4.8 Article

Optofluidic real-time cell sorter for longitudinal CTC studies in mouse models of cancer

出版社

NATL ACAD SCIENCES
DOI: 10.1073/pnas.1814102116

关键词

microfluidic; GEMM; circulating tumor cells; metastasis; single-cell RNA-Seq

资金

  1. Thomas and Sarah Kailath Fellowship
  2. A*STAR (Agency for Science, Technology and Research, Singapore) National Science Scholarship
  3. Lustgarten Foundation
  4. Ludwig Center at MIT
  5. Stand Up To Cancer
  6. Howard Hughes Medical Institute (HHMI) Faculty Scholars Award
  7. HHMI Investigator Program
  8. Searle Scholars Program
  9. Beckman Young Investigator Program
  10. NIH [1R01 CA184956, 5U24A1118672, 1U54CA217377, 1R33CA202820, 2U19AI089992, 1R01HL134539, 2RM1HG006193, 2P01A1039671]
  11. NIH New Innovator Award [1DP2GM119419]
  12. Pew-Stewart Scholars
  13. Sloan Fellowship in Chemistry
  14. Koch Institute from the National Cancer Institute [P30-CA14051]

向作者/读者索取更多资源

Circulating tumor cells (CTCs) play a fundamental role in cancer progression. However, in mice, limited blood volume and the rarity of CTCs in the bloodstream preclude longitudinal, in-depth studies of these cells using existing liquid biopsy techniques. Here, we present an optofluidic system that continuously collects fluorescently labeled CTCs from a genetically engineered mouse model (GEMM) for several hours per day over multiple days or weeks. The system is based on a microfluidic cell sorting chip connected serially to an unanesthetized mouse via an implanted arteriovenous shunt. Pneumatically controlled microfluidic valves capture CTCs as they flow through the device, and CTC-depleted blood is returned back to the mouse via the shunt. To demonstrate the utility of our system, we profile CTCs isolated longitudinally from animals over 4 days of treatment with the BET inhibitor JQ1 using single-cell RNA sequencing (scRNA-Seq) and show that our approach eliminates potential biases driven by intermouse heterogeneity that can occur when CTCs are collected across different mice. The CTC isolation and sorting technology presented here provides a research tool to help reveal details of how CTCs evolve over time, allowing studies to credential changes in CTCs as biomarkers of drug response and facilitating future studies to understand the role of CTCs in metastasis.

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