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Current
Signal Transduction Therapy
ISSN: 1574-3624
Current Signal
Transduction Therapy
Volume 1, Number 2, May 2006
Contents
Life and Death of Nerve Cells: Therapeutic Cytokine Signaling
Pathways Pp. 133-146
Ulrich L.M. Eisel, Knut Biber and Paul G.M. Luiten
[Abstract]
Involvement of Targeting and Scaffolding Proteins in the Regulation
of the EGFR/Ras/MAPK Pathway in Oncogenesis Pp. 147-167
Thomas Grewal, Francesc Tebar, Albert Pol and Carlos
Enrich
[Abstract]
Signalling Cascades in Ventilator-Induced Lung Injury and
Their Implications for Patient Therapies Pp. 169-178
Sarah J. Cooper
[Abstract]
Signal Transduction Therapy Targeting Apoptosis Pathways
in Cancers Pp. 170-190
Simone Fulda and Klaus-Michael Debatin
[Abstract]
T-Cell Zeta Chain Expression, Phosphorylation and
Degradation and Their Role in T-Cell Signal Transduction and
Immune Response Regulation in Health and Disease Pp.
191-208
Theodoros Eleftheriadis, Georgia Antoniadi, Vassilios
Liakopoulos and Alexandros Kortsaris
[Abstract]
Erythropoietin Signaling and Neuroprotection Pp.
209-218
Sermin Genc, Mehtap Y. Egrilmez and Kursad Genc
[Abstract]
Antisense Oligodeoxynucleotide Therapy for Prostate
Cancer Targeting Antiapoptotic Genes Involved in the Mechanism
Mediating Progression to Androgen Independence Pp.
219-226
Hideaki Miyake, Isao Hara, Masato Fujisawa and
Martin E. Gleave
[Abstract]
Integrin-Mediated Drug Resistance Pp. 227-237
Andreja Ambriovi c´-Ristov and Maja Osmak
[Abstract]
Abstracts
[Back to top]
Life and Death of Nerve Cells: Therapeutic Cytokine
Signaling Pathways
Ulrich L.M. Eisel, Knut Biber and Paul G.M.
Luiten
Based on recent research neuroinflammation is more
than just a pathological mechanism in neurodegenerative diseases.
As representatives for the cytokine family we will review
the functions of Interleukin-6 and Tumor Necorosis Factor
with respect to their role in neuroprotection and neurodegeneration.
Both cytokines have been found to be strongly upregulated
during diseases such as Alzheimer’s disease, stroke
or Parkinson’s syndrome. By comparing signaling function
of these cytokines during health and disease it becomes clear
that the role of cytokine mediated tissue modulation depends
very much on the molecular and cellular state of nerve cells
e.g. physiological vs. pathological. Finally, we
will discuss the possibilities of using cytokine activated
pathways as a potential targets for therapeutic avenues.
[Back to top]
Involvement of Targeting and Scaffolding Proteins in the
Regulation of the EGFR/Ras/MAPK Pathway in Oncogenesis
Thomas Grewal, Francesc Tebar, Albert Pol and Carlos
Enrich
The identification of the causes of cancer at
the cellular level has led to the discovery of the Epidermal
Growth Factor Receptor (EGFR)/Ras/Mitogen-Activated Protein
Kinase (MAPK) signaling pathway as a target for the development
of anti-cancer strategies. A variety of therapeutic approaches
to inhibit the EGFR/Ras/MAP module are currently being tested
in clinical trials or have even been approved for the treatment
of some tumors. However, more efficient ways to block the
EGFR/Ras/MAPK pathway in tumor cells still have to be developed.
The subcellular localisation of each member of this module
is of pertinent importance to ensure signaling. Accumulating
evidence suggests that targeting/scaffold proteins regulate
the assembly, localization and activity of EGFR/Ras/MAPK signal
transduction components. In particular proteins that stimulate
the lysosomal downregulation of the EGFR and the targeting
of Ras regulators/effectors to Ras could contribute to improve
strategies to inhibit EGFR/Ras signaling in cancer. These
proteins include the Cbl/CIN85/endophilin pathway, caveolin,
galectins, annexins, Impedes Mitogenic Signal Propagation
(IMP), 14-3-3 and Kinase Suppressor of Ras (KSR). Here we
will review the current literature regarding the potential
of targeting/scaffold proteins to affect the lysosomal targeting
of EGFR and the subcellular localization of the Ras/MAPK signaling
cascade.
[Back to top]
Signalling Cascades in Ventilator-Induced Lung Injury and
Their Implications for Patient Therapies
Sarah J. Cooper
Mechanical ventilation can be lifesaving, but
may initiate and perpetuate ventilator-induced lung injury.
This has many manifestations, from pneumothorax to multi-system
organ failure. Although the precise underlying mechanisms
have not yet been elucidated, various signalling pathways
are thought to be involved and shall be discussed in this
review. A key component in the pathogenesis of lung injury
is ‘biotrauma’, comprising a triggering of intracellular
signalling pathways to upregulate inflammatory processes in
response to alveolar membrane deformation. This mechanotransduction
arises from a possible combination of at least three mechanisms:
Activation of stretch-sensitive alveolar membrane ion channels,
plasma membrane disruption causing a wave of calcium release
and/or integrin activation producing cytoskeletal rearrangement.
The consequence is increased expression of c-fos
and Nuclear Factor-κB,
important regulators of the inflammatory response. Since an
understanding of the signalling cascades involved will help
to design strategies to diminish the immune response, this
review also highlights the implications for therapies to minimise
lung damage in the clinical setting, such as the use of anti-TNF-α-antibody.
There is obviously much scope for future research in this
area, and perhaps further investigation into components of
the cascades will reveal potential targets for therapeutic
interventions? In this way, the mortality of ventilated patients
may be reduced.
[Back to top]
Signal Transduction Therapy Targeting Apoptosis
Pathways in Cancers
Simone Fulda and Klaus-Michael Debatin
Apoptosis, the cell’s intrinsic death program,
is a key regulator of tissue homeostasis. Thus, any imbalance
between cell death and proliferation may favor tumor formation.
Moreover, killing of cancer cells by cytotoxic therapies currently
used in clinical oncology such as chemotherapy or γ-irradiation
is primarily mediated by triggering apoptosis as well as other
forms of cell death in cancer cells. Accordingly, defects
in apoptosis pathways may lead to cancer resistance. Understanding
the molecular pathways that regulate apoptosis in different
types of malignancies and how resistant cancer cells successfully
evade to undergo apoptosis may provide novel opportunities
for cancer drug development. Thus, apoptosis pathways may
be exploited for cancer treatment by directly triggering cell
death in tumor cells, e.g. via ligation of death
receptors, or by enhancing the efficacy of conventional cancer
therapies, e.g. by blockade of anti-apoptotic programs. In
this review we will focus on the potential exploitation of
the death receptor pathway, in particular TRAIL, for cancer
therapy. Also, we will discuss signal transduction therapy
targeting Inhibitor of Apoptosis Proteins (IAPs).
[Back to top]
T-Cell Zeta Chain Expression, Phosphorylation and
Degradation and Their Role in T-Cell Signal Transduction and
Immune Response Regulation in Health and Disease
Theodoros Eleftheriadis, Georgia Antoniadi, Vassilios
Liakopoulos and Alexandros Kortsaris
T-cell zeta chain expression, phosphorylation
and degradation and their role in T-cell signal transduction
and immune response regulation in health and disease.
Zeta chain is a stable constituent of the antigen specific
T-cell receptor and its phosphorylation is one of the earliest
and key events in the T-cell signal transduction. Zeta chain
phosphorylation is strictly controlled by the action of sarcoma-family
kinases and also by phosphatases, indicating its crucial role
in antigen specific T-cell activation. Furthermore, after
its phosphorylation and T-cell activation, ζ-chain
is ubiquitylated and degraded, a fact suggesting that its
level on T-cell surface is also under control and contribute
to the regulation of an initiated immune response.
Zeta chain expression and/or phosphorylation seems to be of
great importance in many clinical conditions from the pathogenesis
of various types of cancer to the immunosuppressive state
in dialysis patients. Its levels are also affected by chronic
inflammation.
In addition to its role in the antigen specific signal transduction,
ζ-chain
is present only in T-cells and natural killer cells, making
it a possible target for immunotherapeutic applications. The
recent discovery of specific inhibitors of ζ-chain
phosphorylation opens new horizons for future research and
for possible therapeutic interventions in various clinical
conditions.
[Back to top]
Erythropoietin Signaling and Neuroprotection
Sermin Genc, Mehtap Y. Egrilmez and Kursad Genc
Erythropoietin (Epo) plays an essential role in the regulation
of erythropoiesis by stimulating growth, preventing apoptosis,
and promoting terminal differentiation of erythroid progenitors.
The Epo receptor belongs to the cytokine receptor superfamily.
Epo and its receptor have been localized to several nonhematopoietic
tissues and cells, including the central and peripheral nervous
systems, endothelial cells and heart. Epo exerts neuronal,
vascular and cardiac protection through multiple signaling
pathways in different models of tissue and cell injury
in vitro and in vivo, such as ischemia, hypoxia,
inflammation and oxidative stress. As a result, Epo has been
suggested as a possible candidate in the treatment of neurological
and cardiac disorders. A better understanding of cellular
pathways and molecules modulated by Epo signaling is crucial
in determining the potential therapeutic application of recombinant
human Epo and may provide further insights in the development
of both better synergistic therapies as well as new molecular
targets. In this review, we summarize the current knowledge
on the signaling pathways by which Epo offers neuroprotection
and cytoprotection, signal transduction systems modulated
by Epo and negative regulation of Epo signaling in the nervous
system.
[Back to top]
Antisense Oligodeoxynucleotide Therapy for Prostate
Cancer Targeting Antiapoptotic Genes Involved in the Mechanism
Mediating Progression to Androgen Independence
Hideaki Miyake, Isao Hara, Masato Fujisawa and
Martin E. Gleave
Androgen-independent (AI) progression remains the main
obstacle to improving the survival of patients with prostate
cancer. Recently, we characterized changes in gene expression
profile during AI progression in the prostate cancer model
systems as well as the clinical specimens, and identified
several genes, including bcl-2, bcl-xL, clusterin, insulin-like
growth factor binding protein (IGFBP)-2, IGFBP-5 and heat
shock protein 27, that are involved in the signal transduction
pathways mediating resistance to various kinds of apoptotic
stimuli. We then showed the efficacy of inactivating such
antiapoptotic genes using antisense (AS) oligodeoxynucleotides
(ODNs) to delay AI progression after androgen withdrawal.
We further demonstrated the synergistic effects of AS ODN
therapy combined with several treatments, such as cytotoxic
chemotherapy, radiation and other molecular targeting therapies.
In this review, we attempted to summarize the progress we
have made in the field of AS ODN strategy against prostate
cancer, and to discuss the preliminary data of the recently
completed phase I clinical trials using AS ODNs as well as
the future prospects of this therapy. The findings presented
in this review may help clarify the significance of AS ODN
therapy targeting relevant genes as an attractive alternative
to conventional strategies for prostate cancer.
[Back to top]
Integrin-Mediated Drug Resistance
Andreja Ambriovi c´-Ristov and Maja Osmak
For many years the mechanisms of intrinsic
or acquired drug resistance have been the major object for
molecular oncologists and clinicians, because resistance to
chemotherapy critically limits the outcome of cancer treatment.
Initially, the interaction of a drug with its molecular target
that yields a lethal lesion has been studied - at the target
level or upstream of this interaction (drug influx and efflux,
detoxification, DNA repair etc.). Later, it was discovered
that downstream cellular responses to a given DNA lesion can
determine the outcome of the therapy, focusing the investigation
on the processes of the programmed cell death. More recently
a new phenomenon of drug resistance has been discovered, called
Cell Adhesion-Mediated Drug Resistance. It is based on the
adherence of cells to extracellular matrix proteins through
adhesive molecules such as integrins. Integrins are cell surface
heterodimeric receptors that mediate cell-extracellular matrix
adhesion. They trigger many intracellular signaling pathways
involved in a cell proliferation, survival/apoptosis, shape,
polarity, motility, and differentiation. Integrins may protect
cancer cells from an array of cytotoxic agents in several
ways. This review will focus on the role of integrins in conferring
resistance to tumor cells. We will discuss specific signal
transduction pathways initiated by integrin ligation as a
source of potential therapeutic targets for the fight against
cancer.
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