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Current Neuropharmacology
ISSN: 1570-159X
Current Neuropharmacology
Volume 3, Number 4, October 2005
Contents
Potential of Bone Marrow Stromal Cells in Applications for
Neuro-Degenerative, Neuro-Traumatic and Muscle Degenerative
Diseases Pp.257
M. Dezawa, H. Ishikawa, M. Hoshino, Y. Itokazu and Y.-i.
Nabeshima
[Abstract]
The Sigma Receptor: Evolution of the Concept in Neuropsycho-pharmacology
Pp.267
T. Hayashi and T.-P. Su
[Abstract]
Role of Altered Structure and Function of NMDA Receptors
inDevelopment of Alcohol Dependence Pp.281
J. Nagy, S. Kolok, A. Boros and P. Dezsð
[Abstract]
Agonists and Antagonists of Metabotropic Glutamate
Receptors:Anticonvulsants and Antiepileptogenic Agents? Pp.299
F.R. Tang
[Abstract]
The Potential of Caffeine for Functional Modification
from CorticalSynapses to Neuron Networks in the Brain Pp.309
H. Yoshimura
[Abstract]
Neuroprotection by Alpha 2-Adrenergic Agonists in
Cerebral Ischemia Pp.317
Y. Zhang and H.K. Kimelberg
[Abstract]
Abstracts
[Back to top]
Potential of Bone Marrow Stromal Cells in Applications
for Neuro-Degenerative, Neuro-Traumatic and Muscle Degenerative
Diseases
Mari Dezawa, Hiroto Ishikawa, Mikio Hoshino, Yutaka Itokazu
and Yo-ichi Nabeshima
Cell transplantation is a promising strategy for the treatment
of neurodegenerative and muscle degenerative diseases. Many
kinds of cells, including embryonic stem cells and tissue
stem cells, have been considered as candidates for transplantation
therapy. Bone marrow stromal cells (MSCs) have great potential
as therapeutic agents since they are easy to isolate and can
be expanded from patients without serious ethical or technical
problems. We discovered a new method for the highly efficient
and specific induction of functional Schwann cells, neurons
and skeletal muscle lineage cells from both rat and human
MSCs. These induced cells were transplanted into animal models
of neurotraumatic injuries, Parkinson's disease, stroke and
muscle dystrophies, resulting in the successful integration
of transplanted cells and an improvement in behavior of the
transplanted animals. Here we focus on the respective potentials
of MSC-derived cells and discuss the possibility of clinical
application in degenerative diseases.
[Back to top]
The Sigma Receptor: Evolution of the Concept in Neuropsychopharmacology
T. Hayashi and T.-P. Su
Although originally proposed as a subtype of opioid receptors,
the sigma receptor is now confirmed to be a non-opioid receptor
that binds diverse classes of psychotropic drugs. Sigma receptors
are subdivided into two subtypes, sigma-1 and sigma-2. The
sigma-1 receptor is a 25-kDa protein possessing one putative
transmembrane domain and an endoplasmic reticulum retention
signal. Sigma-1 receptors are highly expressed in deeper laminae
of the cortex, olfactory bulb, nuclei of mesencephalon, hypothalamus,
and Purkinje cells in the brain. Sigma-1 receptors are predominantly
localized at the endoplasmic reticulum of both neurons and
oligodendrocytes. From behavioral studies, sigma-1 receptors
were shown to be involved in higher-ordered brain functions
including memory and drug dependence. The actions mediated
by sigma-1 receptors at the cellular level can be considered
either as acute or chronic. The acute actions include the
modulation of ion channels (i.e., K+ channel, NMDA receptors,
IP3 receptors) and the sigma-1 receptor translocation. Chronic
actions of sigma-1 receptors are basically considered to be
the result of an up- or down regulation of the sigma-1 receptor
itself. For example, the upregulation of sigma-1 receptors
per se, even without exogenous ligands, promotes
cellular differentiation and reconstitution of lipid microdomains
(lipid rafts) in cultured cells. These findings together suggest
that sigma-1 receptors might possess a constitutive biological
activity, and that sigma-1 receptor ligands might merely work
as modulators of the innate activity of this protein. Recent
in vitro and in vivo studies strongly point
to the possibility that sigma-1 receptors participate in membrane
remodeling and cellular differentiation in the nervous system.
[Back to top]
Role of Altered Structure and Function of NMDA Receptors
in Development of Alcohol Dependence
József Nagy, Sándor Kolok, András
Boros, Péter Dezsð
Long-term alcohol exposure gives rise to development of
physical dependence on alcohol in consequence of changes in
certain neurotransmitter functions. Accumulating evidence
suggests that the glutamatergic neurotransmitter system, especially
the N-methyl-D-aspartate (NMDA) type of glutamate receptors
is a particularly important site of ethanol’s action,
since ethanol is a potent inhibitor of the NMDA receptors
(NMDARs) and prolonged ethanol exposition leads to a compensatory
“upregulation” of NMDAR mediated functions supposedly
contributing to the occurrence of ethanol tolerance, dependence
as well as the acute and delayed signs of ethanol withdrawal.
Recently, expression of different types of NMDAR subunits
was found altered after long-term ethanol exposure. Especially,
the expression of the NR2B and certain splice variant forms
of the NR1 subunits were increased in primary neuronal cultures
treated intermittently with ethanol. Since NMDA ion channels
with such an altered subunit composition have increased permeability
for calcium ions, increased agonist sensitivity, and relatively
slow closing kinetics, the above-mentioned alterations may
underlie the enhanced NMDAR activation observed after long-term
ethanol exposure. In accordance with these changes, the inhibitory
potential of NR2B subunit-selective NMDAR antagonists is also
increased, demonstrating excellent potency against alcohol
withdrawal-induced in vitro cytotoxicity. Although
in vivo data are few with these compounds, according
to the effectiveness of the classic NMDAR antagonists in attenuation,
not only the physical symptoms,but also some affective and
motivational components of alcohol withdrawal, novel NR2B
subunit selective NMDAR antagonists may offer a preferable
alternative in the pharmacotherapy of alcohol dependence.
[Back to top]
Agonists and Antagonists of Metabotropic Glutamate
Receptors: Anticonvulsants and Antiepileptogenic Agents?
Feng Ru Tang
Anticonvulsant and neuroprotective effects of agonist and
antagonist of metabotropic glutamate receptors (mGluRs) have
been known for more than 10 years from multiple studies. However,
it is not certain whether these candidate drugs are also antiepileptic
and antiepileptogenic, as few studies included the chronic
stages to determine whether spontaneous recurrent seizures
could be prevented or stopped. Even in the acute stage, differences
in experimental design such as timing and route of administration
of candidate drugs, age, species and strain of experimental
animal and experimental model make it difficult to determine
the anticonvulsant and neuroprotective effects of each candidate
drug. This paper, reviews in vivo neuropharmacological
studies on agonsists and antagonists of mGluRs in different
seizure and epilepsy models in last more than ten years. By
combining with our neuropharmacological studies on the effect
of mGluR agonists and antagonists in the mouse pilocarpine
model of temporal lobe epilepsy, an ideal model for future
development of mGluR agonists and antagonists as antiepileptogenic
drugs will be proposed.
[Back to top]
The Potential of Caffeine for Functional Modification
from Cortical Synapses to Neuron Networks in the Brain
Hiroshi Yoshimura
Structure and function of the brain are use-dependent variables
based on “synapse plasticity”. Since synapses
are driven by chemical transmitters, synaptic functions are
liable to be modified by extrinsic chemicals displaying affinities
for synaptic receptors or modulators. Caffeine is a widely
used chemical substance that can invade synapses, and has
several biochemical and metabolic actions on synaptic activities.
This review focuses on the actions of caffeine on changes
in structure and function in the region of the hippocampal
formation and neocortex, which exhibit high synapse plasticity.
At the synapse level, various synaptic receptors and channel
activities are modulated by caffeine via mobilization of intracellular
calcium, inhibition of phosphodiesterase, antagonism of adenosine
receptors and GABA receptors. These actions of caffeine enable
neurons to induce plastic changes in the properties of synaptic
activities, such as synaptic transmission efficiency and morphology.
At the network level, caffeine has the ability to activate
cortical neural oscillators that deliver repetitive N-methyl-D-aspartate
receptor-dependent signals to surrounding areas, causing strengthening
of long-range inter-cortical communications. Caffeine might
thus allow reorganization of cortical network functions via
synaptic mobilizations.
[Back to top]
Neuroprotection by Alpha 2-Adrenergic Agonists in
Cerebral Ischemia
Yonghua Zhang and Harold K. Kimelberg
Ischemic brain injury is implicated in the pathophysiology
of stroke and brain trauma, which are among the top killers
worldwide, and intensive studies have been performed to reduce
neural cell death after cerebral ischemia. Alpha 2-adrenergic
agonists have been shown to improve the histomorphological
and neurological outcome after cerebral ischemic injury when
administered during ischemia, and recent studies have provided
considerable evidence that alpha 2-adrenergic agonists can
protect the brain from ischemia/reperfusion injury. Thus,
alpha 2-adrenergic agonists are promising potential drugs
in preventing cerebral ischemic injury, but the mechanisms
by which alpha 2-adrenergic agonists exert their neuroprotective
effect are unclear. Activation of both the alpha 2-adrenergic
receptor and imidazoline receptor may be involved. This mini
review examines the recent progress in alpha 2-adrenergic
agonists - induced neuroprotection and its proposed mechanisms
in cerebral ischemic injury.
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