LBPO.TB02 · 肿瘤生物学 · Late-Breaking

Y chromosome loss drives cellular plasticity through single-cell epigenetic and transcriptional heterogeneity in lung adenocarcinoma

海报缩略图:Y chromosome loss drives cellular plasticity through single-cell epigenetic and transcriptional heterogeneity in lung adenocarcinoma
编号 LB309 展板 9 时间 4/21 09:00–12:00 区域 Section 55 主讲 Kathleen Schlueter, BS;MS
分会场 Late-Breaking Research: Tumor Biology 2
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作者与单位

Kathleen Schlüter1, Mei-Ju May Chen2, Gizem Altun1, Sergio Manzano Sanchez1, Dung-Chi Wu3, Nan Zhang1, Ofir Griess4, Luc Husemann1, Fabian Bradic1, Joseph Cornick1, Oliver Mücke1, Riccardo Moro1, Katherine Kelly1, Sara Chocarro1, Etienne Sollier1, Maria Jose Alonso-De Gennaro5, Siavash Mansouri5, Madeleine Dorsch6, Patricia Munteanu6, Balazs Hegedüs7, Hauke Winter8, Laura V. Klotz8, Mark Kriegsmann9, Felix JF Herth8, Marc A. Schneider8, Daniel Kazdal9, Albrecht Stenzinger9, Alexander Schramm6, Felix J. Hartmann1, Pavlo Lutsik10, Ursula Klingmüller1, Rajkumar Savai5, Rocio Sotillo1, Barbara M. Grüner6, Guy Ron11, Efrat Shema4, Michael Scherer1, Christoph Plass1, Maria Llamazares-Prada1

1DKFZ German Cancer Research Center, Heidelberg, Germany,2National Taiwan University, Taipei, Taiwan,3National Taiwan University and Academia Sinica, Taipei, Taiwan,4Weizmann Institute of Science, Rehovot, Israel,5Max Planck Institute for Heart and Lung Research, Bad Nauheim, Germany,6West German Cancer Center, Essen, Germany,7University Medicine Essen - Ruhrlandklinik, Essen, Germany,8Thoraxklinik at Heidelberg University Hospital, Heidelberg, Germany,9Institute of Pathology at Heidelberg University Hospital, Heidelberg, Germany,10KU Leuven, Leuven, Belgium,11Racah Institute of Physics, Hebrew University, Jerusalem, Israel

摘要 Abstract

Loss of the Y chromosome (LOY) is among the most frequent somatic alterations in the blood of aging men. In cancer, LOY is associated with poor survival across multiple solid entities, including non-small cell lung cancer. Yet, the molecular mechanisms linking LOY and adverse outcomes remain poorly understood. Beyond sex-determining loci, the Y chromosome encodes dosage-sensitive genes, including two epigenetic regulators, whose X-linked homologs escape X-inactivation in females. We hypothesized that LOY results in haploinsufficiency of these regulatory genes, promoting tumor cell plasticity and heterogeneity.We investigated the consequences of LOY in lung adenocarcinoma (LUAD), the most prevalent lung cancer subtype, showing higher incidence and mortality in men. We performed whole-genome and single-cell RNA sequencing of paired tumor and matched normal lung tissue from male LUAD patients, complemented by public datasets. LOY was enriched in malignant cells and less frequent in the tumor microenvironment. To define tumor-cell-intrinsic effects, we generated isogenic A549 single-cell clones with or without the Y chromosome. LOY clones and primary LOY LUAD samples exhibited strong activation of epithelial-to-mesenchymal transition (EMT) programs. Genes that were consistently upregulated in LOY compared to ROY included THY1, LOX, and CDH2, which we also found to be highly abundant on the protein level. These effects were accompanied by increased cell-state plasticity, enhanced adaptation to metabolic and genotoxic stress. At the epigenetic level, we found widespread differences in DNA methylation patterns, especially at gene promoters of EMT genes, indicating an epigenetic underpinning of the phenotype. At the single-cell level, LOY clones showed increased epigenetic and transcriptional heterogeneity. Functionally, LOY conferred a selective advantage in vivo, promoting tumor engraftment and metastatic outgrowth. Together, these findings identify LOY as a previously unrecognized driver of EMT activation and tumor plasticity through epigenetic and transcriptional reprogramming, providing a mechanistic explanation for its association with poor therapy response and adverse clinical outcome in male lung adenocarcinoma.
利益披露 Disclosure
K. Schlüter, None.. M. Chen, None.. G. Altun, None.. S. Manzano Sanchez, None.. D. Wu, None.. N. Zhang, None.. O. Griess, None.. L. Husemann, None.. F. Bradic, None.. J. Cornick, None.. O. Mücke, None.. R. Moro, None.. K. Kelly, None.. S. Chocarro, None.. E. Sollier, None.. M. Alonso-De Gennaro, None.. S. Mansouri, None.. M. Dorsch, None.. P. Munteanu, None.. B. Hegedüs, None.. H. Winter, None.. L. V. Klotz, None.. M. Kriegsmann, None.. F. J. Herth, None.. M. A. Schneider, None.. D. Kazdal, None.. A. Stenzinger, None.. A. Schramm, None.. F. J. Hartmann, None.. P. Lutsik, None.. U. Klingmüller, None.. R. Savai, None.. R. Sotillo, None.. B. M. Grüner, None.. G. Ron, None.. E. Shema, None.. M. Scherer, None.. C. Plass, None.. M. Llamazares-Prada, None.

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