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Current
Gene Therapy
ISSN: 1566-5232
Current Gene Therapy
Volume 11, Number 2,
April 2011
Contents
Hot Topic
Gene Therapy Approaches for Neuroregeneration
Guest Editor: Kirsten Haastert-Talini
Editorial: Pp. 74
Gene Therapy for the Peripheral Nervous System:
A Strategy to Repair the Injured Nerve? Pp. 75-89
Matthew R.J. Mason, Martijn R. Tannemaat, Martijn J.A.
Malessy and Joost Verhaagen
[Abstract] [Purchase
Article]
Cell Adhesion Molecules in Gene and Cell Therapy Approaches
for Nervous System Repair Pp. 90-100
Alexandros A. Lavdas, Florentia Papastefanaki, Dimitra
Thomaidou and Rebecca Matsas
[Abstract] [Purchase
Article]
Gene Therapy Approaches for Neuroprotection and Axonal
Regeneration after Spinal Cord and Spinal Root Injury
Pp. 101-115
Xuenong Bo, Dongsheng Wu, John Yeh and Yi Zhang
[Abstract] [Purchase
Article]
Retinal Ganglion Cell Gene Therapy and Visual System
Repair Pp. 116-131
Mats Hellström and Alan R. Harvey
[Abstract] [Purchase
Article]
General Articles
Therapies for Neurological Disease in the Mucopolysaccharidoses
Pp. 132-143
Donald S. Anson, Chantelle McIntyre and Sharon
Byers
[Abstract] [Purchase
Article]
Optimization of Lentiviral Vectors Generation for
Biomedical and Clinical Research Purposes: Contemporary Trends
in Technology Development and Applications Pp. 144-153
Pankaj Kumar and Chan Woon-Khiong
[Abstract] [Purchase
Article]
Abstracts
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Editorial: Gene Therapy Approaches for
Neuroregeneration
The better the understanding of cellular and molecular
events involved in nervous system degeneration and regeneration
became during the last decades, the more likely have gene
therapy approaches become to improve nervous system regeneration
and to find their position in clinical settings. Gene therapy
based strategies for neuroregeneration mainly aim to provide
target specific neurotrophic support to enhance viability
of diseased or trauma-affected neurons [1, 2]. In addition
to support of neuronal survival, axonal regeneration across
long distances and re-establishment of functional circuits
are needed for successful repair of peripheral and central
nervous system deficits. Therefore not only the introduction
of genes directly into the neuronal or glial target cells
with the aim to support their survival and functionality but
also the transplantation of genetically modified supportive
cells have reached the level of clinical research [3, 4].
With this special issue we want to give insight in gene therapeutic
approaches targeting the injured peripheral nervous system,
the injured dorsal root entry zone and spinal cord as well
as the inner retina. Four comprehensive reviews discuss current
developments in biotechnology as well as the most promising
strategies to include gene therapy into combinatory therapeutic
treatments to restore peripheral as well as central nervous
system functions. Furthermore, advantages as well as limitations,
especially regarding the clinical application of gene therapy
of the lesioned nervous system, are reviewed. Because use
of viral vectors has been shown to be the most efficient way
to introduce the expression of potentially therapeutic gene
products into the nervous system, a special focus has been
put on viral vector systems like adeno associated and lentiviral
vectors.
The first contribution by Mason et al.
discusses efforts to develop gene therapy as an adjunct strategy
to promote peripheral nerve regeneration following neurosurgical
repair which alone often cannot avoid a considerable degree
of functional impairment. Viral-based gene transfer strategies
are reviewed and analyzed regarding their potential to enforce
the regeneration outcome and their clinical applicability.
While Mason et al. mainly describe the introduction of neurotrophic
support for neuroregeneration, the second review by Lavdas
et al. gives insights on the promising genetic
manipulation of cell adhesion molecules in the peripheral
as well as central nervous system. Cell adhesion molecules
are crucial players in axonal pathfinding and formation of
functional circuits which makes them along with neurotrophic
factors the most promising candidates to help long distance
axonal regeneration and appropriate target reinnervation.
Bo et al. provide up-to-date information
on the in vivo, ex vivo and combinatorial
gene delivery of a wide range of therapeutic molecules to
overcome the non-permissive properties that are inhibiting
axonal regeneration after spinal root and spinal cord injury.
Thus the third review clearly demonstrates, how experimental
gene transfer could pave way for the development of new therapeutic
strategies.
The mammalian visual system, in particular the eye and the
optic nerve, are widely used for experimental studies to investigate
the cellular and molecular mechanisms of central nervous system
injury and repair. As a matter of course the current state
of viral-based gene transfer techniques to target inner retinal
neurons are provided by the fourth review from Hellström
and Harvey. This review therefore covers another
important and evolving field of gene therapy approaches in
neuroregeneration that has so far received less attention
than gene delivery to the outer retina for the treatment of
deficits in photoreceptor and retinal epithelium function
[5].
This special issue was set up to provide an overview on cutting-edge
developments in gene transfer technology that will in the
future hopefully enable successful regeneration within the
different parts of the nervous system presented. It was a
great pleasure to work with the authors and I highly appreciate
the dedication and expert knowledge they contributed to this
special issue.
REFERENCES
[1] Zacchigna S, Giacca M. Chapter 20: Gene therapy perspectives
for nerve repair. Int Rev Neurobiol 2009; 87: 381-92.
[2] Lim ST, Airavaara M, Harvey BK. Viral vectors for neurotrophic
factor delivery: a gene therapy approach for neurodegenerative
diseases of the CNS. Pharmacol Res 2010; 61(1): 14-26.
[3] Gogel S, Gubernator M, Minger SL. Progress and prospects:
stem cells and neurological diseases. Gene Ther 2011; 18(1):
1-6.
[4] Madduri S, Gander B. Schwann cell delivery of neurotrophic
factors for peripheral nerve regeneration. J Peripher Nerv
Syst 2010; 15(2): 93-103.
[5] den Hollander AI, Black A, Bennett J, Cremers FP. Lighting
a candle in the dark: advances in genetics and gene therapy
of recessive retinal dystrophies. J Clin Invest 2010; 120(9):
3042-53.
Dr. Kirsten Haastert-Talini
Guest Editor
Current Gene Therapy
Institute for Neuroanatomy
Hannover Medical School, Carl-Neuberg-Str.1, D-30625 Hannover
Germany
Email: haastert.kirsten@mh-hannover.de
Web: http://www.mh-hannover.de/15681.html
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Gene Therapy for the Peripheral Nervous System:
A Strategy to Repair the Injured Nerve?
Matthew R.J. Mason, Martijn R. Tannemaat, Martijn J.A.
Malessy and Joost Verhaagen
Peripheral nerve injury in humans often leads to incomplete
functional recovery. In this review we discuss the potential
for gene therapy to be used as a strategy alongside surgical
repair techniques for the study of peripheral nerve regeneration
in rodent models and with a view to its eventual use for the
promotion of successful regeneration in the clinic. Gene therapy
vectors based on herpes simplex virus, adenovirus, lentivirus
and adeno-associated virus have been developed to deliver
genes to the neurons of the peripheral nervous system, i.e.
primary sensory neurons in the dorsal root ganglia and primary
motor neurons. Adenoviral and lentiviral vectors have also
been used to transduce Schwann cells and fibroblasts in the
injured nerve. We present an overview of these vectors, their
application so far in the peripheral nervous system, their
potential as vectors for enhancing peripheral nerve repair,
and the successful interventions that have been demonstrated
in animal models. We also discuss some of the limitations
of current vectors and how they may be over-come. While the
technology for gene delivery is approaching a state of readiness
for clinical translation, the current range of therapeutic
genes for the repair of the traumatically injured peripheral
nerve is mostly limited to neurotrophic factors delivered
to neurons, Schwann cells or possibly the target organs. Finally,
therefore, we consider what type of therapeutic transgene
may be desirable to enhance nerve regeneration in the future.
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Article]
Cell Adhesion Molecules in Gene and Cell Therapy Approaches
for Nervous System Repair
Alexandros A. Lavdas, Florentia Papastefanaki, Dimitra
Thomaidou and Rebecca Matsas
The inability of the central nervous system (CNS) to efficiently
repair damages results in severe functional impairment after
trauma or neurodegenerative / demyelinating diseases. Regeneration
failure is attributed to inhibitory molecules creating a nonpermissive
environment for axonal regrowth, and dictates the necessity
for the development of novel therapeutic strategies. An emerging
approach for improving regeneration is the use of gene therapy
to manipulate cell adhesion molecule expression in experimental
animal models of degeneration. Alternatively, cell transplantation
to replace lost neurons and the grafting of myelinating cells
to repair demyelinating lesions are promising approaches for
treating CNS injuries and demyelination. Schwann cells (SCs),
oligodendrocyte progenitors, olfactory ensheathing cells and
embryonic and neural stem cells have been shown to form myelin
after transplantation into the demyelinated CNS. The repair
capacity of the peripheral nervous system (PNS) is much higher,
but there is still a limit to the amount of nerve loss that
can be bridged after injury, and longer nerve gaps call for
the use of conduits populated with living cells. In both cases,
the interaction of grafted cells with the host environment
is of paramount importance for the incorporation and functional
integration of these cells and the manipulation of cell adhesion
molecules is an attractive approach towards achieving this
goal. In this review we summarize data from the recent literature
regarding the manipulation of cell adhesion molecule expression
towards CNS and PNS repair and discuss the prospects for future
therapeutic applications.
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Article]
Gene Therapy Approaches for Neuroprotection and Axonal
Regeneration after Spinal Cord and Spinal Root Injury
Xuenong Bo, Dongsheng Wu, John Yeh and Yi Zhang
Recent understanding in pathophysiological mechanisms of spinal
cord and spinal root injuries has facilitated the development
of new strategies to promote neural repair. Gene therapy approaches
have been viewed as the ideal means to achieve long-term local
delivery of therapeutic molecules in the central nervous system
(CNS). Ex vivo gene delivery offers the additional
advantage of providing cellular support for regenerating axons.
In this review, we summarize the studies on viral vector-mediated
gene delivery to spinal cord in animal models, both in
vivo and ex vivo. Most of the studies reported
so far are aimed at delivery of various growth factors, such
as neurotrophins and neuropoietic cytokines. Other molecules
tested include those that interfere with intracellular processes
to prevent cell death, or increase intrinsic regenerating
state of injured neurons, or modify the CNS environment to
make it permissive for axon growth. Several different combinatorial
strategies involving gene delivery are also discussed as it
has been recognized that successful neural repair may require
the synergistic actions of multiple therapeutic managements.
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Retinal Ganglion Cell Gene Therapy and Visual System
Repair
Mats Hellström and Alan R. Harvey
Recent clinical trials have shown that the use of replication
deficient viral vectors to genetically modify cells in the
retina can be of therapeutic benefit in the treatment of certain
inherited degenerative conditions that compromise photoreceptor,
and hence visual, function. This review is focussed primarily
on the use of recombinant adeno-associated viral (rAAV) vectors
to target neurons in inner retina, specifically retinal ganglion
cells (RGCs). Genetic modification of RGCs may be of value
in various ophthalmic conditions in which there is documented
loss of RGCs or damage to their centrally projecting axons.
Such conditions include glaucoma, optic neuritis, vascular
disruption or trauma, and neurological degenerative conditions
such as Alzheimer’s disease. Furthermore, because the
retina and optic nerve (ON) form part of the CNS, the visual
system is a useful experimental model in which to study the
molecular and cellular mechanisms that underlie degenerative
as well as regenerative responses of adult CNS neurons after
injury. Gene therapy studies from a number of laboratories
are first reviewed, involving not only rAAV-based treatments
but also application of lentiviral and adenoviral vectors.
Recent work from our own laboratory is then summarized, in
which intravitreal injection of rAAV2 sero-type vectors is
used to introduce growth promoting genes into injured RGCs.
rAAV encoding a secretable form of ciliary neurotrophic factor
(CNTF) has proved to be particularly effective in promoting
RGC survival and axon regeneration after optic nerve crush
or after transection followed by a peripheral nerve autograft.
In the latter situation we have found that RGCs and their
regenerated axons are maintained for at least 15 months after
the initial injury. We have also combined rAAV gene therapy
with pharmacotherapy to determine if cAMP elevation and additional
intravitreal injections of growth factors can act synergistically
with vector-based delivery of growth-promoting genes.
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Therapies for Neurological Disease in the Mucopolysaccharidoses
Donald S. Anson, Chantelle McIntyre and Sharon
Byers
Intravenous enzyme replacement therapy has been developed
as a viable treatment for most of the somatic pathologies
associated with the mucopolysaccharide storage disorders.
However, approximately two thirds of individuals affected
by a mucopolysaccharide storage disorder also display neurological
disease, in these instances intravenous enzyme replacement
therapy is not viable as the blood-brain barrier severely
limits enzyme distribution from the peripheral circulation
into the central nervous system. Accordingly, much research
is now focussed on developing therapies that specifically
address neurological disease, or somatic and neurological
disease in combination. Therapies designed to address the
underlying cause of central nervous system pathology, that
is the lysosomal storage itself, can be broadly divided into
two groups, those that continue the rationale of enzyme replacement,
and those that address the supply side of the storage equation;
that is the production of storage material. Enzyme replacement
can be further divided by technology (principally direct enzyme
replacement, gene replacement and cell transplantation). Here
we review the current state of the art for these strategies
and suggest possible future directions for research in this
field. In particular, we suggest that any one approach in
itself is unlikely to be as efficacious as a carefully considered
combination therapy, be it a combination of some sort of enzyme
replacement with substrate deprivation, or a combination of
two different replacement technologies or strategies.
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Optimization of Lentiviral Vectors Generation for
Biomedical and Clinical Research Purposes: Contemporary Trends
in Technology Development and Applications
Pankaj Kumar and Chan Woon-Khiong
Classical non-viral methods of gene transfer, such as chemical
transfection, have met with limited success of instillation
of genetic material into non-proliferating cells in vitro.
Among the different kinds of viral vectors, Lentiviral vectors
(LVs) have emerged as robust and versatile tool for ex
vivo and in vivo gene delivery into multiple
cell types including non-dividing cells such as neurons. The
capacity of LVs to maintain stable, long-term transgene expression
and the substantial flexibility in the design of the expression
cassettes account for their increasing use in various pre-clinical
and clinical applications. Additionally, LVs have been hugely
successful in reprogramming induced pluripotent stem cells
(iPSCs). Recent development using LVs in conjunction with
a Cre-Lox based reversible system has opened up many new possibilities
towards therapeutic application of iPSC technology in various
clinical settings. Moreover, improvements in term of biosafety
and efficacy, achieved either by modifying the vector design
or by involving integration-deficient LVs (IDLVs), have important
implications for adoption of LV as the vector of choice for
clinical trials. Several human gene therapy clinical trials
evaluating the use of LVs for treatment of human diseases
such as Parkinson’s disease, β-thalassemia,
X-linked adrenoleukodystrophy (ALD), and AIDS are currently
ongoing. This review will describe the state of the art achieved
by LV technology, its impact on biomedical research, and implications
to human clinical trials as therapeutic gene delivery vehicle
for a wide range of infectious and genetic diseases.
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