Current
Signal Transduction Therapy
ISSN: 1574-3624
Current Signal
Transduction Therapy
Volume 3, Number 2, May 2008
Contents
Liver X Receptor: Crosstalk Node for the Signaling
of Lipid Metabolism, Carbohydrate Metabolism, and Innate Immunity
Pp. 75-81
Michael B. Fessler
[Abstract]
The Role of Parthenolide in Intracellular Signalling
Processes: Review of Current Knowledge Pp. 82-87
Luis Miguel Bedoya, María José Abad and
Paulina Bermejo
[Abstract]
Intracellular Signaling Triggered by Formyl-Peptide
Receptors in Nonphagocytic Cells Pp. 88-96
Annalisa Iaccio, Antonella Angiolillo and
Rosario Ammendola
[Abstract]
Novel Therapeutic Targets for the Treatment of Tubulointerstitial
Fibrosis Pp. 97-111
Jai Prakash, Klaas Poelstra, Harry van Goor, Frits Moolenaar,
Dirk K.F. Meijer and Robbert J. Kok
[Abstract]
Signal Transduction Targets in Prostate Cancer
Pp. 112-128
Hari K. Koul and Lakshmipathi Khandrika
[Abstract]
LGI1 Affects Survival of Neuroblastoma Cells by
Inhibiting Signalling through Phosphoinositide 3-Kinase
Pp. 129-132
Nadia Gabellini and Valentina Masola
[Abstract]
Pathogen-Related Signal Transduction Pathways of
Dendritic Cells: Perspectives for Cancer Immunotherapy
Pp. 133-137
Tomonori Kato, Yasuji Ueda, Hiroaki Kinoh, Kaori
Tsukada, Tomohiko Ichikawa and Yoshikazu Yonemitsu
[Abstract]
Regulation of the PI3K-Akt Network: Current Status and
a Promise for the Treatment of Human Diseases Pp.
138-151
Masayuki Noguchi, Toshiyuki Obata and Futoshi
Suizu
[Abstract]
Abstracts
[Back to top]
Liver X Receptor: Crosstalk Node for the
Signaling of Lipid Metabolism, Carbohydrate Metabolism, and
Innate Immunity
Michael B. Fessler
Liver X Receptor-α
(LXRα,
also known as NR1H3) and LXRβ
(NR1H2) are members of the nuclear receptor superfamily of
ligand-activated transcription factors, a superfamily which
includes the more widely known glucocorticoid receptor, estrogen
receptor, thyroid receptor, and peroxisome proliferator-activated
receptors. The LXRs are activated by physiologic sterol ligands
(e.g., oxysterols) and by synthetic agonists. In recent years,
our understanding of the importance of LXRs has expanded across
several fields of (patho) physiology. Perhaps best known from
a sizeable literature as homeostatic ‘cholesterol sensors’
that drive transcriptional programs promoting cellular cholesterol
efflux, ‘reverse cholesterol transport,’ and bile
acid synthesis, more recent roles for LXRs in glucose homeo-stasis,
atherosclerosis, and innate immunity have also been identified.
These discoveries complement an emerging literature that continues
to draw surprisingly intimate connections between host metabolism
and host defense. The present review will discuss the roles
of LXR in the signaling of metabolism and innate immunity,
and the potential for synthetic LXR agonists as novel therapeutics
in dyslipidemia, atherosclerosis, disordered glucose metabolism,
and inflammation.
[Back to top]
The Role of Parthenolide in Intracellular Signalling
Processes: Review of Current Knowledge
Luis Miguel Bedoya, María José Abad and
Paulina Bermejo
The popularity of medicinal herbs has grown significantly
in recent years despite a dearth of information regarding
their modes of action and continuing concerns over their efficacy.
Recent efforts to elucidate the mechanisms of action of several
anti-inflammatory herbs have focused on a class of compounds,
sesquiterpene lactones, that are believed to be the active
components of these herbal medicines. Sesquiterpene lactones
constitute a large and diverse group of biologically active
plant constituents that have been reported from the Acanthaceae,
Anacardiaceae, Apiaceae, Euphorbiaceae, Lauraceae, Magnoliaceae,
Menispermaceae, Rutaceae, Winteraceae and the Hepatidae (liverworts).
However, the greatest number has been reported from the Asteraceae.
Tanacetum parthenium (feverfew) is one of the most
prominent species in the Asteraceae and a known remedy for
the treatment of various diseases. Feverfew has been used
for at least two millennia for the treatment of fever, as
well as headache, menstrual irregularities and stomach-ache.
Today, feverfew is widely used as a migraine preventive, and
more recently as an aid for those suffering from arthritis
and inflammation. The drug feverfew contains a series of compounds,
particularly sesquiterpene lactones, which, being parthenolide,
are regarded as the main cause of the therapeutic properties
of the plant. Although a few studies have been published which
evaluate the effects of parthenolide in vivo, several
studies have been undertaken to investigate the molecular
basis of the pharmacological effect of parthenolide. This
review will summarize some of the most important reports on
the role of parthenolide in intracellular signalling processes
from the literature data (2004-2007).
[Back to top]
Intracellular Signaling Triggered by Formyl-Peptide
Receptors in Nonphagocytic Cells
Annalisa Iaccio, Antonella Angiolillo and
Rosario Ammendola
Formyl-peptide receptors (FPR) are expressed in several
cell types including phagocytic leukocytes, and a wide variety
of agonists of FPR and of its FPRL1 variant have been identified.
These ligands interact with their specific receptors on the
cellular membrane, and activate specific biological functions
through a G-protein-coupled pathway. In nonphagocytic cells,
agonist/FPR binding also induces transactivation of the constitutive
membrane receptors PDGF-R, EGF-R and uPAR that in turn trigger
specific, characteristic intracellular signal transduction
pathways. The second messengers resulting from the interaction
between ligands and formyl-peptide receptors act on various
intracellular kinases (mitogen-activated protein kinases,
protein kinases C and B, Jun kinase and some tyrosine kinases).
Activation of NADPH oxidase expressed in nonphagocytic cells,
and phosphorylation and nuclear translocation of regulatory
transcriptional factors may be the downstream targets of this
signaling cascade. The activated signal transduction pathways
also lead to various biochemical cellular responses that can
contribute to cell proliferation, and can protect against
cell death and the malignant behavior of several human cancer
cell lines. Dissection of the signaling cascade triggered
by different agonists will shed light on the role of FPRs
in nonphagocytic cells in both human physiology and diseases.
[Back to top]
Novel Therapeutic Targets for the Treatment of Tubulointerstitial
Fibrosis
Jai Prakash, Klaas Poelstra, Harry van Goor, Frits Moolenaar,
Dirk K.F. Meijer and Robbert J. Kok
Approximately 80% of the kidney is composed of tubular
cells which secret and reabsorb substances to and from the
urine. Activated tubular cells play a pivotal role in the
etiology of renal fibrosis. During renal injury, these activated
tubular cells participate in the initiation of fibrogenic
processes which eventually may lead to tubulointerstitial
fibrosis and end stage renal disease (ESRD). Current therapies
such as angiotensin converting enzyme inhibitors, angiotensin
II receptor type-1 antagonists and statins do not suffice
for the treatment of renal fibrosis. However, in recent years,
better understanding of disease mechanisms led to the development
of new drug entities that intervene in the signal transduction
pathways involved in the disease pathogenesis. This review
discusses possible new drugs directed to intracellular signal
transduction pathways such as mitogen-activated protein kinases
(p38, ERK and JNK), growth factors receptor tyrosine kinases
(TGF-β
and PDGF), Rho kinase, and nuclear transcription factors that
are activated during disease. In addition to kinase inhibitors,
novel approaches such as renal-selective drug targeting, recombinant
protein antifibrotic agents and gene silencing concepts are
discussed.
[Back to top]
Signal Transduction Targets in Prostate Cancer
Hari K. Koul and Lakshmipathi Khandrika
According to the American Cancer Society, Prostate cancer
(PCa) is the second leading cause of cancer deaths in men.
Conventional therapies produce a high rate of cure for patients
with localized prostate cancer, but there is no cure once
the disease has spread beyond the prostate. Androgens are
the primary growth factors used by prostate cancer cells initially,
and androgen deprivation remains the only treatment for men
with clinically advanced stage disease; however, prostate
cancer cells eventually progress to androgen independence,
and androgen refractory prostate cancer is ultimately responsible
for the death of PCa patients. There is at present no effective
treatment for hormone-independent PCa.
Normal prostate epithelial cells as well as early-stage-prostate
cancer cells depend on androgens for growth and survival.
However, several molecular mechanisms like mutations to the
androgen receptor (AR), cross-talk between the AR and other
molecular pathways can lead to an independence from androgens
for growth. These casual molecular genetic changes lead to
an epigenetic mechanism where a feed-back autocrine loop between
membrane receptors and associated ligands serves as an essential
component of growth, proliferation and metastasis of prostate
cancer at an advanced and androgen-independent stage. Peptide
growth factors and cytokines are known to exert their effects
by a complex array of mechanisms primarily mediated by signal
transduction pathways. Thus, we rationalized that inhibiting
these epigenetic events could serve as an approach in treatment
of advanced prostate cancer.
In this article we have reviewed all the relevant literature
that describe signal transduction pathways in prostate gland
under normal and malignant conditions. We will also try to
identify possible signal transduction targets for the treatment
of prostate cancer.
[Back to top]
LGI1 Affects Survival of Neuroblastoma Cells by Inhibiting
Signalling through Phosphoinositide 3-Kinase
Nadia Gabellini and Valentina Masola
Overexpression of the leucine-rich, glioma-inactivated
1 (LGI1) gene in neuroblastoma cells inhibited proliferation
and efficiently induced apoptosis. Cell clones stably transfected
with LGI1 cDNA showed greater mortality during a period of
serum starvation in comparison with control cells stably transfected
with empty vector. This observation suggested hindrance of
the PI3K/Akt pathway, a central transducer of survival stimuli
elicited by serum growth factors. Treatment with inhibitors
of PI3K significantly increased the death of control cells
but substantially failed to influence LGI1 cell death, which
was greatest independently of the presence of inhibitors.
Blockage of the PI3K/Akt pathway in LGI1 cells was confirmed
by the lack of serum-induced Akt phosphorylation, in contrast
with the strong response of control cells. Instead, serum-induced
phosphorylation of ERK1/2 was not impaired by the expression
of LGI1. This study showed that overexpression of LGI1 caused
neuroblastoma cell death by blocking activation of the PI3K/Akt
pathway. Thus, the possibility of upregulating LGI1 expression
may be a novel strategy in suppressing oncogenesis and metastasis
sustained by excessive activation of the PI3K/Akt pathway.
[Back to top]
Pathogen-Related Signal Transduction Pathways of
Dendritic Cells: Perspectives for Cancer Immunotherapy
Tomonori Kato, Yasuji Ueda, Hiroaki Kinoh, Kaori
Tsukada, Tomohiko Ichikawa and Yoshikazu Yonemitsu
Dendritic cells (DCs) play a crucial role in translating
innate to adaptive immunity. DC-based cancer immunotherapy
has been under evaluation; however, its clinical benefits
remain limited. A better understanding of DCs is, therefore,
needed to improve clinical outcomes. Toll-like receptors (TLRs)
were initially identified as molecules that recognize and
bind pathogen-associated molecular patterns (PAMPs) leading
to DC maturation. The TLR signaling pathway leads to the activation
of NF-κB,
which initiates the transcription of proinflammatory cytokine
genes. As the sensors of RNA viruses in the cellular cytoplasm,
RNA helicases containing retinoic acidinducible gene-I (RIG-I)
have been shown to recognize the viral RNA genome, and recent
studies have demonstrated that these helicases strongly induce
the upregulation of type I interferons. We recently demonstrated
that RNA viruses strongly activated DCs, and this finding
is expected to aid in the development of improved DC-based
cancer immunotherapy. We then proposed DC-based “immunostimulatory
RNA virotherapy” as a novel therapeutic approach. The
janus kinases (JAKs) and the signal transducers and activators
of transcription (STATs) are key molecules in a major signaling
pathway for modulating DC function; suppressors of cytokine
signaling (SOCSs) inhibit this pathway. Some recent studies
have suggested that the suppression of SOCS family proteins
in DCs modulates immune responses, including anticancer immunity.
Here, we review recent progress in the elucidation of the
mechanisms of signal transduction pathways in DCs; it is hoped
that such investigations will eventually lead to a variety
of DC-based cancer immunotherapies.
[Back to top]
Regulation of the PI3K-Akt Network: Current Status and
a Promise for the Treatment of Human Diseases
Masayuki Noguchi, Toshiyuki Obata and Futoshi
Suizu
The growth factor signals regulate the balance of cell proliferation
and cell death to maintain the homeostasis in vivo;
hence, deregulation of the balance underlies a variety of
human diseases. The PI3K-Akt network is activated by various
cytokines or growth factors and mediates intracellular signals
to regulate a wide variety of cellular responses, including
anti-apoptosis, proliferation, cell cycling, protein synthesis,
glucose metabolism, and telomere activity. Genomic mutations,
alterations, amplifications, and/or translocations of the
oncogenes, tumor suppressor genes, or kinases involved in
the PI3K-Akt regulatory network underlie various human diseases
such as cancers, viral infections, glucose intolerance (or
diabetes mellitus), schizophrenia, and/or autoimmune diseases.
Therefore, targeting the PI3K-Akt network becomes an attractive
goal for drug development.This review article summarizes the
current knowledge about the regulation of the PI3K-Akt signaling
network to highlight therapeutic implications for human diseases.
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