Antihypertensive medication is not associated with increased disease severity in atopic dermatitis in the TREATgermany registry
Moritz M. Hollstein, Stephan Traidl, Thomas Werfel, Jochen Schmitt

Abstract
Genes, proteins, chemicals, diseases, species, mutations and cell lines named across the full text — each resolved to its canonical identifier and authoritative record.
| Characteristics | Antihypertensive Medication | ||
|---|---|---|---|
| Overall | No | Yes | |
| n = 1,417 | n = 1,207 | n = 210 | |
|
| |||
| Mean (SD) | 25.80 (5.13) | 25.24 (4.71) | 29.05 (6.21) |
| n non‐missing | 1,399 | 1,193 | 206 |
| Median, Q1, Q3 | 25, 22, 28 | 24, 22, 27 | 28, 25, 32 |
|
| |||
| Female | 613 (43.5%) | 551 (45.8%) | 62 (30.1%) |
| Male | 795 (56.5%) | 651 (54.2%) | 144 (69.9%) |
| Non‐missing | 1,408 | 1,202 | 206 |
|
| |||
| Mean (SD) | 40.32 (14.58) | 37.72 (13.42) | 55.27 (11.71) |
| n non‐missing | 1,416 | 1,206 | 210 |
| Median, Q1, Q3 | 38, 28, 52 | 35, 26, 48 | 56, 48, 62 |
| Range | 18 ‐ 88 | 18 ‐ 82 | 25 ‐ 88 |
|
| |||
| Mean (SD) | 9.31 (16.18) | 7.23 (13.08) | 21.20 (24.86) |
| n non‐missing | 1,392 | 1,185 | 207 |
| Median, Q1, Q3 | 2, 0,11 | 1, 0, 6 | 9, 0, 40 |
| Characteristics | Antihypertensive Medication | |||
|---|---|---|---|---|
| Overall | No | Yes | p‐value | |
| n = 1,417 | n = 1,207 | n = 210 | ||
|
| 0.087 | |||
| Clear | 33 (2.36%) | 27 (2.26%) | 6 (2.94%) | |
| Almost clear | 123 (8.79%) | 99 (8.28%) | 24 (11.8%) | |
| Mild | 279 (19.9%) | 229 (19.2%) | 50 (24.5%) | |
| Moderate | 400 (28.6%) | 349 (29.2%) | 51 (25.0%) | |
| Severe | 409 (29.2%) | 361 (30.2%) | 48 (23.5%) | |
| Very severe | 155 (11.1%) | 130 (10.9%) | 25 (12.3%) | |
| n non‐missing | 1,399 | 1,195 | 204 | |
|
| 0.006 | |||
| Mean (SD) | 11.73 (7.83) | 11.95 (7.77) | 10.47 (8.07) | |
| n non‐missing | 1,401 | 1,197 | 204 | |
|
| 0.001 | |||
| Mean (SD) | 16.63 (7.68) | 16.91 (7.61) | 14.96 (7.93) | |
| n non‐missing | 1,399 | 1,195 | 204 | |
|
| 0.2 | |||
| Mean (SD) | 15.68 (12.78) | 15.79 (12.74) | 15.02 (13.04) | |
| n non‐missing | 1,409 | 1,201 | 208 | |
|
| 0.3 | |||
| Mean (SD) | 39.83 (16.55) | 40.00 (16.26) | 38.90 (18.16) | |
| n non‐missing | 1,411 | 1,204 | 207 | |
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Taxonomy
TopicsDermatology and Skin Diseases · Allergic Rhinitis and Sensitization · Food Allergy and Anaphylaxis Research
Dear Editors,
Eczema may be of multifactorial origin. It is characterized by skin thickening, redness, scaling, and pruritus. Atopic dermatitis (AD) may be seen as the major cause,1 even though some cases are difficult to diagnose: Patients with intrinsic AD may have late disease onset, preserved skin barrier function, and have metal contact hypersensitivity.2 Drug intake may also cause eczema.3 Recently, Ye and colleagues found prescription of antihypertensive medication increased eczematous dermatitis diagnoses in patients of 60 years and above from 9 per 1,000 patient‐years at baseline to 11 to 12 per 1,000 patient‐years.4 In particular, diuretics (HR: 1.21, 95% CI: 1.19–1.24) and calcium channel blockers (CCBs) (HR: 1.16, 95% CI: 1.14–1.18) showed an association with eczematous lesions. To investigate the association of antihypertensive drugs and AD, we analyzed real‐life data from the TREATgermany registry, one of the largest AD registries worldwide.5, 6
METHODS
TREATgermany, initiated in 2016, is a registry based on a prospective observational cohort study of patients with moderate to severe AD (ethics approval EK TUD 118032016, clinicaltrails.gov listing NCT03057860). Inclusion criteria, methods, and objectives have been published elsewhere.6 Data was extracted for adults (≥ 18 years) in March 2022. For the current analysis, the baseline visit data was used. Data including demographic information (e.g., age, gender), medication, and disease severity was used. Disease severity was assessed by objective SCORing Atopic Dermatitis (oSCORAD), Eczema Area and Severity Index (EASI), patient's global assessment (PGA), and patient‐oriented eczema measure (POEM). The Dermatology Life Quality Index (DLQI) was also assessed. Statistical analyses were conducted using the gtsummary (version 2.0.0) and ggplot2 (3.5.1) packages in R (4.2.1). Quantitative variables are presented as mean and standard deviation (SD).
RESULTS
Of the registry patients, 618 were female (43.6%) and 799 (56.4%) were male (data available on request). Age ranged between 18 and 88 years and averaged 40.4 years (median: 28 years, Q1: 28 years, Q3: 52 years; Table 1). Average disease onset had been at 9.3 years of age. 210/1,417 (14.8%) patients were prescribed antihypertensive medication (Table 1). 150/1,417 (10.6%) were ≥ 60 years. In this subgroup, mean age was 66.3 and ranged between 60 and 88 years (median: 64 years, Q1: 62 years, Q3: 69 years; Table 1), and 71/150 (47.3%) received antihypertensive medication. In the adult cohort and the subgroup ≥ 60 years, hypertensive medication was not associated with increased physician‐reported disease severity (oSCORAD, EASI) or the patient‐reported outcome PGA (Table 2). In the overall cohort, but not in the subgroup, antihypertensive medication was associated with a significantly lower (i.e. better) DLQI and POEM (Table 2).
DISCUSSION
Prior to 2024, research suggested a possible association between calcium channel blocker (CCB) intake and eczematous dermatitis (supplementary Table S1). Recently, Ye and colleagues reported multiple antihypertensive drugs are associated with increased eczematous dermatitis incidence in patients ≥ 60 years: diuretic drugs, CCBs, ACE inhibitors, and β‐blockers.4 The effect size was the smallest for ACE inhibitors (HR, 1.02; 95% CI, 1.00–1.04). It remained unclear whether the associations were causal and clinically meaningful.
From the five Read codes (clinical codes formerly used in the UK National Health Service to record patient data in both primary and secondary care) analyzed by Ye and colleagues, several may be directly attributed to AD in patients ≥ 60 years: “Atopic dermatitis/eczema,” “Infantile eczema,” “Flexural eczema,” and “Allergic (intrinsic) eczema.” Statistically, many other “Eczema NOS” cases may likewise be attributed to AD. Based on a cross‐sectional analysis of 203,813 participants in the All of Us research program, 51% of eczema cases in adolescents were classified as AD.1
Our analyses indicate that antihypertensive medication was not associated with increased disease severity in the full (adult) AD cohort or in the subgroup ≥ 60 years. In a different cohort of heart failure patients, our group was also able to show that pruritus, a major symptom of eczema, was not associated with antihypertensive medication.7 Despite a much smaller sample size in both analyses, these data point towards a negligible clinical relevance of antihypertensive medication in disease severity. From a theoretical standpoint, a causal relationship between eczema and antihypertensive medication would be surprising considering the different pharmacological activities of antihypertensive drugs. Specifically in the case of CCBs, a potential pathomechanism has been proposed.4 CCB‐induced iron uptake and retention in human keratinocytes may cause apoptosis and spongiosis.
These changes may clinically and histomorphologically resemble eczema. When comparing the presented results extracted from the TREATgermany cohort with the findings from Ye et al., the following should be acknowledged: First, TREATgermany does not register mild AD cases. Second, in TREATgermany, AD was diagnosed by dermatologists, while Ye et al. analyzed eczema read codes from primary care. Limitations of the present analyses can be seen in the exclusive use of baseline data, potentially overlooking changes in medication and disease status over time. In addition, relatively small number of patients in the subgroups and the study design restrict causal inferences and generalizability.
In conclusion, in the TREATgermany cohort antihypertensive drugs were not associated with increased disease severity.
FUNDING
TREATgermany is an academic, investigator‐initiated clinical disease registry that is financially supported by AbbVie Deutschland GmbH & Co. KG, Almirall Hermal GmbH, Galderma S.A., LEO Pharma GmbH, Lilly Deutschland GmbH, Pfizer Inc. and Sanofi.
CONFLICT OF INTEREST STATEMENT
J.S. reports institutional grants for investigator‐initiated research from the German Federal Joint Committee, German Ministry of Health, German Ministry of Research, European Union, German Federal State of Saxony, Novartis, Sanofi, ALK, and Pfizer. He participated in advisory board meetings as a paid consultant for Sanofi, Lilly, and ALK. J.S. serves the German Ministry of Health as a member of the German National Council for Health and Care. S.T. and M.H. declare no conflict of interest. T.W. has received honoraria for lectures or scientific advice on atopic dermatitis from AbbVie, Almirall, Galderma, Janssen/JNJ, LEO Pharma, Leti, Lilly, Novartis, Pfizer, and Regeneron/Sanofi.
Supporting information
Supplementary information
The reference list from the paper itself. Each links out to its DOI / PubMed record.
- 1Leasure AC , Cohen JM . Prevalence of eczema among adults in the United States: a cross‐sectional study in the All of Us research program. Arch Dermatol Res. 2022;315(4):999‐1001.35147780 10.1007/s 00403-022-02328-0 · doi ↗ · pubmed ↗
- 2Czarnowicki T , He H , Krueger JG , Guttman‐Yassky E . Atopic dermatitis endotypes and implications for targeted therapeutics. J Allergy Clin Immunol. 2019;143(1):1‐11.30612663 10.1016/j.jaci.2018.10.032 · doi ↗ · pubmed ↗
- 3Morin C , Joly P , Courville P , et al. [Chronic eczematiform eruption in the elderly]. Ann Dermatol Venereol. 2002;129(1 Pt 1):19‐22.11937924 · pubmed ↗
- 4Ye M , Chan LN , Douglas I , Margolis DJ , Langan SM , Abuabara K . Antihypertensive Medications and Eczematous Dermatitis in Older Adults. JAMA Dermatol. 2024;160(7):710.38776099 10.1001/jamadermatol.2024.1230 PMC 11112493 · doi ↗ · pubmed ↗
- 5Bosma AL , Musters AH , Bloem M , et al. Mapping exercise and status update of eight established registries within the TR Eatment of A Topic eczema Registry Taskforce. J Eur Acad Dermatol Venereol. 2023;37(1):123‐136.36018221 10.1111/jdv.18566 PMC 10087854 · doi ↗ · pubmed ↗
- 6Heratizadeh A , Haufe E , Stölzl D , et al. Baseline characteristics, disease severity and treatment history of patients with atopic dermatitis included in the German AD Registry TREA Tgermany. J Eur Acad Dermatol Venereol. 2020;34(6):1263‐1272.31721316 10.1111/jdv.16078 · doi ↗ · pubmed ↗
- 7Soltani S , Hollstein MM , Berliner D , et al. Symptom severity reflected by nyha grade is independently associated with pruritus in chronic heart failure patients. J Eur Acad Dermatol Venereol. 2024;38(7):1410‐1418.38420867 10.1111/jdv.19931 · doi ↗ · pubmed ↗
