Current Pharmaceutical Design, 2004, 10, 3797-3811 Studies on Coumarins and Coumarin-Related Compounds to Determine their Therapeutic Role in the Treatment of Cancer Applied Biochemistry Group, School of Biotechnology, Dublin City University, Glasnevin, Dublin 9, IrelandAbstract: The Benzopyrones are a group of compounds whose members include coumarins and flavonoids. Dietary exposure to benzopyrones is quite significant, as these compounds are found in vegetables, fruit, seeds, nuts, coffee, tea and wine. It is estimated that the average western diet contains approximately 1g/day of mixed benzopyrones. It is, therefore, not difficult to see why extensive research into their pharmacological and therapeutic properties is underway over many years. Coumarin is a natural substance that has shown anti-tumour activity in vivo, with the effect believed to be due to its metabolites (e.g. 7-hydroxycoumarin). This review is based on recent studies of coumarins and coumarin related compounds. Therefore, the focus will be on these relevant compounds and their therapeutic importance.
A recent study has shown that 7-hydroxycoumarin inhibits the release of Cyclin D1, which is overexpressed in manytypes of cancer. This knowledge may lead to its use in cancer therapy. Esculetin inhibits growth and cell cycle progressionby inducing arrest of the G1 phase in HL-60 leukaemia cells, resulting from the inhibition of retinoblastoma proteinphosphorylation. Recent studies investigating the potential of flavonoids as therapeutic agents have suggested they mayhave use in various therapeutic settings ranging from leukaemia treatment to the treatment of patients with HIV. Genisteinis a well-known isoflavone and is a tyrosine kinase inhibitor. Studies have indicated that genistein elicits inhibitory effectson cell growth of various carcinoma cell-lines and may be a potential candidate for cancer therapy.
In our research, we have investigated the effects of coumarins and coumarin-related compounds on a panel of cell-lines. The most recent work involves two cell-lines, MCF-7 a breast carcinoma and A549 a lung carcinoma. Microtitre assayswere performed along with real-time analysis of cell viability using a biosensor called the Cytosensor microphysiometer. These studies suggest that both genistein and esculetin exerted the most potent inhibitory effect on cell growth incomparison to the other two compounds. Key Words: Coumarin, 7-hydroxycoumarin, esculetin, warfarin, genistein, benzopyrones, flavonoids, coumarin derivatives, furanocoumarins, pyranocoumarins, pyrone-substituted coumarins, pharmacokinetics, cytochrome P450 microtitre assay, cell proliferation, MTT, LDH, BrdU, Acid Phosphatase, Cytosensor Microphysiometer, MCF-7, A549, toxicity, signal transduction, cancer treatment, anti-proliferation, cytostatic. INTRODUCTION
Coumarins owe their class name to ‘Coumarou’, the
vernacular name of the tonka bean (Dipteryx odorata Willd.,
Fabaceae), from which coumarin itself was isolated in 1820
[1]. Coumarin is classified as a member of the benzopyrone
family of compounds, all of which consist of a benzene ring
joined to a pyrone ring [2]. The benzopyrones can be
subdivided into the benzo-α-pyrones to which the coumarins belong and the benzo-γ-pyrones, of which the flavonoids are principal members (Fig. 1.1). Fig. (1.1). The chemical structures of benzopyrone subclasses, with the basic coumarin structure (benzo-α-pyrone) [A], and flavonoid OCCURRENCE
(benzo-γ-pyrone) structure [B].
There are four main coumarin sub-types: the simple
along with their glycosides. Furanocoumarins consist of a
coumarins, furanocoumarins, pyranocoumarins and the
five-membered furan ring attached to the coumarin nucleus,
pyrone-substituted coumarins (Table 1.1). The simple
divided into linear or angular types with substituents at one
coumarins (e.g. coumarin, 7-hydroxycoumarin and 6,7-
or both of the remaining benzoid positions. Pyranocoumarin
dihydroxycoumarin), are the hydroxylated, alkoxylated and
members are analogous to the furanocoumarins, but contain
alkylated derivatives of the parent compound, coumarin,
a six-membered ring. Coumarins substituted in the pyronering include 4-hydroxycoumarin [3]. The synthetic com-pound, warfarin, belongs to this coumarin subtype. By virtue
*Address correspondence to this author at the Applied Biochemistry Group,
of its structural simplicity coumarin has been assigned as
School of Biotechnology, Dublin City University, Glasnevin, Dublin 9,Ireland; E-mail: Richard.Okennedy@dcu.ie
head of the benzo-α-pyrones, although it is generally
1381-6128/04 $45.00+.00 2004 Bentham Science Publishers Ltd. 3798 Current Pharmaceutical Design, 2004, Vol. 10, No. 30 Lacy and O’Kennedy
accepted that 7-hydroxycoumarin be regarded as the parent
prises 200 species, is widely distributed in the tropical rain
compound of the more complex coumarins (Table 1.1) [4].
forest where several species are used in folk medicine [10].
Genistein is an isoflavone and belongs to the benzo-γ-
Although most of the natural coumarins in existence have
pyrones. It is a natural component of soy and has been
been isolated from the higher plants, some members have
intensively investigated as a chemopreventitive agent,
been discovered in microorganisms (Fig. 1.2). Some
mainly against hormonally regulated breast and prostate
important coumarin members have been isolated from
microbial sources e.g. novobiocin and coumermycin from
Coumarins comprise a very large class of compounds
Streptomyces, and aflatoxins from Aspergillus species [11,
found throughout the plant kingdom [6-8]. They are found at
12]. The aflatoxins are a group of highly toxic fungal
high levels in some essential oils, particularly cinnamon bark
metabolites and the most commonly occurring member of
oil (7,000 ppm), cassia leaf oil (up to 87,300 ppm) and
the group is aflatoxin B1 [3]. Coumarin group antibiotics,
lavender oil. Coumarin is also found in fruits (e.g. bilberry,
such as novobiocin, coumermycin A1 and clorobiocin, are
cloudberry), green tea and other foods such as chicory [9].
potent inhibitors of DNA gyrase. These antibiotics have been
Most coumarins occur in higher plants, with the richest
isolated from various Streptomyces species and all possess a
sources being the Rutaceae and Umbelliferae. Although
3-amino-4-hydroxy-coumarin moiety and a substituted
distributed throughout all parts of the plant, the coumarins
deoxysugar; noviose, as their structural core that is essential
occur at the highest levels in the fruits, followed by the roots,
for their biological activity. Chlorobiocin differs from novo-
stems and leaves. Environmental conditions and seasonal
biocin in that the methyl group at the C-8 of the coumarin
changes can influence the occurrence in diverse parts of the
ring is replaced by a chlorine atom, and the carbamoyl at the
plant [3]. Recently six new minor coumarins have been
3' of the noviose is substituted by a 5-methyl-2-pyrrolcar-
isolated from the fruits and the stem bark of Calophyllum
boxyl group. Coumermycin A1 contains two of the couma-
dispar (Clusiaceae). The genus Calophyllum, which com-
rin-noviose core joined by a 3-methyl-2,4-dicarboxyl pyrole
Table 1.1. The Four Main Coumarin Subtypes. The Main Structural Features and Examples of Each Coumarin Subtype are Illustrated in this Table Classification Features Examples SIMPLE COUMARINS
5-membered furan ring attached to benzene
FURANOCOUMARINS
6-membered pyran ring attached to benzene
PYRANOCOUMARINS PYRONE-SUBSTITUTED COUMARINS Studies on Coumarins and Coumarin-Related Compounds Current Pharmaceutical Design, 2004, Vol. 10, No. 30 3799 Fig. (1.2). Important coumarin members isolated from microbial sources: [A] Novobiocin, [B] Coumermycin A1, [C] Clorobiocin.
linker and has the same substituted noviose as in chloro-
considered the critical value at which the distribution of a
compound limits its rate of absorption. However, bothcompounds have high partition coefficients (21.5% for
PHARMACOKINETICS
coumarin and 10.4% for 7-hydroxycoumarin), which isconsidered favourable for the rapid absorption of compounds
The pharmacokinetics of coumarin, including the excre-
once they are in aqueous solution. This coupled with the fact
tion of various metabolites, were elucidated over many
that coumarin is non-polar, suggests that in theory coumarin
years. Coumarin is rapidly and almost completely
should cross lipid bilayers easily by passive diffusion [12].
metabolised with little unchanged compound excreted [14].
Pharmacokinetic studies in humans have demonstrated
Absorption and Distribution
that coumarin is completely absorbed from the GIT after oraladministration and extensively metabolised by the liver in
Following oral administration, coumarin is rapidly
the 1st pass with only between 2 and 6% reaching the
absorbed from the gastrointestinal tract and is distributed
systemic circulation intact [9]. The low bioavailability of
throughout the body [9]. Coumarin and 7-hydroxycoumarin
coumarin, in addition to its short half-life (1.02 hrs peroral vs
are both poorly soluble in water (0.22 and 0.031 %,
0.8 hrs intravenous) has brought into question its importance
respectively). These percentages indicate coumarin may have
in vivo and it is now accepted that coumarin is a pro-drug,
reduced bioavailability in vivo, as 0.3% solubility in water is
with 7-hydroxycoumarin being the compound of main
3800 Current Pharmaceutical Design, 2004, Vol. 10, No. 30 Lacy and O’Kennedy
therapeutic relevance. At normal therapeutic plasma
Coumarin is metabolised initially by specific cytochrome
concentrations many drugs exist in the plasma mainly in the
P-450-linked mono-oxygenase enzyme (CYP2A6) system in
bound form. Ritschel [15] and colleagues have shown that
liver microsomes, resulting in hydroxylation to form 7-
35% of coumarin and 47% of 7-hydroxycoumarin bind
hydroxycoumarin. After 7-hydroxylation, coumarin under-
plasma proteins. Availability of the compounds at their target
goes a phase II conjugation reaction resulting in a
tissues should not be problematic since the proportions that
glucuronide conjugation associated with 7-hydroxycoumarin.
bound were well below the accepted critical value of 80%
The 7-hydroxylase activity is exceptionally high in human
binding. The pharmacokinetics of coumarin have been studied
liver microsomes compared with its activity in the livers of
in a number of species including the rat, dog, gerbil, rhesus
other animal species. The activity of coumarin 3-hydroxylase
monkey and in man [9]. Specific antibody recognition for its
is very high in rodent microsomes but is absent in human
antigen is the basis for very selective and sensitive analytical
microsomes. Although coumarin may be metabolised by
methods. This was exploited in numerous formats for the
hydroxylation at all six possible positions (i.e. carbon atoms
pharmacokinetic determination of coumarin and its deri-
3,4,5,6,7, and 8), the most common routes of hydroxylation
vatives. Immunoanalytical approaches have included
are at positions 7 and 3 to yield 7-hydroxycoumarin and 3-
ELISA-based methods for the detection of coumarin and 7-
hydroxycoumarin, respectively (Fig. 1.3). 7-hydroxylation
hydroxycoumarin in urine [16]. Antibody-based biosensors
has received the most attention among the various metabolic
have also been employed, with either electrochemistry, or
steps, predominantly because it is the major metabolic route
surface plasmon resonance (BIAcore) facilitating detection
in humans and is easily analysed. Hydroxylation at carbon 3
of coumarin compounds in various matrices [17, 18].
results in further metabolism via ring opening, yielding twofurther products, o-hydroxyphenyllactic acid (o-HPLA) and
Metabolism o-hydroxyphenylacetic acid (o-HPAA) [9, 14]. Theexpression of CYP enzymes (e.g. CYP2A6) varies between
Traditionally coumarin has been viewed by pharmaco-
individuals due to genetic and environmental factors. These
logists as the ideal model for studying the complex
factors produce inter-individual variation in the metabolism
metabolism of a structurally simple organic molecule, and as
of drugs such as coumarin. The frequency of poor metabo-
such, its metabolic fate has been extensively researched [9,
lisers varies between species, races and ethnic groups. It has
19, 20]. Determining the metabolic fate of coumarin is
been shown that there exists large inter-species and inter-
important in order to utilise the fact that it is metabolised at
individual variability in the activity of these enzymes [21].
several sites, and to access the possible dependence ofcoumarin-induced toxicity on metabolism [14]. Metabolism in Man
The superfamily of cytochromes P450 (CYPs) consists of
The metabolism of coumarin has been investigated in
microsomal hemoproteins that catalyse the oxidative,
vivo and in vitro in a wide range of species including
peroxidative and reductive metabolism of a wide variety of
humans. Human metabolic studies usually involve oral
endogenous and exogenous compounds. The CYP super-
dosage followed by urine collection with or without timed
family is divided into families and subfamilies according to
fractionation [7, 22]. Analysis is by one of a number of
their nucleotide sequence homology. Most biotransforma-
techniques including spectrofluorimetry, HPLC and capillary
tions of xenobiotics (such as drugs) are performed by
electrophoresis [23-25]. Recent in vitro systems employed
enzymes from the families CYP1, CYP2 and CYP3. The
include tissue slices, hepatocytes, subcellular fractions, and
CYP2 family have been examined using the rat, mouse and
purified and cDNA-expressed enzymes [9]. In the majority
rabbit model systems. This family includes seven subfami-
of human subjects studied coumarin is extensively metabo-
lies in mammals. In humans, the most important CYPs
lised to 7-hydroxycoumarin. Some data for various coumarin
regarding drug metabolism are CYP2A6, CYP2C9,
dose levels and collection periods are shown in Table 1.2.
The measurement of urinary 7-hydroxycoumarin following
Table 1.2. Extent of Coumarin Metabolism to 7-HC in Various Species. aCoumarin Administered Orally Unless Otherwise Stated bShilling et al. (1963). cEgan et al. (1990) Dose (mg/kg)a Collection time (hr) Urinary 7-HC (% of Dose) Studies on Coumarins and Coumarin-Related Compounds Current Pharmaceutical Design, 2004, Vol. 10, No. 30 3801 7-hydroxycoumarin 6-hydroxycoumarin 8-hydroxycoumarin CYP2A6 o-hydroxyphenylpropionic acid 5-hydroxycoumarin Coumarin o-coumaric acid 4-hydroxycoumarin Esculetin 3-hydroxycoumarin 3,4-epoxide o-hydroxyphenyllactic acid o-hydroxyphenylacetaldehyde o-hydroxyphenylacetic acid Fig. (1.3). Metabolism of coumarin. All biotransformations are possible, although the metabolism is species-specific.
an oral dose of coumarin has been employed as a biomarker
considerable proportion of coumarin through pathways other
of human hepatic CYP2A6, the cytochrome P-450 (CYP)
that 7-hydroxylation such as the 3,4-epoxidation pathway to
isoform which is responsible for coumarin 7 hydroxylation
in human liver [14]. Some individuals can metabolise a
3802 Current Pharmaceutical Design, 2004, Vol. 10, No. 30 Lacy and O’Kennedy
In humans, there are three genes in the CYP2A sub-
bile. This may result in enterohepatic circulation enhancing
family, however, CYP2A6 is mainly of greater importance,
the exposure of liver cells to toxic coumarin metabolites.
as the other two gene products (CYP2A7 and CYP2A13) are
Species such as syrian hamster, baboon, and humans excrete
either inactive or are not expressed in the liver. CYP2A6
coumarin metabolites primarily in urine. Low level exposure
codes the enzyme catalysing coumarin 7-hydroxylation
to coumarin from diet and from fragrances used in cosmetic
(about 10% of total P450) [26]. Recently, CYP2A6 has been
products would not be expected to produce any hepato-
reported to be polymorphically expressed in the human liver.
toxicity even in individuals with deficient 7-hydroxylase
It has been shown that CYP2A6 participates in metabolism
of nicotine and its metabolite cotinine. Some drugs andchemicals, including coumarin, which is widely used as a
APPLICATIONS OF COUMARIN AND COUMARIN
probe substance for CYP2A6 both in vitro and in vivo, are
DERIVATIVES
also metabolised by this enzyme [27]. Substrates and
The coumarins are of great interest due to their biological
inhibitors currently known to be metabolised by or interfere
properties. In particular, their physiological, bacteriostatic
with CYP2A6 in vitro and in vivo have been summarised by
and anti-tumour activity makes these compounds attractive
Pelkonen [26]. Although 7-hydroxycoumarin is the main
for further backbone derivatisation and screening as novel
human metabolite, other hydroxylation pathways are impor-
therapeutic agents. Weber [30] and co-workers have shown
tant in humans and, as such, the therapeutic relevance of
that coumarin and its metabolite 7-hydroxycoumarin have
non-7-hydroxymetabolites should be examined rather than
antitumour activity against several human tumour cell lines.
Both coumarin and coumarin derivatives have shownpromise as potential inhibitors of cellular proliferation in
TOXICOLOGY
various carcinoma cell lines [12, 31, 32]. In addition it has
Since 1954, coumarin has been classified as a toxic
been shown that 4-hydroxycoumarin and 7-hydroxycoumarin
substance by the FDA, following reports of its possible liver
inhibited cell proliferation in a gastric carcinoma cell line
tumour-producing properties in rats [28]. The FDA banned
its use, labelling as adulterated all foods containing coumarin[12]. Due to tests performed on rodents coumarin was
SIMPLE COUMARINS
referred to as a chemical carcinogen by NIOSH [National
Coumarins and the benzopyrones are representative of a
Institute for Occupational Safety and Health]. However,
very diverse and potentially useful groups of drugs.
caution needs to be taken in extrapolating this information tohuman situations. Various tests (Ames, micronucleus) have
Clinical Uses
shown that coumarin and its metabolites are non-mutagenic[6]. Preliminary results from early studies indicated that
Due to its biochemical properties coumarin was proposed
coumarin was a toxin, but it has been shown since, that the
for use in clinical medicine. It had been evaluated for the
rat is a poor model to compare with the human for this
treatment of various clinical conditions, resulting in the use
particular metabolism [29]. A number of studies have
of a variety of dosing regimens. Recommended doses range
examined the acute, chronic and carcinogenic effects of
from 8mg for the treatment of venous constriction to
coumarin in the rat and mouse. In studies involving the rat,
7000mg/day in anti-neoplastic therapies.
hepatic biochemical and morphological changes have beenexamined for various periods of coumarin administration (1
High Protein Oedema (HPO)
week to 2 years). Depending on dose administered, coumarin
The lymph system is responsible for drainage of inters-
treatment results in an increase in relative weight and
titial fluid within human tissues. Oedema interferes with the
changes in various hepatic biochemical parameters. Single
metabolism of the tissue cells and reduces oxygen transport,
oral doses of coumarin have been shown to produce liver
resulting in problematic wound healing [34]. In the case of
necrosis and increase plasma transaminase activities in
high protein oedemas (HPO), there is an accumulation of
protein in the tissue following trauma or inflammation, with
In contrast, studies involving baboons, syrian hamsters
resulting permeability of the capillaries causing water
and certain mice strains seem to be resistant to acute
leakage in the tissue spaces. Many disease states are associa-
coumarin-induced hepatotoxicity. Species differences in
ted with high protein oedemas, ranging from extremely
coumarin-induced toxicity in vitro have been investigated in
severe and chronic (e.g. lymphoedema and elephantiasis)
cultured hepatocytes. These studies provide evidence for
through more common and acute forms (e.g. burns,
species differences in coumarin-induced toxicity in vitro.
accidental and surgical traumas). All forms have been shown
The relative resistance of human and cynomolgus monkey
to benefit from benzopyrone treatment [35]. Coumarin and
liver slices and/or hepatocytes to coumarin toxicity correlates
numerous other benzopyrones have been tested in high
with coumarin 7-hydroxylation, the major pathway of
protein oedema, and all have been shown to successfully
coumarin metabolism in these species, being a detoxification
reduce the swelling. However, according to Loprinzi [36]
pathway of coumarin metabolism. However, while
and colleagues, coumarin treatment alone is not effective
coumarin-7-hydroxylation pathway is a detoxification
therapy for women who have lymphoedema of the arm after
pathway this does not appear to be the only explanation for
treatment for breast cancer. It may be possible to increase the
resistance of a species to coumarin-induced toxicity. In the
beneficial therapeutic effect of coumarin by using it with
rat coumarin-induced hepatotoxicity appears to be partially
other compounds in combination treatments. The objective
attributable to the excretion of coumarin metabolites in the
of a recent study was to evaluate the oedema-protective
Studies on Coumarins and Coumarin-Related Compounds Current Pharmaceutical Design, 2004, Vol. 10, No. 30 3803
effect of a combination vasoactive drug, coumarin/troxerutin
to the oncologist, as no satisfactory treatment for recurrent
(SB-LOT) plus compression stockings in patients suffering
malignant melanoma currently exists. Studies have shown
from chronic venous insufficiency after decongestion of the
that five years after removal of the primary lesion, the
legs as recommended by the new guidelines. The study
recurrence of malignant melanoma is observed in 55-80% of
confirms the oedema-protective effect of SB-LOT in chronic
venous insufficiency and provides a treatment option for
Original work with coumarin derivatives in the treatment
patients who discontinue compression after a short time [37].
of melanoma focused on the use of warfarin as a
Chronic Infections
maintenance therapy. This compound was known to inhibittumour spread, and to stimulate granulocytes, lymphocytes
In addition to its stimulatory effect on macrophages,
and macrophages [43]. Thornes then began to assess the
coumarin has been shown to activate other cells of the
potential application of coumarin, the parent compound of
immune system. In chronic brucellosis Brucella abortis
warfarin, as an adjuvant therapy in melanoma. Like warfarin,
infects macrophages, thus eluding the immune response [38].
the in vivo actions of coumarin were known to be macro-
When immunostimulatory drugs such as coumarin are
phage-derived. Coumarin was non-toxic and conveniently
administered, the symptoms of chronic brucellosis disappear.
administered, it had no anti-coagulant activity, and a
These results have encouraged the use of coumarin in other
previous administration resulted in subjective improvement
chronic infections such as mononucleosis, mycoplasmosis,
in cancer patients [44, 45]. A more recent study by Velasco-
toxoplasmosis and Q fever. A new antiplasmodial coumarin
Velazquez [46] and colleagues determined the in vitro
has been isolated from the roots of Toddalia asiatica. This
effects of 4-hydroxycoumarin (4-HC) employing the murine
finding supports the traditional use of this plant for the
melanoma cell line B16-F10 and the non-malignant
fibroblastic cell line B82. 4-HC disorganized the actincytoskeleton in B16-F10 cells, but not in B82 fibroblasts. APPLICATION OF SIMPLE COUMARINS IN
Adhesion of tumour cells to extracellular matrix is required
CANCER TREATMENT
during the metastatic process, therefore, 4-HC might be
Anti-cancer drugs have traditionally been targeted to
useful as an adjuvant therapy for melanoma.
damage the aberrantly dividing cell by interrupting the celldivision process [40]. Reagents used include DNA intercalat-
Coumarin in Renal Cell Carcinoma
ing agents (e.g. adriamycin), DNA cross-linking agents (e.g.
The clinical course of renal cell carcinoma (RCC) has
cis-platin), topoisomerase inhibitors (e.g. campothecins),
been well documented, with long-lasting stable periods and
cytoskeleton-disrupting agents (e.g. vinblastin) and anti-
rapid tumour growth its principal features. Surgery remains
metabolites (e.g. mercaptopurine). These drugs though effec-
the standard care for patients whose tumour is confined to
tive, are cytotoxic, and thus exhibit severe side effects, parti-
the kidney. However, many of these patients develop recur-
cularly on normal proliferating tissues such as the haemato-
rent or metastatic disease within months, where the lungs,
poietic system. Often combination therapies, whereby
liver and bones are the common sites of secondary occur-
several cytotoxic agents are combined in the treatment
rence [47]. The outlook for patients with metastatic RCC is
regime, offer better results with fewer toxic side-effects, as
poor, with a 5-year survival rate of less than 10% [48].
they are carefully regulated to allow recovery of normal, butnot malignant cells, from drug exposure [40].
Interest in the coumarin family of compounds stemmed
from reports by Thornes, of the immunomodulatory activity
Currently, chemotherapy, radiotherapy and surgery
of coumarin and its utility in malignant melanoma [49]. The
combined offer the best outcomes for cancer patients, and
clinical activity of coumarin in renal cell carcinoma patients
treatment combinations have been successfully applied to
has been investigated by applying a treatment regime
particular cancer types, for example, Hodgkin’s lymphoma,
described by Thornes (coumarin at 100mg/day oral dosage,
testicular cancer and various leukemias. Coumarins can be
with the addition of cimetidine 4 X 300mgs/day from day
used not only to treat cancer but to treat the side effects
15). This preliminary study yielded some interesting results,
caused by radiotherapy. A recent study investigated the
with 14 objective results among 45 patients with metastatic
efficacy of coumarin/troxerutine combination therapy for the
RCC, and almost no toxic side effects. Validation of this
protection of salivary glands and mucosa in patients
anti-tumour activity was further demonstrated by other
undergoing head and neck radiotherapy. The results suggest
that coumarin/troxerutine have a favourable effect in thetreatment of radiogenic sialadentis and mucositis [41]. The
Following this success, it became clear that additional
interest in coumarin and 7-hydroxycoumarin as anti-cancer
information regarding doses and toxicities was required, and
agents, arose from reports that these agents had achieved
Marshall and colleagues implemented a phase I trial to
objective responses in some patients with advanced mali-
define the maximally tolerated dose, and dose-limiting
toxicities of coumarin and cimetidine. All coumarin doseswere well tolerated, with the most common side effect of
Coumarin in Malignant Melanoma
nausea attributable to the intense aroma of coumarin. Objective responses were observed in 7 patients, all with
Early diagnosis of malignant melanoma facilitates
renal cell carcinoma, these responses being observed across a
surgical removal of the primary lesion and achieves a good
range of coumarin doses (600-5000 mgs) [52]. In vitro
prognosis. However, if the lesion progresses, the risk of
cytotoxic potential and mechanism of action of selected
recurrence becomes serious and represents a major challenge
coumarins using renal cell lines have been investigated
3804 Current Pharmaceutical Design, 2004, Vol. 10, No. 30 Lacy and O’Kennedy
recently [8]. The results obtained suggest that the coumarins
hydroxycoumarin and esculetin were found to inhibit
examined may have a potential therapeutic role to play in the
tyrosine phosphorylation in EGF-stimulated tumour cells in
a time- and dose-dependent manner. It appears that thiseffect may be achieved by reduction of the tyrosine kinase
Coumarin in Prostate Cancer
Prostate cancer is the most common invasive malignancy
A recent study has presented evidence that esculetin
in males and is characterised by a very slow growth rate and
affected phosphorylation of pRB thus inducing G1 arrest of
a wide biological variability, especially with regard to
human leukaemia HL-60 cells. The results demonstrated that
hormonal sensitivity [53, 54]. These two traits have curbed
the treatment with esculetin resulted in an accumulation of
attempts at curative treatments for patients, as most effective
hypophosphorylated pRB in HL-60 cells along with reduc-
chemotherapeutic drugs rely on fast growth kinetics in the
tions of both cyclin D1 and E. This induced the arrest of the
tumour mass, and, due to differential hormonal dependencies,
cell cycle at the G1 phase. Among the released proteins, the
hormonal therapy (androgen deprivation) is not effective in
E2F family of transcription factor has central position. Not
all cases. At present, early detection, and removal of clini-
only does E2F induce gene expression necessary for DNA
cally significant tumours by surgery or radiation, have been
synthesis, it also contributes to the regulation of the cyclin
the focus of clinical strategies. However, patient survival is
D1 and E genes. Esculetin treatment also induced enhanced
dependent on metastases where principal metastatic sites are
expression of the CDKI p27 and a reduced expression of
regional lymph nodes and bone. Eventually, almost every
CDK-4, thus inhibiting pRB phosphorylation [58].
prostate carcinoma that initially regressed on androgen
In a separate study aiming to clarify mechanisms of
deprivation will relapse into a hormonal-insensitive state and
action of 7-hydroxycoumarin and coumarin, the effect on
grow in the absence of androgen. Evidently, better therapeu-
cell cycle progression of the human adenocarcinoma cell line
tic approaches to control both metastases and hormone-
A427 was investigated. These cells are pRB positive and
insensitive prostate carcinomas are required.
have homozygous deletions at the gene of p16INK4A. The
As coumarin had previously appeared to exert immuno-
results showed that 7-hydroxycoumarin had greater cytosta-
modulating effects in other cancers, a small-scale study to
tic activity than coumarin. The inhibition of the cell-cycle at
test the efficacy of coumarin in prostate cancer was set up
transition G1/S is consistent with the cytostatic effect of 7-
[55]. A phase I trial involving 40 patients with metastatic,
hydroxycoumarin. Furthermore, the decrease in the percen-
hormone-naïve or hormone-refractory prostatic cancer was
tage of cells expressing cyclin D1 indicates that the action of
conducted [56]. Participants were administered 3g of
7-hydroxycoumarin involves early events in phase G1.
coumarin daily, and evaluated for toxicity and anti-tumour
Absence of changes in the level of cyclin D1 mRNA
responses. 3 partial responses occurred, all in-patients with
suggests a post-transcriptional effect of 7-hydroxycoumarin.
low tumour loads. One responder remained with 3 respon-
A pathway which regulates post-transcriptionally the levels
sive bone metastases and stable prostate specific antigen
of cyclin D1 is the PI-3K/AKT pathway. If this pathway is
(PSA) levels for 7 years following the trial. Myers [57] and
inhibited it cannot inhibit phosphorylation of GSK-3 which
co-workers examined the effects of various concentrations
(0-500 µg/ml) of coumarin on the proliferation of two renalcell carcinoma cell lines (786-O and A-498) and two
COUMARIN DERIVATIVES AND CANCER
malignant prostatic cell lines (DU145 and LNCaP). After 5
Furanocoumarins
days of treatment, coumarin inhibited the growth of the fourcell lines. The LNCaP prostatic cell line was most sensitive
The furanocoumarins are a therapeutically important
to the inhibitory effects of coumarin.
subtype as they have various clinical applications. Thefuranocoumarins consist of a 5-membered furan ring
Coumarin in Leukaemia
attached to the coumarin nucleus. Two of the most importantand well known furanocoumarins are psoralen (Linear) and
The effect of esculetin, coumarin and 7-hydroxycoumarin
angelicin (Angular). The terms linear and angular refer to the
on the cell cycle and its regulatory molecules has been
orientation of the furan ring with respect to the coumarin
investigated. The cytostatic and cytotoxic nature of 8-nitro-
7-hydroxycoumarin (8-NO2-7-OHC) was determined usingboth human and animal cell lines grown in vitro. This
Psoralens are naturally occurring plant biosynthetic
compound displayed cytotoxic properties in two human cell
metabolites that have been used since ancient times in
lines tested (HL-60 and K562), inducing cell death by
photochemotherapy to treat a number of skin disorders
apoptosis. This compound imposed a cytostatic effect on the
including mycosis fungoides, psoriasis and vitiligo [60].
three other cell lines tested, exerted through a perturbation in
Psoralens have recently found application in the regulation
their cell cycle [31]. The effect of a number of coumarin
of human cervical carcinoma cell proliferation in conjunction
compounds on the growth, metabolism and cell signalling of
with anti-sense technology [61]. Oligonucleotides and their
human tumour cell lines was examined by Cooke [12].
analogs have been used to inhibit protein biosynthesis by
Overall esculetin exhibited the strongest antiproliferative
suppressing the gene expression in a sequence specific
effect on the carcinoma cell lines tested [32]. Given the
manner. The method is called antisense strategy and has
importance of signalling anomalies in cancer cells, tests were
been applied to gene therapy for incurable diseases such as
performed to determine if the cellular target of 7-hydroxy-
cancers and viral infections. Among various reports
coumarin was a signalling pathway component. Both 7-
regarding antisense technology, many have presented clear
Studies on Coumarins and Coumarin-Related Compounds Current Pharmaceutical Design, 2004, Vol. 10, No. 30 3805
evidence that the antisense mechanism participated in the
metastatic tumour will ultimately form. Components of the
regulation of cell growth. Some of the antiproliferative
blood-clotting pathway may contribute to metastasis by
effects of oligo nucleoside phosphorothioates S-oligo may be
trapping cells in capillaries or by facilitating adherence of
attributed to the interaction of S-oligo with certain proteins
cells to capillary walls. Conceivably, anticoagulants could
interfere with this step in the metastatic process [63]. Warfarin has shown particularly promising results in the
Upon UVA irradiation psoralen derivatives have the
treatment of SCCL (Small Cell Carcinoma Lung) a tumour
ability to crosslink covalently with pyrimidine bases (e.g.
cell type that is characterised by a coagulation-associated
thymine and uracil). As psoralen derivatives can inactivate
pathway [64-66]. Studies by Mousa [67] have shown that
gene expression via cross-linking, they have been conjugated
anticoagulation with commonly used agents such as
with oligonucleotides to reinforce antisense effects. During
unfractionated heparin and warfarin (Coumadin) prevent
in vitro experiments psoralen-conjugated S-oligos have
tumour formation by limiting the ability of tumour cells to be
shown resistance to nucleases and, therefore, have exhibited
retained in the pulmonary microvasculature.
significant inhibitory effects upon UVA irradiation. Psoralen-conjugated S-oligos (Ps-S-oligo) were prepared and used to
Recent studies suggest that anticoagulant drugs and cime-
inhibit the proliferation of human cervical carcinoma cells.
tidine therapy in malignancy may improve cancer survival
Upon UVA irradiation of Ps-S-oligo-treated cells, Ps-S-oligo
and inhibit the metastatic process. A study investigated and
complementary to the initiation codon region (Ps-P-As) of
compared the effects of anticoagulant drugs (e.g. warfarin
human papillomavirus (HPV)18-E6*-mRNA of human
and heparin), cimetidine and a combination of cimetidine
cervical carcinoma cells significantly inhibited proliferation.
with anticoagulants on adhesion of highly invasive breast
The E6* protein is tightly correlated with the transformation
cancer cell lines BT-549 and MDA-MB-231 in vitro. A high
of human cervical cells and therefore, its suppression may
anti-adhesion effect was observed with cimetidine and
regulate cellular proliferation. The psoralen-conjugated
warfarin. Anticoagulants such as warfarin can decrease
antisense DNA has significant potential to regulate gene
adhesion and tumour angiogenesis. Application of cimetidine
expression, which may provide useful information to explore
and anticoagulant drugs intensifies the anti-adhesion effect
together with other anti-metastatic effects [68]. There is nowconsiderable evidence that the blood coagulation system
Pyranocoumarins
plays an important role in the biology of malignant tumours. This evidence has been derived from a combination of
Plant materials have a long history of being successfully
clinical, biochemical, histological, and pharmacological
used in the treatment of cancer, both as chemotherapeutic
observations that point to the possibility of favourably
agents and as complementary treatments. The pyrano-
affecting the course of malignant disease with agents that
coumarin compound (+)-3-angeloyl-4-acetoxy-cis-khel-lac-
interfere with blood coagulation pathways [67].
tone was isolated from Radix peucedani, a herb well-knownfor the treatment of respiratory diseases and pulmonary
ISOFLAVONES
hypertension. Resistance of cancer cells to chemotherapeuticagents remains one of the major obstacles in achieving an
For many years now, isoflavones have been investigated
effective treatment for cancer. The molecular mechanism of
by clinicians, pharmacologists and plant physiologists.
multidrug resistance (MDR) in cancer cells may involve
Isoflavones have exceptionally interesting, multidirectional
over-expression of membrane drug efflux pumps, p53
therapeutic properties and the biological activity of these
mutations, and up-regulation of bcl-2, DNA repair or cellular
substances is conditioned by the location of the phenyl ring
detoxification enzymes. P-glycoprotein is over-expressed in
near the third carbon of the benzo-γ-pyrone. Hence, these
various MDR cell lines and functions as an ATP-dependent
compounds, in addition to antiflammatory, antimycotic and
drug efflux pump that rapidly extrudes anti-tumour drugs
radical scavenging properties, also exhibit both estrogenic
from target cancer cells which prevents the drugs from
and anti-estrogenic effects [69]. Genistein (4,5,7-trihydroxy-
exerting their cytotoxic effects. (+)-3-angeloyl-4-acetoxy-
isoflavone) is a natural isoflavone phytoestrogen present in
cis-khel-lactone is a P-glycoprotein inhibitor and studies
soy (Fig. 1.4). In the gastrointestinal tract, the β-glucoside
were recently performed to determine its effect on MDR cell
conjugates of soy are converted by the natural gut microflora
lines. Work by Wu [62] and co-workers demonstrated that
into free genistein and other related isoflavones, which are
this pyranocoumarin causes apoptotic cell death for drug
present in circulating blood, accumulate in tissue and are
sensitive KB-3-1 and multidrug resistant KB-V1 cancer celllines. Strong synergistic interactions were demonstratedwhen the pyranocoumarin was combined with common anti-
tumour drugs such as vincristine, doxorubicin and paclitaxel.
Hence, this pyranocoumarin may have beneficial therapeuticapplication as a MDR reversing agent. However, furtherresearch is necessary to confirm these current findings. Warfarin
Metastasis involves several distinct steps, including one
in which the tumour cell, after entry into the bloodstream,
Fig. (1.4). The basic chemical structure of genistein. It belongs to
comes to rest in a capillary located at a distant site where a
3806 Current Pharmaceutical Design, 2004, Vol. 10, No. 30 Lacy and O’Kennedy
excreted in urine of people who consume high amounts of
γ-irradiated K562 myeloid leukemia cells [73]. Genistein
soy in their diet. Studies have revealed that individuals who
structurally resembles estradiol (E2) and demonstrated weak
consume a traditional diet high in soy products have a low
estrogenic activity in several studies (70,71,74). In humans,
incidence of certain types of cancer, such as breast, prostatic
this compound appears to have both estrogenic and anti-
and colon cancer [70]. Genistein has been shown to inhibit
estrogenic effects, depending on the concentrations of
cancer cell proliferation in vitro and this effect may be
circulating endogenous estrogens and estrogen receptor
attributed to the fact that it is a known tyrosine kinase
(ER).The estrogen agonistic activity in the absence of
inhibitor. Therefore, this compound was chosen to determine
estrogen may account for the beneficial effects of genistein
its effect on two cell lines in vitro. The following section
against atherosclerosis, coronary artery disease, osteoporosis
gives background details on this therapeutically important
and post-menopausal manifestations of hot flushes etc. The
protective effect of genistein against certain forms ofhormone-dependent cancers, such as prostate, may be due to
GENISTEIN
Although genistein belongs to the benzopyrones is not
classed as a coumarin (benzo-α-pyrone). It is a flavonoid and
BENZOPYRONES AND BREAST CANCER
belongs to the benzo-γ-pyrones. Genistein is a phytoestro-
While a significant amount of research regarding the
gen, which belongs to the 'isoflavone' class of compounds.
clinical applications of the benzopyrones has been reported it
These diphenolic compounds structurally resemble estradiol
is important to emphasise that only the ‘warfarin-type’
(E2) and were shown to have some estrogenic activity [71].
anticoagulants belong to mainstream pharmacotherapy. Other
Reports about environmental estrogens, or xenoestro-
types of coumarin compounds are either at the experimental
gens, have been widespread in the last few years. There are
or early clinical trial phase. Hence, additional studies on the
important distinctions between estrogenic compounds of
elucidation of their mechanism of action is necessary to
industrial origin and those that come from plants. Com-
facilitate a greater understanding of these compounds so that
pounds such as insecticide DDT and industrial PCBs have
they may find future clinical application. Recent work
been implicated by some researchers in causing estrogen-
carried out in our laboratory involved the investigation of the
dependent cancers in exposed populations. Unlike some
effects of various benzopyrones on two carcinoma cell lines.
industrial xenoestrogens, which tend to bioaccumulate in
The two cell lines were MCF-7, a breast carcinoma and
adipose tissue and persist in the body for years, phytoestro-
A549, a lung carcinoma. However, the majority of research
gens are readily metabolised and spend relatively little time
focused on the MCF-7 cell line especially with regard to
in the body. The timing of exposure, repeated exposures and
signal transduction and cell cycle regulation studies. In our
levels of exposure to phytoestrogens are important. The two
research the effect of benzopyrones (warfarin, 7-hydroxy-
major classes of phytoestrogens that have captured the most
coumarin, esculetin, and genistein) on the growth and
scientific attention are isoflavones and lignans. Diets rich in
metabolism of human tumour cells was examined. Signal
natural anti-estrogenic substances such as isoflavones have
transduction studies were also performed in order to obtain
been considered as one of the main reasons for significantly
information regarding the mechanism of action of warfarin,
lower incidence of breast cancer in China, Japan, and South
esculetin and genistein on MCF-7 cells.
East Asia. Soybeans are a particularly abundant source of
Previous investigators have used cell proliferation-based
isoflavones such as genistein and daidzein [72].
assays in their chemosensitivity assessment of coumarincompounds [12, 57]. Recently an in vitro proliferation assay
Genistein in Cancer Research
was utilised to determine the anti-tumour activities of
Genistein has been shown to inhibit cancer cell prolifera-
SP500263, a novel next-generation selective estrogen
tion in vitro. This effect is attributed to inhibition of several
receptor modulator (SERM), tamoxifen, and raloxifene in an
key enzymes, especially tyrosine kinase, which plays a
in vitro and in vivo MCF-7 breast cancer model [75]. The
critical role in cell proliferation and transformation. Tyrosine
insensitivity of many human tumour cell lines, previously
kinase is also associated with oncogene expression in breast
tested to growth inhibition by coumarin, seems to confirm
cancer. Breast cancer is one of the most frequently diagnosed
the generally held belief that coumarin is not responsible for
malignancies in women, and its incidence is increasing in
the observed in vivo effects, but is a pro-drug for other active
industrialised nations. Tanos [71] and co-workers have
metabolites. Therefore, in our research we chose initially to
investigated the effect of genistein on human dysplastic and
examine three benzopyrone compounds, namely warfarin,
malignant epithelial breast cell lines, expressing low and
esculetin, and genistein under similar assay procedures, with
high metastatic potentials. They discovered that genistein has
the MCF-7 cell lines and the A549 cell lines. The cell lines
a significant in vitro inhibitory effect on the growth rate of
were exposed to each of the three compounds for 96 hours.
dysplastic (fibrocystic cells) and cancerous breast cells. In
Proliferation assays yielded some interesting information
vitro studies show that genistein also exhibited a synergistic
additive effect when cancer cells were exposed to a genisteinand tamoxifen treatment. These results indicate the potential
1. The potency of growth inhibition by genistein was
of genistein administration alone or in combination with
greater than esculetin which, in turn was greater than
tamoxifen for the treatment of breast cancer [71].
A separate study has shown that genistein treatment has a
2. MCF-7 cells tested were quite sensitive to the effects of
role in triggering cell death and promotes cell cycle arrest on
Studies on Coumarins and Coumarin-Related Compounds Current Pharmaceutical Design, 2004, Vol. 10, No. 30 3807
3. A549 cells did not seem to be as sensitive to the effects
(warfarin and esculetin) was monitored using this technique.
of all three compounds in comparison to MCF-7 cells.
In these experiments the basal metabolic rate of the cells was
However, both genistein and esculetin displayed
determined prior to drug-exposure, and this value was
significant inhibitory effects on A549 cells.
normalised as 100%. This was achieved for each of the fourseparate sensor chambers in the cytosensor. Following drug
The most evident trend from the results was the
exposure all subsequent metabolic rates were expressed as a
sensitivity of both cell lines tested to growth inhibition by
percentage of the basal rate of the particular sensor chamber,
esculetin (6,7-dihydroxycoumarin). This reflects well
ensuring each chamber with its encased cells acted as its own
previous observations by Kolodziej [76] and colleagues and
Cooke & O’Kennedy [30], that a dihydroxy-function ineither an ortho- or meta-format, was an extremely potent
An important result evident from the data collected was
chemical structure for toxicity in human tumour cell lines.
the fact that the cytosensor microphysiometer was more
Since this potency was not evident in either of the single-
sensitive to the effects of the benzopyrones on cellular
hydroxycoumarin compounds, the added potency may be
metabolism than the MTT assay. For example, the MTT
due to the existence of a double hydroxy-function on the
assay detected a decrease in cellular metabolism of ~ 30%
when MCF-7 cells were exposed to 20µg/ml esculetin for24hrs. According to the cytosensor results, the cellular
Assessment of leakage of a wide variety of enzymes is
metabolism in cells exposed to 20µg/ml esculetin decreased
often used for cytotoxicity testing endpoints. Lactate
by ~ 60% over this time period. In fact it would appear from
dehydrogenase (LDH) is a convenient marker because of the
comparing the MTT and cytosensor results for warfarin,
stability of the enzyme activity in the culture system [77]. In
esculetin and genistein, that the cytosensor microphysio-
this study none of the four compounds tested (warfarin, 4-
meter is a much more sensitive predictor of metabolic
hydroxywarfarin, esculetin and 7-hydroxycoumarin) caused
inhibition. The reason for this may be due to the fact that the
significant membrane damage in both cell lines (MCF-7 and
MTT assay relies on the activity of just one group of mitoc-
A549) assessed by LDH assay. There are some drawbacks
hondrial enzymes to predict adverse effects on metabolism,
that should be noted when using the LDH assay. If serum
and in doing so may underestimate metabolic effects. The
contaminates the system with endogenous enzymes they can
MTT assay has been shown to underestimate the growth
mask low levels of leached enzymes, which leads to
inhibitory effects of interferons (IFNs) in the past [79].
underestimation of LDH present. The main drawback of this
Formazan production can also be induced by drugs that
assay, however, is its reliance on the premise that membrane
cause perturbations of the cell cycle [80]. Cells have also
integrity and cellular viability are closely linked. This is not
been observed to metabolise the tetrazolium dye when
always the case, at least in the early stages of cell death; so
lethally damaged and have lost the ability to exclude vital
these assays may not always be true / sensitive indicators of
dyes [81]. Additionally, the test compound may also react
viability. Hence, other assays (MTT, AP; explained later in
with other assay components, e.g. tetrazolium salts, causing
text) must be performed in order to obtain a complete picture
interference, which again may lead to inaccurate results [32].
of the effects of benzopyrones on cells under investigation.
Apart from the increased sensitivity of prediction, the
The effects of warfarin, 7-hydroxycoumarin, esculetin,
cytosensor has several other advantages over the MTT assay
and genistein on cellular metabolism was examined using the
for the detection of metabolic suppression. The ‘real-time’
MTT assay and the cytosensor (where only warfarin and
aspect of detection with the cytosensor yields large amounts
esculetin have been tested on MCF-7 cells). The MTT Assay
of information on the nature of the metabolic suppression
is a well-established colourimetric assay, which can be used
(e.g. time of detrimental effects, etc.), per experiment. To
to detect the effects of agents on cellular metabolism. The
attain this information with an end-point system such as the
assay is based on the cleavage of the yellow tetrazolium salt,
MTT Assay would require multiple, kinetic end-point assays.
MTT (3-[4,5-dimethylthiazol-2-yl]-2,5-diphenyltetrazolium
In addition, the exposure set-up of the cytosensor (flow-
bromide), to purple formazan crystals by mitochondrial
through, perfusive) mimics the in vivo drug delivery/
dehydrogenases. Therefore, cells must not only be alive, but
exposure more than the static exposure set-up of the MTT
also metabolically active for this reaction to occur [12]. The
assay. Finally, the cytosensor microphysiometer allows for
assay can be used in either a long- (96hr) or short-term
reversibility studies to be performed on drug-treated cells to
(24hr) drug-exposure format, to assess the effects of a drug
assess their recovery, an experiment difficult, if not
on cellular growth or metabolism, respectively. Previously,
impossible to achieve with cells following the MTT assay.
the MTT assay has been used to assess the anti-proliferative
The tested benzopyrones (warfarin, esculetin and genistein
on cytosensor) all displayed a dose- and time-dependent
An alternative method was used to evaluate the effect of
effect on cellular metabolism, with genistein followed by
coumarins on cellular metabolism. The cytosensor micro-
esculetin displaying the most potent effects. For warfarin,
physiometer is a biosensing instrument that determines the
only the highest concentration (100µg/ml) irreversibly
extracellular acidification rate of cells, which is closely
suppressed the metabolism of the MCF-7 cells tested.
coupled to their basal metabolic rate. Monitoring of cellular
The acid phosphatase (AP) assay is based on hydrolysis
metabolism is achieved using a pH-sensitive sensor, in ‘real-
of pNPP by intracellular AP in viable cells to produce p-
time’, which offers distinct advantages over the end-point
nitrophenol. The method shows higher sensitivity and
nature of the MTT assay, when examining the effect of
reproducibility in comparison to cell proliferation assays
chemical agents on cellular metabolism [12]. The effect of
based on reduction of tetrazolium salts (e.g. MTT assay) and
24hr exposure of MCF-7 cells to two coumarin compounds
3808 Current Pharmaceutical Design, 2004, Vol. 10, No. 30 Lacy and O’Kennedy
is especially suited to applications where a large number of
inhibit both tyrosine kinase phosphorylation and its kinase
samples are assayed [82, 83]. The AP assay was performed
activity. Therefore, from our research it is evident that
on both cells lines. Both esculetin and genistein were the
esculetin alone inhibits cell proliferation, which can be
most potent proliferative inhibitors. Genistein had a proli-
partially attributed to its tyrosine kinase inhibition activity.
ferative effect at low concentrations only in MCF-7 cells,
Esculetin is known to be a cytostatic drug and the
which was expected and correlates well with previous
inhibition of the cell-cycle at transition G
studies [84]. Overall the AP assay was found to offer the best
with the cytostatic effect of both 7-hydroxycoumarin and
combination of sensitivity, linearity, flexibility, ease of
esculetin. It is also evident from previous studies that
performance, reproducibility and precision, of all the micro-
esculetin primarily effects/inhibits events in the G
the cell cycle [58, 59]. If cells are arrested in G1 phase before
The investigation of how esculetin and warfarin affect the
S phase progression there would be a significant decrease in
signal transduction cascade and cell cycle progression in
DNA synthesis expected in these arrested cells. Therefore,
MCF-7 cells was performed using three different assay
the results obtained indicate there is a significant decrease in
formats. An ELISA for detection of tyrosine phosphorylation
DNA synthesis in MCF-7 cells treated with either esculetin
in whole cells was used in order to determine whether the
or genistein but not warfarin. It is possible that the decrease
agents tested inhibit tyrosine phosphorylation of growth
in DNA synthesis in esculetin-treated MCF-7 cells is due to
factor stimulated EGF-R in MCF-7 cells. The cytosensor
the agent’s ability to induce G1 arrest with no progression to
microphysiometer was utilised to determine if esculetin or
S phase where DNA synthesis occurs. Genistein seems to
warfarin inhibit tyrosine kinase activity in EGF-stimulated
affect cell cycle progression differently to esculetin.
MCF-7 cells. The final assay again utilised the ELISA
Genistein results show that the decline in DNA synthesis
format, with the aim of determining to what extent the agents
occurs at a higher concentration than esculetin and this may
inhibited DNA synthesis in MCF-7 cells. Previous studies
be due to the fact that genistein does not arrest cells at G1
have investigated the effects of E2 on ER stimulation and
phase. Genistein has been shown to inhibit progression later
signal transduction [85-87]. However, breast cancer cells can
at G2/M phase transition [5, 70, 73]. This is after S phase and
be stimulated to proliferate with growth factors in the
therefore, some DNA synthesis may occur. However, this
absence of added estrogen or progesterone. MAP kinase
stop in G2/M phase usually is followed by apoptosis and not
activation increases in response to stimuli such as EGF and
progression into mitosis as would happen in normal cycling
IGF-1. Urokinase type plasminogen activator, FGF-2 and
cells. This leads to a decrease in DNA synthesis as cells die
insulin activate MAP kinase in MCF-7 cells [88-90].
Therefore, it was possible in this study to successfullystimulate the EGF-R in MCF-7 cells with EGF and, in turn,
Taken together the signal transduction and cell cycle
activate the MAP kinase pathway in the absence of E
regulation results indicate what the possible target of
esculetin in MCF-7 cells is and how it affects components of
The regulation of activated MAP kinase in MCF-7 cells
the activated MAP kinase pathway. This inhibition affects
involves inhibitory (TNF-α) as well as stimulatory (EGF)
downstream molecules (e.g. Ras, ERK, Myc and Nuclear
pathways. Research has shown that EGF stimulates activated
ER) with important roles in MAP kinase cascade [93].
MAP kinase within 1-2 minutes in MCF-7 cells. Maximal
Therefore, esculetin can inhibit the receptor tyrosine kinase
stimulation occurs at 6-8 minutes with a decrease in MAP
activity of growth factor receptors such as EGF-R and ER.
kinase stimulation after this time period [91]. The cytosensor
This in turn will prevent growth signals reaching other
results reflect this stimulation pattern as after the transient
signalling intermediates such as Ras, or activation of trans-
maximal stimulation of EGF-R (which will also transiently
cription factors such as Myc. Another signal transduction
stimulate downstream MAP kinase activation), there is a
pathway involves phosphatidylinositol-3-kinase (PI3-K)
decline in stimulation after a short time period of ~10
heterodimer, which is an important mediator of survival
minutes. It was important to determine for this study that the
factors, protecting many cell types from multiple apoptosis-
EGF-R is tyrosine phosphorylated in MCF-7 cells. This has
inducing stimuli. If PI3-K is inhibited (by esculetin inhibi-
been demonstrated and tyrosine kinase activity was also
ting phosphorylation) the signalling pathway is interrupted
detected in Western blots of whole-cell protein extracts from
and the cell is unable to progress into the S phase of the cell
the MCF-7 cell line probed with an anti-phosphotyrosine
antibody [92]. Therefore, when MCF-7 cells were pre-exposed to either esculetin or warfarin it was possible to
CONCLUSIONS
determine if these agents inhibited tyrosine phosphorylationor not. The ELISA for detection of tyrosine phosphorylation
Coumarin and coumarin-related compounds have proved
in MCF-7 cells yielded results that indicated esculetin
for many years to have significant therapeutic potential.
inhibited tyrosine phosphorylation in EGF stimulated cells
They come from a wide variety of natural sources and new
by up to 20% more than control cells. Warfarin is a less
coumarin derivatives are being discovered or synthesised on
potent inhibitor of cell proliferation and metabolic activity
a regular basis. Coumarin is a simple molecule and many of
than esculetin and this may be partly due to the fact that it
its derivatives have been known for more than a century.
shows no significant tyrosine kinase phosphorylation
However, their vital role in plant and animal biology has not
inhibition in comparison to esculetin and the positive control,
been fully exploited. Coumarins have multiple biological
genistein. The observed results from the cytosensor micro-
activities including disease prevention, growth modulation
physiometer correlated well with the ELISA results as both
and anti-oxidant properties. These compounds are known to
sets of results demonstrate that esculetin has the ability to
exert anti-tumour effects and can cause significant changes
Studies on Coumarins and Coumarin-Related Compounds Current Pharmaceutical Design, 2004, Vol. 10, No. 30 3809
in the regulation of immune responses, cell growth and
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Ricerca Finalizzata RFPS-2007-2-634791. Detection, characterization prevention of Major Adverse Cardiac Events after Drug Eluting Stent implantation in patients with Acute Corona- ry Syndrome Dati identificativi del progetto Proposta PS 08 - Sviluppo di nuove strategie conoscitive, diagnostiche, terapeutiche e organiz-zative in pazienti con sindromi coronariche acute Ente pro
TABLE OF CONTENTS Section 2: Plan Structure and Funding / Plan Description . 3 Section 7: Use of Derivative Instruments . 11 Section 8: Performance Objectives and Reporting . 12 Section 11: Responsible Investing & Voting Rights . 16 Section 12: Conflict of Interest and Code of Ethics . 17 Appendix B: Asset Class Policies-Legislative Constraints Teachers’ Pension Plan SIPP A