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CNS
& Neurological Disorders -Drug Targets
ISSN: 1871-5273
CNS & Neurological Disorders
- Drug Targets
Volume 6, Number 5, October 2007
Contents
Neural Stem Cell Therapies in Treating
Neurological Diseases in Adult Brain
Guest Editor: Kunlin Jin
Editorial Pp. 301-302
Neurogenesis in the Adult Brain: ImplicationAlzheimer’s
Disease Pp. 303-310
V. Galvan and D.E. Bredesen
[Abstract]
Regulation of Neurogenesis and Gliogenesis by Stress and Antidepressant
Treatment Pp. 311-320
M. Banasr and R.S. Duman
[Abstract]
Neurogenesis and Stroke Pp. 321-325
D.A. Greenberg
[Abstract]
Adult Neurogenesis and Parkinson’s Disease
Pp. 326-335
O. Arias-Carrión, N. Freundlieb, W.H. Oertel and
G.U. Höglinger
[Abstract]
Cellular Niches for Endogenous Neural Stem Cells in the Adult
Brain Pp. 336-341
J.D. Jordan, D.K. Ma, G.-L. Ming and H. Song
[Abstract]
Could Hippocampal Neurogenesis be a Future Drug Target for
Treating Temporal Lobe Epilepsy? Pp. 342-357
R. Kuruba and A.K. Shetty
[Abstract]
Neurotransmitter Regulation of Adult Neurogenesis: Putative
Therapeutic Targets Pp. 358-374
V.A. Vaidya, K.C. Vadodaria and S. Jha
[Abstract]
Abstracts
[Back to top]
Editorial
Correct diagnosis and effective treatment of diseases are
two essential tasks for a clinical doctor. With advancing
technology, the early and correct diagnosis of diseases is
getting easier; however, the treatment of most diseases remains
one of the biggest challenges for clinical medicine in 21st
century. Broadly speaking, the causes of human diseases can
be classified into two categories: abnormal cell death and
abnormal cell proliferation. Examples of the former are Alzheimer
disease and stroke, both of which cause cell death in the
brain. Cell death in different locations produces different
diseases. For example, Parkinson disease prdouces death of
cells in the substantia nigra, whereas Alzheimer disease prominently
affects the hippocampus and cerebral cortex. Abnormal cell
proliferation is a feature of cancer. Recent studies show
that cancer is initiated from cancer stem cells. In theory,
if we can find an approach to kill cancer stem cells, we can
cure cancer, and if we can induce stem cells to differentiate
into mature cells such as neurons, we will be able to replace
damaged neurons for therapy of neurodegenerative diseases.
Hence, stem cells are important medically both because of
the risk they pose in carcinogenesis, and for the potential
they offer for tissue regeneration or replacement.
Stem cells can be classified into embryonic stem cells (ESCs),
derived from blastocysts, and adult stem cells, which are
found in adult tissues. Both have two important characteristics
that distinguish them from other types of cells. First, they
are unspecialized cells that are able to renew themselves
through mitotic cell division. The second is that under certain
conditions, they can differentiate into a diverse range of
specialized cell types. Pluripotent ESCs can form cells of
all tissues of the adult organism and adult stem cells have
generally been regarded as having the capacity to form only
the cell types of the organ in which they are found; however
some adult stem cells may exhibit multipotency.
Although human ESCs, which were first generated from human
embryos in 1998, hold immense potential for therapeutic use
in cell therapy, they also have disadvantages. This is evident
in the proposed use of such cells to treat neurological diseases
by intracerebral transplantation. First, surgical transplantation
may result in local tissue damage or stroke. Second, the use
of human ESCs is ethically and politically controversial.
Third, neural degeneration in some CNS diseases is extensive,
multifocal or even global, which may require widespread replacement
beyond the capabilities of surgical transplantation. Finally,
intracerebral transplantation may be associated with adverse
effects related to the unregulated function of ectopic tissue.
It was thought for some time that the brains of adult mammals
do not generate new neurons, although Altman first observed
the proliferative potential of adult rodent brain in the 1960s.
After years of debate, it is now accepted that neural stem
cells are present in the rostral subventricular zone (SVZ)
surrounding the lateral ventricles and the subgranular zone
(SGZ) of the hippocampal dentate gyrus (DG) in adult mouse,
rat, non-human primate and human brain. Newly generated cells
in the SGZ can differentiate into mature, functional neurons
and integrate into the DG as granule cells, which are involved
in memory formation in normal brain. More interestingly, endogenous
neural stem cells in these discrete regions proliferate in
response to brain injuries such as stroke and neurodegerative
diseases such as Huntington’s diseases. These disease-induced
newborn cells can migrate into damaged brain regions, where
they differentiate into mature neuronal cells. Therefore,
it might be possible for damaged cells to be replaced from
endogenous neural stem cell pools. However, the innate capacity
for brain repair appears to be limited.
The successful development of neural stem cell recruitment
therapy will depend on our ability to manage the proliferation,
migration, differentiation, and functional integration of
recruited cells using pharmaceutical tools. To deliver on
the promise of neural stem cell research and potential neural
stem cell therapies for maintenance of healthy brain and repair
of central nervous system diseases, much additional work is
needed. This theme issue introduces the latest advances related
to neural stem cells in adult brain and in neurological diseases,
including the molecular mechanisms regulating neural stem
cells in normal brain and the biological behaviors of endogenous
neural stem cells in response to cerebral diseases. Hopefully,
this special issue will provide some valuable information
for development of new strategies to rebuild damaged tissues
by endogenous neural cell replacement.
Kunlin Jin
Buck Institute for Age Research
8001 Redwood Blvd.
Novato, CA 94949
USA
E-mail: kjin@buckinstitute.org
[Back to top]
Neurogenesis in the Adult Brain: Implications for Alzheimer’s
Disease
V. Galvan and D.E. Bredesen
The function of neurogenesis in the adult brain is still
unknown. Interventions such as environmental enrichment and
exercise impinge on neurogenesis, suggesting that the process
is regulated by experience. Conversely, a role for neurogenesis
in learning has been proposed through ‘cellular plasticity’,
a process akin to synaptic plasticity but operating at the
network level. Although neurogenesis is stimulated by acute
injury, and possibly by neurodegenerative processes such as
Alzheimer’s disease (AD), it does not suffice to restore
function. While the role and direction of change in the neurogenic
response at different stages of AD is still a matter of debate,
it is possible that a deficit in neurogenesis may contribute
to AD pathogenesis since at least one of the two regions ostensibly
neurogenic in the adult human brain (the subgranular zone
of the dentage gyrus and the ventriculo-olfactory neurogenic
system) support high-level functions affected in early AD
(associative memory and olfaction respectively). The age of
onset and the rate of progression of sporadic forms of AD
are highly variable. Sporadic AD may have a component of insufficient
neurogenic replacement or insufficient neurogenic stimulation
that is correlated with traits of personal history; the rate
of neurogenesis and the survival of replicating progenitors
is strongly modified by behavioral interventions known to
impinge on the rate of neurogenesis and the probability of
survival of newly born neurons – exercise, enriched
experience, and learning. This view is consistent with epidemiological
data suggesting that higher education and increased participation
in intellectual, social and physical aspects of daily life
are associated with slower cognitive decline in healthy elderly
(“cognitive reserve”) and may reduce the risk
of AD. Although neurogenesis can be modulated exogenously
by growth factors, stimulation of neurogenesis as a mean to
treat neurodegeneration is still for the most part speculative.
Moreover, it is possible that different roles of neurogenesis
during the course of AD are dictated by the degree of permissibility
of the environment in which the process is taking place. A
unique opportunity may exist in which the therapeutic stimulation
of neurogenesis might contribute to functional ‘repair’
of the adult diseased brain, before damage to whole neuronal
networks has ensued. In spite of the considerable gaps in
our knowledge of neurogenesis, and of the considerable limitations
that will need to be overcome before we can intervene in the
process, that new neurons are added continuously to the adult
mammalian brain is a discovery that has already changed the
way we think about neurobiology, and may soon change the way
we understand and approach neurodegenerative diseases such
as AD.
[Back to top]
Regulation of Neurogenesis and Gliogenesis by Stress and Antidepressant
Treatment
M. Banasr and R.S. Duman
Structural and morphological changes in limbic brain
regions are associated with depression, chronic stress and
antidepressant treatment, and increasing evidence supports
the hypothesis that dysregulation of cell proliferation contributes
to these effects. We review the morphological alterations
observed in two brain regions implicated in mood disorders,
the prefrontal cortex and hippocampus, and discuss the similarities
and differences of the cellular consequences of chronic stress.
We briefly discuss the proposed mechanisms implicated in neuroplasticity
impairments that result from stress and that contribute to
mood disorders, with a particular interest in adult neurogenesis
and gliogenesis. This information has contributed to novel
antidepressant medication development that utilizes adult
neurogenesis and gliogenesis as preclinical cellular markers
for predicting antidepressant properties of novel compounds.
[Back to top]
Neurogenesis and Stroke
D.A. Greenberg
Stroke stimulates neurogenesis in select regions of the
adult brain, and the newborn neurons that result can migrate
to areas of ischemic injury, where they may have the capacity
to enhance brain recovery. These observations suggest that
stroke-induced neurogenesis may contribute to endogenous brain
repair after stroke, and that the mechanisms that underlie
neurogenesis may represent potential therapeutic targets.
Alternatively, transplantation of exogenously derived neural
cells might also be an approach to the treatment of stroke.
[Back to top]
Adult Neurogenesis and Parkinson’s Disease
O. Arias-Carrión, N. Freundlieb, W.H. Oertel and
G.U. Höglinger
Parkinson’s disease is a neurodegenerative disorder
characterized by a progressive neuronal loss affecting preferentially
the dopaminergic neurons of the nigrostriatal projection.
Transplantation of fetal dopaminergic precursor cells has
provided the proof of principle that a cell replacement therapy
can ameliorate clinical symptoms in affected patients. Recent
years have provided evidence for the existence of neural stem
cells with the potential to produce new neurons, particularly
of a dopaminergic phenotype, in the adult mammalian brain.
Such stem cells have been identified in so called neurogenic
brain areas, where neurogenesis is constitutively ongoing,
but also in primarily non-neurogenic areas, such as the midbrain
and the striatum, where neurogenesis does not occur under
normal physiological conditions. We review here presently
published evidence to evaluate the concept that endogenous
neural stem cells may have the potential to be instrumentalized
for a non-invasive cell replacement therapy with autologous
neurons to repair the damaged nigrostriatal dopaminergic projection
in Parkinson’s disease.
[Back to top]
Cellular Niches for Endogenous Neural Stem Cells in the Adult
Brain
J.D. Jordan, D.K. Ma, G.-L. Ming and H. Song
Neural stem cells are present throughout life and continuously
give rise to new neurons and glia cells in the mammalian central
nervous system. Accumulating evidence suggests essential roles
of micro-environments, or niches, in supporting active neurogenesis
from endogenous neural stem cells within restricted regions
of the adult brain. These neurogenic niches also regulate
different steps of adult neurogenesis in response to physiological
and pathological stimulations. Recent studies have identified
several cellular niche components, including endothelial cells,
astroglia, ependymal cells, immature progeny of NSCs and mature
neurons. In this review, we discuss identified niche signals
from these cellular components in regulating different steps
of adult neurogenesis. We also highlight some of the potential
therapeutic targets to be manipulated within neurogenic niche
for repair of the adult central nervous system.
[Back to top]
Could Hippocampal Neurogenesis be a Future Drug Target for
Treating Temporal Lobe Epilepsy?
R. Kuruba and A.K. Shetty
The dentate gyrus, a region of the hippocampal formation,
displays the highest level of plasticity in the brain and
exhibits neurogenesis all through life. Dentate neurogenesis,
believed to be essential for learning and memory function,
responds to physiological stimuli as well as pathological
situations. The role of dentate neurogenesis in the pathophysiology
of temporal lobe epilepsy (TLE) has received increased attention
lately because of its disparate response in the early and
chronic stages of the disease. Acute seizures or status epilepticus
immensely enhance dentate neurogenesis and lead to an aberrant
migration of newly born neurons into the dentate hilus and
the formation of epileptogenic circuitry in the injured hippocampus.
Conversely, spontaneous recurrent seizures that arise during
chronic TLE are associated with dramatically reduced dentate
neurogenesis. In this review, we discuss the potential significance
of enhanced but abnormal neurogenesis taking place shortly
after brain injury or the status epilepticus towards the development
of chronic epilepsy, and prospective implications of dramatically
waned dentate neurogenesis occurring during chronic epilepsy
for learning and memory function and depression in TLE. Furthermore,
we confer whether hippocampal neurogenesis is a possible drug
target for preventing TLE after brain injury or the status
epilepticus, and for easing learning and memory impairments
during chronic epileptic conditions. Additionally, we discuss
some possible drugs and approaches that need to be evaluated
in future in animal models of TLE to further understand the
role of neurogenesis in the pathogenesis of TLE and whether
modulation of neurogenesis is useful for treating TLE.
[Back to top]
Neurotransmitter Regulation of Adult Neurogenesis: Putative
Therapeutic Targets
V.A. Vaidya, K.C. Vadodaria and S. Jha
The evidence that new neuron addition takes place in
the mammalian brain throughout adult life has dramatically
altered our perspective of the potential for plasticity in
the adult CNS. Although several recent reports suggest a latent
neurogenic capacity in multiple brain regions, the two major
neurogenic niches that retain the ability to generate substantial
numbers of new neurons in adult life are the subventricular
zone (SVZ) lining the lateral ventricles and the subgranular
zone (SGZ) in the hippocampal formation. The discovery of
adult neurogenesis has also unveiled a novel therapeutic target
for the repair of damaged neuronal circuits. In this regard,
understanding the endogenous mechanisms that regulate adult
neurogenesis holds promise both for a deeper understanding
of this form of structural plasticity, as well as the identification
of pathways that can serve as therapeutic targets to manipulate
adult neurogenesis. The purpose of the present review is to
discuss the regulation of adult neurogenesis by neurotransmitters
and to highlight the relevance of these endogenous regulators
as targets to modulate adult neurogenesis in a clinical context.
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