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Nuclear lamin isoforms differentially contribute to LINC complex-dependent nucleocytoskeletal coupling and whole cell mechanics

Authors :
Stephen A. Adam
Karen L. Reddy
Suganya Sivagurunathan
Chan Young Park
Robert D. Goldman
Yixian Zheng
Tran
Wong X
Jeffrey J. Fredberg
Gregg G. Gundersen
Amir Vahabikashi
Nicdao Fas
Ming Guo
Yu Long Han
Luxton Gg
Publication Year :
2021
Publisher :
Cold Spring Harbor Laboratory, 2021.

Abstract

The ability of a cell to regulate its mechanical properties is central to its function. Emerging evidence suggests that interactions between the cell nucleus and cytoskeleton influence cell mechanics through poorly understood mechanisms. Here we show that A- and B-type nuclear lamin isoforms distinctively modulate both nuclear and cellular volume and selectively stabilize the linker of nucleoskeleton and cytoskeleton (LINC) complexes that couple the nucleus to cytoskeletal actin and vimentin. We reveal, further, that loss of each of the four-known lamin isoforms in the mouse embryonic fibroblasts differentially affects cortical and cytoplasmic stiffness as well as cellular contractility, and then propose a LINC complex mediated model that explains these impaired mechanical phenotypes. Finally, we demonstrate that loss of each lamin isoform softens the nucleus in a manner that correlates with loss of heterochromatin. Together, these findings uncover distinctive roles for each lamin isoform in maintaining cellular and nuclear mechanics.

Details

Database :
OpenAIRE
Accession number :
edsair.doi...........59d2872e5ecc95c3d1aa2059959c0ddd