Current Cancer
Drug Targets
ISSN: 1568-0096
Current Cancer Drug Targets
Volume 7, Number 4, June 2007
Contents
Transription Factors and their Modulated Genes as
Targets for Chemoprevention
Guest Editor: Chuanshu Huang
Editorial Pp. 303
The PI3K/Akt Pathway and Its Downstream Transcriptional
Factors as Targets for Chemoprevention Pp. 305-316
Xinhai Zhang, Boquan Jin and Chuanshu Huang
[Abstract]
AP-1 a Target for Cancer Prevention Pp. 317-324
Connie P. Matthews, Nancy H. Colburn and Matthew R. Young
[Abstract]
Ultraviolet B Regulation of Transcription Factor Families:
Roles of Nuclear Factor-kappa B (NF-κB)
and Activator Protein-1 (AP-1) in UVB-Induced Skin Carcinogenesis
Pp. 325-334
S.J. Cooper and G.T. Bowden
[Abstract]
ATM-NF-κB
Connection as a Target for Tumor Radiosensitization
Pp. 335-342
Kazi Mokim Ahmed and Jian Jian Li
[Abstract]
Transcription Factor NFAT, Its Role in Cancer Development,
and as a Potential Target for Chemoprevention Pp.
343-353
Haitian Lu and Chuanshu Huang
[Abstract]
Transcription Factors: Molecular Targets for Prostate
Cancer Intervention by Phytochemicals Pp. 355-367
Manjinder Kaur and Rajesh Agarwal
[Abstract]
General Articles
Hsp90: A Novel Target for the Disruption of Multiple
Signaling Cascades Pp. 369-388
Stephanie C. Bishop, Joseph A. Burlison and Brian S.J.
Blagg
[Abstract]
Combining Radiation and Cancer Gene Therapy: A Potential
Marriage of Physical and Biological Targeting? Pp.
389-409
M. Hingorani, C.L. White, V.K. Agrawal, L. Vidal , A.
Melcher and K.J. Harrington
[Abstract]
Abstracts
[Back to top]
Editorial
Cancer development is recognized as a multi-stage phenomenon
consisting of initiation, promotion and progression stages.
The rate-limiting steps in multistage carcinogenesis are now
thought to reside during the period of tumor promotion and
progression. Exposure to tumor promoters results in activation
of transcription factors, and regulation of their target genes
through signal transduction pathways, which have been characterized
as tumor promotion and progression stages. Therefore, one
of the most difficult challenges for scientists in the cancer
research field is addressing fundamental questions concerning
the response of mammalian cells to carcinogens at the level
of transcription factors and protein kinases both in vitro
and in vivo. Elucidation of carcinogen-induced signal
transduction pathways leading to the activation of transcription
factors by which gene expression is mediated will therefore,
not only define the central scientific hunt in cancer biology
and open an unprecedented window into the nature of cancer,
but will also be necessary for cancer prevention and therapy
as well.
Chemoprevention can be defined as the use of substances that
interfere with the process of cancer development. Since cancer
is a multifactor disease that requires the modulation of multiple
pathways, chemoprevention could target multiple targets. These
targets include transcription factors, kinase cascades leading
to activation, as well as downstream target genes of those
transcription factors. Although substantial progress has been
made in elucidating signal transduction pathways leading to
the activation of transcription factors induced by carcinogens,
further advances are needed to identify molecular targets
for effective use of chemopreventive agents. This special
issue describes the most recent progress made in this field.
The PI3K/Akt signaling pathway is a relative early event involved
in the mediation of the activation of its downstream transcription
factors. Growing evidence demonstrates that dysregulation
of this pathway is critical for the carcinogenic effect upon
environmental carcinogen exposure. The first review article
provided by Dr. Huang and his colleague summarizes the PI3K/Akt
pathway, its downstream regulated transcriptional factors,
and the dysregulation of this pathway in carcinogenesis, as
well as the chemoprevention strategies targeting those components.
The transcription factor activator protein-1 (AP-1) plays
a pivotal role in inflammation and tumorigenesis, which has
been supported in research both in vitro and in
vivo. AP-1 could also act as a link between chronic inflammation
and tumor development. The second review by Drs. Matthews,
Colburn and Young has addressed the AP-1 family proteins,
its relation to inflammation and cancer development, and as
targets for chemoprevention.
More than 1,000,000 cases of non-melanoma skin cancer (NMSC)
are diagnosed in the Unites States each year. Solar radiation
has been described as an important etiological factor in the
development of NMSC. Damage of cells induced by ultraviolet
B (UVB) light at the DNA level and molecular level initiates
the activation of transcription factor pathways, which in
turn, regulate the expression of a number of genes termed
the “UV response genes”. Nuclear factor-κB
(NF-κB)
and AP-1 are two important transcription factors that are
responsible for the regulation of those response genes. The
review from Dr. Bowden’s group has extensively discussed
the advances made in this research area.
Ionizing radiation (IR) is another environmental carcinogenic
factor. Dr. Li’s review article has focused on recent
findings related to the relationship between ATM and NF-κB
in response to IR, and the association of ATM with the NF-κB
subunit p65 in adaptive radiation response as well.
Nuclear factor of activated T cells (NFAT) is another important
family of transcription factors which have important roles
in various cell functions. In the last a few years, there
has been increasing evidence relating NFAT family proteins
to carcinogenesis, even though various members may have different
roles. Dr. Huang and his colleague have also outlined the
results from the studies in this field.
Recently, chemoprevention by the use of naturally occurring
substances is considered as a priority to reduce the ever-increasing
incidence of cancer. The intervention of multistage carcinogenesis
by modulating intracellular signaling pathways may provide
a molecular basis of chemoprevention with a wide variety of
dietary phytochemicals. In the last review, Dr. Agarwal and
his colleagues have discussed the efficacy of various phytochemicals
in targeting transcription factors in the context of prostate
cancer intervention.
Identification of signaling molecules associated with carcinogenesis
as prime targets of chemopreventive agents has become an area
of great interest. Although six review articles have been
included in the special issue on this topic, I definitely
believe that some cancer related transcription factors and
kinases are not yet included. I wish to have opportunity to
include those studies in a special issue in the near future.
Finally, I would like to thank all the authors for their contribution,
and those who provided excellent manuscript peer-reviews in
a timely fashion.
Chuanshu Huang, M.D., Ph.D.
Associate Professor
Nelson Institute of Environmental Medicine
NYU School of Medicine 57 Old Forge Road,
Tuxedo, NY 10987, USA;
Tel: 845-731-3519; Fax: 845-351-2320;
E-mail: chuanshu@env.med.nyu.edu
[Back to top]
The PI3K/Akt Pathway and Its Downstream Transcriptional
Factors as Targets for Chemoprevention
Xinhai Zhang, Boquan Jin and Chuanshu Huang
The PI3K/Akt signalling pathway and its downstream transcription
factors have been intensively studied for their role in cell
proliferation, survival, cycle control, as well as other cellular
functions. There is growing evidence showing that dysregulation
of this pathway also plays an essential role in cancer development.
The overexpression or permanent activation of RTKs and GPCRs,
as well as the exposure to environmental carcinogens cause
constant activation of PI3K/Akt. On the other hand, PI3K/Akt
themselves can also become hyperactivated due to gene amplification
or PTEN inactivation. Consequently, the targets downstream
of PI3K/Akt can be abnormally activated, which promote proliferation
and survival of cancer cells in carcinogenesis. Among these
targets we find that the NFκB
and AP-1 are the most interesting. Therefore, methods and
compounds aiming to inhibit the altered components of this
pathway can simultaneously prevent the proliferation of tumor
cells and sensitize them toward apoptosis. To this regard,
the natural compounds from vegetables and fruits with high
affinity and non toxicity to target the PI3K/Akt pathway and
prevent cancer are attractive.
[Back to top]
AP-1 a Target for Cancer Prevention
Connie P. Matthews, Nancy H. Colburn and Matthew R. Young
The transcription factor activator protein 1 (AP-1) plays
a pivotal role in tumorigenesis. AP-1 activity is increased
in multiple human tumor types. Inhibitors of AP-1 have been
shown to block tumor promotion, transformation, progression
and invasion. Chronic inflammation and tumor development are
linked. AP-1 may act, in part, by perpetuating the inflammatory
signal. AP-1 is a recognized molecular target of many antioxidant
and anti-inflammatory chemopreventive compounds. This review
focuses on the AP-1 family proteins as targets for chemoprevention.
[Back to top]
Ultraviolet B Regulation of Transcription Factor Families:
Roles of Nuclear Factor-kappa B (NF-κB)
and Activator Protein-1 (AP-1) in UVB-Induced Skin Carcinogenesis
S.J. Cooper and G.T. Bowden
Prolonged and repeated exposure of the skin to ultraviolet
light (UV) leads not only to aging of the skin but also increases
the incidence of non-melanoma skin cancer (NMSC). Damage of
cells induced by ultraviolet B (UVB) light both at the DNA
level and molecular level initiates the activation of transcription
factor pathways, which in turn regulate the expression of
a number of genes termed the “UV response genes”.
Two such transcription factor families that are activated
in this way are those of the nuclear factor-κB
(NF-κB)
and activator protein-1 (AP-1) families. These two transcription
factor families have been identified to be involved in the
processes of cell proliferation, cell differentiation and
cell survival and therefore play important roles in tumorigenesis.
The study of these two transcription factor pathways and the
cross-talk between them in response to UVB exposure may help
with the development of new chemopreventive strategies for
the prevention of UVB-induced skin carcinogenesis.
[Back to top]
ATM-NF-κB
Connection as a Target for Tumor Radiosensitization
Kazi Mokim Ahmed and Jian Jian Li
Ionizing radiation (IR) plays a key role in both areas of
carcinogenesis and anticancer radiotherapy. The ATM (ataxia-telangiectasia
mutated) protein, a sensor to IR and other DNA-damaging agents,
activates a wide variety of effectors involved in multiple
signaling pathways, cell cycle checkpoints, DNA repair and
apoptosis. Accumulated evidence also indicates that the transcription
factor NF-κB
(nuclear factor-kappaB) plays a critical role in cellular
protection against a variety of genotoxic agents including
IR, and inhibition of NF-κB
leads to radiosensitization in radioresistant cancer cells.
NF-κB
was found to be defective in cells from patients with A-T
(ataxia-telangiectasia) who are highly sensitive to DNA damage
induced by IR and UV lights. Cells derived from A-T individuals
are hypersensitive to killing by IR. Both ATM and NF-κB
deficiencies result in increased sensitivity to DNA double
strand breaks. Therefore, identification of the molecular
linkage between the kinase ATM and NF-κB
signaling in tumor response to therapeutic IR will lead to
a better understanding of cellular response to IR, and will
promise novel molecular targets for therapy-associated tumor
resistance. This review article focuses on recent findings
related to the relationship between ATM and NF-κB
in response to IR. Also, the association of ATM with the NF-κB
subunit p65 in adaptive radiation response, recently observed
in our lab, is also discussed.
[Back to top]
Transcription Factor NFAT, Its Role in Cancer Development,
and as a Potential Target for Chemoprevention
Haitian Lu and Chuanshu Huang
The nuclear factor of activated T cells (NFAT) family proteins
are transcription factors that regulate the expression of
a variety of target genes with or without forming complexes
with other transcription factors. Although NFAT proteins have
been extensively investigated and characterized in immune
systems, their role in carcinogenesis are far from being understood.
We, to our knowledge, are first to determine the potential
involvement of the NFAT pathway in cell responses to carcinogen
exposure. Experimental evidence accumulated from our studies
indicate the critical role of NFAT3 in some carcinogen-induced
cell transformation and tumorigenicity. Moreover, NFAT proteins
have been found to be involved in cell cycle regulation, cell
differentiation, cell survival, angiogenesis, and tumor cell
invasion and metastasis. In the meantime, NFAT inhibitors
are being developed with the ultimate aim to specifically
switch off NFAT signaling without side effects. This review
comprehensively reviews the results from the most recent studies,
and also discusses some difficulties in current studies. To
validate whether NFAT can be a promising target for chemoprevention,
more research has to be done to further detail the roles of
NFAT and to differentiate the functions of different members
of this protein family in future studies.
[Back to top]
Transcription Factors: Molecular Targets for Prostate
Cancer Intervention by Phytochemicals
Manjinder Kaur and Rajesh Agarwal
With increasing incidence of cancer at most of the sites,
and growing economic burden and associated psychological and
emotional trauma, it is becoming clearer that more efforts
are needed for cancer cure. Since most of the chemotherapeutic
drugs are non-selective because they are also toxic to the
normal cells, new and improved strategies are needed that
selectively target the killing of cancer cells. Since aberrant
activation of numerous signaling pathways is a key element
of cancer cell survival and growth, blocking all of them is
not that practical, which leads to the step where most of
them commonly converge; the transcription factors. Recent
research efforts, therefore, are also directed on targeting
the activity and activation of transcription factors, which
ultimately control the expression of genes that are involved
in almost all aspects of cell biology. One class of agents
that is becoming increasingly successful, not only in targeting
signaling cascades, but also transcription factors is phytochemicals
present in diet and those consumed as supplement. The added
advantage with these agents is that they are mostly non-toxic
when compared to chemotherapeutic agents. This review focuses
on the efficacy of various phytochemicals in targeting transcription
factors such as AR, Sp1, STATs, E2F, Egr1, c-Myc, HIF-1α,
NF-κB,
AP-1, ETS2, GLI and p53 in the context of prostate cancer
intervention.
[Back to top]
Hsp90: A Novel Target for the Disruption of Multiple
Signaling Cascades
Stephanie C. Bishop, Joseph A. Burlison and Brian S.J.
Blagg
The 90 kDa heat shock proteins (Hsp90) are proving to be an
excellent target for the development of novel anti-cancer
agents designed to selectively block the growth and proliferation
of tumor cells. Since Hsp90 is a molecular chaperone and is
responsible for folding numerous oncogenic proteins, its inhibition
represents a novel approach toward the simultaneous disruption
of multiple signaling cascades. This review summarizes recent
literature implicating Hsp90 as a key facilitator for the
maturation of proteins represented in all six hallmarks of
cancer: 1) growth signal self-sufficiency, 2) anti-growth
signal insensitivity, 3) evasion of apoptosis, 4) unlimited
replicative potential, 5) metastasis and tissue invasion,
and 6) sustained angiogenesis. Also described are recent advances
towards the development of novel Hsp90 inhibitors via
structure-based drug design that have contributed to the number
of compounds undergoing clinical development.
[Back to top]
Combining Radiation and Cancer Gene Therapy: A Potential
Marriage of Physical and Biological Targeting?
M. Hingorani, C.L. White, V.K. Agrawal, L. Vidal , A.
Melcher and K.J. Harrington
The development and progression of cancer is marked by the
acquisition of specific genetic hallmarks that endow tumour
cells with a survival advantage over their normal tissue counterparts.
In the process, tumours frequently develop resistance to radiotherapy
and chemotherapy, and acquire the ability to evade the host
immune response. Cancer gene therapy (CGT) represents an ideal
therapeutic tool to target one or more of these underlying
genetic abnormalities, and restore some form of order, to
the otherwise autonomous and discordant microenvironment of
the tumour.
Most of the current research in CGT is aimed at its development
as a novel form of targeted therapy that can be combined with
other treatment modalities such as radiotherapy and chemotherapy.
CGT may be integrated into radical chemoradiotherapy regimens,
with the rationale of optimising the therapeutic index, through
selective enhancement of radiosensitivity and cytotoxicity
in tumour compared to normal tissues.
CGT strategies have been developed that are aimed at enhancing
the radiosensitivity of tissues by targeting angiogenesis,
silencing abnormal cellular signalling, restoration of apoptosis,
and promotion of immune detection and destruction of tumour
cells. In addition, cytotoxic approaches such as virus directed
enzyme prodrug therapy (VDEPT), genetic radionuclide therapy
(GRANT) and oncolytic viral therapy have been combined with
radiation to augment the cumulative tumour cell kill and overall
therapeutic effect.
In this article, we discuss various CGT strategies that have
been investigated in combination with radiation. All the available
preclinical and clinical evidence is reviewed with special
emphasis on strategies that have already found their way into
the clinic, or those with significant translational potential
for the future.
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