Microraft Array Platform for the Selection of Lymphocytes Based on Target-Cell Killing
Nancy Allbritton, Frank and Julie Jungers Dean of the College of Engineering and Professor of Bioengineering, University of Washington in Seattle
Adoptive cellular therapy (ACT) is an emerging therapeutic in which
cytotoxic T lymphocytes (CTLs) that recognize tumor cell epitopes are
introduced into patients providing immunity against the cancer cells.
For ACT to succeed, CTLs with high tumor-killing efficiency must be
identified, isolated, and characterized. Current technologies do not
enable simultaneous assay of cell behavior or killing followed by
recovery of the most efficient killer cells. A microraft array
technology that measures the ability of individual T cells to lyse a
population of target cells followed by sorting of living cells into a
multi-well plate for expansion and characterization was developed. The
microraft array platform was combined with image processing and analysis
algorithms to track and monitor killing assays over many hours.
Automated cell collection was incorporated into the platform for facile
cell collection from the array. As a proof of principle, human T cells
directed against an influenza antigen were co-cultured with antigen
presenting target cells on the microraft arrays. Target cell killing was
measured by tracking the appearance of dead cells on each microraft
over time. Microrafts with a single CTL demonstrating the greatest rate
of target cell death were identified, cloned, and influenza-antigen
reactivity confirmed. The platform is readily modified to measure the
antigen-specific activity of individual cells within a bulk CTL culture
or the cell heterogeneity within a population of gene-engineered T
cells.
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