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Current
Pharmaceutical Design
ISSN: 1381-6128
Current Pharmaceutical Design
Volume 14, Number 10, 2008
Contents
Advanced Glycation End Products (AGEs) and their Receptor
(RAGE) in Health and Disease
Executive Editor: Sho-ichi Yamagishi
Editorial: Pp. 939
AGE-RAGE System and Carcinogenesis Pp. 940-945
R. Abe and S-i. Yamagishi
[Abstract]
Role of AGEs in Diabetic Nephropathy Pp. 946-952
K. Fukami, S-i. Yamagishi, S. Ueda and S. Okuda
[Abstract]
Role of Advanced Glycation End Products in Diabetic Neuropathy
Pp. 953-961
K. Sugimoto, M. Yasujima and S. Yagihashi
[Abstract]
Role of Advanced Glycation End Products (AGEs) and Oxidative
Stress in Diabetic Retinopathy Pp. 962-968
S-i. Yamagishi, S. Ueda, T. Matsui, K. Nakamura and
S. Okuda
[Abstract]
Advanced Glycation End Products (AGEs) and their Involvement
in Liver Disease Pp. 969-972
H. Hyogo and S-i. Yamagishi
[Abstract]
Possible Involvement of Advanced Glycation End Products (AGEs)
in the Pathogenesis of Alzheimer’s Disease
Pp. 973-978
M. Takeuchi and S-i. Yamagishi
[Abstract]
The Role of AGEs in Cardiovascular Disease Pp. 979-986
K. Jandeleit-Dahm and M.E. Cooper
[Abstract]
Advanced Glycation End Products and Insulin Resistance Pp.
987-989
H. Unoki and S-i. Yamagishi
[Abstract]
General Articles
Potential Strategies for Minimizing Mechanism-Based
Inhibition of Cytochrome P450 3A4 Pp. 990-1000
S-F. Zhou
[Abstract]
Recent Developments in the Chemistry and in the Biological
Applications of Amidoximes Pp. 1001-1047
K.C. Fylaktakidou, D.J. Hadjipavlou-Litina, K.E.
Litinas, E.A. Varella and D.N. Nicolaides
[Abstract]
Abstracts
[Back to top]
Editorial: Advanced Glycation End Products
(AGEs) and their Receptor (RAGE) in Health and Disease
There is a growing body of evidence to show that
AGEs, which form and accumulate at an accelerated rate under
diabetes and normal aging, are implicated in the pathogenesis
of various devastating disorders such as diabetic vascular
complications, coronary heart diseases, Alzheimer’s
disease, cancer growth and metastasis, insulin resistance
and nonalcoholic fatty liver disease. In addition, the engagement
of the receptor for AGEs, RAGE with the macroprotein derivatives
is reported to elicit oxidative stress and vascular inflammation
and subsequently activate the downstream signalings, thereby
being involved in the development and progression of these
devastating disorders. These observations suggest that the
AGEs-RAGE axis is a novel therapeutic target for various disorders.
In this issue, I would like to reinforce the emerging knowledge
regarding AGEs and RAGE as an important mediator in health
and disease. I believe that the issue is helpful for most
of the researchers and physicians in the field of drug design
and clinical pharmacology, especially those who would like
to understand the pathophysiological role of the AGEs-RAGE
system in health and numerous devastating disorders.
Sho-ichi Yamagishi
Department of Medicine
Kurume University School of Medicine
Kurume 830-0011
Japan
E-mail: shoichi@med.kurume-u.ac.jp
[Back to top]
AGE-RAGE System and Carcinogenesis
R. Abe and S-i. Yamagishi
Recent clinical studies have reported an increased risk for
various types of cancers in patients with diabetes. Diabetes
is characterized by increased oxidative stress conditions.
Hyperglycemia induces oxidative stress generation in a variety
of cells via various metabolic pathways, thus causing
oxidative DNA damage, an initial step of carcinogenesis. There
is accumulating evidence that advanced glycation end products
(AGE), senescent macroprotein derivatives formed at an accelerated
rate under normal aging process and diabetes, are involved
in the development and progression of cancers. AGE stimulate
oxidative stress generation through the interaction with a
receptor for AGE (RAGE), while oxidative stress generation
promotes the formation of AGE and increases the expression
of RAGE. These findings suggest that the crosstalk between
the AGE-RAGE system and oxidative stress generation may form
a positive feedback loop, thus further increasing the risk
for cancers in patients with diabetes. This paper reviews
current knowledge about the role of AGE-RAGE system in the
development of various types of cancers.
[Back to top]
Role of AGEs in Diabetic Nephropathy
K. Fukami, S-i. Yamagishi, S. Ueda and S. Okuda
Diabetic nephropathy is the most common cause of end-stage
renal disease in the world, and accounts for a significant
increase in morbidity and mortality in patients with diabetes.
Therapeutic options such as strict blood pressure and/or glycemic
control are effective for preventing the development and progression
of diabetic nephropathy, but the number of diabetic patients
on hemodialysis is still increasing. Therefore, a novel therapeutic
strategy that could halt the progression of diabetic nephropathy
should be developed. Advanced glycation end products (AGEs)
are heterogeneous cross-linked sugar-derived proteins which
could accumulate in glomerular basement membrane, mesangial
cells, endothelial cells, and podocytes in patients with diabetes
and/or end-stage renal failure. AGEs are thought to be involved
in the pathogenesis of diabetic nephropathy via multifactorial
mechanisms such as oxidative stress generation and overproduction
of various growth factors and cytokines. Further, recently,
the cross-talk between AGEs and the renin-angiotensin system
(RAS) has been proposed to participate in diabetic nephropathy.
In addition, activation of the RAS elicits ROS generation
and subsequently stimulates growth factor and cytokine production
by kidney cells as well. These observations suggest that combination
therapy with inhibitors of the RAS and blockers of the AGEs
formation and/or their downstream pathway may be a novel therapeutic
option for preventing diabetic nephropathy. In this paper,
we review the role of AGEs and their receptor system in the
pathogenesis of diabetic nephropathy. We further discuss here
the cross-talk between AGEs and the RAS in the development
and progression of diabetic nephropathy.
[Back to top]
Role of Advanced Glycation End Products in Diabetic Neuropathy
K. Sugimoto, M. Yasujima and S. Yagihashi
Diabetic neuropathy is the commonest form of peripheral
neuropathy in the developed countries of the world. In diabetic
patients, the presence of peripheral neuropathy increases
their risks for developing foot ulceration and subsequent
necrosis that necessitates lower limb amputation. Although
the precise mechanisms underlying diabetic neuropathy remain
unclear, there is evidence that hyperglycemia-induced formation
of advanced glycation end products (AGEs) is related to diabetic
neuropathy; AGE-modified peripheral nerve myelin is susceptible
to phagocytosis by macrophages and contributes to segmental
demyelination; modification of major axonal cytoskeletal proteins
such as tubulin, neurofilament, and actin by AGEs results
in axonal atrophy/degeneration and impaired axonal transport;
and glycation of extracellular matrix protein laminin leads
to impaired regenerative activity in diabetic neuropathy.
Recently, the receptor for AGEs (RAGE) has been found to colocalize
with AGEs in diabetic peripheral nerves. This suggests that,
in diabetic neuropathy, AGEs and AGE/RAGE interactions induce
oxidative stress, result in upregulation of nuclear factor
(NF)-kappaB and various NF-kappaB-mediated proinflammatory
genes, and exaggerate neurological dysfunction, including
altered pain sensation. Additionally, AGE/RAGE-induced oxidative
stress further accelerates formation of glycoxidation products
such as Nepsilon-(carboxymethyl)lysine and pentosidine. Although
new drugs that inhibit the formation of AGEs and block the
AGE-RAGE interaction are being studied, no effective treatment
modalities against AGE-induced nerve injury are currently
available clinically. A therapeutic strategy to prevent and
ameliorate diabetic neuropathy using anti-AGE agents needs
to be established. In this review, the current issues involved
in the role of the glycation process and the potential treatment
options for diabetic neuropathy are explored.
[Back to top]
Role of Advanced Glycation End Products (AGEs) and Oxidative
Stress in Diabetic Retinopathy
S-i. Yamagishi, S. Ueda, T. Matsui, K. Nakamura and
S. Okuda
Diabetic retinopathy is a common and potentially
devastating microvascular complication in diabetes and is
a leading cause of acquired blindness among the people of
occupational age. However, current therapeutic options for
the treatment of sight-threatening proliferative diabetic
retinopathy such as photocoagulation and vitrectomy are limited
by considerable side effects and far from satisfactory. Therefore,
to develop novel therapeutic strategies that specifically
target diabetic retinopathy is actually desired for most of
the patients with diabetes. Chronic hyperglycemia is a major
initiator of diabetic retinopathy. However, recent clinical
study has substantiated the concept of ‘hyperglycemic
memory’ in the pathogenesis of diabetic retinopathy.
Indeed, the Diabetes Control and Complications Trial-Epidemiology
of Diabetes Interventions and Complications (DCCT-EDIC) Research,
has revealed that the reduction in the risk of progressive
retinopathy resulting from intensive therapy in patients with
type 1 diabetes persisted for at least several years after
the DCCT trial, despite increasing hyperglycemia. These findings
suggest a longterm beneficial influence of early metabolic
control on clinical outcomes in type 1 diabetic patients.
Among various biochemical pathways implicated in the pathogenesis
of diabetic retinopathy, the process of formation and accumulation
of advanced glycation end products (AGEs) and their mode of
action are most compatible with the theory ‘hyperglycemic
memory’. Further, there is a growing body of evidence
that AGEs-RAGE (receptor for AGEs) interaction-mediated oxidative
stress generation plays an important role in diabetic retinopathy.
This article summarizes the role of AGEs and oxidative stress
in the development and progression of diabetic retinopathy
and the therapeutic interventions that could prevent this
devastating disorder. We also discuss here the pathological
crosstalk between the AGEs-RAGE and the renin-angiotensin
system in diabetic retinopathy and a potential clinical utility
of telmisartan, an angiotensin II type 1 receptor blocker
with peroxisome proliferator-activated recep-tor-γ-modulating
activity.
[Back to top]
Advanced Glycation End Products (AGEs) and their Involvement
in Liver Disease
H. Hyogo and S-i. Yamagishi
Advanced glycation end products (AGEs) are a heterogeneous
group of molecules, formed in vivo both by non-oxidative
and oxidative reactions of sugars and their adducts to proteins
and lipids. It is now well established that formation and
accumulation of AGEs progress during normal aging, and at
an extremely accelerated rate under diabetes, thus being implicated
in various types of AGEs-related disorders such as diabetic
vascular complications, neurodegenerative diseases and cancers.
There is a growing body of evidence that activation of RAGE
(receptor for AGEs) system is also implicated in these devastating
disorders. Indeed, the engagement of RAGE with AGEs is shown
to elicit oxidative stress generation and subsequently evoke
inflammatory responses in various types of cells including
hepatocytes and hepatic stellate cells. Liver is not only
a target organ, but also an important site for clearance and
catabolism of circulating AGEs. Although there are several
papers to suggest the involvement of AGEs-RAGE system in various
types of liver diseases such as non-alcoholic steatohepatitis,
liver cirrhosis and cancers, as far as we know, there are
few comprehensive reviews to deal with this issue. Therefore,
in this paper, we shortly review the pathological role of
AGEs and RAGE in various liver diseases.
[Back to top]
Possible Involvement of Advanced Glycation End Products (AGEs)
in the Pathogenesis of Alzheimer’s Disease
M. Takeuchi and S-i. Yamagishi
Alzheimer's disease (AD) is the most common cause of dementia
in developed countries. AD is characterized pathologically
by the presence of senile plaques (SPs) and neurofibrillary
tangles (NFTs), the major constituents of which are amyloid
β
protein and tau protein, respectively. Advanced glycation
end-products (AGEs), senescent macroprotein derivatives formed
at an accelerated rate under normal aging, can be identified
immunohistochemically in both SPs and NFTs in AD patients.
Further, recent clinical evidence has suggested diabetes mellitus
as one of the risk factors for the development and progression
of AD. Continuous hyperglycemia is a causative factor for
diabetic vascular complications, and it enhances the generation
of AGEs through the non-enzymatic glycation, thereby being
involved in the pathogenesis of AD as well. Moreover, there
is a growing body of evidence to show that the interaction
of AGEs with a receptor for AGEs (RAGE) elicits reactive oxygen
species generation and vascular inflammation, and subsequently
alters various gene expressions in numerous types of cells,
all of which could contribute to the pathological changes
of diabetic vascular complications and AD. Indeed, we have
recently found that glyceraldehyde-derived AGEs (Glycer-AGE)
induce apoptotic cell death in cultured cortical neuronal
cells. In addition, we also found that neurotoxic effect of
diabetic serum on neuronal cells was blocked by neutralizing
antibody raised against Glycer-AGE. In human AD brains, Glycer-AGE
are actually detected in the cytosol of neurons in the hippocampus
and para-hippocampal gyrus. These observations suggest that
Glycer-AGE play a role in the pathogenesis of AD. In this
review, we discuss the pathophysiological role for AGEs in
the development and progression of AD, especially focusing
on Glycer-AGE.
[Back to top]
The Role of AGEs in Cardiovascular Disease
K. Jandeleit-Dahm and M.E. Cooper
Advanced glycation end-products (AGEs) are generated in the
diabetic milieu, as a result of chronic hyperglycemia and
enhanced oxidative stress. These AGEs, via direct
and receptor dependent pathways promote the development and
progression of cardiovascular disease. AGEs accumulate at
many sites of the body including the heart and large blood
vessels in diabetes. These modified proteins interact with
receptors such as RAGE to induce oxidative stress, increase
inflammation by promoting NFκB
activation and enhance extracellular matrix accumulation.
These biological effects translate to accelerated plaque formation
in diabetes as well as increased cardiac fibrosis with consequent
effects on cardiac function. Strategies to reduce the ligation
of AGEs to their receptors such as agents which reduce AGE
accumulation, soluble RAGE which acts as a competitive antagonist
to the binding of AGEs to RAGE and genetic deletions of RAGE
appear to attenuate diabetes associated atherosclerosis. Benefits
on cardiac dysfunction with these inhibitors of the AGE/RAGE
axis are not as well characterised. In conclusion, therapeutic
strategies targeting AGEs appear to have significant clinical
potential, often in combination with currently used agents
such as inhibitors of the renin-angiotensin system, to reduce
the major burden of diabetes, its associated cardiovascular
complications.
[Back to top]
Advanced Glycation End Products and Insulin Resistance
H. Unoki and S-i. Yamagishi
Non-enzymatic modification of proteins by reducing sugars,
a process that is also known as Maillard reaction, leads to
the formation of advanced glycation end products (AGEs) in
vivo. There is a growing body of evidence that formation
and accumulation of AGEs progress during normal aging, and
at an extremely accelerated rate under diabetes, thus being
involved in the pathogenesis of diabetic vascular complications.
Further, recently, engagement of their receptor, RAGE with
AGEs is shown to activate its down-stream signaling and evoke
oxidative stress and inflammation in diabetes. Since oxidative
stress generation and inflammation are closely associated
with insulin resistance as well, it is conceivable that the
AGEs-RAGE system could play a role in the pathogenesis of
insulin resistance and subsequently the development of diabetes.
In this paper, we review the role of the AGEs-RAGE system
in insulin resistance, especially focusing on its effects
on the insulin-signaling pathways in skeletal muscles and
adipocytes.
[Back to top]
Potential Strategies for Minimizing Mechanism-Based
Inhibition of Cytochrome P450 3A4
S-F. Zhou
Cytochrome P450 (CYP) 3A4, one of the most abundant hepatic
Phase I enzymes, is able to metabolize more than 50% currently
available therapeutic drugs. However, this enzyme is subject
to mechanism-based inhibition by a number of xenobiotics and
commonly-used drugs, which is characterized by NADPH-, time-
and concentration-dependent enzyme inactivation, occurring
when the parental drugs are converted by CYPs to reactive
metabolites. The inactivation of CYP3A4 by drugs may lead
to important clinical consequences, because the inhibition
frequently causes unfavorable drug-drug interactions and toxicity,
depending on many factors associated with the enzyme, drugs
and the patients. Some drugs (e.g. mibefradil) have been withdrawn
from the market since they are eventually identified as CYP3A4
inactivators that can cause toxicity-related fatal events.
Clinical professionals should take proper approaches to avoid
such toxicities when using drugs that are mechanism-based
CYP3A4 inhibitors, in particular, when in combination with
other drugs that are substrates for CYP3A4. These include
early identification of drugs behaving as CYP3A4 inactivators,
rational use of such drugs (e.g. safe drug combination regimen,
dose adjustment or discontinuation of therapy when toxic drug
interactions occur), close therapeutic drug monitoring, and
prediction of the risks for potential drug-drug interactions.
Clinicians should have sound knowledge on drugs that behave
as CYP3A4 inactivators and take cautions for their clinical
use. A fifth approach is the design of drugs with minimal
potential for behaving as a CYP3A4 inactivator. These new
drugs are so called “hard drugs” which are non-metabolizable
(thus mechanism-based CYP3A4 inhibition is avoided), and excreted
through either the bile or kidney, with predictable pharmacokinetics.
Further studies are needed to explore the suitable approaches
for minimizing mechanism-based inhibition of CYP3A4 and thus
avoiding potential toxicities and unfavorable drug-drug interactions.
[Back to top]
Recent Developments in the Chemistry and in the Biological
Applications of Amidoximes
K.C. Fylaktakidou, D.J. Hadjipavlou-Litina, K.E.
Litinas, E.A. Varella and D.N. Nicolaides
Amidoximes are compounds bearing both a hydroxyimino
and an amino group at the same carbon atom which makes them
versatile building blocks for the synthesis of various heterocycles.
Their importance in chemistry along with their rich biology,
make amidoximes an attractive target for medicinal chemists,
biochemists and biologists. Amidoximes and simple O-substituted
derivatives possess very important biological activities functioning
as antituberculotic, antibacterial, bacteriostatic, insecticidal,
elminthicidal, antiviral, herbicidal, fungicidal, antineoplastic,
antiarrythmic, antihypertensive, antihistaminic, anxiolytic-antidepressant,
anti-inflammatory/ antioxidant, antiaggregatory (NO donors)
or plant growth regulatory agents. A number of amidoximes
has already been used as drugs, or currently being in clinical
trials. Their numerous pharmaceutical applications have been
recently enriched, due to the fact that some mechanistic pathways,
concerning their conversion to amidines, as well as their
ability to release NO were clarified, giving a new insight
to their mode of action and allowing the design of new therapeutic
agents.
The main subject of the present review paper is to highlight
aspects concerning chemical and biological questions on this
interesting class of compounds. Some new synthetic methodologies
as well as improvements of previously reported general reactions
involving amidoximes, acylated amidoximes, and amidines are
presented. The biological applications of amidoximes over
the end of 2006 are also extensively reviewed.
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