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Breast tumor stiffness instructs bone metastasis via maintenance of mechanical conditioning

Adam Watson, Adam Grant, Sara S. Parker, Samantha M. Hill, Michael B. Whalen, Jayati Chakrabarti, Michael W. Harman, Mackenzie R. Roman, Brittany L. Forte, Cody Gowan, Raúl Castro-Portuguez, Lindsey K. Stolze, Christian Franck, Darren A. Cusanovich, Yana Zavros, Megha Padi, Casey E. Romanoski, Ghassan Mouneimne

2021Cell Reports83 citationsDOIOpen Access PDF

Abstract

While the immediate and transitory response of breast cancer cells to pathological stiffness in their native microenvironment has been well explored, it remains unclear how stiffness-induced phenotypes are maintained over time after cancer cell dissemination in vivo. Here, we show that fibrotic-like matrix stiffness promotes distinct metastatic phenotypes in cancer cells, which are preserved after transition to softer microenvironments, such as bone marrow. Using differential gene expression analysis of stiffness-responsive breast cancer cells, we establish a multigenic score of mechanical conditioning (MeCo) and find that it is associated with bone metastasis in patients with breast cancer. The maintenance of mechanical conditioning is regulated by RUNX2, an osteogenic transcription factor, established driver of bone metastasis, and mitotic bookmarker that preserves chromatin accessibility at target gene loci. Using genetic and functional approaches, we demonstrate that mechanical conditioning maintenance can be simulated, repressed, or extended, with corresponding changes in bone metastatic potential.

Topics & Concepts

MetastasisBreast cancerCancer researchBiologyPhenotypeRUNX2Tumor microenvironmentCancer cellBone metastasisCancerTranscription factorCell biologyGeneGeneticsTumor cellsCellular Mechanics and InteractionsRNA Research and SplicingCancer Cells and Metastasis
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