ShcA signalling is essential for tumour progression in mouse models of human breast cancer

Ursini‐Siegel, Josie; Hardy, W. Rod; Zuo, Dongmei; Lam, Sonya H.L.; Sanguin-Gendreau, Virginie; Cardiff, Robert D.; Pawson, Tony; Muller, William J.

doi:10.1038/emboj.2008.22

Cited by 132 publications

(222 citation statements)

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“…We have previously shown that the MMTV/NIC strain develops metastatic mammary tumors with comparable latency to other MMTV/activated ErbB2 strains (Ursini- Siegel et al, 2008). Because NIC transgene also co-express Cre recombinase due to the presence of internal ribosome entry site (IRES), mammary epithelial cells expressing activated ErbB2 will excise the conditional ILK allele (Ursini- Siegel et al, 2008). Thus the coupled expression of ErbB2 and Cre recombinase precludes the possibility of obtaining ErbB2-expressing Crenegative 'escapee' populations that could possibly contribute to the tumor.…”

Section: Resultsmentioning

confidence: 95%

“…We have previously shown that ectopic expression of ILK results in induction of metastatic mammary tumors that possess the hallmarks of an EMT phenotype (White et al, 2001). Using an ErbB2 transgenic model (Ursini- Siegel et al, 2008), we have shown that mammary epithelial disruption of ILK resulted in a dramatic delay in mammary tumor induction. Analyses of premalignant ErbB2-expressing mammary epithelium lacking ILK function has revealed that this block in ErbB2 tumor induction is associated with profound block in epithelial proliferation (Figure 2d, Supplementary Figure S2).…”

Section: Discussionmentioning

confidence: 94%

“…To determine if ILK expression is required for the induction of mammary tumors in these MMTV/activated ErbB2 transgenic mice (NIC strain), we introduced the conditional ILK alleles into this strain. We have previously shown that the MMTV/NIC strain develops metastatic mammary tumors with comparable latency to other MMTV/activated ErbB2 strains (Ursini- Siegel et al, 2008). Because NIC transgene also co-express Cre recombinase due to the presence of internal ribosome entry site (IRES), mammary epithelial cells expressing activated ErbB2 will excise the conditional ILK allele (Ursini- Siegel et al, 2008).…”

Section: Resultsmentioning

confidence: 99%

“…Thus the coupled expression of ErbB2 and Cre recombinase precludes the possibility of obtaining ErbB2-expressing Crenegative 'escapee' populations that could possibly contribute to the tumor. Indeed, we successfully showed that this approach results in complete ablation of targeted allele in NIC mice harboring either Stat3 or ShcA conditional alleles (Ursini- Siegel et al, 2008;Ranger et al, 2009).…”

Section: Resultsmentioning

confidence: 99%

“…To investigate the role of ILK in ErbB2 tumor progression, we have assessed the effect of the targeted disruption of ILK in mammary epithelium on both normal mammary development and ErbB2 tumor progression. To accomplish this, we have interbred mice bearing a conditional ILK allele (Terpstra et al, 2003) to separate transgenic mice co-expressing ErbB2 and Cre recombinase in the mammary epithelium (Ursini- Siegel et al, 2008). Although mammary epithelial disruption of ILK had little impact on normal mammary gland development (Supplementary Figure S1A), loss of ILK function in ErbB2-expressing epithelium resulted in a profound proliferative block that was correlated with a dramatic impact in ErbB2 tumor onset and penetrance.…”

Section: Introductionmentioning

confidence: 99%

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Integrin-linked kinase has a critical role in ErbB2 mammary tumor progression: implications for human breast cancer

et al. 2010

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Elevated expression of the integrin-linked kinase (ILK) has been observed in a variety of cancers and has been further correlated with poor clinical outcome. Here, we show that mammary epithelial disruption of ILK results in a profound block in mammary tumor induction. Consistent with these observations, inhibition of ILK function in ErbB2-expressing cells with small molecule inhibitor or RNA interference resulted in profound block in their in vitro invasive properties due to the induction of apoptotic cell death. The rare ILK-deficient tumors that eventually arose overcame this block in tumor induction by an upregulation of ErB3 phosphorylation. These observations provide direct evidence that ILK has a critical role in the initiation phase of ErbB2 tumor induction.

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Section: Resultsmentioning

confidence: 95%

Section: Discussionmentioning

confidence: 94%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Integrin-linked kinase has a critical role in ErbB2 mammary tumor progression: implications for human breast cancer

et al. 2010

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In vivo evidence supporting a metastasis suppressor role for Stard13 (Dlc2) in ErbB2 (Neu) oncogene induced mouse mammary tumors

Basak

Leslie

Dillon

et al. 2017

Genes Chromosomes & Cancer

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Overexpression of dominant oncogenes and the loss of tumor suppressor genes are basic genetic events in the acquisition of the malignant phenotype. The erb-b2 receptor tyrosine kinase 2 (ERBB-2) proto-oncogene is overexpressed in 20-30% of human breast cancers. The StAR related lipid transfer domain containing 13 gene (STARD13), also known as Deleted in Liver Cancer-2 (DLC-2), maps to chromosome band 13q12.3 and is frequently downregulated in human cancers, including 72% of breast cancers. It encodes a RhoGAP protein with sterile α motif (SAM) and StAR-related lipid transfer (START) domains. The objective of this study was to determine if loss of Stard13 plays a role in mammary tumor progression using transgenic mice expressing the activated ErbB-2 (Neu) oncogene and Cre recombinase (NIC) in mammary epithelium under transcriptional control of the murine mammary tumor virus (MMTV) promoter (MMTV-NIC). These mice were crossed with a conditional Stard13 knockout mouse (floxed exon 3), resulting in simultaneous Neu expression and Stard13 deletion, specifically in the mammary epithelium. We found that loss of Stard13 did not alter tumor growth nor significantly modify overall survival and tumor free survival. However, there was an increase in the total number of lung metastases in the Stard13 heterozygous or homozygous mice compared with the parental MMTV-NIC strain. Altogether our results indicate that Stard13 acts as a metastasis suppressor rather than a tumor suppressor gene, in Neu oncogene induced mammary tumorigenesis.

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The Tyrosine Kinome Dictates Breast Cancer Heterogeneity and Therapeutic Responsiveness

Siegel

Ursini‐Siegel

2016

J of Cellular Biochemistry

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Phospho-tyrosine signaling networks control numerous biological processes including cellular differentiation, cell growth and survival, motility, and invasion. Aberrant regulation of the tyrosine kinome is a hallmark of malignancy and influences all stages of breast cancer progression, from initiation to the development of metastatic disease. The success of specific tyrosine kinase inhibitors strongly validates the clinical relevance of tyrosine phosphorylation networks in breast cancer pathology. However, a significant degree of redundancy exists within the tyrosine kinome. Numerous receptor and cytoplasmic tyrosine kinases converge on a core set of signaling regulators, including adaptor proteins and tyrosine phosphatases, to amplify pro-tumorigenic signal transduction pathways. Mutational activation, amplification, or overexpression of one or more components of the tyrosine kinome represents key contributing events responsible for the tumor heterogeneity that is observed in breast cancers. It is this molecular heterogeneity that has become the most significant barrier to durable clinical responses due to the development of therapeutic resistance. This review focuses on recent literature that supports a prominent role for specific components of the tyrosine kinome in the emergence of unique breast cancer subtypes and in shaping breast cancer plasticity, sensitivity to targeted therapies, and the eventual emergence of acquired resistance. J. Cell. Biochem. 117: 1971-1990, 2016. © 2016 Wiley Periodicals, Inc.

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ShcA signalling is essential for tumour progression in mouse models of human breast cancer

Cited by 132 publications

References 42 publications

Integrin-linked kinase has a critical role in ErbB2 mammary tumor progression: implications for human breast cancer

Integrin-linked kinase has a critical role in ErbB2 mammary tumor progression: implications for human breast cancer

In vivo evidence supporting a metastasis suppressor role for Stard13 (Dlc2) in ErbB2 (Neu) oncogene induced mouse mammary tumors

The Tyrosine Kinome Dictates Breast Cancer Heterogeneity and Therapeutic Responsiveness

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