Publications by authors named "Jenna Kitz"

Article Synopsis
  • * In this study, researchers knocked down the Zeb1 transcription factor in PC-3 prostate cancer cells, which showed a p-EMT phenotype with increased invasion, migration, and changes in cellular markers, demonstrating the significance of p-EMT in aggressive cancer behavior.
  • * Treatment with the de-methylating drug 5-azacytidine reduced the aggressive p-EMT characteristics, and DNA methylation analysis identified 10 potential targets,
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Circulating tumor cells (CTCs) present an opportunity to detect/monitor metastasis throughout disease progression. The CellSearch® is currently the only FDA-approved technology for CTC detection in patients. The main limitation of this system is its reliance on epithelial markers for CTC isolation/enumeration, which reduces its ability to detect more aggressive mesenchymal CTCs that are generated during metastasis via epithelial-to-mesenchymal transition (EMT).

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The majority of cancer deaths occur because of metastasis since current therapies are largely non-curative in the metastatic setting. The use of in vivo preclinical mouse models for assessing metastasis is, therefore, critical for developing effective new cancer biomarkers and therapies. Although a number of quantitative tools have been previously developed to study in vivo metastasis, the detection and quantification of rare metastatic events has remained challenging.

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Claudin-low breast cancer is a relatively rare breast cancer subtype. These cancers are typically ER-/PR-/HER2- and express high levels of mesenchymal genes as well as genes associated with inflammation, angiogenesis and stem cell function. In addition to alterations in gene expression, it was recently demonstrated that claudin-low breast cancers express very low levels of the miR-200 family of miRNAs.

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