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Current
Gene Therapy
ISSN: 1566-5232
Current Gene Therapy
Volume 6, Number 2, April 2006
Contents
Gene Therapy for Cystic Fibrosis Airway Disease-
Is Clinical Success Imminent? Pp. 161-179
Donald S. Anson, Gregory J. Smith and David W.
Parsons
[Abstract]
Immuno-Isolation in Cancer Gene Therapy
Pp. 181-191
Pasquale Cirone, Murray Potter, Hal Hirte and Patricia Chang
[Abstract]
Basic and Clinical Aspects of Gene Therapy for
Retinopathy Induced by Diabetes Pp. 193-214
Julia Ho Yee Ting and Donald Keith Martin
[Abstract]
Current Strategies and Future Directions for Eluding
Adenoviral Vector Immunity Pp. 215-226
Dinesh S. Bangari and Suresh K. Mittal
[Abstract]
Cell and Gene-Based Therapies for the Lysosomal
Storage Diseases Pp. 227-241
Bradley L. Hodges and Seng H. Cheng
[Abstract]
Electroporation-Enhanced Nonviral Gene Transfer
for the Prevention or Treatment of Immunological, Endocrine
and Neoplastic Diseases Pp. 243-273
Gérald J. Prud’homme, Yelena Glinka,
Amir S. Khan and Ruxandra Draghia-Akli
[Abstract]
Abstracts
[Back to top]
Gene Therapy for Cystic Fibrosis Airway Disease- Is
Clinical Success Imminent?
Donald S. Anson, Gregory J. Smith and David
W. Parsons
Cystic fibrosis (CF) was one of the first inherited disorders
for which gene therapy was seriously considered as a realistic
option for treatment, and as such, it has long provided a
paradigm for gene therapy of inherited diseases. However,
despite the cloning of the cystic fibrosis transmembrane conductance
regulator gene in 1989, over 15 years later a practical gene
therapy for CF has not eventuated. There are a number of reasons
for this, and analysis of the specific issues that have delayed
the successful development of gene therapy for CF also provides
general insights into the practical complexities involved
in the development of gene therapy for inherited disorders.
The issues which have prevented the application of gene therapy
for CF to date include the lack of suitable gene delivery
technologies, the complexities of the interactions between
the host and vector, the biology of the lung airways, and
the nature of the pathology found in individuals with CF.
We will discuss the history of CF gene therapy with specific
reference to these and other issues that preoccupy the field
at present: namely, the question of what vectors appear to
be suitable for airway gene delivery in CF, what cells must
be targeted, how airway epithelium defences can be overcome
or eluded to allow efficient gene delivery, how to ensure
safe and long-term transgene expression and the need to identify
relevant surrogate success measures that can be used to assess
the outcome of gene therapy in CF patients.
[Back to top]
Immuno-Isolation in Cancer Gene Therapy
Pasquale Cirone, Murray Potter, Hal Hirte and Patricia Chang
The implantation of genetically-modified non-autologous
cells in immuno-protected microcapsules is an alternative
to ex vivo gene therapy. Such cells delivering a
recombinant therapeutic product are isolated from the host’s
immune system by being encapsulated within permselective microcapsules.
This approach has been successful in pre-clinical animal studies
involving delivery of hormone or enzymes to treat dwarfism,
lysosomal storage disease, or hemophilia B. Recently, this
platform technology has shown promise in the treatment for
more complex diseases such as cancer. One of the earliest
strategy was to augment the chemotherapeutic effect of a prodrug
by implanting encapsulated cells that can metabolise prodrugs
into cytotoxic products in close proximity to the cancer cells.
More recent approaches include enhancing tumor cell death
through immunotherapy, or suppressing tumor cell proliferation
through anti-angiogenesis. These can be achieved by delivering
single molecules of cytokines or angiostatin, respectively,
by implanting microencapsulated cells engineered to secrete
these recombinant products. Recent refinements of these approaches
include genetic fusion of cytokines or angiostatin to additional
functional groups with tumor targeting or tumor cell killing
properties, thus enhancing the potency of the recombinant
products. Furthermore, a COMBO strategy of implanting microencapsulated
cells to deliver multiple products targeted to diverse pathways
in tumor suppression also showed much promise. This review
will summarise the application of microencapsulation of genetically-modified
cells to cancer treatment in animal models, the efficacy of
such approaches, and how these studies have led to better
understanding of the biology of cancer treatment. The flexibility
of this modular system involving molecular engineering, cellular
genetic modification, and polymer chemistry provides potentially
a huge range of application modalities, and a tremendous multi-disciplinary
challenge for the future.
[Back to top]
Basic and Clinical Aspects of Gene Therapy for Retinopathy
Induced by Diabetes
Julia Ho Yee Ting and Donald Keith Martin
Diabetes mellitus invariably induces retinopathy which
causes a loss of vision that is the major cause of blindness
in people of working age across most ethnic groups. Although
there have been major advances in gene therapy technologies,
there is still no effective cure-all gene therapy for diabetes
mellitus. This may be due to (i) involvement of multiple
genes that may have different influences on diabetes across
different ethnic groups, (ii) immune response to
viral vectors, (iii) local, specific transfection
only and not into systemic circulation, (iv) lack
of stable long-term expression, and (v) lack of control
of gene expression. Hence, a separate approach to gene therapy
of diabetic retinopathy is necessary due to the difficulties
in treating the underlying diabetes.
Diabetic retinopathy is the inevitable microvascular complication
in the retina from diabetes mellitus. There are possible genetic
bases in several pathophysiological pathways for diabetic
retinopathy, including oxidation of retinal cells, polyol
accumulation pathways, increased non-enzymatic glycation in
retinal cells and the release of growth factors by endothelial
cells.
We review the candidate genes in these putative pathways for
diabetic retinopathy and discuss the challenges for gene therapy.
The eye is an isolated system with a strong blood-retinal
barrier and therefore provides a challenge for delivery of
drugs and vectors from the systemic circulation using traditional
approaches. Newer delivery approaches include the use of nanoparticles,
liposomes, and iontophoresis.
We also consider the social and health economic dimension
of diabetic retinopathy gene therapy. Diabetic retinopathy
is the most common cause of blindness for people of working
age. The loss of visual acuity caused by diabetic retinopathy
creates a detrimental impact on the patient’s quality
of life. This results in quality-of-life costs to the individual,
the health care system and to society. Significant progress
has been made in gene therapy approaches for diabetic retinopathy,
and it appears that this is an important area for continued
research in order to improve visual outcomes and reduce the
healthcare costs of diabetic retinopathy in our communities.
[Back to top]
Current Strategies and Future Directions for Eluding
Adenoviral Vector Immunity
Dinesh S. Bangari and Suresh K. Mittal
Adenoviral (Ad) vectors can efficiently transduce a broad
range of cell types and have been used extensively in preclinical
and clinical studies for gene delivery applications. The presence
of preexisting Ad immunity in the majority of human population
and a rapid development of immune response against the Ad
vector backbone following the first inoculation with the vector
have impeded clinical use of these vectors. In addition, a
number of animal inoculation studies have demonstrated that
high systemic doses of Ad vectors invariably lead to initiation
of acute inflammatory responses. This is mainly due to activation
of innate immunity by vector particles. In general, vector
and innate immune responses drastically limit the vector transduction
efficiency and the duration of transgene expression. In order
to have a predictable response with Ad vectors for gene therapy
applications, the above limitations must be overcome. Strategies
that are being examined to circumvent these drawbacks of Ad
vectors include immunosuppression, immunomodulation, serotype
switching, use of targeted Ad vectors, microencapsulation
of Ad vectors, use of helper-dependent (HD) Ad vectors, and
development of nonhuman Ad vectors. Here we review the current
understanding of immune responses to Ad vectors, and recent
advances in the strategies for immune evasion to improve the
vector transduction efficiency and the duration of transgene
expression. Development of novel strategies for targeting
specific cell types would further boost the utility of Ad
vectors by enhancing the safety, efficacy and duration of
transgene expression.
[Back to top]
Cell and Gene-Based Therapies for the Lysosomal Storage
Diseases
Bradley L. Hodges and Seng H. Cheng
Lysosomal storage disorders (LSD) are a group of approximately
40 genetic diseases that are caused by the deficiency of one
or more lysosomal enzymes. The incidence of LSD is estimated
to be approximately 1 in 7500 live births, which makes this
one of the more prevalent groups of genetic diseases in humans.
The loss in enzymatic activity leads to the accumulation of
undegraded substrates within lysosomes, resulting in distension
of the organelle and subsequent cellular malfunction. Although
palliative treatments such as enzyme replacement therapy (ERT)
or substrate reduction therapy (SRT) have been shown to be
effective for some of the LSD such as Gaucher, Fabry and MPS
I, they are not available as yet, or ineffective, for a large
number of other LSD patients. To fulfill this unmet medical
need, gene therapy is being considered as an alternate or
adjunctive therapy for this group of disorders. A goal of
gene therapy for LSD is to introduce a normal copy of the
DNA for the lysosomal enzyme into a depot organ such as the
liver or muscle with the intent that this will lead to the
sustained production and reconstituion of therapeutic levels
of the enzyme in the affected tissues. Here, we review the
utility of various gene therapy strategies under consideration
for the treatment of the LSD, including viral and non-viral
gene transfer approaches, as well as stem cell transplantation.
[Back to top]
Electroporation-Enhanced Nonviral Gene Transfer for
the Prevention or Treatment of Immunological, Endocrine and
Neoplastic Diseases
Gérald J. Prud’homme, Yelena Glinka,
Amir S. Khan and Ruxandra Draghia-Akli
Nonviral gene transfer is markedly enhanced by the application
of in vivo electroporation (also denoted electrogene
transfer or electrokinetic enhancement). This approach is
safe and can be used to deliver nucleic acid fragments, oligonucleotides,
siRNA, and plasmids to a wide variety of tissues, such as
skeletal muscle, skin and liver. In this review, we address
the principles of electroporation and demonstrate its effectiveness
in disease models. Electroporation has been shown to be equally
applicable to small and large animals (rodents, dogs, pigs,
other farm animals and primates), and this addresses one of
the major problems in gene therapy, that of scalability to
humans. Gene transfer can be optimized and tissue injury minimized
by the selection of appropriate electrical parameters. We
and others have applied this approach in preclinical autoimmune
and/or inflammatory diseases to deliver either cytokines,
anti-inflammatory agents or immu-noregulatory molecules. Electroporation
is also effective for the intratumoral delivery of therapeutic
vectors. It strongly boost DNA vaccination against infectious
agents (e.g., hepatitis B virus, human immunodeficiency
virus-1) or tumor anti-gens (e.g., HER-2/neu, carcinoembryonic
antigen). In addition, we found that electroporation-enhanced
DNA vaccination against islet-cell antigens ameliorated autoimmune
diabetes. One of the most likely future applications, however,
may be in intramuscular gene transfer for systemic delivery
of either endocrine hormones (e.g., growth hormone
releasing hormone and leptin), hematopoietic factors (e.g.,
erythropoietin, GM-CSF), antibodies, enzymes, or numerous
other protein drugs. In vivo electroporation has
been performed in humans, and it seems likely it could be
applied clinically for nonviral gene therapy.
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