|
Current
Gene Therapy
ISSN: 1566-5232
Current Gene Therapy
Volume 9, Number 1, February 2009
Contents
Gene Therapy Approaches to Ataxias Pp. 1-8
Filip Lim and Javier Diaz-Nido
[Abstract] [Full
text article] [PMID:
19275566 PubMed - indexed for MEDLINE]
TRAIL Gene Therapy: From Preclinical
Development to Clinical Application Pp.
9-19
Thomas S. Griffith, Brittany Stokes, Tamara
A. Kucaba, James K. Earel, Jr., Rebecca L. VanOosten, Erik
L. Brincks and Lyse A. Norian
[Abstract] [Full
text article] [PMID:
19275567 PubMed - indexed for MEDLINE]
HIV-1 Gene Therapy at Pre-Integration and Provirus DNA Levels
Pp. 20-25
Reza Nazari and Sadhna Joshi
[Abstract] [Full
text article] [PMID:
19275568 PubMed - indexed for MEDLINE]
A Possible Approach for Stem Cell Gene
Therapy of Fanconi Anemia Pp. 26-32
Liting Song
[Abstract] [Full
text article] [PMID:
19275569 PubMed - indexed for MEDLINE]
The Potential of Viral Vector-Mediated
Gene Transfer to Prolong Corneal Allograft Survival Pp.
33-44
Douglas G.A. Parker, Helen M. Brereton,
Douglas J. Coster and Keryn A. Williams
[Abstract] [Full
text article] [PMID:
19275570 PubMed - indexed for MEDLINE]
Systemic Therapeutic Gene Delivery for
Cancer: Crafting Paris’ Arrow Pp.
45-60
Alex W. Tong, Chris M. Jay, Neil Senzer,
Phillip B. Maples and John Nemunaitis
[Abstract] [Full
text article]
[PMID: 19275571 PubMed - indexed for MEDLINE]
Abstracts
[Back to top] [PMID:
19275566 PubMed - indexed for MEDLINE]
Gene Therapy Approaches to Ataxias
Filip Lim and Javier Diaz-Nido
[Full
text article]
Gene therapy has been a clinical possibility since 1989
and the steadily increasing number of clinical trials now
includes strategies targeting neurodegenerative conditions
such as lysosomal storage disease, multiple sclerosis, Alzheimer´s
and, Parkinson´s disease. In spite of lack of knowledge
of the molecular causes of these diseases, results so far
in these trials have been promising. Thus there is gaining
confidence in the potential to develop effective treatments
based on gene transfer for neurological diseases in the near
future. Furthermore, the accelerating progress in knowledge
of the molecular pathologies of neurogenetic disorders, including
rare diseases such as the ataxias, makes them even more amenable
to gene therapy. Here we review recent preclinical studies
relevant to gene therapy of ataxias and discuss developments
needed to bring these strategies into the clinic.
[Back to top] [PMID:
19275567 PubMed - indexed for MEDLINE]
TRAIL Gene Therapy: From Preclinical Development to Clinical
Application
Thomas S. Griffith, Brittany Stokes, Tamara
A. Kucaba, James K. Earel, Jr., Rebecca L. VanOosten, Erik
L. Brincks and Lyse A. Norian
[Full
text article]
Numerous studies have investigated the potential use
of TNF-related apoptosis-inducing ligand (TRAIL) as a cancer
therapeutic since its discovery in 1995 – because TRAIL
is a potent inducer of apoptosis in tumor cells but not in
normal cells and tissues. Consequently, a great deal is known
about TRAIL/TRAIL receptor expression, the molecular components
of TRAIL receptor signaling, and methods of altering tumor
cell sensitivity to TRAIL-induced apoptosis. Our laboratory
was the first to report the possibility of TRAIL gene transfer
therapy as an alternative method of using TRAIL as an antitumor
therapy. As with recombinant proteins administered systemically,
intratumoral TRAIL gene delivery also has limitations that
can restrict its full potential. Translating the preclinical
TRAIL studies into the clinic has started, with the hope that
TRAIL will exhibit robust tumoricidal activity against human
primary tumors in situ with minimal toxic side effects.
[Back to top] [PMID:
19275568 PubMed - indexed for MEDLINE]
HIV-1 Gene Therapy at Pre-Integration and Provirus DNA Levels
Reza Nazari and Sadhna Joshi
[Full
text article]
AIDS is the result of infection by a lentivirus, HIV-1,
which primarily infects CD4+ T cells and macrophages. There
is presently no vaccine and none will be available in the
foreseeable future. Highly active antiretroviral drug therapy
has led to a dramatic reduction of viral load in many infected
individuals, and has decreased mortality in the developing
world. However, besides long-term drug toxicity and eventual
emergence of drug-resistant strains, withdrawal from the therapy
(even after effective and continuous treatment) results in
re-emergence of the virus since cells harbouring the latent
viral reservoirs persist. These issues highlight the need
for alternative therapies, e.g. gene therapy.
This review summarizes various gene therapy strategies that
target early stages of HIV-1 life cycle. We will cover strategies
that allow interference at the level of the released virion
RNA, reverse transcriptase, pre-integration complex, integrase,
dsDNA and provirus DNA in gene-modified cells.
[Back to top]
[PMID:
19275569 PubMed - indexed for MEDLINE]
A Possible Approach for Stem Cell Gene Therapy of Fanconi
Anemia
Liting Song
[Full
text article]
Fanconi anemia (FA) is an inherited chromosomal recessive
syndrome characterized by cellular hypersensitivity to DNA
crosslinking agents and bone marrow failure, which cause aplastic
anemia, and an increased incidence of malignancy. 13 complementation
groups are currently discovered, and 13 distinct genes have
been cloned (FANCA, FANCB, FANCC, FANCD1, FANCD2, FANCE, FANCF,
FANCG, FNACI, FANCJ, FANCL, FANCM, FANCN).
Stem cells can theoretically divide to other cells without
limit as long as a person is still alive. The stem cells that
form blood and immune cells are known as hematopoietic stem
cells. Hematopoietic stem cells can be acquired from a Fanconi
anemia patient, whereas genomic DNA can be obtained easily
from blood cells of a normal person. Normal genes also can
be synthesised by PCR method.
Normal genomic DNA will be delivered into a patient’s
stem cells via microinjection or transfection after enzyme
digestion; the defective genes might be repaired by homologous
genetic recombination. The gene-corrected stem cells can be
transplanted into the same patient finally. It is possible
that human genomic DNA to be considered as materials for homologous
genetic recombination to repair defective genes in vivo.
This might be an efficient method for gene therapy, which
has no or less immunological rejection for Fanconi anemia
and some genetic diseases. Several related observations and
experiments are discussed to support this possible means of
stem cell gene therapy of Fanconi anemia.
[Back to top] [PMID:
19275570 PubMed - indexed for MEDLINE]
The Potential of Viral Vector-Mediated Gene Transfer to Prolong
Corneal Allograft Survival
Douglas G.A. Parker, Helen M. Brereton,
Douglas J. Coster and Keryn A. Williams
[Full
text article]
The cornea is a particularly attractive target for gene
therapy designed to improve the outcome of corneal transplantation.
First, there is a clear and well-defined clinical need. Second,
because donor corneas can be preserved for days if not weeks
within an eye bank, ex vivo transduction of a donor
cornea can be carried out without the urgency associated with
many other forms of transplantation. Finally, the partial
sequestration of the eye from the systemic circulation decreases
the likelihood of spillover of vector and transgene, and the
immune privileged nature of the cornea and anterior segment
affords a degree of protection from immune responses directed
against the vector. A wide range of vectors has been investigated
for gene transfer to the cornea. A number of viral vectors,
in particular, have proved to be efficient at transducing
the cornea and in association with a variety of transgenes,
have been used successfully to prolong corneal allograft survival
significantly in animal models. The most suitable such vector
for future clinical studies in corneal transplantation has
yet to be determined, but the most likely include recombinant
adenoviral, adeno-associated viral and lentiviral vectors.
In this review, we examine the ability of these viral vectors
to transduce the cornea, and summarise those studies in which
gene therapy has been used to prolong experimental corneal
allograft survival.
[Back to top] [PMID:
19275571 PubMed - indexed for MEDLINE]
Systemic Therapeutic Gene Delivery for Cancer: Crafting Paris’
Arrow
Alex W. Tong, Chris M. Jay, Neil Senzer,
Phillip B. Maples and John Nemunaitis
[Full
text article]
Tremendous strides have been made in proteogenomics and
RNA interference technologies. Hence “personalized”
cancer gene therapy has become a foreseeable rather than a
predictable reality. Currently, the lack of an optimized,
systemic gene delivery vehicle remains a key limiting factor
for developing effective treatment applications. Since their
introduction by Felgner in 1987, cationic lipids have been
an attractive consideration for gene delivery, in view of
their biocompatibility, biodegradability, low toxicity, and
low immunogenicity. Successful in vivo transgene
expression by cationic lipid- or cationic polymer-based delivery
depends critically on a long circulating half life (<48
h), a definable systemic biodistribution with target-specific
cancer localization, and efficient cell entry and internalization.
Ideally, the agent should have a hydrophobic, stabilized core
that ensures integrity of the therapeutic entity in vivo,
a biocompatible, neutrally charged shell (ζ
potential of ±10
mv) for enhanced, “stealth” circulation, and a
suitable size (~50-200 nm in diameter) for access into the
tumor neovasculature and reduced reticuloendothelial system
(RES) uptake. “Smart” receptortargeting moieties
can redirect intracellular trafficking. Additional engineered
features have also been incorporated to minimize lysosomal
degradation (membrane fusogenic lipids or proton sponge),
promote endosomal escape into cytoplasm (cell penetrating
peptides, triblock copolymer construction), and enhance nuclear
entry and activate the endogenous transcriptional machinery
(inclusion of a nuclear localization signal). Improvements
in each of these respective areas of study have converged
to yield promising in vivo results.
|
