Ascites analysis by a microfluidic chip allows tumor-cell profiling

Author(s)

Peterson, Vanessa M.; Castro, Cesar M.; Chung, Jaehoon; Miller, Nathan C.; Ullal, Adeeti V.; Castano, Maria D.; Penson, Richard T.; Lee, Hakho; Birrer, Michael J.; Weissleder, Ralph; ... Show more Show less

Abstract

Ascites tumor cells (ATCs) represent a potentially valuable source of cells for monitoring treatment of ovarian cancer as it would obviate the need for more invasive surgical biopsies. The ability to perform longitudinal testing of ascites in a point-of-care setting could significantly impact clinical trials, drug development, and clinical care. Here, we developed a microfluidic chip platform to enrich ATCs from highly heterogeneous peritoneal fluid and then perform molecular analyses on these cells. We evaluated 85 putative ovarian cancer protein markers and found that nearly two-thirds were either nonspecific for malignant disease or had low abundance. Using four of the most promising markers, we prospectively studied 47 patients (33 ovarian cancer and 14 control). We show that a marker set (ATC[subscript dx]) can sensitively and specifically map ATC numbers and, through its reliable enrichment, facilitate additional treatment-response measurements related to proliferation, protein translation, or pathway inhibition.

Date issued

2013-12

URI

http://hdl.handle.net/1721.1/89088

Department

Massachusetts Institute of Technology. Institute for Medical Engineering & Science
Harvard University--MIT Division of Health Sciences and Technology

Journal

Proceedings of the National Academy of Sciences

Publisher

National Academy of Sciences (U.S.)

Citation

Peterson, V. M., C. M. Castro, J. Chung, N. C. Miller, A. V. Ullal, M. D. Castano, R. T. Penson, H. Lee, M. J. Birrer, and R. Weissleder. “Ascites Analysis by a Microfluidic Chip Allows Tumor-Cell Profiling.” Proceedings of the National Academy of Sciences 110, no. 51 (December 2, 2013): E4978–E4986.

Version: Final published version

ISSN

0027-8424

1091-6490