High-Throughput Proteomic Profiling to Evaluate Differentiation Syndrome With Menin Inhibition

Key Points

Differentiation syndrome is linked to menin inhibition, with notable inflammatory protein changes observed during treatment.
Dynamic changes in soluble protein levels were identified using a nucleic acid-linked immuno-sandwich assay, a novel high-throughput technique.
The analysis was applied to pediatric AML patients, revealing significant insights into inflammatory responses related to menin inhibitors.
Insights gained may lead to better monitoring and management strategies for differentiation syndrome in AML therapy.

Abstract

High-throughput proteomic profiling provides a comprehensive analysis of systemic cancer effects and tumor microenvironment interactions. Characterizing soluble proteins driving inflammation in acute myeloid leukemia (AML) offers insight into inflammatory diseases like differentiation syndrome related to AML therapies like menin inhibitors. We present our application of nucleic acid-linked immuno-sandwich assay, a novel technology leveraging next-generation sequencing for high-throughput, ultrasensitive characterization of secreted inflammatory proteins in plasma or serum. Here, we report its use to identify dynamic soluble protein changes during treatment and at the time of suspected differentiation syndrome in pediatric AML patients treated with the menin inhibitor revumenib (NCT04065399 and NCT05360160).

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High-Throughput Proteomic Profiling to Evaluate Differentiation Syndrome With Menin Inhibition

Key Points

Abstract

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