Karen Marfurt
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Publication
Featured researches published by Karen Marfurt.
PLOS ONE | 2015
Mark Jesus M. Magbanua; Michael J. Pugia; Jin Sun Lee; Marc Jabon; Victoria Wang; Matthew A. Gubens; Karen Marfurt; Julia Pence; Harwinder Sidhu; Arejas Uzgiris; Hope S. Rugo; John W. Park
Size selection via filtration offers an antigen-independent approach for the enrichment of rare cell populations in blood of cancer patients. We evaluated the performance of a novel approach for multiplex rare cell detection in blood samples from metastatic breast (n = 19) and lung cancer patients (n = 21), and healthy controls (n = 30) using an automated microfluidic filtration and multiplex immunoassay strategy. Captured cells were enumerated after sequential staining for specific markers to identify circulating tumor cells (CTCs), circulating mesenchymal cells (CMCs), putative circulating stem cells (CSCs), and circulating endothelial cells (CECs). Preclinical validation experiments using cancer cells spiked into healthy blood demonstrated high recovery rate (mean = 85%) and reproducibility of the assay. In clinical studies, CTCs and CMCs were detected in 35% and 58% of cancer patients, respectively, and were largely absent from healthy controls (3%, p = 0.001). Mean levels of CTCs were significantly higher in breast than in lung cancer patients (p = 0.03). Fifty-three percent (53%) of cancer patients harbored putative CSCs, while none were detectable in healthy controls (p<0.0001). In contrast, CECs were observed in both cancer and control groups. Direct comparison of CellSearch® vs. our microfluidic filter method revealed moderate correlation (R2 = 0.46, kappa = 0.47). Serial blood analysis in breast cancer patients demonstrated the feasibility of monitoring circulating rare cell populations over time. Simultaneous assessment of CTCs, CMCs, CSCs and CECs may provide new tools to study mechanisms of disease progression and treatment response/resistance.
Analytical Chemistry | 2016
Zane Baird; Valentina Pirro; Stephen T. Ayrton; Adam Hollerbach; Cathleen Hanau; Karen Marfurt; Mary Foltz; R. Graham Cooks; Michael J. Pugia
A method is presented for the detection of circulating tumor cells (CTC) using mass spectrometry (MS), through reporter-ion amplification. Particles functionalized with short-chain peptides are bound to cells through antibody-antigen interactions. Selective release and MS detection of peptides is shown to detect as few as 690 cells isolated from a 10 mL blood sample. Here we present proof-of-concept results that pave the way for further investigations.
Archive | 2017
Michael J. Pugia; Julia Philip; Karen Marfurt
Archive | 2015
Michael J. Pugia; Julia Philip; Karen Marfurt; Mary Foltz
Archive | 2014
Michael J. Pugia; Karen Marfurt
Archive | 2014
Michael J. Pugia; Karen Marfurt
Archive | 2017
Michael J. Pugia; Julia Philip; Karen Marfurt
Archive | 2017
Michael J. Pugia; Julia Philip; Karen Marfurt
ASCO Meeting Abstracts | 2015
Xiaolei Qiu; Hilda Beas; Madeleine Matias; Monalisa Ray; Sunil Pandit; Harwinder Sidhu; Albert Chmura; Rong Jiang; Sebastian Kronmueller; Julia Philip; Karen Marfurt; Michael J. Pugia; Omar Perez; Steven Robert Pirie-Shepherd; Arejas Uzgiris
Archive | 2014
Michael J. Pugia; Karen Marfurt