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This is a comprehensive reference survey on the identification and
development of promising cancer chemopreventive agents that will
help stimulate further novel research and new approvable drugs. For
each agent, the authors review the relevant mechanisms of action,
the criteria for populations benefiting from intervention, the
safety and pharmacodynamics, clinical study design emphasizing the
use of precancers, and early associated cellular and molecular
biomarkers of carcinogenesis. The pharmacologic and/or mechanistic
classes discussed range from antimutagens, antiinflammatories, and
the nuclear receptor superfamily, to signal transduction
modulators, antioxidants, vitamins, and minerals. The overall focus
is on molecular targets and mechanisms. A second volume,
"Strategies in Chemoprevention", describes the exciting
methodologies that will accelerate progress in this field and
discusses the state of clinical development of chemoprevention in
the various human cancer target organs.
Despite significant advances in cancer treatment and measures of
neoplastic progression, drug effect (or early detection, overall
cancer incidence has increased, pharmacodynamic markers), and
markers that measure cancer-associated morbidity is considerable,
and overall prognosis as well as predict responses to specific
therapy. cancer survival has remained relatively flat over the past
All these biomarkers have the potential to greatly augment several
decades (1,2). However, new technology the development of
successful chemoprevention therapies, allowing exploration of
signal transduction pathways, but two specific types of biomarkers
will have the most identification of cancer-associated genes, and
imaging of immediate impact on successful chemopreventive drug
tissue architecture and molecular and cellular function is
development-those that measure the risk of developing increasing
our understanding of carcinogenesis and cancer invasive
life-threatening disease, and those whose mo- progression. This
knowledge is moving the focus of cancer lation can "reasonably
predict" clinical benefit and, therapeutics, including cancer
preventive treatments, to therefore, serve as surrogate endpoints
for later-occurring drugs that take advantage of cellular control
mechanisms clinical disease. Thus far, the biomarker that best
measures to selectively suppress cancer progression. these two
phenomena is intraepithelial neoplasia (IEN) Carcinogenesis is now
visualized as a multifocal, because it is a near obligate precursor
to cancer.
A comprehensive reference survey on the identification and
development of promising cancer chemopreventive agents that will
help stimulate further novel research and new approvable drugs. For
each agent, the authors review the relevant mechanisms of action,
the criteria for populations benefiting from intervention, the
safety and pharmacodynamics, clinical study design emphasizing the
use of precancers, and early associated cellular and molecular
biomarkers of carcinogenesis. The pharmacologic and/or mechanistic
classes discussed range from antimutagens, antiinflammatories, and
the nuclear receptor superfamily, to signal transduction
modulators, antioxidants, vitamins, and minerals. The overall focus
is on molecular targets and mechanisms. A second volume, Strategies
in Chemoprevention, describes the exciting methodologies that will
accelerate progress in this field and discusses the state of
clinical development of chemoprevention in the various human cancer
target organs.
Despite significant advances in cancer treatment and measures of
neoplastic progression, drug effect (or early detection, overall
cancer incidence has increased, pharmacodynamic markers), and
markers that measure cancer-associated morbidity is considerable,
and overall prognosis as well as predict responses to specific
therapy. cancer survival has remained relatively flat over the past
All these biomarkers have the potential to greatly augment several
decades (1,2). However, new technology the development of
successful chemoprevention therapies, allowing exploration of
signal transduction pathways, but two specific types of biomarkers
will have the most identification of cancer-associated genes, and
imaging of immediate impact on successful chemopreventive drug
tissue architecture and molecular and cellular function is
development-those that measure the risk of developing increasing
our understanding of carcinogenesis and cancer invasive
life-threatening disease, and those whose mo- progression. This
knowledge is moving the focus of cancer lation can "reasonably
predict" clinical benefit and, therapeutics, including cancer
preventive treatments, to therefore, serve as surrogate endpoints
for later-occurring drugs that take advantage of cellular control
mechanisms clinical disease. Thus far, the biomarker that best
measures to selectively suppress cancer progression. these two
phenomena is intraepithelial neoplasia (IEN) Carcinogenesis is now
visualized as a multifocal, because it is a near obligate precursor
to cancer.
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