| Current
Neurovascular Research
ISSN: 1567-2026
Current Neurovascular Research
Volume 4, Number 2, May 2007
Contents
Editorial Pp. 73
Experimental Models of Discovery: Prediction and Protection
must Proceed "Hand-in-Hand"
K. Maiese
ORIGINAL ARTICLES
Establishment of Cholinergic Neuron-like Cell Lines With Differential
Vulnerability to Nitrosative Stress Pp. 75-88
D.A. Personett, K. Williams, K.A. Baskerville and M. McKinney
[Abstract]
Preconditioning with Chronic Cerebral Hypoperfusion
Reduces a Focal Cerebral Ischemic Injury and Increases Apurinic/Apyrimidinic
Endonuclease/ Redox Factor-1 and Matrix Metalloproteinase-2
Expression Pp. 89-97
S-A. Choi, E.H. Kim, J.Y. Lee, H.S. Nam, S.H. Kim, G.W.
Kim, B.I. Lee and J.H. Heo
[Abstract]
REVIEW ARTICLES
Current Advances in the Treatment of Parkinson’s Disease
with Stem Cells Pp. 99-109
K.A. Trzaska and P. Rameshwar
[Abstract]
The Zebrafish Model: Use in Studying Cellular Mechanisms
for a Spectrum of Clinical Disease Entities Pp. 111-120
C-H. Hsu, Z-H. Wen, C-S. Lin and C. Chakraborty
[Abstract]
Role of Ischemic Blood-Brain Barrier on Amyloid Plaques
Development in Alzheimer’s Disease Brain Pp.
121-129
R. Pluta
[Abstract]
Microglial Signal Transduction as a Target of Alcohol
Action in the Brain Pp. 131-142
K. Suk
[Abstract]
The Role of Neurotrophins in Axonal Growth, Guidance,
and Regeneration Pp. 143-151
M.G. Lykissas, A.K. Batistatou, K.A. Charalabopoulos and
A.E. Beris
[Abstract]
Abstracts
[Back to top]
Editorial
Experimental Models of Discovery: Prediction and Protection
must Proceed "Hand-in-Hand"
K. Maiese
With the continued expansion of medical technologies
and new strategies for human disease, we can sometimes fall
prey to the belief that successful clinical therapies will
consistently employ the desired attributes of safety and efficacy
as common denominators. Yet, even for some remarkable and
presumably safe diagnostic techniques such as magnetic resonance
imaging, these assumptions may fall short of our actual experience.
For example, there exist potential adverse effects of exposure
to elevated magnetic field levels that exist during magnetic
resonance imaging. It is true that magnetic fields occur naturally
throughout the planet, but human derived magnetic fields can
further enhance the intensity of naturally occurring magnetic
fields. Industries that involve railways operating from direct
current electrical supply sources or that employ magnetic
levitation train systems can lead to the exposure of significant
magnetic fields. In addition, commercial activities related
to aluminum or steel production using intensified alternating
currents also can result in magnetic fields that may be beyond
normal human tolerance. In the healthcare system, magnetic
resonance imaging for diagnostics can easily generate increased
magnetic fields that may pose risks for both magnetic resonance
imaging technicians and the patients under evaluation.
Adverse affects from strong magnetic fields are multifaceted
and can result in the acute onset of gastric distress, nausea,
and vertigo. In regards to more long-term effects, magnetic
field exposure has been tied to cerebral neoplasms, lung carcinoma,
and hematological cancers. Some studies have suggested that
exposure to magnetic fields can increase the risk of spontaneous
abortions. More recent work involving magnetic resonance imaging
previously published in this journal adds further concern
to potential developmental abnormalities with magnetic field
exposure by demonstrating in rodents exposed to a 1.5 T magnetic
resonance image field for one week the subsequent onset of
reference memory deficits (Yang et al., 2007). It
should be noted that further work especially with more rigorous
controls and statistically powered clinical trials is required,
since some prior investigations did not exclude for the effects
of confounding variables such as concurrent toxic substance
exposure.
So how does one develop new therapies that will offer efficacy
for disease treatment, but also will not harm the afflicted
individual patient? Early scientific investigation has provided
us with both a clear vision and a solid foundation for future
discovery. During the 1700s, Antoine Lavoisier, Karl Scheele,
and Joseph Priestley independently relied upon a variety of
experimental models to illustrate that air and its component
oxygen were vital to sustain processes associated with combustion
as well as life. Lavoisier subsequently carried this work
further with animal models to illustrate that oxygen based
upon concentration and duration of exposure could be either
beneficial or toxic to an organism. These early models of
experimentation laid some of the groundwork for today's science
and the critical reliance upon both cell and animal models
for the investigation of the etiology and treatment of human
disease processes.
Present models of human disease have become so diverse in
nature that it would be almost inconceivable for one to foresee
from several years past that the genetic construction of cell
lines or the reliance upon aquatic animal models could for
the most part accurately predict and sharply focus therapeutic
strategies for a wide range of clinical disorders. This issue
of Current Neurovascular Research serves to highlight
the vantage points of a broad discipline of experimental models
that promote the development of basic research to the realities
of clinical care. In original and review articles, unique
strategies describe the use of fused embryonic rodent neurons
with neuroblastoma cell lines, the deployment of embryonic,
neuronal, and adult mesenchymal stem cells for chronic neurodegenerative
disorders, the development of ischemic animal models for furthering
the understanding of the cellular pathways that occur during
stroke and Alzheimer's disease, and the burgeoning reliance
upon the Zebrafish model for a host of human disorders. Although
it is unlikely that any single experimental model of human
disease will ever be capable of replicating the complex disease
processes of the human body, it is clear that the visionary
minds of Lavoisier, Scheele, and Priestley have led us upon
an exciting path of discovery coupled with great insight and
we are enthusiastic in this issue of Current Neurovascular
Research to hopefully foster this same course for our
readers today.
Kenneth Maiese
Editor-in-Chief
[Back to top]
Establishment of Cholinergic Neuron-like Cell Lines With Differential
Vulnerability to Nitrosative Stress
D.A. Personett, K. Williams, K.A. Baskerville and M. McKinney
Cholinergic cell lines were established by fusion of embryonic
day 17 wild-type neurons from rat basal forebrain (BF) and
upper brainstem (BS) with N18tg neuroblastoma cells. Isolated
clones expressed choline acetyltransferase (ChAT) and neuronal
nitric oxide synthase (nNOS) activities that were increased
upon differentiation with retinoic acid. Clones from the BF
expressed high levels of the tyrosine kinase type A (TrkA)
receptor expression and activation of the mitogen-activated
kinase ERK2 upon treatment with nerve growth factor. Like
wild-type cholinergic populations, the six clones studied
were variably resistant to nitric oxide (NO) excess from addition
of S-nitroso-N-acetyl-D, L-penicillamine (SNAP). Of these,
the BS2 clone exhibited resistance like in vivo BS
cholinergic neurons, while the MS10 clone mimicked in
vivo BF vulnerability. Apoptosis in response to NO excess
was preceded by increases in mito-chondrial responses bax/bcl-2
ratios, but cytochrome C was not released. Mitochondrial levels
of apoptosis initiating factor (AIF) were either unchanged
or increased, and only in MS clones was endonuclease G (EndoG)
released. Microarray data indicated the existence of endoplasmic
reticular (ER) stress and caspase-4 and caspase-12 were involved
in the pathway to DNA fragmentation. The array data also indicated
a survival role for mdm2, and its blockade rendered vulnerable
the brainstem survivor clone BS2.
Akt and ERK1/2 pathways were activated in response to NO and
their blockade increased DNA fragmentation. Blockade of GSK-3α/β,
a downstream target of Akt, reduced SNAP toxicity and this
was more prominent in basal forebrain clones. We have identified
two cholinergic cell lines useful for molecular studies of
cholinergic vulnerability. We hypothesize that, in cholinergic
neurons, control of ER stress signaling may be a major factor
in differential vulnerability.
[Back to top]
Preconditioning with Chronic Cerebral Hypoperfusion
Reduces a Focal Cerebral Ischemic Injury and Increases Apurinic/Apyrimidinic
Endonuclease/ Redox Factor-1 and Matrix Metalloproteinase-2
Expression
S-A. Choi, E.H. Kim, J.Y. Lee, H.S. Nam, S.H. Kim, G.W.
Kim, B.I. Lee and J.H. Heo
Atherosclerosis may cause severe stenosis of the arteries
supplying the brain, which induces chronic cerebral hypoperfusion.
Although an infarction often occurs in the chronically hypoperfused
brain area, it has been uncertain whether the stroke severity
is attenuated or increased when further decrease of blood
flow occurs. To test the hypothesis that chronic cerebral
hypoperfusion is protective against the subsequent severe
ischemia, we examined the effect of chronic cerebral hypoperfusion
on brains subjected to acute focal ischemia. Spontaneous hypertensive
rats were subjected to middle cerebral artery occlusion/reperfusion
four weeks after bilateral common carotid artery ligation
(BCAL) or sham operation. The rats with BCAL had smaller infarctions,
determined by 2,3,5-triphenyltetrazolium hydrochloride staining,
and less severe neurologic deficits than those with sham operation.
The number of DNA-damaged cells, examined by the in situ
nick translation study, was significantly reduced in animals
with BCAL. Immunoreactivity for apurinic/apyrimidinic endonuclease/redox
factor-1, which plays a role in cellular defense mechanism,
was markedly increased in those with BCAL. Indirect evidence
of extracellular matrix remodeling, which might be associated
with adaptive arteriogenesis or angiogenesis, was obtained
in the form of increased matrix metalloproteinase-2 activity
in them. These findings provide experimental evidence that
chronic cerebral hypoperfusion would be protective against
subsequent severe ischemic insults.
[Back to top]
Current Advances in the Treatment of Parkinson’s Disease
with Stem Cells
K.A. Trzaska and P. Rameshwar
Stem cell replacement has emerged as the novel therapeutic
strategy for Parkinson’s disease (PD). Control of motor
behavior is lost in PD due to the selective degeneration of
mesencephalic dopamine neurons (DA) in the substantia nigra.
This progressive loss of DA neurons results in devastating
symptoms for which there is no cure. Debilitating side effects
often result from chronic pharmacological treatment, hence
current investigations into cell transplantation therapy as
a substitute and/or adjuvant to other therapeutics. Clinical
trials with fetal DA tissue have provided evidence that cell
transplantation could be a viable alternative. Limited availability
of fetal tissue, combined with variable outcome led to emphasis
on other sources of cells, such as stem cells. This review
focuses on three stem cell sources (embryonic, neural, and
adult mesenchymal). Also discussed is the molecular differentiation
into mature DA neurons, the various protocols that have been
developed to generate DA neurons from various stem cells,
and the current state of stem cell therapy for PD.
[Back to top]
The Zebrafish Model: Use in Studying Cellular Mechanisms
for a Spectrum of Clinical Disease Entities
C-H. Hsu, Z-H. Wen, C-S. Lin and C. Chakraborty
Although the zebrafish model provides an important platform
for the study of developmental biology, recent work with the
zebrafish model has extended its application to a wide variety
of experimental studies relevant to human disease. Currently,
the zebrafish model is used for the study of human genetic
disease, caveolin-associated muscle disease, homeostasis,
kidney development and disease, cancer, cardiovascular disorders,
oxidative stress, caloric restriction, insulin-like pathways,
angiogenesis, neurological diseases, liver disease, hemophilia,
bacterial pathogenesis, apoptosis, osteoporosis, immunological
studies, germ cell study, Bardet-Biedl syndrome gene (BBS11),
Alzheimer's disease, virology studies and vaccine development.
Here we describe the essential use of the zebrafish model
that applies to several clinical diseases. With increased
understanding of the cellular mechanisms responsible for disease,
we can use knowledge gained from the zebrafish model for the
development of therapeutics.
[Back to top]
Role of Ischemic Blood-Brain Barrier on Amyloid Plaques
Development in Alzheimer’s Disease Brain
R. Pluta
This review demonstrated that ischemic brain injury induces
chronic changes in blood-brain barrier in the gray and white
matter. This insufficiency of blood-brain barrier may allow
entry of uncellular blood components such as different fragments
of amyloid precursor protein and cellular blood components
like leukocytes and platelets into the brain parenchyma. These
blood components may have chronic harmful effects on the ischemic
neuronal cells, axons and myelin and can intensify and finish
the neuropathology in ischemic brain parenchyma. Pathological
accumulation of different toxic fragments of amyloid precursor
protein in extracellular space and myelinated axons appears
after ischemic blood-brain barrier injury and seem to be concomitant
with, but independent of neuronal ischemic cytoplasmic injury.
It seems that ischemic blood-brain barrier disturbances may
play an important, both direct and indirect role in the pathogenesis
of extra- and intracellular space in gray and white matter
lesions following ischemic episode. This neuropathology appears
to have similar character and distribution as in sporadic
Alzheimer’s disease. This review presented chronic micro-blood-brain
barrier openings in ischemic gray and white matter lesions
that probably would act as seeds of future Alzheimer’s
amyloid plaques.
[Back to top]
Microglial Signal Transduction as a Target of Alcohol
Action in the Brain
K. Suk
Although alcohol is believed to exert deleterious effects
on the nervous system in general, its specific effect on the
brain’s immune system remains poorly understood. In
particular, the effects of alcohol consumption on the immune
and inflammatory responses in the central nervous system (CNS)
have not been extensively investigated. Here, reviewed is
the recent progress on how ethanol influences the signal transduction
pathways of the inflammatory activation of brain microglia,
which are thought to function as the resident immune defense
system of the brain. Microglia are the CNS representatives
of macrophages, which have the ability to clean up cellular
debris. Microglia participate in neuroinflammation in response
to various intrinsic or extrinsic stimuli. It has been recently
suggested that microglial signal transduction is one of the
main targets of ethanol action in the brain: ethanol exposure
selectively modulates the intra-cellular signal transductions
of microglia, rather than globally inhibiting signaling pathways
in a nonspecific manner. Deregulation by ethanol of the inflammatory
activation signaling of microglia may contribute to the derangement
of CNS immune and inflammatory responses.
[Back to top]
The Role of Neurotrophins in Axonal Growth, Guidance,
and Regeneration
M.G. Lykissas, A.K. Batistatou, K.A. Charalabopoulos and
A.E. Beris
Neurotrophins are proteins that regulate neuronal
survival, axonal growth, synaptic plasticity and neurotransmission.
They are members of the neurotrophic factors family and include
factors such as the nerve growth factor (NGF), the brain derived
neurotrophic factor (BDNF), the neurotrophin-3 (NT-3), and
the neurotrophin-4/5 (NT-4/5). These molecules bind to two
types of receptors: i) tyrosine kinase receptors (TrkA, TrkB,
TrkC) and ii) a common neurotrophin receptor (p75NTR). The
two receptor types can either suppress or enhance each other’s
actions. Neurotrophins have a multifunctional role both in
the central and peripheral nervous system. They have been
suggested as axonal guidance molecules during the growth and
regeneration of nerves. It has also been proven that they
stimulate axonal growth by mediating the polymerization and
accumulation of F-actin in growth cones and axon shafts. Neurotrophins,
as other neurotrophic factors, have been shown that they reduce
neuronal injury by exposure to excitotoxins, glucose deprivation,
or ischemia. Furthermore, the nerve regeneration promoting
effect of these growth factors is well documented for many
different models of central or peripheral nervous system injury.
Several studies have shown that exogenous administration of
these factors has protective properties for injured neurons
and stimulates axonal regeneration. Based on these properties,
these molecules may be used as therapeutic agents for treating
degenerative diseases and traumatic injuries of both the central
and peripheral nervous system.
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