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Chapter 18. The Nuclear Membrane and Mechanotransduction: Impaired Nuclear Mechanics and Mechanotransduction in Lamin A/C Deficient Cells

  1. Derek J. Chadwick Organizer,
  2. Jamie Goode
  1. Jan Lammerding1,
  2. Richard T. Lee1,2,*

Published Online: 7 OCT 2008

DOI: 10.1002/0470093765.ch18

Book Title

Nuclear Organization in Development and Disease: Novartis Foundation Symposium 264

Nuclear Organization in Development and Disease: Novartis Foundation Symposium 264

Additional Information

How to Cite

Lammerding, J. and Lee, R. T. (2008) The Nuclear Membrane and Mechanotransduction: Impaired Nuclear Mechanics and Mechanotransduction in Lamin A/C Deficient Cells, in Nuclear Organization in Development and Disease: Novartis Foundation Symposium 264 (eds D. J. Chadwick and J. Goode), John Wiley & Sons, Ltd, Chichester, UK. doi: 10.1002/0470093765.ch18

Author Information

  1. 1

    Biological Engineering Division, Massachusetts Institute of Technology, 77 Massachusetts Avenue, Cambridge, MA 02139, USA

  2. 2

    Cardiovascular Division, Brigham & Women's Hospital, Partner's Research Facility, Room 279, 65 Landsdowne St, Cambridge, MA 02139, USA

*Cardiovascular Division, Brigham & Women's Hospital, Partner's Research Facility, Room 279, 65 Landsdowne St, Cambridge, MA 02139, USA and Biological Engineering Division, Massachusetts Institute of Technology, 77 Massachusetts Avenue, Cambridge, MA 02139, USA

Publication History

  1. Published Online: 7 OCT 2008
  2. Published Print: 14 JAN 2005

Book Series:

  1. Novartis Foundation Symposia

Book Series Editors:

  1. Novartis Foundation

ISBN Information

Print ISBN: 9780470093733

Online ISBN: 9780470093764

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CHAPTER TOOLS

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Keywords:

  • defective lamin A/C;
  • increased cellular mechanical sensitivity;
  • lamin A/C deficient fibroblasts;
  • impaired nuclear mechanics and mechanotransduction;
  • mechanically activated gene regulation;
  • strain-induced signalling;
  • impaired transcriptional activation;
  • mechanotransduction cascade

Summary

Mutations in the lamin A/C gene cause a variety of human diseases including Emery-Dreifuss muscular dystrophy, dilated cardiomyopathy and Hutchinson-Gilford progeria syndrome. The tissue specific effects of lamin mutations are unclear, in part because the function of lamin A/C is incompletely defined, but the many muscle specific phenotypes suggest that defective lamin A/C could increase cellular mechanical sensitivity. Lamin A/C deficient fibroblasts were subjected to mechanical strain to measure nuclear mechanical properties and strain-induced signalling. We found that lamin A/C deficient fibroblasts are characterized by impaired nuclear mechanics and mechanotransduction, reflected by increased nuclear deformations, increased nuclear fragility, attenuated expression of mechanosensitive genes, and impaired transcriptional activation, leading to impaired viability of mechanically strained cells. Lamins and other nuclear envelope proteins can thus affect several levels of the mechanotransduction cascade, altering nuclear and cytoskeletal mechanics as well as playing an important role in mechanically activated gene regulation. Individual mutations in the lamin A/C gene could potentially selectively interfere with any of these functions, explaining the tissue-specific effects observed in the laminopathies.

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