Your search keyword '"basal subtype"' showing total 20 results

1. INHBA is a mediator of aggressive tumor behavior in HER2+ basal breast cancer

Author

Moqing Liu, Rebecca Smith, Tiera Liby, Kami Chiotti, Claudia S. López, and James E. Korkola

Subjects

HER2+ breast cancer, Lapatinib, Resistance, Basal subtype, INHBA, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Resistance to HER2-targeted therapeutics remains a significant clinical problem in HER2+ breast cancer patients with advanced disease. This may be particularly true for HER2+ patients with basal subtype disease, as recent evidence suggests they receive limited benefit from standard of care HER2-targeted therapies. Identification of drivers of resistance and aggressive disease that can be targeted clinically has the potential to impact patient outcomes. Methods We performed siRNA knockdown screens of genes differentially expressed between lapatinib-responsive and -resistant HER2+ breast cancer cells, which corresponded largely to luminal versus basal subtypes. We then validated hits in 2-d and 3-d cell culture systems. Results Knockdown of one of the genes, INHBA, significantly slowed growth and increased sensitivity to lapatinib in multiple basal HER2+ cell lines in both 2-d and 3-d cultures, but had no effect in luminal HER2+ cells. Loss of INHBA altered metabolism, eliciting a shift from glycolytic to oxidative phosphorylative metabolism, which was also associated with a decrease in tumor invasiveness. Analysis of breast cancer datasets showed that patients with HER2+ breast cancer and high levels of INHBA expression had worse outcomes than patients with low levels of INHBA expression. Conclusions Our data suggest that INHBA is associated with aggressiveness of the basal subtype of HER2+ tumors, resulting in poor response to HER2-targeted therapy and an invasive phenotype. We hypothesize that targeting this pathway could be an effective therapeutic strategy to reduce invasiveness of tumor cells and to improve therapeutic response.

Published

2022

2. Development of a Clinically Applicable NanoString-Based Gene Expression Classifier for Muscle-Invasive Bladder Cancer Molecular Stratification.

Author

Olkhov-Mitsel, Ekaterina, Yu, Yanhong, Lajkosz, Katherine, Liu, Stanley K., Vesprini, Danny, Sherman, Christopher G., and Downes, Michelle R.

Subjects

*RNA analysis, *SEQUENCE analysis, *CANCER invasiveness, *CANCER chemotherapy, *IMMUNOHISTOCHEMISTRY, *MULTIVARIATE analysis, *CANCER relapse, *GENE expression profiling, *DESCRIPTIVE statistics, *PROPORTIONAL hazards models, BLADDER tumors

Abstract

Simple Summary: Molecular subtyping of muscle-invasive bladder cancer (MIBC) via gene expression can improve therapeutic decision-making and disease prognosis. However, the currently used molecular classification tools are based on complex transcriptomic profiling methodology that hinders timely translation to clinical practice. In this study, we evaluated the NanoString nCounter platform and conventional GATA3-CK5/6 immunohistochemistry for the molecular classification of MIBC in primary care settings. The methodologies were highly concordant and allowed us to explore differences in clinicopathologic parameters and prognosis between intrinsic MIBC molecular subtypes in a cohort of 138 MIBCs. Transcriptional profiling of muscle-invasive bladder cancer (MIBC) using RNA sequencing (RNA-seq) technology has demonstrated the existence of intrinsic basal and luminal molecular subtypes that vary in their prognosis and response to therapy. However, routine use of RNA-seq in a clinical setting is restricted by cost and technical difficulties. Herein, we provide a single-sample NanoString-based seven-gene (KRT5, KRT6C, SERPINB13, UPK1A, UPK2, UPK3A and KRT20) MIBC molecular classifier that assigns a luminal and basal molecular subtype. The classifier was developed in a series of 138 chemotherapy naïve MIBCs split into training (70%) and testing (30%) datasets. Further, we validated the previously published CK5/6 and GATA3 immunohistochemical classifier which showed high concordance of 96.9% with the NanoString-based gene expression classifier. Immunohistochemistry-based molecular subtypes significantly correlated with recurrence-free survival (RFS) and disease-specific survival (DSS) in univariable (p  =  0.006 and p  =  0.011, respectively) and multivariate cox regression analysis for DSS (p = 0.032). Used sequentially, the immunohistochemical- and NanoString-based classifiers provide faster turnaround time, lower cost per sample and simpler data analysis for ease of clinical implementation in routine diagnostics. [ABSTRACT FROM AUTHOR]

Published

2022

3. Basal/squamous and mixed subtype bladder cancers present poor outcomes after neoadjuvant chemotherapy in the VESPER trial.

Author

Groeneveld CS, Pfister C, Culine S, Harter V, Krucker C, Fontugne J, Dixon V, Sirab N, Bernard-Pierrot I, de Reyniès A, Radvanyi F, and Allory Y

Abstract

Background: Neoadjuvant chemotherapy (NAC) is the standard treatment for muscle-invasive bladder cancer (MIBC), yet 40% of patients progress, emphasizing the need for biomarkers predictive for response or chemoresistance. Gene expression-based subtypes may serve as biomarkers, though which subtypes will respond, notably when it comes to the basal subtype, remains contentious., Patients and Methods: This post hoc study analyzed 300 NAC-treated patients enrolled in the GETUG/AFU VESPER trial, with transurethral diagnostic formalin-fixed paraffin-embedded tissue which underwent pathological review before being sequenced. 'Mixed' subtype was defined for tumors displaying at least two different Consensus molecular subtypes in separate regions. We evaluated the association between molecular subtypes and outcome after NAC. Tumors with remaining tissue at cystectomy (n = 83) were compared with pre-treatment tumors., Results: Cases were classified basal/squamous (Ba/Sq) (n = 84), luminal unstable (n = 57), stroma-rich (n = 53), mixed (n = 48), luminal papillary (n = 39), luminal non-specific (n = 18), and neuroendocrine-like (n = 1), with 30/48 mixed cases including a Ba/Sq component. Compared with other molecular subtypes in a multivariate Cox model, Ba/Sq (pure or mixed) patients had an increased hazard ratio (HR) of progression-free survival [HR 2.0, 95% confidence interval (CI) 1.36-3.0]. Mixed tumors were associated with decreased metabolic activity that could account for chemoresistance. Ba/Sq and mixed non-responders mostly maintained their subtype at cystectomy and have fewer myeloid dendritic cells after NAC. Tumors classified luminal papillary at transurethral resection of the urinary bladder tumor exhibited an increase in T CD4+ and macrophage signatures after NAC. Other subtypes did not show significant immune changes after NAC. Our study design relied on detailed pathological review, which precluded evaluating the mixed subtype in published datasets. Furthermore, the sample size for post-NAC analyses constrained the statistical power of these findings., Conclusions: Our findings underscore the importance of recognizing intra-tumor heterogeneity in MIBC and its role in chemoresistance associated with Ba/Sq subtype, and provide valuable insights that could help future treatment development and improve patient outcomes., (Copyright © 2024 European Society for Medical Oncology. Published by Elsevier Ltd. All rights reserved.)

Published

2024

4. INHBA is a mediator of aggressive tumor behavior in HER2+ basal breast cancer.

Author

Liu, Moqing, Smith, Rebecca, Liby, Tiera, Chiotti, Kami, López, Claudia S., and Korkola, James E.

Subjects

ONCOGENES, DRUG resistance, T-test (Statistics), DESCRIPTIVE statistics, KAPLAN-Meier estimator, COMBINED modality therapy, DATA analysis software, BIOLOGICAL assay, BREAST tumors

Abstract

Background: Resistance to HER2-targeted therapeutics remains a significant clinical problem in HER2+ breast cancer patients with advanced disease. This may be particularly true for HER2+ patients with basal subtype disease, as recent evidence suggests they receive limited benefit from standard of care HER2-targeted therapies. Identification of drivers of resistance and aggressive disease that can be targeted clinically has the potential to impact patient outcomes.Methods: We performed siRNA knockdown screens of genes differentially expressed between lapatinib-responsive and -resistant HER2+ breast cancer cells, which corresponded largely to luminal versus basal subtypes. We then validated hits in 2-d and 3-d cell culture systems.Results: Knockdown of one of the genes, INHBA, significantly slowed growth and increased sensitivity to lapatinib in multiple basal HER2+ cell lines in both 2-d and 3-d cultures, but had no effect in luminal HER2+ cells. Loss of INHBA altered metabolism, eliciting a shift from glycolytic to oxidative phosphorylative metabolism, which was also associated with a decrease in tumor invasiveness. Analysis of breast cancer datasets showed that patients with HER2+ breast cancer and high levels of INHBA expression had worse outcomes than patients with low levels of INHBA expression.Conclusions: Our data suggest that INHBA is associated with aggressiveness of the basal subtype of HER2+ tumors, resulting in poor response to HER2-targeted therapy and an invasive phenotype. We hypothesize that targeting this pathway could be an effective therapeutic strategy to reduce invasiveness of tumor cells and to improve therapeutic response. [ABSTRACT FROM AUTHOR]

Published

2022

5. Multi-Omic Data Interpretation to Repurpose Subtype Specific Drug Candidates for Breast Cancer

Author

Beste Turanli, Kubra Karagoz, Gholamreza Bidkhori, Raghu Sinha, Michael L. Gatza, Mathias Uhlen, Adil Mardinoglu, and Kazim Yalcin Arga

Subjects

breast cancer, drug repositioning, non-cancer therapeutics, repurposing, basal subtype, personalized metabolic models, Genetics, QH426-470

Abstract

Triple-negative breast cancer (TNBC), which is largely synonymous with the basal-like molecular subtype, is the 5th leading cause of cancer deaths for women in the United States. The overall prognosis for TNBC patients remains poor given that few treatment options exist; including targeted therapies (not FDA approved), and multi-agent chemotherapy as standard-of-care treatment. TNBC like other complex diseases is governed by the perturbations of the complex interaction networks thereby elucidating the underlying molecular mechanisms of this disease in the context of network principles, which have the potential to identify targets for drug development. Here, we present an integrated “omics” approach based on the use of transcriptome and interactome data to identify dynamic/active protein-protein interaction networks (PPINs) in TNBC patients. We have identified three highly connected modules, EED, DHX9, and AURKA, which are extremely activated in TNBC tumors compared to both normal tissues and other breast cancer subtypes. Based on the functional analyses, we propose that these modules are potential drivers of proliferation and, as such, should be considered candidate molecular targets for drug development or drug repositioning in TNBC. Consistent with this argument, we repurposed steroids, anti-inflammatory agents, anti-infective agents, cardiovascular agents for patients with basal-like breast cancer. Finally, we have performed essential metabolite analysis on personalized genome-scale metabolic models and found that metabolites such as sphingosine-1-phosphate and cholesterol-sulfate have utmost importance in TNBC tumor growth.

Published

2019

6. Multi-Omic Data Interpretation to Repurpose Subtype Specific Drug Candidates for Breast Cancer.

Author

Turanli, Beste, Karagoz, Kubra, Bidkhori, Gholamreza, Sinha, Raghu, Gatza, Michael L., Uhlen, Mathias, Mardinoglu, Adil, and Arga, Kazim Yalcin

Subjects

BREAST cancer, TRIPLE-negative breast cancer, THERAPEUTICS, ANTI-infective agents, METABOLITE analysis, ANTI-inflammatory agents

Abstract

Triple-negative breast cancer (TNBC), which is largely synonymous with the basal-like molecular subtype, is the 5th leading cause of cancer deaths for women in the United States. The overall prognosis for TNBC patients remains poor given that few treatment options exist; including targeted therapies (not FDA approved), and multi-agent chemotherapy as standard-of-care treatment. TNBC like other complex diseases is governed by the perturbations of the complex interaction networks thereby elucidating the underlying molecular mechanisms of this disease in the context of network principles, which have the potential to identify targets for drug development. Here, we present an integrated "omics" approach based on the use of transcriptome and interactome data to identify dynamic/active protein-protein interaction networks (PPINs) in TNBC patients. We have identified three highly connected modules, EED, DHX9, and AURKA, which are extremely activated in TNBC tumors compared to both normal tissues and other breast cancer subtypes. Based on the functional analyses, we propose that these modules are potential drivers of proliferation and, as such, should be considered candidate molecular targets for drug development or drug repositioning in TNBC. Consistent with this argument, we repurposed steroids, anti-inflammatory agents, anti-infective agents, cardiovascular agents for patients with basal-like breast cancer. Finally, we have performed essential metabolite analysis on personalized genome-scale metabolic models and found that metabolites such as sphingosine-1-phosphate and cholesterol-sulfate have utmost importance in TNBC tumor growth. [ABSTRACT FROM AUTHOR]

Published

2019

7. Breast Cancer Subtypes: Two Decades of Journey from Cell Culture to Patients

Author

Zhao, Xiangshan, Gurumurthy, Channabasavaiah Basavaraju, Malhotra, Gautam, Mirza, Sameer, Mohibi, Shakur, Bele, Aditya, Quinn, Meghan G., Band, Hamid, Band, Vimla, Rhim, Johng S., editor, and Kremer, Richard, editor

Published

2012

8. Bone Marrow Derived Mesenchymal Stem/Stromal Cells and Tumor Growth

Author

Mishra, Pravin J., Banerjee, Debabrata, and Bagley, Rebecca G., editor

Published

2010

9. Development of a Clinically Applicable NanoString-Based Gene Expression Classifier for Muscle-Invasive Bladder Cancer Molecular Stratification

Author

Ekaterina Olkhov-Mitsel, Yanhong Yu, Katherine Lajkosz, Stanley K. Liu, Danny Vesprini, Christopher G. Sherman, and Michelle R. Downes

Subjects

Cancer Research, Oncology, muscle-invasive bladder cancer, molecular classification, molecular taxonomy, luminal subtype, basal subtype, neuronal subtype, NanoString, gene expression

Abstract

Transcriptional profiling of muscle-invasive bladder cancer (MIBC) using RNA sequencing (RNA-seq) technology has demonstrated the existence of intrinsic basal and luminal molecular subtypes that vary in their prognosis and response to therapy. However, routine use of RNA-seq in a clinical setting is restricted by cost and technical difficulties. Herein, we provide a single-sample NanoString-based seven-gene (KRT5, KRT6C, SERPINB13, UPK1A, UPK2, UPK3A and KRT20) MIBC molecular classifier that assigns a luminal and basal molecular subtype. The classifier was developed in a series of 138 chemotherapy naïve MIBCs split into training (70%) and testing (30%) datasets. Further, we validated the previously published CK5/6 and GATA3 immunohistochemical classifier which showed high concordance of 96.9% with the NanoString-based gene expression classifier. Immunohistochemistry-based molecular subtypes significantly correlated with recurrence-free survival (RFS) and disease-specific survival (DSS) in univariable (p  =  0.006 and p  =  0.011, respectively) and multivariate cox regression analysis for DSS (p = 0.032). Used sequentially, the immunohistochemical- and NanoString-based classifiers provide faster turnaround time, lower cost per sample and simpler data analysis for ease of clinical implementation in routine diagnostics.

Published

2022

10. Metastasierung von Brustkrebszellen in Knochen, Lunge und Lymphknoten steigert die Resistenz gegenüber ionisierender Strahlung.

Author

Hara, Takamitsu, Iwadate, Manabu, Tachibana, Kazunoshin, Waguri, Satoshi, Takenoshita, Seiichi, and Hamada, Nobuyuki

Subjects

ANIMAL experimentation, ANIMALS, BONE tumors, BREAST tumors, CELL lines, DOSE-response relationship (Radiation), LUNG tumors, METASTASIS, MICE, RADIATION, RADIATION doses, RESEARCH funding

Abstract

Copyright of Strahlentherapie und Onkologie is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2017

11. Targeting the Urokinase Plasminogen Activator System Combined with Chemotherapy-a Potentially Novel Therapeutic Approach for Pancreatic Cancer

Author

Hosen, S. M. ; https://orcid.org/0000-0001-5789-3418

Subjects

Pancreatic Ductal Adenocarcinoma (PDAC), Pancreatic stellate cell, Urokinase Plamsminogen Activation System (uPA), PLAU, HGF-c/Met pathway, Therapeutic Strategy, Tumor Microenvironment Modulation, Orthotopic Xenograft Models, Combination Therapy, Syngeneic Model, Epithelial-Mesenchymal Transition (EMT), Cancer Stemness, Aggressive Phenotypes, Immune Suppresion, PI3K/Akt and MAPK/ERK Pathways, Extracellular Matrix Degradation, Basal Subtype, Early and Advanced Stages of PDAC, OICR, ICGC, TCGA-PAAD, anzsrc-for: 321111 Solid tumours

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is recognised as an exceptionally aggressive form of cancer, notorious for its limited treatment options, resistance to chemotherapy, and consequent poor prognosis. This dissertation comprehensively explores the potential of targeting the urokinase plasminogen activator (uPA) system, a well-documented factor in cancer progression as a therapeutic strategy in PDAC management, particularly in conjunction with the chemotherapeutic agent, Gemcitabine. Using publicly available datasets, we first demonstrated that upregulation of PLAU, the gene encoding uPA, is associated with poor prognosis and aggressive phenotypes. This upregulation is particularly prominent in the basal subtype of PDAC, which has a high mortality rate. We then focused on the effects of selective uPA inhibition with BB20-30F, both individually and in combination with Gemcitabine, using orthotopic xenograft models that mimic early and advanced stages of pancreatic cancer. The findings revealed that uPA inhibition with BB20-30F alone and in combination with Gemcitabine resulted in tumour growth and metastasis suppression, likely through inhibition of cancer cell proliferation, extracellular matrix degradation, and epithelial-mesenchymal transition (EMT). The combination treatment notably suppressed cancer stemness, a key factor in tumour initiation, recurrence, and resistance. Subsequently, the experiments were replicated in an immunocompetent syngeneic orthotopic model of advanced PDAC to account for the immune system's role in cancer progression. The results further validated the efficacy of uPA inhibition and the combination treatment, suggesting that these could modulate the tumour microenvironment to boost the anti-tumour immune response. Finally, we elucidated the underlying mechanisms behind these effects using in vitro co-culture experiments. uPA inhibition with BB2-30F, alone or combined with Gemcitabine, significantly decreased cancer cell proliferation and migration and promoted apoptosis. These effects were mediated by inhibiting Akt and ERK phosphorylation, suggesting the involvement of the PI3K/Akt and MAPK/ERK pathways. This comprehensive study underscores the therapeutic potential of targeting the uPA system in PDAC, either individually or in combination with existing treatments, thus opening new avenues for improving PDAC patient outcomes.

Published

2023

12. Molecular Taxonomy and Immune Checkpoint Therapy in Bladder Cancer.

Author

Guo CC and Czerniak B

Subjects

Humans, Biomarkers, Tumor genetics, Biomarkers, Tumor metabolism, Genomics, Urinary Bladder Neoplasms genetics, Urinary Bladder Neoplasms therapy

Abstract

Bladder cancer is a heterogeneous disease, which exhibits a wide spectrum of clinical and pathologic features. Recent genomic studies have revealed that distinct molecular alterations may underlie the diverse clinical behaviors of bladder cancer, leading to a novel molecular classification. The intrinsic molecular subtypes exhibit distinct gene expression signatures and different clinicopathologic features. Genomic alterations also underlie the development of bladder cancer histologic subtypes. Genomic characterization provides new insights to understanding the biology of bladder cancer and improves the diagnosis and treatment of this complex disease. Biomarkers can aid the selection of patients for immune checkpoint therapy., Competing Interests: Disclosure The authors have nothing to disclose., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

13. Meta-analysis of gene expression profiling reveals novel basal gene signatures in MCF-10A cells transformed with cadmium

Author

Scott H. Garrett, Brent Voels, Carley S Knudsen, Xu Dong Zhou, Sonalika Singhal, Seema Somji, Aaron A. Mehus, Kyle Wegner, Donald A. Sens, Sandeep Singhal, Swojani Shrestha, and Katrina Blommel

Subjects

0301 basic medicine, cadmium, Cancer, MCF-10A, basal subtype, Biology, Gene signature, medicine.disease, Gene expression profiling, 03 medical and health sciences, Basal (phylogenetics), 030104 developmental biology, 0302 clinical medicine, breast cancer, Oncology, Cell culture, 030220 oncology & carcinogenesis, Gene expression, Cancer research, medicine, Gene, Carcinogen, Meta-Analysis

Abstract

Cadmium (Cd2+) is an environmental toxicant and a human carcinogen. Several studies show an association of Cd2+ exposure to the development of breast cancer. Previously, we have transformed the immortalized non-tumorigenic cell line MCF-10A with Cd2+ and have demonstrated that the transformed cells have anchorage independent growth. In a separate study, we showed that transformation of the immortalized urothelial cells with the environmental carcinogen arsenite (As3+) results in an increase in expression of genes associated with the basal subtype of bladder cancer. In this study, we determined if transformation of the MCF-10A cells with Cd2+ would have a similar effect on the expression of basal genes. The results of our study indicate that there is a decrease in expression of genes associated with keratinization and cornification and this gene signature includes the genes associated with the basal subtype of breast cancer. An analysis of human breast cancer databases indicates an increased expression of this gene signature is associated with a positive correlation to patient survival whereas a reduced expression/absence of this gene signature is associated with poor patient survival. Thus, our study suggests that transformation of the MCF-10A cells with Cd2+ produces a decreased basal gene expression profile that correlates to patient outcome.

Published

2020

14. Loss of E-cadherin is not a necessity for epithelial to mesenchymal transition in human breast cancer.

Author

Hollestelle, Antoinette, Peeters, Justine, Smid, Marcel, Timmermans, Mieke, Verhoog, Leon, Westenend, Pieter, Heine, Anouk, Chan, Alan, Sieuwerts, Anieta, Wiemer, Erik, Klijn, Jan, Spek, Peter, Foekens, John, Schutte, Mieke, den Bakker, Michael, and Martens, John

Abstract

Epithelial to mesenchymal transition (EMT) is typically defined by the acquisition of a spindle cell morphology in combination with loss of E-cadherin and upregulation of mesenchymal markers. However, by studying E-cadherin inactivation in 38 human breast cancer cell lines, we noted that not all cell lines that had undergone EMT had concomitantly lost E-cadherin expression. We further investigated this discrepancy functionally and in clinical breast cancer specimens. Interestingly, reconstitution of wild-type E- cadherin cDNA in a E-cadherin negative cell line that had undergone EMT (MDA-MB-231) did not revert the spindle morphology back to an epithelial morphology. Neither were changes observed in the expression of several markers known to be involved in the EMT process. Similarly, upregulation of E-cadherin via global DNA demethylation in eleven cell lines that had undergone EMT did not induce a change in cell morphology, nor did it alter the expression of EMT markers in these cells. Next, we extracted genes differentially expressed between cell lines that had undergone EMT versus cell lines that had not undergone EMT. Caveolin-1 was identified to be an excellent marker for EMT, irrespective of E-cadherin status (specificity and sensitivity of 100 %). Consistent with our observations in the breast cancer cell lines, expression of Caveolin-1 identified a subset of basal breast cancers, particularly of metaplastic pathology, and only 50 % of these lacked E-cadherin expression. The discrepancy between E-cadherin loss and EMT was thus reproduced in clinical samples. Together, these results indicate that in human breast cancer loss of E-cadherin is not causal for EMT and even not a necessity. [ABSTRACT FROM AUTHOR]

Published

2013

15. CK8/18 expression, the basal phenotype, and family history in identifying BRCA1-associated breast cancer in the Ontario site of the Breast Cancer Family Registry.

Author

Mulligan, Anna Marie, Pinnaduwage, Dushanthi, Bane, Anita L., Bull, Shelley B., O'Malley, Frances P., and Andrulis, Irene L.

Subjects

*TUMORS, *BREAST cancer, *BREAST tumors, *BIOMARKERS, *GERM cells, *GENETIC mutation

Abstract

The article focuses on a study designed to determine the relationship of CK8/18 with BRCA1-associated tumors. The study involves 58 patients with BRCA1 germline mutations chosen from the Ontario Familial Breast Cancer Registry (OFBCR) as well as controls who are negative for BRCA mutations. The carriers and controls have been assessed and compared in terms of family history characteristics, morphologic parameters and biomarker status. Findings indicate that there is a significant reduction in CK8/18 tumor expression in BRCA1-tumors.

Published

2011

16. Metastasis of breast cancer cells to the bone, lung, and lymph nodes promotes resistance to ionizing radiation

Author

Hara, Takamitsu, Iwadate, Manabu, Tachibana, Kazunoshin, Waguri, Satoshi, Takenoshita, Seiichi, and Hamada, Nobuyuki

Published

2017

17. Meta-analysis of gene expression profiling reveals novel basal gene signatures in MCF-10A cells transformed with cadmium.

Author

Blommel K, Knudsen CS, Wegner K, Shrestha S, Singhal SK, Mehus AA, Garrett SH, Singhal S, Zhou X, Voels B, Sens DA, and Somji S

Abstract

Cadmium (Cd 2+ ) is an environmental toxicant and a human carcinogen. Several studies show an association of Cd 2+ exposure to the development of breast cancer. Previously, we have transformed the immortalized non-tumorigenic cell line MCF-10A with Cd 2+ and have demonstrated that the transformed cells have anchorage independent growth. In a separate study, we showed that transformation of the immortalized urothelial cells with the environmental carcinogen arsenite (As 3+ ) results in an increase in expression of genes associated with the basal subtype of bladder cancer. In this study, we determined if transformation of the MCF-10A cells with Cd 2+ would have a similar effect on the expression of basal genes. The results of our study indicate that there is a decrease in expression of genes associated with keratinization and cornification and this gene signature includes the genes associated with the basal subtype of breast cancer. An analysis of human breast cancer databases indicates an increased expression of this gene signature is associated with a positive correlation to patient survival whereas a reduced expression/absence of this gene signature is associated with poor patient survival. Thus, our study suggests that transformation of the MCF-10A cells with Cd 2+ produces a decreased basal gene expression profile that correlates to patient outcome., Competing Interests: CONFLICTS OF INTEREST Authors have no conflicts of interest to declare.

Published

2020

18. Morphological classification of pancreatic ductal adenocarcinoma that predicts molecular subtypes and correlates with clinical outcome.

Author

N Kalimuthu S, Wilson GW, Grant RC, Seto M, O'Kane G, Vajpeyi R, Notta F, Gallinger S, and Chetty R

Subjects

Adult, Aged, Carcinoma, Pancreatic Ductal genetics, Deep Learning, Female, Gene Expression Regulation, Neoplastic, Humans, Kaplan-Meier Estimate, Male, Middle Aged, Observer Variation, Pancreatic Neoplasms genetics, Prognosis, Reproducibility of Results, Transcriptome, Pancreatic Neoplasms, Carcinoma, Pancreatic Ductal pathology, Pancreatic Neoplasms pathology

Abstract

Introduction: Transcriptional analyses have identified several distinct molecular subtypes in pancreatic ductal adenocarcinoma (PDAC) that have prognostic and potential therapeutic significance. However, to date, an indepth, clinicomorphological correlation of these molecular subtypes has not been performed. We sought to identify specific morphological patterns to compare with known molecular subtypes, interrogate their biological significance, and furthermore reappraise the current grading system in PDAC., Design: We first assessed 86 primary, chemotherapy-naive PDAC resection specimens with matched RNA-Seq data for specific, reproducible morphological patterns. Differential expression was applied to the gene expression data using the morphological features. We next compared the differentially expressed gene signatures with previously published molecular subtypes. Overall survival (OS) was correlated with the morphological and molecular subtypes., Results: We identified four morphological patterns that segregated into two components ('gland forming' and 'non-gland forming') based on the presence/absence of well-formed glands. A morphological cut-off (≥40% 'non-gland forming') was established using RNA-Seq data, which identified two groups (A and B) with gene signatures that correlated with known molecular subtypes. There was a significant difference in OS between the groups. The morphological groups remained significantly prognostic within cancers that were moderately differentiated and classified as 'classical' using RNA-Seq., Conclusion: Our study has demonstrated that PDACs can be morphologically classified into distinct and biologically relevant categories which predict known molecular subtypes. These results provide the basis for an improved taxonomy of PDAC, which may lend itself to future treatment strategies and the development of deep learning models., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2020. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2020

19. Dysregulation of EMT Drives the Progression to Clinically Aggressive Sarcomatoid Bladder Cancer.

Author

Guo, Charles C., Majewski, Tadeusz, Zhang, Li, Yao, Hui, Bondaruk, Jolanta, Wang, Yan, Zhang, Shizhen, Wang, Ziqiao, Lee, June Goo, Lee, Sangkyou, Cogdell, David, Zhang, Miao, Wei, Peng, Grossman, H. Barton, Kamat, Ashish, Duplisea, Jonathan James, Ferguson III, James Edward, Huang, He, Dadhania, Vipulkumar, and Gao, Jianjun

Abstract

Sarcomatoid urothelial bladder cancer (SARC) displays a high propensity for distant metastasis and is associated with short survival. We report a comprehensive genomic analysis of 28 cases of SARC and 84 cases of conventional urothelial carcinoma (UC), with the TCGA cohort of 408 muscle-invasive bladder cancers serving as the reference. SARCs show a distinct mutational landscape, with enrichment of TP53 , RB1 , and PIK3CA mutations. They are related to the basal molecular subtype of conventional UCs and could be divided into epithelial-basal and more clinically aggressive mesenchymal subsets on the basis of TP63 and its target gene expression levels. Other analyses reveal that SARCs are driven by downregulation of homotypic adherence genes and dysregulation of the EMT network, and nearly half exhibit a heavily infiltrated immune phenotype. Our observations have important implications for prognostication and the development of more effective therapies for this highly lethal variant of bladder cancer. • Sarcomatoid carcinoma develops by progression of basal urothelial carcinoma • It is divided into epithelial and mesenchymal (the most aggressive) subsets • Dysregulation of cell cycle and EMT networks drives the progression • Sarcomatoid carcinoma has infiltrated immune phenotype with upregulation of PD-L1 Guo et al. report that sarcomatoid carcinoma of the bladder evolves by the progression of the basal subtype of conventional urothelial carcinoma with the enrichment of mutagenesis signature 1 and mutations of TP53 , RB1 , and PIK3CA. It is driven by the dysregulation of the EMT network and shows increased immune infiltrate with overexpression of PD-L1. [ABSTRACT FROM AUTHOR]

Published

2019

20. Matrix-producing Carcinoma as an Aggressive Triple-negative Breast Cancer: Clinicopathological Features and Response to Neoadjuvant Chemotherapy.

Author

Shimada K, Ishikawa T, Yamada A, Sugae S, Narui K, Shimizu D, Chishima T, and Endo I

Subjects

Adult, Female, Humans, Middle Aged, Antineoplastic Agents therapeutic use, Neoadjuvant Therapy, Triple Negative Breast Neoplasms drug therapy, Triple Negative Breast Neoplasms pathology

Abstract

Background: Breast matrix-producing carcinomas (MPCs) are rare, and usually triple-negative (TNBC; i.e. oestrogen receptor-, progesterone receptor-, and human epidermal growth factor receptor 2-negative). This study evaluated the clinical features, immunohistochemical profiles, and pathological response to neoadjuvant chemotherapy (NAC) of patients with MPCs., Patients and Methods: Five MPCs were identified among 247 patients with TNBC receiving anthracycline- and taxane-based NAC. Pathological response was assessed using surgical specimens., Results: All tumours were histological grade 3 according to pre-treatment core biopsies. Mean Ki-67 and p53 positivity were 65% and 90%, respectively. All tumours were TNBC, and epidermal growth factor receptor-, cytokeratin 5/6-, and vimentin-positive. Grade 3 (pathological complete response) was achieved in 0% (0/5) and 32% (77/242) of those with MPCs and with TNBCs of no specific histological type, respectively, and grade 1a (poor response) in 80% (4/5) and 13% (31/242), respectively., Conclusion: MPCs are basal-type TNBCs expressing epithelial-mesenchymal transition markers, with a poor response to standard NAC. Further studies are needed to improve the treatment of this rare but aggressive tumour., (Copyright© 2019, International Institute of Anticancer Research (Dr. George J. Delinasios), All rights reserved.)

Published

2019