Community herbal monograph on
Arctium lappa
L., radix
To be specified for the individual finished product.
Well-established use
Traditional use
With regard to the registration application of
Article 16d(1) of Directive 2001/83/EC as
amended
i) Herbal substance
Not applicable.
ii) Herbal preparations
a)
Comminuted herbal substance
b)
Powdered herbal substance
c)
Liquid extract (DER 1:1), extraction solvent
ethanol 25% V/V
e)
Tincture (ratio of herbal substance to
extraction solvent 1:10), extraction solvent
ethanol 45% V/V
f)
Tincture (ratio of herbal substance to
extraction solvent 1:5), extraction solvent
ethanol 25% V/V
Well-established use
Traditional use
Comminuted herbal substance as herbal tea for
oral use.
Herbal preparations in solid or liquid dosage forms
for oral use.
The pharmaceutical form should be described by
2 The declaration of the active substance(s) for an individual finished product should be in accordance with relevant herbal
quality guidance.
3 Dried, total or cut roots of
Arctium lappa
L. (=
A. major
Gaertn.),
A. minus
(Hill) Bernh.,
A. tomentosum
Mill. (
Asteraceae
)
and from related species, hybrids or mixtures thereof. The root is collected in the autumn of the first year or in the spring
of the second year. The material complies with DAC 2008 "Klettenwurzel – Bardanae radix"
4 Codex Francais 1949
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Arctium lappa
L., radix
EMA/HMPC/246763/2009
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Well-established use
Traditional use
the European Pharmacopoeia full standard term.
4.1.
Therapeutic indications
Well-established use
Traditional use
Indication 1)
Traditional herbal medicinal product used to
increase the amount of urine to achieve flushing
of the urinary tract as an adjuvant in minor
urinary tract complaints.
Indication 2)
Traditional herbal medicinal product used in
temporary loss of appetite.
Indication 3)
Traditional herbal medicinal product used in
treatment of seborrhoeic skin conditions.
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 and Elderly
a) Comminuted herbal substance:
single dose: 2-6 g as an infusion, 3 times daily.
b) Powdered herbal substance: single dose
350 mg, 3 to 5 times daily.
c) Liquid extract: 2-8 ml, 3 times daily.
d) Soft extract: single dose 0.2 g, daily dose
1-2 g.
e) Tincture (45% V/V): 8-12 ml, 3 times daily.
f) Tincture (25% V/V): 8-12 ml, 3 times daily.
The use in children and adolescents under
18 years of age is not recommended (see section
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Arctium lappa
L., radix
EMA/HMPC/246763/2009
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Well-established use
Traditional use
4.4 ‘Special warnings and precautions for use’).
Duration of use
Indication 1) and 2)
If the symptoms persist longer than 2 weeks during
the use of the medicinal product, a doctor or a
qualified health care practitioner should be
consulted.
Indication 3)
If the symptoms persist longer than 4 weeks during
the use of the medicinal product, a doctor or a
qualified health care practitioner should be
consulted.
Method of administration
Oral use.
For preparations other than tea: to ensure an
increase of the amount of urine, adequate fluid
intake is required during treatment.
4.3.
Contraindications
Well-established use
Traditional use
Hypersensitivity to the active substance or to
plants of the
Asteraceae
family.
4.4.
Special warnings and precautions for use
Well-established use
Traditional use
Indication 1), 2) and 3)
The use in children and adolescents under 18
years of age has not been established due to lack
of adequate data.
If the symptoms worsen during the use of the
medicinal product, a doctor or a qualified health
care practitioner should be consulted.
Indication 1)
If complaints of symptoms such as fever, dysuria,
spasms or blood in the urine occur during the use
of the
medicinal product, a doctor or a qualified
health care professional should be consulted.
Concomitant treatment with synthetic diuretics is
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Arctium lappa
L., radix
EMA/HMPC/246763/2009
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Well-established use
Traditional use
not recommended.
For preparations containing ethanol, the
appropriate labelling for ethanol, taken from the
‘Guideline on excipients in the label and package
leaflet of medicinal products for human use’, must
be included.
4.5.
Interactions with other medicinal products and other forms of
interaction
Well-established use
Traditional use
None reported.
4.6.
Pregnancy and lactation
Well-established use
Traditional use
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
Anaphylactic shock has been reported. The
frequency is not known.
If other adverse reactions not mentioned above
occur, a doctor or a qualified health care
practitioner should be consulted.
Well-established use
Traditional use
No case of overdose has been reported.
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L., radix
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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.
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.
Adequate tests on reproductive toxicity,
genotoxicity and carcinogenicity have not been
performed.
Well-established use
Traditional use
Not applicable.
16 September 2010
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L., radix
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Assessment Report
Table of contents
Table of contents
................................................................................................................... 2
1. Introduction....................................................................................................................... 3
2. Historical data on medicinal use ...................................................................................... 10
2.1. Information on period of medicinal use in the Community ...................................... 1
0
preparations and indications..................................................................................... 1
2
3. Non-Clinical Data ............................................................................................................. 15
preparation(s) and relevant constituents thereof ......................................................... 1
5
preparation(s) and relevant constituents thereof ......................................................... 1
9
preparation(s) and constituents thereof ..................................................................... 2
1
3.4. Overall conclusions on non-clinical data............................................................... 2
1
4. Clinical Data ..................................................................................................................... 22
4.1. Clinical Pharmacology ....................................................................................... 2
2
including data on relevant constituents ...................................................................... 2
2
including data on relevant constituents ...................................................................... 2
2
4.2. Clinical Efficacy ................................................................................................ 2
2
4.2.1. Dose response studies.................................................................................... 2
2
4.2.2. Clinical studies (case studies and clinical trials).................................................. 2
2
4.2.3. Clinical studies in special populations (e.g. elderly and children)........................... 2
2
4.3. Overall conclusions on clinical pharmacology and efficacy ...................................... 2
2
5. Clinical Safety/Pharmacovigilance................................................................................... 23
5.1. Overview of toxicological/safety data from clinical trials in humans.......................... 2
3
5.2. Patient exposure .............................................................................................. 2
3
5.3. Adverse events and serious adverse events and deaths ......................................... 2
3
5.4. Laboratory findings .......................................................................................... 2
4
5.5. Safety in special populations and situations ......................................................... 2
4
5.6. Overall conclusions on clinical safety ................................................................... 2
5
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L., radix
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1.
Introduction
1.1.
Description of the herbal substance(s), herbal preparation(s) or
combinations thereof
Botanical description
Arctium lappa
L. is known under the synonyms:
Latin:
Arctium majus
BERNH.
,
Lappa communis
var.
major
COSSON
et
GERM
.,
Lappa major
GAERTN.
,
Lappa officinalis
ALL
.,
Lappa vulgaris
HILL.
,
Lappa vulgaris
var.
major
NEILR
English: beggars button, burdock, cockle-bur, cockle-button, common burdock, cuckold-dock, great
but, great clotbur, greater burdock, hardock, hare burr, hurr-bur, stick-button, bat weed
French: bardane, bouillon noir, choux d’ânes, glouteron, gouteron, grande bardane, grateau, grateron,
herbe aux pouilleux, herbe aux teigneux, oreille de géant, pignet, teigneux
German: große Klette, Dollenkraut, gemeine Klette
Italian: bardana, bardana maggiore, farfariaccio, lappa bardana, lappola
Dutch: grote klis, grote klit, dokke, kladden, klevers, Jan-plak-an
Japanese: gobo
(Blaschek 1998, Delfosse 1998, De Smet 1993, Leclerc 1966, Van Os 1980, Wichtl 1994).
Arctium lappa
L. is a biennial member of the
Compositae
(
Asteraceae
) that can reach one meter and a
half. It has large cordiform leaves. The purple flowers appear from July until September. The spherical
flower head, three to four centimeters in diameter, has rough hairs (Delfosse 1998, Lambinon 1998).
Native in Europe, Northern Asia and North America (Wichtl 1994).
Herbal substance(s)
Folium
The leaves are collected from 1-year old plants and dried (Blaschek 1998).
The use of fresh leaves is described in literature (Leclerc 1966, Valnet 2001).
Constituents:
- Sesquiterpenes: The dried leaves contain
essential oil, arctiol, dehydrofukinone, eremophilene,
-
eudesmol, fukinanolide, fukinone and petasitolone. The fresh leaves contain onopordopicrin and the
ground leaves arctiopicrin.
- Triterpenes: Free terpene alcohols, free sterols, triterpene esters.
From the petrolether extract of dried leaves are isolated: free triterpene alcohols (α-amyrine, β-
amyrine, lupeol, phytol, ω-taraxasterol, taraxasterol), triterpene alcohol acetates (taraxasterol
acetate, α-amyrine acetate, β-amyrine acetate, lupeol acetate, ω-taraxasterol acetate) triterpene
alcohol esters with long chain fatty acids (taraxasterolester, α-amyrine ester, β-amyrine ester,
lupeolester, phytolester, ω-taraxasterolester).
- Fatty Acids: 94.7% saturated (C
14
- C
26
) and 5.3% unsaturated (C
18
) fatty acids.
- Phenol Carbonic Acid: Caffeic acid.
- Ascorbic Acid, -Mucilage, Tannins.
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Arctium lappa
L., radix
EMA/HMPC/246764/2009
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(Blascheck 1998).
Semen (fructus)
The mature fruit is collected in autumn and dried. Thereafter, the dried fruit is purified and dried again
in the sun (Blaschek 1998).
The dried, ripe fruit is collected in autumn (Chinese Pharmacopoeia 1995, Körfers 2009).
Constituents:
- Fatty Oils: The seeds contain about 16% fatty oils
,
namely linoleic acid, oleic acid, octadecatrienic
acid, palmitic acid, stearic acid, eicosatrienic acid, arachidonic acid, myristinic acid, linolenic acid,
heptadecanic acid, margarinic acid and pentadecanic acid.
- Lignans: The fruit contains a broad spectrum of lignans. Lignans with two phenylpropane units:
arctiin, arctigenin, matairesinol. Lignans with three phenylpropane units (“sesquilignans”): lappaol A,
lappaol B, lappaol C, lappaol D, lappaol E. Lignans with four phenylpropane units (“dilignans”):
lappaol F, lappaol H, neoarctin A, neoarctin B and diarctigenin.
- Daucosterol (fruit).
Radix
The most recent official definition is included in DAC 2008: dried, total or cut roots of
Arctium lappa
L.
(=
A. major
Gaertn.),
A. minus
(Hill) Bernh.,
A. tomentosum
Mill. (
Asteraceae
) and from related
species, hybrids or mixtures thereof. The root is collected in the autumn of the first year or in the
spring of the second year.
Similar or identical definitions can be found in Barnes (2007), Blaschek (1998), De Smet (1993), Duke
(1988), Uchiyama (2005) and Wichtl (1994).
Constituents:
- Volatile constituents, essential oil: There are only 0.06-0.18% of essential oil in the roots of
Arctium
lappa
L., altough this fraction is well investigated. More than 60 subclasses are known.
Blaschek (1998) categorizes them as follows:
Aliphatic hydrocarbons: aplotaxen, dihydroaplotaxen, 1-heptadecen, 1-pentadecen
Aliphatic and aromatic aldehydes: phenylacetaldehyde, propionaldehyde, benzaldehyde,
butyraldehyde, caproicaldehyde, isovaleraldehyde and others
Carbonic acids: carbonic acids from C
2
until C
13
and also tiglic acid, isovaleric acid among others
Pyrazines: 2-methoxy-3-methylpyrazin and six other 2-alkyl (C
3
-C
5
)-3-methoxypyrazines
Sesquiterpenes: α-guajen, cyperen, costic acid, dehydrocostuslacton
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L., radix
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H
2
C
H
2
C
CH
2
O
O
Figure 1: dehydrocostuslacton
- Lappaphenes: Lappaphen-a and lappaphen-b are isolated from the fresh root.
- Sulfur-free polyacetylenes:
The polyacetylenes percentage is higher in a fresh root than in a dried
root. More than ten
different polyacetylenes can be identified. 1,11-tridecadiene-3,5,7,9-tetrayne is
the most important one.
Figure 2: 1,11-tridecadiene-3,5,7,9-tetrayne
- Sulfur-containing polyacetylenes (thiophenes):
arctinal, arctinol A, arctinol B, arctinon-A, arctinon-B,
arctinon-A-acetaat, arctic acid B, arctic acid C and arctic acid-B-methylester have been isolated.
OH
S
OH
S
H
3
C
Figure 3: arctinol
- Phenolcarbonic acids and tannins: The fresh root contains 1.9 up to 3.65% polyphenols with
chlorogenic acid, isochlorogenic acid and caffeic acid. More recent tests show the presence of
derivatives of quinic acid. The root also contains a small amount of tannins.
- Lignans:
neoarctin A and the lignanolide arctiin.
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L., radix
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O
MeO
O
H
OMe
OMe
Figure 4: arctiin
- Triterpenes: 15.2% triterpenester, 12.8% free sterols (sitosterol, stigmasterol, a.o.), 10.7%,
triterpenacetates, 2.9% triterpenacids and 2.4% triterpenalcohols (α-amyrine, β-amyrine, lupeol,
-
taraxasterol, phytol) are isolated from the petrolether extract of the dried root.
- Fatty acids: 0.4 until 0.8% fatty acids including linolenic acid, linoleic acid, myristic acid,
palmitic-
and stearic-acids
- Polysaccharides: The total carbohydrates may represent up to 70% of the dry mass and contain
mainly inulin (about 45%).
- Other constituents: The aminoacid fraction contains γ-guanidino-n-butyric acid. Also vitamin C (23
mg/100 g) has been found.
- Baicalin
O
OH
O
O
O
OH
H
H
O
H
OH
O
Figure 5: baicalin
- Aplotaxene
Figure 6: aplotaxene
Herbal preparation(s)
Apart from the references cited, market information was included (Barnes 2007, Blaschek 1998,
Delfosse 1998, Leclerc 1966, Valnet 2001, Van Hellemont 1985).
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L., radix
EMA/HMPC/246764/2009
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Hagers Handbuch der Pharmazeutischen Praxis (Blaschek 1998) mentions different fluid extracts of
Radix Bardanae (Extractum Bardanae):
- Extractum Bardanae Portug.
- Extractum Bardanae Brasil.
- Extractum lappae fluidum
- Extractum lappae fluidum Brasil.
- Extractum lappae majoris stabilisatae
No further details could be retrieved for those preparations.
Combinations of herbal substance(s) and/or herbal preparation(s) including a description of
vitamin(s) and/or mineral(s) as ingredients of traditional combination herbal medicinal products
assessed, where applicable.
‘Essiac’ is described as a formula that consists of four herbal substances:
Arctium lappa
L.,
Rheum
palmatum
L.,
Rumex acetosella
L.
and
Ulmus rubra
L. The preparation is only partially characterised.
Indication: cancer treatments but no convincing clinical evidence is available (Capasso 2003, Ulbricht
2009).
1.2.
Information about products on the market in the Member States
Regulatory status overview
Member State Regulatory Status
Comments
Austria
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Belgium
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Bulgaria
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Cyprus
MA
TRAD
Other TRAD
Other Specify: No information
Czech Republic
MA
TRAD
Other TRAD
Other Specify: Only combination
products
Denmark
MA
TRAD
Other TRAD
Other Specify: Only combination
products
Estonia
MA
TRAD
Other TRAD
Other Specify: Only food supplements
Finland
MA
TRAD
Other TRAD
Other Specify: No information
France
MA
TRAD
Other TRAD
Other Specify: Registered products on
the market since 1980
Germany
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered products
Greece
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered products
Hungary
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered products
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Iceland
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Ireland
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Italy
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Latvia
MA
TRAD
Other TRAD
Other Specify: No information
Liechtenstein
MA
TRAD
Other TRAD
Other Specify: No information
Lithuania
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Luxemburg
MA
TRAD
Other TRAD
Other Specify: No information
Malta
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
The Netherlands
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Norway
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Poland
MA
TRAD
Other TRAD
Other Specify: No information
Portugal
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Romania
MA
TRAD
Other TRAD
Other Specify: No information
Slovak Republic
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Slovenia
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
Spain
MA
TRAD
Other TRAD
Other Specify: Preparations authorized:
see detailed information
below
Sweden
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
United Kingdom
MA
TRAD
Other TRAD
Other Specify: No authorized or
registered preparations
MA: Marketing Authorisation
TRAD: Traditional Use Registration
Other TRAD: Other national Traditional systems of registration
Other: If known, it should be specified or otherwise add ’Not Known’
This regulatory overview is not legally binding and does not necessarily reflect the legal status of the
products in the MSs concerned.
Czech Republic
In the Czech Republic, a fixed combination (herbal tea) is used. This tea contains Phaseoli fructus sine
semine, Myrtilli herba, Salviae officinalis herba, Galegae herba, Polygonii avicularis herba, Taraxaci
radix cum herba, Rubi fruticosi folium, Foeniculi fructus, Bardanae radix and Liquiritiae radix.
Indication: adjuvant therapy in diabetes.
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L., radix
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Denmark
An ayurvedic fixed combination is available in Denmark. It contains 40 mg
Arctium lappa
L. per tablet
and 18 other ingredients. No information on details of the preparation is given.
Indication: claudicatio intermittens.
France
Powdered herbal substance in hard capsules.
A preparation containing powdered herbal substance in capsules is on the market in France since 1980.
It contains 350 mg powdered herbal substance per capsule.
Posology: 1 capsule 3 times daily (up to 5 capsules if necessary).
Indications:
- traditionally used in seborrhoeic skin conditions
- traditionally used to promote urinary and digestive elimination functions.
Extract in hard capsules
A preparation with dry extract made with ethanol 70% V/V (DER 2.5-4.5:1), on the market in France
since 1994.
It contains 200 mg dry extract per capsule.
Posology: 1 capsule 2 times daily.
Indications: Traditionally used in seborrhoeic skin conditions.
Spain
In Spain powdered or cut herbal substance is on the market as tea since 1973.
A daily dose of 3 g to 6 g can be taken.
Indication: facilitating the elimination of urine.
The herbal substance is also available in combination products.
There is partial information about other products on the Spanish market. The date of commercialising
is not specified.
Liquid extract (DER 1:1) 25-50 drops, 1 to 3 times daily
Tincture (1:10) 50 drops 1 to 3 times daily
Dry extract (DER 5:1) 1 g daily
The solvents for all these preparations are not specified.
These preparations are similar to the ones mentioned in the BHP (1983), cited by Barnes (2007) and
Blaschek (1998).
Indication: similar uses as presented in registered products.
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L., radix
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2.
Historical data on medicinal use
2.1.
Information on period of medicinal use in the Community
Arctium lappa
L. has been widely used in folk medicine (Gentil 2006). Besides, the root and leaves are
listed by the Council of Europe as a natural source of food flavouring (category N2) (Barnes 2007).
An herbal tea called ‘Essiac plus’ contains the same four substances as ‘Essiac’ (
Arctium lappa
L.,
Rheum palmatum
L.,
Rumex acetosella
L.
and
Ulmus rubra
L.) plus four additional herbs:
Nasturtium
officinale
L.,
Cnicus benedictus
L.,
Trifolium pratense
L
.
and
Laminaria digitata
(Huds.) Lamour.
Indication: The tea is used by cancer patients during chemo- and radiation therapy. No further details
about concentration and doses are given (Tai and Cheung 2005).
According to Tai and Cheung (2005), a product called ‘Flor-Essence’ at high concentrations has shown
in vitro
differential inhibitory effect on different human cancer cell lines.
In Spain, powdered or cut root is on the market as tea since 1973. The oral use of preparations with
non specified root extract is reported by Leclerc (1966).
In some countries, mainly in Japan, a cultivated form of
Arctium lappa
L. is used as a vegetable (De
Smet 1993).
2.2.
Information on traditional/current indications and specified
substances/preparations
Folium
Preparation
Single dose
Daily dose
References
Macerate: fresh leaves macerated
during one night in salted vinegar
(1:125)
Or fresh leaves as such
External use as
cataplasm: no
dose specified
External use as
cataplasm: no
dose specified
Leclerc 1966,
Valnet 2001
- Macerate: fresh leaves macerated during one night in salted vinegar (1:125)
Terray, cited by Leclerc (1966), reports good results when using the fresh macerated leaves wrapped
around the painful body parts of patients with rheumatism. This can create an urticarial reaction which
is considered to be even more beneficial (Leclerc 1966).
- Unknown way of administration and posology:
Tea infusions of leaves are used for stomach ulcer and gastritis. In case of infection of mouth and
pharynx, a decoction is used to gargle. Topically it is used to treat skin diseases, insect bites (Bruneton
1999), itching and scratches (Blaschek 1998). Leaves may help to treat bruises, tumours and gouty
swellings (Duke 1988).
Kloss, cited by Duke (1988), describes the leaves as ‘excellent for cancer sores, gonorrhea, gout,
leprosy, rheumatism, sciatica, scrofula and syphilis’. They have been used to treat bladder stones,
eczema, gallstones, gout, and skin afflictions (Duke 1988).
Alcoholic extracts of the leaves are used for treating psoriasis and seborrhoeic eczema. Extracts would
also promote hair growth and are used in the production of cosmetics (Blaschek 1998).
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L., radix
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The crushed leaves of
Arctium lappa
L. were also applied on snake bites. Beneficial effects have been
attributed to a modification of the main constituents in the venom. The oxidation that happens is
thought to be similar to the one of potassium permanganate (Leclerc 1966, Valnet 2001).
As the traditional use is restricted to
ex-tempore
preparations of the fresh leafs, no monograph on
Arctium lappa
L., folium is proposed.
Semen
Preparation
Single dose
Daily dose
References
Dried seeds
4–6 g
6-12 g
Valnet 2001
Körfers 2009
The seeds of
Arctium lappa
are used in Korea for their supposed diuretic, anti-inflammatory and
detoxifying effect. In TCM, the freshly crushed herbal substance is used to treat cough, flu, pharyngitis
and infections
of the respiratory tract (Chinese Pharmacopoeia 1995, Körfers 2009). It is also used for
measles, mumps, rubella, erysipelas and carbuncles (Blaschek 1998) and in Urolithiasis (Valnet 2001).
In Asia, the seeds are used to treat constipation, flatulence, abscesses, dropsy, acne, scarlet fever, flu,
snakebite, measles, scrofula and smallpox. Tinctures of the seeds are used for the treatment of kidney
diseases, psoriasis, prurigo and acne (Duke 1988).
As only very limited information on the traditional use of the seeds within the Community is available
(Blaschek 1998, Valnet 2001), no monograph on
A. lappa
L., fructus is proposed.
Radix
Use of different herbal preparations:
Antibacterial and antimycotic use
Quoted from Bézanger-Beauquesnes (1980): ’’
… The fresh radix of Arctium lappa has antibacterial and
antimycotic properties by the presence of polyenes and polyines, more particularly diene-tetraine …”.
No further reference is made to specific preparations. This use dates from 1960 or before that date.
Rheumatism
Root preparations have been used for rheumatism (Bradley 1992).
The root of
Arctium lappa
L
.
is described as a blood purifier, it is believed to clear toxins from the
bloodstream (De Smet 1993).
In folk medicine, root infusions and plasters are often used for its anti-inflammatory activity (De Smet
1993).
The root has been used for gout (Valnet 2001).
Choleretic and diuretic use
Quoted from Bézanger-Beauquesnes (1980): “
… A choleretic and diuretic action is due to alcoholic
acids related to hydromethacrylic acid. The components for its putative hypoglycemic activity are
not known. All these properties lead to a purification-activity of the radix in certain nutritional and
dermatological conditions and furunculosis …”.
No further reference is made to specific
preparations. This use dates from 1960 or before that date.
Burdock root has been considered to have diuretic and diaphoretic actions to stimulate hepato-biliary
function (Bradley 1992).
According to DAC 2008, the root is used in case of gout, rheumatism and to promote urinary
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Arctium lappa
L., radix
EMA/HMPC/246764/2009
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elimination and sweating.
The root can also be used as a diaphoretic and diuretic remedy.
Arctium lappa
L. promotes sweating,
which helps to release toxins through the skin. It also promotes more urine production and gives
further elimination of toxins via the kidneys and bladder (De Smet 1993, Duke 1988).
It is also used as a laxative for renal or urinary calculi, jaundice and furunculosis (De Smet
1993).
Treatment against urolithiasis has been mentioned by Valnet (2001).
Skin disorders
Root preparations have been used for skin disorders, seborrheic eczema and for stimulation of the
hair growth. The hairy character of the plant might explain the belief of its hair growing
characteristics (Bradley 1992).
Acording to DAC 2008, the root is externally used in seborrhoe of the skin, other skin diseases, wounds
and acne.
It is also used against eczema
(De Smet 1993).
Topical application can be used to treat poorly healing wounds, ichtyosis, psoriasis, acne and other skin
diseases. The radix can also be added to bathwater. In the past, Oleum Bardanae was used topically
for seborrheic eczema. Most of the sources are copying each other, referring to the BHP (1983), which
is in fact a compilation of former BHP editions (BHP 1976). This preparation has to be considered as
being traditionally used for more than 30 years.
Gastro-intestinal complaints
According to DAC (2008), the root is widely used in popular medicine: orally for treatment of
gastro-intestinal complaints and loss of appetite.
Coffee surrogate
The roasted root can be consumed as a coffee surrogate (Blaschek 1998).
Glandular tumors
The root decoction alleviates ulcerated, glandular and white tumours (Duke 1988).
2.3.
Specified strength/posology/route of administration/duration of use
for relevant preparations and indications
Preparation
& Indication
Single dose
Daily dose
References
Radix (= dried root)
Skin disorders
2-6 g of cut root per
cup water, let it rest
during several hours
and subsequently let it
boil during 1 hour.
Filter (decoction).
3 single doses
Barnes 2007,
Delfosse 1998, Van
Hellemont 1985
Radix (= dried root)
(Uro-)lithiasis
Measles
Decoction, 40 g per
liter, cook for 10
minutes.
(Uro-) Lithiasis 2-3
cups per day
measles: 1 coffee-
spoon every 5
minutes for two
hours
Valnet 2001
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L., radix
EMA/HMPC/246764/2009
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Preparation
& Indication
Single dose
Daily dose
References
Radix (= dried root)
Gout
60 g/l, cook for 5
minutes.
2 l per day
Valnet 2001
Radix (= dried root)
Seborrhoea, impetigo, acne
3 handful/l, cook for
20 minutes.
external use for
washings
Valnet 2001
Powdered dried root
Skin disorders
Diuretic / diaphoretic
Rheumatism
2-6 g per cup as an
infusion.
2–4 g mixed with a
suitable liquid.
3 single doses
Blaschek 1998
Valnet 2001
BHP 1976
Powdered dried root
Traditionally used in
seborrhoeic skin conditions;
Traditionally used to promote
urinary and digestive
elimination functions
350 mg
350 mg
3 times daily (up
to 5 capsules if
necessary).
On the market in
France since 1980
Liquid extract of root (DER
1:1), extraction solvent 25%
ethanol V/V
Liver crisis and liver
congestion
Diuretic
Skin disorders and
rheumatism
2-8 ml
3 single doses
Barnes 2007
Blaschek 1998
BHP 1976
One small spoon (5
ml)
4 to 5 doses a day
Delfosse 1998
Van Hellemont
1985
Market information
from Spain
3 doses
25 to 50 drops
3 times daily
Bradley 1992
2-6 ml
Tincture of root (1:5) in 25%
ethanol V/V
Skin disorders and
rheumatism
Diuretic
8-12 ml
3 times daily
Bradley 1992
BHP 1976
Tincture of root (1:10) in
45% ethanol V/V
Skin disorders and
rheumatism
Diuretic
8-12 ml
3 single doses
Barnes 2007
Blaschek 1998
BHP 1976
50 drops
3 doses
Market information
from Spain
Decoction of root (1:20) or
decoction of 30 g root/l
Skin disorders and
rheumatism
No information
available
500 ml
Barnes 2007
Blaschek 1993
BHP 1976
Winter 1984
Dried root or decoction
2-6 g
3 times daily
Bradley 1992
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Arctium lappa
L., radix
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Preparation
& Indication
Single dose
Daily dose
References
Skin disorders and
rheumatism
BHP 1976
Radix nebulisate (1:4)
(No details on preparation
available)
Liver function
Diuretic
Skin disorders
1 or 2 capsules of 50
mg
3 single doses
Delfosse 1998
Van Hellemont
1985
Van Hellemont
1986
Arctium lappa L. T.M. (Ø)
Liver function
Diuretic
Skin disorders
50 drops
3 single doses
Delfosse 1998
Van Hellemont
1985
Syrup of root
(1)
:
Root soft stabilized extract
Codex Francais (1949) 20 g
Sirupus simplex ad 400 g
Liver function
Diuretic
Skin disorders
15 ml
9 doses
Garnier 1961
Pills:
Root soft stabilized extract
Codex Francais (1949),
extract 0.20 g
Liquorice powder Q.s.
Liver function
Diuretic
Skin disorders
See daily dose
5-10 pills
Leclerc 1966
Garnier 1961
Elixir:
Root soft stabilized extract
Codex Francais (1949) 8 g
Garrus elixir 80 g
Sirupus Simplex ad 200 g
Liver function
Diuretic
Skin disorders
See daily dose
Up to 9 spoons
(15 ml)
Leclerc 1966
Garnier 1961
(1)
Soft stabilised extract of the root:
A stabilised soft extract is described in the Codex Français (1949) and cited by Garnier (1961).
R/
Arctium lappa,
powdered root 1000 g
Distilled water 8000 g
Macerate of the root in 5000 g distilled water during 12 hours under regular mixing and filter under pressure.
Macerate the residue in the remaining part of the water during 12 hours and filter under pressure.
Mix both filtrates and evaporate the water under reduced pressure until 3000 g remain. Let the fluid settle and filter
after 24 hours. Evaporate under reduced pressure ‘au bain-marie’ until a soft consistency is obtained.
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L., radix
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3.
Non-Clinical Data
3.1.
Overview of available pharmacological data regarding the herbal
substance(s), herbal preparation(s) and relevant constituents thereof
Activity of isolated compounds
:
Antitumor properties
In 2008, a study investigated the anti-cancer properties of
arctiin
, a major lignan constituent of
Arctium lappa
L. 100-250 μM arctiin has a maximum growth inhibitory effect on several types of cancer
cells, although it did not completely inhibit cell growth. There is a down-regulation of cyclin D1 protein
expression. This induced suppression occurs in various types of human tumor cells, including
osteosarcoma, lung, colorectal, cervical and breast cancer, melanoma, transformed renal cells and
prostate cancer (Matsuzaki 2008).
A diet containing 0.1, 0.02 or 0.004% arctiin was administered for 18 weeks. Arctiin has been
evaluated to exert no definite effects on prostate carcinogenesis in SV 40 T antigen transgenic rats at
least in the experiment, although a weak inhibitory tendency was found in high dose groups (Zeng
2005).
Baicalin, a natural compound of
Arctium lappa
L. and genistin, a baicalin derivative, were found to be
potent and selective inhibitors of terminal deoxyribonucleotidyltransferase (TdT), an eukaryotic DNA-
polymerase. The IC50 of baicalin and genistin to TdT were respectively 18.6µM and 28.7µM. These
inhibitors can be used as tools and molecular probes to distinguish DNA polymerases and to clarify
their
in vivo
biological function (Uchiyama 2005).
Antioxidative effects and anti-inflammatory effects
Inhibitors of NO production in macrophages are important targets in the treatment of inflammatory
diseases, such as rheumatoid arthritis. The
lignans isolappaol C, lappaol C, lappaol D, lappaol F
and
diarctigenin
were isolated from a methanolic extract of the seeds from
Arctium lappa
L. They
were investigated in their inhibitory effects on the NO production in LPS-stimulated RAW264.7 cells. As
a result, lappaol F and diarctigenin inhibited NO production with IC50 values of 9.5 and 9.6 µM,
respectively. The other three compounds were inactive (Park 2007).
Kim (2008) describes the anti-inflammatory activity of
Arctium lappa
L. In Korea, the seeds of
Arctium
lappa
L. are used for the treatment of inflammatory diseases. The study of Kim evaluates the
pharmacological potential of
Arctium lappa
L. in NF-κB-associated inflammatory disorders. NF-κB is a
transcription factor that plays an important role in the initiation and amplification of inflammatory
responses.
Diarctigenin
, a lignan from
Arctium lappa
L. (0.6-30μM), was found to inhibit the
production of many inflammatory mediators in macrophages such as PGE2, IL-6 and others.
Diarctigenin down-regulated the expression of the inflammatory genes at the transcription level
through suppression of NF-κB activation.
According to Knipping (2008),
Arctium lappa
L. might be a promising natural component for use in
anti-allergic treatment. In their investigation,
arctiin
was able to significantly reduce the release of
inflammatory mediators
in vitro
(through inhibition of degranulation and cys-leukotriene release).
Arctiin was also able to inhibit acute skin response in mice
in vivo
.
Prebiotic effects
In 2008, Li studied the prebiotic potential of components of
Arctium lappa
L. They found that
inulin
of
the root from
Arctium lappa
L. (1% w/v) promoted the specific growth rate of "beneficial bacteria"
in
vitro
and
in vivo
. The final bacterial mass in the medium with inulin of
Arctium lappa
L. was greater
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L., radix
EMA/HMPC/246764/2009
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than that in the medium without inulin of
Arctium lappa
L. By stimulating the growth of these
lactobacilli and bifidobacteria
in vitro,
the resistance to disease is thought to increase because these
micro-organisms may retard the growth of pathogenic bacteria. There is also a production of inhibitory
substances. Furthermore, these beneficial bacteria may have an immunomodulatory effect. The
results of the
in vivo
study with mice confirmed the prebiotic effectiveness which was found in the
in
vitro
study. However, studies on human subjects are needed to investigate whether
Arctium lappa
L.
may have beneficial effects (Li 2008).
Other effects
Arctiin
, a constituent of Fructus Bardanae, delays germination of other plant seeds. The anatomy of
the stem is not influenced but in the root abnormal germination (= deformation of the root with root
hairs that are shorter and twisted) is induced by
Arctium lappa
L. Due to short and twisted root hairs
the nutrition intake is possibly heavily disturbed. An interaction with DNA is also observed. However,
the kind of interaction is not yet clear (Blaschek 1998).
Activity of preparations from the leaves:
Hypoglycaemic effects
The possible anti-diabetic effect of
Arctium lappa
L. has been intensively examined.
Although the root of
Arctium lappa
L. has been found to cause hypoglycaemia in rats, newer studies
have reported that oral administration of leaves to normal mice did not affect glucose homeostasis.
Swanston-Flatt (1989) found that a treatment for 28 days with preparations of
Arctium lappa
L. gave
an aggravation of hyperglycaemia, together with polydipsia and a loss of body weight in
Streptozotocin-induced diabetic mice. They used a
decoction
prepared by addition of
1 g of dried
leaves to 400 ml of cold water (Blaschek 1998, De Smet 1993, Swanston-Flatt 1989).
Antibacterial activity
Gentil (2006) examined the antibacterial activity of an
ethyl acetate fraction
extracted from the
leaves of
Arctium lappa
L., solubilized in propylene glycol (concentration not known). Twenty-seven
canine maxillaries were inoculated with a mixed bacterial suspension of
Pseudomonas aeruginosa,
Escherichia coli, Lactobacillus acidophilus, Streptococcus mutans
and
Candida albicans
. The growth of
all these microorganisms was inhibited by the medications prepared from an ethyl acetate fraction of
Arctium lappa
L. (on the 14
th
and 30
th
day). Gentil (2006) hypothesized that the antimicrobial activity
can be attributed to the presence of flavonoids and tannins respectively.
Antioxidative effects and anti-inflammatory effects
Kardašová and Machová (2006) isolated eleven polysaccharides including from the leaves of
Arctium
lappa
L. The polysaccharides were investigated for their ability to inhibit peroxidation of soybean
lecithin liposomes by OH radicals. The antioxidant activity value of the
polysaccharide
from the
leaves of
Arctium lappa
L. (31.3 x 10
-3
mM) was
9.8%, while the activity of eight other
polysaccharides
ranged from 20 to 45%.
Activity of preparations from the seeds:
Platelet Activating Factor (PAF) antagonism
Platelet Activating Factor (PAF) induces platelet aggregation. In 1992, Iwakami tested the inhibitory
effects of the extracts of different plants.
Lignans
in the seeds of
Arctium lappa
L. (
arctigenin,
lappaol A and C
) have been found to inhibit the binding of platelet activating factor to rabbit platelets
(74% inhibition at 200 μg/ml hot aqueous extract of the seeds) (Blaschek 1998, Iwakami 1992).
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Hypoglycemic effect
In 2008, Xu studied the possible hypoglycaemic effect, effect on glucose tolerance and effect on serum
insulin of
Fructus Arctii (8.0% w/w)
in diabetic and normal animal models. Experimental diabetes
was induced in mice with a single injection of alloxan (90 mg/kg body weight), which is similar to
diabetes type I. Hyperglycaemic-hyperlipidemia diabetes was induced in rats; this is similar to diabetes
type II. The induction was accomplished by giving a fat emulsion which was prepared by dissolving and
mixing lard (20 g), methylthiouracil (1 g), cholesterin (5 g), sodium glutamate (1 g), saccharose (5 g),
fructose (5 g), propylene glycol (30 mg) and Tween 80 (20 ml) in 100 ml water; at 10 ml/kg each day
for ten days. After fasting for at least 12 hours, they received alloxan 50 mg/kg.
Total lignan
was
given to mice and rats daily for 10 days at doses of 2.0, 1.0, 0.5 g/kg and 1.38, 0.69, 0.35 g/kg
respectively. A significant increase in the plasma insulin level was observed in the diabetic mice and
rats. The blood glucose levels were reduced and glucose tolerance was improved. In type I mice, there
was also an increase in serum cholesterol and triglycerides, which represents a risk of coronary heart
disease. More research is needed to study the mechanism of action and the long-term effects.
Antimicrobial activity
An
ethanolic extract
from the fruit of
Arctium lappa
L. inhibited the growth of
Aspergillus parasiticus
.
Two percent of
Arctium lappa
L. (part of the plant not specified) was used in an enriched medium,
which was inoculated with spores and incubated at 28°C for 9 days. In the presence of
Arctium lappa
L., no sporulation of
Aspergillus parasiticus
occurred (Bahk and Marth 1983).
Antioxidative effects and anti-inflammatory effects
According to Knott (2008), natural
Arctium lappa
L. fruit extract
(no specifications given) may
improve clinical signs of ageing skin.
In vitro
studies on human dermal fibroblasts and monocyte-
derived dendritic cells showed that pure
arctiin
stimulates collagen synthesis and decreases
interleukin-6 and tumor necrosis factor-alpha concentration, respectively. Topical
in vivo
application of
an
Arctium lappa
L. fruit extract-containing formulation stimulated procollagen synthesis and increased
hyaluronan synthase-2 expression and hyaluronan levels. The formulation also reduced wrinkle volume
in the crow’s feet area.
Studies in tumor models
A
70% ethanol extract
from Fructus Bardanae showed potent antiproliferative activity against B cell
hybridoma cells (MH60). The active ingredients were (-)-arctigenin with the most potent activity
(IC
50
:1.0 µM), (+)-7,8-didehydroarctigenin and (-)-matairesinol. The activity was associated with the
induction of apoptosis (Matsumoto 2006).
According to Ishihara (2006), hyperthermia is an effective option for cancer therapy, complementary
to chemotherapy or radiotherapy. However, cancer cells may develop thermotolerance. A specific
inhibitor of HSP’s (Heat Shock Proteins) in cancer cells would be useful, since it is critical to prevent
the induction of thermotolerance, when hypertermia is used to treat cancer. Ishihara used mammalian
cells and reported that
a methanolic extract
from the fruits of
Arctium lappa
L. (100 µg/ml)
suppressed the expression of HSP, which was induced by heat shock. Further investigation identified
arctigenin
as the active component in the extract (100 µM). Further experiments showed that not
only the 100 µg/ml extract and 100 µM arctigenin but also a 50 µg/ml extract and 50 µM arctigenin
suppressed the synthesis of HSP70. Arctiin was not found to have an inhibitory effect.
According to Awale (2006), targeting nutrient-deprived cancer cells may be a new strategy in
anticancer drug development. Antiangiogenic therapy is an attractive approach for cancer therapy.
However, cancer cells can survive even under extreme conditions, such as that characterized by low
nutrient and oxygen supply. A
CH
2
Cl
2
-soluble extract
of the dried seeds of
Arctium lappa
L.
was
found to exhibit 100% preferential cytotoxicity against nutrient-deprived cells at a concentration of 50
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L., radix
EMA/HMPC/246764/2009
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μg/ml.
Arctigenin
was identified as the primary compound responsible for such preferential
cytotoxicity.
Activity of preparations from the root:
Anti-mutagenic activity
Arctium lappa
L. root may contain a desmutagenic factor with a molecular weight >300 000, which
might be a lignin-like compound containing about 10% sugar (De Smet 1993).
Arctium lappa
L. reduced the mutagenicity to
Salmonella typhimurium
(TA98, TA100) of mutagens (not
specified) both requiring and not requiring S9 metabolic activation. A lignan-like stucture is probably
responsible for this desmutagenic activity. The addition of fibre (5%) of roots of
Arctium lappa
L. to the
diet of rats apparently gave protection against toxicity of various artificial food colours (Barnes 2007).
Antioxidative effects and anti-inflammatory effects
Lin
(2002)
induced liver damage with ethanol and CCl
4
. When administering
Arctium lappa
L. extract
orally to rats, there was an improvement of the biochemical parameters. A normal saline solution of a
dry extract with water
of
Arctium lappa
L. roots was administered to the rats (300 mg/kg). The
hepatoprotective mechanism of
Arctium lappa
L. may be linked to its antioxidant activity, which
decreases the oxidative stress of hepatocytes.
Di Mambro (2005) has considered that topical use of antioxidants can protect and possibly correct
oxidative skin damage by neutralizing free radicals. The antioxidant effect of an
extract of a mixture
of
Arctium lappa
L. root,
Glycyrrhiza glabra
L. and
Symphytum officinale
L. (at final concentrations of
0.125, 0.25, 0.50, 1.0, 2.0 and 4.0 µl/ml) was evaluated by Di Mambro (2005) as well as the inhibition
of lipid peroxidation, induced by Fe
2+
. The antioxidant effect was measured by evaluating their H-donor
capabilities and their free radical scavenging effects by studying changes of the chemiluminescence
intensity. The results suggest there is some antioxidative effect, although this activity is lower than the
one of the
Glycyrrhiza glabra
L. and
Ginkgo biloba
L. extracts alone and the formulations containing
these extracts.
Abdominal angiostrongyliasis in humans is caused by the parasite
Angiostrongylus costaricensis
. The
effect of an
aqueous extract
of the root of
Arctium lappa
L. (1:10 m/v) on the evolution of intestinal
lesions induced by this parasite was evaluated in mice (500 mg/kg) by Fante (2008). These
researchers concluded
Arctium lappa
L. is not useful for humans affected by abdominal
angiostrongyliasis, since the aqueous extract of
Arctium lappa
L. did not interfere with disease
progression and did not protect against the lesions induced by
Angiostrongylus costaricensis
in mice.
Activity of
Arctium lappa
in general:
Antimicrobial activity
Arctium lappa
L. (different parts of the plant) is used for the treatment of various infectious diseases.
This antimicrobial activity has been associated with the positive effects of
Arctium lappa
L. on kidney
diseases: nephritis and chronical glomerulonephritis (Blaschek 1998). Its antifurunculous effect may be
explained the same way (Barnes 2007).
The antimicrobial activity is attributed to the polyacetylene constituents, although only traces have
been found in the dried herb. Furthermore, arctiopicrin shows antibiotic activity against Gram-positive
bacteria (concentrations not specified). The leaf, flower and root of
Arctium lappa
L. have antibiotic
activity against Gram-negative bacteria (
Escherichia coli, Shigella flexneri, Shigella sonnei
). Gram-
positive activity (e.g.
Staphylococcus aureus, Bacillus subtilis, Mycobacterium smegmatis
) has only
been reported for the leaf and flower (Barnes 2007).
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Activity of
Arctium lappa
in mixtures:
‘Essiac’
2
(see II.3.1.) a formula that consists of four herbal substances (
Arctium lappa
L.,
Rheum
palmatum
L.,
Rumex acetosella
L.
and
Ulmus rubra
L.) was tested. The preparation is only partially
characterised.
Indication: cancer treatments but no convincing clinical evidence is available (Capasso 2003, Ulbricht
2009).
‘Essiac’ has been reported to inhibit cell proliferation and to induce differentiation in human prostate
cancer cell lines
in vitro
. Leonard (2006)
has indicated that ‘Essiac’ has potent antioxidant and DNA-
protective properties.
The results of their study demonstrate that ‘Essiac’ scavenges
OH radicals, O
2
-
radicals and radicals
produced by the RAW264.7 cellular reaction with Cr(VI). ‘Essiac’ also inhibited lipid peroxidation in cell
membranes caused by exposure to
OH radicals and inhibited DNA damage due to
OH radicals
produced by the Fenton reaction (Leonard
2006).
Kulp (2006) have reported that ‘Essiac’ can stimulate the
in vitro
growth of human breast cancer cells
through estrogen receptor mediated as well as estrogen receptor independent mechanisms of action.
No further details about concentration are given. Moreover, Essiac is a mixture.
According to Tai and Cheung (2005), Flor-Essence at high concentrations show
in vitro
differential
inhibitory effect on different human cancer cell lines.
Bennett (2004), however, showed that Flor-Essence can promote DMBA-induced (dimethyl-
benz[a]anthracene) mammary tumor initiation in Sprague-Dawley rats. This observation is in contrast
with widely available anecdotal evidence that this commercially available herbal tonic will suppress or
inhibit tumour growth.
Miscelaneous effects in general:
- Positive effects on nephrosis (fructus Bardanae) (Blaschek 1998).
- Effect against urolithiasis: This effect has been investigated by Grases (1994) using female Wistar
rats. They concluded that beneficial effects of a.o. Arctium lappa L. on urolithiasis can be attributed to
some disinfectant action.
- Diuretic effect (Blaschek 1998).
The above mentioned effects are described without further specification of the extracts or compounds
used.
3.2.
Overview of available pharmacokinetic data regarding the herbal
substance(s), herbal preparation(s) and relevant constituents thereof
Arctiin
In vitro
data:
To investigate the metabolism of arctiin, an experiment with gastric juice (pH 1.2–1.5) and intestinal
flora of rats was performed in 1992. This experiment indicated that arctiin was not affected by gastric
juice. In the intestinal tract a cleavage of the glycosidic binding (resulting in arctigenin) occurs rapidly,
2
Essiac is a common name for complex plant mixtures. By the general us of the name, some confusion about the
composition exists and the translation of pharmacological activities into practice remains difficult (Ulbricht 2009).
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L., radix
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mainly followed by 3”-demethylation of the aglycons (to form 2-(3”, 4”-dihydroxybenzyl)-3-(3’, 4’-
dimethoxybenzyl)-butyrolactone) (Blaschek 1998).
In 2003, another
in vitro
investigation demonstrated that after incubation of arctiin with a human fecal
suspension, not only (2R,3R)-2-(3',4'-dihydroxybenzyl)-3-(3",4"-dimethoxybenzyl)butyrolactone was
formed, but also five other metabolites: (-)-arctigenin, (2R,3R)-2-(3'-hydroxybenzyl)-3-(3",4"-
dimethoxybenzyl)butyrolactone, (2R,3R)-2-(3'-hydroxybenzyl)-3-(3"-hydroxy-4"-
methoxybenzyl)butyrolactone, (2R,3R)-2-(3'-hydroxybenzyl)-3-(3",4"-dihydroxybenzyl)butyrolactone,
and (-)-enterolactone (Xie 2003).
In vivo
data:
200 mg arctiin/kg was administered to rats. One hour after administration, arctigenin was detected in
serum. Four hours after administration, arctigenin reached its maximal serum concentration, and four
hours later arctigenin was not detectable anymore. Neither arctiin nor 2-(3”, 4”-dihydroxybenzyl)-3-
(3’, 4’-dimethoxybenzyl)-butyrolactone, which was found to be the main metabolite, were present in
the serum of the rats, not even the conjugated form of the metabolite. On the other hand, the
concentration of conjugated arctigenin was thirty times higher than the concentration of free
arctigenin. Investigation of the content of the intestinal tract of rats that were fed with arctiin,
demonstrated that 2-(3”, 4”-dihydroxybenzyl)-3-(3’, 4’-dimethoxybenzyl)-butyrolactone was formed.
Incubation of 2-(3”, 4”-dihydroxybenzyl)-3-(3’, 4’-dimethoxybenzyl)-butyrolactone with liver cytosol of
rats, in the presence of S-adenosylmethionin, demonstrated that it was rapidly and completely 3”-
methylated to arctigenin by COMT (in only three minutes) (Blaschek 1998).
Figure 7: Possible pathway for the transformation of actiin (1) by human intestinal bacteria (Xie 2003).
Pharmacokinetic interactions with other medicinal products
In vitro
data:
An ethanolic (55% v/v ethanol:water) extract of
Arctium lappa
L. root was tested for possible inhibition
of CYP3A4, CYP19 and CYP2C19. Chlorogenic acid was used as a marker substance in the extracts.
Assessment report on
Arctium lappa
L., radix
EMA/HMPC/246764/2009
Page 20/26
Finally, the activity of an equivalent of 800 µg herbal substance was tested against 2 ng of
ketoconazole.
Among 10 plant extracts tested, the extract from the root of
Arctium lappa
L. was only a weak inhibitor
of CYP3A4 (10
th
place on 10), CYP19 (9
th
place on 10) and CYP2C19 (4
th
place on 4). There were
batch-to-batch differences with inhibition percentages varying between 11% and 33% (Scott 2006,
Williamson 2009).
3.3.
Overview of available toxicological data regarding the herbal
substance(s)/herbal preparation(s) and constituents thereof
Carcinogenicity
Carcinogenicity data on the roots of
Arctium lappa
L
.
come from a study by Hirono (1977). Six male
and six female rats were treated with a diet containing 33% of roots of
Arctium lappa
L. for 120 days.
No tumors were detected in any animal (De Smet 1993).
Reproductive toxicity
Matsui reported no affection on fertility of female mice when injected twice a day for five days
subcutaneously with an extract of
Arctium lappa
L. This extract was prepared by boiling unspecified
plant parts in water (De Smet 1993).
Genotoxicity
No tests on preparations from
A. lappa
, root have been performed. Aqueous and methanolic extracts
from fruits of
Arctium lappa
L. were screened for mutagenicity in
Salmonella typhimurium
strains TA
98 and TA 100 and
Bacillus subtilis
strains H17 Rec
+
and M45 Rec
-
. The aqueous extract gave a
positive response in
Salmonella typhimurium
TA 98 only in the presence of S9 mix, whereas the
methanolic extract was positive in the
Bacillus subtilis
rec-assay (De Smet 1993).
Yamamoto (1982) tested an aqueous or methanolic extract from
Arctium
fruits in
Salmonella
typhimuriu
m TA 98 and TA100 in the absence or presence of rat liver S-9 mix. No mutagenicity was
observed (De Smet 1993).
In vivo
studies have shown that fresh or boiled plant juice from
Arctium lappa
L. may cause a
significant reduction in DMBA(7,12-dimethylbenz(a)anthracene)-induced chromosome aberrations
(Barnes 2007).
The relevance of those studies for the assessment of preparations of the root is unclear.
3.4.
Overall conclusions on non-clinical data
Pharmacology
Arctium lappa
L. is recommended in various conditions, mostly based on long-term use and
experience. A lot of
in vitro
studies in cell cultures, microbial strains and biochemical models and
in
vivo
studies in rats and mice have already been performed. Despite these efforts, the
pharmacodynamic profile of
Arctium lappa
L. is not fully established.
No safety concerns are originating from the available data on the pharmacological profile.
Pharmacokinetics
From
in vitro
and
in vivo
experiments in an intestinal environment there is evidence for phase II kinetic
activity of actiin. From
in vivo
experiments (rats) Tmax for arctigenin and excretion parameters could
be determined. These data have no relevance for the traditional use of
A. lappa
, radix. The reported
actions on the Cytochrome-system do not present a reason for concern.
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Arctium lappa
L., radix
EMA/HMPC/246764/2009
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Toxicology
Very limited studies did not result in any signs of
in vivo
carcinogenicity (rats). Because studies did
focus on other parts of the plant, the genotoxicity and toxicity on reproduction cannot be fully assessed
for the root and root-derived preparations. However, the available data do not point to any serious
concern with respect to safety.
4.
Clinical Data
4.1.
Clinical Pharmacology
4.1.1.
Overview of pharmacodynamic data regarding the herbal
substance(s)/preparation(s) including data on relevant constituents
No data available.
4.1.2.
Overview of pharmacokinetic data regarding the herbal
substance(s)/preparation(s) including data on relevant constituents
No data available.
4.2.
Clinical Efficacy
4.2.1.
Dose response studies
No data available.
4.2.2.
Clinical studies (case studies and clinical trials)
No data available.
‘Essiac’ (see section 1.1 and 1.2) has been used for breast-cancer treatment, secondary prevention,
improving quality of life and controlling negative side-effects of conventional breast-cancer treatment.
A retrospective cohort study in 510 women with a diagnosis of primary breast cancer demonstrated
that ‘Essiac’, although it appears to be safe at the doses taken (total daily dose 43.6 ± 20.8 ml which
correspond to the labelling of most ‘Essiac’ products), does not have a significant effect on HR-QOL
(health-related quality of life) or mood states such as anxiety or vigor (Zick 2006).
‘Essiac’ may contain a lot of preparations, usually insufficiently specified, which provides additional
confusion. Well-defined trials testing ‘Essiac’ or individual herbal components are necessary to derive
any sound conclusions (Ulbricht 2009).
4.2.3.
Clinical studies in special populations (e.g. elderly and children)
No data available.
4.3.
Overall conclusions on clinical pharmacology and efficacy
There is a lack of clinical research assessing the effects of
Arctium lappa
L. in monopreparations and
controlled clinical trials are absent. However, there is a long-standing, consistent traditional use in
dermatological and urological complaints.
Assessment report on
Arctium lappa
L., radix
EMA/HMPC/246764/2009
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5.
Clinical Safety/Pharmacovigilance
5.1.
Overview of toxicological/safety data from clinical trials in humans
No data available.
5.2.
Patient exposure
No exact data on patient exposure are available. However, the long-standing use and the inclusion in
many standard handbooks of Phytotherapy and in official pharmacopoeias and compendia make a wide
exposure plausible.
5.3.
Adverse events and serious adverse events and deaths
Adverse events
Dermatological reactions
The rough hairs of the above-earth parts of
Arctium lappa
L. can result in mechanical irritation of the
skin (De Smet 1993).
Rodriguez (1995) reported three cases of contact dermatitis caused by
Arctium lappa
L. plasters
applied for anti-inflammatory purposes. They describe two men in their thirties and one 14-year-old
girl who had an erythematous exudative dermatitis after applying a plaster of
Arctium lappa
L.
There are no unambiguous reported cases of contact allergy to
Arctium lappa
L., though Rodriguez
(1995) reports it as an irritant substance without further details; however, the root as well as aerial
parts may be involved. It should be noted that urticaria has been reported after the topical use of the
leaves (see 1.1), however this reaction has been attributed as a "beneficial effect" (Leclerc 1966).
Allergic reactions are likely to be associated with the presence of sesquiterpene-lactones such as
arctiopicrin that is a weak sensitizer. Also dehydrocostuslactone, which is found in
Saussurea lappa
Clarke and Laurel oil, is well-known to cause allergic reactions (Hausen 1997). For this reason, a cross-
reaction with other
Asteraceae
can be assumed.
Ocular reactions
The rough hairs of
Arctium lappa
L. fruit may hook on clothing. Within the bur and attached to seed
pods,
Arctium lappa
L. has thousands of tiny barbed needles. If these needles imbed in the
conjunctiva, it may cause serious ocular reactions. Because they are very small, they are often missed
by doctors who are not familiar with the plant. An
Arctium lappa
L. caused ophthalmic irritation can be
recognised by the presence of linear scratch marks running in random directions on the cornea. The
needle tip causes direct abrasion every time the eyelid moves, thus causing serious damage. The
toxicity of a water soluble noxious agent may also play a role, which is suggested from animal tests.
An aqueous extract caused severe reactions, which were not observed following the injection of an oily
extract (De Smet 1993).
Animal-data
For dogs (especially long-hair breeds) and occasionally cats who run free in areas with
Arctium lappa
L.
the so called ‘burr tongue’ is commonly seen. The hair-like shafts of
Arctium lappa
L. have a little hook
on the tip by which the bur sticks to the fur of the animals. When an animal wants to remove this bur,
mostly by licking and chewing, some of the shafts may penetrate the membrane of the mouth and
tongue. This causes fibrous granulation (De Smet 1993).
Assessment report on
Arctium lappa
L., radix
EMA/HMPC/246764/2009
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Serious adverse events and deaths
Anaphylactic shock
Only one case of serious allergy to
Arctium lappa
L
.
is known. A 53-year-old Japanese man was
diagnosed to be in anaphylactic shock after eating boiled burdock root. His symptoms were redness
over his entire body, dyspnea and a low blood pressure of 64/29 mmHg. He recovered after
subcutaneous injection of epinephrine (1 mg) and an intravenous drip of lactate Ringer’s solution
containing hydrocortisone (100 mg) and dexamethasone (8 mg). Sasaki (2003) warns of similar cases
world-wide because burdock root is often used as an ingredient in tea or folk medicines in Western
countries (Sasaki 2003).
Some remarks have to be made on this case. Apart from burdock, the patient consumed also carrot
and curry with his rice. Skin prick tests revealed an allergic predisposition for burdock but also for
carrot (not for curry). Boiled as well as raw plant materials were used for allergy testing (Sasaki 2003).
Atropine like poisoning
De Smet (1993) mentions anticholinergic poisoning, due to adulteration or contamination with
belladonna root. This is also reported by Barnes (2007). The patient exhibited symptoms of atropine-
like poisoning after ingestion of
Arctium lappa
L. tea. Atropine is not a constituent of
Arctium lappa
L
.
,
but analysis showed that the tea was contaminated with an herbal source of solanaceous alkaloïds,
possibly belladonna root.
Contamination with
Atropa belladonna
L. is reported in many handbooks. Older roots and roots that
show a blue colour after treatment with iodine solutions (indicator for Radix Belladonnae) may not be
used for this reason. According to Blaschek (1998), also substitution with
Symphytum officinale
L. or
Rumex obtusifolius
L. may also occur.
5.4.
Laboratory findings
No data available.
5.5.
Safety in special populations and situations
It has been reported that
Arctium lappa
L. may cause uterine stimulation and therefore the use of
Arctium lappa
L. should be avoided during pregnancy and lactation (Barnes 2007). However, no case
reports or pharmacological studies that would support this assumption were found.
Intrinsic (including elderly and children) /extrinsic factors
None known.
Drug interactions
According to Barnes (2007), there are no documented interactions. Nevertheless, the authors warn
with respect to the potential interactions with other medicines, particularly those with similar or
opposing effects. Apart from this general statement, no clinical evidence is available; consequently, no
warning should be included in the monograph.
Arctium lappa
L. has also been associated with diuretic effects. Nothing is known about possible
additive effects when
Arctium lappa
L. is taken concomitantly with diuretic drugs. No statement is
needed in the monograph.
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Arctium lappa
L., radix
EMA/HMPC/246764/2009
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Tinctures of
Arctium lappa
L. may contain high concentrations of alcohol and may lead to vomiting if
used with disulfiram. This aspect is covered in the monograph by a general warning on ethanol
containing preparations.
Use in pregnancy and lactation
In vivo
uterine stimulant action has been reported. In view of this and the lack of toxicity data, the use
of burdock during pregnancy and lactation is not recommended (Barnes 2007). However, as neither
case reports on toxicity nor pharmacological studies demonstrating an effect on the uterus have been
found, the standard warning has been included in the monograph; i.e. that the use is not
recommended due to insufficient data.
No case of overdose has been reported.
Drug abuse
Drug abuse has not been reported.
Withdrawal and rebound
None reported.
Effects on ability to drive or operate machinery or impairment of mental ability
No studies on the effect on the ability to drive and use machines have been performed.
5.6.
Overall conclusions on clinical safety
Under the conditions of use mentioned in the monograph
A. lappa
, root can be considered as safe.
There is evidence for local irritation, due to the barbed needles on the bur of the plant. These are not
relevant for the root. Allergic reactions may occur; probably due to sesquiterpene-lactones. The quality
of the herbal substance should be checked rigorously as contamination with
Atropa belladonna
may
occur.
6.
Overall conclusions
Some constituents of
Arctium lappa
L. are well investigated and documented. Many authors have
described various pharmacological activities of
Arctium lappa
L. seed extracts or isolated constituents
in animals or
in vitro
.
Despite their long tradition and their widespread use, there are no data available from controlled
clinical studies using herbal preparations containing
Arctium lappa
L. root. In conclusion,
Arctium lappa
L. root preparations can only be considered for traditional use. More clinical research is needed to
confirm the pharmacological properties.
The monograph on
Arctium lappa
L. is restricted to the root as there is no documented use of
medicinal products from the leaves and there is insufficient evidence on the traditional use of the
seeds.
Assessment report on
Arctium lappa
L., radix
EMA/HMPC/246764/2009
Page 25/26
Benefit-risk assessment
Quality
There is no Arctii lappae radix monograph in the European Pharmacopoeia. The most recent official
monograph comes from DAC 2008. Contamination with
Atropa belladonna
root has been mentioned, as
well as exchanges with
Symphytum officinale
L. and
Rumex obtusifolius
L.
Conclusion: Contamination or adulteration of
Arctium lappa
root with serious health risks are possible
and need to be excluded by adequate quality control in the framework of a registration procedure.
Safety
There are very few side effects due to root preparations. The main risks are allergic reactions
associated with sesquiterpene-lactones. There is one case of an anaphylactic reaction after eating
boiled burdock. No overdoses with root preparations have been reported. Reproductive toxicity and
genotoxicity were tested with non specified preparations or plant parts other than the root. No
carcinogenicity was reported after feeding rats with root-enriched food; however this study does not
comply with current standards. Other possible effects (e.g. interference with antidiabetic medicines)
were seen in experimental conditions with plant parts other than root. There are no concerns about
interactions with conventional medicines.
Arctium lappa
root has been repeatedly associated with
antimutagenic activity
in vitro
. However, a list entry cannot be made as adequate tests on reproductive
toxicity, genotoxicity and carcinogenicity have not been performed with Arctii lappae radix.
Conclusion: Preparations of
Arctium lappa
root can be considered as safe but no list entry can be
prepared.
Efficacy
Therapeutic indications for herbal preparations of
Arctium lappa
root as given in the monograph are
based on more than 30 years traditional use in Europe but not supported by validated clinical
experience. Even open clinical observations are missing. The use in seborrhoeic skin conditions (ICD
L21, ATC D11AX) in urinary complaints and in stimulation of appetite is plausible on the basis of its
long-standing, consistent use in those indications as well as inclusion in standard handbooks and
official compendia. The diuretic use of herbal medicinal products with
Arctium lappa
root should not
replace conventional diuretics with antihypertensive and heart protective therapeutic effects. The use
in case of temporary loss of appetite must be considered as purely symptomatic, while it should not be
continuously used without a clear diagnosis.
Conclusion: Traditional therapeutic use of
Arctium lappa
is safe under the conditions addressed in the
monograph.
Annex
List of references
Assessment report on
Arctium lappa
L., radix
EMA/HMPC/246764/2009
Page 26/26
Source: European Medicines Agency
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