A Computational Model of YAP/TAZ Mechanosensing
Meng Sun, Fabian Spill, Muhammad H. Zaman

TL;DR
This paper introduces a computational model that links mechanical properties of the cellular environment to biochemical signaling pathways involving YAP/TAZ, elucidating their role in cell fate decisions and mechanosensing.
Contribution
The novel model integrates ECM mechanics with intracellular signaling, revealing how YAP/TAZ activity responds to mechanical cues and pathway interactions, advancing understanding of mechanotransduction.
Findings
Adhesion molecules can rescue YAP/TAZ activity in soft environments.
YAP/TAZ response varies with molecule concentration changes.
Interaction of LIMK and LATS explains YAP/TAZ pathway synergy.
Abstract
In cell proliferation, stem cell differentiation, chemoresistance and tissue organization, the ubiquitous role of YAP/TAZ continues to impact our fundamental understanding in numerous physiological and disease systems. YAP/TAZ is an important signaling nexus integrating diverse mechanical and biochemical signals, such as ECM stiffness, adhesion ligand density, or cell-cell contacts, and thus strongly influences cell fate. Recent studies show that YAP/TAZ mechanical sensing is dependent on RhoA-regulated stress fibers. However, current understanding of YAP/TAZ still remains limited due to the unknown interaction between the canonical Hippo pathway and cell tension. To identify the roles of key signaling molecules in mechanical signal sensing and transduction, we present a novel computational model of the YAP/TAZ signaling pathway. This model converts ECM mechanical properties to…
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