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The research in the Lammerding lab is focused
on subcellular mechanics and the cellular signaling response to
mechanical stimulation. In particular, we are studying how mutations
in nuclear envelope proteins such as lamin can render cells more
sensitive to mechanical stress and affect their mechanotransduction
signaling. Insights gained from this work can lead to a better
understanding of the molecular mechanism underlying laminopathies, a
diverse group of diseases including Emery-Dreifuss muscular dystrophy,
Hutchison-Gilford progeria syndrome, and familial partial
lipodystrophy.
To
achieve these goals, we are developing novel experimental techniques
to (i) study nuclear mechanical properties in intact cells and isolated
nuclei, to (ii) investigate the physical coupling between the nucleus
and the cytoskeleton, and to (iii) examine how changes in these
properties can affect the cellular response to mechanical stimulation.
Currently,
we are applying these techniques to human skin fibroblasts
obtained from laminopathy patients and healthy controls and to
fibroblasts and myoblasts from mouse models of these diseases. In
addition, we are using mouse models of Emery-Dreifuss muscular
dystrophy created in Dr. Colin Stewart’s laboratory to study the in
vivo consequences of these cellular defects.
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Jan Lammerding,
Ph.D.
Instructor in Medicine (HMS)
Associate Biophysicist (BWH)
Office: Partners Research
Building, Rm 283
65
Landsdowne St
Cambridge,
MA 02139
USA
Phone: (617) 768-8273
Fax: (617) 768-8280
Email: 
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