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Foeniculum (Foeniculi amari fructus)


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Authorisation details
Latin name of the genus: Foeniculum
Latin name of herbal substance: Foeniculi amari fructus
Botanical name of plant: Foeniculum vulgare Miller subsp. vulgare var. vulgare
English common name of herbal substance: Bitter Fennel
Status: F: Final positive opinion adopted
Date added to the inventory: 23/11/2005
Date added to priority list: 23/11/2005
Outcome of European Assessment: Community herbal monograph
Community list entry
Additional Information:






Product Characteristics
COMMUNITY HERBAL MONOGRAPH ON FOENICULUM VULGARE MILLER SUBSP.
VULGARE VAR. VULGARE , FRUCTUS
1. N AME OF THE MEDICINAL PRODUCT
To be specified for the individual finished product.
2. Q UALITATIVE AND QUANTITATIVE COMPOSITION 1 , 2
Well-established use
Traditional use
With regard to the registration application of
Article 16d(1) of Directive 2001/83/EC as
amended.
Foeniculum vulgare Miller subsp. vulgare var.
vulgare ), fructus (Fennel, Bitter)
i) Herbal substance
Dried fennel, bitter
ii) Herbal preparations
Dried fennel, bitter, comminuted
3. PHARMACEUTICAL FORM
Well-established use
Traditional use
Herbal substance or herbal preparation as herbal
tea for oral use.
The pharmaceutical form should be described by
the European Pharmacopoeia full standard term.
1 The material complies with the Ph. Eur. monograph (ref. 01/2005:0824).
2 The declaration of the active substance(s) for an individual finished product should be in accordance with
relevant herbal quality guidance.
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4. C LINICAL PARTICULARS
4.1. Therapeutic indications
Well-established use
Traditional use
a) Traditional herbal medicinal product for
symptomatic treatment of mild, spasmodic
gastro-intestinal complaints including bloating
and flatulence.
b) Traditional herbal medicinal product for
symptomatic treatment of minor spasm
associated with menstrual periods.
c) Traditional herbal medicinal product used as
an expectorant in cough associated with cold.
The product is a traditional herbal medicinal
product for use in specified indications
exclusively based upon long-standing use.
4.2. Posology and method of administration
Well-established use
Traditional use
Posology
Adults
Single dose
1.5 to 2.5 g of (freshly 3 ) comminuted fennel fruits
with 0.25 l of boiling water (brew for 15 minutes)
three times daily as a herbal tea.
Adolescents over 12 years of age, Indication a)
Adult dose
Children between 4 and 12 years of age,
Indication a)
Average daily dose
3-5 g of (freshly 3 ) comminuted fruits as a herbal
tea, in three divided doses, for short-term use in
mild
transitory
symptoms
only
(less than one week)
The use is not recommended in children under
4 years of age (see section 4.4 Special warnings
and precautions for use).
3 For commercial preparation of crushed fennel fruits the applicant must carry out appropriate stability testing
related to the content of essential oil components.
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Well-established use
Traditional use
Duration of use
Adults
Adolescents over 12 years of age , Indication a)
Not to be taken for more than 2 weeks.
Children between 4 and 12 years of age,
Indication a)
For short-term use in mild transitory symptoms
only (less than one week).
If the symptoms persist during the use of the
medicinal product, a doctor or a qualified health
care practitioner should be consulted.
Method of administration
Oral use.
4.3. Contraindications
Well-established use
Traditional use
Hypersensitivity to the active substance and its
preparations or to Apiaceae (Umbelliferae)
( aniseed, caraway, celery, coriander and dill)
or to anethole.
4.4. Special warnings and precautions for use
Well-established use
Traditional use
The use is not recommended in children under 4
years of age due to the lack of adequate data and
paediatrician advice should be sought.
4.5. Interactions with other medicinal products and other forms of interaction
Well-established use
Traditional use
None reported.
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4.6. Pregnancy and lactation
Well-established use
Traditional use
There are no data from the use of fennel fruit in
pregnant patients.
It is unknown if fennel constituents are excreted
in human breast milk.
In the absence of sufficient data, the use during
pregnancy and lactation is not recommended.
4.7. Effects on ability to drive and use machines
Well-established use
Traditional use
No studies on the effect on the ability to drive and
use machines have been performed.
4.8. Undesirable effects
Well-established use
Traditional use
Allergic reactions to fennel, affecting the skin or
the respiratory system may occur. The frequency
is not known.
If other adverse reactions not mentioned above
occur, a doctor or a qualified health care
practitioner should be consulted.
4.9. Overdose
Well-established use
Traditional use
No case of overdose has been reported.
5. PHARMACOLOGICAL PROPERTIES
5.1. Pharmacodynamic properties
Well-established use
Traditional use
Not required as per Article 16c(1)(a)(iii) of
Directive 2001/83/EC as amended.
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5.2. Pharmacokinetic properties
Well-established use
Traditional use
Not required as per Article 16c(1)(a)(iii) of
Directive 2001/83/EC as amended.
5.3. Preclinical safety data
Well-established use
Traditional use
Not required as per Article 16c(1)(a)(iii) of
Directive 2001/83/EC as amended, unless
necessary for the safe use of the product.
A fennel aqueous extract was tested in an Ames
test on Salmonella typhimurium strains TA98,
TA100 and turned out as negative. Results from
studies carried out in laboratory animals showed
a weak mutagenic activity of anethole.
The genotoxic risk 4 related to estragole is not
considered to be relevant in the specified
conditions of use due to the small amount
present in herbal infusions prepared from fennel.
6. PHARMACEUTICAL PARTICULARS
Well-established use
Traditional use
Not applicable.
7. DATE OF COMPILATION / LAST REVISION
5 July 2007
4 Please refer to the HMPC ‘Public statement on the use of herbal medicinal products containing estragole’
(EMEA/HMPC/137212/2005).
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Assessment Report
Assessment Report
FOENICULUM VULGARE MILLER (bitter fennel, sweet fennel)
Botanical species
Foeniculum vulgare Miller subsp.
and variety
vulgare var. vulgare (bitter fennel)
Foeniculum vulgare Miller subsp.
vulgare var. dulce (Miller) Thellung
Botanical family
Apiaceae (Umbelliferae)
Botanical synonyms
Anethum foeniculum L.
Foeniculum capillaceum Gilib.
Foeniculum officinale All.
Common names
Fennel
(English)
Venkel
(Dutch)
Fenkoli
(Finnish)
Fenouil
(French)
Fenchel
(German)
Finocchio amaro (o selvatico)
dolce (o romano)
(Italian)
Fennikel
(Norwegian)
Fankal
(Swedish)
Part of the plant
Fruit (whole cremocarp and mericarp)
Pharmaceutical preparations
Herbal substance or herbal preparations in solid or
liquid dosage forms or as a herbal tea for oral use
Rapporteurs
Prof. Vittorio Silano
Assessors
Prof. Vittorio Silano
Prof. Gioacchino Calapai
Dr. Marisa Delbò
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(sweet fennel)
Hinojo
(Spanish)
Dr. Marisa Delbò
TABLE OF CONTENTS
I. Introduction
page 4
II.1. Phyto-chemical characterization
“ 5
II.2 Absorption, metabolism and excretion
“ 6
II.3. Pharmacodynamics
“ 7
II.3.1 Mode of action
“ 7
Spasmolytic effect on contracted smooth muscles
“ 7
Antiinflammatory effect
“ 7
Secretolytic and expectorant effects
“ 7
Estrogenic effects
“ 8
Antimicrobial effect
“ 10
Anti-tumour effect
“ 10
Hepato-protective effect
“ 10
Hypotensive effect
“ 10
Hypoglycemic effect
“ 10
Local anaesthetic activity
“ 10
Other effects
“ 10
III.1 Preparations marketed in Europe
“ 11
III.2Posology, duration of use, method of administration
“ 12
III.3 Clinical studies
“ 13
III.4 Clinical studies in special populations
“ 13
III.4.1 Use in children
“ 13
III.4.2 Use during pregnancy and lactation
14
III.5 Traditional use
“ 15
IV. Safety
“ 16
IV.1 Genotoxic and carcinogenic risk
“ 16
IV.1.1 Preclinical data
“ 16
Mutagenicity and carcinogenicity
“ 16
Anethole
“ 16
Estragole
“ 17
IV.1.2. Clinical data
“ 18
IV.1.3 Conclusion
“ 18
Antitumour activity of anethole
“ 18
Antioxydant activity of fennel extracts
“ 19
IV.2.1 Acute toxicity
“ 19
IV.2.2 Subchronic toxicity
“ 20
IV.2.3 Reproductive toxicity
“ 20
IV.3 Contraindications
“ 21
IV.4 Special warnings and precautions for use
“ 21
IV.5 Undesirable effects
“ 21
IV.6 Interactions
“ 21
IV.7 verdose
“ 22
V. verall Conclusion
“ 22
Community herbal monographs
Annex
Community list entries
Annex
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II.Clinical Pharmacology
“ 5
II.3.2 Other studies
8
III Clinical efficacy
“ 11
Conclusion
“ 18
IV.2. Toxicity
“ 19
References
Annex
I. Introduction
This assessment report reviews the available scientific data for bitter fennel and sweet fennel (i.e.
Foeniculum vulgare Miller sp . vulgare var . vulgare and Foeniculum vulgare Miller sp. vulgare
var . dulce ( Miller ) Thellung, respectively) and particularly clinical data. Bitter and sweet fennels
belong to the Apiaceae botanical family and to the capillaceum botanical subspecies. The material
of interest for medicinal use is the fruit (i.e. whole cremocarp and mericarp), sweet fennel being
more broadly used. This herbal substance is administered after crushing in solid or liquid dosages
(Niesel, 1992). The essential oil obtained by steam distillation from the dry ripe fruits is also used.
In preparing this report, a number of data sources were reviewed. The main ones are as follows:
The ESCOP monographs published in 2003;
The results of a literature search carried out in mid 2005 by the Italian National Institute of
Health in Pubmed;
The results of a data search carried out in mid 2005 by the Italian National Institute of
Health in several electronic archives (i.e. Napralert, Caplus, Dart, Toxcenter, Embase and
Medline);
The bibliographic references made available by the Association of the European Self-
Medication Industry (AESGP) at the end of 2005;
The monographs of “ Foeniculi amari fructus ”, of “ Foeniculi dulcis fructus ” and of “ Bitter-
fennel fruit oil ” present in the current (5 th edition) of the European Pharmacopoeia and of
sweet-fennel fruit oil (“ Foeniculi aetheroleum ”) in the Italian Pharmacopoeia (XI Ed.);
The Council of Europe monograph on Foeniculum vulgare as a cosmetic ingredient (2002);
The monograph on Foeniculum vulgare Mill. published in Teuscher et al. (2005);
The results of a data search carried out at the end of 2005 on Micromedex (including
Martindale, Drugdex, Posindex, Altmedex, Reprotox, Herbal Medicines: A Guide for Health-
Care Professionals);
The results of a data search carried out at the end of 2005 on phytovigilance data banks
available on internet (i.e. www/farmacovigilanza.org;
The result of the update in literature search carried out in Pubmed until the end of June 2007
by the Department of Clinical and Experimental Medicine and Pharmacology of Messina
University.
Fennel crushed fruits as infusions, tincture, syrups and honey are traditionally used (see section
III.5 Traditional use) for the treatment of a variety of symptoms including:
Dyspeptic complaints, a broad range of adverse symptoms including, among others,
spasmodic ailments involving altered functional motility of local smooth muscles induced by
anomalous hormonal secretions, Helicobacter infections, stress and psychological
disturbances and other idiopathic causes;
Bloating and flatulence, symptoms associated with an altered composition of intestinal flora
mainly caused by food borne infections or physiological alterations causing a slowing down
of the intestinal content transit;
Infantile colic, a self-limiting condition caused by immaturity of gastro-intestinal tract
resulting in excessive gas formation and intestinal cramping due to contractions of smooth
muscular layers;
Primary dysmenorrhea, a condition associated with ovulatory cycles, caused by myometrial
contractions induced by prostaglandins originating in secretory endometrium, which results
in uterine ischemia and pain; and
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Catarrh, an excessive secretion of epithelial cells due to respiratory tract infections generally
also inducing prostaglandin-mediated bronchoconstriction; this secretion, cleared by
pneumocyte cilia, consists mainly of flaked away epithelial cells, micro-organisms and
mononuclear cells.
These uses are substantiated mainly by empirical data deriving from investigations carried out
into the constituents and their pharmacology, while only poor clinical data are available.
II. Clinical Pharmacology
II.1.Phyto-chemical characterization
Bitter fennel is characterized by a content of essential oil not lower than 40 ml per kg anhydrous
fruit, whereas sweet fennel only contains not less than 20 ml of essential oil per kg anhydrous
fruit.
The oil in bitter fennel fruits has been reported to contain not less than 60% anethole and 15%
fenchone and not more than 6% estragole, whereas in sweet fennel fruits the oil contains not less
than 80% anethole (as determined with reference to anethol R that consists of at least 99% trans -
anethole) and not more than 7.5% fenchone and 10% estragole (European Pharmacopoeia,
1/2005:824; European Pharmacopoeia, 1/2005:825; Brand, 1993; Tóth, 1967; Trenkle K 1969,
1971 and 1972). The essential oils of bitter and sweet fennels also contain relatively small
amounts of alpha-pinene, limonene, p-cymene, beta-pinene, beta-myrcene and of a variety of
other compounds (for some examples, see Table 1).
Table 1- Compounds identified in essential oils obtained by steam
distillation from ripe fruits of bitter and sweet fennels
Compound Bitter fennel (+) Sweet fennel (++)
--------------- -------------------- ----------------------
Trans -anethole
55.0-75.0%
79.8-83.1%
Fenchone
12.0-25.0%
4.6%
Estragole
6.0 % (max)
3.9-5.1%
Alpha-pinene
1.0-10.0%
3.6-0.3%
Limonene
0.9-5.0%
2.2-3.8%
Alpha-pinene/Limonene > 1.0
Cis -anethole 0.5% (max)
Anisaldehyde 2.0 (max)
Beta-myrcene 1.4%
(+) Monograph on bitter fennel fruit oil (European Pharmacopeia-5 th Ed)
(++) Monograph on sweet fennel fruit oil (Italian Pharmacopoeia-XI Ed);
Dadalioglu and Evrendilek (2004)
Crushed or powdered fennel fruits gradually lose their volatile constituents upon aging (Czygan,
1989). Teabags examined 30 days after opening showed in general a loss of essential oil ranging
from 4 to 10%; moreover, in these samples a decrease of anethole content and an increase of
anisaldehyde content (considered as the degradation product of the former) was also evident (Bilia
et al., 2002).
Some chemotypes are known for their lower content of trans -anethole (less than 50%), higher
content of fenchone (more than 30%) and higher content of estragole (more than 30%) (Teuscher
et al., 2005).
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The essential oil contents of 10 samples of dry, ripe fennel fruits of different origin, obtained by
hydrodistillation, were analysed by gas chromatography-mass spectrometry (GC-MS); the 16 main
constituents of each sample were identified, trans -anethole, estragole, limonene and fenchone
being the most abundant. The amounts of trans -anethole and estragole were inversely proportional,
so that clear phytochemical differences within the investigated samples were observed (Miraldi,
1999).
A considerable variability among relative proportions of different compounds in fennel fruits has
been observed in relation to the methodology used to extract the essential oil. Table 2 shows the
differences observed among relative amounts of the main components extracted from the same
sample (unknown variety) of fennel fruits by simultaneous distillation–extraction (SDE) or
supercritical fluid extraction (SFE), as analysed by GC-MS.
Table 2 - Relative amounts of main components extracted from fennel fruit by simultaneous
distillation–extraction (SDE) or supercritical fluid extraction (SFE) (+)
Compound
SDE
SFE
Trans -anethole
49.21%
63.80%
Fenchone
19.33%
12.71%
Estragole
25.84%
20.33%
Alpha -pinene
0.62%
0.31%
Limonene +
1,8-cineolo
1.01%
0.87%
Cis -anethole
0.12%
0.10%
Beta -myrcene
0.17%
0.13%
p-Anisaldehyde
1.90%
0.99%
(Diaz-Maroto et al., 2005).
Chemical compositions of volatiles in infusions or microwave decoctions prepared from crushed
fruits or in teas from pre-packaged tea bags or in instant teas may be very different among
themselves and from volatiles obtained by hydro-distillation of crushed fruits (Forster, 1983; Bilia
et al., 2002). Anethole (30-90%) and/or anisaldehyde (0.7-51.0%) were detected in all the samples;
estragole (0.8-4.1%), eugenol (1.5-11.3%) and fenchone (0.5-47.0%) were detected in most
samples (Bilia et al., 2002).
The fennel fruits also contain water-soluble glycosides of monoterpenoid, alkyl and aromatic
compounds (Kitajima et al., 1998) as well as, among other substances, proteins, cellulose, lignin,
pectins, triglycerides containing mainly petrosilinic, oleic and linoleic acids, wax esters, phospholipids,
phytosterols (e.g. beta -sitosterol and stigmasterol), flavonoids, hydroxycoumarins, furanocoumarins
and vitamins (tocopherol and tocotrienol) (Kunzemann and Herrmann, 1977; Zlatanov, 1994; Ivanov
and Aitzetmuller, 1995; Reiter and Brandt, 1985; Council of Europe, 2002).
This AR supports the establishment of individual Community herbal monographs and/or
Community list entries on bitter fennel fruit, sweet fennel fruit and bitter fennel fruit oil that
comply with the European Pharmacopoeia monographs 5 th Ed.
II.2 Absorption, metabolism and excretion
No data available for fennel in human beings or animals.
After oral administration of radioactively-labelled trans -anethole (as the methoxy- 14 C compound) to
5 healthy volunteers at dose levels of 1, 50 and 250 mg on separate occasions, it was rapidly absorbed.
54-69% of the dose (detected as 14 C) was eliminated in the urine and 13-17% in exhaled carbon
dioxide; none was detected in the faeces. The bulk of elimination occurred within 8 hours and,
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irrespective of the dose level, the principal metabolite (more than 90% of urinary 14 C) was 4-
methoxyhippuric acid (Caldwell and Sutton, 1988). Trans-anethole is metabolized in part to the
inactive metabolite 4-methoxybenzoic acid (Schulz et al., 1998). An earlier study with 2 healthy
subjects taking 1 mg of trans -anethole gave similar results (Sangster et al., 1987).
In mice and rats trans -anethole is reported to be metabolized by O-demethylation and by oxidative
transformation of the C3-side chain. After low doses (0.05 and 5 mg/kg body weight (b.w.)) O-
demethylation occurred predominantly, whereas higher doses (up to 1,500 mg/kg b.w.) gave rise to
higher yields of oxygenated metabolites (Sangster et al., 1984a and 1984b).
II.3. Pharmacodynamics
II.3.1 Mode of action
The medicinal use of fennel is largely due to antispasmodic, secretolytic, secretomotor and
antibacterial effects of its essential oil.
Spasmolytic effect on contracted smooth muscles
Fennel fruit alcoholic extracts and oil exerted a relaxing effect on in vitro pre-contracted smooth
muscles from different organs (tracheal, ileal and uterine) by antagonizing several contraction-
inducing agents.
The relaxant effect of fennel aqueous extract, ethanolic extract and essential oil on methacholine
pre-contracted isolated tracheal chains of guinea pig was studied by Boskabady and Kathami
(2003) and by Boskabady et al. (2004). A bronchodilatory effect of the fennel ethanolic extract
and essential oil was detected, possibly partly due to a potassium channel opening effect, whereas
no relaxant effect was detected in the fennel aqueous extract.
Fennel oil significantly and dose-dependently reduced the intensity of oxytocin-induced contractions
(p<0.01 at 50 μg/ml) and PGE 2 -induced contractions (p<0.01 at 10 and 20 μg/ml) of the isolated
rat uterus. The oil also reduced the frequency of contractions induced by PGE 2 (but not by
oxytocin) (Ostad et al., 2001).
A 30%-ethanolic extract from bitter fennel produced a concentration-dependent decrease in
acetylcholine-and histamine-induced contractility of isolated guinea pig ileum at concentrations of
2.5-10 ml/litre; however, taking into account the effect of ethanol, only the results with histamine
were significant (p<0.005 at 10 ml/litre) (Forster et al., 1980). In the same test system, the extract at
2.5 and 10 ml/litre also concentration-dependently reduced carbachol-induced contractility (Forster,
1983). Fennel essential oil was also reported, at a concentration of 10 mg/ml, to antagonize the
action of acethylcoline, pilocarpine, physostigmine or of barium chloride on intestinal jejunum
isolated from different animals (quoted by Teuscher at al., 2005).
Fennel essential oil (5 to 25 ml of distillate administered to dogs by means of a catheter inserted
into an intestinal fistula) (Plant and Miller, 1926) and anethole (10 to 25 ml/l of physiological
solution in which an isolated mouse intestinal jejunum is plunged) (Imaseki et al., 1962) induced
intestinal motility at low concentrations, but an intestinal relaxation was observed at
concentrations higher than 50 mg/l.
Anti-inflammatory effect
Oral pre-treatment of rats with a dry 80%-ethanolic extract from sweet fennel at 100 mg/kg b.w.
inhibited carrageenan-induced paw oedema by 36% (p<0.01) compared to 45% inhibition by
indometacin at 5 mg/kg (Mascolo et al., 1987).
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Secretolytic and expectorant effects
Anethole and fenchone vapour were given by inhalation to urethanized rabbits as doses of 1 to 243
mg/kg b.w. added to the steam vaporizer (the amount actually absorbed by the animals being
considerably less, estimated as not more than 1% of that added to the vaporizer). Inhalation of
anethole did not affect the volume but produced a dose-dependent (1-9 mg/kg) decrease in the
specific gravity of respiratory tract fluid. Inhalation of fenchone produced a dose-dependent (1-9
mg/kg) augmentation of the volume output of respiratory tract fluid and a dose-dependent (1-27
mg/kg) decline in its specific gravity (Boyd and Sheppard, 1971).
An increase of about 12% in mucociliary transport velocity was observed in isolated ciliated
epithelium from the frog oesophagus 90 seconds after application of 200 µl of an infusion from
bitter fennel (4.6 g per 100 ml of water) (Müller-Limmroth and Fröhlich, 1980).
Fennel aqueous extracts, in a concentration of 10% weight/volume, increased gastric acid
secretion in the stomach of anesthetized rats from the basal level of 0.12 to 0.42 ml (p<0.02). It
has been shown that fennel increases gastric acid secretion. An experiment showed that following
administration of an fennel aqueous extract, the increase in acid production in aspirin-injured
stomachs compared to that in healthy stomachs was markedly reduced, leading to the conclusion
that gastric stimulation requires a healthy, intact gastric mucosa (Vasudevan et al., 2000).
Thirty-eight women affected by idiopathic hirsutism were treated, in a double-blind placebo
controlled study, for 12 weeks, twice a day, on their face with a cream containing 2%, 1% or 0%
of fennel fruit extract obtained with ethanol in a Soxhlet apparatus for 5 hours. In both treatment
groups (and more in the 2% fennel fruit extract), a significant reduction in facial hair growth and
diameter was observed (Javidnia et al., 2003).
Subacute oral administration of an acetonic extract from fennel to adult female ovarectomized rats at
0.5-2.5 mg/kg b.w./day caused dose-dependent estrogenic effects: induction of the estrus phase
(after 10 days, in 40% of rats at 0.5 mg/kg, in 100% at 2.5 mg/kg), increase in mammary gland
weight (p<0.05 at 0.5 mg/kg, p<0.01 at 2.5 mg/kg) and increase in weights of endometrium, cervix
and vagina (p<0.01 to p<0.001 at 2.5 mg/kg). Estrogenic effects were also evident in mature male
rats after treatment with the extract at 1.5 or 2.5 mg/kg b.w./day for 15 days: no significant change
in body or organ weights but, particularly at the higher dose, significant changes in protein and
acid and alkaline phosphatase in the testes, vas deferens, seminal vesicles and prostate (Malini et
al., 1985). An increased weight of mammal glands was also observed following administration of
the fennel extract to non-ovarectomized rats (quoted by Teuscher al., 2005).
Trans -anethole administered orally to immature female rats at 80 mg/kg b.w. for 3 days
significantly increased uterine weight to 2 g/kg compared to 0.5 g/kg in controls and 3 g/kg in
animals given estradiol valerate subcutaneously at 0.1 µg/rat/day (p<0.001). The results confirmed
that trans- anethole has estrogenic activity; other experiments showed that it has no anti-estrogenic,
progestational, anti-progestational, androgenic or anti-androgenic activity (Dhar, 1995).
Estrogenic activity of trans -anethole at high concentrations has been determined by a sensitive
and specific bioassay using recombinant yeast cells expressing the human estrogen receptor
(Howes et al., 2002).
Antimicrobial effect
Fennel fruit extracts and oil as well as some oil components, exhibited in vitro strong inhibitory
activities against the growth of a wide spectrum of bacteria and fungi known to be pathogenic for
man and other species.
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Estrogenic effects
Acetone, n-butanol, ethanol and ether extracts of fennel inhibited the growth of a range of bacteria
including Escherichia coli and Staphylococcus aureus , and also exhibited antifungal activity against
Candida albicans and other organisms (Maruzzella et al., 1959).
Fennel oil inhibited the growth of Escherichia coli (Minimal inhibitory concentration (MIC): 0.5%
V/V), Staphylococcus aureus (MIC: 0.25%), Salmonella typhimurium (MIC: 1.0%) and Candida
albicans (MIC: 0.5%) using the agar dilution method (Hammer et al, 1999). Significant
antibacterial activity of the oil (10 μl of undiluted oil added to wells in the agar plates) was
demonstrated against Brevibacterium linens, Clostridium perfringens, Leuconostoc cremoris and
Staphylococcus aureus (Ruberto et al., 2000) . Earlier studies also demonstrated the antibacterial
activity of the oil (Afzal and Akhtar, 1981, Ramadan et al., 1972).
In vitro growth of Candida albicans strain ATCC 10261 was inhibited by fennel essential oil
(Ezzat, 2001).
Bactericidal activities of a number of plant essential oils, including fennel fruit oil, and of their
isolated constituents were tested against Campylobacter jejuni, Escherichia coli , Listeria
monocytogenes and Salmonella enterica (Friedman et al., 2002) . Fennel fruit oil was shown to
reduce bacterial activity of all tested bacteria ( C. jejuni > S. enterica > E. coli > L.
monocytogene s). As far as the antibacterial activity of isolated compounds is concerned, estragole
had an inhibitory pattern close to that of the fennel oil; limonene showed an inhibitory activity only
on C. jejuni and L. monocytogenes and trans -anethole only inhibited C. jejuni.
An essential oil, extracted by hydro-distillation of bitter fennel crushed fruits and containing as
major components 59% trans -anethole,15% limonene and 12.6% fenchone, was tested in vitro for
antibacterial activity against 27 different phytopathogenic bacterial species and 2 mycopathogenic
ones (Lo Cantore, 2004). An antibacterial activity of the oil was detected against several gram-
negative bacteria (i.e. Pseudomonas syringae pv. atrofaciens and pv. glycinae, P. tolaasil, Erwinia
carotovora subsp. carotovora and subsp, atroseptica, Agrobacterium tumefaciens, Burkholderia
gladioli pv. agaricicola, Xanthomonas campestris pv. phaseoli, pv. phaseoli var. fuscans pv.
vesicatoria and pv. campestris) as well as against a few gram-positive bacteria (i.e. Clavibacter
michiganensis subsp. michiganensis and subsp. sepedonicus and Rhodococcus fascians ). The
antibacterial activity of the fennel oil against the tested strains was much lower (generally below
1/1,000) than that of purified rifampicin.
Essential oil, extracted by steam distillation from fennel fruits and containing 83% trans -anethole,
2.6% p-anisaldehyde, 0.94% carvone, 5.12% estragole, 1.23% alpha-tujone, 3.77% limonene and
0.27% alpha-pinene, showed, when applied in vitro at concentrations between 5 and 80 μl/ml,
significant inhibitory effects on several foodborne bacteria ( Salmonella typhymurium >
Escherichia coli O157:H7 > Listeria monocytogenes > Staphylococcus aureus) (Dadalioglu and
Evrendilek, 2004) .
Growth of 4 Streptococcus strains (i.e. KCTC 3065, NHS 1DD, UBF GTFC, and GS-5) was
inhibited completely by an in vitro concentration of 80 ppm of fennel oil containing about 78%
trans -anethole and minor amounts of limonene, estragole and fenchone. As a similar inhibition of
the growth of the above mentioned Streptococcus strains by 70 ppm of trans -anethole was
observed, it was concluded that trans -anethole was responsible for the antibacterial activity of
fennel oil (Park et al., 2004).
The essential oils of anise (500 ppm), fennel (2,000 ppm) and other olants showed a dose-
dependent inhibitory effect on the growth of tested fungi including Aspergillus flavus, A.
parasiticus, A. ochraceus and Fusarium moniliformis (Farag et al., 1989; Hasan, 1994; Soher,
1999; Soliman and Badeaa, 2002).
The aniseed and fennel oils were found to have a high antibacterial activity against Staphylococcus
aureus (responsible for bases, sepses and skin infections), Streptococcus haemoliticus (causing
infection of the throat and nose) , Bacillus subtilis (infection in immunecompromised patients) ,
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Pseudomonas aeruginosa (causing hospital acquired infection) , Escherichia coli (responsible for
urogenital tract infections and diarrhoea) , Klebsella species and Proteus vulgaris (Singh et al.,
2002).
II.3.2 Other studies
Anti-tumour effect
See section IV.1.1. Preclinical data
Hepatoprotective effect
The hepatoprotective activity of steam distilled essential oil from fennel fruit was studied by
Ozbek et al. (2003a) by using the carbon tetrachloride induced acute liver injury model in rats.
When simultaneously administered with carbon tetrachloride, the fennel oil significantly reduced
hepatotoxicity as shown by the decreased levels (p<0.01) of serum aspartate amino-transferase,
alanine aminotransferase, alkaline phosphatase and bilirubin.
These results were confirmed by Ozbek et al. (2004) with a steam distilled essential oil from
fennel fruit (main components: trans -anethole 74.8%; limonene 11.1%; eugenol 4.7%; fenchone
2.5%; alpha-pinene 1.3% and beta-ocimene 1.2%) administered to rats a few times a week for
seven weeks, evaluating the above-mentioned biochemical markers as well as rat body weight and
liver histopathology.
No such activity was detected by Ozbek et al. (2003b) in the diethyl ether extract obtained by
maceration of fennel fruit for two hours, separation of the liquid phase and evaporation of the
solvent (so-called ‘fixed fennel oil’).
Hypotensive effect
A lyophilized aqueous extract of fennel administered orally at 190 mg/kg b.w. (equivalent to
crude herbal substance at 1,000 mg/kg) for 5 days significantly lowered the systolic blood
pressure of spontaneously hypertensive (SH) rats (p<0.05), but had no effect on normotensive rats.
The extract also significantly increased the urine output of SH rats, by 80% at day 3 (p<0.05), and
increased renal excretion of sodium and potassium (p<0.05), suggesting that fennel acts mainly as a
diuretic and natriuretic in the SH rats (El Bardai et al., 2001).
A hypoglycemic effect was observed in alloxan-induced diabetic mice treated with steam distilled
fennel essential oil, but not with fixed fennel oil (Ozbek, 2002; Ozbek et al., 2003b).
Trans -anethole concentration-dependently reduced electrically-evoked contractions of rat phrenic
nerve-hemidiaphragm, by 10.3% at 10 -3 μg/ml, by 43.9% at 10 -2 μg/ml, by 79.7% at 10 -1 μg/ml
and by 100% at 1 μg/ml (Ghelardini et al., 2001).
In the rabbit conjunctival reflex test, solutions of trans -anethole admistered into the conjunctival
sac increased concentration-dependently the number of stimuli required to evoke the conjunctival
reflex (p<0.001); the effect was comparable to that of procaine (Ghelardini et al., 2001).
Other effects
Fennel essential oil had a spasmogenic effect on smooth muscle of isolated guinea-pig ileum at a
concentration of 8 x 10 -5 g/ml. On a skeletal muscle preparation of isolated rat phrenic nerve
diaphragm, it caused contracture and inhibition of the twitch response to nerve stimulation at a
concentration of 2 x 10 -4 g/ml (Lis-Balchin and Hart, 1997).
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Hypoglycemic effect
Local anaesthetic activity
Anethole was reported to have a contractile effect on smooth muscle (Reiter and Brandt, 1985).
It was also reported to increase the pentobarbital-induced sleeping time in mice (Marcus and
Lichtenstein, 1982).
Addition of 0.5% of fennel to the diet of rats for 6 weeks shortened food transit time by 12%
(p<0.05) (Platel and Srinivasan, 2001). Fennel oil increased the pentobarbital-induced sleeping
time in mice following simultaneous intra-peritoneal (i.p.) administration (Marcus and
Liechtenstein, 1982).
Fennel administered orally at 24 mg/kg b.w. increased spontaneous movement of the stomach in
unanaesthetized rabbits and reduced the inhibition of stomach movement induced by sodium
pentobarbitone (Niiho et al., 1977).
An aqueous extract of fennel (10% w/v), perfused through the stomach of anaesthetized rats at
0.15 ml/minute and collected over periods of 20 minutes, significantly increased gastric acid
secretion (p<0.02) to more than 3-fold compared to the basal secretion determined from perfusion of
saline solution (Vasudevan et al., 2000).
III. Clinical efficacy
III.1 Preparations marketed in Europe
Herbal teas
Fennel fruit, sweet ( Fructus Foeniculi , Species) is marketed in Latvia since 1970 with the
following indications: Orally as a carminative, for gastrointestinal disorders and spasms, as
galactagogue increases breast-milk production, may be taken as a mild expectorant. For children
as an infusion can be given for colic and as carminative (ATC code: V03 AX).
Daily dosage: 5.0-7.0 g crude drug or equivalent preparations as an infusion. Infusion: pour 180
ml of hot water over a tablespoon (~ 5.0 g) of the fruits, allow them to stand for 20 minutes, then
remove the fruits with a strainer. ½ cup of the freshly prepared infusion is drunk 2-3 times daily
before eating. For children aged up to 4 years daily dose is 1 teaspoon, for children aged 4 to 10
years – 1 dessertspoon of the fruits.
Sweet fennel herbal tea is authorised in France since February 1990, traditionally used in the
symptomatic treatment of digestive upsets such as epigastric distension, slow digestion, eructation,
flatulence, with the following posology: 1.8 g 2 to 3 times daily.
In Germany the authorised indications since 1996 for bitter fennel herbal tea are: symptomatic
treatment of dyspeptic complaints such as minor gastrointestinal spasms, repletion and flatulence.
For the relief of symptoms in coughs and colds with viscous mucilage. Posology: 2.5 g herbal
substance/150 ml water 2-3 daily.
The indications authorised in Austria for the herbal tea are the following:
Dyspeptic complaints such as mild, spasmodic gastro-intestinal ailments, anorexia, bloating and
flatulence. Effect on hormones such as stimulating milk production. Catarrh of the upper
respiratory tract, cough (expectorant)
Posology: Adult daily dose: 5-7 g of crushed fruits as an infusion or similar preparation.
Children, average daily dose: 0-1 year of age: 1-2 g of crushed fruits as an infusion; 1-4 years of
age: 1.5 - 3 g; 4-10 years of age: 3-5 g; 10-16 years of age: the adult dose.
Herbal tea is also authorised in the Czech Republic as an adjuvant in mild gastrointestinal
complaints such as bloating, flatulence and minor spasms and in catarrhs of the upper respiratory
tract; posology: 1.5 g poured with 0.25 l of boiling water (extracted for 15 minutes) three times
daily (no restrictions).
In Poland herbal tea has been traditionally used over 30 years in digestive disorders, spastic
complaints, feeling of fullness and flatulence, as spasmolytic and cholagogic. It is also used as
expectorant in inflammations of upper respiratory tract and in lactagogue mixtures. Posology:
Infusion made of 1 teaspoon of fruits in a glass of boiling water. Drink 1/3 – 1/2 of portion 3 – 2
times a day. For children in single doses of one teaspoon. Not abuse during pregnancy and
lactation.
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Fennel powder
Hard capsules containing sweet fennel powder are authorised in France since November 1990
with the following indications:
- Traditionally used in the symptomatic treatment of digestive upsets such as: epigastric
distension, slow digestion, eructation, flatulence.
- Traditionally used as an adjuvant treatment for the painful component of functional digestive
disorders.
Posology: 390 mg 3 times a day (if necessary: until 1,950 mg daily)
Bitter Fennel fruit oil
Bitter fennel fruit oil is authorised as a syrup in Germany since 1978 for the relief of symptoms in
coughs and colds with viscous mucilage in children over one year. Posology: 3 times daily 1 cup,
equivalent 0.003 g fennel oil
No authorised/registered products are on the market in the following European countries:
Belgium, Ireland, Italy, The Netherlands, Portugal, Finland and Norway.
Various fixed combinations containing fennel are authorised/registered in different European
countries.
Food supplements containing fennel are on the market.
III.2 Posology, duration of use, method of administration
Posology
There are no dose-finding studies available.
The recommended dosage for adults and children over 12 years of age is supported by clinical
experience and expert opinions (Brand, 1993; Czygan and Hiller, 2002; Dorsch et al., 2002;
Leclerc, 1983; Valnet, 1990).
Fennel fruit (Blumenthal et al., 1998) :
Adult and children over 12 years:
5-7 g of crushed fennel fruits as single dose per day or in multiple divided doses as a herbal tea or
similar preparations.
Fennel tincture (Blumenthal et al., 2000): 5 to 7.5 ml two to three times daily
Fennel oil (Blumenthal et al., 1998): 0.2 ml essential oil, as single dose per day or in multiple
divided doses .
The use in the paediatric age (see section III.4.1 Use in children) is not recommended for the
presence of estragole, whose exposure should be minimised in young children.
The posology recommended by the HMPC per age category and in the different indications can be
found in the corresponding Community herbal monographs/Community list entries.
Duration of use
Unless otherwise advised by a physician or pharmacist, one should not consume fennel oil for an
extended period (several weeks) (Blumenthal et al., 1998).
Because of the poor evidence of clinical trials, considering the lack of available safety data on long-
term use of fennel preparations and due to the potential toxicity of trans -anethole and estragole, a
limit of two weeks is consistent with a self-medication indication, which is the case for traditional
herbal medicinal products.
If the symptoms persist during the use of the medicinal product, a doctor or a qualified health care
practitioner should be consulted.
Method of administration : Oral use.
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III.3 Clinical studies
Primary dysmenorrhoea
Primary dysmenorrhoea, a condition associated with ovulatory cycle, is due to myometrial
contractions induced by prostaglandins originating in secretory endometrium, which results in
pain. Intensity of pain of thirty patients with moderate to severe dysmenorrhoea was recorded by
using a linear analog technique for 5 days in three consecutive cycles (first cycle: no treatment;
second cycle: treatment with mefenamic acid-250 mg q6h, orally; third cycle: treatment with a 2%
fennel oil obtained by steam distillation of dried fruit-25 drops q4h, orally) (Jahromi et al., 2003).
Although the study was not blinded and the sample tested was small, the results obtained suggest
that both treatments effectively (p<0.001) reduced menstrual pain as compared to the control
cycle, mefenamic acid being more active than fennel oil. However, five cases, representing 16.6%
of all treated cases, withdrew from the study due to fennel’s odour and one subject reported a mild
increase in the amount of menstrual flow during the fennel treated cycle.
Conclusion
Investigations available in human beings on the role of fennel in reducing pain in primary
dysmenorrhoeal are very preliminary. However, the likelihood of the postulated effect is
considerably increased by several in vitro studies showing that fennel fruit alcoholic extracts and
oil exerted a relaxing effect on in vitro pre-contracted smooth muscles from tracheal, ileal and
uterine tissues by antagonizing several contraction- inducing agents.
III.4 Clinical studies in special populations
III.4.1 Use in children
Anti-colic effect
The efficacy of fennel tea for treating infantile colic was addressed by Weizman et al. (1993).
A randomised, placebo-controlled study, carried out on 121 (62 in the treated group and 59 in the
control group) infants between 2 to 12 weeks of age, suggested that an oral administration for
7 days of a 0.1% fennel seed oil emulsion in water (corresponding to about 12 mg/kg b.w. and
day) is significantly superior (p<0.01) to placebo in decreasing intensity of infantile colic.
Relief of colic symptoms was assessed as a decrease of cumulative crying to less than 9 hours per
week. No side effects were noted in the treated infants with colic (Alexandrovich et al., 2003). As
the postulated mechanism in the pathogenesis of colic is a spasm of the intestinal smooth muscles,
the therapeutic effect of fennel fruit oil was interpreted as possibly secondary to a spasmolytic
action.
A randomised, double-blind, placebo-controlled trial was carried out to investigate the
effectiveness and side effects of a phytotherapeutic agent based on enpowdered extracts of
Matricariae recutita L . , Foeniculum vulgare M. var dulce and Melissa officinalis L. in the
treatment of 93 breastfed colicky infants. The results showed that colicky infants treated with the
extract improved within 1 week of treatment (Savino F et al., 2005).
Iten and Saller in 2004 published a comment to the statement of the German 'Bundesinstitut für
gesundheitlichen Verbraucherschutz und Veterinärmedizin' (BgVV, May 2001), where consumers
are advised to reduce their intake of foods or fruits containing estragole for reasons of health. The
crucial points of criticism concerned the transfer of data obtained in animal models to the human
situation as well as the high doses of the applied monosubstance and difference in estragole
metabolism between mice and men. The authors concluded admitting the lack of epidemiological
and clinical studies on use of fennel tea but, at the same time, declared that in their opinion the
probability of a serious cancerogenic potential risk connected with the consumption of fennel tea
seems to be negligibly small.
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Conclusion
Investigations available in human beings on the role of fennel in reducing pain in infantile colic
are very preliminary. However, the likelihood of the postulated effect is considerably increased by
several in vitro studies showing that fennel fruit alcoholic extracts and oil exerted a relaxing effect
on in vitro pre-contracted smooth muscles from tracheal, ileal and uterine tissues by antagonizing
several contraction-inducing agents.
The missing data cannot be extrapolated from the use in adults and available data cannot be accepted
for supporting the use in children for safety reasons, on the basis of Eur. Ph requirements for the
content of estragole (no more than 5.0% in bitter fennel and no more than 10.0 % in sweet fennel).
Considering that even authors, who are in favour of the use of fennel without limits in children admit
the lack of epidemiological studies (the type of studies that could give more information on safety),
according to the recommendations of the HMPC ‘Public statement on the use of herbal medicinal
products containing estragole’, “the exposure of estragole to sensitive groups such young children,
pregnant and breastfeeding women should be minimised.”
The use of fennel oil in children and adolescents under 18 years of age is therefore contraindicated
(lack of data and presence of estragole).
The prescription of fennel tea in infants and children under 4 years of age should be restricted to
the paediatrician and no general recommendation for the use without any medical advice should be
given.
The indicative average daily dose for symptomatic treatment of mild, spasmodic gastro-intestinal
complaints including bloating, and flatulence coming from the traditional use in Austria may be
the following:
3 months-1 year of age: 1-2 g of comminuted fruits as an infusion
1-4 years of age: 1.5-3 g of comminuted fruits as an infusion.
In children between 4 and 12 years of age, with the aim to minimise the exposure to estragole, a
short-term use (less than one week) of fennel tea in mild transitory symptoms according to the
traditional Austrian posology is considered acceptable: 3-5 g of comminuted fruits, in three
divided doses.
III.4.2 Use during pregnancy and lactation
There are no clinical studies available.
According to Madaus (1938), fennel oil produces an excitation of the gravid uterus and can lead to
abortion. An estrogenic activity (see section II.3.1) and anti-fertility and foetal cell toxicity effects
(see section IV.2) have been shown for fennel oil and trans -anethole in rats.
Moreover, a descriptive retrospective survey on 86 consultations due to ingestion of herbal
infusion with abortive intent received at the Toxicological Information and Advisory Centre of
Montevideo between 1986 and 1999 (Ciganda and Laborde, 2001) indicated that multi-systemic
failure was found in those patients that had taken Ruta only and Ruta together with parsley and
fennel. Death occurred in four patients, who had ingested Ruta (two cases Ruta alone and two
cases Ruta with parsley and fennel).
In view of the above-mentioned data, as a precautionary measure, the use of fennel oil and
alcoholic extracts is not recommended during pregnancy and lactation.
Despite the fact that the European Scientific Cooperative on Phytotherapy reports that the herbal
substance and preparations of fennel at the recommended dosage may be used during pregnancy
and lactation (ESCOP, 2003), no data are available in relation to the use of fennel during pregnancy
and lactation at the recommended dosages. According to the recommendations of the HMPC ‘Public
statement on the use of herbal medicinal products containing estragole’, “the exposure of estragole
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to sensitive groups such young children, pregnant and breastfeeding women should be
minimised.”
It is unknown if fennel constituents are excreted in human breast milk.
III.5 Traditional use
Anti-asthma and dyspnea effects have been described for fennel in Iranian ancient medical
books (Avesina, 1985). Applications in the treatment of catarrh of the upper respiratory tract has
been described in several handbooks and treaties (Brand et al., 1993; Czygan and Hiller, 2002;
Madaus, 1976; Sweetman, 2002; Merkes, 1980; Weiss, 1997; and Müller-Limmroth and
Fröhlich, 1980).
Fennel fruit has also been reported as useful in the treatment of dyspeptic complaints such as
mild, spasmodic gastro-intestinal ailments, bloating and flatulence (Brand et al., 1993; Czygan
and Hiller, 2002; Madaus, 1976; Schilcher, 1984 and 1986).
Fennel fruit has also been reported to be in use in some areas for many years to relieve painful
menstruation, symptoms of female climacteric and other purposes (Hare et al., 1916; Albert-
Puleo, 1980; Zargari, 1991; Mills et al., 2000; Jahromi et al., 2003).
Fennel fruit (Xiaohuixiang) has been in use for many centuries in Chinese Medicine, generally
as decoction with other herbs (L’Italia Agricola, 1989, Chinese Herbal Medicine 1999, p.203-
204) and the Chinese Herbal Medicine (1999, p.502-503) classifies fennel fruit as being able “to
control gastrointestinal smooth muscle” and to treat “stomach ache”. Fennel fruit (Xiaohuixiang)
is described in the Pharmacopoeia of the People’s Republic of China (English edition, 2005,
Vol. I;) with the action: “to dispel cold and relieve pain, to regulate the stomach function”. The
indications reported in the Chinese Pharmacopoeia are as follows: “it is used for lower
abdominal pain with cold sensation, dysmenorrhoea; distending pain in the epigastrium with
reduced appetite, vomiting and diarrhoea; hydrocele testis”.
For oral use in Traditional Chinese Medicine (TCM) the dosage is 3-6 g per day as a herbal tea
in single or divided doses.
According to the TCM, fennel fruit can be ‘hotted’ and wrapped in a bag (10 grams) for ironing
the lower abdomen to treat abdominal pain of cold type (Liu Gan Zhong et al., 2003).
Fructus Foeniculi processed with salt acts to dispel “cold” from the interior and relieve pain. It
is used for lower abdominal pain with cold sensation, dysmenorrhoea. This magisterial
preparation described in appendix II D of the Chinese Pharmacopoeia, is traditionally prescribed
by physicians when kidneys or renal function are involved.
Otherwise, according to the TCM criteria, fennel fruit should not be taken in the following
conditions:
Internal “Heat” due to Yin Deficit (SATCM 2002)
- Febrile disease with persistent high fever (internal “Heat” in the Qi System) ( Chinese Materia
Medica , TianJin. 2001 )
- Late stage of febrile disease (“Heat” syndrome due to Yin deficiency) (SATCM 2002)
- Acute infections of the gastro – enteric tract (internal “Fire” and toxins) (SATCM 2002)
- Acute inflammation of the gastro – enteric tract such as gastritis, gastric or duodenal ulcer,
irritable bowels disease, etc. (Endogenous “Heat” in Stomach and Intestine) (SATCM 2002)
- Constipation due to dryness (Deficit of body fluid due to Yin Deficiency) (SATCM 2002)
Fennel has been used as lactagogue since antiquity with no side effects reported (Keller, 1992).
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The Treaty “Farmacologia Teorica e Pratica”, also named “Farmacopea Italiana” of Giuseppe
Orosi (1851- Vincenzo Mansi Ed.-Livorno) lists fennel fruit in the Materia Medica Botanica
Chapter (Orosi, 1851).
IV. Safety
IV.1 Genotoxic and carcinogenic risk
IV.1.1 Preclinical data
Mutagenicity and carcinogenicity
Aqueous and methanolic extracts of fennel did not show any mutagenic activity in the Ames test
using Salmonella typhimurium strains TA 98 and TA 100, with or without metabolic activation
(Morimoto et al., 1982; Yamamoto et al., 1982), whereas fennel oil (2.5 mg/plate) was mutagenic
(Marcus and Lichtenstein, 1982). The two extracts showed no activity also in the Bacillus subtilis
rec- ' assay (Morimoto et al., 1982).
Sweet fennel oil was found to be mutagenic in the Bacillus subtilis DNA-repair test (Sekizawa
and Shibamoto, 1982), but fennel oil did not show any activity in the chromosomal aberration
test using a Chinese hamster fibroblast cell line (Ishidate et al., 2000).
Anethole
From a series of studies in mice, Miller et al. (1983) concluded that anethole fed to female CD-1 mice
in the diet or given orally or by i.p. injection to male pre-weaning B6C3F1 mice was not a hepato-
carcinogen; although these studies were not carried out for test animal lifetimes, safrole and estragole
were found to be highly active as liver carcinogens in both these tests.
Another bioassay carried out in Sprague–Dawley (SD) rats, administered 0.25, 0.5, or 1% anethole in
the diet for 121 weeks, showed the occurrence of a small, but statistically significant, incidence of
hepatocellular carcinomas in female rats receiving 1% anethole (Truhaut et al., 1989). These
hepatocellular carcinomas were associated with other histological changes to the liver as those
observed after enzymes inducers (Newberne et al., 1989) and were considered as not caused by a
direct genotoxic effect of trans -anethole (Lin, 1991). Reed et al. (1992) also showed that i.p.
administration of anethole to SD rats increased liver weight, microsomal protein and cytochrome P-
450 content.
In nine Salmonella studies to detect base-pair substitutions or frameshift mutations without
metabolic activation, anethole was uniformly negative and this was also the case in four studies
with activation after careful consideration of all experimental conditions (Heck et al., 1989; Hsia et
al., 1979; Marcus and Liechtenstein, 1982; Mortelmans et al., 1986; Nestmann et al., 1980;
Sekizawa and Shibamoto, 1982; Swanson et al., 1979; To et al., 1982). The four findings suggesting
a weak mutagenic potential of anethole (Marcus and Liechtenstein, 1982; Swanson et al., 1979;
Mortelmans et al., 1986; Sekizawa and Shibamoto, 1982; Lin, 1991) were the result of the use of
non-standard protocols (using longer pre-incubation times, excessive quantities of S-9 protein
and/or the addition of co-factors) and have also been found to be irreproducible (Gorelick, 1995 and
Marshall and Caldwell, 1996).
Anethole was found to be mutagenic in the mouse lymphoma assay which is known for its extreme
sensitivity and poor selectivity for genotoxicity (Gorelik, 1995; Heck et al., 1989; Caldwell, 1993;
Casciano et al., 1992).
Other results showing the absence of mutagenic potential of anethole include assays in Escherichia
coli (Sekizawa and Shibamoto, 1982) and in Saccharomyces cerevisiae (Nestmann and Lee, 1983).
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A mouse micronucleus assay was negative, with no micronuclei found at 6 and 30 hours after
anethole administration (Marzin, 1979). Similarly, in the mouse bone marrow micronucleus test,
oral pre-treatment of mice with trans -anethole at 40-400 mg/kg b.w. 2 and 20 hours before the
administradion of the genotoxins cyclophosphamide, procarbazine, N-methyl-N 7 -nitro-N-
nitrosoguanidine, urethane, ethyl methane sulfonate, no significant increase in genotoxicity was
observed (Abraham, 2001).
Very low levels of DNA adducts were evidenced after administration of anethole to mice, whereas
150 and 220 times as many adducts were detected following administration of safrole and estragole,
respectively (Phillips et al., 1984).
Unscheduled DNA synthesis (UDS) assays in rat hepatocytes did not indicate any mutagenic
potential of anethole (Howes et al., 1990; Muller et al., 1994).
Anethole has three primary metabolites in the rat and the pathway of toxicological concern is that of
epoxidation of the 1,2 double bond at the side chain; in fact, 3’-hydroxylation does not result in
genotoxicity or marked cytotoxicity and O-demethylation is a detoxication reaction (Sangster et al.,
1984a and 1984b; Bounds and Caldwell, 1996). Cytotoxicity of anethole is enhanced when the
cellular epoxide defence mechanisms of conjugation with reduced glutathione and hydration by
cytosolic epoxide hydrolase are severely compromised; however, modulation of epoxide
metabolism by the same mechanism in cultured cells failed to induce UDS by anethole nor was
there a UDS response in hepatocytes of female rats dosed with anethole in vivo (Marshall and
Caldwell, 1996). The synthetic epoxide of anethole was also tested and found to be cytotoxic, but
not genotoxic. The lack of induction of UDS by anethole epoxide provided a further support to the
hypothesis that marginal hepatocarcinogenesis observed in female rats given 1% anethole in the diet
for 121 weeks was not initiated by a genotoxic event (Marshall and Caldwell, 1996).
To date very little is known about the metabolism of trans -anethole by humans. Caldwell’s
research group published two articles on metabolism of trans -anethole in humans, both including
essentially the same experiments (Sangster, Caldwell et al., 1987; Caldwell and Sutton, 1988). The
fundamental conclusion of the authors regarding these experiments is only that “the pattern of
urinary metabolites of trans -anethole is unaffected by dose size”. Any consideration on the risk
influence is lacking. These Caldwell’s experiments show essentially the difference in anethole
metabolism between rodents and humans.
In 1999, the USA Expert Panel of FEMA (Flavour and Extract Manufacturers’ Association) released
a review of scientific data relevant to the safety evaluation of trans -anethole as a flavouring
substance. The review concluded that trans -anethole can be “generally recognised as safe” (GRAS)
at low level of intake (54 μg/kg b.w./day) (Newberne et al., 1999).
In the 51 st meeting of the Joint FAO/WHO Expert Committee on Food Additives (JECFA) a
document on safety evaluation of trans -anethole was prepared; the conclusions were that trans -
anethole and its metabolites are unlikely to be genotoxic in vivo ; the cytotoxic metabolite, anethole
epoxide, was suggested to be the possible causative agent of the hepatotoxic effect observed in pre-
clinical studies in rats. The report of JECFA recommended that the acceptable daily intake (ADI)
should not exceed the dose 2 mg/kg b.w. on the basis of scientific pre-clinical data published on
trans -anethole (JECFA, 1999).
Estragole
Estragole, a minor constituent of fennel oil, has shown its ability to produce genotoxic effects in
bacteria, yeasts and mammalian cells, while no mutagenic activity was observed in Salmonella
typhimurium probably because of the absence of the complex metabolism needed for
bioactivation (EMEA/HMPC, 2005).
It has been shown that estragole and its 1'-hydroxy metabolite caused significant increases in the
incidences of hepatocellular carcinomas in male CD-1 mice that received the compounds by
subcutaneous injection at 1-22 days of age (Drinkwater et al., 1976).
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Estragole or its metabolite, 1’-hydroxyestragole, administered to mice binds readily to DNA and
several DNA adducts have been characterized. Several studies showed the carcinogenic effects of
estragole in mice (mainly malignant liver tumours); moreover, 1’-hydroxyestragole and other
metabolites and synthetic derivatives were shown to be potent carcinogens in mice (Wiseman et
al., 1987; EMEA/HMPC, 2005).
The EMEA/HMPC (2005) assessment is that the profiles of metabolism, metabolic activation and
covalent binding of estragole are dose-dependent and tend to markedly decrease at low levels of
exposure (less than linear decrease with respect to dose); according to this assessment, rodent
studies indicate that these events are probably minimal in the dose range 1-10 mg estragole/kg
b.w., which is approximately 100-1,000 times the anticipated human exposure to this substance
from traditional diet and as added flavouring substance.
The major metabolic pathway of low doses of estragole as established in rats and mice is
O-demethylation with carbon dioxide being the terminal metabolite, but as the dose increases the
proportion of O-demethylation decreases and other pathways, notably 1’-hydroxylation, come
into prominence.
Conclusion
In conclusion, fennel oil extracts were found to be mutagenic in vitro and studies carried out in
laboratory animals showed a weak mutagenic potential of anethole. However, trans -anethole is
reported as “generally recognised as safe” at the intake of 54 μg/kg b.w./day) and the ADI is about
0-2 mg/kg b.w.
Several studies have shown the carcinogenic effects of estragole and some of its metabolites in
mice (mainly malignant liver tumours). The EMEA/HMPC (2005) assessment is that the profiles
of metabolism, metabolic activation and covalent binding of estragole are dose-dependent and
tend markedly to decrease at low levels of exposure. The genotoxic risk related to estragole is not
considered to be relevant for adults in the recommended dosage due to the small amount present in
fennel oil but the risk cannot be calculated with high doses or prolonged use or in young children.
IV.1.2 Clinical data
No data available.
IV.1.3 Conclusion
Anti-tumor activity of anethole
In Swiss albino mice with Ehrlich ascites tumour (EAT) in the paw, anethole administered orally
at 500 or 1,000 mg/kg on alternate days for 60 days significantly and dose-dependently reduced
tumour weight (p<0.05 at 500 mg/kg, p<0.01 at 1,000 mg/kg), tumour volume (p<0.01 at 500
mg/kg, p<0.001 at 1,000 mg/kg) and body weight (p<0.05 to 0.01) compared to EAT-bearing
controls. Mean survival time increased from 54.6 days to 62.2 days (500 mg/kg) and 71.2 days
(1,000 mg/kg). Histopathological changes were comparable to those after treatment with
cyclophosphamide (a standard cytotoxic drug). These and other results demonstrated the anti-
carcinogenic, cytotoxic and non-clastogenic nature of anethole (Al-Harbi et al., 1995).
Anethole at a concentration below 1 mM has been shown to be in vitro a potent inhibitor of
tumour necrosis factor (TNF)-induced cellular responses, such as activation of nuclear factor-
kappa B (NF-κB) and other transcription factors, and also to block TNF-induced activation of the
apoptotic pathway. This might explain the role of anethole in suppression of inflammation and
carcinogenesis (Chainy et al., 2000).
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In the mouse bone marrow micronucleus test, oral pre-treatment of mice with trans -anethole at
40-400 mg/kg b.w. 2 and 20 hours before i.p. injection of genotoxins led to moderate, dose-
dependent protective effects against known genotoxins such as cyclophosphamide, pro-carbazine,
N-methyl-N'-nitrosoguanidine, urethane and ethyl methane sulfonate (p<0.05 to p<0.01 at various
dose levels). No significant increase in genotoxicity was observed when trans -anethole (40-400
mg/kg b.w.) was administered alone (Abraham, 2001).
Antioxidant activity of fennel extracts
The inhibitory effects of some constituents isolated from a methanolic extract of fennel fruit were
investigated on the oxidation of linoleic acid and on the activation of inactive hyaluronidase.
Among the test compounds, six stilbene trimers, miyabenol C, cis -miyabenol C, foeniculoside I,
foeniculoside II, foeniculoside III and foeniculoside IV, exhibited greater antioxidative activities
than butylated hydroxyanisole (BHA). Furthermore, miyabenol C and cis -miyabenol C showed
strong hyaluronidase inhibitory effects (Ono et al., 1997).
Antioxidant activity of fennel oil against lipid peroxidation was demonstrated in the thiobarbituric
acid reactive species assay and in a micellar model system (Ruberto et al., 2000).
The antioxidant activities of fennel fruit aqueous and ethanolic extracts were compared in vitro to
those of standard antioxidants such as BHA, butylated hydroxutoluene and tocopherols in various
antioxidant assays including total antioxidant, free radical scavenging, superoxide anion radical
scavenging, hydrogen peroxide scavenging, metal chelating activities and reducing power (Oktay et
al., 2003). Both fennel extracts showed effective reducing power, free radical scavenging, hydrogen
peroxide scavenging and metal chelating activities.
Antioxidant activity of an aqueous extract from fennel fruit (as evaluated in vitro from amounts
needed for 50% scavenging of superoxide radicals or for 50% inhibition of lipid peroxide or for
5 0% inhibition of hydroxyl radicals) was found to be higher than that of ascorbic acid and
comparable to those of 4 other umbelliferous fruits (Satyanarayana et al., 2004).
Considering the above-mentioned data and all uses of fennel fruit, it is further concluded that
human exposure resulting from short-term use of fennel fruit-based medicinal products,
complying with the above-mentioned specifications, is unlikely to pose any significant cancer
risk.
IV.2. Toxicity
IV.2.1 Acute toxicity
Oral administration of an ethanolic extract of fennel to mice at 0.5, 1 and 3 g/kg b.w. caused no
mortality and no significant difference in body and vital organ weights or in external
morphological, haematological or spermatogenic parameters in comparison with the control
group over a period of 24 hours (Shah et al., 1991).
Values of the oral LD 50 corresponding to 3.8 g/kg b.w. (Opdyke, 1974) and 3.12 g/kg b.w. (von
Skramlik, 1959) had been reported for fennel oil in rats, but in a more recent study the oral LD 50
was estimated to be 1.326 g/kg b.w. (Ostad et al., 2001). In this last study, animals treated with
the highest dose showed prostration, sedation, respiratory distress, movement disorders,
unresponsiveness to external stimulation, hind limb weakness, tremor and fasciculation in dorsal
muscles during the first 24 h from single dose ingestion. In treated animal groups with lower
doses the most evident adverse effect was sedation. In all groups, the amount of 24h urine
increased parallel to the amount of fennel oil administered.
The dermal LD 50 in rabbits was estimated to be higher than 5,000 mg/kg (Opdyke, 1974).
Fennel extracts in high dosages resulted in abnormal movements, tremor, fasciculation and
drowsiness in experimental animals (Ostad et al., 2000).
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Oral LD 50 values per kg b.w. were determined for trans -anethole as 1.8-5 g in mice, 2.1-3.2 g in
rats, and 2.16 g in guinea pigs; i.p. LD 50 values for trans -anethole were determined as 0.65-1.41
g/kg b.w. in mice and 0.9-2.67 g/kg b.w. in rats (Lin, 1991).
Anethole activates the central nervous system and its excessive use may lead to convulsions
(Zagari, 1991).
IV.2.2 Subchronic toxicity
In 90-day experiments in rats, 0.1% of trans -anethole in their diet caused no toxic effects.
However, dose-related oedema of the liver was reported at higher levels of 0.3%, 1% and 3%,
which have no therapeutic value (Lin, 1991).
Male rats receiving 0.25% of anethole in their diet for 1 year showed no toxic effects, while other
receiving 1% for 15 weeks had slight oedematous changes in liver cells (Hagan et al., 1967).
Rats given trans -anethole as 0.2, 0.5, 1 or 2% of their diet for 12-22 months showed no effects at
any level on clinical chemistry, haematology, histopathology or mortality. Slower weight gain and
reduced fat storage were noted at the 1% and 2% levels (Lin, 1991; Le Bourhis, 1973).
Oral administration in drinking water of an ethanolic extract of fennel to mice at 100 mg/kg b.w.
and day for 3 months caused significant body weight gain in male mice and weight loss in females.
Alopecia was observed in 3/10 males, swollen testes in 1/10 males and penile erection in 2/10
males. No toxic symptoms were observed in females. It caused no significant differences in
mortality or in haematological and spermatogenic parameters in comparison with the control group
(Shah et al., 1991).
IV.2.3 Reproductive toxicity
Malini et al. (1985) showed estrogenic activity of the seed extract in both male and female rats.
The protein concentration was found to be significantly decreased in testes and vas deferens and
increased in seminal vesicles and prostate gland, following oral administration of an acetone
extract of Foeniculum vulgare seeds at the doses of 150 μg/kg and 250 μg/kg for 15 days in male
rats. Moreover, the activity of acid and alkaline phosphatase decreased in all these tissues. Only
the alkaline phosphatase was unchanged in vasa. The same doses of the extract, after oral
administration for 10 days in female rats, caused vaginal cornification and estrus cycle. The
lower doses caused increase in weight of mammary glands and the higher doses increased the
weight of oviduct, endometrium, myometrium, cervix and vagina.
Trans -anethole exerted dose-dependent anti-implantation activity after oral administration to adult
female rats on days 1-10 of pregnancy. Compared to control animals (all of which delivered normal
offspring on completion of term), trans -anethole administered at 50, 70 and 80 mg/kg b.w.
inhibited implantation by 33.3%, 66.6% and 100% respectively. Further experiments at the
80 mg/kg dose level showed that in rats given trans -anethole only on days 1-2 of pregnancy normal
implantation and delivery occurred; in those given anethole only on days 3-5, implantation was
completely inhibited; and in those given trans- anethole only on days 6-10, three out of five rats
failed to deliver at term. No gross malformations of offspring were observed in any of the groups.
The results demonstrated that trans -anethole has anti-fertility activity. From comparison with the
days 1-2 group (lack of anti-zygotic activity), the lower level of delivery in the days 6-10 group was
interpreted as a sign of early abortifacient activity (Dhar, 1995).
Ostad et al. (2004) exposed cultivated limb bud cells obtained from day 13 rat embryo to
concentrations of fennel essential oil between 0.0186 and 9.3 mg/ml for 5 days at 37°C.
A significant reduction in the number of stained differentiated foci due to cell loss rather than
decreased cell differentiation was observed in the presence of fennel essential oil. These findings
were interpreted as a toxic effect of fennel essential oil on foetal cells with no evidence of
teratogenicity.
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The body of the data indicates that reproductive system is a target for the action of fennel extracts
and its principal constituent trans -anethole, which may cause changes in male and female organs
and tissues involved directly or indirectly in the reproductive mechanisms. Consequences of these
changes are not easily predictable or detectable in humans. However they cannot definitely be
excluded.
IV.3 Contraindications
Persons with hypersensitivity to the active substance or to Apiaceae (Umbelliferae) (aniseed,
caraway, celery, coriander and dill) or to anethole should avoid the use of fennel preparations and
fennel oil. A cross-allergenicity between fennel and celery has been reported (Stager et al., 1991).
The use of fennel oil in children and adolescents under 18 years of age is contraindicated because
of the lack of data and because of the presence of estragole.
IV.4 Special warnings and precautions for use
The use of fennel tea is not recommended in children under 4 years of age due to the lack of
adequate data and paediatrician advice should be sought.
Preparation with high fennel content (> 7 g of herbal substance) should not be taken for more than
two weeks without medical advice.
If excessive doses are ingested, the estrogenic activity of fennel oil may affect hormone therapy,
including the oral contraception and hormone replacement therapy (see sections IV.6 Interactions
and II.3.1. Mode of action - Estrogenic effects).
Patients should seek medical advice if symptoms persist for more two weeks or worsen upon
administration of the medicinal product.
IV.5 Undesirable effects
Allergic reactions to fennel, affecting the skin or the respiratory system, occur rarely (Levy, 1948;
Schwartz et al., 1997; Blumenthal et al., 1998).
Enzyme immunoassay inhibition studies with one patient’s serum revealed cross-reactivity among
the IgE components deriving from aniseed, fennel, caraway, coriander and dill extracts (Garcia
Gonzalez et al., 2002).
Rare cases of contact dermatitis to anethole containing preparations (Andersen, 1978; Franks,
1998) have been reported.
It has been observed that fennel contains coumarin-derivatives, which competitively can inhibit
vitamin K and may interfere with blood clotting (Shlosberg and Egyed, 1985). No further data are
available.
Fennel contains small amounts of bergapten, a linear furocoumarin that might be responsible for
phototoxicity (Kwon et al., 2002).
IV.6 Interactions
Fennel contains a high amount of minerals, mainly calcium, magnesium, iron, zinc, manganese,
and copper. It has been shown in the rat that co-administration of fennel and ciprofloxacin may
lead to decreased bioavailability of ciprofloxacin in rats due to formation of a ciprofloxacin-cation
complex with possible decrease of ciprofloxacin efficacy. Formation of a ciprofloxacin-cation
complex resulted in reduced ciprofloxacin absorption. Co-administration of ciprofloxacin with
© EMEA 2008
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fennel led to a 83% reduction in ciprofloxacin C max while T max remained virtually unaffected
resulting in a significant reduction in area under the curve. This interaction has not been observed
in humans (Zhu et al., 1999).
Investigations showing liver enzymes-inducing effects of compounds present in fennel oil strongly
raise the possibility for interactions of fennel with other medicinal products to take place.
In fact, experiments in which rats were injected intra-peritoneally with a mixture of trans -anethole
(100 mg/kg b.w.) and [ 14 C]parathion (1.5 mg/kg) showed no significant effect of trans -anethole on
metabolism and excretion of the insecticide. However, when rats were fed a diet containing 1% of
trans- anethole for 7 days and subsequently cell fractions from the livers of these rats were incubated
for 2 hours with [ 14 C]parathion, significantly less unchanged parathion (1.6%) was recovered
compared to controls (12.5%). The data were interpreted as suggesting that feeding trans -anethole to
rats for 7 days induced the synthesis of parathion-degrading liver enzymes (Marcus and Lichtenstein,
1982).
Limonene was found to increase levels of reduced glutathione in mouse liver (Reicks and
Crankshaw, 1993) and beta -myrcene was found to increase levels of specific subtypes of
cytochrome P450 in rat liver (De-Oliveira et al., 1997).
Excessive doses of preparations containing fennel oil may affect hormone therapy or oral
contraception (see section IV.4 Special warnings and precautions for use). If the patient is on other
medications, he/she should seek medical advice.
IV.7 Overdose
No data available.
V. Overall Conclusion
The traditional uses of fennel for “dyspeptic complaints such as mild, spasmodic gastro-intestinal
ailments, bloating and flatulence” and “catarrh of the upper respiratory tract” are supported not
only by expert’s opinion and clinical experience, but also by available data.
Clinical trials showing the efficacy of fennel as a smooth muscles spasmolytic remedy are limited
and preliminary, but pharmacological data show a significant relaxing effect of fennel alcoholic
extracts and essential oil on tracheal, ileal and uterine smooth muscles contracted by several
contraction-inducing agents (i.e. metacholine, oxytocin, PGE 2, acetylcholine, carbachol and
histamine).
Moreover, the ability to counteract prostaglandins actions may also explain the anti-inflammatory
effect observed following an oral administration to rats.
The above-mentioned effects are also likely to play a beneficial role in the treatment of
inflammation of mucous membranes of upper respiratory tract with an excessive secretion of
epithelial cells induced by respiratory tract infections, generally also inducing prostaglandin-
mediated bronchoconstriction. Moreover, this indication is also made plausible by the secretolytic
and expectorant effects exhibited by anethole and fenchone, two main components of fennel oil,
when administered by inhalation to urethanized rabbits.
It has been shown that both anethole and estragole given intravenously (10 mg/kg) elicit in the
laboratory animal vagal effects causing a transitory bradycardic and depressor effect (de Siqueira,
2006).
Lastly, when considering the plausibility of the above indications, particularly with reference to
inflammation of mucous membranes of upper respiratory tract, bloating and flatulence, the likely role
of a number of compounds detected in fennel fruit and very active in inhibiting growth of pathogenic
bacteria and fungi should not be underestimated.
© EMEA 2008
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On the basis of long-standing use and experience, the HMPC recommends the following
indications for bitter fennel fruit and sweet fennel fruit: “Traditional herbal medicinal product
i) for symptomatic treatment of mild, spasmodic gastro-intestinal complaints including bloating
and flatulence;
ii)
for symptomatic treatment of minor spasm associated with menstrual periods;
iii)
used as an expectorant in cough associated with cold.”
No other traditional medicinal uses of fennel are supported by adequate data.
For bitter fennel oil, traditional use is known only as “ an expectorant in cough associated with
cold ” and is recommended by the HMPC.
For fennel fruit, long-standing use in TCM is also documented with indication i) and ii) when the
symptoms are triggered or worsen by “cold” and improve by “heat” application.
© EMEA 2008
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Source: European Medicines Agency



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