AK GUIDELINES .pdf

Transcript

Received: 29 August 2023 | Accepted: 23 January 2024

DOI: 10.1111/jdv.19897

GUIDELINES

European consensus-­based interdisciplinary guideline for
diagnosis, treatment and prevention of actinic keratoses,
epithelial UV-­induced dysplasia and field cancerization on
behalf of European Association of Dermato-­Oncology, European
Dermatology Forum, European Academy of Dermatology and
Venereology and Union of Medical Specialists (Union Européenne
des Médecins Spécialistes)

Lidija Kandolf1 | Ketty Peris2,3 | Josep Malvehy4 | Klara Mosterd5,6 |
7,8 9 7,8
Markus V. Heppt | Maria Concetta Fargnoli | Carola Berking | Petr Arenberger10 |
Matilda Bylaite-­Bučinskiene11 | Veronique del Marmol12 | Thomas Dirschka13,14 |
Brigitte Dreno15 | Ana-­Maria Forsea16 | Catherine A. Harwood17 | Axel Hauschild18 |
Ida Marie Heerfordt19 | Roland Kauffman20 | Nicole Kelleners Smeeths5,6 |
Aimilios Lallas21 | Celeste Lebbe22 | Ulrike Leiter23 | Caterina Longo24 |
1 25 4 26
Željko Mijušković | Giovanni Pellacani | Susana Puig | Philippe Saiag |
27 28 29 30
Mirna Šitum | Eggert Stockfleth | Carmen Salavastru | Alexander Stratigos |
31 23
Iris Zalaudek | Claus Garbe | on behalf of European Association of Dermato-­Oncology,
European Dermatology Forum, European Academy of Dermatology and Venereology and Union of
Medical Specialists (Union Européenne des Médecins Spécialistes)

Correspondence
Lidija Kandolf, Department of Dermatology, Abstract
Faculty of Medicine, University of Defence, A collaboration of multidisciplinary experts from the European Association of
Military Medical Academy, Belgrade, Serbia.
Email: [email protected] Dermato-­Oncology, the European Dermatology Forum, the European Academy
of Dermatology and Venereology, and the European Union of Medical Specialists
was formed to develop European recommendations on AK diagnosis and treatment,
based on current literature and expert consensus. This guideline addresses the epi-
demiology, diagnostics, risk stratification and treatments in immunocompetent as
well as immunosuppressed patients. Actinic keratoses (AK) are potential precursors
of cutaneous squamous cell carcinoma (cSCC) and display typical histopathologic
and immunohistochemical features of this malignancy in an early stage. They can
develop into cSSC in situ and become invasive in a low percentage of cases. AK is the
most frequent neoplasia in white populations, frequently occurring within a cancer-
ous field induced by ultraviolet radiation. Since it cannot be predicted, which lesion
will progress to cSCC and when treatment is usually recommended. The diagnosis of

For Affiliation refer page on 18

© 2024 European Academy of Dermatology and Venereology.

J Eur Acad Dermatol Venereol. 2024;00:1–24.  wileyonlinelibrary.com/journal/jdv | 1
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2 |    EUROPEAN GUIDELINE FOR TREATMENT OF AK

AK and field cancerization is made by clinical examination. Dermatoscopy, confocal
microscopy, optical coherence tomography or line-­field confocal-­OCT can help in
the differential diagnosis of AK and other skin neoplasms. A biopsy is indicated in
clinically and/or dermatoscopically suspicious and/or treatment-­refractory lesions.
The choice of treatment depends on patients' and lesion characteristics. For single
non-­hyperkeratotic lesions, the treatment can be started upon patient's request with
destructive treatments or topical treatments. For multiple lesions, field cancerization
treatment is advised with topical treatments and photodynamic therapy. Preventive
measures such as sun protection, self-­examination and repeated field cancerization
treatments of previously affected skin areas in high-­risk patients are advised.

I N T RODUC T ION Scope

Societies in charge This guideline was developed to assist clinicians in diagnos-
ing and treating patients with epithelial dysplasia, including
This guideline was developed on behalf of the European AK. In recent years, significant rise of incidence of keratino-
Dermatology Forum (EDF). The European Association of cyte cancers is evident, leading to the increased burden on
Dermato-­Oncology (EADO) coordinated the authors' con- the society. Also, advances were made in understanding of
tributions as part of its Guideline Program in Oncology keratinocyte dysplasia, and the concept of field cancerization
(GPO). The editors and coordinators responsible for the was introduced and adopted by the dermatology commu-
formulation of the guideline were Lidija Kandolf, Claus nity. Different classification schemes of epithelial dysplasia
Garbe, Josep Malvehy, Klara Mosterd, Maria Concetta and AK were developed to guide the treatment approach in
Fargnoli, Markus Heppt and Carola Berking. To ensure everyday practice. New insights in the efficacy and safety of
the interdisciplinary quality of the guidelines, they were different topical treatments and destructive methods for this
developed in cooperation with the European Dermatology condition were also developed. It is recognized by the sci-
Forum (EDF) and the European Union of Medical entific community that these conditions should be treated
Specialists (Union Européenne des Médecins Spécialistes, and monitored to prevent the transformation to invasive
UEMS). cutaneous squamous cell carcinoma. Thus, the use of these
guidelines that incorporate the updated scientific knowledge
in the field of definition, diagnosis and treatment of epithe-
Disclaimer lial dysplasia, AK and field cancerization in clinical routine
should improve patient care.
All statements related to the definition, classification, diag-
nosis and treatment of actinic keratosis (AK) correspond to
the current scientific knowledge, based on the data from the Target population
literature available at the time of printing the guidelines.
The attending physician invoking these guideline recom- The guidelines have been prepared for the clinicians who
mendations must consider scientific progress since the pub- take care of the patients with AK and keratinocyte carcino-
lication of the guideline. The user remains responsible for mas in general. These are mainly dermatologists.
all diagnostic and therapeutic applications, medications
and doses. Just as adherence to the guidelines may not con-
stitute defence against a claim of negligence (malpractice), Objectives and formulation of questions
deviation from them should not necessarily be deemed
negligent. These guidelines will require updating approxi- The guidelines have been developed and organized in clear
mately every 2 years but advances in medical sciences may sections, based on the latest data from the literature, to sup-
demand an earlier update. Registered trademarks (pro- port clinicians in finding the answers to questions relevant
tected product names) are not specified in these guidelines. to the everyday practice on: (a) definition of AK and field
This work is protected by copyrights in all its parts. Any cancerization and their relation to cutaneous squamous cell
utilization outside the provision of the copyright act with- carcinoma (cSSC); (b) epidemiology and pathophysiology;
out the written permission by the GPO of the EADO is pro- (c) which examinations methods are reliable for diagnosis
hibited and punishable by law. No part of this work may be and do we need histopathologic confirmation? (d) is there a
reproduced in any way without written permission by the rationale for early treatment of AK and which patient should
GPO. This applies to duplications, translations, microfilm- receive which treatment? (e) how we should follow-­up pa-
ing and the storage, application and utilization in electronic tients with AK and (f) what preventive measure can be ad-
systems, intranets and Internet. vised to the patients?
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KANDOLF et al.     | 3

Principles of methodology Financing

The literature search was carried out by the authors using The authors did this work on a voluntary basis and did
PubMed, and only articles published until September 2022 not receive any honorarium. Travel costs for participation
were included. Search strings were used, which cannot all be in Consensus Conferences were paid by the authors them-
listed here. In principle, the search strings are constructed selves. Accommodation during the Consensus Conferences
in such a way that the search is primarily carried out in the was reimbursed in part by EADO.
titles and abstracts of the publication, including the terms
AK, keratinocyte dysplasia, field cancerization, preven-
tion, diagnosis and treatment. All diagnostic and treatment DE F I N I T ION, E PI DE M IOL OGY,
recommendations summarized in the respective tables are A ET IOL OGY A N D DI AGNOSIS
evaluated on the basis of evidence-­based data or formulated
as expert consensus if no sufficient evidence is available. Definition
The methodology of these updated guidelines is based on
the standards of the AGREE II instrument.1 The levels of Actinic keratosis (AK) is a common cutaneous keratinocyte
evidence are graded according to the Oxford classification dysplasia characterized by the abnormal proliferation of
(Table 1).2 atypical epidermal keratinocytes (keratinocyte intraepider-
The grades of recommendation were classified as follows: mal neoplasia (KIN)). In World Health Organization (WHO)
classification of skin tumours, it is listed as a carcinoma pre-
A: Strong recommendation. Syntax: ‘shall’. cursor.6 Multiple terms have been used in the literature to
B: Recommendation. Syntax: ‘should’. define this lesion including ‘solar keratosis’, ‘senile keratosis’,
C: Weak recommendation. Syntax: ‘may/can’. ‘keratosis senilis’, ‘senile keratoma’, ‘keratoma senile’7 and ‘in
X: Should not be recommended. situ SCC type AK’.8 AK is either considered as a precancerous
0: Recommendation pending. Currently not available or lesion that may possibly ‘transform’ into invasive SCC (iSCC),
not sufficient evidence to make a recommendation in fa- or as in situ SCC (intraepidermal proliferation of atypical
vour or against. keratinocytes) that may progress to an invasive stage. This
An expert consensus was presented, where there was in- concept is based on the fact that AK is cytologically indistin-
sufficient evidence. guishable from in situ SCC and has a number of molecular
alterations common to SCC.9,10 The term in situ SCC should
be used with caution with patients, because the term ‘carci-
Source guidelines noma’ is associated with morbidity that does not correspond
to the clinical diagnosis since AKs in most cases do not trans-
Source guidelines for guideline adaptation of recommenda- form into an iSCC. However, it should be communicated to
tions was the German S3 guideline on actinic keratosis and patients that currently it is not possible to predict the progres-
the American Academy of Dermatology guidelines on ac- sion of single AK lesions to invasive cSCC (Table 2).
tinic keratosis,3-­5 since previously published guidelines ex-
pired (i.e. published 5 or more years ago).
Concept of field cancerization

Consensus building process Field cancerization is defined as an area of subclinical changes
in the periphery of clinically visible AKs that displays genetic
The consensus building process was conducted as follows: changes similar to those found in AK lesions.11,12 Clinically, a
In a first-­round, medical experts who participated in their definition of field cancerization has been established by expert
national guideline development processes were involved in opinion consensus and systematic review has been stated as
producing an initial draft. A consensus meeting was held in ‘the anatomical area with or adjacent to AK and visibly sun-­
Rome, Italy, on 24 and 25 November with final outcomes: damaged skin characterized by at least two of the following
(1) the approval of the text and (2) a consensus rate of signs: telangiectasia, atrophy, pigmentation abnormalities and
agreement of at least 80%, for recommendations provided a sandpaper like texture’. It is unclear whether a visible AK le-
in structured boxes and the figure. Voting of the recom- sion is required for field cancerization13 (Table 2).
mendations included the selection of ‘Agree’, ‘Disagree’
or ‘Abstential’ vote, and the possibility of providing com-
ments in case of disagree/abstential. The consensus vote Pathophysiology
on the recommendations and the finalization of the draft
were conducted among coauthors by email between 1 and AKs result from excessive chronic sun exposure and are
24 December 2022. located mainly on areas with chronically sun-­damaged
 4
|   
TA BL E 1 Oxford centre for evidence-­based medicine 2011 level of evidence.

Question Step 1 (level 1a) Step 2 (level 2a) Step 3 (level 3a) Step 4 (level 4a) Step 5 (level 5)
b b
How common is the problem? Local and current random Systematic review of surveys Local non-­random sample Case-­series N/A
sample surveys (or that allow matching to local
censuses) circumstancesb
Is this diagnostic or monitoring Systematic review of cross-­ Individual cross-­sectional Non-­consecutive studies, or studies Case–control studies, or poor or Mechanism-­based
test accurate? (Diagnosis) sectional studies with studies with consistently without consistently applied non-­independent reference reasoning
consistently applied applied reference standard reference standardsb standardb
reference standard and and blinding
blinding
What will happen if we do not Systematic review of inception Inception cohort studies Cohort study or control arm of Case-­series or case–control N/A
add a therapy? (Prognosis) cohort studies randomized triala studies, or poor-­quality
prognostic cohort studyb
Does this intervention help? Systematic review of Randomized trial or Non-­randomized controlled cohort/ Case-­series, case–control studies Mechanism-­based
(Treatment benefits) randomized trials or n-­of-­1 observational study with follow-­up studyb or historically controlled reasoning
trials dramatic effect studiesb
What are the COMMON harms? Systematic review of Individual randomized Non-­randomized controlled cohort/ Case-­series, case–control, or Mechanism-­based
(Treatment harms) randomized trials, trial or (exceptionally) follow-­up study (post-­marketing historically controlled studiesb reasoning
systematic review of nested observational study with surveillance) provided there are
case–control studies, n-­ dramatic effect sufficient numbers to rule out a
of-­1 trial with the patient common harm. (For long-­term
you are raising the question harms the duration of follow-­up
about, or observational must be sufficient)b
study with dramatic effect
What are the RARE harms? Systematic review of Randomized trial or

EUROPEAN GUIDELINE FOR TREATMENT OF AK
(Treatment harms) randomized trials or n-­of-­1 (exceptionally)
trial observational study with
dramatic effect
Is this (early detection) test Systematic review of Randomized trial Non-­randomized controlled cohort/ Case-­series, case–control, or Mechanism-­based
worthwhile? (Screening) randomized trials follow-­up studyb historically controlled studiesb reasoning
a
Level may be graded down on the basis of study quality, imprecision, indirectness (study PICO does not match questions PICO), because of inconsistency between studies, or because the absolute effect size is very small; Level may be
graded up if there is a large or very large effect size.
b
As always, a systematic review is generally better than an individual study.

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KANDOLF et al.     | 5

TA BL E 2 Definitions of actinic keratosis and field cancerization.
epidemiological data are scarce and often marred by numerous
Definitions of biases. Prevalence varies greatly across countries, depending
AK and field on study setting, UV radiation level and patient characteris-
cancerization Consensus-­based statement
tics.29 In the UK, 15.4% of males and 5.9% of females have AK
GCP AK is a precancerous lesion that may progress into lesions, while in those older than 70 years, the prevalence in-
invasive SCC. Actinic keratosis shall be used as
creases to 34% of whites over 70 years.30 In Australia, up to 60%
the preferred term in clinical practice8,9
An area of field cancerization is defined as an area of people over 40 years old have AK.31 In Spain, AK prevalence
of subclinical changes in the periphery of visible was observed in 28.6% of the population over 45 years, with
AKs that displays genetic changes similar to higher rates in men than women.32 In Italy, AK prevalence was
those found in AKs11,12
27.4% and in Switzerland 25.3%.33-­35 Higher rates in men than
Expert consensus Strength of recommendation: 100% in women were also observed in all epidemiologic studies in
Germany, the overall prevalence of AK was 2.66%, with rates
higher in men than in women, and prevalence increasing with
skin.14-­16 UVB radiation can induce mutations and deregu- age, with the highest rates observed in the 61–70 age group.28
lation of tumour suppressor proteins such as p53, p16INK4a
and PTEN that are considered a crucial molecular mecha-
nism in the development of AK and cSCC.10,17,18 UV radiation Risk factors for AK
and infections with human papillomaviruses (HPV) may act
as cofactors in the development of AK, although the role of A meta-­analysis, including mainly European studies, inves-
HPV is still controversial.19-­25 Immunosuppression increases tigated risk factors in immunocompetent individuals.23,29
the risk of cancers that are associated with viral infection. In Factors associated with an increased risk of AK were male sex,
particular, the risk of cSCC which has been associated with age >45 years, fair skin type, light hair colour, light eye colour,
beta HPV infection is increased by more than 100-­fold in im- freckles on face/arms, positive history of non-­melanoma skin
munosuppressed patients.22-­24 In a systematic review, 58.5% cancer (NMSC), sunburns in childhood and adulthood, se-
of AKs were positive for beta HPV, 40.2% for gamma HPV vere sunburn, chronic occupational and/or recreational sun
and only a few were positive for alpha subtypes.24 However, exposure, baldness, and use of potentially photosensitizing
it has been found that T-­cell immunity against commensal thiazide diuretics or other photosensitizing cardiac drugs. On
papillomaviruses suppresses skin cancer in immunocompe- the contrary, factors associated with a reduced risk of AK were
tent hosts, and the loss of this immunity rather than the on- sunscreen use and history of atopy. No association was found
cogenic effect of HPVs may contribute to causes the markedly between patients' education level and the risk of AK, abnormal
increased risk of cSCC in immunosuppressed patients.25 body mass index, alcohol consumption and smoking status.
Sensitivity analysis yielded consistent results. IRF4, MC1R and
TYR genes, that are involved in various kinds of human pig-
Development of AK towards cSCC mentation traits as well as in skin cancers, were identified as
significant risk factors for AK in the north-­western European
AKs may undergo spontaneous regression, remain stable study population.33 Chronically immunosuppressed patients
or further progress to invasive malignancy. It has been sug- especially organ transplant recipients (OTRs) have a higher risk
gested that invasive cSCC may develop in two ways: (1) by for developing AK and SCC.36 In OTRs, the prevalence of pa-
transformation of a clinically pre-­existing individual AK or tients with AKs increases with longer duration of immunosup-
(2) de novo, from a subclinical UV-­damaged single cell in a pression.37 A recent study showed that the variability of AKs in
field of cancerization. The first way seems to occur in 0.1%– a 12-­month period was associated with an increased risk of SCC
16% in clinically pre-­existing AKs, based on the data about in OTRs.38 In another study, presence of AK patches and their
the risk of malignant transformation of a single actinic kera- number, as well as the number of AKs and area affected by AKs,
tosis.26 The second pathway is based on field changes which was predictive of SCC development in OTR.39 Genetic skin dis-
can be detected in about 80% of histopathologically exam- eases associated with impaired DNA repair mechanisms and
ined cSCC.27 A meta-­analysis found progression rates of disorders with a deficient melanin biosynthesis are associated
AKs to SCC varying from 0% to 0.075% per lesion-­year, with with a higher risk for the development of AK.40,41
a risk of up to 0.53% per lesion-­year in patients with prior
history of keratinocyte cancer (NMSC).28 Rates of regression
of single lesions ranged between 15% and 63% after 1 year, C L I N IC A L A N D NON-­I N VA SI V E
with a recurrence rate of 15%–53% after 1 year follow-­up.28 DI AGNOSIS OF A K s

Clinical features
Epidemiology
AKs typically manifest as rough, scaly skin coloured to red
Since AK are not included in cancer databases or population-­ light or dark brown patches, papules or plaques commonly
based incidence rates and AKs are often not biopsied, located on chronically sun-­damage body sites. The diameter
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6 |    EUROPEAN GUIDELINE FOR TREATMENT OF AK

of AKs generally ranges from a few millimetres to several pattern (grade 1), a ‘strawberry pattern’, namely background
centimetres.42 The clinical features along with the typical an- erythema interrupted by white-­coloured follicular openings
atomical site allow a correct clinical diagnosis in most cases, that might be filled with keratin plugs (grade 2), or structure-
although the differential diagnosis with basal cell carcinoma less white to yellow areas (grade 3).53,54 Dermatoscopy may
(BCC) and inflammatory disorders may be sometimes chal- help to differentiate solitary AK grade III (with structure-
lenging. Also, lichenoid keratosis (i.e. lichen-­ planus like less yellow and white colour and erythema with strawberry
keratosis) and Bowen disease have to be considered in dif- pattern, focally) and Bowen's disease (with coiled vessels).
ferential diagnosis, particularly in solitary lesions. Clinical Moreover, dermatoscopy can aid in the assessment of treat-
variants include pigmented, Bowenoid and lichenoid AK.43 ment response and in the differential diagnosis of AK. In the
While the latter two are usually diagnosed on histopatho- cases of pigmented AK, dermatoscopy may help to rule out
logic examination, pigmented AK is commonly present in lentigo maligna44,55 based on the presence of enlarged white
sun-­damaged skin, and therefore, differential diagnosis may follicular openings, double lines between the hair follicles,
include lentigo maligna. The number and location of lesions, background erythema and scaly surface in AKs. In AKs lo-
similar morphology using the comparative approach and cated on non-­facial skin, the follicular openings are less pre-
rough surface on palpation represent important clues for the dominant and dermatoscopy mainly reveals erythema and
diagnosis of AK.44,45 Clinical signs suggesting progression to superficial scales. Dermatoscopy can also help to identify
iSCC (iSCC) include lesion induration, bleeding, discomfort, early signs of iSCC due to the presence of coiled/glomerular
pain and increase in thickness and diameter.43 AKs seldom or polymorphous vessels and white circles, which are rarely
appear as a solitary lesion; indeed, often an entire region is observed in AK.54
affected. Individual AK lesions have been clinically graded
based on their thickness using the Olsen classification sys-
tem.46 Grade 1 lesions are slightly palpable, more easily felt Confocal microscopy and optical coherence
than seen, grade 2 lesions are moderately thick and easily tomography (OCT) (Table 4)
seen and felt, and grade 3 lesions are very thick and hyper-
keratotic. This severity index was combined with the count- In combination with clinical examination and dermatos-
ing of lesions in a limited area for the assessment of clinical copy, reflectance confocal microscopy (RCM) and optical
trials. However, counting individual lesions is not reproduc- coherence tomography (OCT) can help in the differential
ible even among experts.47 Although the Olsen classification diagnosis of AK and SCC, pigmented AK and lentigo ma-
failed to reliably correlate with the histological severity of ligna. The superficial orientation in the epidermis makes
the lesions, it has been shown to be strongly correlated with AK suitable for non-­invasive imaging tools, but on the other
the risk of cSCC development in a recent study.48 Other clin- hand, the presence of hyperkeratotic scale may impair image
ical severity indexes have been proposed considering the en- resolution and diagnostic accuracy. RCM and OCT have
tire area affected by AKs.49-­51 Additionally, a recent practice also been extensively applied to monitor treatment efficacy
related approach classified AK based on the overall burden of AKs.56-­60 The RCM terms that describe better diagnostic
of disease into the following categories52: (1) single AK (less features of AK include hyperkeratosis, parakeratosis, scale
than 5 AKs in a defined field), (2) multiple AKs (6+ lesions in and atypical honeycombed pattern, architectural disarray
a defined field), (3) field cancerization (6+ lesions associated and targetoid cells.61-­63
with sun-­damaged skin and hyperkeratosis) and (4) AKs as-
sociated with immunosuppression.
Line-­field confocal optical coherence
tomography (LC-­OCT)
Dermatoscopy (Table 3)
LC-­OCT in vertical and horizontal sections of the lesions
Dermatoscopy improves the clinical diagnosis of AK and has have been used in to identify AKs criteria that include an out-
been reported to achieve a diagnostic sensitivity and speci- lined dermo-­epidermal junction without broad strands.64,65
ficity of 98.7% and 95.0%, respectively. Depending on the LC-­OCT has also correlated with histological images to
clinical aspects, dermatoscopy reveals either a red network evaluate the proliferative pattern of AK that has been associ-
ated with resistant to treat AK and the risk of progression.66
TA BL E 3 Clinical and dermatoscopic diagnosis of actinic keratosis.
TA BL E 4 Other non-­invasive imaging for actinic keratosis.
Consensus-­based statement
Consensus-­based statement
Grade of The diagnosis of actinic keratosis and
recommendation: B field cancerization is made by clinical GCP Confocal microscopy, OCT and LC-­OCT
examination. Dermatoscopy can help can help in the differential diagnosis
in the differential diagnosis of actinic of actinic keratosis and other skin
keratosis and other skin neoplasms neoplasms
Level of evidence: 1 Strength of consensus: 100% Strength of consensus: 100%
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KANDOLF et al.     | 7

H ISTOPAT HOL OGIC DI AGNOSIS papillary dermis and forming round nests of atypical ke-
ratinocytes; Pro III (papillary sprouting) to spiky or filiform
Histopathologic confirmation papillary elongation of atypical keratinocytes protruding
into upper dermis and exceeding the thickness of the over-
Histopathological confirmation is recommended to an lying epidermis.69,70 Interestingly, proliferative AKs are not
equivocal lesions especially in the differential diagnosis of correlated with Olsen grade or KIN criteria.
cutaneous SCC (cSCC) or BCC (Table 5). Also, for type III
AK and bowenoid AK, differential diagnosis with Bowen's
disease can be difficult. The presence of basal cells in pali- TR EATMENT OF ACTINIC K ER ATOSES
sades along the basement membrane and the dysplasia of the
adnexal and follicular epithelium, which is present in BD Rationale for treatment
and absent in AK, can help in differentiating these two enti-
ties.67 A skin biopsy should be taken if one or more of the The most important reason for treatment of AK is to prevent
following clinical features are present which may indicate the transformation to invasive cSCC.52 The risk of progres-
cSCC or other types of skin cancer: infiltration, induration, sion varies from 0.025% to 20% per year and is significantly
ulceration, pigmentation, rapid enlargement and pain.68 A higher in immunosuppressed patients, such as solid organ
biopsy should also be considered if coiled, dotted, hairpin transplant recipients.71 Furthermore, if the patient has had
or polymorphous vessels and/or white circles or whitish ho- previous cSCC in the field, the risk for developing the sec-
mogeneous areas are detected on dermatoscopy or if inva- ond cSCC is 40.7% at 5 years.72 As there is currently no way
sion is suspected on RCM, OCT and LC-­OCT. According to accurately predict which lesion will develop into cSCC
to their clinico-­pathological appearance, various types of or when this might occur, treatment is recommended.
AK have been described, including pigmented, atrophic, Treatment of AK can be lesion-­directed or field-­directed.
bowenoid, lichenoid, acantholytic and hyperkeratotic AKs. Lesion-­directed treatments target individual AKs, whereas
The Rowert–Hubert histological classification has been sug- field-­directed treatments have the advantage of treating
gested to assess the severity degree of single AK lesions52: multiple, widespread and subclinical AKs that may occur
(1) early in situ cSCC, type AK I corresponds to atypical within a field of chronically sun-­damaged skin, commonly
keratinocytes in the basal and supra-­basal layers (the lower referred to as field cancerization.73 Field-­ directed treat-
third) of the epidermis; (2) early in situ cSCC, type AK II is ments are nowadays the focus of AK treatment as most of
constituted by atypical keratinocytes extending to the lower them are convenient, can be self-­administrated and most
two-­thirds of the epidermis; (3) in situ cSCC, type AK III importantly they target subclinical damage. Weinstock
consists of atypical keratinocytes extending to more than et al.74 found that field treatment with 5-­f luorouracil (5-­FU)
two-­thirds of the full thickness of the epidermis. The clas- reduced the risk of cSCC compared to placebo after 1 year in
sification was suggested to predict the risk of AK to progress patients with severe AKs and a history of at least two cSCCs:
to cSCC. However, in a recent study it was demonstrated 1% of patients treated with 5-­FU developed a cSCC, com-
that AK I are the most frequent lesions associated to cSCC pared to 4% in the placebo group. In another study, the total
(so-­called differentiated pattern) and that Rowert–Hubert 4-­year risk of developing cSCC in a field treated area of AK
classification cannot predict the transformation of AKs.27 was 3.7%, but significantly increased to 20.9% in patients
Additional evidence suggests that hair follicles may contrib- with Olsen grade III AK and to 33.5% in patients with Olsen
ute significantly to the development of deeply invasive SCC grade II AK patients with an indication for retreatment.48
and that the depth of follicular extension in AK correlates Thus, for multiple severe AKs with a history of previous
with the depth of invasion of an associated iSCC.13,27 Based cSCC, field treatment and retreatments are highly recom-
on these and other findings from the recent studies, the PRO mended. For mild AKs (Olsen grade I), field treatment can
classification of AKs was suggested, which is based on the also be recommended, but well-­instructed self-­examination
histological growth pattern. The histological growth pattern can be considered.
of AKs appeared to be associated to treatment resistance and Field-­directed treatments are not suitable for all patients.
progression to invasive cSCC. Pro I (basal-­growth pattern) The long duration of treatment can impact adherence, and
corresponds to crowding of basal atypical keratinocytes; they may cause unwanted cosmetic effects. In some patients,
Pro II to budding of atypical keratinocytes into the upper lesion-­directed treatments are preferred, as they have the
benefit of being performed under the supervision of a phy-
TA BL E 5 Biopsy and histopathological examination. sician and are less time-­consuming. Lesion-­directed treat-
ments commonly involve ablative procedures as surgery
Consensus-­based statement
(shave, excision), cryosurgery/cryotherapy and laser therapy.
GCP Biopsy is not routinely required for the diagnosis of actinic Surgical treatments are usually reserved for AKs that are
keratosis unresponsive to other treatments and in cases of uncertain
Biopsy shall be done in clinically and/or dermatoscopically
diagnosis.75
suspicious and/or treatment-­refractory lesions
There is no standard treatment for AKs, and physicians
Strength of consensus: 100%
should make decisions considering both lesion (number,
PIGMENTATA LICHENOIDE
ATROFICA ACANTOLITICA
BOWENOIDE IPERCHERATOSICA
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8 |    EUROPEAN GUIDELINE FOR TREATMENT OF AK

location, histology) and patient characteristics (age, com- Cryotherapy (Table 8)
pliance, immune status).76 Also, treatment decisions should
be made in a patient–physician shared decision process Cryosurgery, or cryotherapy, is a lesion-­directed treatment,
(Table 6). with a focus on treating a single or a limited number of AKs.
This procedure is considered to be a standard initial first-­
line treatment in patients with a limited number of AKs,81
Surgical procedures (Table 7) as it is easy to perform and time-­efficient. By using low tem-
perature (liquid nitrogen −196°C), cryotherapy targets and
Curettage is the most frequently performed surgical pro- kills precancerous cells directly by inducing cell rupture due
cedure in AK management and particularly suitable for to osmotic shock and intracellular formation of ice crystals.
solitary lesions. According to a recent meta-­ a nalysis, In addition, it leads indirectly to a delayed cell termination
combinations with destructive treatments such as electro-­ process by inducing vascular necrosis due to thrombosis and
desiccation or cryosurgery are more effective than photo- a release of neo-­antigens. To attain the effective temperature
dynamic therapy, 5-­f luorouracil or imiquimod in treating of at least −40°C on the edge of the lesion, the cycle of freez-
in situ SCC or superficially invasive SCCs.77 Moreover, ing and thawing should be repeated.82 Sensitive areas such
curettage is a standard procedure established in photody- as eyes should be protected.83 AK I-­II are subject to a single
namic therapy (PDT) protocols to ablate superficial kerato- freeze–thaw cycle with a freezing time between 5 and 20 s.84
sis, above all in thick hyperkeratotic AK. Deeper shavings Two freeze–thaw cycles of 10 s each are indicated for large
or scalpel excisions instead are preferred in suspicious le- and hypertrophic lesions.85 Prior removal of hyperkeratotic
sions, in which histology of the entire specimen appears scales is recommended, either by gentle curettage or by appli-
justified.75 In AK, surgical treatments are usually limited cation of urea or salicylic acid containing keratolytic agents
to lesion-­d irected removal of single or isolated AKs. After 2 weeks before cryosurgery.83 Cure rates of cryotherapy as
primary field-­d irected treatment, any remaining AK may single treatment for AK range from 39% to 83%.86 The effi-
be effectively treated with a lesion-­d irected surgical ap- cacy depends on the experience of the dermatologist and the
proach.78 Surgical interventions, in general, have the ad- protocol used.87 Combination of cryosurgery with a topical
vantage to allow for histopathologic examination of the intervention may be more effective than cryosurgery alone
removed tissue specimen. Histology is particularly advised in patients with multiple AKs and field cancerization.88
if AKs is refractory to standard therapy, in relapsing AKs,
or in those suspicious of cSCCs (e.g. in thickening, pain-
ful or bleeding lesions, particularly in immunosuppressed Laser ablation (Table 9)
patients).79 The drawbacks of surgical techniques are that
usually only single lesions will be removed, anaesthesia is AK can be treated with laser therapy, either alone or in
needed, and permanent depigmentation or even scarring combination with other treatments like PDT. The most
may develop.80
TA BL E 8 Cryosurgery.

TA BL E 6 Indication for treatment of actinic keratosis. Consensus-­based statement
Grade of Cryosurgery shall be offered as a first-­line
Consensus-­based statement
recommendation: A standard treatment for solitary AK84,85
Expert consensus Treatment-­decision should be made on a case-­ Cryosurgery in combination with
by-­case basis considering patient-­related curettage and topical treatments shall
factors and lesion characteristics. be offered in multiple AKs and field
For patients with previous cSCC and/or cancerization.84,89
immunosuppression treatment should be Level of evidence: 1 Systematic review and meta-­a nalysis,84,89
considered prospective multicentre study 90
Strength of consensus: 100% Strength of consensus: 100%

TA BL E 9 Laser ablation for AKs.
TA BL E 7 Surgery and laser ablation for lesion-­d irected treatment
Evidence-­based statement
of AK.
Grade of Ablative laser treatment should be offered
Consensus-­based statement recommendation: B as one of the options for single or
GCP Curettage, shave or excisional biopsy can be offered for single multiple AKs, but it is not superior to
or few hyperkeratotic lesions. Histological examination is cryotherapy or 5-­FU treatment.
strongly recommended in treatment-­resistant cases and Level of evidence: 2 Single-­centre randomized controlled
in lesions suspicious for iSCC.81 trials91,92
Strength of consensus: 100% Strength of consensus: 100%
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KANDOLF et al.     | 9

commonly used lasers for ablative treatment in AKs are the its metabolites into RNA and DNA. The benefits of 5-­FU
CO2 and Er:YAG lasers, which remove the epidermis and su- treatment for AK were assessed based on five studies with
perficial dermis to stimulate re-­epithelialization. However, moderate-­to-­h igh quality efficacy, four studies with 5%
traditional laser treatment can have side effects such as hy- 5-­FU once daily and one with 5% 5-­FU twice daily.94-­96
popigmentation and scarring, as well as immediate side ef- The largest placebo-­controlled randomized trial (VAKCC
fects like erythema, oedema, itching, hyperpigmentation and trial) showed field treatment of AKs on the face with 5%
scaling, which usually resolve within 2 weeks but may take 5-­FU, twice daily for 4 weeks, to be more effective than
longer to heal. Ablative laser treatment appears to be more placebo for complete AK clearance at 6 months (38% vs.
effective than fractional laser treatment. There are only two 17%; p < 0.01).94 Two placebo-­controlled randomized clini-
randomized controlled trials (RCTs) comparing it to 5-­FU cal trials evaluating 0.5% 5-­FU cream suggested the low
cream.89-­91 Hantash et al. compared CO2 laser with 5-­FU ap- concentration of 5-­FU to be more effective than placebo
plied twice daily for 3 weeks with no significant difference in reduction from baseline of AK lesion counts and lesion
while Ostertag et al. did find a significant difference in fa- clearance.95,96 The main adverse event, often the primary
vour of the Er:YAG laser in comparison with 5-­FU treatment reason for discontinuation of the treatment with 5-­FU,
twice daily for 4–7 weeks. However, after 12 months post-­ remains local irritation. The number of AK lesions at
treatment, there was no difference in efficacy, whereas more baseline may predict the severity of local skin reactions.97
side effects were noted in the Er:YAG treated group.89,90 CO2 New formulation of 4% fluorouracil in aqueous cream
laser was compared to cryosurgery in a single-­centre RCT in- once daily was compared with twice daily treatment with
cluding 200 patients.92 In both groups, the cosmetic outcome 5%-­FU in a double-­blind multicentre study involving 841
was good. Complete responses at 3 months were, respectively, subjects. It revealed similar efficacy, but better tolerability
65.3% and 71.1%, respectively, in the laser and cryotherapy of the 4% formulation (30% vs. 60% application site skin
groups, but decreased to 14% and 53% at 1 year. Therefore, reaction). Field treatment of face and scalp area 10°C, cloudless to overcast sky, no
rain). Two pivotal phase III trials conducted in Australia Grade of recommendation: B Combined treatments should
and Europe compared daylight PDT with conventional PDT be offered to patients with
multiple and/or hyperkeratotic
with MAL in a multicentre, investigator-­blinded, controlled lesions, large treatment fields
intraindividual trial as a non-­inferiority analysis.140,141 At and treatment resistance to
12 weeks after a single PDT cycle, the lesion complete clear- monotherapies.
ance rate was not inferior to conventional MAL-­PDT (89% Level of evidence: 1 Randomized controlled trials,84,90,146
vs. 93% in Australia, 70% vs. 74% in Europe), but daylight systematic review and
PDT was significantly less painful in both trials. Dirschka meta-­a nalysis.149
et al.142 compared daylight PDT with BF-­200 ALA versus Strength of consensus: 100%
MAL in a large-­scale, multicentre, split-­face non-­inferiority
study. The patient-­ specific complete clearance rate was
42.9% for ALA versus 38.8% for MAL. The lesion-­specific lesions may benefit from a sequential use of field-­and lesion-­
clearance rates were similar for both photosensitizers (79.8% directed treatment (see Combination treatment).
for ALA, 76.5% for MAL). The study reported a signifi-
cantly higher recurrence rate for MAL (31.6%) compared
with ALA (19.9%) after 12 months of follow-­up. A similar Combination treatments: Should it be the rule?
comparison was performed by Räsänen et al. in 2019 in a (Table 17)
multicentre double-­blind non-­sponsored trial. Both photo-
sensitizers were applied to one side of the face. The lesion-­ A multitude of interventions for the treatment of AK exists
specific clearance rate was 79.7% for ALA versus 73.5% for which are often combined either simultaneously or sequen-
MAL. The complete clearance rates were 27.5% for both pho- tially. The rationale for an upfront combination approach
tosensitizers.143 From these data, we conclude that ALA and is to take advantage of the strengths and distinct mecha-
MAL are equally effective when used for daylight PDT. The nisms of action of different interventions, thereby achiev-
advantages of daylight PDT over conventional PDT include ing synergistic effects.145 The application of a primarily
minimal to no pain, the possibility to treat large fields and field-­d irected approach can be focally complemented by
the lack of a requirement for artificial light sources. lesion-­d irected modalities such as cryosurgery, laser ab-
lation, or shave excision for hyperkeratotic or treatment-­
refractory lesions. Pre-­t reatment with topical agents may
Field cancerization treatment (Table 16) even unmask and reveal subclinical lesions within a treat-
ment field which can subsequently be targeted with a
Although an exact definition has not yet been agreed upon, the lesion-­d irected treatment. Conversely, following a primar-
concept of field cancerization is increasingly being acknowl- ily field-­d irected therapy, subclinical lesions and field can-
edged and considered for treatment selection and preven- cerization can be managed by a field-­d irected treatment
tion of AK. Agents approved for large-­field applications such which prevents the progression of subclinical lesions to
as 5-­f luorouracil 5%, 5-­f luorouracil 4%, PDT or imiquimod become clinically visible AK. 3 Recent analyses have shown
3.75% are preferable for multiple thin lesions as the field is that treatment combinations result in significantly higher
commonly ill-­defined and expands over a larger area. Studies lesion clearance compared to respective monotherapies.
employing RCM provided evidence that subclinical changes In particular, such efficacy benefits were demonstrated
are efficiently resolved by topical treatments.144 Diclofenac for laser-­ a ssisted conventional PDT,93 PDT combined
sodium is also suitable for large fields but may be less effec- with pre-­ t reatment by microneedling,146 cryosurgery
tive for lesion clearance. Patients with multiple hyperkeratotic combined with topical agents88 and 0.5% 5-­FU followed
 14683083, 0, Downloaded from https://onlinelibrary.wiley.com/doi/10.1111/jdv.19897 by Gerardo Palmisano - University Cattolica, Piacenza , Wiley Online Library on [21/03/2024]. See the Terms and Conditions (https://onlinelibrary.wiley.com/terms-and-conditions) on Wiley Online Library for rules of use; OA articles are governed by the applicable Creative Commons License
KANDOLF et al.     | 15

by cryosurgery.147,148 Furthermore, there is evidence that that it does not reduce the number of new keratinocyte can-
combining several field-­d irected treatments can augment cers in OTRs.151 For clinically manifest AK, the evidence
their efficacy. A systematic review identified 10 RCTs with for active interventions is surprisingly low.152 A system-
a total sample size of n = 277.149 Four studies investigated atic review identified only eight small, randomized trials
a combination of PDT with imiquimod cream, three with with 242 OTR, 6 out of 8 which evaluated PDT (but only
5-­FU and one each with ingenol mebutate, tazarotene gel 2 imiquimod and one each for 5-­f luorouracil, diclofenac
and calcipotriol ointment. Patients treated with a com- gel and cryotherapy).152 Here, field-­d irected treatments
bination had higher rates of complete and partial lesion showed higher clearance rates than lesion-­d irected treat-
clearance,149 implying that treatment combinations can ments, underlining the paramount importance of treating
achieve higher clearance rates compared to monothera- the entire field in this high-­risk population (see Field-­
pies. Nevertheless, a combination of interventions should directed treatments). Conventional MAL-­PDT showed the
always be discussed on a case-­by-­c ase basis, and mono- most favourable clearance rates (40%–76.4%), followed by
therapies will in many cases be sufficient to achieve lesion imiquimod (27.5%–62.1%), diclofenac sodium (41%) and
clearance and disease control. Patients with simultaneous 5-­fluorouracil 5% (11%), while ablative laser treatment
discrete and hyperkeratotic lesions, large treatment fields showed the lowest lesion clearance (5%–31%). Importantly,
and treatment resistance to monotherapies may benefit there were no graft rejections under topical therapies.152
from combinations. In a recent small RCT, treatment with sunscreen, 5-­FU
and imiquimod was used for prevention of cSCC in OTR,
and treatment with 5-­FU was found to be superior in AK
Treatment of AK in immunocompromised clearance as a surrogate biomarker of cSCC prevention.153
patients (Table 18) Immunosuppressed patients commonly show multiple
and metachronous evolving lesions over large fields. Thus,
Compared to immunocompetent individuals, chroni- purely lesion-­d irected treatments are usually not sufficient
cally immunosuppressed patients show significantly in- to achieve disease control. Due to a more aggressive dis-
creased morbidity and mortality due to the development ease course and a higher portion of treatment-­resistant le-
of iSCC.150 Important mainstays for secondary prevention sions, repeated treatment is often necessary. The threshold
are early modification of the immunosuppressive regimens to biopsy lesions to rule out progression to cSCC should
by eliminating of azathioprine and switching to mTOR be lower than in immunocompetent individuals. Most
inhibitor-­containing immunosuppression, photoprotec- evidence for the subgroup of immunosuppressed patients
tion and chemoprevention with retinoids. Although in is available for PDT, imiquimod and diclofenac sodium. 3
immunocompetent individuals, dietary supplementation Dragieva et al. evaluated conventional MAL-­PDT in 14
with oral nicotinamide (vitamin B3) was found to be ef- renal and 3 cardiac transplant recipients. The lesion clear-
fective in prevention of cSCC, in a recent trial it was found ance rate assessed 16 weeks after two PDT cycles was
90.3% in the MAL-­treated group versus 0% in the vehi-
TA BL E 18 Treatment of AK in immunocompromised patients.
cle group. Complete response of the entire treatment field
was achieved in 75.4% and partial response (>75% of all
Evidence-­based statement lesions per field cleared) in 94.1%.154 A European, mul-
Grade of recommendation: B Conventional PDT with illumination by a ticentre, double-­blind, interindividual randomized trial
red-­light source, 5-­FU 5% cream and evaluated imiquimod 5% cream versus placebo in 30 kid-
diclofenac sodium 3% in hyaluronic ney, 4 liver and 9 heart transplant patients. The complete
acid gel 2.5% should be offered to
immunocompromised patients with
response rate was 62.1% for imiquimod (100% in the liver
single and multiple AKs and field transplant group, 65% in the kidney transplant group and
cancerization 42.9% in the heart transplant group) versus 0% for pla-
Grade of recommendation: C Imiquimod 5% or 3.75% cream may be cebo.155 Importantly, anecdotally reported graft rejection
offered for treatment of single and or deterioration of the graft function was not observed in
multiple AKs and field cancerization
this trial.133,134,155 Adverse events of imiquimod were local
in selected immunocompromised
patients site application reactions, fatigue, headache, diarrhoea,
Daylight PDT may be offered to nausea, rash, unspecified skin reactions and leukopenia.
immunocompromised patients with Togsverd-­Bo et al.156 investigated MAL-­PDT and imiqui-
single and multiple AKs and field
mod in 35 OTR. PDT resulted in higher lesion clearance
cancerization
Field-­d irected treatments have higher at a 3-­month follow-­up albeit at the cost of more intense
clearance rates than lesion-­d irected local skin reactions. The median patient-­specific complete
treatments in this high-­risk clearance was 78% for PDT versus 61% for imiquimod.
population
Diclofenac sodium was investigated in a double-­blind,
Level of evidence: 2–3 Randomized controlled trials,153 placebo-­controlled, randomized trial in 32 OTR (18 renal,
systematic review152
8 cardiac and 6 liver transplant recipients).131 The com-
Strength of consensus: 78.5%
plete clearance of all lesions in the treated field was 41%
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16 |    EUROPEAN GUIDELINE FOR TREATMENT OF AK

(kidney transplants 30.7%, liver transplants 40%, heart midday should be completely avoided or postponed to the
transplants 75%) versus 0% in the placebo group. Partial morning and evening hours. Sunburn should be avoided at
clearance of at least 75% of lesions was observed in 59% for any time.
diclofenac versus 16.7% for placebo. The recurrence after In high-­risk patients (e.g. OTRs) with multiple AK, field
diclofenac treatment was 55% after 9.3 months. Adverse cancerization, or a history of multiple non-­melanoma skin
events included mild to moderate erythema, scaling, itch- cancers regular (e.g. yearly) treatments of previously affected
ing and skin irritation with oedema.131 Based on the avail- skin areas can be considered with PDT, 5-­FU or imiquimod
able evidence, Massey and co-­ workers have developed as a preventive topical measure. In the Veterans Affairs
consensus-­based recommendations on the prevention of Keratinocyte Carcinoma Chemoprevention (VAKCC) trial,
cSCC in solid organ transplant recipients.157 The key rec- one treatment course of 5-­FU 5% cream twice daily over
ommendations for the treatment of AK in OTR patients 4 weeks effectively reduced AK counts and the need for
include cryosurgery for scattered AK, field therapy with additional spot treatments for AK for more than 2 years.94
5-­f luorouracil for AK grouped in one anatomical area, and Similarly, the formation of new AK was reduced with 5-­FU
for field cancerized skin, and acitretin therapy for patients in this trial by prospectively tracking individual lesions
with a high rate of multiple skin cancers or high-­r isk cSCC. over 36 months in this high-­risk population having more
For thick AKs, a combination of lesion-­d irected and field than 2 keratinocyte carcinomas in the past 5 years.160 In
therapy with cryotherapy was recommended, and immu- the LEIDA trials, imiquimod 5% cream was superior to di-
nosuppression reduction or modification should be dis- clofenac 3% gel in preventing histological change to grade
cussed with patients with high-­r isk cSCC.157 This group of III AK or invasive SCC and AK recurrence over 3 years.118
patients should be managed in specialist centres. However, this trial did not include a high-­risk population as
in the VAKCC trial.
There has been long-­ standing controversy and in-
Treatment algorithm tense debate on the use of systemic chemoprevention in
high-­r isk situations. Agents investigated for oral che-
Proposed treatment algorithm is presented in Figure 1 moprevention include oral retinoids, nonsteroidal anti-­
(modified from Gupta et al.158). For single non-­ inflammatory drugs (NSAID), capecitabine, as well as
hyperkeratotic lesions, destructive or field-­ d irected dietary supplements and vitamins (beta-­carotene, nic-
treatments can be started, although monitoring and self-­ otinamide). Most of these agents failed to show a clear
examination can also be advised. For multiple lesions, benefit for prevention and may even be associated with
field-­d irected treatments and PDT are advised. For hy- harmful side effects. Oral nicotinamide (vitamin B3)
perkeratotic lesions, pre-­t reatment with destructive meth- 500 mg twice daily showed a rate reduction for cSCC of
ods (curettage, cryotherapy or laser) is advised before 30% in immunocompetent individuals with two or more
field-­d irected treatment. For AKs in immunosuppressed confirmed keratinocyte carcinomas in the past 5 years.161
patients, PDT might be preferred, although other topi- However, there was no effect after nicotinamide discon-
cal treatments might be effective and safe, and for AKs in tinuation, and it is unclear if the preventive effects also
specific high-­r isk regions and in treatment-­resistant cases pertain to AK. Also, oral nicotinamide which was found
surgery is indicated. Preventive measures (sun/protec- does not reduce the number of new keratinocyte cancers
tion, self/examination), repeated treatments and in pa- in OTRs.151 Recent consensus-­based recommendations
tients with previous iSCC chemoprevention are advised on the prevention of cSCC in OTR suggest initiation of
(Figure 1). acitretin and discussion of immunosuppression reduc-
tion or modification for patients who develop multiple
skin cancers at a high rate (10 cSCC per year) or develop
PR E V E N T ION OF A K high-­r isk cSCC (defined by a tumour with approximately
≥20% risk of nodal metastasis). However, no consen-
All patients with AK should be advised to apply the ap- sus recommendation was achieved for OTR with a first
propriate protective measures against solar UV radiation low risk cSCC or multiple AK or field cancerization.157
(Table 19). The following measures should be recommended: Likewise, the German S3 guideline on prevention of skin
avoidance of intensive intermittent (UV peaks) and chronic cancer does not make any recommendations for chemo-
sunlight exposure, wearing of appropriate clothing, applica- prevention in AK. 3,78
tion of sunscreen with a high sun protection factor (≥ 30)
including ear rims and lips, no use of sun beds, and discon-
tinuation or change of light-­sensitizing drugs (e.g. hydro- FOL L OW-­U P OF A K
chlorothiazide). In more detail, the following UV protection
measures should be taken to avoid excessive UV exposure: The surveillance and follow-­up strategies for AK are not
In case of medium and high UV irradiance (UV index 3–7), standardized and notoriously understudied (Table 20). The
shade should be sought during midday. In case of very high response to any treatment should be assessed 3 months after
UV irradiance (UV index ≥8), outdoor activities during the end of treatment clinically, dermatoscopically, and if
14683083, 0, Downloaded from https://onlinelibrary.wiley.com/doi/10.1111/jdv.19897 by Gerardo Palmisano - University Cattolica, Piacenza , Wiley Online Library on [21/03/2024]. See the Terms and Conditions (https://onlinelibrary.wiley.com/terms-and-conditions) on Wiley Online Library for rules of use; OA articles are governed by the applicable Creative Commons License
| 17

Treatment algorithm for actinic keratoses (adapted from Gupta et al.158).
KANDOLF et al.

FIGU R E 1
 14683083, 0, Downloaded from https://onlinelibrary.wiley.com/doi/10.1111/jdv.19897 by Gerardo Palmisano - University Cattolica, Piacenza , Wiley Online Library on [21/03/2024]. See the Terms and Conditions (https://onlinelibrary.wiley.com/terms-and-conditions) on Wiley Online Library for rules of use; OA articles are governed by the applicable Creative Commons License
18 |    EUROPEAN GUIDELINE FOR TREATMENT OF AK

3
TA BL E 19 Prevention of AKs. Dermatologia, Università Cattolica del Sacro Cuore, Rome, Italy
4
Dermatology Department of Hospital Clinic of Barcelona, IDIBAPS, CIBER de
Evidence-­based statement Enfermedades Raras, Instituto Carlos III, University of Barcelona, Barcelona, Spain
5
Department of Dermatology, Maastricht University Medical Centre+
Grade of recommendation: B Individuals at high-­risk of AKs, Comprehensive Cancer Centre, Maastricht, The Netherlands
6
including those occupationally GROW-­School for Oncology and Reproduction, Maastricht University, Maastricht,
exposed to UV irradiation and The Netherlands
7
immunocompromised and all Department of Dermatology, Uniklinikum Erlangen, Friedrich-­A lexander-­
patients with AK should be University Erlangen-­Nürnberg, Erlangen, Germany
8
Comprehensive Cancer Center Erlangen-­European Metropolitan Area of
advised to apply the appropriate
Nuremberg (CC ER-­EMN), Erlangen, Germany
protective measures against UV 9
Dermatology, Department of Biotechnological and Applied Clinical Sciences,
irradiation University of L'Aquila, L'Aquila, Italy
10
Grade of recommendation: C In high-­risk patients (e.g. organ Department of Dermatovenereology, Third Faculty of Medicine, Charles
transplant recipients, OTR) with University and University Hospital of Kralovske Vinohrady, Prague, Czech
Republic
multiple AK, field cancerization, 11
Clinic of Infectious Diseases and Dermatovenereology, Centre of
or a history of multiple
Dermatovenereology, Vilnius University, Vilnius, Lithuania
keratinocyte skin cancers 12
Department of Dermatology, University Hospital Erasme, Université Libre de
regular (e.g. yearly) treatments Bruxelles, Brussels, Belgium
of previously affected skin areas 13
Faculty of Health, University Witten-­Herdecke, Witten, Germany
14
with photodynamic therapy, CentroDerm Clinic, Wuppertal, Germany
15
5-­f luorouracil or imiquimod as Nantes Université, INSERM, CNRS, Immunology and New Concepts in
a preventive topical measure can ImmunoTherapy, INCIT, UMR 1302/EMR6001, Nantes, France
16
be considered Department of Oncologic Dermatology, Elias University Hospital Bucharest,
Carol Davila University of Medicine and Pharmacy, Bucharest, Romania
Level of evidence: 2–3 Randomized controlled trials, 17
Centre for Cell Biology and Cutaneous Research, Blizard Institute, Barts and The
systematic review of randomized London School of Medicine and Dentistry, Queen Mary University of London,
controlled trials59,113,159 London, UK
18
Department of Dermatology, University Hospital (UKSH), Kiel, Germany
Strength of consensus: 100% 19
Department of Dermatology, Copenhagen University Hospital -­Bispebjerg and
Frederiksberg, Copenhagen, Denmark
20
Department of Dermatology, Venereology and Allergology, Frankfurt University
TA BL E 2 0 Follow-­up of patients with AK. Hospital, Frankfurt, Germany
21
First Department of Dermatology, Aristotle University, Thessaloniki, Greece
22
Consensus-­based statement Université Paris Cite, AP-­HP Dermato-­oncology, Cancer institute APHP, Nord
Paris cité, INSERM U976, Saint Louis Hospital, Paris, France
23
Expert consensus Patients with AK should be educated for Centre for Dermatooncology, Department of Dermatology, Eberhard Karls
self-­skin examination and sun protection University, Tuebingen, Germany
24
and referred for skin examination due to Skin Cancer Center, Azienda Unità Sanitaria Locale -­IRCCS di Reggio Emilia,
the common risk of recurrences and the Reggio Emilia, Italy
25
Department of Dermatology, University of Modena and Reggio Emilia, Modena,
development of new lesions as well as of
Italy
other types of keratinocyte carcinomas 26
Department of General and Oncologic Dermatology, Ambroise Paré Hospital,
Strength of consensus: 100% APHP, & EA 4340 “Biomarkers in Cancerology and Hemato-­Oncology”, UVSQ,
Université Paris-­Saclay, Boulogne-­Billancourt, France
27
Department of Dermatology and Venereology, Sestre Milosrdnice University
Hospital Center, Zagreb, Croatia
available, with additional non-­invasive imaging techniques. 28
Skin Cancer Center, Department of Dermatology, Ruhr-­University Bochum,
If there is evidence for treatment resistance, retreatment or a Bochum, Germany
biopsy is recommended. 29
Department of Pediatric Dermatology, Colentina Clinical Hospital, Carol Davila
University of Medicine and Pharmacy, Bucharest, Romania
Patients with AK should be educated for self-­skin exam- 30
1st Department of Dermatology-­Venereology, National and Kapodistrian
ination and sun protection and referred for skin examination University of Athens, Andreas Sygros Hospital, Athens, Greece
due to the common risk of recurrences and the development 31
Dermatology Clinic, Maggiore Hospital, Department of Medical Sciences,
University of Trieste, Trieste, Italy
of new lesions as well as of other types of keratinocyte car-
cinomas. In patients with AKs and a history of cSCC, fol-
low-­up schedules should follow the guidelines for cSCC. F U N DI N G I N F OR M AT ION
Each follow-­up includes a thorough skin check of the chron- The development of the current set of guidelines was sup-
ically sun-­exposed body areas at a minimum. The frequency ported solely by funds of the EADO which were used to
of follow-­up should be based on the number and dynamics of mainly support the consensus meeting without honoraria
previous AKs, the history of previous keratinocyte carcino- and without reimbursement of travel costs.
mas, and the immune status and medication of the patient.
In immunosuppressed patients, close follow-­up visits with a C ON F L IC T OF I N T E R E S T S TAT E M E N T
dermatologist (e.g. every 3–6 months) are recommended. LK: None for the present manuscript. Consulting fees from
MSD, Merck, Abbvie, Janssen and honoraria for lectures
A F F I L I AT ION S and educational events by BMS, MSD, Novartis, Merck,
1
Department of Dermatology, Faculty of Medicine, University of Defence, Military Roche, Abbvie and Janssen. KP: None for the present manu-
Medical Academy, Belgrade, Serbia
2
UOC di Dermatologia, Dipartimento di Scienze Mediche e Chirurgiche script. Grants from Sanofi, Novartis, Abbvie and Almirall.
Addominali ed Endrocrino Metaboliche, Fondazione Policlinico Universitario A. Consulting fees from Sanofi, honoraria for lectures and
Gemelli – IRCCS, Rome, Italy educational events from Lilly, Sanofi and Sun Pharma,
 14683083, 0, Downloaded from https://onlinelibrary.wiley.com/doi/10.1111/jdv.19897 by Gerardo Palmisano - University Cattolica, Piacenza , Wiley Online Library on [21/03/2024]. See the Terms and Conditions (https://onlinelibrary.wiley.com/terms-and-conditions) on Wiley Online Library for rules of use; OA articles are governed by the applicable Creative Commons License
KANDOLF et al.     | 19

participation in advisory boards Abbvie and Almirall. Leo present manuscript. Grants to institution from MSD/
Pharma, Lilly, Janssen, Sanofi, Pierre Fabre, Sun Pharma, Merck, Philogen, Pierre Fabre, Regeneron, Roche, Sanofi-­
Biogen, Galderma and Philogen. JM: None for the pre- Genzyme, Novartis Pharma, Eisai. Honoraria for lec-
sent manuscript. Honoraria for lectures and educational tures and educational events from MSD/Merck, Pierre
events from Almirall, Pierre Fabre, ISDIN, BMS, MSD and Fabre, Regeneron, Roche, Sanofi-­ G enzyme, Novartis
Sunpharma, support for attending meetings and/or travel Pharma, Eisai, participation in Advisory boards MSD/
Almirall, ISDIN, Sunpharma, participation in advisory Merck, Pierre Fabre, Regeneron, Roche, Sanofi-­G enzyme,
boards Pierre Fabre, Almirall, stock options Athena tech Novartis Pharma, Eisai, Immunocore, Replimune and
and Dermavision. KM: None for the present manuscript. Seagen. RK: None for the present manuscript. Grants to
Grants from institution, Health Foundation Limburg, institution from AbbVie, Amgen, Biontech, BMS, Celgene,
ZonMW. Consulting fees from Sunpharma, Almirall, Galderma, Janssen, Leo, Lilly, Merck, MSD, Novartis,
honor