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Massively Parallel Single-Cell Mitochondrial DNA Genotyping and Chromatin Profiling

About This Webinar

Natural mitochondrial DNA (mtDNA) mutations enable the inference of clonal relationships among cells. mtDNA can be profiled along with measures of cell state, but has not yet been combined with the massively parallel approaches needed to tackle the complexity of human tissue. Here, we introduce a high-throughput, droplet-based mitochondrial single-cell assay for transposase-accessible chromatin with sequencing (scATAC-seq), a method that combines high-confidence mtDNA mutation calling in thousands of single cells with their concomitant high-quality accessible chromatin profile. This enables the inference of mtDNA heteroplasmy, clonal relationships, cell state and accessible chromatin variation in individual cells. We reveal single-cell variation in heteroplasmy of a pathologic mtDNA variants, which we associate with intra-individual chromatin variability, cell type specificity, and clonal evolution. We clonally trace thousands of cells from cancers, linking epigenomic variability to subclonal evolution, and infer cellular dynamics of differentiating hematopoietic cells in vitro and in vivo. Taken together, our approach enables the study of cellular population dynamics and clonal properties in vivo.

Who can view: Everyone
Webinar Price: Free
Featured Presenters
Webinar hosting presenter
Stanford Science Fellow, Genetics and Pathology, Stanford School of Medicine
Caleb Lareau is currently a Stanford Science Fellow in the School of Medicine at Stanford University. He completed his PhD at Harvard Medical School where he co-lead the development of multiple new single-cell approaches for measuring cell state and lineage. Caleb’s current research focuses on enhancing and applying multi-modal single cell technologies to understand fundamental properties of clonal cell dynamics in health and disease.
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