Integrating Flow Cytometry with Next Generation Sequencing to Find Determinants of Protein Secretion
Richard James, Principal Investigator and Associate Professor, Seattle Children’s Research Institute and University of Washington
Protein secretion drives many functions in vivo; however, methods to
link secretions with surface markers and transcriptomes have been
lacking. By accumulating secretions close to secreting cells held within
cavity-containing hydrogel nanovials, we demonstrate workflows to
analyze the amount of IgG secreted from single human antibody-secreting
cells and link this information to surface marker expression and
transcriptional profiles from the same cells. Measurements using flow
cytometry and imaging flow cytometry corroborated an association between
levels of IgG secretion and CD138 expression. Using
oligonucleotide-labeled antibodies and droplet-based sequencing, we show
that pathways encoding protein localization to the endoplasmic
reticulum, NADH complex assembly, and mitochondrial respiration were
most associated with high IgG secretion. Altogether, this method links
secretion information to cell surface and single-cell sequencing
information (SEC-seq) and enables exploration of links between genome
and secretory function, laying the foundation for numerous discoveries
in immunology, stem cell biology, and beyond.
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