Seventeen-gene signature from enriched Her2/Neu mammary tumor-initiating cells predicts clinical outcome for human HER2
            <sup>+</sup>
            :ERα
            <sup>−</sup>
            breast cancer

Liu, Jeff C.; Voisin, Véronique; Bader, Gary D.; Deng, Tao; Pusztai, Lajos; Symmans, W. Fraser; Esteva, Francisco J.; Egan, Sean E.; Zacksenhaus, Eldad

doi:10.1073/pnas.1201105109

Cited by 70 publications

(84 citation statements)

References 28 publications

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“…However, the importance of Atg1 and TBK1 in HER2 þ breast cancer in which RAS is activated at a significantly lower level is largely unknown. To investigate the role of these factors in HER2 þ breast cancer, we first analyzed their expression in primary and secondary (transplanted) mammary Her2/Neu tumors (19). Both Atg1/ Ulk1 and Tbk1 were readily detected by RNA microarray (Supplementary Fig.…”

Section: Her2mentioning

confidence: 99%

“…This model was also used to identify TICs and tumorsphere-forming units (TFU; refs. 9,18), and to generate a powerful prognostic signature for HER2 þ breast cancer (19), demonstrating its utility in modeling the human disease. Here, we show that following several passages of Her2/Neu tumor cells as adherent or nonadherent cells, they become enriched for p53 mutations, and that tumorsphere but not monolayer cells maintain TICs.…”

Section: Her2mentioning

confidence: 99%

“…RNA extracted from TBK1-IItreated HCC1954 cells was subject to transcriptional profiling and global gene set enrichment analysis (GSEA; ref. 40), followed by "functional enrichment maps" to visualize the results (19,41). Lists of genes/pathways that were highly up-or downregulated are shown in Supplementary Table S4A and S4B.…”

Section: Tbk1-ii Induces Cell-cycle Arrest Not Apoptosismentioning

confidence: 99%

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shRNA Kinome Screen Identifies TBK1 as a Therapeutic Target for HER2+ Breast Cancer

et al. 2014

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Section: Her2mentioning

confidence: 99%

Section: Her2mentioning

confidence: 99%

Section: Tbk1-ii Induces Cell-cycle Arrest Not Apoptosismentioning

confidence: 99%

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shRNA Kinome Screen Identifies TBK1 as a Therapeutic Target for HER2+ Breast Cancer

et al. 2014

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“…The correlation between IL-20R1 and GAS3 genes was assessed by Pearson Correlation method with median-centered, log-2-transformed, and Robust Multi-array Average normalized microarray gene expression values. Kaplan-Meier curves and HRs were generated as described (16).…”

Section: Discussionmentioning

confidence: 99%

mda-7/IL-24 Expression Inhibits Breast Cancer through Upregulation of Growth Arrest-Specific Gene 3 (gas3) and Disruption of β1 Integrin Function

Liu

et al. 2013

Molecular Cancer Research

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Melanoma differentiation-associated gene (MDA)-7)/interleukin (IL)-24, a member of the IL-10 family of cytokines, inhibits growth of various human cancer cells, yet the underlying mechanism is largely unknown. Here, we report that mda-7/IL-24 efficiently suppresses the development of rat mammary tumors in vivo. Microarray analysis for genes differentially expressed in rat mammary tumor cells overexpressing MDA-7/IL-24 compared with those that do not express this cytokine identified growth arrest-specific gene-3 (gas3) as a target for mda-7/IL-24. Upregulation of gas3 by mda-7/IL-24 was STAT3 dependent. Induction of gas3 inhibited attachment and proliferation of tumor cells in vitro and in vivo by inhibiting the interaction of b1 integrin with fibronectin. A mutated GAS3, which is unable to bind b1 integrin, was also unable to inhibit fibronectin-mediated attachment and cell growth both in adherent and suspension cultures, suggesting that GAS3 exerts its effects through interaction with and regulation of b1 integrin. Thus, mda-7/IL-24 inhibits breast cancer growth, at least in part, through upregulation of GAS3 and disruption of b1 integrin function. Importantly, the expression of the mda-7/IL-24 receptor, IL-20R1, is highly correlated with GAS3 expression in human breast cancer (P ¼ 1.02 Â 10 À9

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“…Approximately 15%-30% of patients with stage I breast cancer and up to 40% of stage II node-negative patients will have a recurrence with local therapy alone. The disparity in outcomes within groups of similar histopathologic characteristics speaks to the incredible heterogeneity of this disease [3,4]. How to better define and identify these higher risk individuals has been an area of intense investigation for more than a decade [5].…”

Section: Introductionmentioning

confidence: 99%

Genome-Based Risk Prediction for Early Stage Breast Cancer

et al. 2014

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Tests to better characterize tumor genomic architecture are quickly becoming a standard of care in oncology. For breast cancer,the use ofgene expression assays for early stage disease is already common practice. These tests have found a place in risk stratifying the heterogeneous group of stage I-II breast cancers for recurrence, for predicting chemotherapy response, and for predicting breast cancer-related mortality. In the last 5 years, more assays have become available to the practicing oncologist. Given the rapidity with which this field has evolved, it is prudent to review the tests, their indications, and the studies from which they have been validated. We present a comprehensive review of the available gene expression assays for early stage breast cancer. We review data for several individual tests and comparative studies looking at risk prediction and cost-effectiveness.

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Seventeen-gene signature from enriched Her2/Neu mammary tumor-initiating cells predicts clinical outcome for human HER2 ⁺ :ERα ⁻ breast cancer

Cited by 70 publications

References 28 publications

shRNA Kinome Screen Identifies TBK1 as a Therapeutic Target for HER2+ Breast Cancer

shRNA Kinome Screen Identifies TBK1 as a Therapeutic Target for HER2+ Breast Cancer

mda-7/IL-24 Expression Inhibits Breast Cancer through Upregulation of Growth Arrest-Specific Gene 3 (gas3) and Disruption of β1 Integrin Function

Genome-Based Risk Prediction for Early Stage Breast Cancer

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Seventeen-gene signature from enriched Her2/Neu mammary tumor-initiating cells predicts clinical outcome for human HER2 + :ERα − breast cancer

Cited by 70 publications

References 28 publications

shRNA Kinome Screen Identifies TBK1 as a Therapeutic Target for HER2+ Breast Cancer

shRNA Kinome Screen Identifies TBK1 as a Therapeutic Target for HER2+ Breast Cancer

mda-7/IL-24 Expression Inhibits Breast Cancer through Upregulation of Growth Arrest-Specific Gene 3 (gas3) and Disruption of β1 Integrin Function

Genome-Based Risk Prediction for Early Stage Breast Cancer

Contact Info

Product

Resources

About

Seventeen-gene signature from enriched Her2/Neu mammary tumor-initiating cells predicts clinical outcome for human HER2 ⁺ :ERα ⁻ breast cancer