Scientific Presentation

Single-Cell Multiomics Enables Superior MRD Detection and Therapeutic Insight in Myeloid Malignancies

Single-Cell Multiomics Enables Superior MRD Detection and Therapeutic Insight in Myeloid Malignancies

Andrew Owens, PhD

Description

Sensitive detection of measurable residual disease (MRD) and therapy-resistant clones is critical in myeloid malignancies, yet standard bulk assays often miss rare subpopulations or misclassify benign clonal hematopoiesis. Single-cell multiomic profiling overcomes these limitations by simultaneously capturing genotype and phenotype. This approach offers superior sensitivity over conventional methods, accurately distinguishing leukemic from preleukemic cells while mapping co-mutant subclones and clonal hierarchies. These high-resolution insights improve relapse prediction, define biomarkers, and characterize resistance mechanisms. Consequently, single-cell multiomics establishes a unified framework that strengthens both clinical monitoring and precision therapeutic development.

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A promotional graphic for Mission Bio featuring a red background and a headshot of Andrew Owens Ph.D., Field Application Scientist. The text announces a presentation titled "Single-Cell Multiomics Enables Superior MRD Detection and Therapeutic Insight in Myeloid Malignancies," which was presented at Oxford Global NextGen Omics on April 1, 2026. The Mission Bio logo is displayed in the top left corner.
Single-Cell Multiomics Enables Superior MRD Detection and Therapeutic Insight in Myeloid Malignancies Single-Cell Multiomics Enables Superior MRD Detection and Therapeutic Insight in Myeloid Malignancies

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