Skip NavigationSkip to Content
Return Return to Search Results

Clinical Evolution of Epithelial-Mesenchymal Transition in Human Carcinomas

  1. Author:
    Navas, Tony
    Kinders,Robert
    Lawrence, Scott M
    Ferry-Galow,Katherine
    Borgel, Suzanne
    Hollingshead, Melinda G
    Srivastava,Apurva
    Alcoser, Sergio Y
    Makhlouf, Hala R [ORCID]
    Chuaqui, Rodrigo
    Wilsker,Deborah
    Konaté, Mariam M
    Miller, Sarah B
    Voth,Andrea
    Chen,Li
    Vilimas,Tomas
    Subramanian, Jyothi
    Rubinstein, Lawrence
    Kummar, Shivaani
    Chen, Alice P [ORCID]
    Bottaro, Donald P [ORCID]
    Doroshow, James H
    Parchment,Ralph

  2. Author Address

    Clinical Pharmacodynamic Biomarkers Program, Frederick National Laboratory for Cancer Research, NCI at Frederick., Clinical Pharmacodynamics Biomarker Program, Frederick National Laboratory of Cancer Research, NCI at Frederick., CGR, Leidos Biomedical Research Inc., Clinical Pharmacodynamics Biomarker Program, Frederick National Laboratory for Cancer Research, NCI at Frederick., Developmental Therapeutics Program, SAIC-Frederick Inc., Biological Testing Branch, National Cancer Institute., Applied/Developmental Research Directorate, Frederick National Laboratory of Cancer Research, Leidos Biomedical Research, Inc., BTB, National Cancer Institute., Cancer Diagnosis Program, Division of Cancer Treatment and Diagnosis, National Cancer Institute., Clinical Pharmacodynamics Biomarkers Program, Frederick National Laboratory for Cancer Research, NCI at Frederick., Division of Cancer Treatment and Diagnosis, National Cancer Insitute., Clinical Pharmacodynamic Biomarkers Program, Frederick National Laboratory for Cancer Research., Molecular Characterization Lab, Frederick National Laboratory for Cancer Research., Biometric Research Program, National Institutes of Health, National Cancer Institute., Division of Oncology, Stanford University School of Medicine., Urologic Oncology Branch, National Cancer Institute., Clinical Pharmacodynamic Biomarkers Program, Frederick National Laboratory for Cancer Research, NCI at Frederick parchmentr@mail.nih.gov.,
    1. Year: 2020
    2. Date: JAN 15
    3. Epub Date: 2019 11 15
  2. Journal: Cancer research
    1. 80
    2. 2
    3. Pages: 304-318
  4. Type of Article: Article
  5. ISSN: 0008-5472
  1. Abstract:

    The significance of the phenotypic plasticity afforded by epithelial-mesenchymal transition (EMT) for cancer progression and drug resistance remains to be fully elucidated in the clinic. We evaluated epithelial-mesenchymal phenotypic characteristics across a range of tumor histologies using a validated, high-resolution digital microscopic immunofluorescence assay (IFA) that incorporates beta-catenin detection and cellular morphology to delineate carcinoma cells from stromal fibroblasts and that quantitates the individual and colocalized expression of the epithelial marker E-cadherin (E) and the mesenchymal marker vimentin (V) at subcellular resolution ("EMT-IFA"). We report the discovery of beta-catenin(+) cancer cells that coexpress E-cadherin and vimentin in core-needle biopsies from patients with various advanced metastatic carcinomas, wherein these cells are transitioning between strongly epithelial and strongly mesenchymal-like phenotypes. Treatment of carcinoma models with anticancer drugs that differ in their mechanism of action (the tyrosine kinase inhibitor pazopanib in MKN45 gastric carcinoma xenografts and the combination of tubulin-targeting agent paclitaxel with the BCR-ABL inhibitor nilotinib in MDA-MB-468 breast cancer xenografts) caused changes in the tumor epithelial-mesenchymal character. Moreover, the appearance of partial EMT or mesenchymal-like carcinoma cells in MDA-MB-468 tumors treated with the paclitaxel-nilotinib combination resulted in upregulation of cancer stem cell (CSC) markers and susceptibility to FAK inhibitor. A metastatic prostate cancer patient treated with the PARP inhibitor talazoparib exhibited similar CSC marker upregulation. Therefore, the phenotypic plasticity conferred on carcinoma cells by EMT allows for rapid adaptation to cytotoxic or molecularly targeted therapy and could create a form of acquired drug resistance that is transient in nature. Significance: Despite the role of EMT in metastasis and drug resistance, no standardized assessment of EMT phenotypic heterogeneity in human carcinomas exists; the EMT-IFA allows for clinical monitoring of tumor adaptation to therapy.

    See More

  1. Keywords:

External Sources

  1. View Full Text
  2. DOI: 10.1158/0008-5472.CAN-18-3539
  3. PMID: 31732654
  4. View record in Web of Science®
  5. WOS: 000508480100016
  6. PII : 0008-5472.CAN-18-3539

Library Notes

  1. Fiscal Year: FY2019-2020
NCI at Frederick

You are leaving a government website.

This external link provides additional information that is consistent with the intended purpose of this site. The government cannot attest to the accuracy of a non-federal site.

Linking to a non-federal site does not constitute an endorsement by this institution or any of its employees of the sponsors or the information and products presented on the site. You will be subject to the destination site's privacy policy when you follow the link.

ContinueCancel