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Current
Gene Therapy
ISSN: 1566-5232
Current Gene Therapy
Volume 8, Number 4, August 2008
Contents
Advances in Helper-Dependent Adenoviral Vector Research
Pp. 222-235
María M. Segura, Raúl Alba, Assumpció
Bosch and Miguel Chillón
[Abstract]
RNA Interference: New Therapeutics in Allergic Diseases
Pp. 236-246
Chen-Chen Lee and Bor-Luen Chiang
[Abstract]
Gene therapy for Multiple Myeloma Pp.
247-255
Yasuo Adachi, Naoko Yoshio-Hoshino and
Norihiro Nishimoto
[Abstract]
Current Antioxidant Molecular Therapies
for Oxidative Stress Related Ailments Pp.
256-263
Martha E. Ramos-Márquez and
Fernando Siller-López
[Abstract]
CCR5 as Target for HIV-1 Gene Therapy Pp.
264-272
Reza Nazari and Sadhna Joshi
[Abstract]
Perspectives on the Use of Gene Therapy
for Chronic Joint Diseases Pp. 273-286
Steven C. Ghivizzani, Elvire Gouze, Jean-Noel Gouze, Jesse
D. Kay, Marsha L. Bush, Rachael S. Watson, Padraic P. Levings,
David M. Nickerson, Patrick T. Colahan, Paul D. Robbins and
Christopher H. Evans
[Abstract]
Cytoglobin: A Novel Potential Gene Medicine for Fibrosis
and Cancer Therapy Pp. 287-294
Yinghui Lv, Qizhao Wang, Yong Diao and
Ruian Xu
[Abstract]
Abstracts
[Back to top]
Advances in Helper-Dependent Adenoviral Vector
Research
María M. Segura, Raúl Alba, Assumpció
Bosch and Miguel Chillón
The immunogenicity and cytotoxicity associated with early
generations of adenoviral vectors provided a strong incentive
for the development of helper-dependent adenovirus, a last
generation of adenoviral vectors that is devoid of all viral
coding sequences. These vectors have shown to mediate longer
high-level transgene expression in vivo with reduced
toxicity and thus offer enormous potential for human gene
therapy. In addition, they possess a considerably larger cloning
capacity than conventional adenoviral vectors making the transfer
of large cDNAs, multiple transgenes and longer tissuespecific
or regulable promoters possible. In this article, we review
the progress made with helper-dependent adenoviral vectors.
The development and optimization of scalable production processes
and strategies for helper removal will be presented. Current
chromatography options available for vector purification and
the new challenges facing researchers for the separation of
empty particles and/or helper viruses will be discussed. Finally,
we will describe recent advances made in our understanding
of their interaction with the immune system and their potential
as gene delivery vehicles in vivo for the treatment
of diseases affecting liver, skeletal muscle and brain.
[Back to top]
RNA Interference: New Therapeutics in Allergic Diseases
Chen-Chen Lee and Bor-Luen Chiang
Since the RNAi mechanisms were established in 1990, the
rapid progression of RNAi application from animal to clinical
trails in human diseases has shown its enormous therapeutic
potential. In this review, RNAi therapeutics in allergic diseases
is discussed, from RNAi mechanisms and design to challenges
and potential targets in allergic diseases. Current reported
studies on investigating RNAi therapy in vitro and
in vivo are also reviewed. Although there are promising
studies in RNAi-based therapy, understanding further the detailed
mechanisms of RNAi-based therapy and investigating more effective
delivery methods are required for future development.
[Back to top]
Gene therapy for Multiple Myeloma
Yasuo Adachi, Naoko Yoshio-Hoshino and
Norihiro Nishimoto
Prognosis of multiple myeloma (MM) remains insufficient despite
the intervention of high dose chemotherapy with auto- or allo-
hematopoietic stem cell transplantation and the advent of
molecular target drugs such as thalidomide, lenalidomide,
and bortezomib. Further development or new concepts of therapeutic
approaches are still required for MM treatment. Current standard
protocol for MM treatment does not include gene delivery method
or oncolytic virus approaches. Since MM is a disorder originated
from B cell lineage, it involves immunological aspects in
both pathogenesis and clinical manifestations. Therefore,
the comprehension of immunology as well as oncology is essential
to exploit new therapeutic approaches. Recently, novel therapeutic
concepts for MM have been emerging. In this review, we present
current progress of gene therapy related to MM treatments
as well as the overview of MM treatment history.
[Back to top]
Current Antioxidant Molecular Therapies for Oxidative Stress
Related Ailments
Martha E. Ramos-Márquez and
Fernando Siller-López
Oxidative cell damage is a natural occurring phenomenon
due to the aerobic conditions where cells are embedded; however,
such injury can efficiently be controlled and repaired by
the inherent antioxidants of the cell. When the oxidant/antioxidant
balance is disrupted towards the former by any chemical, biological
or physical insult a pathological state could be developed,
therefore, an extensive list of compounds with proved or assumed
antioxidants properties has largely been used for improving
or restoring the health status. Pharmacological therapies
as well as dietary or complementary therapies are continuously
being investigated for the counteracting of the harmful or
damaging effects of oxidation in cells or tissues. However,
critical antioxidant levels are not always achieved at the
target damaged cells by these approaches; on the other side,
the expression of recombinant antioxidant genes specifically
directed to the afflicted cell by gene delivery has shown
remarkable results. In this review we summarize the literature
focused on some of the current antioxidant molecular pharmacological
strategies with particular emphasis to the gene transfer protocols
involved in the treatment of oxidative stress-related disorders.
[Back to top]
CCR5 as Target for HIV-1 Gene Therapy
Reza Nazari and Sadhna Joshi
Acquired immune deficiency syndrome (AIDS) is caused by a
lentivirus, human immunodeficiency virus type-1 (HIV-1). Viral
entry is mediated by specific interaction of the viral envelope
(Env) glycoprotein with a cell surface molecule CD4 which
serves as the primary receptor and a chemokine (C-C or C-X-C
motif) receptor CCR5 or CXCR4 which serves as a co-receptor.
The viral Env, the cellular CD4 receptor, or the CCR5/CXCR4
co-receptors may be the targets of therapeutic interventions.
Compared to the high variability of the viral Env protein,
lack of variability in the CD4 receptor and the CCR5 or CXCR4
co-receptor makes them better targets to prevent viral entry.
Downregulation of CD4 or CXCR4 is likely to have harmful consequences
for the immune function or cellular maturation and homing.
In contrast, individuals who lack functional CCR5 have no
apparent immune defects, and show decreased susceptibility
to HIV-1 infection and delayed progression to AIDS. CCR5 is
essential for HIV-1 infection through all routes of transmission.
Therefore, its downregulation may not only prevent disease
progression, but also the spread of HIV-1 transmission. To
block CCR5 function, a number of molecules were developed,
including low molecular weight compounds, chemokines, N-terminally–modified
chemokine analogues, chemokine-derived molecules, chemokin-beased
synthetic peptides, and anti-CCR5 monoclonal antibodies. Gene
therapy strategies were developed using intrakines and intrabodies
to prevent cell surface expression of CCR5 and zinc finger-nucleases,
or using small interfering RNAs, antisense RNAs, or ribozymes
to decrease co-receptor synthesis.
[Back to top]
Perspectives on the Use of Gene Therapy for Chronic Joint
Diseases
Steven C. Ghivizzani, Elvire Gouze, Jean-Noel Gouze, Jesse
D. Kay, Marsha L. Bush, Rachael S. Watson, Padraic P. Levings,
David M. Nickerson, Patrick T. Colahan, Paul D. Robbins and
Christopher H. Evans
Advances in molecular and cellular biology have identified
a wide variety of proteins including targeted cytokine inhibitors,
immunomodulatory proteins, cytotoxic mediators, angiogenesis
inhibitors, and intracellular signalling molecules that could
be of great benefit in the treatment of chronic joint diseases,
such as osteo- and rheumatoid arthritis. Unfortunately, protein-based
drugs are difficult to administer effectively. They have a
high rate of turnover, requiring frequent readministration,
and exposure in non-diseased tissue can lead to serious side
effects. Gene transfer technologies offer methods to enhance
the efficacy of protein-based therapies, enabling the body
to produce these molecules locally at elevated levels for
extended periods. The proof of concept of gene therapies for
arthritis has been exhaustively demonstrated in multiple laboratories
and in numerous animal models. This review attempts to condense
these studies and to discuss the relative benefits and limitations
of the methods proposed and to discuss the challenges toward
translating these technologies into clinical realities.
[Back to top]
Cytoglobin: A Novel Potential Gene Medicine for Fibrosis
and Cancer Therapy
Yinghui Lv, Qizhao Wang, Yong Diao and
Ruian Xu
Attempts have been made by conventional gene therapy
to suppress hepatic fibrogenesis, but potential oncogenic
activity may prevent its clinical use. Recently, a novel major
approach has been developed for resolution of liver fibrosis
and cirrhosis: inactivation of hepatic stellate cells (HSC)
using the endogenous expressing gene, which could mediate
the homeostatic adaptation of liver. Cytoglobin (Cygb), originally
identified in cultured rat HSC, is in a new class of heme
containing proteins known as the hexacoordinate globin superfamily.
These proteins exhibit peroxidase activity against hydrogen
peroxides and lipid hydroperoxides. Considerable attention
has been focused on the potential benefits of use of Cygb
in fibrosis therapy, as up-regulation of Cygb expression could
reduce oxidant stress, suppress HSC differentiation to a myofibroblast-like
phenotype and eventually prevent the progress of liver fibrosis.
Cygb has also been found to be a candidate tumor suppressor
gene that might provide a new option for cancer gene therapy.
In this review we systematically analyze the potential of
Cygb as a prospective gene medicine for curing fibrosis, cancer,
and other diseases such as diabetes. The molecular structure,
regulation and subcellular location of Cygb are reviewed as
well.
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