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2004 Volume No 7- pages
12-26
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Title: Glutamate signalling and its potential application
to tissue engineering of bone
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Author: Deborah J. Mason
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Address: School of Biosciences, Cardiff University,
Museum Avenue, Cardiff, CF10 3US, U.K
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E-mail: masondj@cardiff.ac.uk
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Key Words: Glutamate, bone tissue engineering, glutamate
transporters, glutamate receptors, osteocytes, osteoblasts,
osteoclasts, ion channels, mechanical load.
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Publication date: April 7th 2004
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Abstract: Mechanical loading of the skeleton is
important for maintenance of adequate bone mass and defined
mechanical stimuli are highly osteogenic. The identification
of mechanoresponsive signalling molecules in bone may allow
osteogenic signals to be mimicked. This approach would be
useful in the treatment of bone pathologies where the skeleton
is too weak to withstand osteogenic forces and to tissue engineering
of bone where the mechanical environment of bone cells is
disrupted. Glutamate has been implicated as a mediator of
mechanical signalling in bone. Evidence for glutamate signalling
in bone, its role in mechanotransduction and potential applications
of this pathway to tissue engineering of bone is considered
in this review. Glutamate receptors, transporters and proteins
that regulate glutamate release, are all expressed in bone
cells. Glutamate receptor activation affects both osteoblast
and osteoclast phenotypes revealing a potential for therapeutic
manipulation of glutamate signalling to enhance bone formation.
Glutamate transporters contribute to this system by regulating
extracellular glutamate concentrations and acting as glutamate-gated
ion channels. Artificial regulation of glutamate receptors
or transporters may be used to increase the bone forming capacity
of osteoblasts. This novel approach may potentially enhance
bone tissue engineering strategies.
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