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1. Osteopontin is a therapeutic target that drives breast cancer recurrence

Author

Yu Gu, Tarek Taifour, Tung Bui, Dongmei Zuo, Alain Pacis, Alexandre Poirier, Sherif Attalla, Anne-Marie Fortier, Virginie Sanguin-Gendreau, Tien-Chi Pan, Vasilios Papavasiliou, Nancy U. Lin, Melissa E. Hughes, Kalie Smith, Morag Park, Michel L. Tremblay, Lewis A. Chodosh, Rinath Jeselsohn, and William J. Muller

Subjects
Science
Abstract

Abstract Recurrent breast cancers often develop resistance to standard-of-care therapies. Identifying targetable factors contributing to cancer recurrence remains the rate-limiting step in improving long-term outcomes. In this study, we identify tumor cell-derived osteopontin as an autocrine and paracrine driver of tumor recurrence. Osteopontin promotes tumor cell proliferation, recruits macrophages, and synergizes with IL-4 to further polarize them into a pro-tumorigenic state. Macrophage depletion and osteopontin inhibition decrease recurrent tumor growth. Furthermore, targeting osteopontin in primary tumor-bearing female mice prevents metastasis, permits T cell infiltration and activation, and improves anti-PD-1 immunotherapy response. Clinically, osteopontin expression is higher in recurrent metastatic tumors versus female patient-matched primary breast tumors. Osteopontin positively correlates with macrophage infiltration, increases with higher tumor grade, and its elevated pathway activity is associated with poor prognosis and long-term recurrence. Our findings suggest clinical implications and an alternative therapeutic strategy based on osteopontin’s multiaxial role in breast cancer progression and recurrence.

Published
2024
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2. Targeting fatty acid oxidation enhances response to HER2-targeted therapy

Author

Ipshita Nandi, Linjia Ji, Harvey W. Smith, Daina Avizonis, Vasilios Papavasiliou, Cynthia Lavoie, Alain Pacis, Sherif Attalla, Virginie Sanguin-Gendreau, and William J. Muller

Subjects
Science
Abstract

Abstract Metabolic reprogramming, a hallmark of tumorigenesis, involves alterations in glucose and fatty acid metabolism. Here, we investigate the role of Carnitine palmitoyl transferase 1a (Cpt1a), a key enzyme in long-chain fatty acid (LCFA) oxidation, in ErbB2-driven breast cancers. In ErbB2+ breast cancer models, ablation of Cpt1a delays tumor onset, growth, and metastasis. However, Cpt1a-deficient cells exhibit increased glucose dependency that enables survival and eventual tumor progression. Consequently, these cells exhibit heightened oxidative stress and upregulated nuclear factor erythroid 2-related factor 2 (Nrf2) activity. Inhibiting Nrf2 or silencing its expression reduces proliferation and glucose consumption in Cpt1a-deficient cells. Combining the ketogenic diet, composed of LCFAs, or an anti-ErbB2 monoclonal antibody (mAb) with Cpt1a deficiency significantly perturbs tumor growth, enhances apoptosis, and reduces lung metastasis. Using an immunocompetent model, we show that Cpt1a inhibition promotes an antitumor immune microenvironment, thereby enhancing the efficacy of anti-ErbB2 mAbs. Our findings underscore the importance of targeting fatty acid oxidation alongside HER2-targeted therapies to combat resistance in HER2+ breast cancer patients.

Published
2024
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3. Integrated multi-omics analysis of adverse cardiac remodeling and metabolic inflexibility upon ErbB2 and ERRα deficiency

Author

Catherine R. Dufour, Hui Xia, Wafa B’chir, Marie-Claude Perry, Uros Kuzmanov, Anastasiia Gainullina, Kurt Dejgaard, Charlotte Scholtes, Carlo Ouellet, Dongmei Zuo, Virginie Sanguin-Gendreau, Christina Guluzian, Harvey W. Smith, William J. Muller, Etienne Audet-Walsh, Alexey A. Sergushichev, Andrew Emili, and Vincent Giguère

Subjects
Biology (General), QH301-705.5
Abstract

Murine hearts deficient in ErbB2 and/or ERRα are used to profile the adverse cardiac remodeling associated with potential targeted breast cancer treatments by phosphoproteomic, transcriptomic and metabolomic profiling.

Published
2022
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4. Coordinated activation of c-Src and FOXM1 drives tumor cell proliferation and breast cancer progression

Author

Ipshita Nandi, Harvey W. Smith, Virginie Sanguin-Gendreau, Linjia Ji, Alain Pacis, Vasilios Papavasiliou, Dongmei Zuo, Stella Nam, Sherif S. Attalla, Sung Hoon Kim, Sierra Lusson, Hellen Kuasne, Anne-Marie Fortier, Paul Savage, Constanza Martinez Ramirez, Morag Park, John A. Katzenellenbogen, Benita S. Katzenellenbogen, and William J. Muller

Subjects
Oncology, Therapeutics, Medicine
Abstract

Activation of the tyrosine kinase c-Src promotes breast cancer progression and poor outcomes, yet the underlying mechanisms are incompletely understood. Here, we have shown that deletion of c-Src in a genetically engineered model mimicking the luminal B molecular subtype of breast cancer abrogated the activity of forkhead box M1 (FOXM1), a master transcriptional regulator of the cell cycle. We determined that c-Src phosphorylated FOXM1 on 2 tyrosine residues to stimulate its nuclear localization and target gene expression. These included key regulators of G2/M cell-cycle progression as well as c-Src itself, forming a positive feedback loop that drove proliferation in genetically engineered and patient-derived models of luminal B–like breast cancer. Using genetic approaches and small molecules that destabilize the FOXM1 protein, we found that targeting this mechanism induced G2/M cell-cycle arrest and apoptosis, blocked tumor progression, and impaired metastasis. We identified a positive correlation between FOXM1 and c-Src expression in human breast cancer and show that the expression of FOXM1 target genes predicts poor outcomes and associates with the luminal B subtype, which responds poorly to currently approved therapies. These findings revealed a regulatory network centered on c-Src and FOXM1 that is a targetable vulnerability in aggressive luminal breast cancers.

Published
2023
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5. Pharmacological or genetic inhibition of iNOS prevents cachexia‐mediated muscle wasting and its associated metabolism defects

Author

Jason Sadek, Derek T Hall, Bianca Colalillo, Amr Omer, Anne‐Marie K Tremblay, Virginie Sanguin‐Gendreau, William Muller, Sergio Di Marco, Marco Emilio Bianchi, and Imed‐Eddine Gallouzi

Subjects
cachexia, cancer, inflammation, iNOS, metabolism, Medicine (General), R5-920, Genetics, QH426-470
Abstract

Abstract Cachexia syndrome develops in patients with diseases such as cancer and sepsis and is characterized by progressive muscle wasting. While iNOS is one of the main effectors of cachexia, its mechanism of action and whether it could be targeted for therapy remains unexplored. Here, we show that iNOS knockout mice and mice treated with the clinically tested iNOS inhibitor GW274150 are protected against muscle wasting in models of both septic and cancer cachexia. We demonstrate that iNOS triggers muscle wasting by disrupting mitochondrial content, morphology, and energy production processes such as the TCA cycle and acylcarnitine transport. Notably, iNOS inhibits oxidative phosphorylation through impairment of complexes II and IV of the electron transport chain and reduces ATP production, leading to energetic stress, activation of AMPK, suppression of mTOR, and, ultimately, muscle atrophy. Importantly, all these effects were reversed by GW274150. Therefore, our data establish how iNOS induces muscle wasting under cachectic conditions and provide a proof of principle for the repurposing of iNOS inhibitors, such as GW274150 for the treatment of cachexia.

Published
2021
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6. An ErbB2/c-Src axis links bioenergetics with PRC2 translation to drive epigenetic reprogramming and mammary tumorigenesis

Author

Harvey W. Smith, Alison Hirukawa, Virginie Sanguin-Gendreau, Ipshita Nandi, Catherine R. Dufour, Dongmei Zuo, Kristofferson Tandoc, Matthew Leibovitch, Salendra Singh, Jonathan P. Rennhack, Matthew Swiatnicki, Cynthia Lavoie, Vasilios Papavasiliou, Carolin Temps, Neil O. Carragher, Asier Unciti-Broceta, Paul Savage, Mark Basik, Vincent van Hoef, Ola Larsson, Caroline L. Cooper, Ana Cristina Vargas Calderon, Jane Beith, Ewan Millar, Christina Selinger, Vincent Giguère, Morag Park, Lyndsay N. Harris, Vinay Varadan, Eran R. Andrechek, Sandra A. O’Toole, Ivan Topisirovic, and William J. Muller

Subjects
Science
Abstract

Polycomb Repressor Complex 2 (PRC2) is frequently up-regulated in cancers. Here, the authors show that the tyrosine kinase c-Src stimulates mitochondrial function to signal energy sufficiency to mTORC1, increasing translation of the PRC2 subunits EZH2 and SUZ12 to support ErbB2-dependent tumours.

Published
2019
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7. Reduction of Global H3K27me3 Enhances HER2/ErbB2 Targeted Therapy

Author

Alison Hirukawa, Salendra Singh, Jarey Wang, Jonathan P. Rennhack, Matthew Swiatnicki, Virginie Sanguin-Gendreau, Dongmei Zuo, Kamilia Daldoul, Cynthia Lavoie, Morag Park, Eran R. Andrechek, Thomas F. Westbrook, Lyndsay N. Harris, Vinay Varadan, Harvey W. Smith, and William J. Muller

Subjects
Biology (General), QH301-705.5
Abstract

Summary: Monoclonal antibodies (mAbs) targeting the oncogenic receptor tyrosine kinase ERBB2/HER2, such as Trastuzumab, are the standard of care therapy for breast cancers driven by ERBB2 overexpression and activation. However, a substantial proportion of patients exhibit de novo resistance. Here, by comparing matched Trastuzumab-naive and post-treatment patient samples from a neoadjuvant trial, we link resistance with elevation of H3K27me3, a repressive histone modification catalyzed by polycomb repressor complex 2 (PRC2). In ErbB2+ breast cancer models, PRC2 silences endogenous retroviruses (ERVs) to suppress anti-tumor type-I interferon (IFN) responses. In patients, elevated H3K27me3 in tumor cells following Trastuzumab treatment correlates with suppression of interferon-driven viral defense gene expression signatures and poor response. Using an immunocompetent model, we provide evidence that EZH2 inhibitors promote interferon-driven immune responses that enhance the efficacy of anti-ErbB2 mAbs, suggesting the potential clinical benefit of epigenomic reprogramming by H3K27me3 depletion in Trastuzumab-resistant disease. : Hirukawa et al. link Trastuzumab resistance in ErbB2+ breast cancers with activity of the methyltransferase EZH2, a key epigenetic regulator. By silencing retrotransposons, EZH2 suppresses type-I interferon signaling to limit immune surveillance. Retrotransposon de-repression following EZH2 inhibition triggers interferon responses and sensitizes immunocompetent in vivo models to ErbB2 antibody therapy. Keywords: ErbB2/HER2, breast cancer, Polycomb Repressor Complex 2, PRC2, epigenetics, Trastuzumab resistance, endogenous retroviruses, immune surveillance, type I interferon signaling, transcriptional silencing

Published
2019
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8. Supplemental Figure 4 FIP1C is a negative modulator of Akt and MAPK activation in an ErbB2-driven model from Rab11-FIP1C Is a Critical Negative Regulator in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Jim C. Norman, Douglas Strathdee, Lewis Chodosh, Morag Park, Gordon B. Mills, Michael Hallett, Shirley Campbell, Julie M. Livingstone, Shreya Mitra, Laura Jones, Virginie Sanguin-Gendreau, Cynthia Lavoie, Julie-Émilie Huot-Marchand, Jason Turpin, Louise Mitchell, and Pierre-Luc Boulay

Abstract

The Supplemental Figure 4 consists in key additionnal data sets to support and supplement Figure 5. Briefly, this supplemental figure 4 shows immunohistochemistry staining performed on FIP1C-MTB-NDL and NIC/FIP1C mammary tumors to examine activation of key component of ErbB2 signaling. Our results indicates that induction of FIP1C decreases endogenous level of P-Erk1/2 and FASN. In contrast, deletion of FIP1C significantly increases P-Erk1/2 and FASN.

Published
2023

9. Supplemental Figure 2 In vitro role of FIP1C in regulating cell proliferation in ErbB2/neuNDL primary cells from Rab11-FIP1C Is a Critical Negative Regulator in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Jim C. Norman, Douglas Strathdee, Lewis Chodosh, Morag Park, Gordon B. Mills, Michael Hallett, Shirley Campbell, Julie M. Livingstone, Shreya Mitra, Laura Jones, Virginie Sanguin-Gendreau, Cynthia Lavoie, Julie-Émilie Huot-Marchand, Jason Turpin, Louise Mitchell, and Pierre-Luc Boulay

Abstract

The Supplemental Figure 2 shows alternative strategy to understand and investigate the pathobiological function of FIP1C in ErbB2-mediated breast cancer progression. Briefly, this supplemental data sets report that we established primary ErbB2/neuNDL cell line and generated FIP1C-overexpressed (His-FIP1C) and FIP1C-depleted cell lines (shFIP1C)to examine cell proliferation, cell motility and β1-integrin trafficking in a ErbB2-dependent context. Our results show that overexpression of FIP1C decrease cell proliferation and EGF-promoted cell invasion in an ErbB2-dependent context. However, the depletion of FIP1C using shRNA approach leads into increase cell proliferation as well as cell migration and invasion fate in an ErbB2-dependent context. This in vitro characterization of FIP1C-proficient and -deficient ErbB2/neuNDL cell lines is a supplement panel to support the Figure 2.

Published
2023

10. Supplemental Figure 3 Characterization of FIP1C/ErbB2/neuNDL cell lines in regulating tumor growth using athymic NCr mice from Rab11-FIP1C Is a Critical Negative Regulator in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Jim C. Norman, Douglas Strathdee, Lewis Chodosh, Morag Park, Gordon B. Mills, Michael Hallett, Shirley Campbell, Julie M. Livingstone, Shreya Mitra, Laura Jones, Virginie Sanguin-Gendreau, Cynthia Lavoie, Julie-Émilie Huot-Marchand, Jason Turpin, Louise Mitchell, and Pierre-Luc Boulay

Abstract

The Supplemental Figure 3 contains additionnal and key data sets to supplement the Figure 4. Briefly, we used the FIP1C-proficient and -deficient ErbB2/neuNDL cell lines to confirm the in vivo data related to cell proliferation analysis as presented at Figure 4. The Supplemental Figure 3 indicates that overexpression of FIP1C significantly decrease Ki67 levels and Cyclin-dependent inhibitors such as p21/CIP1 and p16/INK4A.

Published
2023

11. Supplemental Figure 5 FIP1C is not distribute at adjacent junctional complexes. Clinical relevance of FIP1C in Her2-positive breast cancer patients from Rab11-FIP1C Is a Critical Negative Regulator in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Jim C. Norman, Douglas Strathdee, Lewis Chodosh, Morag Park, Gordon B. Mills, Michael Hallett, Shirley Campbell, Julie M. Livingstone, Shreya Mitra, Laura Jones, Virginie Sanguin-Gendreau, Cynthia Lavoie, Julie-Émilie Huot-Marchand, Jason Turpin, Louise Mitchell, and Pierre-Luc Boulay

Abstract

The Supplemental Figure 5 demonstrates that FIP1C does not co-localize with E-cadherin and therefore FIP1C acts indirectly on E-cadherin status in ErbB2-driven model. Additionnally, this Supplemental Figure 5 shows that FIP1C levels is inversely correlated with Her2 grade status as reported by TCGA human data sets.

Published
2023

12. Data from Rab11-FIP1C Is a Critical Negative Regulator in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Jim C. Norman, Douglas Strathdee, Lewis Chodosh, Morag Park, Gordon B. Mills, Michael Hallett, Shirley Campbell, Julie M. Livingstone, Shreya Mitra, Laura Jones, Virginie Sanguin-Gendreau, Cynthia Lavoie, Julie-Émilie Huot-Marchand, Jason Turpin, Louise Mitchell, and Pierre-Luc Boulay

Abstract

Rab coupling protein (FIP1C), an effector of the Rab11 GTPases, including Rab25, is amplified and overexpressed in 10% to 25% of primary breast cancers and correlates with poor clinical outcome. Rab25 is also frequently silenced in triple-negative breast cancer, suggesting its ability to function as either an oncogene or a tumor suppressor, depending on the breast cancer subtype. However, the pathobiologic role of FIP family members, such as FIP1C, in a tumor-specific setting remains elusive. In this study, we used ErbB2 mouse models of human breast cancer to investigate FIP1C function in tumorigenesis. Doxycycline-induced expression of FIP1C in the MMTV-ErbB2 mouse model resulted in delayed mammary tumor progression. Conversely, targeted deletion of FIP1C in the mammary epithelium of an ErbB2 model coexpressing Cre recombinase led to accelerated tumor onset. Genetic and biochemical characterization of these FIP1C-proficient and -deficient tumor models revealed that FIP1C regulated E-cadherin (CDH1) trafficking and ZONAB (YBX3) function in Cdk4-mediated cell-cycle progression. Furthermore, we demonstrate that FIP1C promoted lysosomal degradation of ErbB2. Consistent with our findings in the mouse, the expression of FIP1C was inversely correlated with ErbB2 levels in breast cancer patients. Taken together, our findings indicate that FIP1C acts as a tumor suppressor in the context of ErbB2-positive breast cancer and may be therapeutically exploited as an alternative strategy for targeting aberrant ErbB2 expression. Cancer Res; 76(9); 2662–74. ©2016 AACR.

Published
2023

13. Supplemental Figure Legends from Rab11-FIP1C Is a Critical Negative Regulator in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Jim C. Norman, Douglas Strathdee, Lewis Chodosh, Morag Park, Gordon B. Mills, Michael Hallett, Shirley Campbell, Julie M. Livingstone, Shreya Mitra, Laura Jones, Virginie Sanguin-Gendreau, Cynthia Lavoie, Julie-Émilie Huot-Marchand, Jason Turpin, Louise Mitchell, and Pierre-Luc Boulay

Abstract

This file contains the supplemental figure legends

Published
2023

14. Supplemental Materials and Methods from Rab11-FIP1C Is a Critical Negative Regulator in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Jim C. Norman, Douglas Strathdee, Lewis Chodosh, Morag Park, Gordon B. Mills, Michael Hallett, Shirley Campbell, Julie M. Livingstone, Shreya Mitra, Laura Jones, Virginie Sanguin-Gendreau, Cynthia Lavoie, Julie-Émilie Huot-Marchand, Jason Turpin, Louise Mitchell, and Pierre-Luc Boulay

Abstract

This file contains supplemental materials and methods

Published
2023

15. Supplemental Figure 1 Schematics of the tetracycline inducible-FIP1C-MTB and inducible knock-out FIP1C mouse models from Rab11-FIP1C Is a Critical Negative Regulator in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Jim C. Norman, Douglas Strathdee, Lewis Chodosh, Morag Park, Gordon B. Mills, Michael Hallett, Shirley Campbell, Julie M. Livingstone, Shreya Mitra, Laura Jones, Virginie Sanguin-Gendreau, Cynthia Lavoie, Julie-Émilie Huot-Marchand, Jason Turpin, Louise Mitchell, and Pierre-Luc Boulay

Abstract

This Supplemental Figure 1 describes engineering of FIP1C inducible mouse model and condition knockout. Moreover, Supplemental Figure 1 provides data related to the elucidation of the physiological role of FIP1C during mamamry gland outgrowth as a supplement of Figure 1. Overall,the modulation of FIP1C levels in mammary gland does not affect normal mammary gland development.

Published
2023

23. Supplementary Figure 6 from β-Catenin Signaling Is a Critical Event in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Michael Hallett, Michael Kahn, Vincent Giguère, Robert L. Sutherland, Elena Lopez-Knowles, Sara J. Zardawi, Ewan K.A. Millar, Sandra A. O'Toole, Geneviève Deblois, Tung Bui, Virginie Sanguin-Gendreau, Robert Lesurf, and Babette Schade

Abstract

PDF file - 153K, Inhibition of b-catenin signalling impacts on proliferative and transcriptional properties of basal breast cancer line.

Published
2023

25. Supplementary Figure 1 from β-Catenin Signaling Is a Critical Event in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Michael Hallett, Michael Kahn, Vincent Giguère, Robert L. Sutherland, Elena Lopez-Knowles, Sara J. Zardawi, Ewan K.A. Millar, Sandra A. O'Toole, Geneviève Deblois, Tung Bui, Virginie Sanguin-Gendreau, Robert Lesurf, and Babette Schade

Abstract

PDF file - 139K, ErbB2KI mammary tumors express basal/myoepithelial markers and contain cells co-expressing Krt8 and Krt14.

Published
2023

26. Supplementary Figure 4 from β-Catenin Signaling Is a Critical Event in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Michael Hallett, Michael Kahn, Vincent Giguère, Robert L. Sutherland, Elena Lopez-Knowles, Sara J. Zardawi, Ewan K.A. Millar, Sandra A. O'Toole, Geneviève Deblois, Tung Bui, Virginie Sanguin-Gendreau, Robert Lesurf, and Babette Schade

Abstract

PDF file - 135K, Loss of endogenous β-catenin in ErbB2KI-derived mammary tumor cells (TM15 c10-2 and c7-2) impairs their invasion capacity in vitro.

Published
2023

28. Data from Uncoupling of PI3K from ErbB3 Impairs Mammary Gland Development but Does Not Impact on ErbB2-Induced Mammary Tumorigenesis

Author

William J. Muller, Carmen Birchmeier, Virginie Sanguin-Gendreau, Thomas Müller, and Hicham Lahlou

Abstract

The formation of ErbB2/ErbB3 heterodimers plays a critical role in ErbB2-mediated signaling in both normal mammary development and mammary tumor progression. Through 7 phosphoinositide 3-kinase (PI3K) phosphotyrosine-binding sites, ErbB3 is able to recruit PI3K and initiate the PI3K/AKT signaling pathway. To directly explore the importance of the ErbB3/PI3K pathway in mammary development and tumorigenesis, we generated a mouse model that carries a mutant ErbB3 allele lacking the seven known PI3K-binding sites (ErbB3Δ85). Mice homozygous for the ErbB3Δ85 allele exhibited an initial early growth defect and a dramatic impairment of mammary epithelial outgrowth. Although homozygous adult mice eventually recovered from the growth defect, their mammary glands continued to manifest the mammary outgrowth and lactation defects throughout their adult life. Interestingly, despite the presence of a profound mammary gland defect, all of the female ErbB3Δ85 mice developed metastatic ErbB2-induced mammary tumors secondary to mammary epithelial expression of an activated ErbB2 oncogene capable of compensatory PI3K signaling from both EGF receptor and ErbB2. Our findings therefore indicate that, although ErbB3-associated PI3K activity is critical for mammary development, it is dispensable for ErbB2-induced mammary tumor progression. Cancer Res; 72(12); 3080–90. ©2012 AACR.

Published
2023

39. Data from Distinct ErbB-2–Coupled Signaling Pathways Promote Mammary Tumors with Unique Pathologic and Transcriptional Profiles

Author

William J. Muller, Michael Hallett, Boonim L. Jung, Robert D. Cardiff, Virginie Sanguin-Gendreau, Daniela Cernea, Sonya H.L. Lam, and Babette Schade

Abstract

ErbB-2 overexpression and amplification occurs in 15% to 30% of human invasive breast carcinomas associated with poor clinical prognosis. Previously, we have shown that four ErbB-2/Neu tyrosine-autophosphorylation sites within the cytoplasmic tail of the receptor recruit distinct adaptor proteins and are sufficient to mediate transforming signals in vitro. Two of these sites, representing the growth factor receptor binding protein 2 (Grb2; Neu-YB) and the Src homology and collagen (Shc; Neu-YD) binding sites, can induce mammary tumorigenesis and metastasis. Here, we show that transgenic mice bearing the two other ErbB-2 autophosphorylation sites (Neu-YC and Neu-YE) develop metastatic mammary tumors. A detailed comparison of biological profiles among all Neu mutant mouse models revealed that Neu-YC, Neu-YD, and Neu-YE mammary tumors shared similar pathologic and transcriptional features. By contrast, the Neu-YB mouse model displayed a unique pathology with a high metastatic potential that correlates with a distinct transcriptional profile, including genes that promote malignant tumor progression such as metalloproteinases and chemokines. Furthermore, Neu-YB tumor epithelial cells showed abundant intracellular protein level of the chemokine CXCL12/SDF-1α, which may reflect the aggressive nature of this Neu mutant mouse model. Taken together, these findings indicate that activation of distinct Neu-coupled signaling pathways has an important impact on the biological behavior of Neu-induced tumors. [Cancer Res 2007;67(16):7579–88]

Published
2023

40. Supplementary Figure 3 from β-Catenin Signaling Is a Critical Event in ErbB2-Mediated Mammary Tumor Progression

Author

William J. Muller, Michael Hallett, Michael Kahn, Vincent Giguère, Robert L. Sutherland, Elena Lopez-Knowles, Sara J. Zardawi, Ewan K.A. Millar, Sandra A. O'Toole, Geneviève Deblois, Tung Bui, Virginie Sanguin-Gendreau, Robert Lesurf, and Babette Schade

Abstract

PDF file - 104K, Comparison of ErbB2KI, MMTV/NIC, and other transgenic mouse models of breast cancer.

Published
2023

43. Emergence of β1 integrin-deficient breast tumours from dormancy involves both inactivation of p53 and generation of a permissive tumour microenvironment

Author

Frédéric Ancot, Tung Bui, Virginie Sanguin-Gendreau, William J. Muller, Yu Gu, and Dongmei Zuo

Subjects
Cancer Research, Stromal cell, Breast Neoplasms, Mice, Transgenic, Biology, Senescence, Article, law.invention, Extracellular matrix, Cell growth, Mice, Breast cancer, law, Fibrosis, Genetics, medicine, Tumor Microenvironment, Animals, Humans, Fibroblast, Molecular Biology, Integrin beta1, Cancer, medicine.disease, medicine.anatomical_structure, Cancer research, Suppressor, Dormancy, Extracellular signalling molecules, Female, Tumor Suppressor Protein p53, Infiltration (medical)
Abstract

The molecular and cellular mechanisms underlying mammary tumour dormancy and cancer recurrence are unclear and remain to be elucidated. Here, we report that mammary epithelial-specific disruption of β1 integrin in a murine model of Luminal B human breast cancer drastically impairs tumour growth with proliferation block, apoptosis induction and cellular senescence. β1 integrin-deficient dormant lesions show activation of the tumour suppressor p53, and tumours that circumvent dormancy possess p53 mutation analogous to those in human disease. We further demonstrate that mammary epithelial deletion of p53 in β1 integrin-deficient mice fully rescues tumour dormancy and bypasses cellular senescence. Additionally, recurrent β1 integrin-deficient tumours exhibit fibrosis with increased cancer-associated fibroblast infiltration and extracellular matrix deposition, absent in fast-growing β1 integrin/p53-deficient lesions. Taken together, these observations argue that β1 integrin modulates p53-dependent cellular senescence resulting in tumour dormancy and that pro-tumourigenic stromal cues and intrinsic genetic mutation are required for dormancy exit.

Published
2021

44. Abstract PS17-31: Investigating the estrogen receptor Y537S mutation in transgenic models of luminal B breast cancer

Author

Cynthia Lavoie, Joshua Roccamo, William J. Muller, Dongmei Zuo, Gabriella Johnson, Zheqi Li, Steffi Oesterreich, Virginie Sanguin-Gendreau, and Adrian V. Lee

Subjects
Cancer Research, business.industry, Point mutation, Mutant, Estrogen receptor, Cancer, Context (language use), medicine.disease, Metastatic breast cancer, Breast cancer, Oncology, Cancer research, Medicine, business, Tamoxifen, medicine.drug
Abstract

Breast cancer is the most prevalent cancer in women and over two-thirds of cases express the estrogen receptor (ER). Significantly, metastatic ER positive breast cancer is the leading cause of breast cancer mortality. Despite the success of endocrine therapy to treat ER-positive breast cancers, resistance to treatment is a major problem and relapse commonly occurs though patients initially respond well to treatment. The ER Y537S mutant represents one of the most common gain-of-function mutations detected in the metastatic biopsies of patients with ER-positive breast cancer. Previous in-vitro analyses have shown that the ER Y537S mutant exhibits enhanced ER transcriptional activity by adopting a ligand-independent agonist confirmation. In our study, we seek to provide a deeper understanding of the role of this mutant by modeling the human ER Y537S mutant (ER Y541S in mice). Our lab has generated a Cre-inducible knock-in mouse model expressing the activating point mutation driven by the endogenous ER promoter, and it has been shown that when expressed ubiquitously the mutated ER leads to dramatic developmental effects. In order to further our observations in the context of endocrine resistant metastatic breast cancer, we characterize mamary tumour growth of the ER Y541S mutant in combination with luminal B models of mammary tumourigenesis. Consistent with the notion that these ER mutations occur seldom in primary tumours, preliminary data shows that tumour onset and tumour outgrowth is unaffected by the activating point mutation. When analysing tumours from both ER mutant and wildtype ER control animals, it was found that tumours with mutant ER display more basal-like cytokeratins at the RNA level via RNA sequencing and at the protein level via immunohistochemistry. This expression pattern is often associated with poorer prognosis in the clinic. Through ongoing analyses, we also seek to better understand our model through tumour regression studies (doxycycline withdrawal), treatment with tamoxifen and blocking the main source of estrogens via ovariotomies. By studying the ER Y537S mutation in models of luminal B breast cancer, we hope to investigate the factors leading to tumour recurrence and provide a deeper understanding of potential escape pathways to therapy. Citation Format: Gabriella Johnson, Joshua Roccamo, Cynthia Lavoie, Dongmei Zuo, Virginie Sanguin-Gendreau, Adrian Lee, Zheqi Li, Steffi Oesterreich, William Muller. Investigating the estrogen receptor Y537S mutation in transgenic models of luminal B breast cancer [abstract]. In: Proceedings of the 2020 San Antonio Breast Cancer Virtual Symposium; 2020 Dec 8-11; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2021;81(4 Suppl):Abstract nr PS17-31.

Published
2021

45. Physiological expression of PI3K H1047R mutation reveals its anti-metastatic potential in ErbB2-driven breast cancer

Author

Alexandra M, Simond, Tung, Bui, Dongmei, Zuo, Virginie, Sanguin-Gendreau, Trisha, Rao, Wayne A, Phillips, Robert D, Cardiff, and William J, Muller

Subjects
Phosphatidylinositol 3-Kinases, Carcinoma, Intraductal, Noninfiltrating, Class I Phosphatidylinositol 3-Kinases, Receptor, ErbB-2, Mutation, Humans, Breast Neoplasms, Female, Phosphatidylinositol 3-Kinase
Abstract

p110α is a catalytic subunit of phosphoinositide 3-kinase (PI3K), a major downstream effector of receptor tyrosine kinase ErbB2, that is amplified and overexpressed in 20-30% of breast cancers, 40% of which have an activating mutation in p110α. Despite the high frequency of PIK3CA gain-of-function mutations, their prognostic value is controversial. Here, we employ a knock-in transgenic strategy to restrict the expression of an activated form of ErbB2 and p110α kinase domain mutation (p110α

Published
2021

46. Pharmacological or genetic inhibition of iNOS prevents cachexia‐mediated muscle wasting and its associated metabolism defects

Author

Marco Bianchi, Bianca Colalillo, Amr Omer, Sergio Di Marco, William J. Muller, Jason Sadek, Imed-Eddine Gallouzi, Anne-Marie K. Tremblay, Virginie Sanguin-Gendreau, Derek T Hall, Sadek, J., Hall, D. T., Colalillo, B., Omer, A., Tremblay, A. -M. K., Sanguin-Gendreau, V., Muller, W., Di Marco, S., Bianchi, M. E., and Gallouzi, I. -E.

Subjects
Cachexia, Inflammation, Oxidative phosphorylation, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, medicine, cancer, Animals, Humans, Musculoskeletal System, Wasting, PI3K/AKT/mTOR pathway, 030304 developmental biology, 0303 health sciences, business.industry, Muscles, AMPK, Articles, medicine.disease, Muscle atrophy, Mitochondria, 3. Good health, iNOS, Muscular Atrophy, inflammation, 030220 oncology & carcinogenesis, Knockout mouse, Cancer research, Molecular Medicine, medicine.symptom, business, metabolism
Abstract

Cachexia syndrome develops in patients with diseases such as cancer and sepsis and is characterized by progressive muscle wasting. While iNOS is one of the main effectors of cachexia, its mechanism of action and whether it could be targeted for therapy remains unexplored. Here, we show that iNOS knockout mice and mice treated with the clinically tested iNOS inhibitor GW274150 are protected against muscle wasting in models of both septic and cancer cachexia. We demonstrate that iNOS triggers muscle wasting by disrupting mitochondrial content, morphology, and energy production processes such as the TCA cycle and acylcarnitine transport. Notably, iNOS inhibits oxidative phosphorylation through impairment of complexes II and IV of the electron transport chain and reduces ATP production, leading to energetic stress, activation of AMPK, suppression of mTOR, and, ultimately, muscle atrophy. Importantly, all these effects were reversed by GW274150. Therefore, our data establish how iNOS induces muscle wasting under cachectic conditions and provide a proof of principle for the repurposing of iNOS inhibitors, such as GW274150 for the treatment of cachexia., Cachexia is a condition marked by severe skeletal muscle atrophy in patients affected by diseases such as cancer or sepsis. The inflammation‐induced factor inducible nitric oxide synthase (iNOS) was found to promote muscle wasting by causing mitochondrial dysfunction and energetic stress.

Published
2021

47. Reduction of Global H3K27me3 Enhances HER2/ErbB2 Targeted Therapy

Author

William J. Muller, Morag Park, Jonathan P. Rennhack, Dongmei Zuo, Harvey W. Smith, Jarey Wang, Alison Hirukawa, Thomas F. Westbrook, Kamilia Daldoul, Matthew R. Swiatnicki, Salendra Singh, Lyndsay Harris, Vinay Varadan, Cynthia Lavoie, Virginie Sanguin-Gendreau, and Eran R. Andrechek

Subjects
0301 basic medicine, medicine.medical_treatment, Endogenous retrovirus, macromolecular substances, General Biochemistry, Genetics and Molecular Biology, Receptor tyrosine kinase, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Immune system, Interferon, Trastuzumab, Medicine, skin and connective tissue diseases, neoplasms, lcsh:QH301-705.5, biology, business.industry, EZH2, medicine.disease, 030104 developmental biology, lcsh:Biology (General), biology.protein, Cancer research, business, 030217 neurology & neurosurgery, medicine.drug
Abstract

Summary: Monoclonal antibodies (mAbs) targeting the oncogenic receptor tyrosine kinase ERBB2/HER2, such as Trastuzumab, are the standard of care therapy for breast cancers driven by ERBB2 overexpression and activation. However, a substantial proportion of patients exhibit de novo resistance. Here, by comparing matched Trastuzumab-naive and post-treatment patient samples from a neoadjuvant trial, we link resistance with elevation of H3K27me3, a repressive histone modification catalyzed by polycomb repressor complex 2 (PRC2). In ErbB2+ breast cancer models, PRC2 silences endogenous retroviruses (ERVs) to suppress anti-tumor type-I interferon (IFN) responses. In patients, elevated H3K27me3 in tumor cells following Trastuzumab treatment correlates with suppression of interferon-driven viral defense gene expression signatures and poor response. Using an immunocompetent model, we provide evidence that EZH2 inhibitors promote interferon-driven immune responses that enhance the efficacy of anti-ErbB2 mAbs, suggesting the potential clinical benefit of epigenomic reprogramming by H3K27me3 depletion in Trastuzumab-resistant disease. : Hirukawa et al. link Trastuzumab resistance in ErbB2+ breast cancers with activity of the methyltransferase EZH2, a key epigenetic regulator. By silencing retrotransposons, EZH2 suppresses type-I interferon signaling to limit immune surveillance. Retrotransposon de-repression following EZH2 inhibition triggers interferon responses and sensitizes immunocompetent in vivo models to ErbB2 antibody therapy. Keywords: ErbB2/HER2, breast cancer, Polycomb Repressor Complex 2, PRC2, epigenetics, Trastuzumab resistance, endogenous retroviruses, immune surveillance, type I interferon signaling, transcriptional silencing

Published
2019

48. An ErbB2/c-Src axis links bioenergetics with PRC2 translation to drive epigenetic reprogramming and mammary tumorigenesis

Author

Salendra Singh, Vasilios Papavasiliou, Catherine R. Dufour, Jane Beith, Ipshita Nandi, Eran R. Andrechek, Virginie Sanguin-Gendreau, Ewan K.A. Millar, Lyndsay Harris, Asier Unciti-Broceta, Mark Basik, Harvey W. Smith, Sandra A O'Toole, Carolin Temps, Vincent van Hoef, Vinay Varadan, Vincent Giguère, Cynthia Lavoie, Matthew R. Swiatnicki, Ola Larsson, Paul Savage, Alison Hirukawa, Kristofferson Tandoc, Jonathan P. Rennhack, Christina I. Selinger, Matthew Leibovitch, Neil O. Carragher, Ana Cristina Vargas Calderon, Ivan Topisirovic, Dongmei Zuo, Morag Park, Caroline Cooper, and William J. Muller

Subjects
0301 basic medicine, Carcinogenesis, Receptor, ErbB-2, General Physics and Astronomy, 02 engineering and technology, mTORC1, medicine.disease_cause, Epigenesis, Genetic, CSK Tyrosine-Protein Kinase, Mice, Adenosine Triphosphate, Breast cancer, Mice, Inbred NOD, lcsh:Science, Multidisciplinary, biology, EZH2, Polycomb Repressive Complex 2, Middle Aged, 021001 nanoscience & nanotechnology, Cancer metabolism, Mitochondria, Cell biology, src-Family Kinases, Histone methyltransferase, Female, 0210 nano-technology, PRC2, Cell signalling, Proto-oncogene tyrosine-protein kinase Src, Adult, Science, Repressor, Breast Neoplasms, Mice, Transgenic, macromolecular substances, Mechanistic Target of Rapamycin Complex 1, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Cell Line, Tumor, medicine, Animals, Humans, Enhancer of Zeste Homolog 2 Protein, Mammary Glands, Human, Cancer models, Oncogenes, General Chemistry, Oncogene ErbB2, 030104 developmental biology, Protein Biosynthesis, biology.protein, lcsh:Q
Abstract

Dysregulation of histone modifications promotes carcinogenesis by altering transcription. Breast cancers frequently overexpress the histone methyltransferase EZH2, the catalytic subunit of Polycomb Repressor Complex 2 (PRC2). However, the role of EZH2 in this setting is unclear due to the context-dependent functions of PRC2 and the heterogeneity of breast cancer. Moreover, the mechanisms underlying PRC2 overexpression in cancer are obscure. Here, using multiple models of breast cancer driven by the oncogene ErbB2, we show that the tyrosine kinase c-Src links energy sufficiency with PRC2 overexpression via control of mRNA translation. By stimulating mitochondrial ATP production, c-Src suppresses energy stress, permitting sustained activation of the mammalian/mechanistic target of rapamycin complex 1 (mTORC1), which increases the translation of mRNAs encoding the PRC2 subunits Ezh2 and Suz12. We show that Ezh2 overexpression and activity are pivotal in ErbB2-mediated mammary tumourigenesis. These results reveal the hitherto unknown c-Src/mTORC1/PRC2 axis, which is essential for ErbB2-driven carcinogenesis., Polycomb Repressor Complex 2 (PRC2) is frequently up-regulated in cancers. Here, the authors show that the tyrosine kinase c-Src stimulates mitochondrial function to signal energy sufficiency to mTORC1, increasing translation of the PRC2 subunits EZH2 and SUZ12 to support ErbB2-dependent tumours.

Published
2019

49. Rab11-FIP1C Is a Critical Negative Regulator in ErbB2-Mediated Mammary Tumor Progression

Author

Shreya Mitra, Julie Livingstone, Cynthia Lavoie, Michael Hallett, Julie Émilie Huot-Marchand, Douglas Strathdee, Gordon B. Mills, Shirley Campbell, Pierre Luc Boulay, Morag Park, Louise Mitchell, Lewis A. Chodosh, William J. Muller, Jim C. Norman, Jason Turpin, Laura M. Jones, and Virginie Sanguin-Gendreau

Subjects
0301 basic medicine, Cancer Research, Receptor, ErbB-2, Immunoblotting, Fluorescent Antibody Technique, Cre recombinase, Breast Neoplasms, Context (language use), medicine.disease_cause, Article, CDH1, Mice, 03 medical and health sciences, Breast cancer, medicine, Animals, Humans, skin and connective tissue diseases, Mice, Knockout, Mammary tumor, Oncogene, biology, business.industry, Mammary Neoplasms, Experimental, Cancer, medicine.disease, Cell Transformation, Neoplastic, 030104 developmental biology, Oncology, rab GTP-Binding Proteins, Immunology, Disease Progression, Cancer research, biology.protein, Heterografts, Female, business, Carcinogenesis
Abstract

Rab coupling protein (FIP1C), an effector of the Rab11 GTPases, including Rab25, is amplified and overexpressed in 10% to 25% of primary breast cancers and correlates with poor clinical outcome. Rab25 is also frequently silenced in triple-negative breast cancer, suggesting its ability to function as either an oncogene or a tumor suppressor, depending on the breast cancer subtype. However, the pathobiologic role of FIP family members, such as FIP1C, in a tumor-specific setting remains elusive. In this study, we used ErbB2 mouse models of human breast cancer to investigate FIP1C function in tumorigenesis. Doxycycline-induced expression of FIP1C in the MMTV-ErbB2 mouse model resulted in delayed mammary tumor progression. Conversely, targeted deletion of FIP1C in the mammary epithelium of an ErbB2 model coexpressing Cre recombinase led to accelerated tumor onset. Genetic and biochemical characterization of these FIP1C-proficient and -deficient tumor models revealed that FIP1C regulated E-cadherin (CDH1) trafficking and ZONAB (YBX3) function in Cdk4-mediated cell-cycle progression. Furthermore, we demonstrate that FIP1C promoted lysosomal degradation of ErbB2. Consistent with our findings in the mouse, the expression of FIP1C was inversely correlated with ErbB2 levels in breast cancer patients. Taken together, our findings indicate that FIP1C acts as a tumor suppressor in the context of ErbB2-positive breast cancer and may be therapeutically exploited as an alternative strategy for targeting aberrant ErbB2 expression. Cancer Res; 76(9); 2662–74. ©2016 AACR.

Published
2016

50. β-Catenin haploinsufficiency promotes mammary tumorigenesis in an ErbB2-positive basal breast cancer model

Author

William J. Muller, Robert D. Cardiff, Babette Schade, Tung Bui, Olulanu H. Aina, and Virginie Sanguin-Gendreau

Subjects
0301 basic medicine, Pathology, medicine.medical_specialty, Beta-catenin, Epithelial-Mesenchymal Transition, Lung Neoplasms, Receptor, ErbB-2, Plakoglobin, Mice, Transgenic, Haploinsufficiency, Corrections, Adherens junction, 03 medical and health sciences, Mammary tumor virus, medicine, Tumor Cells, Cultured, Animals, Epithelial–mesenchymal transition, RNA, Small Interfering, beta Catenin, Multidisciplinary, biology, Wnt signaling pathway, Mammary Neoplasms, Experimental, 030104 developmental biology, Tumor progression, Catenin, Cancer research, biology.protein, Female, gamma Catenin, Signal Transduction
Abstract

Aberrant activation of β-catenin through its activity as a transcription factor has been observed in a large proportion of human malignancies. Despite the improved understanding of the β-catenin signaling pathway over the past three decades, attempts to develop therapies targeting β-catenin remain challenging, and none of these targeted therapies have advanced to the clinic. In this study, we show that part of the challenge in antagonizing β-catenin is caused by its dual functionality as a cell adhesion molecule and a signaling molecule. In a mouse model of basal ErbB2 receptor tyrosine kinase 2 (ErbB2)-positive breast cancer (ErbB2KI), which exhibits aberrant β-catenin nuclear signaling, β-catenin haploinsufficiency induced aggressive tumor formation and metastasis by promoting the disruption of adherens junctions, dedifferentiation, and an epithelial to mesenchymal transition (EMT) transcriptional program. In contrast to the accelerated tumor onset observed in the haploid-insufficient ErbB2 tumors, deletion of both β-catenin alleles in the ErbB2KI model had only a minor impact on tumor onset that further correlated with the retention of normal adherens junctions. We further showed that retention of adherens junctional integrity was caused by the up-regulation of the closely related family member plakoglobin (γ-catenin) that maintained both adherens junctions and the activation of Wnt target genes. In contrast to the ErbB2KI basal tumor model, modulation of β-catenin levels had no appreciable impact on tumor onset in an ErbB2-driven model of luminal breast cancer [murine mammary tumor virus promoter (MMTV-NIC)]. These observations argue that the balance of junctional and nuclear β-catenin activity has a profound impact on tumor progression in this basal model of ErbB2-positive breast cancer.

Published
2017

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