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Tumour suppressor EP300, a modulator of paclitaxel resistance and stemness, is downregulated in metaplastic breast cancer

by Min, Haoxiang , Hu, Yunhui , Asaduzzaman, Muhammad , Coombes, R. Charles , Lam, Eric W.-F. , Gallon, John , Raguz, Selina , Constantinou, Stephanie , Singh, Poonam , Lin, Meng-Lay , Shousha, Sami , Yagüe, Ernesto , Ali, Simak

in Agar / Analysis / Antineoplastic agents / Apoptosis / ATP Binding Cassette Transporter, Subfamily G, Member 2 - genetics / Breast cancer / Breast Neoplasms - drug therapy / Breast Neoplasms - genetics / Breast Neoplasms - pathology / Calpain - genetics / Cancer research / Carcinoembryonic Antigen - genetics / CD44 antigen / Cell Plasticity - genetics / Cell proliferation / Cell Proliferation - genetics / Colon / Colon cancer / Colorectal cancer / Cytoskeleton / DNA microarrays / Drug resistance / Drug Resistance, Neoplasm - genetics / E-cadherin / E1A-Associated p300 Protein - genetics / Epithelial cells / Female / Gene expression / Gene Expression Regulation, Neoplastic - drug effects / Genes / GPI-Linked Proteins - genetics / Humans / Immunohistochemistry / Lentivirus - genetics / Mammary gland / MCF-7 Cells / Medicine / Medicine & Public Health / Mesenchyme / Metastases / Neoplasm Metastasis / Neoplasm Proteins - genetics / Neoplastic Stem Cells - metabolism / Neoplastic Stem Cells - pathology / Oncology / Paclitaxel / Paclitaxel - administration & dosage / Physiological aspects / Preclinical Study / Proto-Oncogene Proteins c-bcl-2 - genetics / Stem cells / Transcription / Transforming Growth Factor beta2 - genetics / Tumors

2017

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Tumour suppressor EP300, a modulator of paclitaxel resistance and stemness, is downregulated in metaplastic breast cancer

2017

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Tumour suppressor EP300, a modulator of paclitaxel resistance and stemness, is downregulated in metaplastic breast cancer

2017

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Journal Article

Tumour suppressor EP300, a modulator of paclitaxel resistance and stemness, is downregulated in metaplastic breast cancer

Min, Haoxiang,

Hu, Yunhui,

Asaduzzaman, Muhammad,

Coombes, R. Charles,

Lam, Eric W.-F.,

Gallon, John,

Raguz, Selina,

Constantinou, Stephanie,

Singh, Poonam,

Lin, Meng-Lay,

Shousha, Sami,

Yagüe, Ernesto,

Ali, Simak

2017

Overview

Purpose We have previously described a novel pathway controlling drug resistance, epithelial-to-mesenchymal transition (EMT) and stemness in breast cancer cells. Upstream in the pathway, three miRs (miR-106b, miR-93 and miR-25) target EP300, a transcriptional activator of E-cadherin. Upregulation of these miRs leads to the downregulation of EP300 and E-cadherin with initiation of an EMT. However, miRs regulate the expression of many genes, and the contribution to EMT by miR targets other than EP300 cannot be ruled out. Methods We used lentiviruses expressing EP300-targeting shRNA to downregulate its expression in MCF-7 cells as well as an EP300 -knocked-out colon carcinoma cell line. An EP300-expression plasmid was used to upregulate its expression in basal-like CAL51 and MDA-MB-231 breast cancer cells. Drug resistance was determined by short-term proliferation and long-term colony formation assays. Stemness was determined by tumour sphere formation in both soft agar and liquid cultures as well as by the expression of CD44/CD24/ALDH markers. Gene expression microarray analysis was performed in MCF-7 cells lacking EP300. EP300 expression was analysed by immunohistochemistry in 17 samples of metaplastic breast cancer. Results Cells lacking EP300 became more resistant to paclitaxel whereas EP300 overexpression increased their sensitivity to the drug. Expression of cancer stem cell markers, as well as tumour sphere formation, was also increased in EP300-depleted cells, and was diminished in EP300-overexpressing cells. The EP300-regulated gene signature highlighted genes associated with adhesion ( CEACAM5 ), cytoskeletal remodelling ( CAPN9 ), stemness ( ABCG2 ), apoptosis ( BCL2 ) and metastasis ( TGFB2 ). Some genes in this signature were also validated in a previously generated EP300-depleted model of breast cancer using minimally transformed mammary epithelial cells. Importantly, two key genes in apoptosis and stemness, BCL2 and ABCG2 , were also upregulated in EP300-knockout colon carcinoma cells and their paclitaxel-resistant derivatives. Immunohistochemical analysis demonstrated that EP300 expression was low in metaplastic breast cancer, a rare, but aggressive form of the disease with poor prognosis that is characterized by morphological and physiological features of EMT. Conclusions EP300 plays a major role in the reprogramming events, leading to a more malignant phenotype with the acquisition of drug resistance and cell plasticity, a characteristic of metaplastic breast cancer.

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Publisher

Springer US,Springer,Springer Nature B.V

Subject

Agar

/ Analysis

/ Antineoplastic agents

/ Apoptosis

/ ATP Binding Cassette Transporter, Subfamily G, Member 2 - genetics

/ Breast cancer

/ Breast Neoplasms - drug therapy