PO.CL06.03 · 临床研究

Disrupting the lipid-ETV6 axis: A therapeutic vulnerability in Ewing sarcoma

编号 7878 展板 9 时间 4/22 09:00–12:00 区域 Section 47 主讲 Yuan Gao, PhD
分会场 Targeted Therapies, Predispositions, and Survivorship in Pediatric Cancers
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作者与单位

Yuan Gao, Hang Zhao

Pharmacology, Case Western Reserve University School of Medicine, Cleveland, OH

摘要 Abstract

Ewing sarcoma is a transcriptionally driven pediatric cancer with few targetable dependencies. Through a gain-of-function metabolic screen, we discovered that Ewing sarcoma cells exhibit lineage-specific hypersensitivity to activation of glycerophospholipid metabolism. Mechanistic studies revealed that phosphatidic acid (PA), a central lipid signaling molecule, directly binds to the transcriptional repressor ETV6, an essential and selective dependency in Ewing sarcoma. PA binding disrupts ETV6 oligomerization and chromatin occupancy, leading to de-repression of its target genes. We further mapped this interaction to a unique five-amino acid motif in the ETV6 ETS domain and generated lipid-insensitive mutants that retain DNA binding but resist PA-induced inactivation. CRISPR activation of endogenous PA-producing enzymes phenocopied the effects of exogenous PA, supporting a direct role for lipid signaling in modulating ETV6 function and tumor cell viability. These findings define a previously unrecognized lipid-sensitive transcriptional state in Ewing sarcoma and reveal the ETV6-PA axis as a novel therapeutic target.
利益披露 Disclosure
Y. Gao, None.. H. Zhao, None.

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