-positive and p95HER2-negative HER2-positive breast tumors. Clin Cancer Res; 16(9); 2688–95. ©2010 AACR.

Published

2023

17. Supplementary Figure 4 from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

PDF file 64K, Unsupervised clustering of the core biomarker modulation in cell lines, xenograft tumors, and in tumors from three patients in the 100mg cohort

Published

2023

18. Data from Early Adaptation and Acquired Resistance to CDK4/6 Inhibition in Estrogen Receptor–Positive Breast Cancer

Author

Violeta Serra, Nicholas C. Turner, Lesley-Ann Martin, Mitch Dowsett, José Baselga, Christopher J. Lord, Sunil Pancholi, Richard Elliott, Javier Cortés, Meritxell Bellet, Judit Grueso, Olga Rodriguez, Marta Guzman, Alex Pearson, Isaac Garcia-Murillas, Rosalind J. Cutts, Martín A. Rivas, Uzma Asghar, Marta Palafox, and Maria Teresa Herrera-Abreu

Abstract

Small-molecule inhibitors of the CDK4/6 cell-cycle kinases have shown clinical efficacy in estrogen receptor (ER)-positive metastatic breast cancer, although their cytostatic effects are limited by primary and acquired resistance. Here we report that ER-positive breast cancer cells can adapt quickly to CDK4/6 inhibition and evade cytostasis, in part, via noncanonical cyclin D1-CDK2–mediated S-phase entry. This adaptation was prevented by cotreatment with hormone therapies or PI3K inhibitors, which reduced the levels of cyclin D1 (CCND1) and other G1–S cyclins, abolished pRb phosphorylation, and inhibited activation of S-phase transcriptional programs. Combined targeting of both CDK4/6 and PI3K triggered cancer cell apoptosis in vitro and in patient-derived tumor xenograft (PDX) models, resulting in tumor regression and improved disease control. Furthermore, a triple combination of endocrine therapy, CDK4/6, and PI3K inhibition was more effective than paired combinations, provoking rapid tumor regressions in a PDX model. Mechanistic investigations showed that acquired resistance to CDK4/6 inhibition resulted from bypass of cyclin D1–CDK4/6 dependency through selection of CCNE1 amplification or RB1 loss. Notably, although PI3K inhibitors could prevent resistance to CDK4/6 inhibitors, they failed to resensitize cells once resistance had been acquired. However, we found that cells acquiring resistance to CDK4/6 inhibitors due to CCNE1 amplification could be resensitized by targeting CDK2. Overall, our results illustrate convergent mechanisms of early adaptation and acquired resistance to CDK4/6 inhibitors that enable alternate means of S-phase entry, highlighting strategies to prevent the acquisition of therapeutic resistance to these agents. Cancer Res; 76(8); 2301–13. ©2016 AACR.

Published

2023

19. Supplementary Table 3 from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

PDF file 168K, Pearson and Spearman correlation with survival fraction for all cell lines together or individual cell lines

Published

2023

20. Supplementary Table 5 from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

XLS file 37K, RPPA quantification of laser captured microscopy needle biopsies in patients from the 100mg cohort

Published

2023

21. Data from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

Purpose: The oncogenic PI3K/Akt/mTOR pathway is an attractive therapeutic target in cancer. However, it is unknown whether the pathway blockade required for tumor growth inhibition is clinically achievable. Therefore, we conducted pharmacodynamic studies with GDC-0068, an ATP competitive, selective Akt1/2/3 inhibitor, in preclinical models and in patients treated with this compound.Experimental Design: We used a reverse phase protein array (RPPA) platform to identify a biomarker set indicative of Akt inhibition in cell lines and human-tumor xenografts, and correlated the degree of pathway inhibition with antitumor activity. Akt pathway activity was measured using this biomarker set in pre- and post-dose tumor biopsies from patients treated with GDC-0068 in the dose escalation clinical trial.Results: The set of biomarkers of Akt inhibition is composed of 10 phosphoproteins, including Akt and PRAS40, and is modulated in a dose-dependent fashion, both in vitro and in vivo. In human-tumor xenografts, this dose dependency significantly correlated with tumor growth inhibition. Tumor biopsies from patients treated with GDC-0068 at clinically achievable doses attained a degree of biomarker inhibition that correlated with tumor growth inhibition in preclinical models. In these clinical samples, compensatory feedback activation of ERK and HER3 was observed, consistent with preclinical observations.Conclusion: This study identified a set of biomarkers of Akt inhibition that can be used in the clinical setting to assess target engagement. Here, it was used to show that robust Akt inhibition in tumors from patients treated with GDC-0068 is achievable, supporting the clinical development of this compound in defined patient populations. Clin Cancer Res; 19(24); 6976–86. ©2013 AACR.

Published

2023

22. Supplementary Table 4 from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

PDF file 161K, Tumor PIK3CA and PTEN status

Published

2023

23. Supplementary Materials and Methods from Early Adaptation and Acquired Resistance to CDK4/6 Inhibition in Estrogen Receptor–Positive Breast Cancer

Author

Violeta Serra, Nicholas C. Turner, Lesley-Ann Martin, Mitch Dowsett, José Baselga, Christopher J. Lord, Sunil Pancholi, Richard Elliott, Javier Cortés, Meritxell Bellet, Judit Grueso, Olga Rodriguez, Marta Guzman, Alex Pearson, Isaac Garcia-Murillas, Rosalind J. Cutts, Martín A. Rivas, Uzma Asghar, Marta Palafox, and Maria Teresa Herrera-Abreu

Abstract

Supplementary Materials and Methods

Published

2023

24. Supplementary Table 1 from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

XLS file 41K, RPPA biomarkers

Published

2023

25. Supplementary Figure Legends from Early Adaptation and Acquired Resistance to CDK4/6 Inhibition in Estrogen Receptor–Positive Breast Cancer

Author

Violeta Serra, Nicholas C. Turner, Lesley-Ann Martin, Mitch Dowsett, José Baselga, Christopher J. Lord, Sunil Pancholi, Richard Elliott, Javier Cortés, Meritxell Bellet, Judit Grueso, Olga Rodriguez, Marta Guzman, Alex Pearson, Isaac Garcia-Murillas, Rosalind J. Cutts, Martín A. Rivas, Uzma Asghar, Marta Palafox, and Maria Teresa Herrera-Abreu

Abstract

Supplementary Figure Legends

Published

2023

26. Supplementary Figures 1 through 7 from Early Adaptation and Acquired Resistance to CDK4/6 Inhibition in Estrogen Receptor–Positive Breast Cancer

Author

Violeta Serra, Nicholas C. Turner, Lesley-Ann Martin, Mitch Dowsett, José Baselga, Christopher J. Lord, Sunil Pancholi, Richard Elliott, Javier Cortés, Meritxell Bellet, Judit Grueso, Olga Rodriguez, Marta Guzman, Alex Pearson, Isaac Garcia-Murillas, Rosalind J. Cutts, Martín A. Rivas, Uzma Asghar, Marta Palafox, and Maria Teresa Herrera-Abreu

Abstract

Supplementary Figure 1: Early adaptive resistance limits the efficacy of CDK4/6 inhibition. High-throughput drug screen identified PI3K-mTOR inhibitors as sensitizers to CDK4/6 inhibitors. Supplementary Figure 2: Determinants of sensitivity to the combination CDK4/6 and PI3K inhibition. Supplementary Figure 3: Early adaptation to CDK4/6 inhibition is mediated by non-canonical cyclin D1-CDK2 interaction. IGF1R inhibition increases sensitivity to CDK4/6 inhibition in MCF-7 cells. Supplementary Figure 4: Palbociclib induced senescence like morphology is reversible. Supplementary Figure 5: Acquired palbociclib resistance through RB1 loss or CCNE1 amplification/expression. Supplementary Figure 6: Body weight of mice during vehicle, BYL719, LEE011 or combination treatment. Supplementary Figure 7: The combination LEE011 and BYL719 is more effective in ER positive PDX than single agent treatments.

Published

2023

27. Supplementary Data from Evaluation and Clinical Analyses of Downstream Targets of the Akt Inhibitor GDC-0068

Author

José Baselga, Premal Patel, Josep Tabernero, Andrés Cervantes, Desamparados Roda, Cristina Saura, Mark R. Lackner, Vanitha Ramakrishnan, Garret Hampton, Matthew Wongchenko, Jenny Q. Wu, Marie-Claire Wagle, Yuanyuan Xiao, Michelle Nannini, Deepak Sampath, Marta Guzman, Olga Rodríguez, Sumati Murli, Maurizio Scaltriti, Ludmila Prudkin, Violeta Serra, and Yibing Yan

Abstract

PDF file 117K, Supplementary Materials and Methods -Supplementary Figure Legends -Supplementary Table Legends

Published

2023

28. Supplementary Figure 2 from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Author

José Baselga, Joaquin Arribas, Josep Lluis Parra, Carlos Garcia-Echeverria, Michel Maira, Serena Di Cosimo, Francesco Atzori, Elisabeth Llonch, Maria Luisa Botero, Marta Guzman, Vanesa Valero, Pieter J.A. Eichhorn, Maurizio Scaltriti, Ben Markman, and Violeta Serra

Abstract

Supplementary Figure 2 from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Published

2023

29. Data from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Author

José Baselga, Joaquin Arribas, Josep Lluis Parra, Carlos Garcia-Echeverria, Michel Maira, Serena Di Cosimo, Francesco Atzori, Elisabeth Llonch, Maria Luisa Botero, Marta Guzman, Vanesa Valero, Pieter J.A. Eichhorn, Maurizio Scaltriti, Ben Markman, and Violeta Serra

Abstract

Phosphatidylinositol-3-kinase (PI3K) pathway deregulation is a common event in human cancer, either through inactivation of the tumor suppressor phosphatase and tensin homologue deleted from chromosome 10 or activating mutations of p110-α. These hotspot mutations result in oncogenic activity of the enzyme and contribute to therapeutic resistance to the anti-HER2 antibody trastuzumab. The PI3K pathway is, therefore, an attractive target for cancer therapy. We have studied NVP-BEZ235, a dual inhibitor of the PI3K and the downstream mammalian target of rapamycin (mTOR). NVP-BEZ235 inhibited the activation of the downstream effectors Akt, S6 ribosomal protein, and 4EBP1 in breast cancer cells. The antiproliferative activity of NVP-BEZ235 was superior to the allosteric selective mTOR complex inhibitor everolimus in a panel of 21 cancer cell lines of different origin and mutation status. The described Akt activation due to mTOR inhibition was prevented by higher doses of NVP-BEZ235. NVP-BEZ235 reversed the hyperactivation of the PI3K/mTOR pathway caused by the oncogenic mutations of p110-α, E545K, and H1047R, and inhibited the proliferation of HER2-amplified BT474 cells exogenously expressing these mutations that render them resistant to trastuzumab. In trastuzumab-resistant BT474 H1047R breast cancer xenografts, NVP-BEZ235 inhibited PI3K signaling and had potent antitumor activity. In treated animals, there was complete inhibition of PI3K signaling in the skin at pharmacologically active doses, suggesting that skin may serve as surrogate tissue for pharmacodynamic studies. In summary, NVP-BEZ235 inhibits the PI3K/mTOR axis and results in antiproliferative and antitumoral activity in cancer cells with both wild-type and mutated p110-α. [Cancer Res 2008;68(19):8022–30]

Published

2023

30. Supplementary Table 1 from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Author

José Baselga, René Bernards, Joan Seoane, Vanesa Valero, Roderick L. Beijersbergen, Wouter Nijkamp, Marta Guzman, Violeta Serra, Maurizio Scaltriti, Magüi Gili, and Pieter J.A. Eichhorn

Abstract

Supplementary Table 1 from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Published

2023

31. Supplementary Figure 3 from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Author

José Baselga, Joaquin Arribas, Josep Lluis Parra, Carlos Garcia-Echeverria, Michel Maira, Serena Di Cosimo, Francesco Atzori, Elisabeth Llonch, Maria Luisa Botero, Marta Guzman, Vanesa Valero, Pieter J.A. Eichhorn, Maurizio Scaltriti, Ben Markman, and Violeta Serra

Abstract

Supplementary Figure 3 from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Published

2023

32. Supplementary Figure 2 from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Author

José Baselga, René Bernards, Joan Seoane, Vanesa Valero, Roderick L. Beijersbergen, Wouter Nijkamp, Marta Guzman, Violeta Serra, Maurizio Scaltriti, Magüi Gili, and Pieter J.A. Eichhorn

Abstract

Supplementary Figure 2 from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Published

2023

33. Supplementary Figure 1 from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Author

José Baselga, Joaquin Arribas, Josep Lluis Parra, Carlos Garcia-Echeverria, Michel Maira, Serena Di Cosimo, Francesco Atzori, Elisabeth Llonch, Maria Luisa Botero, Marta Guzman, Vanesa Valero, Pieter J.A. Eichhorn, Maurizio Scaltriti, Ben Markman, and Violeta Serra

Abstract

Supplementary Figure 1 from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Published

2023

34. Supplementary Legends 1-4 from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Author

José Baselga, Joaquin Arribas, Josep Lluis Parra, Carlos Garcia-Echeverria, Michel Maira, Serena Di Cosimo, Francesco Atzori, Elisabeth Llonch, Maria Luisa Botero, Marta Guzman, Vanesa Valero, Pieter J.A. Eichhorn, Maurizio Scaltriti, Ben Markman, and Violeta Serra

Abstract

Supplementary Legends 1-4 from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Published

2023

35. Supplementary Figure 3 from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Author

José Baselga, René Bernards, Joan Seoane, Vanesa Valero, Roderick L. Beijersbergen, Wouter Nijkamp, Marta Guzman, Violeta Serra, Maurizio Scaltriti, Magüi Gili, and Pieter J.A. Eichhorn

Abstract

Supplementary Figure 3 from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Published

2023

36. Data from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Author

José Baselga, René Bernards, Joan Seoane, Vanesa Valero, Roderick L. Beijersbergen, Wouter Nijkamp, Marta Guzman, Violeta Serra, Maurizio Scaltriti, Magüi Gili, and Pieter J.A. Eichhorn

Abstract

Small molecule inhibitors of HER2 are clinically active in women with advanced HER2-positive breast cancer who have progressed on trastuzumab treatment. However, the effectiveness of this class of agents is limited by either primary resistance or acquired resistance. Using an unbiased genetic approach, we performed a genome wide loss-of-function short hairpin RNA screen to identify novel modulators of resistance to lapatinib, a recently approved anti-HER2 tyrosine kinase inhibitor. Here, we have identified the tumor suppressor PTEN as a modulator of lapatinib sensitivity in vitro and in vivo. In addition, we show that two dominant activating mutations in PIK3CA (E545K and H1047R), which are prevalent in breast cancer, also confer resistance to lapatinib. Furthermore, we show that phosphatidylinositol 3-kinase (PI3K)–induced lapatinib resistance can be abrogated through the use of NVP-BEZ235, a dual inhibitor of PI3K/mTOR. Our data show that deregulation of the PI3K pathway, either through loss-of-function mutations in PTEN or dominant activating mutations in PIK3CA, leads to lapatinib resistance, which can be effectively reversed by NVP-BEZ235. [Cancer Res 2008;68(22):9221–30]

Published

2023

37. Supplementary Figure 4 from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Author

José Baselga, Joaquin Arribas, Josep Lluis Parra, Carlos Garcia-Echeverria, Michel Maira, Serena Di Cosimo, Francesco Atzori, Elisabeth Llonch, Maria Luisa Botero, Marta Guzman, Vanesa Valero, Pieter J.A. Eichhorn, Maurizio Scaltriti, Ben Markman, and Violeta Serra

Abstract

Supplementary Figure 4 from NVP-BEZ235, a Dual PI3K/mTOR Inhibitor, Prevents PI3K Signaling and Inhibits the Growth of Cancer Cells with Activating PI3K Mutations

Published

2023

38. Supplementary Figure 1 from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Author

José Baselga, René Bernards, Joan Seoane, Vanesa Valero, Roderick L. Beijersbergen, Wouter Nijkamp, Marta Guzman, Violeta Serra, Maurizio Scaltriti, Magüi Gili, and Pieter J.A. Eichhorn

Abstract

Supplementary Figure 1 from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Published

2023

39. Supplementary Table 2 from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Author

José Baselga, René Bernards, Joan Seoane, Vanesa Valero, Roderick L. Beijersbergen, Wouter Nijkamp, Marta Guzman, Violeta Serra, Maurizio Scaltriti, Magüi Gili, and Pieter J.A. Eichhorn

Abstract

Supplementary Table 2 from Phosphatidylinositol 3-Kinase Hyperactivation Results in Lapatinib Resistance that Is Reversed by the mTOR/Phosphatidylinositol 3-Kinase Inhibitor NVP-BEZ235

Published

2023

40. High p16 expression and heterozygous RB1 loss are biomarkers for CDK4/6 inhibitor resistance in ER+ breast cancer

Author

Stefan Michiels, Cristina Saura, Cristina Viaplana, Marta Palafox, Abel Gonzalez-Perez, Alejandra Bruna, Paolo Nuciforo, Marta Guzman, Arribas Joaquín, Meritxell Bellet, Alicia García-Sanz, Violeta Serra, Faye Su, Olga Rodriguez, Nuria Lopez-Bigas, Analia Azaro, Monica Arnedos, Javier Hernández-Losa, Maurizio Scaltriti, Mafalda Oliveira, Laia Monserrat, Marta Capelán, Maria Teresa Herrera-Abreu, Carlos Caldas, Guillermo Villacampa, Leonardo Mina, Judit Grueso, Chandra S. Verma, Srinivasaraghavan Kannan, Robert Clarke, Nusaibah Ibrahimi, R. Dienstmann, Andreu Ódena, Nicholas C. Turner, Fara Brasó-Maristany, Aleix Prat, Mònica Sánchez-Guixé, Kui Lin, Gonzalez-Perez, Abel [0000-0002-8582-4660], Oliveira, Mafalda [0000-0001-9152-8799], Ibrahimi, Nusaibah [0000-0003-4537-0323], Kannan, Srinivasaraghavan [0000-0002-9539-5249], Sánchez-Guixé, Mònica [0000-0002-9430-4413], Hernández, Javier [0000-0003-1526-3201], Clarke, Robert B [0000-0001-5407-3123], Caldas, Carlos [0000-0003-3547-1489], Arribas, Joaquín [0000-0002-0504-0664], Michiels, Stefan [0000-0002-6963-2968], Turner, Nicholas C [0000-0001-8937-0873], Prat, Aleix [0000-0003-2377-540X], Nuciforo, Paolo [0000-0003-1380-0990], Lopez-Bigas, Nuria [0000-0003-4925-8988], Scaltriti, Maurizio [0000-0002-5522-1447], Saura, Cristina [0000-0001-8296-5065], Serra, Violeta [0000-0001-6620-1065], Apollo - University of Cambridge Repository, Institut Català de la Salut, [Palafox M, Monserrat L, Òdena A, Sánchez-Guixé M, Rodríguez O, Guzmán M, Grueso J] Experimental Therapeutics Group, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. [Bellet M, Bellet M, Capelán M, Azaro A, Saura C] Breast Cancer and Melanoma Group, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. Servei d’Oncologia Mèdica, Vall d’Hebron Hospital Universitari, Barcelona, Spain. [Villacampa G, Viaplana C, Dienstmann R] Oncology Data Science Group, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. [Gonzalez-Perez A] Institute for Research in Biomedicine (IRB Barcelona), Barcelona, Spain. Research Program on Biomedical Informatics, Universitat Pompeu Fabra, Barcelona, Spain. [Hernández J] Grup de Recerca de Patologia Molecular Translacional, Vall d’Hebron Institut de Recerca (VHIR), Barcelona, Spain. [Arribas J] CIBERONC, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. Growth Factors Laboratory, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. Departament de Bioquímica i Biologia Molecular, Universitat Autònoma de Barcelona, Bellaterra, Spain. IMIM (Hospital del Mar Medical Research Institute), Barcelona, Spain. Institució Catalana de Recerca i Estudis Avançats (ICREA), Barcelona, Spain. [Nuciforo P] Molecular Oncology Group, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. [Serra V] Experimental Therapeutics Group, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. CIBERONC, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects

endocrine system, Physiological Phenomena::Pharmacological and Toxicological Phenomena::Pharmacological Phenomena::Drug Resistance::Drug Resistance, Neoplasm [PHENOMENA AND PROCESSES], endocrine system diseases, Neoplasms::Neoplasms by Site::Breast Neoplasms [DISEASES], Ubiquitin-Protein Ligases, Otros calificadores::Otros calificadores::/farmacoterapia [Otros calificadores], General Physics and Astronomy, Antineoplastic Agents, Breast Neoplasms, Other subheadings::Other subheadings::/drug therapy [Other subheadings], Predictive markers, Chemical Actions and Uses::Pharmacologic Actions::Molecular Mechanisms of Pharmacological Action::Enzyme Inhibitors::Protein Kinase Inhibitors [CHEMICALS AND DRUGS], General Biochemistry, Genetics and Molecular Biology, Càncer de mama, Phosphatidylinositol 3-Kinases, Text mining, Breast cancer, Er breast cancer, Medicine, Humans, Cancer models, neoplasms, Protein Kinase Inhibitors, Resistència als medicaments, fenómenos fisiológicos::fenómenos farmacológicos y toxicológicos::fenómenos farmacológicos::resistencia a medicamentos::resistencia a los antineoplásicos [FENÓMENOS Y PROCESOS], neoplasias::neoplasias por localización::neoplasias de la mama [ENFERMEDADES], Multidisciplinary, Manchester Cancer Research Centre, acciones y usos químicos::acciones farmacológicas::mecanismos moleculares de acción farmacológica::inhibidores enzimáticos::inhibidores de proteínas cinasas [COMPUESTOS QUÍMICOS Y DROGAS], business.industry, ResearchInstitutes_Networks_Beacons/mcrc, Inhibitor resistance, Cyclin-Dependent Kinase 4, General Chemistry, Cyclin-Dependent Kinase 6, Proteïnes quinases - Inhibidors, Retinoblastoma Binding Proteins, Receptors, Estrogen, Drug Resistance, Neoplasm, Drug resistance, Mama - Càncer - Tractament, Cancer research, Female, business, Biomarkers

Abstract

CDK4/6 inhibitors combined with endocrine therapy have demonstrated higher antitumor activity than endocrine therapy alone for the treatment of advanced estrogen receptor-positive breast cancer. Some of these tumors are de novo resistant to CDK4/6 inhibitors and others develop acquired resistance. Here, we show that p16 overexpression is associated with reduced antitumor activity of CDK4/6 inhibitors in patient-derived xenografts (n = 37) and estrogen receptor-positive breast cancer cell lines, as well as reduced response of early and advanced breast cancer patients to CDK4/6 inhibitors (n = 89). We also identified heterozygous RB1 loss as biomarker of acquired resistance and poor clinical outcome. Combination of the CDK4/6 inhibitor ribociclib with the PI3K inhibitor alpelisib showed antitumor activity in estrogen receptor-positive non-basal-like breast cancer patient-derived xenografts, independently of PIK3CA, ESR1 or RB1 mutation, also in drug de-escalation experiments or omitting endocrine therapy. Our results offer insights into predicting primary/acquired resistance to CDK4/6 inhibitors and post-progression therapeutic strategies. This study has been supported by the Susan G. Komen Foundation (CCR15330331) and by the Catalan Agency AGAUR (2017 SGR 540) [to V.S.]. V.S. received funds from the Instituto de Salud Carlos III: grants PI13/01714, CP14/00228, MV15/00041, CPII19/00033 and PI20/00892. M.P. received a Juan de la Cierva Grant from the Ministerio de Economía y Competitividad (FJCI-2015-25412), L.Mo. a grant from FI-AGAUR (2019 FI_B 01199), F.B-M. a grant from the Fundación Científica Asociación Española Contra el Cáncer (AECC_Postdoctoral17-1062) and M.S-G, a Marie Slodowska-Curie Innovative Training Networks PhD fellowship (H2020-MSCA-ITN-2015_675392). This work was supported by Breast Cancer Research Foundation (BCRF-19-08), Instituto de Salud Carlos III Project Reference number AC15/00062 and the EC under the framework of the ERA-NET TRANSCAN-2 initiative co-financed by FEDER, Instituto de Salud Carlos III (CB16/12/00449 and PI19/01181) and Asociación Española Contra el Cáncer (to J.A.). R.B.C. laboratory is supported by Breast Cancer Now (grant numbers: MAN-Q1 and MAN-Q2), NIHR Manchester Biomedical Research Centre (IS-BRC-1215-20007) and EdiREX Horizon 2020 grant No.731105. The xenograft program in the C.C. laboratory is supported by Cancer Research UK and also received funding from an EU H2020 Network of Excellence (EuroCAN). This work has been supported by NIH grants P30 CA008748 and RO1CA190642-01, the CDMRP grant BC171535P1, and the Breast Cancer Research Foundation [to M.S.]. A.P. received funds from Instituto de Salud Carlos III—PI16/00904 and PI19/01846, Breast Cancer Now—2018NOVPCC1294, Breast Cancer Research Foundation-AACR Career Development Awards for Translational Breast Cancer Research 19-20-26-PRAT, Fundació La Marató TV3 201935-30, the European Union’s Horizon 2020 research and innovation program H2020-SC1-BHC-2018-2020. IRB Barcelona is a recipient of a Severo Ochoa Centre of Excellence Award from the Spanish Ministry of Economy and Competitiveness (MINECO; Government of Spain) and is supported by CERCA (Generalitat de Catalunya). C. S. Verma reports grants from MSD International and grants from Ipsen outside the submitted work.

Published

2022

41. The PARP1 selective inhibitor saruparib (AZD5305) elicits potent and durable antitumor activity in patient-derived BRCA1/2-associated cancer models

Author

Andrea Herencia-Ropero, Alba Llop-Guevara, Anna D. Staniszewska, Joanna Domènech-Vivó, Eduardo García-Galea, Alejandro Moles-Fernández, Flaminia Pedretti, Heura Domènech, Olga Rodríguez, Marta Guzmán, Enrique J. Arenas, Helena Verdaguer, Fernando J. Calero-Nieto, Sara Talbot, Luis Tobalina, Elisabetta Leo, Alan Lau, Paolo Nuciforo, Rodrigo Dienstmann, Teresa Macarulla, Joaquín Arribas, Orland Díez, Sara Gutiérrez-Enríquez, Josep V. Forment, Mark J. O’Connor, Mark Albertella, Judith Balmaña, and Violeta Serra

Subjects

PARP inhibitors, PARP1 selective, Targeted therapy, Breast cancer, DNA damaging agent, BRCA1/2, Medicine, Genetics, QH426-470

Abstract

Abstract Background Poly (ADP-ribose) polymerase 1 and 2 (PARP1/2) inhibitors (PARPi) are targeted therapies approved for homologous recombination repair (HRR)-deficient breast, ovarian, pancreatic, and prostate cancers. Since inhibition of PARP1 is sufficient to cause synthetic lethality in tumors with homologous recombination deficiency (HRD), PARP1 selective inhibitors such as saruparib (AZD5305) are being developed. It is expected that selective PARP1 inhibition leads to a safer profile that facilitates its combination with other DNA damage repair inhibitors. Here, we aimed to characterize the antitumor activity of AZD5305 in patient-derived preclinical models compared to the first-generation PARP1/2 inhibitor olaparib and to identify mechanisms of resistance. Methods Thirteen previously characterized patient-derived tumor xenograft (PDX) models from breast, ovarian, and pancreatic cancer patients harboring germline pathogenic alterations in BRCA1, BRCA2, or PALB2 were used to evaluate the efficacy of AZD5305 alone or in combination with carboplatin or an ataxia telangiectasia and Rad3 related (ATR) inhibitor (ceralasertib) and compared it to the first-generation PARPi olaparib. We performed DNA and RNA sequencing as well as protein-based assays to identify mechanisms of acquired resistance to either PARPi. Results AZD5305 showed superior antitumor activity than the first-generation PARPi in terms of preclinical complete response rate (75% vs. 37%). The median preclinical progression-free survival was significantly longer in the AZD5305-treated group compared to the olaparib-treated group (> 386 days vs. 90 days). Mechanistically, AZD5305 induced more replication stress and genomic instability than the PARP1/2 inhibitor olaparib in PARPi-sensitive tumors. All tumors at progression with either PARPi (39/39) showed increase of HRR functionality by RAD51 foci formation. The most prevalent resistance mechanisms identified were the acquisition of reversion mutations in BRCA1/BRCA2 and the accumulation of hypomorphic BRCA1. AZD5305 did not sensitize PDXs with acquired resistance to olaparib but elicited profound and durable responses when combined with carboplatin or ceralasertib in 3/6 and 5/5 models, respectively. Conclusions Collectively, these results show that the novel PARP1 selective inhibitor AZD5305 yields a potent antitumor response in PDX models with HRD and delays PARPi resistance alone or in combination with carboplatin or ceralasertib, which supports its use in the clinic as a new therapeutic option.

Published

2024

42. PI3K activation promotes resistance to eribulin in HER2-negative breast cancer

Author

Mireia Parés, Javier Cortes, Marta Guzman, Cristina Viaplana, Rodrigo Dienstmann, Alejandra Bruna, Carlos Caldas, Fiorella Ruiz-Pace, Albert Gris-Oliver, Patricia Cozar, Pilar Anton, Antonio Llombart-Cussac, Violeta Serra, Mònica Sánchez-Guixé, Martín A. Rivas, Jose Perez-Garcia, Celina Garcia-Garcia, Paolo Nuciforo, Joaquín Arribas, Olga Rodriguez, Maria Teresa Calvo, Judit Grueso, Mafalda Oliveira, and Yasir H. Ibrahim

Subjects

Cancer Research, Anthracycline, Class I Phosphatidylinositol 3-Kinases, Receptor, ErbB-2, medicine.medical_treatment, AKT1, Apoptosis, Breast Neoplasms, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Breast cancer, Biomarkers, Tumor, Tumor Cells, Cultured, medicine, Animals, Humans, Phosphorylation, Furans, PI3K/AKT/mTOR pathway, Cell Proliferation, Chemotherapy, business.industry, Cell Cycle, Ketones, medicine.disease, Xenograft Model Antitumor Assays, Metastatic breast cancer, Gene Expression Regulation, Neoplastic, Oncology, chemistry, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, Female, business, Proto-Oncogene Proteins c-akt, Eribulin

Abstract

BACKGROUND: Eribulin is a microtubule-targeting agent approved for the treatment of advanced or metastatic breast cancer (BC) previously treated with anthracycline- and taxane-based regimens. PIK3CA mutation is associated with worse response to chemotherapy in oestrogen receptor-positive (ER+)/human epidermal growth factor receptor 2-negative (HER2−) metastatic BC. We aimed to evaluate the role of phosphoinositide 3-kinase (PI3K)/AKT pathway mutations in eribulin resistance. METHODS: Resistance to eribulin was evaluated in HER2− BC cell lines and patient-derived tumour xenografts, and correlated with a mutation in the PI3K/AKT pathway. RESULTS: Eleven out of 23 HER2− BC xenografts treated with eribulin exhibited disease progression. No correlation with ER status was detected. Among the resistant models, 64% carried mutations in PIK3CA, PIK3R1 or AKT1, but only 17% among the sensitive xenografts (P = 0.036). We observed that eribulin treatment induced AKT phosphorylation in vitro and in patient tumours. In agreement, the addition of PI3K inhibitors reversed primary and acquired resistance to eribulin in xenograft models, regardless of the genetic alterations in PI3K/AKT pathway or ER status. Mechanistically, PI3K blockade reduced p21 levels likely enabling apoptosis, thus sensitising to eribulin treatment. CONCLUSIONS: PI3K pathway activation induces primary resistance or early adaptation to eribulin, supporting the combination of PI3K inhibitors and eribulin for the treatment of HER2− BC patients.

Published

2021

43. Identification of a Molecularly-Defined Subset of Breast and Ovarian Cancer Models that Respond to WEE1 or ATR Inhibition, Overcoming PARP Inhibitor Resistance

Author

Violeta Serra, Anderson T. Wang, Marta Castroviejo-Bermejo, Urszula M. Polanska, Marta Palafox, Andrea Herencia-Ropero, Gemma N. Jones, Zhongwu Lai, Joshua Armenia, Filippos Michopoulos, Alba Llop-Guevara, Rachel Brough, Aditi Gulati, Stephen J. Pettitt, Krishna C. Bulusu, Jenni Nikkilä, Zena Wilson, Adina Hughes, Paul W.G. Wijnhoven, Ambar Ahmed, Alejandra Bruna, Albert Gris-Oliver, Marta Guzman, Olga Rodríguez, Judit Grueso, Joaquin Arribas, Javier Cortés, Cristina Saura, Alan Lau, Susan Critchlow, Brian Dougherty, Carlos Caldas, Gordon B. Mills, J. Carl Barrett, Josep V. Forment, Elaine Cadogan, Christopher J. Lord, Cristina Cruz, Judith Balmaña, Mark J. O'Connor, Institut Català de la Salut, [Serra V] Experimental Therapeutics Group, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. CIBERONC, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. [Wang AT, Polanska UM] AstraZeneca Oncology R&D, Cambridge, United Kingdom. [Castroviejo-Bermejo M, Palafox M, Llop-Guevara A, Guzman M, Rodríguez O, Grueso J] Experimental Therapeutics Group, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. [Herencia-Ropero A] Experimental Therapeutics Group, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. Departament de Bioquímica i Biologia Molecular, Universitat Autònoma de Barcelona, Bellaterra, Spain. [Arribas J] CIBERONC, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. Growth Factors Laboratory, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. [Cortés J] Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. [Saura C] Servei d’Oncologia Mèdica, Vall d’Hebron Hospital Universitari, Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. Breast Cancer and Melanoma Group, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. [Cruz C] Experimental Therapeutics Group, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. Servei d’Oncologia Mèdica, Vall d’Hebron Hospital Universitari, Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. High Risk and Familial Cancer, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain. [Balmaña J] Servei d’Oncologia Mèdica, Vall d’Hebron Hospital Universitari, Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. High Risk and Familial Cancer, Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects

Cancer Research, Neoplasms::Neoplasms by Site::Breast Neoplasms [DISEASES], Antineoplastic Agents, Cell Cycle Proteins, Ataxia Telangiectasia Mutated Proteins, neoplasias::neoplasias por localización::neoplasias de las glándulas endocrinas::neoplasias ováricas [ENFERMEDADES], Carcinoma, Ovarian Epithelial, Poly(ADP-ribose) Polymerase Inhibitors, Chemical Actions and Uses::Pharmacologic Actions::Molecular Mechanisms of Pharmacological Action::Enzyme Inhibitors::Protein Kinase Inhibitors [CHEMICALS AND DRUGS], Humans, Other subheadings::/therapeutic use [Other subheadings], Protein Kinase Inhibitors, Ovarian Neoplasms, neoplasias::neoplasias por localización::neoplasias de la mama [ENFERMEDADES], acciones y usos químicos::acciones farmacológicas::mecanismos moleculares de acción farmacológica::inhibidores enzimáticos::inhibidores de proteínas cinasas [COMPUESTOS QUÍMICOS Y DROGAS], Otros calificadores::/uso terapéutico [Otros calificadores], BRCA1 Protein, Neoplasms::Neoplasms by Site::Endocrine Gland Neoplasms::Ovarian Neoplasms [DISEASES], Nucleosides, Ovaris - Càncer - Tractament, Protein-Tyrosine Kinases, Oncology, Mama - Càncer - Tractament, Phthalazines, Female, Biomarkers, Proteïnes quinases - Inhibidors - Ús terapèutic

Abstract

Cáncer de mama y de ovario; Inhibición WEE1 Càncer de mama i d'ovari; Inhibició WEE1 Breast and ovarian cancer; WEE1 inhibition Purpose: PARP inhibitors (PARPi) induce synthetic lethality in homologous recombination repair (HRR)-deficient tumors and are used to treat breast, ovarian, pancreatic, and prostate cancers. Multiple PARPi resistance mechanisms exist, most resulting in restoration of HRR and protection of stalled replication forks. ATR inhibition was highlighted as a unique approach to reverse both aspects of resistance. Recently, however, a PARPi/WEE1 inhibitor (WEE1i) combination demonstrated enhanced antitumor activity associated with the induction of replication stress, suggesting another approach to tackling PARPi resistance. Experimental Design: We analyzed breast and ovarian patient-derived xenoimplant models resistant to PARPi to quantify WEE1i and ATR inhibitor (ATRi) responses as single agents and in combination with PARPi. Biomarker analysis was conducted at the genetic and protein level. Metabolite analysis by mass spectrometry and nucleoside rescue experiments ex vivo were also conducted in patient-derived models. Results: Although WEE1i response was linked to markers of replication stress, including STK11/RB1 and phospho-RPA, ATRi response associated with ATM mutation. When combined with olaparib, WEE1i could be differentiated from the ATRi/olaparib combination, providing distinct therapeutic strategies to overcome PARPi resistance by targeting the replication stress response. Mechanistically, WEE1i sensitivity was associated with shortage of the dNTP pool and a concomitant increase in replication stress. Conclusions: Targeting the replication stress response is a valid therapeutic option to overcome PARPi resistance including tumors without an underlying HRR deficiency. These preclinical insights are now being tested in several clinical trials where the PARPi is administered with either the WEE1i or the ATRi. This work was supported by the Spanish Instituto de Salud Carlos III (ISCIII), an initiative of the Spanish Ministry of Economy and Innovation partially supported by European Regional Development FEDER Funds (FIS PI17/01080 to V. Serra, PI12/02606 to J. Balmaña); European Research Area-NET, Transcan-2 (AC15/00063), Asociación Española contra el Cáncer (AECC; LABAE16020PORTT), the Agència de Gestió d'Ajuts Universitaris i de Recerca (AGAUR; 2017 SGR 540), La Marató TV3 (654/C/2019), and ERAPERMED2019–215 to V. Serra. We also acknowledge the GHD-Pink program, the FERO Foundation, and the Orozco Family for supporting this study (to V. Serra). V. Serra was supported by the Miguel Servet Program (ISCIII; CPII19/00033); M. Castroviejo-Bermejo and C. Cruz (AIOC15152806CRUZ) by AECC; A. Herencia-Ropero by Generalitat de Catalunya-PERIS (SLT017/20/000081); M. Palafox by Juan de la Cierva (FJCI-2015–25412); A. Lau by AECC and Generalitat de Catalunya-PERIS (INVES20095LLOP, SLT002/16/00477); A. Gris-Oliver by FI-AGAUR (2015 FI_B 01075). This work was supported by Breast Cancer Research Foundation (BCRF-19–08), Instituto de Salud Carlos III Project Reference number AC15/00062, and the EC under the framework of the ERA-NET TRANSCAN-2 initiative co-financed by FEDER, Instituto de Salud Carlos III (CB16/12/00449 and PI19/01181), and Asociación Española Contra el Cáncer (to J. Arribas). The xenograft program in the Caldas laboratory was supported by Cancer Research UK and also received funding from an EU H2020 Network of Excellence (EuroCAN). The RPPA facility is funded by NCI #CA16672.

Published

2022

44. MYC Inhibition Halts Metastatic Breast Cancer Progression by Blocking Growth, Invasion, and Seeding

Author

Daniel Massó-Vallés, Marie-Eve Beaulieu, Toni Jauset, Fabio Giuntini, Mariano F. Zacarías-Fluck, Laia Foradada, Sandra Martínez-Martín, Erika Serrano, Génesis Martín-Fernández, Sílvia Casacuberta-Serra, Virginia Castillo Cano, Jastrinjan Kaur, Sergio López-Estévez, Miguel Ángel Morcillo, Mohammad Alzrigat, Loay Mahmoud, Antonio Luque-García, Marta Escorihuela, Marta Guzman, Joaquín Arribas, Violeta Serra, Lars-Gunnar Larsson, Jonathan R. Whitfield, and Laura Soucek

Abstract

MYC's role in promoting tumorigenesis is beyond doubt, but its function in the metastatic process is still controversial. Omomyc is a MYC dominant negative that has shown potent antitumor activity in multiple cancer cell lines and mouse models, regardless of their tissue of origin or driver mutations, by impacting on several of the hallmarks of cancer. However, its therapeutic efficacy against metastasis has not been elucidated yet. Here we demonstrate for the first time that MYC inhibition by transgenic Omomyc is efficacious against all breast cancer molecular subtypes, including triple-negative breast cancer, where it displays potent antimetastatic properties both in vitro and in vivo. Importantly, pharmacologic treatment with the recombinantly produced Omomyc miniprotein, recently entering a clinical trial in solid tumors, recapitulates several key features of expression of the Omomyc transgene, confirming its clinical applicability to metastatic breast cancer, including advanced triple-negative breast cancer, a disease in urgent need of better therapeutic options. Significance: While MYC role in metastasis has been long controversial, this manuscript demonstrates that MYC inhibition by either transgenic expression or pharmacologic use of the recombinantly produced Omomyc miniprotein exerts antitumor and antimetastatic activity in breast cancer models in vitro and in vivo, suggesting its clinical applicability.

Published

2022

45. MYC Inhibition Halts Metastatic Breast Cancer Progression by Blocking Growth, Invasion, and Seeding

Author

Daniel Massó-Vallés, Marie-Eve Beaulieu, Toni Jauset, Fabio Giuntini, Mariano F. Zacarías-Fluck, Laia Foradada, Sandra Martínez-Martín, Erika Serrano, Génesis Martín-Fernández, Sílvia Casacuberta-Serra, Virginia Castillo Cano, Jastrinjan Kaur, Sergio López-Estévez, Miguel Ángel Morcillo, Mohammad Alzrigat, Loay Mahmoud, Antonio Luque-García, Marta Escorihuela, Marta Guzman, Joaquín A

Published

2022

46. 1901 - RICKETTSIOSIS, ¿UNA ENFERMEDAD OLVIDADA? ANÁLISIS CLÍNICO-EPIDEMIOLÓGICO EN PROVINCIA DE ALBACETE

Author

Merino, Rocío Garví, Puchol, Jordi Olucha, Pérez, Marta Guzmán, and Fernández, Marcos Sánchez

Published

2023

47. Genetic Alterations in the PI3K/AKT Pathway and Baseline AKT Activity Define AKT Inhibitor Sensitivity in Breast Cancer Patient-derived Xenografts

Author

Fara Brasó-Maristany, Mònica Sánchez-Guixé, Andreu Ódena, Aleix Prat, Olga Rodriguez, Yasir H. Ibrahim, Alejandra Bruna, Elza C. de Bruin, Barry R. Davies, Alan Barnicle, Laia Monserrat, Judit Grueso, Carlos Caldas, Guillermo Villacampa, Nicholas C. Turner, Avinash Reddy, Paolo Nuciforo, Albert Gris-Oliver, Joaquín Arribas, Violeta Serra, Gordon B. Mills, Maurizio Scaltriti, Caroline S. Hirst, Mafalda Oliveira, Gaia Schiavon, Cristina Saura, Marta Guzman, Marta Palafox, Pedram Razavi, Mireia Parés, and Rodrigo Dienstmann

Subjects

0301 basic medicine, Cancer Research, Paclitaxel, Class I Phosphatidylinositol 3-Kinases, DNA Mutational Analysis, AKT1, P70-S6 Kinase 1, Breast Neoplasms, Tuberous Sclerosis Complex 1 Protein, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Breast cancer, Antineoplastic Combined Chemotherapy Protocols, medicine, Biomarkers, Tumor, PTEN, Animals, Humans, Pyrroles, Breast, Protein kinase B, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Mastectomy, biology, Fulvestrant, business.industry, TOR Serine-Threonine Kinases, Ribosomal Protein S6 Kinases, 70-kDa, medicine.disease, Prognosis, Metastatic breast cancer, Xenograft Model Antitumor Assays, 030104 developmental biology, Pyrimidines, Oncology, Chemotherapy, Adjuvant, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Mutation, biology.protein, Cancer research, Female, business, Proto-Oncogene Proteins c-akt, medicine.drug, Signal Transduction

Abstract

Purpose: AZD5363/capivasertib is a pan-AKT catalytic inhibitor with promising activity in combination with paclitaxel in triple-negative metastatic breast cancer harboring PI3K/AKT-pathway alterations and in estrogen receptor–positive breast cancer in combination with fulvestrant. Here, we aimed to identify response biomarkers and uncover mechanisms of resistance to AZD5363 and its combination with paclitaxel. Experimental Design: Genetic and proteomic markers were analyzed in 28 HER2-negative patient-derived xenografts (PDXs) and in patient samples, and correlated to AZD5363 sensitivity as single agent and in combination with paclitaxel. Results: Four PDX were derived from patients receiving AZD5363 in the clinic which exhibited concordant treatment response. Mutations in PIK3CA/AKT1 and absence of mTOR complex 1 (mTORC1)-activating alterations, for example, in MTOR or TSC1, were associated with sensitivity to AZD5363 monotherapy. Interestingly, excluding PTEN from the composite biomarker increased its accuracy from 64% to 89%. Moreover, resistant PDXs exhibited low baseline pAKT S473 and residual pS6 S235 upon treatment, suggesting that parallel pathways bypass AKT/S6K1 signaling in these models. We identified two mechanisms of acquired resistance to AZD5363: cyclin D1 overexpression and loss of AKT1 p.E17K. Conclusions: This study provides insight into putative predictive biomarkers of response and acquired resistance to AZD5363 in HER2-negative metastatic breast cancer.

Published

2019

48. A RAD51 assay feasible in routine tumor samples calls PARP inhibitor response beyond BRCA mutation

Author

Jean-Yves Masson, Judith Balmaña, Alejandra Bruna, Cristina Saura, Sara Gutiérrez-Enríquez, Marta Castroviejo-Bermejo, José Baselga, Carlos Caldas, Mark J. O'Connor, Alejandro Moles-Fernández, Xavier Serres-Créixams, Judit Grueso, Olga Rodriguez, Marta Guzman, Olivier Deas, Cristina Cruz, Stefano Cairo, Yasir H. Ibrahim, Rodrigo Dienstmann, Sandra Bonache, Guillermo Villacampa, M.T. Vidal, Benedetta Pellegrino, Jacques Simard, Cristina Viaplana, J. Carl Barrett, Patricia Gomez, Javier Cortés, Paolo Nuciforo, Mandy Ducy, Albert Gris-Oliver, Jean-Gabriel Judde, Violeta Serra, Orland Diez, Vicente Peg, Alba Llop-Guevara, Graham Dellaire, Jos Jonkers, Isabel T. Rubio, Jonkers, Jos [0000-0002-9264-9792], Balmaña, Judith [0000-0002-0762-6415], Serra, Violeta [0000-0001-6620-1065], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Medicine (General), RAD51, homologous recombination, QH426-470, Piperazines, chemistry.chemical_compound, Mice, 0302 clinical medicine, Medicine, PARP inhibitors, Research Articles, Cancer, education.field_of_study, 3. Good health, 030220 oncology & carcinogenesis, PARP inhibitor, Molecular Medicine, Biomarker (medicine), Heterografts, Female, Research Article, PALB2, Population, Antineoplastic Agents, Breast Neoplasms, Poly(ADP-ribose) Polymerase Inhibitors, Olaparib, 03 medical and health sciences, R5-920, Breast cancer, Genetics, Biomarkers, Tumor, Animals, Humans, Pharmacology & Drug Discovery, education, Biomarkers & Diagnostic Imaging, business.industry, Inhibitors, BRCA mutation, medicine.disease, BRCA1, 030104 developmental biology, chemistry, Drug Resistance, Neoplasm, Cancer research, Phthalazines, Rad51 Recombinase, business

Abstract

Poly(ADP‐ribose) polymerase (PARP) inhibitors (PARPi) are effective in cancers with defective homologous recombination DNA repair (HRR), including BRCA1/2‐related cancers. A test to identify additional HRR‐deficient tumors will help to extend their use in new indications. We evaluated the activity of the PARPi olaparib in patient‐derived tumor xenografts (PDXs) from breast cancer (BC) patients and investigated mechanisms of sensitivity through exome sequencing, BRCA1 promoter methylation analysis, and immunostaining of HRR proteins, including RAD51 nuclear foci. In an independent BC PDX panel, the predictive capacity of the RAD51 score and the homologous recombination deficiency (HRD) score were compared. To examine the clinical feasibility of the RAD51 assay, we scored archival breast tumor samples, including PALB2‐related hereditary cancers. The RAD51 score was highly discriminative of PARPi sensitivity versus PARPi resistance in BC PDXs and outperformed the genomic test. In clinical samples, all PALB2‐related tumors were classified as HRR‐deficient by the RAD51 score. The functional biomarker RAD51 enables the identification of PARPi‐sensitive BC and broadens the population who may benefit from this therapy beyond BRCA1/2‐related cancers.

Published

2018

49. Loss of USP28-mediated BRAF degradation drives resistance to RAF cancer therapies

Author

Christopher Nötzel, Zhou Siqin, Javier Cortes, Brendan Pang, Marta Guzman, Touati Benoukraf, Pieter Johan Adam Eichhorn, Nesaretnam Barr Kumarakulasinghe, Violeta Serra, Zul Fazreen Adam Isa, Nishi Kumari, Patrick Jaynes, Prasanna Vasudevan Iyengar, Paolo Nuciforo, Azad Saei, Wai Leong Tam, John Lalith Charles Richard, Eva Muñoz-Couselo, Henry Yang, and Marta Palafox

Subjects

0301 basic medicine, MAPK/ERK pathway, Proto-Oncogene Proteins B-raf, F-Box-WD Repeat-Containing Protein 7, MAP Kinase Signaling System, Immunology, Glycine, Down-Regulation, Apoptosis, Article, 03 medical and health sciences, Mice, Downregulation and upregulation, Cell Line, Tumor, Immunology and Allergy, Medicine, Animals, Humans, Sulfones, Vemurafenib, neoplasms, Melanoma, Research Articles, business.industry, Protein Stability, Rigosertib, Cancer, medicine.disease, Prognosis, 030104 developmental biology, HEK293 Cells, Drug Resistance, Neoplasm, Proteolysis, Cancer research, Signal transduction, business, Ubiquitin Thiolesterase, V600E, Gene Deletion, medicine.drug

Abstract

Adaptive responses have been demonstrated to limit activity to targeted therapies. Saei et al. show that loss of USP28/FBW7-mediated BRAF degradation is observed in a proportion of melanoma patients and can be responsible for resistance through upregulation of MAPK signaling pathway., RAF kinase inhibitors are clinically active in patients with BRAF (V600E) mutant melanoma. However, rarely do tumors regress completely, with the majority of responses being short-lived. This is partially mediated through the loss of negative feedback loops after MAPK inhibition and reactivation of upstream signaling. Here, we demonstrate that the deubiquitinating enzyme USP28 functions through a feedback loop to destabilize RAF family members. Loss of USP28 stabilizes BRAF enhancing downstream MAPK activation and promotes resistance to RAF inhibitor therapy in culture and in vivo models. Importantly, we demonstrate that USP28 is deleted in a proportion of melanoma patients and may act as a biomarker for response to BRAF inhibitor therapy in patients. Furthermore, we identify Rigosertib as a possible therapeutic strategy for USP28-depleted tumors. Our results show that loss of USP28 enhances MAPK activity through the stabilization of RAF family members and is a key factor in BRAF inhibitor resistance., Graphical Abstract

Published

2017

50. Dual mTORC1/2 and HER2 Blockade Results in Antitumor Activity in Preclinical Models of Breast Cancer Resistant to Anti-HER2 Therapy

Author

Josep Tabernero, José Baselga, Christian Rommel, Maria Teresa Calvo, Katti Jessen, Marta Guzman, Celina Garcia-Garcia, Maurizio Scaltriti, José Francisco Pérez, Yi Liu, Claudia Aura, Yasir H. Ibrahim, Judit Grueso, and Violeta Serra

Subjects

MAPK/ERK pathway, Cancer Research, Programmed cell death, Receptor, ErbB-2, Blotting, Western, Mice, Nude, Antineoplastic Agents, Apoptosis, Breast Neoplasms, mTORC1, Mechanistic Target of Rapamycin Complex 1, Pharmacology, Antibodies, Monoclonal, Humanized, Lapatinib, Mice, Phosphatidylinositol 3-Kinases, Trastuzumab, Tumor Cells, Cultured, medicine, Animals, Humans, Phosphorylation, Extracellular Signal-Regulated MAP Kinases, skin and connective tissue diseases, Protein Kinase Inhibitors, neoplasms, Protein kinase B, PI3K/AKT/mTOR pathway, Benzoxazoles, business.industry, TOR Serine-Threonine Kinases, Cell Cycle, Proteins, Drug Synergism, Xenograft Model Antitumor Assays, Pyrimidines, Oncology, Drug Resistance, Neoplasm, Multiprotein Complexes, Quinazolines, Female, business, Proto-Oncogene Proteins c-akt, Transcription Factors, medicine.drug

Abstract

Purpose: The PI3K/Akt/mTOR pathway is an attractive target in HER2-positive breast cancer that is refractory to anti-HER2 therapy. The hypothesis is that the suppression of this pathway results in sensitization to anti-HER2 agents. However, this combinatorial strategy has not been comprehensively tested in models of trastuzumab and lapatinib resistance. Experimental Design: We analyzed in vitro cell viability and induction of apoptosis in five different cell lines resistant to trastuzumab and lapatinib. Inhibition of HER2/HER3 phosphorylation, PI3K/Akt/mTOR, and extracellular signal-regulated kinase (ERK) signaling pathways was evaluated by Western blotting. Tumor growth inhibition after treatment with lapatinib, INK-128, or the combination of both agents was evaluated in three different animal models: two cell-based xenograft models refractory to both trastuzumab and lapatinib and a xenograft derived from a patient who relapsed on trastuzumab-based therapy. Results: The addition of lapatinib to INK-128 prevented both HER2 and HER3 phosphorylation induced by INK-128, resulting in inhibition of both PI3K/Akt/mTOR and ERK pathways. This dual blockade produced synergistic induction of cell death in five different HER2-positive cell lines resistant to trastuzumab and lapatinib. In vivo, both cell line–based and patient-derived xenografts showed exquisite sensitivity to the antitumor activity of the combination of lapatinib and INK-128, which resulted in durable tumor shrinkage and exhibited no signs of toxicity in these models. Conclusions: The simultaneous blockade of both PI3K/Akt/mTOR and ERK pathways obtained by combining lapatinib with INK-128 acts synergistically in inducing cell death and tumor regression in breast cancer models refractory to anti-HER2 therapy. Clin Cancer Res; 18(9); 2603–12. ©2012 AACR.

Published

2012