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Septins provide microenvironment sensing and cortical actomyosin partitioning in motile amoeboid T lymphocytes

https://doi.org/10.1126/sciadv.adi1788

Zhovmer, Alexander S. ; Manning, Alexis ; Smith, Chynna ; Nguyen, Ashley ; Prince, Olivia ; Sáez, Pablo J. ; Ma, Xuefei ; Tsygankov, Denis ; Cartagena-Rivera, Alexander X. ; Singh, Niloy A. ; et al ( January 2024 , Science Advances)

The all-terrain motility of lymphocytes in tissues and tissue-like gels is best described as amoeboid motility. For amoeboid motility, lymphocytes do not require specific biochemical or structural modifications to the surrounding extracellular matrix. Instead, they rely on changing shape and steric interactions with the microenvironment. However, the exact mechanism of amoeboid motility remains elusive. Here, we report that septins participate in amoeboid motility of T cells, enabling the formation of F-actin and α-actinin–rich cortical rings at the sites of cell cortex–indenting collisions with the extracellular matrix. Cortical rings compartmentalize cells into chains of spherical segments that are spatially conformed to the available lumens, forming transient “hourglass”-shaped steric locks onto the surrounding collagen fibers. The steric lock facilitates pressure-driven peristaltic propulsion of cytosolic content by individually contracting cell segments. Our results suggest that septins provide microenvironment-guided partitioning of actomyosin contractility and steric pivots required for amoeboid motility of T cells in tissue-like microenvironments.

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Free, publicly-accessible full text available January 5, 2025
Viscoelastic parameterization of human skin cells characterize material behavior at multiple timescales

https://doi.org/10.1038/s42003-021-02959-5

Parvini, Cameron H. ; Cartagena-Rivera, Alexander X. ; Solares, Santiago D. ( January 2022 , Communications Biology)

Abstract
Countless biophysical studies have sought distinct markers in the cellular mechanical response that could be linked to morphogenesis, homeostasis, and disease. Here, an iterative-fitting methodology visualizes the time-dependent viscoelastic behavior of human skin cells under physiologically relevant conditions. Past investigations often involved parameterizing elastic relationships and assuming purely Hertzian contact mechanics, which fails to properly account for the rich temporal information available. We demonstrate the performance superiority of the proposed iterative viscoelastic characterization method over standard open-search approaches. Our viscoelastic measurements revealed that 2D adherent metastatic melanoma cells exhibit reduced elasticity compared to their normal counterparts—melanocytes and fibroblasts, and are significantly less viscous than fibroblasts over timescales spanning three orders of magnitude. The measured loss angle indicates clear differential viscoelastic responses across multiple timescales between the measured cells. This method provides insight into the complex viscoelastic behavior of metastatic melanoma cells relevant to better understanding cancer metastasis and aggression.

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