Anais Brasileiros de Dermatologia

This publication is an update of the ‘‘Consensus on the therapeutic management of atopic dermatitis --- Brazilian Society of Dermatology’’ published in 2019, considering the novel, targeted-oriented systemic therapies for atopic dermatitis. The initial recommendations of the current consensus for systemic treatment of patients with atopic dermatitis were based on a recent review of scientiﬁc published data and a consensus was reached after voting. The Brazilian Society of Dermatology invited 31 experts from all regions of Brazil and 2 international experts on atopic dermatitis who fully contributed to the process. The methods included an e-Delphi study to avoid bias, a literature search and a ﬁnal consensus meeting. The authors added novel approved drugs in Brazil and the indication for phototherapy and systemic therapy for AD. The therapeutical response to systemic treatment is hereby reported in a suitable form for clinical practice and is also part of this updated manuscript.


Introduction
Tuberous Sclerosis Complex (TSC) is a neurocutaneous syndrome with variable phenotypes and autosomal dominant inheritance.It is due to pathogenic DNA alterations in either TSC1 (OMIM 605284) or TSC2 (OMIM 191092) genes and is characterized by benign tumors (hamartomas) in distinct organs, mainly the brain, skin, heart, kidneys, and lungs. 1,2he TSC1 gene (9q34) encodes hamartin, and TSC2 (16p13.3)codes for tuberin.Under physiological conditions, hamartin, tuberin and TBC1D7 (OMIM 612655) proteins form a cytoplasmic complex that suppresses cell growth by inhibiting the mechanistic Target of Rapamycin (mTOR). 1,3,4TSC1 or TSC2 bi-allelic loss of function impairs the inhibitory effect on the mTOR pathway, causing abnormal cell differentiation and growth, resulting in hamartomatous lesions (Table 1). 3---5ince 2012 the presence of a pathogenic alteration in TSC1 or TSC2 is a definite and sufficient criterion to diagnose TSC, regardless of the clinical findings. 4In 2021, the genetic diagnostic criterion was reaffirmed, and the combination of clinical criteria leading to definite or possible clinical diagnoses was maintained (Table 1). 3 There were however few changes in the clinical criteria.Multiple cortical tubers and/or radial migration lines have replaced the general term cortical dysplasia as a major criterion, and sclerotic bone lesions were reinstated as a minor criterion (Table 1). 3 Patients with definite, possible, or suspected TSC diagnosis should be followed up by a multidisciplinary team for the early identification of signs and symptoms, clinical management, and therapeutic intervention, resulting in better clinical outcomes. 3,4he association between TSC genotypes and phenotypes has been studied, highlighting TSC2 alterations more frequently among patients with earlier presentations of seizures, the presence of West syndrome (epileptic/infantile spasms with onset in infancy or early childhood associated with hypsarrhythmia and developmental regression), and more severe cognitive deficit. 2 Although genotypephenotype analyses mainly focus on neurological and renal signs, which are the major causes of morbidity and mortality, 3 dermatological signs are one of the earliest clinical presentations, and their detection can lead to suspected TSC. 5,6SC has been often underdiagnosed notably in developing countries. 7The early onset of some cutaneous signs is highly suggestive of TSC (Table 1).Given their importance to the diagnosis and treatment of this neurocutaneous genetic disorder, this study aimed at characterizing the skin lesions of 37 patients with definite clinical and genetic diagnoses of TSC.The authors additionally classified patients according to the gene involved and verified in each gene category the frequency of specific skin lesions.The authors describe in the TSC cohort a significant association between ungual fibromas and TSC2 alterations.Patients included in the study were clinically diagnosed with TSC according to Northrup et al. (2013)  4 and had a pathogenic DNA variant previously identified by Sanger, Multiplex Ligation-dependent Probe Amplification (MLPA) or Next-Generation Sequencing (NGS) in either TSC1 (NM 000368.4)or TSC2 (NM 000548.3)genes at the University of São Paulo, São Paulo, Brazil (data not shown).After the publication of the updated diagnostic criteria (Northrup  et al., 2021), 3 data were reviewed accordingly and no alteration was made.In this ambispective study, once the family had provided written informed consent, the medical records were retrospectively reviewed.Then patients were prospectively seen by the Pediatric Dermatology team during a joint effort for the care of TSC patients in Oct/2021 and Oct/2022.Information (identification, age, dates, genetic study result, and description of the skin lesions) was registered and clinical lesions were photographed.Data were statistically analyzed in Excel ® .

Subjects and methods
The sample was non-probabilistically and systematically selected by convenience, in order of appointment and admission to the study.Measures of central tendency and dispersion were expressed as mean ± standard deviation for continuous variables with symmetrical distribution and median (Interquartile Range [IQR]) for those with asymmetrical distribution.Categorical variables were expressed as absolute and relative frequencies.The Mann-Whitney non-parametric test was used to estimate the difference Underlined terms highlight updated criteria. 3efinite TSC clinical diagnosis: two major features or one major plus two or more minor features.Possible TSC clinical diagnosis: one major criterion or at least two minor criteria.
a Combination of these two major criteria without other features does not meet the criteria for a definite diagnosis.
between continuous variables with asymmetric distribution and the Fisher's exact and Pearson's Chi-Square tests were used to estimate the difference between categorical variables.All tests considered a minimum significance level of 5%, 10% type II error, and magnitude of the effect of estimated difference between mutated genes four times.

Results
The study sample comprised a total of 37 patients (36 unrelated patients), with definite clinical and genetic diagnoses of TSC, including 20 (54.1%) boys and 17 (45.9%)girls.All of them had at least one dermatological sign considered as a TSC diagnostic criterion (Table 1).All patients had first skin lesion onset before 18 years of age.The median age at TSC diagnosis was 18 months (IQR: 8---60), and the median age at dermatologic evaluation was 16 years (IIQ: 9---24.5).Twenty-seven families could inform the first cutaneous sign identified in the patient.The patients' median age at its onset was 3 months (IQR: 0---19), and the most frequent skin lesion first identified was hypomelanotic leaf macula (25/27; p < 0.001).Considering patients according to sex, no difference was observed in first cutaneous signs, age at its onset, age at TSC diagnosis, or mutated gene (p > 0.05; Table 2).
All 37 TSC patients had DNA assessed by sequencing, including two siblings.The 36 pathogenic DNA alterations were found in the TSC1 gene in four unrelated individuals (11.1%) and in TSC2 in 32 (88.9%) patients, defining a TSC2:TSC1 mutation ratio of 8:1.There were three frameshifting variants and one large deletion in TSC1.The two siblings had a TSC1 pathogenic mutation, summing up five individuals with alterations in this gene.TSC2 mutations comprised seven frameshiftings, seven unique missense, six unique nonsense, three splicing, and three in-frame deletion variants, plus three large deletions and one large duplication.One TSC2 nonsense variant was found in three unrelated patients, totaling 32 patients with TSC2 mutations.
The frequencies of TSC1 and TSC2 pathogenic alterations were similar between sexes (Table 2; p = 0.34).Age at first skin lesion onset and age at TSC diagnosis were available for 5 and 22 patients with TSC1 and TSC2 pathogenic DNA alterations, respectively.There were no significant differences between patient groups with distinct altered genes when comparisons were made for ages at first skin lesion, at TSC diagnosis, or type of first skin lesion (Table 3; p > 0.05).

Discussion
TSC-associated skin lesions should be recognized by general practitioners and pediatricians as they are commonly the first noticeable signs of this disease and comprise four of the eleven major criteria and three of the seven minor criteria for the clinical diagnosis of TSC (Table 1).Early diagnosis is important for follow-up and appropriate treatment initiation, limiting the growth of lesions and related morbidity.MTOR inhibitors received clinical approval as oral therapy for specific TSC lesions, such as everolimus to treat subependymal giant cell astrocytoma, 8 renal angiomyolipoma, 9   adjunctive treatment of TSC-partial onset seizures 10 ; and sirolimus (rapamycin) for lymphangioleiomyomatosis. 11In clinical studies, topical sirolimus decreases angiofibromas, hypomelanotic macules, or cephalic plaques, and is well tolerated by children. 12---14Therefore, TSC skin lesions are not only important for the diagnosis of the disease but can be effectively treated by targeting mTOR hyperactivation.

and as
In this cohort of 37 patients with definite clinical and genetic diagnoses of TSC, the most common initial skin sign was hypomelanotic macules, which were also the most frequent dermatological presentation (92.5%).Hypomelanotic macules occur in approximately 90% of patients and have their onset usually at birth or in early childhood, 6 as observed (n = 27 informative cases; mean age of 3 months; Table 2).Other first skin signs less often observed were confetti-like lesions, fibrous cephalic or intraoral fibrous plaques (Table 2).Among one-month-old infants with at least one suggestive sign of TSC, hypomelanotic macules were the cause of the diagnosis suspicion in 31% of them. 15n patients up to four months of age, hypomelanotic macules were the initial sign in 35%. 7The present study did not assess non-dermatological signs.It confirms that among skin lesions hypomelanotic macules are the most frequent first sign in TSC patients (Table 2).
Facial angiofibromas were the second most frequent lesion (87.5%), followed by cephalic plaques (80%).Overall angiofibroma estimated occurrence (75%) 6 rises in the second decade of life upon puberty. 7Thus, angiofibromas' frequency depends on the mean age of the patients at enrollment in the cohort.Shagreen plaques are generally observed from the first decade of life on, more commonly after five years of age, 5,16 in a frequency (50%) similar to the one observed by us (55%).Confetti-like lesions were detected in 67.5% of patients.They usually start in the first decade  of life but have limited usefulness in adults as a diagnostic criterion, as they can develop as a consequence of chronic sun exposure. 6A history of onset in early childhood is suggestive of TSC. 5 Intraoral fibromas occur in 20%---50% of patients, more frequently in adults than in children. 6Accordingly, the authors detected these lesions in ten TSC patients (25%).Skin lesion distribution was not different between sexes (Table 2).Gingival fibromas have been identified more frequently among males than females. 17he mean age at diagnosis was 18 months in this sample, 15 months later than the mean age at first skin sign detection, and later than the mean age at diagnosis from a recent study (n = 86; 6 months) that also adopted the same diagnostic criteria. 4In this German study, cardiac rhabdomyoma, a major TSC clinical criterion (Table 1), detected by prenatal fetal imaging contributed to diagnosing earlier the disease in 22% of cases. 6It appears that patients in the Brazilian cohort have heterogeneous access to fetal imaging analyses and depend more commonly on tertiary referral hospitals for the establishment of the TSC diagnosis.
Genetic testing is useful to confirm the diagnosis of TSC, particularly in clinically challenging cases in the early stages.In this analysis, TSC1 and TSC2 pathogenic variants were observed in 13.5% (5/37) and 86.5% (32/37) of patients, respectively, reasonably above the ratio observed  by other studies. 17---21The predominance of TSC2 pathogenic genetic alterations, eight times more common than TSC1 pathogenic variants, was observed among females (8-fold among females and 3.4-fold among males; Table 2).The chance of a TSC2 mutation was 10-fold higher in the presence of ungual fibromas, although these data should be viewed with caution because of the wide confidence interval associated with the small number of cases with a TSC1 mutation.
A more severe neurological phenotype may be associated with TSC2 mutation, 17---21 while skin lesions and genotype association appear more variable among studies, except for facial angiofibromas.The TSC natural history database disclosed a significant association between TSC2 mutation and angiofibromas. 22The mean grade of facial angiofibroma appears to be higher in patients with a TSC2 than TSC1 alteration. 18The authors did not observe a difference in the number of angiofibromas, which could be due to the low number of patients with a TSC1 mutation, although there appears to be a trend of increasing numbers of angiofibromas in the presence of a TSC2 gene muta-tion (Fig. 4A).In another study, children at age of two years with a TSC1 gene mutation had less hypomelanotic macules and facial angiofibromas than those with a TSC2 genetic alteration. 23By contrast, Shagreen patches have been observed more frequently in patients with a TSC1 than TSC2 gene alteration. 17Among 38 TSC patients with at least one cutaneous sign, dermatological examination alone was sufficient to establish a definite diagnosis of the disease in 34, demonstrating the importance of early recognition of skin lesions. 24,25he TSC cohort from a reference clinical center in Southern Brazil discloses the association between ungual fibromas and TSC2 genetic alteration.One limitation is the small sample size and the limited number of patients with TSC1 pathogenic variants.Further studies are necessary to evaluate TSC dermatological presentation association with genotype.The authors confirm the importance of detecting skin lesions for early identification of TSC.Clinicians should be aware of TSC's possible mucocutaneous lesions, their variable expressivity, and the natural history of the disease. 26

Figure 1 (
Figure1 (A---B) Hypomelanotic macules on the patient's abdomen (A) and shagreen plaque on the back of an adolescent patient (B).

Figure 2 (
Figure 2 (A---B) Confetti-like lesions (arrows) in the anterior tibial region (A) and ungual fibromas in 4 th and 5 th fingers of an adult patient (B).

Table 1
Major and minor criteria for the clinical diagnosis of TSC according to Northrup et al. (2021) 3 .

Table 2
Age at onset of first skin lesion, TSC diagnosis, and first cutaneous signs according to sex.

Table 3
Age at onset of first skin lesion, TSC diagnosis, and total cutaneous signs according to the gene harboring the pathogenic alteration.
b n = 22.c Mann-Whitney test.d Fisher's exact test.