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Current
Neurovascular Research
ISSN: 1567-2026
Current Neurovascular Research
Volume 5, Number 3, August 2008
Contents
Haptoglobin Polymorphism and Lacunar Stroke Pp.
153-158
Julie Staals, Barbe M.A. Pieters, Iris L.H. Knottnerus, Rob
P.W. Rouhl, Robert J. van Oostenbrugge, Joris R. Delanghe
and Jan Lodder
[Abstract]
Enhanced Tolerance against Early and Late Apoptotic
Oxidative Stress in Mammalian Neurons through Nicotinamidase
and Sirtuin Mediated Pathways Pp. 159-170
Zhao Zhong Chong and Kenneth Maiese
[Abstract]
Progressive Brain Damage and Alterations
in Dendritic Arborization after Collagenase-Induced Intracerebral
Hemorrhage in Rats Pp. 171-177
Angela P. Nguyen, Hang D. Huynh, Suzanne
B. Sjovold and Frederick Colbourne
[Abstract]
Transient Cerebral Ischemia Leads to
TGF- β2
Expression in Golgi Apparatus Organelles Pp.
178-184
Zhiping Hu, Jie Fan, Liuwang Zeng, Wei Lu,
Xiangqi Tang, Jie Zhang and Ting Li
[Abstract]
Basolateral Aggregated Rat Amyloid β(1-42)
Potentiates Transmigration of Primary Rat Monocytes through
a Rat Blood-Brain Barrier Pp. 185-192
Christian Humpel
[Abstract]
Hemoglobin Neurotoxicity is Attenuated
by Inhibitors of the Protein Kinase CK2 Independent of Heme
Oxygenase Activity Pp. 193-198
Jing Chen-Roetling, Zhi Li and Raymond
F. Regan
[Abstract]
Neurofibrillary Tangles and Senile Plaques
in Alzheimer’s Brains are Associated with Reduced Capillary
Expression of Vascular Endothelial Growth Factor and Endothelial
Nitric Oxide Synthase Pp. 199-205
John Provias and Brian Jeynes
[Abstract]
Post Traumatic Lesion absence of β-Dystroglycan-Immunopositivity
in Brain Vessels Coincides with the Glial Reaction and the
Immunoreactivity of Vascular Laminin Pp. 206-213
Adrienn Szabó and Mihály
Kálmán
[Abstract]
Abstracts
[Back to top]
Haptoglobin Polymorphism and Lacunar Stroke
Julie Staals, Barbe M.A. Pieters, Iris L.H.
Knottnerus, Rob P.W. Rouhl, Robert J. van Oostenbrugge, Joris
R. Delanghe and Jan Lodder
Haptoglobin (Hp) 2-2 phenotype has been associated with peripheral
and coronary artery disease and risk of vascular complications
in diabetic patients, but any association of Hp polymorphism
with cerebrovascular disease has not been explored so far.
We aimed to study Hp polymorphism in a sample of 124 patients
with a rather homogeneous type of cerebrovascular disease,
namely first symptomatic lacunar stroke due to small vessel
disease, in comparison with a large (n=918) control group.
Hp phenotypes were determined using starch gel electrophoresis.
Hp1 allele frequency was significantly higher in patients
than in controls (0.480 vs. 0.395, p<0.05), mainly
due to a lower Hp2-2 phenotype frequency (25.0 vs.
36.3 %; OR 0.59; 95%CI 0.38-0.90; p<0.05). This was even
more pronounced in younger (=60 years) patients (Hp1 allele
frequency 0.539). Concomitant asymptomatic lacunar lesions
were present in 82 patients, extensive white matter lesions
in 47 patients.
The association between Hp1 and lacunar stroke suggests that
Hp may serve different functions depending on the pathological
processes in various types of vascular disease in different
organs. The association between Hp1 and lacunar stroke may
relate to blood-brain barrier dysfunction, to the association
between hypertension and cerebral small vessel disease, or
a special dependence of small vessel wall integrity on Hp2-2
related angiogenic potential. The presence of concomitant
signs of cerebral small vessel disease weakened the association
between Hp1 and lacunar stroke, which could reflect a difference
in underlying vascular pathophysiology in which Hp phenotype
may play a different role.
[Back to top]
Enhanced Tolerance against Early and Late Apoptotic
Oxidative Stress in Mammalian Neurons through Nicotinamidase
and Sirtuin Mediated Pathways
Zhao Zhong Chong and Kenneth Maiese
Focus upon therapeutic strategies that intersect between
pathways that govern cellular metabolism and cellular survival
may offer the greatest impact for the treatment of a number
of neurodegenerative and metabolic disorders, such as diabetes
mellitus. In this regard, we investigated the role of a Drosophila
nicotinamidase (DN) in mammalian SH-SY5Y neuronal cells during
oxidative stress. We demonstrate that during free radical
exposure to nitric oxide generators DN neuronal expression
significantly increased cell survival and blocked cellular
membrane injury. Furthermore, DN neuronal expression prevented
both apoptotic late DNA degradation and early phosphatidylserine
exposure that may serve to modulate inflammatory cell activation
in vivo. Nicotinamidase activity that limited nicotinamide
cellular concentrations appeared to be necessary for DN neuroprotection,
since application of progressive nicotinamide concentrations
could abrogate the benefits of DN expression during oxidative
stress. Pathways that involved sirtuin activation and SIRT1
were suggested to be vital, at least in part, for DN to confer
protection through a series of studies. First, application
of resveratrol increased cell survival during oxidative stress
either alone or in conjunction with the expression of DN to
a similar degree, suggesting that DN may rely upon SIRT1 activation
to foster neuronal protection. Second, the overexpression
of either SIRT1 or DN in neurons prevented apoptotic injury
specifically in neurons expressing these proteins during oxidative
stress, advancing the premise that DN and SIRT1 may employ
similar pathways for neuronal protection. Third, inhibition
of sirtuin activity with sirtinol was detrimental to neuronal
survival during oxidative stress and prevented neuronal protection
during overexpression of DN or SIRT1, further supporting that
SIRT1 activity may be necessary for DN neuroprotection during
oxidative stress. Implementation of further work to elucidate
the cellular mechanisms that govern nicotinamidase activity
in mammalian cells may offer novel avenues for the treatment
of disorders tied to oxidative stress and cellular metabolic
dysfunction.
[Back to top]
Progressive Brain Damage and Alterations in Dendritic Arborization
after Collagenase-Induced Intracerebral Hemorrhage in Rats
Angela P. Nguyen, Hang D. Huynh, Suzanne
B. Sjovold and Frederick Colbourne
Intracerebral hemorrhage (ICH) was widely believed to be a
monophasic event whereby cell death occurs from the initial
space-occupying effects of the hematoma. However, we now know
that secondary degenerative events contribute to delayed cell
death, functional impairment and clinical deterioration. In
three experiments, we further characterized the long-term
maturation of injury in the collagenase model of striatal
ICH in rat. First, we quantified the volume of tissue lost
from 7 to 60 days showing that tissue loss more than doubled
over this time. As the volume of tissue lost does not distinguish
gray from white matter damage, gold chloride staining was
used in a second experiment in ICH rats that survived 7 or
60 days. The mid-sagittal area of the corpus callosum significantly
declined (22%) over this period, whereas the hippocampal and
anterior commissures were not affected. A third experiment
used the Golgi-Cox stain to examine dendritic arborization
of peri-hematoma and contralateral medium spiny neurons of
the striatum. We found an early and sustained increase in
dendritic arborization in the non-lesioned hemisphere, whereas
there was initial atrophy of peri-hematoma striatal neurons
that eventually recovered to normal. These findings show that
tissue loss, including white matter atrophy, continues over
extended periods after ICH making it a potential target for
cytoprotective agents. Finally, the dendritic alterations
in both ipsi- and contralateral striatal neurons likely influence
spontaneous recovery and are potential targets to further
improve it.
[Back to top]
Transient Cerebral Ischemia Leads to TGF-β2
Expression in Golgi Apparatus Organelles
Zhiping Hu, Jie Fan, Liuwang Zeng, Wei Lu,
Xiangqi Tang, Jie Zhang and Ting Li
Transforming growth factor2 (TGFβ2)
is a prototypic member of a large superfamily of multifunctional
cytokines, and its potential mechanisms of the neuroprotective
activity in ischemic stroke and subcellular compartmentalization
are largely unknown. The present study investigated TGF-β2
protein expression in hippocampal neuronal cells after transient
forebrain ischemia (TFI). TFI was induced in male adult gerbils
with bilateral occlusion of both common carotid arteries for
10 minutes. With immunohistochemical methods we observe the
expression of TGF-β2
and morphological alternation in Golgi appratus (GA) in different
postischemic periods and sham-operation (6 hours, 1, 3 and
7 days). In addition, the subcellular localization of TGF-
β2 is determined in trans-Golgi network (TGN)
by double-labeling confocal immunofluorographs with TGN38.The
results showed that TGF-β2
persistent express in the ischemic animals and it peaks at
3 days, then decreased 7 days postocclusion. No significant
alterations to the GA were noted at the point of 6 hours,1
and 3 days following TFI, but there are a few neurons in which
the GA lost the normal network-like configuration and its
elements decreased in cortical cells from gerbils survived
7 days postocclusion. In addition, TGF-β2
was colocalized with TGN38 in the TGN after TFI .Taken together,
this result suggested that TGF-β2
protein expression increased in neurons after ischemia, which
may represent an endogenous adaptative response of the brain
damage and its secretion via GA after ischemia is
supposed to be beneficial for GA . Furthermore, fragmentation
of GA is not common phenomenon in the ischemia, but intact
GA structural of neurons is beneficial for cell survival.
[Back to top]
Basolateral Aggregated Rat Amyloid β(1-42)
Potentiates Transmigration of Primary Rat Monocytes through
a Rat Blood-Brain Barrier
Christian Humpel
Monocytes adhere and transmigrate through a blood-brain
barrier (BBB) during a normal immune patrol and after pathological
events. It is well established that the transmigration of
monocytes through the BBB is stimulated by soluble amyloidβ.
The aim of the present study was to explore if aggregated
amyloidβ
added to the basolateral side of a BBB may modulate the adhesion
and migration of primary rat monocytes through a monolayer
of rat brain capillary endothelial cells (BCEC). Monocytes
were freshly isolated from rat blood by negative magnetic
selection and applied to the apical side of a fully confluent
BCEC-monolayer with or without pre-treatment with soluble
or aggregated amyloidβ.
Aggregation was performed by incubation of amyloidβ
(1-42) for 2 weeks in acidic medium at 37°C. The
monocytes adhered at the apical side of a BCEC-monolayer within
30-90 min (approx. 1,500 cells/well), and transmigrated to
the basolateral side within 18 hours (approx. 40,000 cells/well),
when stimulated with 1 ng/ml monocyte chemotactic protein-1.
Soluble amyloidβ
(1-42) (100 ng/ml) significantly enhanced the adhesion
and migration of monocytes after 90 min, which was modulated
by antibodies against platelet-endothelial cell adhesion molecule-1,
intracellular adhesion molecule-1, receptor for advanced glycosylation
end products and low density lipoprotein-related protein-1
but not vascular cell adhesion molecule-1. Addition of aggregated
amyloidβ
(1-42) to the basolateral side potentiated the transmigration
of monocytes. In conclusion, aggregated amyloidβ
(1-42) stimulates the transmigration of monocytes through
a BBB, which is of importance in Alzheimers disease.
[Back to top]
Hemoglobin Neurotoxicity is Attenuated by Inhibitors of the
Protein Kinase CK2 Independent of Heme Oxygenase Activity
Jing Chen-Roetling, Zhi Li and Raymond
F. Regan
The heme oxygenase (HO) enzymes catalyze the rate-limiting
step of heme breakdown, and may accelerate oxidative injury
to neurons exposed to heme or hemoglobin. HO-1 and HO-2 are
activated in vitro by the phosphatidylinositol 3-kinase
(PI3K)/Akt and protein kinase C (PKC)/CK2 pathways, respectively.
The present study tested the hypotheses that CK2, PKC, and
PI3K inhibitors would reduce both HO activity and neuronal
vulnerability to hemoglobin in murine cortical cultures. Oxidative
cell injury was quantified by LDH release and malondialdehyde
assays. HO activity was assessed by carbon monoxide assay.
Consistent with prior observations, treating primary cortical
cultures with hemoglobin for 16h resulted in release of approximately
half of neuronal LDH and a seven-fold increase in malondialdehyde.
Both endpoints were significantly reduced by the CK2 inhibitors
4,5,6,7-tetrabromobenzotriazole (TBB) and 2-dimethyl-amino-4,5,6,7-tetrabromo-1H-benzimidazole
(DMAT), and by the PKC inhibitor GF109203X; the PI3K inhibitors
LY294002 and wortmannin had no effect. None of these inhibitors
altered basal HO activity. The 1.9-fold activity increase
observed after hemoglobin treatment was largely prevented
by LY294002 and LY303511, a structural analog of LY294002
that does not inhibit PI3K activity. It was not reduced by
wortmannin, TBB or GF109203X. These results suggest that the
protective effect of CK2 and PKC inhibitors in this model
is not dependent on reduction in HO activity. In this culture
system that expresses both HO-1 and HO-2, HO activity does
not appear to be primarily regulated by the PKC/CK2 or PI3K
pathways.
[Back to top]
Neurofibrillary Tangles and Senile Plaques in Alzheimer’s
Brains are Associated with Reduced Capillary Expression of
Vascular Endothelial Growth Factor and Endothelial Nitric
Oxide Synthase
John Provias and Brian Jeynes
There is significant evidence to suggest that a dysfunctional
blood-brain barrier [BBB] may contribute to the pathogenesis
of some Alzheimer’s disease [AD] lesions. An indicator
for this could be diminished capillary vascular endothelial
growth factor [VEGF] and / or endothelial nitric oxide synthase
[eNOS] activity in AD brains. Cortical samples were taken
from the superior temporal and calcarine cortices of ten confirmed
AD and ten non-demented comparison brains. Contiguous coronal
sections were stained using immunohistochemistry techniques
to stain for tau protein, beta- amyloid [Aβ]
n-termini [40 & 42],
VEGF and eNOS. Standardized regions of cortex were randomly
selected. Areas of ten contiguous field-diameters of comparable
and full cortical widths were observed in each section and
the densities of neurofibrillary tangles [NFTs], senile plaques
[SPs] and Aβ,
VEGF and eNOS positive capillaries were recorded. In both
AD cortices there were significant inverse correlations
found between both VEGF and eNOS-positive microvessels and
the presence of NFTs, and each of the amyloid isoforms in
SPs and amyloid-positive capillaries [p < 0.01]. In addition
there was a significant positive correlation between
VEGF and eNOS densities in both cortices [p< 0.01].These
results suggest that diminished VEGF and eNOS activity in
particularly lesion prone regions of AD brains may contribute
to the pathogenesis of NFT and / or SP lesions.
[Back to top]
Post Traumatic Lesion absence of β-Dystroglycan-Immunopositivity
in Brain Vessels Coincides with the Glial Reaction and the
Immunoreactivity of Vascular Laminin
Adrienn Szabó and Mihály
Kálmán
Following brain lesions, the gliovascular basal lamina
undergoes destruction and the gliovascular connections ‘decouple’.
Laminin receptors, as dystroglycan, are essential in these
processes. The present study compares the immunoreactivities
of β-dystroglycan,
glial fibrillary acidic protein (GFAP), and laminin following
stab wounds in adult rats. In intact brain the vessels were
immunopositive to β-dystroglycan,
whereas the laminin of their basal lamina proved to be unavailable
to immunoreactions. Following stab wound, however, the adjacent
vessels lost their immunopositvity to β-dystroglycan,
whereas immunopositivity to laminin became detectable in them.
In an advanced stage of glial reaction the territory of GFAP
immunopositive reactive astrocytes coincided with the area
where vessels lost their immuno-positivity to β-dystroglycan.
When glial reaction regressed, the β-dystroglycan
immunopositivity re-appeared, and laminin immunopositivity
became undetectable again. Post-lesional disappearance of
vascular β-dystroglycan
immunostaining was described earlier, and was attributed to
the cleavage of β-dystroglycan
by matrix metalloproteinases as a mechanism of the decoupling
of the gliovascular connections. Our results, which were obtained
in a different type of lesion support that the loss of vascular
β-dystroglycan
immunopositivity is a general phenomenon following cerebral
lesions, and an indirect marker of gliovascular decoupling.
For the first time coincidences were presented between vascular
immuno-negativity to β-dystroglycan,
glial reaction and detectability of laminin. Manifestation
of laminin immunoreactivity also indicates gliovascular decoupling.
Coincidence between glial reaction and lack of vascular β-dystroglycan
suggests mutual enhancement between them. The observations
may have clinico-pathologic importance since similar investigations
may help to follow the progression and regression of post-lesion
processes.
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