Guidelines for treatment of atopic eczema (atopic dermatitis) part i
Guidelines for treatment of atopic eczema (atopicdermatitis) Part I
J. Ring,†,‡,* A. Alomar,§ T. Bieber,– M. Deleuran,†† A. Fink-Wagner,‡‡ C. Gelmetti,§§ U. Gieler,––J. Lipozencic,††† T. Luger,‡‡‡ A.P. Oranje,§§§ T. Scha¨fer,––– T. Schwennesen,†††† S. Seidenari,‡‡‡‡D. Simon,§§§§ S. Sta¨nder,‡‡‡ G. Stingl,–––– S. Szalai,††††† J.C. Szepietowski,‡‡‡‡‡ A. Taı¨eb,§§§§§T. Werfel,––––– A. Wollenberg,†††††† U. Darsow,†,‡ For the European Dermatology Forum (EDF), and theEuropean Academy of Dermatology and Venereology (EADV), the European Task Force on Atopic Der-matitis (ETFAD), European Federation of Allergy (EFA), the European Society of Pediatric Dermatology(ESPD), and the Global Allergy and Asthma European Network (GA2LEN)
†Department of Dermatology and Allergy Biederstein, Christine Ku¨hne-Center for Allergy Research and Education (CK-CARE),Technische Universita¨t Mu¨nchen, Munich, Germany‡Division of Environmental Dermatology and Allergy, Helmholtz Zentrum Mu¨nchen ⁄ TUM, ZAUM-Center for Allergy andEnvironment, Munich, Germany§Department of Dermatology, Hospital de Sant Pau, Universitat Autonoma Barcelona, Barcelona, Spain–Department of Dermatology and Allergy, University Bonn, Bonn, Germany††Department of Dermatology, Aarhus University Hospital, Aarhus, Denmark‡‡EFA Project and Fundraising Officer, Konstanz, Germany§§Istituto di Scienze Dermatologiche, Universita` di Milano, Milano, Italy––Department of Psychosomatics and Psychotherapy, University of Gießen and Marburg GmbH, Gießen, Germany†††Department of Dermatology and Venereology, University Hospital Center Zagreb, Zagreb, Croatia‡‡‡Department of Dermatology, Competence Center Chronic Pruritus, University Hospital of Mu¨nster, Mu¨nster, Germany§§§Department of Pediatric Dermatology, Erasmus MC – Sophia Children’s Hospital, Rotterdam, The Netherlands–––Institute for Social Medicine, University Lu¨beck, Lu¨beck, Germany††††Deutscher NEURODERMITIS Bund (DNB), Hamburg, Germany‡‡‡‡Department of Dermatology, University of Modena and Reggio Emilia, Modena, Italy§§§§Department of Dermatology, Universita¨tsklinik fu¨r Dermatologie, Bern, Switzerland––––Department of Dermatology, University of Vienna, Vienna, Austria†††††Department of Dermatology, Heim Pa´l Children’s Hospital, Budapest, Hungary‡‡‡‡‡Department of Dermatology, Venereology and Allergology, Wroclaw Medical University, Wroclaw, Poland§§§§§Department of Dermatology and Pediatric Dermatology, Hoˆpital St Andre´, Bordeaux, France–––––Department of Dermatology and Allergy, Hannover Medical School, Hannover, Germany††††††Department of Dermatology and Allergy, Ludwig-Maximilian University, Munich, Germany*Correspondence: J. Ring. E-mail: [email protected]
The existing evidence for treatment of atopic eczema (atopic dermatitis, AE) is evaluated using the national standard
Appraisal of Guidelines Research and Evaluation. The consensus process consisted of a nominal group process and
a DELPHI procedure. Management of AE must consider the individual symptomatic variability of the disease. Basic
therapy is focused on hydrating topical treatment, and avoidance of specific and unspecific provocation factors.
Anti-inflammatory treatment based on topical glucocorticosteroids and topical calcineurin inhibitors (TCI) is used for
exacerbation management and more recently for proactive therapy in selected cases. Topical corticosteroids remain
the mainstay of therapy, but the TCI tacrolimus and pimecrolimus are preferred in certain locations. Systemic
immune-suppressive treatment is an option for severe refractory cases. Microbial colonization and superinfection
may induce disease exacerbation and can justify additional antimicrobial treatment. Adjuvant therapy includes UV
irradiation preferably with UVA1 wavelength or UVB 311 nm. Dietary recommendations should be specific and given
only in diagnosed individual food allergy. Allergen-specific immunotherapy to aeroallergens may be useful in
selected cases. Stress-induced exacerbations may make psychosomatic counselling recommendable. ‘Eczema
school’ educational programs have been proven to be helpful. Pruritus is targeted with the majority of the
recommended therapies, but some patients need additional antipruritic therapies.
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
A. Alomar has been speaker for Almirall, Astellas, Leti. T. Bieber has been advisor, speaker or investigator for ALK
Abello´, Astellas, Bencard, Galderma, Glaxo SmithKline, Leo, Novartis, Stallergenes. U. Darsow has been speaker,
investigator and ⁄ or been a member of advisory boards for Allergopharma, ALK Abello´, Bencard, GSK, Hermal, Novartis
Pharma, Stallergenes, Stiefel. M. Deleuran has been a speaker, participated in clinical trials and ⁄ or been a member of
advisory boards for Merck, Novartis, Astellas, Leo Pharma, NatImmune, Pergamum, Pierre Fabre and Janssen-Cilag.
A.-H. Fink-Wagner received honorarium from Pharmaxis and Chiesi during the last 3 years and was employed before
that by Nycomed. J. Ring has been advisor, speaker or investigator for ALK Abello´, Allergopharma, Almirall ⁄ Hermal,
Astellas, Bencard, Biogen-Idec, Galderma, Glaxo SmithKline, Leo, MSD, Novartis, Phadia, PLS Design, Stallergenes.
S. Sta¨nder was or is adviser, speaker and ⁄ or investigator for Aesca Pharma, Almirall ⁄ Hermal, Astellas Pharma,
Beiersdorf AG, Birken, Essex Pharma, GSK, Pierre Fabre, Maruho, 3M Medica, Mundipharma, Novartis Pharma,
Serentis, and Serono. Z. Szalai is investigator of clinical trials for Astellas, Novartis, Pfizer, Abbott, Pierre Fabre. A.
Taı¨eb has received consulting and clinical trial honoraria from Pierre Fabre, Astellas, Almirall ⁄ Hermal, Leo and Novartis.
T. Werfel has been advisor, speaker or investigator for ALK Abello´, Astellas and Novartis. A. Wollenberg has received
research funding and lecture honoraria from, conducted clinical trials for, or is a paid consultant to Astellas, Basilea,
GSK, Loreal, Merck, Novartis, MSD. Other authors declared no conflict of interest.
individuals) and subsequent increased susceptibility to
Atopic eczema (AE; atopic dermatitis, eczema, ‘Neurodermitis’ in
German speaking countries, endogenous eczema) is an inflamma-
• Obvious strong psychosomatic influence with an imbal-
tory, pruritic, chronic or chronically relapsing skin disease occur-
ance in the autonomic nervous system with subsequent
ring often in families with other atopic diseases (bronchial asthma
increased production of mediators from various inflam-
and ⁄ or allergic rhinoconjunctivis1).
matory cells (e.g. eosinophilic leucocytes).
Atopic eczema is one of the most common skin diseases which
In the management of AE these various pathogenic reactions
affects up to 20% of children and 1–3% of adults in most coun-
have to be considered in an individual approach regarding the
tries of the world.2 AE is often the first step in the development of
abnormal reactivity patterns found in the individual patient
other atopic diseases as rhinitis and ⁄ or asthma.
In the diagnoses of AE several criteria have been established.3,4
After establishing the diagnosis of AE, the severity of the disease
There is no pathognomonic laboratory biomarker for diagnosis of
has to be determined. The classical method is the ‘Scoring of
AE, since the most typical feature, the elevation of total or
Atopic Dermatitis’ (SCORAD) developed by the European Task
allergen-specific IgE levels in serum or the detection of IgE-
Force of Atopic Dermatitis (ETFAD). The SCORAD has been
mediated sensitization in the skin test, is not present in all individ-
modified by several authors.7 AE with a SCORAD higher than 40
uals suffering from AE; for this latter group the term ‘intrinsic’
is generally regarded as ‘severe’, whereas AE with a SCORAD
(non-IgE-associated) AE has been introduced to distinguish it
below 20 can be regarded as ‘mild’.
from ‘extrinsic’ (IgE-associated) forms of AE.5 This controversy in
It has to be mentioned that the majority of cases with AE can
terminology is going on until today1,6 and has practical implica-
be regarded as ‘mild’ with 10–20% of patients suffering from
tions with regard to specific avoidance strategies in the manage-
severe eczematous skin lesions7; this percentage seems to be higher
ment of this disease. In the aetiopathophysiology of AE several
in the adult AE population. In the following, the most important
aspects have to be taken into consideration:
strategies in management and medication will be briefly discussed.
Apart from strong genetic influence (80% concordance in
monozygous twins, 20% in heterozygous twins), there are charac-
teristic features in pathophysiology as follows:
The guideline committee decided that these guidelines should
• Immune deviation towards Th2 in the initiation phase
strictly concentrate on therapeutic regimens and omit longer
chapters on clinical entity, diagnosis or pathophysiology of the
• Deficient skin barrier function (‘dry’ skin) due to abnormal
lipid metabolism and ⁄ or epidermal structural protein forma-tion (filaggrin mutation, protease inhibitor deficiency, etc.)
• Abnormal microbial colonization with pathogenic organ-
The existing evidence-based National guideline from Germany,8
isms such as Staphylococcus aureus or Malassezia furfur
the HTA report9 as well as the position statement of the ETFAD10
(compared with Staphylococcus epidermidis in normal
were compared and evaluated using the national standard
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
Guidelines for treatment of atopic eczena
Appraisal of Guidelines Research and Evaluation (AGREE). The
to the last internal review. The comments of the participating soci-
committee decided that all the documents fulfilled enough criteria
eties were forwarded to the chapter authors and considered during
to be used as the base of the new evidence-based European
Guidelines on Treatment of Atopic Eczema.
These guidelines will require updating approximately every
Newer literature published after the German Guidelines8 and the
5 years. Based on new HTA reports the development of a S3
ETFAD Position Statement10 was searched using medline,
This guideline has been prepared for physicians, especially derma-
The evaluation of the literature focused on the efficacy of the ther-
tologists, paediatricians, general practitioners and all specialists
apeutic modality and was assessed with regard to the methodolog-
taking care of patients suffering from AE. Also patients and rela-
ical quality of the study according to the well-known criteria of
tives should be able to get reliable information and evaluation with
regard to evidence-based therapeutic modalities.
Based on the grade of evidence recommendations were classified
Basic treatment of disturbed skin barrierfunction and emollient therapy (‘skin care’)
The committee designated especially important areas as those
requiring consensus. The consensus process consisted of a nominal
Dry skin is one of the main symptoms of AE and part of the defini-
group process and a DELPHI procedure. Consensus conferences
tion. There is now scientific evidence in humans and mice of geneti-
were held in Berlin October 2009, Cavtat May 2010, Munich July
cally driven skin barrier anomalies that facilitate allergen
2010 and Goteborg October 2010, where the sections regarding
penetration into the skin with an increased proneness to irritation
consensus were discussed by the entire guidelines group following
and subsequent cutaneous inflammation. Filaggrin deficiency is the
best defined anomaly, which gives rise to a deficiency in small waterbinding molecules resulting from normal filaggrin catabolism.11
Besides that, a lack of stratum corneum intercellular lipids and an
According to the EDF standard operation procedure all European
inadequate ratio between compounds (cholesterol, essential fatty
dermatological societies were invited to review the guidelines prior
acids, ceramides) enhance trans-epidermal water loss leading to epi-dermal micro-fissuring. Barrier disruption leads to inflammation,and protease-antiprotease imbalance is a crucial intermediate step.12
The skin must be cleansed thoroughly, but gently and carefully to
get rid of crusts and mechanically eliminate bacterial contaminants
in the case of bacterial super-infection. Cleansers with or without
antiseptics (the duration of action of antiseptics is very limited,
thus mechanical cleansing is probably more important) in non-
irritant and low allergen formulas available in various galenic
forms (syndets, aqueous solutions) may be used. It is easier to
perform this first stage of gentle cleansing of skin on the nappy
mattress rather than directly in the bathtub in infants. A further
cleansing followed by a rapid rinse is performed in the bath(27–30°C). The short duration of the bath (only 5 min) and theuse of bath oils (last 2 min of bathing) are aimed at avoiding
Table 2 Classification of strength of recommendation
epidermal dehydration. Topical emollients are preferentially
applied directly after a bath or a shower following gentle drying
when the skin is still slightly humid.
Adding sodium hypochlorite to the bath-water seems very
important because of its bacterial count inhibiting activities. It
may be advised to every treatment in AE. A recently published
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
study13 showed that children who took a bath using half a cup
of bleach per full standard tub were relieved of their AE relateditching. The bleach apparently had very little odour. Salt baths
Short-term (3–6 weeks) Several studies in children (e.g. 23,24
may be beneficial because of removing the dead keratolytic
and one in a mixed children-adult population25 showed a variable,
material.14 In heavily impetiginized or ichthyotic skin salt baths
but consistent evidence of short-term steroid sparing effect in mild
Long-term maintenance therapy Maintenance of stable disease
The direct use of emollients on inflamed skin is poorly tolerated
can be obtained with emollients used twice weekly or more fre-
and it is better to treat the acute flare first. Emollients are the
quently in a subset of patients, after an induction of remission with
mainstay of maintenance therapy. Hydration of the skin is usu-
topical corticosteroids. Several studies derived comparable results
ally maintained by at least twice daily application of moisturizers
for intermittent emollient therapy and time to relapse, using com-
with a hydrophilic base, e.g. 5% urea. The use of barrier oint-
parable study designs in adults and children.26,27 Regimens for
ments, bath oil, shower gel, emulsions or micellar solutions
basic ⁄ maintenance therapy are still awaiting validation based on
enhancing the barrier effect is also recommended. The cost of
systemic reviews and a Cochrane review (Oranje in prep.).
high-quality (low in contact allergens) emollient therapies oftenrestrict their use because such therapies are considered to be
non-prescription drugs (except, e.g. Finland, where prescription
Emollients should be prescribed in adequate amounts and these
and reimbursement are usual) and the quantities required are
should be used liberally and frequently, e.g. for emollient
usually high (150–200 g per week in young children, up to
cream ⁄ ointment a minimum of 250 g per week. Emollient bath
500 g in adults). A better molecular and biochemical knowledge
oils and soap substitutes should also be used. In winter time more
of the skin in AE should provide access to barrier improving
lipid ingredients are preferable (3b, C).
topical agents. There is limited evidence-based proof for the use
A regular use of emollient has a short- and long-term steroid
sparing effect in mild to moderate AE. An induction of remissionwith topical corticosteroids is required first (2a, B).
Ingredients and possible risks of emollients
The rapid progress in better molecular and biochemical knowl-
Glycerol seems better tolerated (less smarting effect) than urea plus
edge on the predisposing AE background should provide access to
sodium chloride.16 Usually, the recommendation is to use emol-
scientifically designed barrier improving topical agents, which
lients immediately after bathing and soft pad drying. A small study
indeed correspond to a major part of the aetiologic treatment of
suggests that emollient applied alone without bathing have a
the disease and are not limited to a mere symptomatic one (4, D).
longer duration as measured by capacitance.17
Propylene glycol is easily irritating in young children aged less
than 2 years and should not be used in these young children.
There is evidence that the large preventive use of emollients con-
Many patients are desperate when they hear from their physicians
taining allergens such as peanut18 or oat19 may increase the risk of
that AE is not ‘curable’. It is important to explain the difference
skin sensitization and allergy. Only emollient preparations devoid
between the genetic predisposition towards hypersensitive and dry
of proteinaceous allergens and haptens (contact allergy) should be
skin which cannot be ‘cured’ today and the acute eczematous skin
used, especially in the most vulnerable age group before the age of
lesions which can very well be treated and disappear. The identifi-
cation of individual provocation factors is crucial in the manage-
Sole use of emollients without sufficient topical anti-inflam-
ment of AE and their avoidance allows longer phases of remission
matory therapy involves a considerable risk for disseminated
or total clearance of symptoms. In avoidance recommendations
bacterial and viral infection, which is already increased in AE
one has to distinguish between primary, secondary and tertiary
prevention measures. Among provocation factors, specific andnon-specific elicitors have to be distinguished.
Certain moisturizers could improve skin barrier function in
atopics and reduce skin susceptibility to irritants21. Lode´n et al.
Numerous factors and substances from the environment can irri-
found in a comparative study between a glycerol-containing cream
tate the sensitive skin of patients with AE and can elicit eczema
and placebo an improvement over time in both groups indicating
flares. They may be physical, like mechanic irritants (e.g. wool),
the importance of emollient treatment in AE. Another study in
chemical (acids, bleaches, solvents and water) or biological
adult AE patients suggested an effect of coconut oil on Staphylo-
(microbes) in nature. Information on unspecific irritants and their
role in aggravating eczema is a crucial prerequisite for long-term
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
Guidelines for treatment of atopic eczena
management of patients with AE. Here also the adequate skin care
environment. In high altitude mountain climate pollen counts
and hygiene procedures in cleansing and dressing have to be dis-
are usually lower than in the average living areas.
cussed with the patient (see also Part II, ‘Educational Program,Eczema School’).
Animal epithelia Many patients are already aware that contact
Negative effects of air pollutants upon the development and
with animals is leading to a deterioration of the skin symptoms.
maintenance of AE, like tobacco smoke or volatile organic com-
Although in former times avoidance of pets was a central feature
pounds (VOCs) in indoor environments and traffic exhaust in
in primary prevention recommendations for atopy, this has been
the outdoor air have to be mentioned. There is evidence from
modified as follows: cat epithelia exposure is regarded by most
epidemiological trials that exposure to indoor chemicals, such as
authors as a risk factor, so it should be avoided. There is no evi-
formaldehyde, increases skin barrier disturbance;28 a mixture of
dence that dogs increase the risk of AE in children. Once a patient
volatile organic compounds has been shown to increase the
is sensitized and allergic to a pet, avoidance is absolutely necessary.
intensity of atopy patch test (APT) reactions to aero-allergens in
There is no evidence that pet keeping has a preventive effect in
patients with AE.29 Exposure to traffic exhaust has been shown
primary prevention of AE among normal population.
to be associated with an increased risk to develop AE in pre-school children.30,31
Dietary recommendations See chapter ‘Dietary intervention’.
Exposure to environmental tobacco smoke measured as urinary
cotinin ⁄ creatinin ratio was associated with a significant elevated
Clothing and textiles Smooth clothing and avoidance of irritat-
risk to develop AE, which was especially pronounced in children
ing fabrics and fibres is essential in the avoidance of primary skin
irritation. Too occlusive clothing inducing heat sensations should
Avoidance strategies regarding tobacco smoke as well as traffic
be avoided. Early ear-piercing and use of nickel-releasing jewellery
exhaust exposure in young children have been introduced in the
has been found to be associated with a significantly elevated risk
recent S3 guideline for primary prevention of atopy in
of nickel contact allergy in young girls.42 Special recommenda-
Germany.33,34 Certain food ingredients like alcohol, additives or
tions have to be given in individual counselling programs with
vasoactive amines may also trigger eczematous skin flares35; see
regard to the choice of profession. There is common consensus
that occupations with marked skin-damaging activity or contactwith strongly sensitizing substances should be avoided by patients
Aeroallergens Aeroallergens have been shown to elicit eczema-
tous skin lesions. In a rather high percentage of patients with AE
There is some evidence that house dust mite avoidance strategies,
the APT is positive (30–50%).36 Most common airborne allergens
especially encasings, can reduce house dust mite and house dust
eliciting eczema are derived from house dust mites of the species
allergen content in indoor air and by that improve AE. The latter
Dermatophagoides pteronyssinus and D. farinae. Also mold expo-
is controversial, since some RCTs did not show this effect
sure in damp indoor environment has been found to be associated
There is evidence that house dust mite avoidance and high
House dust mites are living in a complex eco-system consisting
altitude climate may give benefit to patients suffering from AE
of air humidity, temperature and organic material. They accom-
pany humans and are most commonly present in dust from mat-
There is a rationale for using protective clothes (eczema
tresses or bedroom floors. Normal cleaning measures help only
overalls), although good studies are missing (–, D).
little in decreasing house dust mite allergen present in the room.
In spring and summertime pollen exposure may exacerbate AE
Encasings of mattresses and beddings protect humans from mites
in the air-exposed skin areas; pollen avoidance measures can be
contained in mattresses. There are also mite-proof pyjamas
(‘eczema overalls’). There are some studies showing a clear-cut
When classical patch tests are positive, relevant contact allergens
benefit from house dust mite avoidance strategies in the improve-
Rehabilitation programs in mite-free environments – like in
alpine climate – have shown to lead to significant and long-lasting improvement of AE.38–40 Pollen in the outdoor air also
can elicit flares of AE as has been shown in a nested case con-
Among food allergens, cow’s milk, hen‘s egg, wheat, soy, tree nuts
trol study in preschool children.41 Pollen avoidance is difficult
and peanuts are most frequently responsible for eczema or
under everyday conditions in most parts of Europe except
exacerbation in infancy.44 In older children, adolescents and adults
when air conditioning with pollen filters is used in the indoor
pollen related food allergy should be taken into account.45,46
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
Different types of clinical reactions to food have been described
• The drop-out-rate in AE studies is particularly high in
in patients with AE: Early reactions, such as urticaria, gastrointesti-
nal or respiratory symptoms occur within 120 min after the
• There is no convincing evidence that a milk- or egg-free
administration of the allergens. Late phase responses, manifesting
elimination diet is beneficial in general when unselected
as eczematous lesions, occur after 2–48 h or some days. After oral
groups of patients with AE were studied.
food challenge, about 50% of children with AE who reacted to
• There is no evidence for a benefit in the use of elementary
food showed both immediate and delayed reactions and 15%
or few food restricted diets in patients with AE.
showed worsening of eczema only.47 The personal history is often
A recently published systematic review identified a single pro-
not helpful predicting late reactions to food with a positive predic-
spective controlled study that supports the notion that a direct
tive value of only 30% as opposed to 80% for immediate reac-
elimination diet (in the study: egg exclusion) may be beneficial for
the course of AE in sensitized patients with clinical symptoms
Sensitizations to food can be identified by means of in vivo tests
[skin prick tests (SPT), prick–prick tests] and in vitro tests (serumspecific IgE). In addition, patch tests proved to be useful forstudying delayed food-related skin responses. In vitro tests are
valuable when SPT cannot be applied (e.g. dermographism or
Patients with moderate to severe AE should observe a diet elimi-
UV- and drug induced skin hypo-reactivity, eczema at the test
nating those foods that elicitated clinical early or late reactions
site, lack of compliance for SPT in infancy, etc.). Moreover,
upon controlled oral provocation tests (2b, B).
in vitro specific IgE to food allergens give better quantitative datafor the grade of sensitization which helps to estimate the proba-
bility of the risk of a clinical reaction (although precise decisionpoints are not available) and it offers the opportunity to test
single recombinant allergens which may have a better diagnostic
Effective topical therapy depends on three fundamental principles:
specificity than testing with food extracts for some foods (e.g.
sufficient strength, sufficient dosage and correct application. Topi-
omega-5-gliadin in wheat allergy, Gly m 4 in pollen-related soy
cal treatment should always be applied on hydrated skin, especially
when using ointments. The emollient should be applied first when
Atopy patch tests are performed with self-made food material
it is a cream, 15 min before the anti-inflammatory topical is
applied to the back with large test chambers for 48–72 h. Food
applied and when it is an ointment 15 min after. Patients with
APT are not standardized for routine use.48 So far, APTs have
acute, oozing and erosive lesions, and children in particular, some-
demonstrated to improve the accuracy of skin testing in the diag-
times do not tolerate standard topical application, and may first
nosis of allergy to cow’s milk, egg, cereals, and peanuts in AE
be treated with ‘wet wraps’ until the oozing stops. They are highly
patients.49–55 Whereas immediate-type reactions are associated
effective in acute eczema and improve tolerance. The use of wet-
with SPT positivity, delayed ones are related to positive responses
wrap dressings with diluted corticosteroids for up to 14 days
to APTs. However, food challenge is not replaced by patch test-
(usual is rather up to 3 days) is a safe crisis intervention treatment
of severe and ⁄ or refractory AE with temporary systemic bioactivity
The double-blind placebo-controlled food challenge is considered
of the corticosteroids as the only reported serious side-effects.60,61
the gold standard for diagnosing food allergy.57 In AE, the evalua-
Even without wet wraps, topical therapy is time consuming:
tion of delayed reactions after 24 or 48 h by trained personal is
patients should plan 30 min for one session. One well-conducted
mandatory as stated by a recent position paper of the EAACI.58
treatment per day is usually sufficient; oozing eczema may require
Challenge tests based on repeated exposure to food enable the
a few days with higher treatment frequency.
assessment of delayed adverse responses.49,50,54,55 The major flaw
By tradition, anti-inflammatory topical therapy has been
is that they do not offer the opportunity to exclude placebo reac-
administered to lesional skin only and has been stopped or tapered
tions and ⁄ or coincidental influences of other trigger factors of AE
down once visible lesions were cleared. This traditional, reactive
during the prolonged challenge period.
approach has in the last years been challenged by the proactive
Unfortunately, the effects of dietary interventions on the course
treatment concept, which is defined as a combination of prede-
of AE have been studied in a few controlled studies only so far.
fined, long-term, low dose, anti-inflammatory treatment appliedto previously affected areas of skin in combination with liberal use
In a systematic review9 eight randomized, controlled studies
of emollients on the entire body and a predefined appointment
studying the effect of an elimination diet on existing AE were
schedule for clinical control examinations.62 The first trial with
identified and summarized in the following way:
intermittent topical steroid use was published already in 1999.63
• Elimination diets are difficult to be performed even in a
The proactive, usually twice weekly treatment regimen is started
motivating atmosphere during a clinical study.
after all lesions have successfully been treated by an intensive, usu-
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
Guidelines for treatment of atopic eczena
ally twice daily treatment approach in addition to ongoing emolli-
pimecrolimus cream 1% combined with fluticasone were similar
ent therapy for previously unaffected skin. Clinical trial data are
available for a number of steroid products as well as for tacrolimus
In a recent paper, it has been observed that glucocorticoids
inhibited the double-stranded RNA (dsRNA)-induced release of
Application amount of topical anti-inflammatory therapy
thymic stromal lymphopoietin in the atopic cytokine milieu
should follow the finger-tip unit (FTU) rule. A FTU is the amount
at much lower concentrations than calcineurin inhibitors,
of ointment expressed from a tube with a 5-mm diameter nozzle
suggesting that they could be effective in the treatment of
and measured from the distal skin-crease to the tip of the index
AE when exogenous or endogenous dsRNA is involved in the
finger (0.5 g); this is an adequate amount for application to two
adult palm areas, which is approximately 2% of an adult body sur-face area.
Topical corticosteroids are important anti-inflammatory drugs to
be used in AE, especially in the acute phase (–, D).
Topical glucocorticosteroids are a first-line anti-inflammatory
Topical corticosteroids have a significant effect improving skin
treatment, applied on inflammatory skin according to the
lesions compared to placebo (1b, A).
needs (pruritus, sleeplessness, new flare). Numerous substances
Topical corticosteroids with an improved risk-benefit ratio are
are available in a variety of formulations. Evidence-based anti-
inflammatory effects in AE were reported by different investiga-
The efficacy of topical glucocorticosteroids (1b, A) can be
tors.26,63,65 With mild disease activity, a small amount of topical
increased by using wet wraps (1b, A).
corticosteroids twice to thrice weekly (monthly amounts in the
Proactive ‘therapy’, e.g. twice weekly application in the long-
mean range of 15 g in infants, 30 g in children and up to 60–90 g
term follow-up may help to reduce relapses (1b, A).
in adolescents and adults), associated with a liberal use of emol-lients generally allows a good maintenance keeping SCORAD val-
ues below 15–20. Such monthly amounts of even potent topical
Both TCI, tacrolimus ointment and pimecrolimus cream, are
steroids usually do not have adverse systemic or local effects.
licenced for topical eczema treatment. Various aspects of these
Topical corticosteroids are grouped by potency, which should
drugs have been reviewed in detail.73,74 The efficacy of both formu-
be known to prescribers. In addition, there are different genera-
lations has been demonstrated against placebo in clinical trials for
tions of substances, which may differ in their risk-benefit ratio.
short-term75,76 and long-term use of these substances.77,78 In addi-
Potent and very potent corticosteroids (Group III and IV) are
tion, proactive tacrolimus ointment therapy has been shown to be
more likely to cause depression of adrenal function than group I
safe and effective for up to 1 year in reducing the number of flares
(mild) and II (moderate strength) treatments, but their systemic
and improving the quality of life in adult patients and children.79,80
effects will decrease more quickly due to more rapid restitution
The anti-inflammatory potency of 0.1% tacrolimus ointment is
of the skin barrier.66 Itch is the key symptom for evaluation of
similar to a corticosteroid with intermediate activity,81 while the
response to treatment, and tapering should not be initiated
latter is clearly more active than 1.0% pimecrolimus cream.82
before the itch has disappeared. Dose tapering should be gradual
Safety data of both TCI have been reported in many clinical tri-
to avoid withdrawal rebound; tapering strategies consist of using
als, demonstrating the safety of these drugs in daily routine use.
a less potent corticosteroid on a daily base, or keeping a more
The most frequently observed side-effect is a transient warmth
potent one while reducing the frequency of application (intermit-
sensation or transient burning at the application site during the
tent regimen). One well-conducted, correctly dosed treatment per
first days of application.75,82 It starts about 5 min after each
day is sufficient.67,68 The most constructive way to spare steroids
application of the drug and may last up to 1 h, but intensity and
and avoid steroid-related side-effects is not to spare them during
duration typically decrease within 1 week to zero.83 Generalized
acute flares, but through consequent baseline emollient skin care
viral infections such as eczema herpeticum (EH) or eczema
combined with early anti-inflammatory intervention to stabilize
molluscatum (EM) have been observed during topical calcineurin
the disease and prevent treatment-intensive flares.69 Usually one
inhibitor treatment,84,85 but a high number of clinical trials failed
daily application of topical steroids is sufficient.
to demonstrate an increased frequency or showed only a transient
The special aspects and potential adverse effects of topical
increase (reviewed in86–89). In contrast with corticosteroids, none
corticosteroids in pregnancy are reviewed in a recent S3 guide-
of the TCI induces skin atrophy.90,91 This favours their use over
line.70 Twice weekly application of fluticasone significantly reduced
topical corticosteroids in delicate body areas such as the eyelid
the risk of relapses of eczema in a ‘proactive’ strategy.26,63,65
region, the perioral skin, the genital area, the axilla region or the
The combination of topical corticosteroids with topical calci-
inguinal fold and for topical long-term management. Two safety
neurin inhibitors (TCI) does not seem to be useful. At least in pae-
aspects of TCI regarding potentially increased malignancy rates are
diatric patients with severe AE, the efficacy and safety profile of
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
discussed from time to time in the scientific community and the
whom they are contraindicated. According to the latest knowledge,
media – lymphoma risk and white skin cancer risk. Clinical and
there is no scientific evidence of an increased risk for malignancy
preclinical data do not indicate an increased risk of the induction
due to a topical treatment with calcineurin inhibitors.94a
of lymphoma over a period of 6 years92 or photocarcinogenicityfor TCI,93,94 but since the continuous oral administration of the
calcineurin inhibitor cyclosporine is associated with an increased
TCI are important anti-inflammatory drugs to be used in AE
photocarcinogenicity risk in solid organ transplant patients, UV
protection e.g. with sunscreens has been advised.81 The interpreta-
TCI have a significant effect compared to placebo in short-term
tion of the lymphoma risk should consider the fact, that a diagno-
and long-term treatment of AE (1b, A).
sis of AD as such is associated with an increased risk for
TCIs are especially indicated in problem areas (face, intertrig-
lymphoma.92 A recent letter sent out on EMEA directive in 2012
nous sites, anogenital area; 1b, A).
from the manufacturing company of tacrolimus ointment to all
Proactive therapy with twice weekly application of tacrolimus
dermatologists in the EU could have induced again a feeling of
ointment may reduce relapses (1b, A).
potential long-term risk of malignancies, but in fact it did not
Effective sun protection should be recommended in patients
communicate any new safety data, and indeed reassured physi-
cians to follow the current label of tacrolimus ointment. Accordingto the latest knowledge, there is no scientific evidence of an
increased risk for malignancy due to a topical treatment with calci-
Itch is the most important clinical symptom in AE, with peculiar
neurin inhibitors.94a The use of TCI under wet wraps or on erosive
impact on emotional dimensions of perception as compared to
lesions may increase systemic absorption.
other pruritic dermatoses like urticaria. Concerning pruritus
The efficacy of long-term monotherapy with tacrolimus oint-
accompanying AE, few studies investigate the antipruritic effect
ment has been shown in children and adults.81,82 Less data are
only. In most studies, pruritus is part of the total symptom score
available for children under 2 years of age.95,96 Pimecrolimus
using the EASI and SCORAD. For example, topical and systemic
cream has been studied in infants and children in a combination
corticosteroids, TCI, cyclosporine and UV-irradiation have signifi-
regimen with topical corticosteroids,97,98 the latter being given if a
cant influence on pruritus while only single studies specifically
flare occurred. Both TCI are approved in the EU from 2 years of
investigate the relief of pruritus intensity (Table 3).
age and above. Highquality long-term safety data have recentlybeen published from a 4-year tacrolimus and 26 weeks pimecroli-mus study.99,100 The cost effectiveness of proactive therapy with
Table 3 Antipruritic therapies in AE. Recommendation for topi-
topical tacrolimus has been demonstrated for moderate AE and is
cal and systematical therapies based on clinical trials and expert
even higher in severe AE in a recent study with adult patients,100a
whereas the cost effectiveness of first-line treatment with TCI has
not been shown conclusively. However, in children with AE,
twice-weekly treatment with tacrolimus 0.03% ointment has been
observed to reduce the number of flares and to prolong time spent
free from flares with no additional cost in children with moderate
factors: avoidance of toolong and hot bathing,
AE, and may be cost-saving in those with moderate and severe
In addition, the long-term, effective treatment of patients with
AE may have a beneficial effect also on respiratory symptoms, and
serum IgE.103 In adults, long-term treatment with 0.1% tacrolimus
ointment appears to be at least as effective as a corticosteroid regi-
men for the trunk and extremities, and more effective in the face
Pimecrolimus, t*Ultraviolet light (NB-UVB)
and neck area. Both topical tacrolimus and corticosteroids increase
skin recall activity, and decrease serum IgE in patients with good
treatment response. Taken together, these results suggest that skin
inflammation in AE should be treated effectively, which could lead
to an improvement in the Th1 ⁄ Th2 balance in the skin, and to
long-term improvement in the severity of the AE.103,104
These drugs are recommended for use as second-line therapy
for the short-term and non-continuous treatment of AE in patients
AE, atopic eczema; t, topically; o, orally.
who do not respond adequately to topical corticosteroids or in
*As proven by randomized, controlled trials.
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
Guidelines for treatment of atopic eczena
Antipruritic therapy in AE is multidimensional treating the
study proved that Narrowband-UVB was more effective than
symptom itself, the contributing factors such as dry skin, inflam-
mation and the related scratch lesions. Therefore, several generalmeasures can be recommended (see ‘Basic treatment’). Based on
expert opinion, short-term relief of pruritus can be achieved by
There is evidence that UV-therapy can be used in AE to relieve
topicals containing urea, camphor or menthol preparations as well
pruritus. Narrow band UVB seems to be most preferable (2b, B).
as wet, cooling or fat-moist wrappings,61 wrappings with black tea,short and lukewarm showers. Unspecific physical modalities are
Cyclosporine A See ‘Systemic Immunosuppression’ (Part II).
described to be beneficial like acupuncture,105 and cutaneous fieldstimulation.106
Intravenous Immunoglobulin therapy See ‘Systemic Immuno-suppression’.
Anti-inflammatory therapies acting on pruritus
Mycophenolat mofetil See ‘Systemic Immunosuppression’.
Glucocorticosteroids Several studies describe the anti-inflam-matory effect of topical corticosteroids in AE, in which pruritus
was one parameter among others such as erythema, induration,scaling and excoriation (see chapter Topical Anti-inflammatory
Topical anaesthetics Local anaesthetics such as benzocaine, lido-
Therapy). In sum, these studies suggest that topical corticosteroids
caine, polidocanol as well as a mixture of prilocaine and lidocaine
have a rapid antipruritic effect and can also be used in ‘proactive’
are widely used as short-term effective topical antipruritics. In
therapy.107 No study focuses solely on the onset, mechanisms and
experimental studies, the antipruritic effect of local anaesthetics
duration of the pruritus relief in AE. However, it seems likely that
was demonstrated in AE118 but controlled clinical trials investigat-
the anti-inflammatory effect of glucocorticosteroids is responsible
ing the antipruritic effects of local anaesthetics in AE are pending.
to partly abolish pruritus.108 This also holds true for systemic
Case series described the efficacy of a combination of polidocanol
glucocorticosteroids, for which no specific studies on an anti-itch
and 5% urea.119 In children with AE, the combination showed a
pruritus improvement of 30% in comparison with an emollient.120None of these substances is licenced for AE in Europe.
There is evidence that topical corticosteroids can be used in the
initial phase of AE exacerbation to control pruritus (1b, A).
Although there is evidence that short-term application of topicallocal anaesthetics may reduce itch sensation in AE (4, C), routine
Interferon (IFN) gamma Interferon gamma appears to have a
clinical use in AE cannot be recommended as an adjuvant antipru-
beneficial effect on pruritus in AE.109 In a double-blind study, pru-
ritus was reduced by 50% even 1–2 years after long-term treat-ment with recombinant human interferon gamma.110
Cannabinoid receptor agonist Topical cannabinoid receptor ag-onists have been described to exhibit antipruritic and analgesic
properties. Experimentally induced pain, itch and erythema could
There is evidence that systemic IFN gamma influences AE itch,
be reduced by application of a topical cannabinoid agonist.121 One
however, therapeutical use was not further investigated following
cosmetic product containing the cannabinoid agonist N-palmitoy-
lethanolamin was used in a multicentric, large cohort, open labelstudy as adjuvant treatment in AE.25 2456 patients including over
inhibitors Topical calcineurin inhibitors relieve
900 children applied the cream twice daily. Pruritus and the need
significantly pruritus in AE. Itch is completely relieved after the
to use corticosteroids were reduced up to 60%.
first days of treatment in adults and children. Studies report ofrelief even 3 days of topical application of tacrolimus111,112 and
There is preliminary evidence that topical N-palmitoylethanolaminmay be effective as an adjuvant antipruritic therapy in AE, but fur-
ther trials are needed before an evidence based recommendation
There is evidence that TCI can be used in AE until clearance of
Capsaicin Capsaicin, a naturally occurring alkaloid and the
UV therapy UV irradiation relieves pruritus in AE demonstrated
principal pungent of hot chilli peppers, has been advocated to be
in a study that compared UVB to placebo treatment.115 Also a
antipruritic in various dermatoses. Repeated topical application of
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
capsaicin releases and prevents specifically the reaccumulation of
randomized studies in AE. A dosage of 10 and 20 mg each once
neuropeptides in unmyelinated, polymodal C-type cutaneous
per day showed significant relief of pruritus in three studies.131–133
nerves. Capsaicin exerts its functions via binding to a capsaicin-
In open label trials and one double-blind, placebo-controlled
specific receptor, i.e. the transient receptor potential channel
study trial, the only orally active mu-opioid antagonist naltrexone
vanilloid (TRPV1) which is located on free nerve endings.
25–150 mg per day showed considerable antipruritic effects.134,135
Concerning AE, experimental studies122 and case series123 report
None of these substances is currently licenced for treatment of
on clear itch reduction. No controlled study was performed as of
Although there is evidence that opioid receptor antagonists nal-
There is preliminary evidence that capsaicin is useful in the treat-
trexone and nalmefene may reduce AE itch (1b, A), there is insuf-
ment of AE itch but further trials are needed before an evidence
ficient data to recommend routine use of these substances in AE.
based recommendation can be given (4, B).
Topical doxepin Five percent doxepin cream exhibited antipru-
Selective serotonin reuptake inhibitors The antipruritic effect
ritic effects in controlled studies in AE.124 However, topical doxe-
of the selective serotonin reuptake inhibitor paroxetin and fluvox-
pin therapy is not licenced and not used in any European country
amin was investigated in an open label trial in dermatological
due to an increased risk of contact allergy, especially when the
patients. Single patients with pruritus due to AE were included
which responded with considerable reduction of pruritus. In thesepatients, the pruritus was reduced about half of intensity (maximal
antipruritic effect score, 45.0 ± 7.1%).136
At the moment there is not enough RCT evidence to support theuse of doxepin in the treatment of AE itch (2b, B).
At the moment there is not enough RCT evidence to support the
Topical mast cell stabilizers Mast cell mediators such as
use of selective serotonin reuptake inhibitors paroxetine and flu-
tryptase and histamine contribute to induction of pruritus in AE.
voxamine in the treatment of AE itch (4, C).
Accordingly, the application of mast cell degranulation inhibitorsor stabilizers seems reasonable. However, in a multicenter, double-
blind, placebo-controlled trial applying 3% hydrogel formulation
Antihistamines have been used for decades, in an attempt to relieve
of tiacrilast (mast cell inhibitor) against vehicle in atopic dermati-
pruritus in patients with AE. However, only a few randomized
tis, there was no significant improvement of pruritus.125 In
controlled trials have been conducted and they have in the majority
another study, pruritus in children with AE responded to topical
shown only a weak or no effect in decreasing pruritus.137–142
sodium cromoglycate,126 which was proven by a recent placebo-
The first generation of sedative antihistamines, such as hydroxy-
zine, clemastine fumarate and dimetinden maleate, may allow abetter sleep pattern in acute situations with exacerbations of eczema
(evidence level D). Concerning the newer non-sedating antihista-
At the moment there is not enough RCT evidence to support the
mines, single studies using loratadine, ceterizine or fexofenadine
use of mast cell stabilizers in the treatment of AE itch (2b, B).
demonstrated no or only a weak relief of pruritus in AE143–145. Asignificant, but clinically small, antipruritic effect of fexofenadine
Leukotriene receptor antagonists Preliminary studies showed
60 mg twice daily has been described.108 An effect on itch of a high
reduction of pruritus in patients with AE during treatment with
dosage of 20–40 mg ceterizine daily has been observed, but this
the leukotriene receptor antagonists zafirlukast and zileuton.128–130
effect was primarily attributed to sedation.144
However, due to a high rate of side-effects the substances were not
Diepgen et al.146 reported in infants with severe AE acorticoste-
developed to regular therapies of AE.
roid sparing effect of ceterizine and judged this as an indirect mea-sure for the efficacy of ceterizine on pruritus. Murata et al.147
compared in patients with pruritic diseases (including eczema
At the moment there is not enough RCT evidence to support the
cases) effects of sedating and non-sedating antihistamines: similar
safe use of leukotriene receptor antagonists in the treatment of AE
effects on itch intensity were seen, but only non-sedating antihista-
mines reduced significantly the impairment in work productivityand daily activity.
Opioid receptor antagonists naltrexone and nalmefene The
In general, antihistamines are safe to use, also for a long period
mu-opioid receptor antagonist nalmefene was applied in controlled,
of time,148 and the major advantage seems to be relief of the symp-
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
Guidelines for treatment of atopic eczena
toms of co-morbidities such as allergic asthma, rhino-conjunctivi-
The use of silver-coated textiles and silk fabric with the durable
tis, urticarial dermographism and urticaria. Topical antihistamines
antimicrobial finish AEGIS ADM 5772 ⁄ S can reduce S. aureus col-
have no effect on itch beyond that of their cooling vehicles.
onization and eczema severity.164–166 These newer options are still
under investigation. Of note, there is some concern about the
There are limited data for the antipruritic effect of antihista-
safety of silver-coated textiles in infants and toddlers.
mines (H1-antagonists) in AE, and the effect of both first and sec-
Secondary infections with yeasts, dermatophytes or streptococ-
ond generation antihistamines on pruritus, in patients suffering
cal infections have also been implicated as trigger factors in AE.167
Intense erythema in skin folds of children with a flare of AE maywarrant a search for streptococcal skin infection. In general, signs
of secondary infections should be treated if present. Antimycotics
There is not enough evidence to support the general use of both
are proposed for the treatment of ‘head and neck’ variant of AE,
first and second generation antihistamines (H1-antagonists) for
often associated with Malassezia sympodialis superinfection
treatment of pruritus in AE (1b, A).
(recently reviewed by Darabi et al.168 Systemic ketoconazole169and topical ciclopiroxolamine170 have been shown to improve
eczema significantly within 4 weeks in placebo-controlled trials in
A number of defects in innate cutaneous immunology may
patients with ‘head-neck-shoulder dermatitis’. Instead of keto-
explain the high rate of cutaneous colonization with Staphylococ-
conazol, other imidazole derivates (fluconazol or itraconazol) are
cus aureus (up to 90% in moderate to severe eczema) in
proposed nowadays due to a better benefit : side effect ratio.
AE.149,150 There is evidence for an association of S. aureus-derived
Viral infections are occurring more frequently in AE patients
exotoxins including superantigens and pore forming haemolysins
than in normal individuals, with a tendency to disseminated,
with disease exacerbation,151–153 reviewed by De Benedetto
widespread disease and named after the causative virus as eczema
et al.149 and Niebuhr and Werfel150 supporting early observations
molluscatum, eczema vaccinatum or EH.20 EH has been described
that the density of S. aureus colonization in AE is significantly
following corticosteroid and calcineurin inhibitor therapy, but
correlated with clinical severity,154 and that patients with severe
recent data indicate that patients with severe, untreated AE, a high
AE may improve (but not be cured) by antistaphylococcal treat-
total serum-IgE and early onset of AE are at risk for EH, whereas
ment.155 In severe exacerbations systemic antibiotic treatment
pretreatment with topical corticosteroids does not imply a risk.171
The mainstay of EH therapy is prompt systemic antiviral chemo-
In general, improving eczema with anti-inflammatory regimen
therapy with i.v. aciclovir, but a number of alternative treatment
(i.e. TCS, TCI and UV) decreases staphyloccocal colonization. This
led to the clinical concept that patients with high numbers of colo-nizing S. aureus can benefit from combination treatment with cor-
ticosteroids and antimicrobial treatment, in most cases using
Oral antibiotics have no benefit on the skin condition in AE as
topical antiseptics like triclosan, chlorhexidine or cristal violet
long as skin lesions are not obviously superinfected (1b, A).
0.3%.156,157 In addition, a combination of natriumhypochlorite in
A short-term treatment with systemic antibiotics may be benefi-
baths with antibiotics has recently been published to have minor
cial if the skin is obviously superinfected with bacteria (2b, B).
to moderate effects on eczema in children with AE.13 However,
There is evidence from open observational studies only that
formal evidence on beneficial effects of topical antiseptics coming
antiseptic substances are beneficial for the treatment of AE (4, C).
from prospective controlled studies is still not available. A recent
An antimycotic therapy may be efficient in AE patients suffering
Cochrane review did not find any benefit for antibacterial soaps
from the ‘head and neck’ variant (2b, B).
(1 trial, 50 participants), or antibacterial bath additives (2 trials, 41
Topical glucocorticosteroids or calcineurin inhibitors reduce the
participants), or topical antibiotics ⁄ antiseptics (4 studies, 95
colonization rate of Staphylococcus aureus in AE (4, C).
Antiseptic textiles have a moderate clinical effect on AE (2b, B).
Apart from specific indications such as overt secondary infection
The long-term application of topical antibiotics is not recom-
or presence of beta-hemolytic streptococci159,160 or from visual
mend due to the risk of increasing resistances and sensitizations (the
superinfections of the skin with S. aureus, treatment of eczema
latter being relevant for a subgroup of topical antibiotics only; –, D).
with antibiotics had no effect in regards to clinical improvement
EH should be treated without delay using systemic antiviral
and sparing of steroids161 and should therefore not be performed.
therapy, such as systemic aciclovir (4, D).
Besides being not effective on the severity of eczema, antibioticeradication of S. aureus as a long-term strategy bears the risk of
increasing prevalence of antibiotic resistance.162,163 Particularly,
The work was supported by Christine Ku¨hne-Center for
topical antibiotics should not be used for longer periods in the
Allergy Research and Education (CK-CARE) Davos, Munich,
Journal of the European Academy of Dermatology and Venereology ª 2012 European Academy of Dermatology and Venereology
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∗Hadassah Medical Organization, [email protected]†Rutgers University, Newark N.J., [email protected] c 2006 The Berkeley Electronic Press. All rights reserved. Abstract Increased global terrorism has given rise to unique medical requirements that may be de-scribed as terror medicine. Using Israeli experience as a reference base, this paper notes fourbroad areas of ter