|
Current
Signal Transduction Therapy
ISSN: 1574-3624
Current Signal
Transduction Therapy
Volume 2, Number 1, January 2007
Contents
Extracellular Matrix and Aberrant Signaling in
Lung Carcinoma: Role of Fibronectin in the Control of Human
Lung Carcinoma Cell Growth, Apoptosis and Resistance to Therapy
Pp. 1-10
ShouWei Han and Jesse Roman
[Abstract] [Full
Text Article]
Regulation of Polymorphonuclear Leukocyte-Intestinal
Epithelial Cell Interactions: Signalling Events and Potential
Drug Targets Pp. 11-19
Paul Hofman
[Abstract] [Full
Text Article]
Signal Transduction Therapy: Challenges to Clinical
Trial Design Pp. 21-30
Syed A. Hussain, Daniel W. Rea, Nicholas D. James and
Daniel H. Palmer
[Abstract] [Full
Text Article]
IL-13 and its Signal Pathway: Promising Targets in
the Development of a Therapeutic Agent for Bronchial Asthma
Pp. 31-40
Kenji Izuhara, Kazuhiko Arima, Sachiko Kanaji, Taisuke
Kanaji and Shoichiro Ohta
[Abstract] [Full
Text Article]
Cellular Signaling in Cartilage Tissue Engineering
Pp. 41-48
Mikko J. Lammi
[Abstract] [Full
Text Article]
The Role of Connexins in Carcinogenesis: Review of
Current Knowledge Pp. 49-56
Kanczuga-koda Luiza, Sulkowski Stanislaw, Koda Mariusz,
Wincewicz Andrzej, Rutkowski Tadeusz and Moniuszko Mariola
[Abstract] [Full
Text Article]
Advances in Molecular Therapeutic Approaches to Patients
with Malignant Gliomas Pp. 57-76
Herbert B. Newton
[Abstract] [Full
Text Article]
Glial Reaction in Parkinson’s Diseases: Inflammatory
Activation Signaling of Glia as a Potential Therapeutic Target
Pp. 77-90
Dong-Kug Choi and Kyoungho Suk
[Abstract] [Full
Text Article]
Signal Transduction Therapy of Diabetic Vascular Complication
Pp. 91-100
Sho-ichi Yamagishi, Kazuo Nakamura, Takanori Matsui, Yumiko
Yoshida, Katsuhiko Takenaka, Yuko Jinnouchi and Tsutomu Imaizumi
[Abstract] [Full
Text Article]
Abstracts
[Back to top]
Extracellular Matrix and Aberrant Signaling in Lung Carcinoma:
Role of Fibronectin in the Control of Human Lung Carcinoma
Cell Growth, Apoptosis and Resistance to Therapy
ShouWei Han and Jesse Roman
[Full
Text Article]
Despite recent advances in understanding the molecular biology
of lung carcinoma and the introduction of multiple new chemotherapeutic
agents for its treatment, its dismal five-year survival rate
(<15%) has not changed substantially. The lack of advancements
in this area reflects the limited knowledge available concerning
the factors that promote oncogenic transformation and proliferation
of carcinoma cells in the lung. Tumor growth and invasion
are not only the result of malignant transformation, but also
depend on environmental influences from their surrounding
stroma, local growth factors, and systemic hormones. In particular,
the composition of the extracellular matrix is believed to
affect malignant behavior in vivo. This document
reviews information that implicates the matrix glycoprotein
fibronectin in regulation of lung carcinoma cell proliferation,
apoptosis and resistance to therapy. Fibronectin is highly
expressed in chronic lung disorders where most lung carcinomas
are identified. Data available to date indicate that by binding
to specific integrin receptors expressed on tumor cells, fibronectin
stimulates a number of intracellular signals implicated in
the pathobiology of lung carcinogenesis including GTPases,
mitogen-activated protein kinases, and the PI3-Kinase/Akt/mTOR
pathway. Targeting fibronectin and integrin-mediated signals
in tumor cells represents a promising target for the development
of effective anti-cancer strategies.
[Back to top]
Regulation of Polymorphonuclear Leukocyte-Intestinal
Epithelial Cell Interactions: Signalling Events and Potential
Drug Targets
Paul Hofman
[Full
Text Article]
A crucial event in the inflammatory response is recruitment
of polymorphonuclear leukocytes (PMNL) to a site of infection
or injury. PMNL-epithelial interactions involve many fundamental
cell processes, including adhesion, migration, secretion,
phagocytosis and apoptosis. Thus, migration of PMNL across
epithelial-lined organs is a primary event component of host
defense. Moreover, PMNL transepithelial migration often results
in disease symptoms. New insights into leukocyte-epithelial
signalling mechanisms have emerged that are beginning to shed
light on the role of many molecular interactions in regulating
the rate of PMNL transepithelial migration. Knowledge of the
basic mechanisms that control the activation of pro-inflammatory
transcription factors, and how these innate immune signalling
pathways lead to an activation of the adaptative immune response
that maintains the chronically inflamed state, is essential
for pharmacological manipulation of intestinal inflammation.
This review highlights recent advances in our understanding
of the different mechanisms of PMNL-epithelial cell adhesive
interactions at the level of cell surface protein-protein
binding events, and in intracellular signal transduction pathways
that regulate the PMNL transepithelial migration. Finally,
the potential modulation of these different signal pathways
as possible therapeutic goals will be discussed.
[Back to top]
Signal Transduction Therapy: Challenges to Clinical
Trial Design
Syed A. Hussain, Daniel W. Rea, Nicholas D. James and
Daniel H. Palmer
[Full
Text Article]
The most important change that will emerge over the coming
decade for management of cancer is the shift from conventional
chemotherapy and radiotherapy to novel targeted therapies.
The rapid expansion in the understanding of the molecular
biological basis of cancer provides potential targets for
novel therapies. Many molecules, with a variety of cellular
targets are now entering the clinic with the emergence of
some promising data. The key now is to define the patient
population most likely to benefit from these agents through
identification of clinical and biological markers indicating
a sensitive tumour phenotype.
The ongoing clinical development of signal transduction inhibitors
presents several challenges to the existing dogma of clinical
trial design. For example, in early phase trials the traditional
endpoint of objective response rate may not be the most useful
in selecting cytostatic agents, which nevertheless may possess
clinically relevant activity. Rather, such trials should focus
on the in vivo measurement of biological activity
in order to define the optimum schedule of treatment that
results in maximal inhibition of the therapeutic target. In
later phase trials, endpoints such as progression free survival
may be more useful than response rate, although of course
there is no substitute for the endpoints of overall survival
and quality of life, improvements in which these agents must
demonstrate for them to be accepted into the cancer treatment
armamentarium.
Epidermal growth factor receptor tyrosine kinase inhibitors
(EGFR TKI) that have entered clinical trials will be discussed
and the successes and failures of these trials will be used
to illustrate the obstacles that confront the assessment of
the activity of these agents so that this may guide the future
development of other new agents by optimising clinical trial
design.
Signal transduction inhibitors may allow us to overcome resistance
or restore sensitivity to conventional chemotherapy. The integration
of these molecules with existing therapies should be based
on robust pre-clinical data indicating potentially beneficial
additive or even synergistic interactions. The correct clinical
management strategy can be guided by preclinical modelling
but can only be validated by carefully designed clinical trials.
These will at the very least need to be conducted with correlative
translational research elements that will allow us to select
the most appropriate treatment strategy for individual patients.
[Back to top]
IL-13 and its Signal Pathway: Promising Targets in
the Development of a Therapeutic Agent for Bronchial Asthma
Kenji Izuhara, Kazuhiko Arima, Sachiko Kanaji, Taisuke
Kanaji and Shoichiro Ohta
[Full
Text Article]
The incidence of allergic diseases has dramatically increased
in recent decades, especially in urban and industrialized
areas. It has been reported that, at present, one third of
the population in Japan suffers from bronchial asthma, atopic
dermatitis, or allergic rhinitis. The medical cost for treating
such patients is huge and on the increase. Thus, it is important
socially as well as medically to establish more useful strategies
to overcome allergic disorders. Bronchial asthma is a complex
disease characterized by airway inflammation involving a Th2-cytokine,
interleukin (IL)-13. A substantial body of evidence has accumulated
pointing to the pivotal role of IL-13 in the pathogenesis
of bronchial asthma. Therefore, IL-13 and its signal pathway
are thought to be promising targets to develop a therapeutic
agent for bronchial asthma. In this article, we summarize
the biological properties of IL-13 itself and its signal transduction
pathway, the pathological roles of IL-13 in bronchial asthma,
and the agents to inhibit the IL-13 signals that are now under
development.
[Back to top]
Cellular Signaling in Cartilage Tissue Engineering
Mikko J. Lammi
[Full
Text Article]
Osteoarthritis is a common disease in humans, which is caused
by progressive degradation of articular cartilage and imbalance
of extracellular matrix turnover. It usually causes pain and
malfunction of the affected joints, and the incidence of this
disease increases with aging. Classical treatment for osteoarthritis
is pain alleviation and, in progressed disease, surgical operations.
New surgical techniques include transplantation of autologous
chondrocytes or osteochondral plugs to the lesion area. However,
these techniques have the problem of limited cell and tissue
sources available for transplantation. Therefore, cartilage
engineering and use of mesenchymal stem cells have raised
a lot of interest as therapeutic approaches. Various strategies
are being tested for their ability to provide tissue constructs
that could be used as a replacement for the damaged cartilage.
Growth factors, cytokines and mechanical forces are known
to direct chondrogenesis and the maintenance of chondrocytic
phenotype, although the cellular signaling events involved
are often poorly known. Yet, understanding of the signal transduction
mechanisms involved in chondrogenesis and cartilage tissue
engineering will be very important, especially to learn how
to guide stem cells into the desired differentiation path.
This review aims to summarize the known signal transduction
pathways involved with osteoarthritis, cartilage mechanobiology
and differentiation of mesenchymal stem cells to chondrocytes.
[Back to top]
The Role of Connexins in Carcinogenesis: Review of
Current Knowledge
Kanczuga-koda Luiza, Sulkowski Stanislaw, Koda Mariusz,
Wincewicz Andrzej, Rutkowski Tadeusz and Moniuszko Mariola
[Full
Text Article]
Gap junctional intercellular communication is a mechanism
for direct cell-to-cell signaling and is mediated by gap junctions,
which consist of transmembrane proteins called connexins.
Many physiological roles have been proposed for gap junctions
such as maintenance of tissue homeostasis, regulation of tissue
development, electrical and metabolic coupling as well as
regulation of cellular growth, differentiation and apoptosis.
Signaling is especially altered via gap junctions
in cancer. Furthermore, these membrane channels are believed
to be engaged in metastasis. Involvement of aberrant gap junctional
intercellular communication in carcinogenesis and tumor suppressing
role of connexin genes has been well documented. However,
clear explanation is required for the role of connexins that
are localized in intracellular compartment of cancerous cells
and participate in apoptosis and metastasis as well.
The present review is confined to role of connexins in a cell
signaling during carcinogenesis, regulation of apoptosis and
involvement in metastasis. Potential role of gap junctions
and connexins in therapy of cancers was analyzed, too.
[Back to top]
Advances in Molecular Therapeutic Approaches to Patients
with Malignant Gliomas
Herbert B. Newton
[Full
Text Article]
Malignant gliomas remain refractory to conventional treatment
approaches, including radiotherapy and cytotoxic chemotherapy.
Molecular neuro-oncology has now begun to clarify the transformed
phenotype of high-grade gliomas and identify oncogenic pathways
that might be amenable to small molecule “targeted”
therapy. Growth factor signaling pathways are often up-regulated
in these tumors and contribute to oncogenesis through autocrine
and paracrine mechanisms. Excessive growth factor receptor
stimulation can also lead to overactivity of the downstream
Ras signaling pathway. Other internal signal transduction
pathways that may become dysregulated during transformation
include PI3K, Akt, and mTOR. In addition, function of the
cell cycle and apoptotic pathways are often abnormal in malignant
glial cells. “Targeted” therapy against the growth
factor signaling and Ras pathways include tyrosine kinase
inhibitors (e.g., imatinib, erlotinib) and farnesyltransferase
inhibitors (e.g., R115777). Molecular therapeutic small molecules
specific to PI3K and mTOR include LY294002 and CCI-779, respectively.
“Targeted” approaches to the apoptosis and cell
cycle pathways include small molecular modulators, peptide
CDK inhibitors, and proteasomal inhibitors. Further development
of “targeted” therapies designed to modulate the
activity of these pathways, and evaluation of these new agents
in clinical trials, will be needed to improve survival and
quality of life for patients with malignant gliomas.
[Back to top]
Glial Reaction in Parkinson’s Diseases: Inflammatory
Activation Signaling of Glia as a Potential Therapeutic Target
Dong-Kug Choi and Kyoungho Suk
[Full
Text Article]
Although the main cause of many neurodegenerative diseases
is unknown, the glial reaction is considered to be a consequence
of neuronal cell death in Alzheimer's disease, Parkinson's
disease, and Huntington's disease. In Parkinson's disease,
postmortem examination and experimental animal models exposed
to neurotoxin reveals a dramatic loss of dopaminergic neurons
in the substantia nigra associated with a massive astrogliosis
and the presence of activated microglial cells. These glial
cells can release deleterious compounds such as proinflammatory
prostaglandins and cytokines, which may act by stimulating
reactive oxygen species in glial cells, or which may exert
a more direct effect on dopaminergic neurons by activating
receptors that contain death domains involved in neuronal
apoptosis. The anti-inflammatory drugs and the tetracycline
derivative minocycline have been shown to reduce glial activation
and protect the substantia nigra in an animal model of the
disease. Inhibition of the glial reaction and the inflammatory
processes may thus represent a therapeutic target to reduce
neuronal degeneration in Parkinson's disease. Elucidation
of molecular mechanisms underlying intracellular signal transductions
of glial activation will provide promising means of controlling
neuroinflammation and the subsequent neurodegeneration.
[Back to top]
Signal Transduction Therapy of Diabetic Vascular Complication
Sho-ichi Yamagishi, Kazuo Nakamura, Takanori Matsui, Yumiko
Yoshida, Katsuhiko Takenaka, Yuko Jinnouchi and Tsutomu Imaizumi
[Full
Text Article]
Diabetic vascular complication is a leading cause of
end-stage renal failure, acquired blindness, a variety of
neuropathies and accelerated atherosclerosis, which could
account for disabilities and high mortality rates in patients
with diabetes. There is a growing body of evidence to conclude
that intensive control of plasma glucose and blood pressure
is crucial for effectively reducing diabetic vascular complication.
So far, various molecular mechanisms have been proposed to
play a role in the development and progression of diabetic
vascular complication. In this paper, we review potential
therapeutic strategies for the prevention of diabetic vascular
complication, especially focusing on the signal transduction
pathways activated under diabetes.
|
