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000148819 1001_ $$aDeville, Sara Sofia$$b0
000148819 245__ $$aThe Extracellular, Cellular, and Nuclear Stiffness, a Trinity in the Cancer Resistome-A Review.
000148819 260__ $$aLausanne$$bFrontiers Media$$c2019
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000148819 520__ $$aAlterations in mechano-physiological properties of a tissue instigate cancer burdens in parallel to common genetic and epigenetic alterations. The chronological and mechanistic interrelation between the various extra- and intracellular aspects remains largely elusive. Mechano-physiologically, integrins and other cell adhesion molecules present the main mediators for transferring and distributing forces between cells and the extracellular matrix (ECM). These cues are channeled via focal adhesion proteins, termed the focal adhesomes, to cytoskeleton and nucleus and vice versa thereby affecting the pathophysiology of multicellular cancer tissues. In combination with simultaneous activation of diverse downstream signaling pathways, the phenotypes of cancer cells are created and driven characterized by deregulated transcriptional and biochemical cues that elicit the hallmarks of cancer. It, however, remains unclear how elastostatic modifications, i.e., stiffness, in the extracellular, intracellular, and nuclear compartment contribute and control the resistance of cancer cells to therapy. In this review, we discuss how stiffness of unique tumor components dictates therapy response and what is known about the underlying molecular mechanisms.
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000148819 7001_ $$0P:(DE-HGF)0$$aCordes, Nils$$b1
000148819 773__ $$0PERI:(DE-600)2649216-7$$a10.3389/fonc.2019.01376$$gVol. 9, p. 1376$$p1376$$tFrontiers in oncology$$v9$$x2234-943X$$y2019
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