Topical pimecrolimus versus betamethasone for oral lichen planus: a randomized clinical trial.
Betamethasone
CD133
Cancer stem cells
Oral lichen planus
Pimecrolimus
Journal
Clinical oral investigations
ISSN: 1436-3771
Titre abrégé: Clin Oral Investig
Pays: Germany
ID NLM: 9707115
Informations de publication
Date de publication:
Feb 2019
Feb 2019
Historique:
received:
29
01
2018
accepted:
05
06
2018
pubmed:
18
6
2018
medline:
1
8
2019
entrez:
18
6
2018
Statut:
ppublish
Résumé
Oral lichen plans (OLP) is a potentially malignant inflammatory mucocutaneous disease. CD133 is an investigated surface marker for cancer stem-like cells (CSCs) that may be involved in tumor initiation in head and neck carcinomas. We compared short-term clinical effectiveness of topical pimecrolimus as selective inflammatory cytokine release inhibitor with betamethasone cream for erosive/atrophic OLP and investigated the influence of this therapy on CD133 expression. Thirty patients were randomly assigned into two equal groups to receive topical pimecrolimus (group I) or betamethasone (group II) four times daily for 4 weeks. A marker lesion in each patient were assessed at baseline using clinical score (CS) and visual analog scale (VAS) then at 1, 2, and 4 weeks and after 4 weeks of treatment-free period. CD133 expression was detected in pre- and post-treatment immunostained sections. Both drugs showed a reduction in CS, VAS, and CD133 expressions after treatment termination (p < 0.001). Pimecrolimus-treated lesions showed significant higher 1st week reduction in severity (33.1% (22.2)), pain score (57.53% (14.27)), less recurrence in follow-up period and less CD133 expression by the end of the 1st 4 weeks compared with betamethasone. Pimecrolimus showed earlier clinical response and less recurrence rate compared with standard topical corticosteroid in symptomatic OLP lesions, and both treatment reduced CD133-positive CSC population. The study proved the benefits of topical pimecrolimus in early management of painful lesions of OLP and its ability to inhibit CSCs, suggesting a possible role in reducing risk of malignant transformation.
Identifiants
pubmed: 29909565
doi: 10.1007/s00784-018-2519-6
pii: 10.1007/s00784-018-2519-6
doi:
Substances chimiques
AC133 Antigen
0
Glucocorticoids
0
Immunosuppressive Agents
0
pimecrolimus
7KYV510875
Betamethasone
9842X06Q6M
Tacrolimus
WM0HAQ4WNM
Types de publication
Journal Article
Randomized Controlled Trial
Langues
eng
Pagination
947-956Références
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