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Current
Gene Therapy
ISSN: 1566-5232
Current Gene Therapy
Volume 7, Number 1, February 2007
Contents
Gene Modified Cell Transplantation for Vascular
Regeneration Pp. 1-6
Satoshi Murasawa and Takayuki Asahara
[Abstract] [Full
text article]
New Vectors and Strategies for Cardiovascular
Gene Therapy Pp. 7-23
Agnieszka Jazwa, Alicja Jozkowicz and Jozef Dulak
[Abstract] [Full
text article]
Gene Therapy for Ocular Neovascularization
Pp. 25-33
Peter A. Campochiaro
[Abstract] [Full
text article]
Gene Therapy in Disorders of Lipoprotein Metabolism
Pp. 35-47
Stefan F.C. Vaessen, Jaap Twisk, John J.P. Kastelein and
Jan Albert Kuivenhoven
[Abstract] [Full
text article]
Meganucleases and DNA Double-Strand Break-Induced
Recombination: Perspectives for Gene Therapy Pp.
49-66
Frédéric Pâques and Philippe Duchateau
[Abstract] [Full
text article]
Electrotransfer as a Non Viral Method of Gene Delivery
Pp. 67-77
Cyril Favard, David S. Dean and Marie-Pierre Rols
[Abstract] [Full
text article]
Abstracts
[Back to top]
Gene Modified Cell Transplantation for Vascular Regeneration
Satoshi Murasawa and Takayuki Asahara
[Full
text article]
Cell Transplantation is one of the powerful tools to
ameliorate the capillary flow in ischemic condition. EPC (Endothelial
Progenitor Cell) was identified in adult peripheral blood
and thought to be a suitable candidate for cell transplantation.
Also, gene therapy is already promising choice for enhancing
angiogenic property. The combination of cell transplantation
and gene therapy should be more effective way to regenerate
vasculature in ischemic region. Recently, several research
reports have come out regarding gene modified cell transplantation.
We will mainly focus on the background of EPC, and then gene
modified EPC findings in this review.
[Back to top]
New Vectors and Strategies for Cardiovascular
Gene Therapy
Agnieszka Jazwa, Alicja Jozkowicz and Jozef Dulak
[Full
text article]
Cardiovascular diseases are the major cause of morbidity and
mortality in both men and women in industrially developed
countries. These disorders may result from impaired angiogenesis,
particularly in response to hypoxia. Despite many limitations,
gene therapy is still emerging as a potential alternative
for patients who are not candidates for traditional revascularization
procedures, like angioplasty or vein grafts. This review focuses
on recent approaches in the development of new gene delivery
vectors, with great respect to newly discovered AAV serotypes
and their modified forms. Moreover, some new cardiovascular
gene therapy strategies have been highlighted, such as combination
of different angiogenic growth factors or simultaneous application
of genes and progenitor cells in order to obtain stable and
functional blood vessels in ischemic tissue.
[Back to top]
Gene Therapy for Ocular Neovascularization
Peter A. Campochiaro
[Full
text article]
Ocular neovascularization is a major cause of blindness and
visual disability in developed countries. There has been considerable
recent progress identifying molecular signals that participate
in ocular neovascularization and it appears that imbalances
between stimulatory and inhibitory proteins contribute. Re-establishing
balance by ocular gene transfer to block stimulators or increase
expression of endogenous inhibitors is an appealing therapeutic
approach, because it provides a potential means to achieve
sustained intraocular effects with little impact on the rest
of the body. Proof-of-concept has been provided in animal
models using several vector systems and several transgenes
and completion of a phase I study testing intraocular injection
of an adenoviral vector expressing pigment epithelium-derived
factor is an important mile-stone that will help to accelerate
future progress. It is likely that additional vectors and
transgenes will enter clinical trials in the near future.
This report discusses the rationale and experimental evidence
regarding several candidate transgenes.
[Back to top]
Gene Therapy in Disorders of Lipoprotein Metabolism
Stefan F.C. Vaessen, Jaap Twisk, John J.P. Kastelein and
Jan Albert Kuivenhoven
[Full
text article]
Current pharmacologic interventions in lipid metabolism
are insufficient in a subset of patients at increased risk
of cardiovascular disease. In particular, several monogenetic
disorders of lipid metabolism with diverse clinical complications
are beyond treatment to date. Somatic gene transfer is a potential
approach to treat these disorders. This review describes the
efforts made thus far to develop gene therapy for 3 major
classes of dyslipidemia: Increased levels of low-density lipoprotein
cholesterol, reduced levels of high-density lipoprotein cholesterol
and increased plasma triglyceride levels. For many of the
genetic causes underlying these conditions, proof-of-principle
studies have been performed and in combination with improved
vectors some of these strategies may be feasible for clinical
use in the future.
[Back to top]
Meganucleases and DNA Double-Strand Break-Induced
Recombination: Perspectives for Gene Therapy
Frédéric Pâques and Philippe Duchateau
[Full
text article]
Meganucleases are sequence-specific endonucleases recognizing
large (>12 bp) sequence sites and several laboratories
have used these proteins to induce highly efficient gene targeting
in mammalian cells. The recent development of artificial endonucleases
with tailored specificities has opened the door for a wide
range of new applications, including therapeutic ones: redesigned
endonucleases cleaving chosen sequences could be used to in
gene therapy to correct mutated genes or introduce transgenes
in chosen loci. Such “targeted” approaches markedly
differ from current gene therapy strategies based on the random
insertion of a complementing virus-borne transgene. As a consequence,
they should bypass the odds of random insertion. Artificial
fusion proteins including Zinc-Finger binding domains have
provided important proofs of concept, however the toxicity
of these proteins is still an issue. Today custom-designed
homing endonucleases, the natural meganucleases, could represent
an efficient alternative. After a brief description of the
origin of the technology, current systems based on redesigned
endonucleases will be presented, with a special emphasis on
the recent advances in homing endonuclease engineering. Finally,
we will discuss the main issues that will need to be addressed
in order to bring this promising technology to the patient.
[Back to top]
Electrotransfer as a Non Viral Method of Gene Delivery
Cyril Favard, David S. Dean and Marie-Pierre Rols
[Full
text article]
Over the last few decades, various vectors have been
developed in the field of gene therapy. There still exist
a number of important unresolved problems associated with
the use of viral as well as non viral vectors. These techniques
can suffer from secondary toxicity or low gene transfer efficiency.
Therefore an efficient and safe method of DNA delivery still
needs to be found for medical applications. DNA electrotransfer
is a physical method that consists of the local application
of electric pulses after the introduction of DNA into the
extra cellular medium. As electrotransfer has proven to be
one of the most efficient and simple non viral methods of
delivery, it may provide an important alternative technique
in the field of gene therapy. The present review focuses on
questions related to the mechanism of DNA electrotransfer,
i.e. the basic physical processes responsible for the electropermeabilisation
of lipid membranes. It also addresses the current limitations
of the method as applied to DNA transfer, in particular its
efficiency in achieving in vitro gene expression
in cells and also its potential use for in vivo gene
delivery.
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