Current Cancer
Drug Targets
ISSN: 1568-0096
Current Cancer Drug Targets
Volume 6, Number 8, December 2006
Contents
Mechanisms of Resistance to Imatinib in
CML Patients: A Paradigm for the Advantages and Pitfalls of
Molecularly Targeted Therapy Pp. 645-657
E. Ritchie and G. Nichols
[Abstract]
Can we Target the Chemokine Network for Cancer
Therapeutics? Pp. 659-670
Ryan Giles and Robert D. Loberg
[Abstract]
The JAK-STAT Pathway: A Therapeutic Target in Hematological
Malignancies Pp. 671-679
A. Ferrajoli, S. Faderl, F. Ravandi and Z. Estrov
[Abstract]
Modulation of the Cell Cycle and Induction of Apoptosis
in Human Cancer Cells by Synthetic Bile Acids Pp.
681-689
Nam Deuk Kim, Eunok Im, Young Hyun Yoo and Yung Hyun Choi
[Abstract]
EGFR-Targeting Monoclonal Antibodies in Head and Neck
Cancer Pp. 691-710
Igor Astsaturov, Roger B. Cohen and Paul M. Harari
[Abstract]
Chemopreventive Agents Alters Global Gene Expression
Pattern: Predicting their Mode of Action and Targets
Pp. 711-727
Bhagavathi A. Narayanan
[Abstract]
Anti-Invasive and Anti-Metastasis Strategies: New
Roads, New Tools and New Hopes Pp. 729-751
Laurent Dollé, Herman T. Depypere and Marc E. Bracke
[Abstract]
Abstracts
[Back to top]
Mechanisms of Resistance to Imatinib in
CML Patients: A Paradigm for the Advantages and Pitfalls of
Molecularly Targeted Therapy
E. Ritchie and G. Nichols
One of the challenges of cancer therapeutics
is to discover targets unique to the tumor cell population.
Constitutively activated tyrosine kinases play a role in the
malignant phenotype in a number of different cancers. While
the kinases may be present in the normal cell, the cancer
cell is often dependent upon the activation of the kinase
for the maintenance of malignant growth. Inhibition of kinase
activation may therefore selectively inhibit malignant proliferation.
In the case of chronic myelogenous leukemia (CML), the activated
tyrosine kinase (BCR-ABL) is due to a chromosomal translocation
that defines this disease, and is necessary for malignant
transformation. Imatinib mesylate (Gleevec, Novartis) is a
small molecule tyrosine kinase inhibitor, developed through
the chemical modification to be selected for a small number
of tyrosine kinases present in human cells. This agent is
also orally bioavailable and has been found to be effective
in clinical trials. We have learned much through the clinical
use of this agent. 1) Specific targeting of activated signal
transduction pathways may be effective in inhibiting cancer
cells. 2) Cancer cells may not only be inherently resistant
to small molecule inhibitors, but may also develop resistance
after exposure to the inhibitor. 3) Increased knowledge regarding
critical signal transduction pathways, the structure of the
molecules that are being targeted and the inhibitors themselves,
will allow us to understand resistance as it develops and
create new molecules to bypass resistance. We will discuss
imatinib as an important example of the success and pitfalls
of targeted therapeutics for cancer.
[Back to top]
Can we Target the Chemokine Network
for Cancer Therapeutics?
Ryan Giles and Robert D. Loberg
The paradigm of cancer development and metastasis
has been redefined to encompass a more comprehensive interaction
between the tumor and microenvironment within which the tumor
cells reside. Despite the realization that this more comprehensive
relationship has changed the current paradigm of cancer research,
the struggle continues to more completely understand the pathogenesis
of the disease and the ability to appropriately identify and
design novel targets for therapy. Chemokines and chemokine
receptors are being investigated for their role in tumor development
and metastasis and may prove to be useful therapeutic targets.
The chemokine family is a complex network of molecules that
are ubiquitously expressed and perform a variety of functions
most notably regulating the immune system. Here we review
the importance of chemokines in the tumor-stromal interaction
and discuss current concepts for targeting the chemokine network.
[Back to top]
The JAK-STAT Pathway: A Therapeutic Target
in Hematological Malignancies
A. Ferrajoli, S. Faderl, F. Ravandi and Z. Estrov
The development and function of hematopoietic cells
depends on complex signaling pathways that are mediated by
numerous cytokines and their receptors. The Janus kinase-signal
transducer and activator of transcription (JAK-STAT) pathway
is prominent both in normal hematopoiesis and in hematological
malignancies. STATs are phosphorylated on tyrosine residues
via JAK kinases and on serine residues by a variety of serine/threonine
kinases. STATs then dimerize, translocate to the nucleus and
bind DNA, initiating the transcription of target genes. STAT
proteins mediate cell growth, differentiation, apoptosis,
transformation, and other fundamental cell functions.
Recently, mutations in the JAK2 gene driving the proliferation
of the neoplastic clone have been identified in myeloproliferative
disorders. In addition constitutive activation of the JAK-STAT
pathway has been reported in various types of leukemias such
as acute myelogenous leukemia, T-LGL leukemia, and multiple
myeloma. This review describes the pathophysiological role
of this pathway in hematological malignancies and the potential
benefits of JAK-STAT inhibition.
[Back to top]
Modulation of the Cell Cycle and Induction
of Apoptosis in Human Cancer Cells by Synthetic Bile Acids
Nam Deuk Kim, Eunok Im, Young Hyun Yoo and Yung
Hyun Choi
In this paper, we will outline the current understanding
of cell cycle modulation and induction of apoptosis in cancer
cells by natural and synthetic bile acid. Bile acid homeostasis
is tightly regulated in health, and their cellular and tissue
concentrations are restricted. However, when pathophysiological
processes impair their biliary secretion, hepatocytes are
exposed to elevated concentrations of bile acids which trigger
cell death. In this context, we developed several newly synthesized
bile acid derivatives. These synthetic bile acids modulated
the cell cycle and induced apoptosis in several human cancer
cells similar to natural bile acids. In human breast and prostate
cancer cells with different tumor suppressor p53 status, synthetic
bile acid-induced growth inhibition and apoptosis were associated
with up-regulation of Bax and p21WAF1/CIP1 via
a p53-independent pathway. In Jurkat human T cell leukemia
cells, the synthetic bile acids induced apoptosis through
caspase activation. In addition to this, the synthetic bile
acids induced apoptosis in a JNK dependent manner in SiHa
human cervical cancer cells, via induction of Bax
and activation of caspases in PC3 prostate cancer cells and
induction of G1 phase arrest in the cell cycle in HT29 colon
cancer cells. Moreover, they induced apoptosis in four human
glioblastoma multiform cell lines (i.e., U-118MG, U-87MG,
T98G, and U-373MG) and one human TE671 medulloblastoma cells.
In addition to this, a chenodeoxycholic acid derivative, called
HS-1200, significantly decreased the growth of TE671 medulloblastoma
tumor size and increased life span in non-obese diabetic and
severe combined immunodeficient (NOD/SCID) mice. Therefore,
these new synthetic bile acids, which are novel apoptosis
mediators, might be applicable to the treatment of various
human cancer cells.
[Back to top]
EGFR-Targeting Monoclonal Antibodies in
Head and Neck Cancer
Igor Astsaturov, Roger B. Cohen and Paul M. Harari
The epidermal growth factor (EGF) and its receptor
were discovered nearly 40 years ago. Over the past decade
interruption of this pathway has been exploited in the treatment
of various solid tumors. Antibodies that interfere with ligand
binding to and dimerization of the EGFR (and small molecules
that inhibit the EGFR tyrosine kinase) are anti-proliferative,
radiosensitizing, and synergistic with DNA-damaging cytotoxic
agents. Proposed mechanisms of radio- and chemosensitization
include enhanced apoptosis, interference with DNA repair and
angiogenesis, receptor depletion from the cell surface and
antibody-dependent cell-mediated cytotoxicity.
This article provides the reader with a comprehensive review
of EGFR-targeting antibodies under development for the treatment
of head and neck squamous cell cancer (HNSCC) and also summarizes
relevant clinical data in this disease with small molecule
EGFR inhibitors. One of the monoclonal antibodies, cetuximab,
recently received full FDA approval for the treatment of patients
with locoregionally advanced (with radiation) or metastatic
HNSCC (as a single agent). Regulatory approval followed reporting
of a large international study in which the addition of cetuximab
to definitive radiation therapy in HNSCC resulted in statistically
significant improvements in locoregional control and overall
survival. Results of the pivotal trial, other clinical data
supporting the regulatory approval, and a preview of the next
generation of clinical trials are presented. Considerable
work remains to be done, particularly to enhance our understanding
of factors that may predict for favorable response to EGFR
inhibitor therapy and to evaluate the impact of integrating
anti-EGFR therapies into complex chemoradiation programs delivered
with curative intent.
[Back to top]
Chemopreventive Agents Alters Global Gene
Expression Pattern: Predicting their Mode of Action and Targets
Bhagavathi A. Narayanan
Chemoprevention has the potential to be a major
component of colon, breast, prostate and lung cancer control.
Epidemiological, experimental, and clinical studies provide
evidence that antioxidants, anti-inflammatory agents, n-3
polyunsaturated fatty acids and several other phytochemicals
possess unique modes of action against cancer growth. However,
the mode of action of several of these agents at the gene
transcription level is not completely understood. Completion
of the human genome sequence and the advent of DNA microarrays
using cDNAs enhanced the detection and identification of hundreds
of differentially expressed genes in response to anticancer
drugs or chemopreventive agents. In this review, we are presenting
an extensive analysis of the key findings from studies using
potential chemopreventive agents on global gene expression
patterns, which lead to the identification of cancer drug
targets. The summary of the study reports discussed in this
review explains the extent of gene alterations mediated by
more than 20 compounds including antioxidants, fatty acids,
NSAIDs, phytochemicals, retinoids, selenium, vitamins, aromatase
inhibitor, lovastatin, oltipraz, salvicine, and zinc. The
findings from these studies further reveal the utility of
DNA microarray in characterizing and quantifying the differentially
expressed genes that are possibly reprogrammed by the above
agents against colon, breast, prostate, lung, liver, pancreatic
and other cancer types. Phenolic antioxidant resveratrol found
in berries and grapes inhibits the formation of prostate tumors
by acting on the regulatory genes such as p53 while activating
a cascade of genes involved in cell cycle and apoptosis including
p300, Apaf-1, cdk inhibitor p21, p57 (KIP2), p53 induced Pig
7, Pig 8, Pig 10, cyclin D, DNA fragmentation factor 45. The
group of genes significantly altered by selenium includes
cyclin D1, cdk5, cdk4, cdk2, cdc25A and GADD 153. Vitamine
D shows impact on p21(Waf1/Cip1) p27 cyclin B and cyclin A1.
Genomic expression profile with vitamin D indicated differential
expression of gene targets such as c-JUN, JUNB, JUND, FREAC-1/FoxF1,
ZNF-44/KOX7, plectin, filamin, and keratin-13, involved in
antiproliferative, differentiation pathways. The agent UBEIL
has a remarkable effect on cyclin D1. Curcumin mediated NrF2
pathway significantly altered p21(Waf1/Cip1) levels. Aromatase
inhibitors affected the expression of cyclin D1. Interestingly,
few dietary compounds listed in this review also have effect
on APC, cdk inhibitors p21(Waf1/Cip1) and p27. Tea polyphenol
EGCG has a significant effect on TGF-β
expression, while several other earlier studies have shown
its effect on cell cycle regulatory proteins. This review
article reveals potential chemoprevention drug targets, which
are mainly centered on cell cycle regulatory pathway genes
in cancer.
[Back to top]
Anti-Invasive and Anti-Metastasis Strategies:
New Roads, New Tools and New Hopes
Laurent Dollé, Herman T. Depypere and Marc
E. Bracke
Unfortunately, the anticancer drugs that are used
nowadays in the clinic have only limited success. To provide
a significant clinical advancement, new concepts have to be
introduced to aid the design of new tools for therapy. Cancer
is not only restricted to neoplastic cells, but rather it
involves an ensemble of protagonists. In addition, the evolution
of cancer is extremely complex, since multiple cellular activities
are involved. Some key steps in the evolution to a metastatic
tumor have been shown to be no useful targets. Targeting the
stroma cells, however, could bring a new efficiency in anticancer
treatment. Targeting the disorganized tissue architecture
at the primary site and the restoration of the cell death
program in cancer cells appears to create new possibilities
in drug design. Also the cytoskeleton, which represents a
dynamic set due to its plasticity and multiplicity, seems
to be a promising target in anticancer therapy. Moreover,
the evolving knowledge of the role of metastasis suppressor
genes in regulating cancer cell growth at the secondary site
suggests that they could serve as new targets for therapeutic
intervention. This review intends to highlight the unraveling
of new therapeutic pathways, and to unveil new powerful research
tools for combating metastasis.
|
