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ASCL1, NKX2-1, and PROX1 co-regulate subtype-specific genes in small-cell lung cancer

Karine Pozo, Rahul K. Kollipara, Demetra P. Kelenis, Kathia E. Rodarte, Morgan S. Ullrich, Xiaoyang Zhang, John D. Minna, Jane E. Johnson

2021iScience57 citationsDOIOpen Access PDF

Abstract

Lineage-defining transcription factors (LTFs) play key roles in small-cell lung cancer (SCLC) pathophysiology. Delineating the LTF-regulated genes operative in SCLC could provide a road map to identify SCLC dependencies. We integrated chromatin landscape and transcriptome analyses of patient-derived SCLC preclinical models to identify super-enhancers (SEs) and their associated genes in the ASCL1-, NEUROD1-, and POU2F3-high SCLC subtypes. We find SE signatures predict LTF-based classification of SCLC, and the SE-associated genes are enriched with those defined as common essential genes in DepMap. In addition, in ASCL1-high SCLC, we show ASCL1 complexes with NKX2-1 and PROX1 to co-regulate genes functioning in NOTCH signaling, catecholamine biosynthesis, and cell-cycle processes. Depletion of ASCL1 demonstrates it is a key dependency factor in preclinical SCLC models and directly regulates multiple DepMap-defined essential genes. We provide LTF/SE-based subtype-specific gene sets for SCLC for further therapeutic investigation.

Topics & Concepts

Transcription factorGeneBiologyTranscriptomeEnhancerChromatinCancer researchComputational biologyNotch signaling pathwayGeneticsGene expressionLung Cancer Research StudiesRNA modifications and cancerNeuroendocrine Tumor Research Advances