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Research reports
IJAR-75Res.QXD
5/19/02 9:37 AM
Page 63
Research R e p o r t s B
O B
H
A R R I S
and 50% oil concentrations delayed
PAPILLOMAS AND SAGE
appearance by 1 and 3 weeks, respec-
Salvia libanotica (synonymous with
tively. At week 16, application of 5%,
S. triloba and S. fruticosa) is widespread
50% and 100% essential oil inhibited
in Lebanon and traditionally used by
tumour incidence by 11%, 30% and
Middle Eastern herbalists to treat
33% respectively and tumour yield by
headaches, gastric and respiratory
42%, 41% and 78%, respectively. The
problems. Although the antimicrobial
chronic topical applications of sage oil
properties of the essential oil have
did not affect skin morphology, weight,
been investigated, its effect on skin car-
survival or behaviour of treated ani-
cinogenesis has not been evaluated up
mals, implying that the applications
until now.
were not toxic.
As mutations caused by tumour
Sage oil was also applied to a
initiation are irreversible, it is impor-
receiving either sage oil intraperi-
tant in skin cancer prevention to iden-
toneally (4% and 8%), by gavage
tify compounds that act against the
(0.3 ml of 100%) or by topical applica-
reversible
of
tion (5%, 50% and 100%) 20 minutes
tumorigenesis. Lebanese researchers
before each TPA treatment. The inci-
(Gali-Muhtasib and Affara, 2001)
dence and yield of skin tumours were
therefore examined the effect of Salvia
recorded weekly for 20 weeks and
libanotica essential oil on the tumour-
tumour weight and volume were
promoting activities of 12-O-tetrade-
recorded at weeks 17 and 20.
propagation
phase
(SP-1) that was originally induced by treatment with TPA, i.e. the same as the in-vivo study. At doses higher than 50 g/ml, the essential oil significantly inhibited cell proliferation in a dosedependent manner without being toxic. This result was consistent with the in-vivo topical application tests.
canoylphorbol-13-acetate (TPA) on
The gavage and i.p. applications
tumours initiated with 7,12-dimethyl-
of sage essential oil did not reduce
benz[a]anthracine (DMBA).
tumour incidence or yield, but signifi-
The essential oil was distilled
cantly reduced the weight of papillo-
from the fresh leaves (yield 1.5–1.9%)
mas by 80% and 55% (using the 8%
and found to contain 1,8-cineole
dose), respectively. These results were
(57.4%) and camphor (8.4%) as the
explained in terms of problems with
main components. The LD50 of the
pharmacodynamics and bioavailability.
essential oil in mice was determined as
In contrast, the topical applica-
a 12% concentration.
mouse papilloma-derived cell line
tion of sage essential oil significantly
The authors concluded that S. libanotica essential oil was a potent antitumour-promoting agent against carcinogenesis in mice and that further study could develop the oil as an effective chemopreventive agent against skin cancer.
TEA TREE AND INFLAMMATION
Mice were initiated with a single
reduced the tumour-promoting effects
The essential oil of Melaleuca alternifolia
topical application of DMBA and 3
of TPA both by inhibiting new papillo-
has demonstrated anti-inflammatory
weeks later, promotion was started
mas and the growth of existing ones.
activity in animal models and its main
twice weekly by topical application of
The
highest
component, terpinen-4-ol, has been
TPA to shaved dorsal skin. Test mice
inhibitory activity, causing a 4-week
found to suppress the production of
were divided into three groups, each
delay in tumour appearance, whilst 5%
pro-inflammatory cytokines in human
100%
T h e I n t e r n a t i o n a l J o u r n a l o f A r o m a t h e r a p y 2002
oil
vol
had
12
no
the
1
63
0962-4562/02/$ - see front matter © 2002 Elsevier Science Ltd.
All Rights Reserved.
IJAR-75Res.QXD
5/19/02 9:37 AM
Page 64
monocytes. To further investigate the
acted as a selective barrier, only allowing
through the skin and their effect upon
mechanism of anti-inflammatory activ-
penetration of the more water-soluble
inflammatory cells in-vivo are required.
ity, an Australian group (Brand et al.,
components into the dermis. Used at concentrations found in
2001) focussed their attention on
the whole oil (and equivalent to
COLON CANCER
0.031% essential oil), terpinen-4-ol
For more than 10 years, epidemiological
demonstrated
dose-
studies have shown that the dietary
peroxide, superoxide, singlet oxygen,
dependent suppression of superoxide
consumption of plant products may
hydroxyl radicals, hypochlorous acid
production in monocytes stimulated
reduce the incidence of colorectal can-
and various chloramines. They are
with fMLP and LPS, but not PMA. The
cer. The identification of phytochemi-
formed when macrophages and neu-
two former compounds bind to cell
cals with antitumour activity is hoped
trophils are stimulated, assembling
receptors and act on intracellular pro-
to lead to significant advances in the
(NADPH) oxidase on their plasma
tein kinase C. As terpinen-4-ol did not
prevention of human cancer. Some
membranes,
oxygen-derived
reactive
species
(ODRS). These species include hydrogen
a
significant
subsequently
exert an effect before the addition of
monoterpenoids that are found in
promote the reduction of oxygen in
the agonist, it must act at a point after
many essential oils have already been
the extracellular fluid. The ODRS are
the receptor phase. At an equivalent
found to possess antitumour activity.
important for host defences, being
concentration of between 0.00025% and
For example, limonene has demon-
both antitumoral and antimicrobial,
0.001% essential oil, ␣-terpineol sup-
strated antitumour activity against
but their production during acute and
pressed the superoxide production
breast, lung, stomach, liver and skin
chronic inflammation is cytotoxic and
induced by all three agonists, suggest-
cancers in animals and is undergoing
may cause tissue and DNA damage.
ing that it worked on protein kinase
clinical trials in humans. Geraniol, a
which
Human neutrophils and mono-
C or a precursor. The two components
monoterpene alcohol, has also demon-
cytes were isolated from healthy volun-
therefore had a different inhibitory
strated antitumour activity against
teers and their superoxide production
mode of action upon superoxide
a range of animal cancer cells both
determined by means of chemilumi-
production.
in-vitro and in-vivo. Thus a French team
nescence resulting from oxidation of a
The water-soluble components
(Carnesecchi et al., 2001) decided to
fluorescent compound. Measurements
had no significant effect on stimulated
investigate its activity with regard to
were taken in the presence of one of
superoxide production by neutrophils.
colonic cancer cells.
three superoxide agonists; N-formyl-
1,8-cineole was inactive with regard to
They examined the in-vitro effect
methionyl-leucyl-phenylalanine
both cell types. Analysis of the uptake
of geraniol on the growth of a human
(fMLP),
from
of both components by monocytes and
colonic cancer cell line, Caco-2.
Escherichia coli (LPS) or phorbol 12-
neutrophils revealed no significant
Geraniol was added to cell cultures at
myristate 13-acetate (PMA).
differences.
concentrations between 100 M and
lipopolysaccharide
The effects of tea tree essential oil
The study implied that M. alterni-
500 M and was found to inhibit cell
and its water-soluble components (ter-
folia essential oil has potential as an
proliferation in a dose-dependent
pinen-4-ol, 1,8-cineole and ␣-terpineol)
anti-inflammatory agent since it con-
manner. At 400 M, it caused a 70%
were investigated upon superoxide
tains water-soluble components that
inhibition of cell growth and this con-
production in the absence and pres-
may selectively regulate cell function
centration was therefore used in fur-
ence of agonists. It was found that
during inflammation. This means that
ther experiments.
whole tea tree oil contained compo-
neutrophils could be fully active in
Apoptosis and cytotoxicity induced
nents that activated cell superoxide
eliminating foreign antigens whilst
by geraniol were investigated as possi-
production. However, it was not
monocyte superoxide production was
ble causes of the growth inhibition,
thought likely that the blood cells
suppressed and oxidative tissue dam-
using DNA fragmentation and the
would be exposed to whole essential oil
age prevented. Further research into
release of lactate dehydrogenase (into
in-vivo, since the stratum corneum
the penetration of tea tree components
the culture medium), respectively.
© 2002 Elsevier Science Ltd.
All Rights Reserved.
64
T h e I n t e r n a t i o n a l J o u r n a l o f A r o m a t h e r a p y 2002
vol
12
no
1
IJAR-75Res.QXD
5/19/02 9:37 AM
Page 65
It was found that geraniol did not
effect on the growth of human colon
indicator. The minimum agar concen-
induce apoptosis or exhibit cytotoxicity
cancer cells, was cytostatic in effect,
tration (MAC) of essential oil was
and so cell cycle analysis was then per-
had no cytotoxicity and inhibited
defined as the concentration of oil
formed over a 6-day period. In the
DNA synthesis. The low toxicity of
absorbed in agar after incubation for
presence of geraniol, cells accumulated
geraniol will enable future in-vivo stud-
3 days on an MID plate.
in the S phase of growth (where DNA is
ies in colon cancer prevention to be
replicated) whilst numbers in the G1
performed.
A third test used a standard agar dilution assay where the essential oils or their major components were incor-
phase (the phase before S, where the
porated into the agar medium before
cells become metabolically active)
ANTIFUNGAL VAPOUR
gradually decreased. Interestingly, this
inoculation with the fungi. The mini-
result differed from the antitumour
The determination of the antimycotic
mum inhibitory concentration (MIC)
effects of another monoterpenoid, per-
activity of essential oils is usually per-
was defined as the lowest concentra-
illyl alcohol, which decreased the num-
formed in aqueous media (e.g. agar)
tion of essential oil or component
ber of human breast cancer cells in the
but there have been no reports of the
inhibiting visible colony formation
S phase whilst increasing cells in the
effect of essential oil vapour against
after 3 days. The essential oil/compo-
G1 phase.
dermatophytes. A Japanese study
nent content of the MIC agar was
It was thus shown that geraniol
(Inouye et al., 2001) developed a novel
determined as before; the MAC here
inhibited DNA synthesis within the
method of evaluating the effect of
defined as the concentration of essen-
cell. This was further proven by the
essential oil vapour on fungi and at the
tial oil/component remaining in the
addition of radiolabelled thymidine
same time, the concentration of essen-
agar of an MIC plate.
and geraniol to cell cultures; the incor-
tial oil absorbed into the agar medium.
The results for both fungal species
Seven essential oils were used in
were almost identical with antifungal
poration of thymidine into cellular the
bark,
activity in the order: cinnamon bark9
To investigate the mechanism
lemongrass, thyme CT carvacrol, per-
lemongrass9thyme9perilla9laven-
whereby geraniol inhibited DNA syn-
illa, lavender, tea tree and lemon)
der9tea tree9lemon. The MID values
thesis, the effects of geraniol on cellular
against
dermatophytes
were less than the MIC values in all the
polyamine metabolism were examined.
Trichophyton rubrum and T. mentagro-
oils examined, e.g. for cinnamon bark
The activities of two key enzymes were
phytes. The agar medium was inocu-
an MID of 0.25 and an MIC of 12.5.
monitored. In the presence of geraniol,
lated with either fungi and placed in
The MAC values by vapour contact
ornithine decarboxylase activity (an
an airtight box. A filter paper impreg-
were 1.4–4.7 times less than the MACs
activity that is enhanced during cancer
nated with 100 l of essential oil (two-
by agar dilution. The results demon-
growth) was reduced by 50% whilst
fold dilutions in ethyl alcohol) was
strated that fungal growth was inhib-
S-adenosylmethionine decarboxylase
placed in each box. Then 1 ml of air
ited by lesser amounts of essential oils
activity increased by 30%. This was
was periodically extracted from each
by vapour contact than by solution con-
accompanied by a 40% decrease in the
box and the essential oil content veri-
tact, i.e. vapour contact was more effec-
cellular putrescine pool and a concomi-
fied. The minimum inhibitory dose
tive. The testing of the major essential
DNA was reduced by 55%.
experiment
the
⫺1
(cinnamon
two
tant 60% increase in the N-acetylsper-
(MID g/ml
air space) was defined
oil components showed that these
midine pool. Overall, these results
as the minimum quantity of essential
components were responsible for the
demonstrated that geraniol activated
oil added to inhibit growth of the fungi
antimycotic activity of their parent oils.
intracellular polyamine catabolism,
after 3 days (at which time the controls
Using four selected essential oils,
although it was not certain if polyamine
had developed a visible colony).
their effect by vapour contact was
The agar from each MID plate
examined in more detail. Perilla,
was removed and the absorbed essen-
thyme and lemongrass killed fungal
research
tial oil extracted and estimated using
conidia (spores), inhibited germination
showed that geraniol had a potent
the predominant component as an
and hyphal elongation at 1–4 g/ml⫺1,
depletion was solely responsible for the antiproliferative effect. In
conclusion,
the
© 2002 Elsevier Science Ltd.
T h e I n t e r n a t i o n a l J o u r n a l o f A r o m a t h e r a p y 2002
vol
12
no
1
65
All Rights Reserved.
IJAR-75Res.QXD
5/19/02 9:37 AM
whilst
lavender
was
Page 66
effective
at
⫺1
40–60 g/ml . The in-vivo effectiveness of thyme and perilla essential oils was then
and
The effect of the oil and individ-
anisaldehyde (2.6%). The whole oil
ual components were also examined
and the three individual components
with regard to enhancement of human
were used in the experiments.
immune cell growth by adding them to
(87.8%),
limonene
(3.9%)
tested in experimental dermatophyto-
As antimutagenicity is one of the
cultures of T and B lymphocytes. At a
sis in guinea pigs. Their feet were inoc-
first methods to be employed when
concentration of 1 g/L the essential oil
ulated with T. mentagrophytes and after
screening new compounds for anticar-
enhanced the growth of cell lines by up
infection was established, the feet were
cinogenic activity, the test solutions
to 200%, whereas individual compo-
wrapped in gauze. A disc impregnated
were individually added to a trans-
nents had far fewer effects. Kinetic
with either 20 mg of thyme oil or 20 mg
formed Chinese hamster ovary cell line
analysis using the B lymphocyte cell
of perilla oil was then attached to the
(CHO AS-52), a line more efficient in
line revealed that the whole oil
gauze and occluded. This procedure
detecting deletion-type mutations than
enhanced growth by 180% within the
was repeated once a day for 3 days and
bacteria. In the presence of a strong
first 10 minutes of contact, whereas the
the level of infection evaluated. There
mutagenic substance, 1.0 g/L of essen-
individual components started to
was no significant difference in efficacy
tial oil improved antimutagenicity by
slowly
between the two oils. Neither resolved
75% as compared to the control. The
minutes.
the infection completely but the sever-
addition of the three main compo-
ity was significantly reduced in com-
nents in the same concentrations did
that the essential oil of A. rugosa could
parison to the controls.
not provide the same level of protec-
selectively inhibit the proliferation of
It was concluded that the use of
tion as the whole oil. Both anisalde-
human cancer cells and promote
essential oils in the vapour state for
hyde and limonene had greater activity
human immune cell growth. The
antimycotic purposes was promising.
than methyl chavicol.
essential oil was more effective than
enhance
growth
after
20
The series of experiments showed
There was homogenous absorption of
Cytotoxicity testing was carried
individual components, indicating a
vapour over a wide skin surface (effi-
out on a normal human liver cell line.
synergistic effect between them and/or
cient percutaneous absorption of
Both the whole oil and its three com-
other minor components within the
vaporized thyme and perilla was shown
ponents were shown to possess low
oil. It was stressed that as a preliminary
in mice but the data was not given) and
cytotoxicity by inhibiting less than 12%
report, more investigations using
there was little chemical irritation due
of normal growth at a concentration of
in-vivo methods were necessary to fully
to the slow rate of absorption. It was
0.8 g/L. The cytotoxicity of the three
elucidate the effects of the oil on
noted that most antifungal agents cur-
individual components was less than
human cancer cells.
rently in clinical use are non-volatile.
that of the whole oil, with anisaldehyde possessing the least. The antimutagenic effect of the
REFERENCES Brand, C., Ferrant, A., Prager, R.H.,
ANTICANCER AGASTACHE
whole oil and the three individual
Riley, T.V., Carson, C.F., Finlay-
Agastache rugosa (Korean mint or wrin-
components was then tested using
Jones, J.J., Hart, P.H. (2001) The
kled giant hyssop) is a plant widely dis-
human lung, liver, gastric and breast
water-soluble components of the
tributed throughout Asia and has been
carcinoma cell lines. The oil at 1 g/L
essential oil of Melaleuca alternifolia
used extensively as a source of flavour-
inhibited the proliferation of all cancer
(tea tree oil) suppress the production
ing and oil due to its unique taste char-
cell lines, having the greatest effect on
acteristics. A Korean team (Kim et al.,
lung cancer cells with an inhibition of
2001) investigated its effects on human
82%. Gastric carcinoma cells were the
cancer cell lines and lymphocytes.
least affected. The components had
of superoxide by human monocytes, but
not
neutrophils,
activated
in-vitro. Inflamm. Res. 50: 213–219. Carneseecchi,
S.,
Schneider,
J.,
Ceraline, J., Duranton, B., Gosse, F.,
The flower essential oil was
lower activities than the whole oil, with
Seiler, N., Raul, F. (2001) Geraniol, a
obtained by steam distillation and
methyl chavicol demonstrating the
component of plant essential oils,
found to contain mainly methyl chavicol
highest anticancer activity.
inhibits
growth
and
polyamine
© 2002 Elsevier Science Ltd.
All Rights Reserved.
66
T h e I n t e r n a t i o n a l J o u r n a l o f A r o m a t h e r a p y 2002
vol
12
no
1
IJAR-75Res.QXD
5/19/02 9:37 AM
Page 67
biosynthesis in human colon cancer
Inouye, S., Uchida, K., Yamaguchi, H.
Park, Y.S., Hwang, S.J., Kim, J.H.
cells. J. Pharm. Exper. Ther. 298:
(2001) In-vitro and in-vivo anti-
(2001) The effect of the oil of
197–200.
Trichophyton activity of essential oils
Agastache rugosa O. Kuntze and three
by vapour contact. Mycoses 44:
of its components on human cancer
99–107.
cell lines. J. Essent. Oil Res. 13:
Gali-Muhtasib, H.U., Affara, N.I. (2001) Chemopreventive effects of sage oil on skin papillomas in mice. Phytomedicine 7: 129–136.
Kim, M.H., Chung, W.T., Kim, Y.K.,
214–218.
Lee, J.H., Lee, H.Y., Hwang, B.,
© 2002 Elsevier Science Ltd.
T h e I n t e r n a t i o n a l J o u r n a l o f A r o m a t h e r a p y 2002
vol
12
no
1
67
All Rights Reserved.
5/19/02 9:37 AM
Page 63
Research R e p o r t s B
O B
H
A R R I S
and 50% oil concentrations delayed
PAPILLOMAS AND SAGE
appearance by 1 and 3 weeks, respec-
Salvia libanotica (synonymous with
tively. At week 16, application of 5%,
S. triloba and S. fruticosa) is widespread
50% and 100% essential oil inhibited
in Lebanon and traditionally used by
tumour incidence by 11%, 30% and
Middle Eastern herbalists to treat
33% respectively and tumour yield by
headaches, gastric and respiratory
42%, 41% and 78%, respectively. The
problems. Although the antimicrobial
chronic topical applications of sage oil
properties of the essential oil have
did not affect skin morphology, weight,
been investigated, its effect on skin car-
survival or behaviour of treated ani-
cinogenesis has not been evaluated up
mals, implying that the applications
until now.
were not toxic.
As mutations caused by tumour
Sage oil was also applied to a
initiation are irreversible, it is impor-
receiving either sage oil intraperi-
tant in skin cancer prevention to iden-
toneally (4% and 8%), by gavage
tify compounds that act against the
(0.3 ml of 100%) or by topical applica-
reversible
of
tion (5%, 50% and 100%) 20 minutes
tumorigenesis. Lebanese researchers
before each TPA treatment. The inci-
(Gali-Muhtasib and Affara, 2001)
dence and yield of skin tumours were
therefore examined the effect of Salvia
recorded weekly for 20 weeks and
libanotica essential oil on the tumour-
tumour weight and volume were
promoting activities of 12-O-tetrade-
recorded at weeks 17 and 20.
propagation
phase
(SP-1) that was originally induced by treatment with TPA, i.e. the same as the in-vivo study. At doses higher than 50 g/ml, the essential oil significantly inhibited cell proliferation in a dosedependent manner without being toxic. This result was consistent with the in-vivo topical application tests.
canoylphorbol-13-acetate (TPA) on
The gavage and i.p. applications
tumours initiated with 7,12-dimethyl-
of sage essential oil did not reduce
benz[a]anthracine (DMBA).
tumour incidence or yield, but signifi-
The essential oil was distilled
cantly reduced the weight of papillo-
from the fresh leaves (yield 1.5–1.9%)
mas by 80% and 55% (using the 8%
and found to contain 1,8-cineole
dose), respectively. These results were
(57.4%) and camphor (8.4%) as the
explained in terms of problems with
main components. The LD50 of the
pharmacodynamics and bioavailability.
essential oil in mice was determined as
In contrast, the topical applica-
a 12% concentration.
mouse papilloma-derived cell line
tion of sage essential oil significantly
The authors concluded that S. libanotica essential oil was a potent antitumour-promoting agent against carcinogenesis in mice and that further study could develop the oil as an effective chemopreventive agent against skin cancer.
TEA TREE AND INFLAMMATION
Mice were initiated with a single
reduced the tumour-promoting effects
The essential oil of Melaleuca alternifolia
topical application of DMBA and 3
of TPA both by inhibiting new papillo-
has demonstrated anti-inflammatory
weeks later, promotion was started
mas and the growth of existing ones.
activity in animal models and its main
twice weekly by topical application of
The
highest
component, terpinen-4-ol, has been
TPA to shaved dorsal skin. Test mice
inhibitory activity, causing a 4-week
found to suppress the production of
were divided into three groups, each
delay in tumour appearance, whilst 5%
pro-inflammatory cytokines in human
100%
T h e I n t e r n a t i o n a l J o u r n a l o f A r o m a t h e r a p y 2002
oil
vol
had
12
no
the
1
63
0962-4562/02/$ - see front matter © 2002 Elsevier Science Ltd.
All Rights Reserved.
IJAR-75Res.QXD
5/19/02 9:37 AM
Page 64
monocytes. To further investigate the
acted as a selective barrier, only allowing
through the skin and their effect upon
mechanism of anti-inflammatory activ-
penetration of the more water-soluble
inflammatory cells in-vivo are required.
ity, an Australian group (Brand et al.,
components into the dermis. Used at concentrations found in
2001) focussed their attention on
the whole oil (and equivalent to
COLON CANCER
0.031% essential oil), terpinen-4-ol
For more than 10 years, epidemiological
demonstrated
dose-
studies have shown that the dietary
peroxide, superoxide, singlet oxygen,
dependent suppression of superoxide
consumption of plant products may
hydroxyl radicals, hypochlorous acid
production in monocytes stimulated
reduce the incidence of colorectal can-
and various chloramines. They are
with fMLP and LPS, but not PMA. The
cer. The identification of phytochemi-
formed when macrophages and neu-
two former compounds bind to cell
cals with antitumour activity is hoped
trophils are stimulated, assembling
receptors and act on intracellular pro-
to lead to significant advances in the
(NADPH) oxidase on their plasma
tein kinase C. As terpinen-4-ol did not
prevention of human cancer. Some
membranes,
oxygen-derived
reactive
species
(ODRS). These species include hydrogen
a
significant
subsequently
exert an effect before the addition of
monoterpenoids that are found in
promote the reduction of oxygen in
the agonist, it must act at a point after
many essential oils have already been
the extracellular fluid. The ODRS are
the receptor phase. At an equivalent
found to possess antitumour activity.
important for host defences, being
concentration of between 0.00025% and
For example, limonene has demon-
both antitumoral and antimicrobial,
0.001% essential oil, ␣-terpineol sup-
strated antitumour activity against
but their production during acute and
pressed the superoxide production
breast, lung, stomach, liver and skin
chronic inflammation is cytotoxic and
induced by all three agonists, suggest-
cancers in animals and is undergoing
may cause tissue and DNA damage.
ing that it worked on protein kinase
clinical trials in humans. Geraniol, a
which
Human neutrophils and mono-
C or a precursor. The two components
monoterpene alcohol, has also demon-
cytes were isolated from healthy volun-
therefore had a different inhibitory
strated antitumour activity against
teers and their superoxide production
mode of action upon superoxide
a range of animal cancer cells both
determined by means of chemilumi-
production.
in-vitro and in-vivo. Thus a French team
nescence resulting from oxidation of a
The water-soluble components
(Carnesecchi et al., 2001) decided to
fluorescent compound. Measurements
had no significant effect on stimulated
investigate its activity with regard to
were taken in the presence of one of
superoxide production by neutrophils.
colonic cancer cells.
three superoxide agonists; N-formyl-
1,8-cineole was inactive with regard to
They examined the in-vitro effect
methionyl-leucyl-phenylalanine
both cell types. Analysis of the uptake
of geraniol on the growth of a human
(fMLP),
from
of both components by monocytes and
colonic cancer cell line, Caco-2.
Escherichia coli (LPS) or phorbol 12-
neutrophils revealed no significant
Geraniol was added to cell cultures at
myristate 13-acetate (PMA).
differences.
concentrations between 100 M and
lipopolysaccharide
The effects of tea tree essential oil
The study implied that M. alterni-
500 M and was found to inhibit cell
and its water-soluble components (ter-
folia essential oil has potential as an
proliferation in a dose-dependent
pinen-4-ol, 1,8-cineole and ␣-terpineol)
anti-inflammatory agent since it con-
manner. At 400 M, it caused a 70%
were investigated upon superoxide
tains water-soluble components that
inhibition of cell growth and this con-
production in the absence and pres-
may selectively regulate cell function
centration was therefore used in fur-
ence of agonists. It was found that
during inflammation. This means that
ther experiments.
whole tea tree oil contained compo-
neutrophils could be fully active in
Apoptosis and cytotoxicity induced
nents that activated cell superoxide
eliminating foreign antigens whilst
by geraniol were investigated as possi-
production. However, it was not
monocyte superoxide production was
ble causes of the growth inhibition,
thought likely that the blood cells
suppressed and oxidative tissue dam-
using DNA fragmentation and the
would be exposed to whole essential oil
age prevented. Further research into
release of lactate dehydrogenase (into
in-vivo, since the stratum corneum
the penetration of tea tree components
the culture medium), respectively.
© 2002 Elsevier Science Ltd.
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It was found that geraniol did not
effect on the growth of human colon
indicator. The minimum agar concen-
induce apoptosis or exhibit cytotoxicity
cancer cells, was cytostatic in effect,
tration (MAC) of essential oil was
and so cell cycle analysis was then per-
had no cytotoxicity and inhibited
defined as the concentration of oil
formed over a 6-day period. In the
DNA synthesis. The low toxicity of
absorbed in agar after incubation for
presence of geraniol, cells accumulated
geraniol will enable future in-vivo stud-
3 days on an MID plate.
in the S phase of growth (where DNA is
ies in colon cancer prevention to be
replicated) whilst numbers in the G1
performed.
A third test used a standard agar dilution assay where the essential oils or their major components were incor-
phase (the phase before S, where the
porated into the agar medium before
cells become metabolically active)
ANTIFUNGAL VAPOUR
gradually decreased. Interestingly, this
inoculation with the fungi. The mini-
result differed from the antitumour
The determination of the antimycotic
mum inhibitory concentration (MIC)
effects of another monoterpenoid, per-
activity of essential oils is usually per-
was defined as the lowest concentra-
illyl alcohol, which decreased the num-
formed in aqueous media (e.g. agar)
tion of essential oil or component
ber of human breast cancer cells in the
but there have been no reports of the
inhibiting visible colony formation
S phase whilst increasing cells in the
effect of essential oil vapour against
after 3 days. The essential oil/compo-
G1 phase.
dermatophytes. A Japanese study
nent content of the MIC agar was
It was thus shown that geraniol
(Inouye et al., 2001) developed a novel
determined as before; the MAC here
inhibited DNA synthesis within the
method of evaluating the effect of
defined as the concentration of essen-
cell. This was further proven by the
essential oil vapour on fungi and at the
tial oil/component remaining in the
addition of radiolabelled thymidine
same time, the concentration of essen-
agar of an MIC plate.
and geraniol to cell cultures; the incor-
tial oil absorbed into the agar medium.
The results for both fungal species
Seven essential oils were used in
were almost identical with antifungal
poration of thymidine into cellular the
bark,
activity in the order: cinnamon bark9
To investigate the mechanism
lemongrass, thyme CT carvacrol, per-
lemongrass9thyme9perilla9laven-
whereby geraniol inhibited DNA syn-
illa, lavender, tea tree and lemon)
der9tea tree9lemon. The MID values
thesis, the effects of geraniol on cellular
against
dermatophytes
were less than the MIC values in all the
polyamine metabolism were examined.
Trichophyton rubrum and T. mentagro-
oils examined, e.g. for cinnamon bark
The activities of two key enzymes were
phytes. The agar medium was inocu-
an MID of 0.25 and an MIC of 12.5.
monitored. In the presence of geraniol,
lated with either fungi and placed in
The MAC values by vapour contact
ornithine decarboxylase activity (an
an airtight box. A filter paper impreg-
were 1.4–4.7 times less than the MACs
activity that is enhanced during cancer
nated with 100 l of essential oil (two-
by agar dilution. The results demon-
growth) was reduced by 50% whilst
fold dilutions in ethyl alcohol) was
strated that fungal growth was inhib-
S-adenosylmethionine decarboxylase
placed in each box. Then 1 ml of air
ited by lesser amounts of essential oils
activity increased by 30%. This was
was periodically extracted from each
by vapour contact than by solution con-
accompanied by a 40% decrease in the
box and the essential oil content veri-
tact, i.e. vapour contact was more effec-
cellular putrescine pool and a concomi-
fied. The minimum inhibitory dose
tive. The testing of the major essential
DNA was reduced by 55%.
experiment
the
⫺1
(cinnamon
two
tant 60% increase in the N-acetylsper-
(MID g/ml
air space) was defined
oil components showed that these
midine pool. Overall, these results
as the minimum quantity of essential
components were responsible for the
demonstrated that geraniol activated
oil added to inhibit growth of the fungi
antimycotic activity of their parent oils.
intracellular polyamine catabolism,
after 3 days (at which time the controls
Using four selected essential oils,
although it was not certain if polyamine
had developed a visible colony).
their effect by vapour contact was
The agar from each MID plate
examined in more detail. Perilla,
was removed and the absorbed essen-
thyme and lemongrass killed fungal
research
tial oil extracted and estimated using
conidia (spores), inhibited germination
showed that geraniol had a potent
the predominant component as an
and hyphal elongation at 1–4 g/ml⫺1,
depletion was solely responsible for the antiproliferative effect. In
conclusion,
the
© 2002 Elsevier Science Ltd.
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65
All Rights Reserved.
IJAR-75Res.QXD
5/19/02 9:37 AM
whilst
lavender
was
Page 66
effective
at
⫺1
40–60 g/ml . The in-vivo effectiveness of thyme and perilla essential oils was then
and
The effect of the oil and individ-
anisaldehyde (2.6%). The whole oil
ual components were also examined
and the three individual components
with regard to enhancement of human
were used in the experiments.
immune cell growth by adding them to
(87.8%),
limonene
(3.9%)
tested in experimental dermatophyto-
As antimutagenicity is one of the
cultures of T and B lymphocytes. At a
sis in guinea pigs. Their feet were inoc-
first methods to be employed when
concentration of 1 g/L the essential oil
ulated with T. mentagrophytes and after
screening new compounds for anticar-
enhanced the growth of cell lines by up
infection was established, the feet were
cinogenic activity, the test solutions
to 200%, whereas individual compo-
wrapped in gauze. A disc impregnated
were individually added to a trans-
nents had far fewer effects. Kinetic
with either 20 mg of thyme oil or 20 mg
formed Chinese hamster ovary cell line
analysis using the B lymphocyte cell
of perilla oil was then attached to the
(CHO AS-52), a line more efficient in
line revealed that the whole oil
gauze and occluded. This procedure
detecting deletion-type mutations than
enhanced growth by 180% within the
was repeated once a day for 3 days and
bacteria. In the presence of a strong
first 10 minutes of contact, whereas the
the level of infection evaluated. There
mutagenic substance, 1.0 g/L of essen-
individual components started to
was no significant difference in efficacy
tial oil improved antimutagenicity by
slowly
between the two oils. Neither resolved
75% as compared to the control. The
minutes.
the infection completely but the sever-
addition of the three main compo-
ity was significantly reduced in com-
nents in the same concentrations did
that the essential oil of A. rugosa could
parison to the controls.
not provide the same level of protec-
selectively inhibit the proliferation of
It was concluded that the use of
tion as the whole oil. Both anisalde-
human cancer cells and promote
essential oils in the vapour state for
hyde and limonene had greater activity
human immune cell growth. The
antimycotic purposes was promising.
than methyl chavicol.
essential oil was more effective than
enhance
growth
after
20
The series of experiments showed
There was homogenous absorption of
Cytotoxicity testing was carried
individual components, indicating a
vapour over a wide skin surface (effi-
out on a normal human liver cell line.
synergistic effect between them and/or
cient percutaneous absorption of
Both the whole oil and its three com-
other minor components within the
vaporized thyme and perilla was shown
ponents were shown to possess low
oil. It was stressed that as a preliminary
in mice but the data was not given) and
cytotoxicity by inhibiting less than 12%
report, more investigations using
there was little chemical irritation due
of normal growth at a concentration of
in-vivo methods were necessary to fully
to the slow rate of absorption. It was
0.8 g/L. The cytotoxicity of the three
elucidate the effects of the oil on
noted that most antifungal agents cur-
individual components was less than
human cancer cells.
rently in clinical use are non-volatile.
that of the whole oil, with anisaldehyde possessing the least. The antimutagenic effect of the
REFERENCES Brand, C., Ferrant, A., Prager, R.H.,
ANTICANCER AGASTACHE
whole oil and the three individual
Riley, T.V., Carson, C.F., Finlay-
Agastache rugosa (Korean mint or wrin-
components was then tested using
Jones, J.J., Hart, P.H. (2001) The
kled giant hyssop) is a plant widely dis-
human lung, liver, gastric and breast
water-soluble components of the
tributed throughout Asia and has been
carcinoma cell lines. The oil at 1 g/L
essential oil of Melaleuca alternifolia
used extensively as a source of flavour-
inhibited the proliferation of all cancer
(tea tree oil) suppress the production
ing and oil due to its unique taste char-
cell lines, having the greatest effect on
acteristics. A Korean team (Kim et al.,
lung cancer cells with an inhibition of
2001) investigated its effects on human
82%. Gastric carcinoma cells were the
cancer cell lines and lymphocytes.
least affected. The components had
of superoxide by human monocytes, but
not
neutrophils,
activated
in-vitro. Inflamm. Res. 50: 213–219. Carneseecchi,
S.,
Schneider,
J.,
Ceraline, J., Duranton, B., Gosse, F.,
The flower essential oil was
lower activities than the whole oil, with
Seiler, N., Raul, F. (2001) Geraniol, a
obtained by steam distillation and
methyl chavicol demonstrating the
component of plant essential oils,
found to contain mainly methyl chavicol
highest anticancer activity.
inhibits
growth
and
polyamine
© 2002 Elsevier Science Ltd.
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66
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vol
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no
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Page 67
biosynthesis in human colon cancer
Inouye, S., Uchida, K., Yamaguchi, H.
Park, Y.S., Hwang, S.J., Kim, J.H.
cells. J. Pharm. Exper. Ther. 298:
(2001) In-vitro and in-vivo anti-
(2001) The effect of the oil of
197–200.
Trichophyton activity of essential oils
Agastache rugosa O. Kuntze and three
by vapour contact. Mycoses 44:
of its components on human cancer
99–107.
cell lines. J. Essent. Oil Res. 13:
Gali-Muhtasib, H.U., Affara, N.I. (2001) Chemopreventive effects of sage oil on skin papillomas in mice. Phytomedicine 7: 129–136.
Kim, M.H., Chung, W.T., Kim, Y.K.,
214–218.
Lee, J.H., Lee, H.Y., Hwang, B.,
© 2002 Elsevier Science Ltd.
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