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Publication : Mechanical Stiffness Controls Dendritic Cell Metabolism and Function.

First Author  Chakraborty M Year  2021
Journal  Cell Rep Volume  34
Issue  2 Pages  108609
PubMed ID  33440149 Mgi Jnum  J:316003
Mgi Id  MGI:6716140 Doi  10.1016/j.celrep.2020.108609
Citation  Chakraborty M, et al. (2021) Mechanical Stiffness Controls Dendritic Cell Metabolism and Function. Cell Rep 34(2):108609
abstractText  Stiffness in the tissue microenvironment changes in most diseases and immunological conditions, but its direct influence on the immune system is poorly understood. Here, we show that static tension impacts immune cell function, maturation, and metabolism. Bone-marrow-derived and/or splenic dendritic cells (DCs) grown in vitro at physiological resting stiffness have reduced proliferation, activation, and cytokine production compared with cells grown under higher stiffness, mimicking fibro-inflammatory disease. Consistently, DCs grown under higher stiffness show increased activation and flux of major glucose metabolic pathways. In DC models of autoimmune diabetes and tumor immunotherapy, tension primes DCs to elicit an adaptive immune response. Mechanistic workup identifies the Hippo-signaling molecule, TAZ, as well as Ca(2+)-related ion channels, including potentially PIEZO1, as important effectors impacting DC metabolism and function under tension. Tension also directs the phenotypes of monocyte-derived DCs in humans. Thus, mechanical stiffness is a critical environmental cue of DCs and innate immunity.
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