Evolving utility of apremilast in dermatological disorders for off-label indications

Mehta, Hitaishi; Sharma, Apoorva; Dogra, Sunil

doi:10.1111/ced.15377

Cited by 6 publications

(7 citation statements)

References 70 publications

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“…By cross-linking with T cell membranes (e.g. CD4-positive and TH2 subsets), c-AMP can also inhibit T cell proliferation by acting as a regulator of T cells [7]. In terms of inflammatory regulation, PDE-4 may be involved in the regulation of eosinophil and neutrophil chemotaxis and degranulation [7,8].…”

Section: Inflammation and Pde-4mentioning

confidence: 99%

“…CD4-positive and TH2 subsets), c-AMP can also inhibit T cell proliferation by acting as a regulator of T cells [7]. In terms of inflammatory regulation, PDE-4 may be involved in the regulation of eosinophil and neutrophil chemotaxis and degranulation [7,8]. These effects are mediated by PDE-4-mediated increases in IL-8, leukotriene B4 and superoxide anion levels in neutrophils.…”

Section: Inflammation and Pde-4mentioning

confidence: 99%

“…The PDEs superfamily is divided into 11 species, ranging from PDE1-PDE11 [6]. PDE-4 is currently the most diverse subfamily of PDEs and is widely expressed in a variety of cell types [6,7]. These enzymes are intimately involved in a variety of physiological activities such as brain function, phagocyte/monocyte activation, cardiomyocyte contraction, vascular smooth muscle proliferation and neutrophil infiltration, to name a few.…”

Section: Introductionmentioning

confidence: 99%

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Advances in the Study of PDE4 Inhibitors in Dermatological Disorders

Jiang,

Wang,

et al. 2024

AJST

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Since the 1980s, phosphodiesterase 4 (PDE-4) has been one of the most prominent targets for the treatment of inflammatory diseases. More recently, a number of synthetic ligands targeting PDE-4 have received more attention in the academic and pharmaceutical communities and are expected to have applications in these diseases. Due to various potential side effects of PDE-4 inhibitors, there are several obstacles to the clinical translation of specific PDE-4 inhibitors from the preclinical to the clinical phase. Therefore, similar to roflumilast in chronic obstructive pulmonary disease, many PDE-4 inhibitors can take up to 30 years or even longer from development to clinical application. This article is a review of the development of PDE-4 inhibitors, such as crisaborole and apremilast, for use in skin disorders.

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Section: Inflammation and Pde-4mentioning

confidence: 99%

Section: Inflammation and Pde-4mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Advances in the Study of PDE4 Inhibitors in Dermatological Disorders

Jiang,

Wang,

et al. 2024

AJST

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“…In pemphigus, additional mechanisms may regulate Dsg internalization and p38MAPK signaling. The broad clinical application of PDE4 inhibitors such as apremilast in skin diseases may suggest that adrenergic signaling also is important for modulation of keratinocyte biology in other diseases 229 . For instance, coincidences of psoriasis and pemphigus and elevated risk in psoriasis patients to become affected by pemphigus may argue for similar mechanisms driving pathogenesis 230–232 …”

Section: Camp Stabilizes Keratinocyte Desmosomal Adhesion Via Phospho...mentioning

confidence: 99%

cAMP: A master regulator of cadherin‐mediated binding in endothelium, epithelium and myocardium

et al. 2023

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Regulation of cadherin‐mediated cell adhesion is crucial not only for maintaining tissue integrity and barrier function in the endothelium and epithelium but also for electromechanical coupling within the myocardium. Therefore, loss of cadherin‐mediated adhesion causes various disorders, including vascular inflammation and desmosome‐related diseases such as the autoimmune blistering skin dermatosis pemphigus and arrhythmogenic cardiomyopathy. Mechanisms regulating cadherin‐mediated binding contribute to the pathogenesis of diseases and may also be used as therapeutic targets. Over the last 30 years, cyclic adenosine 3′,5′‐monophosphate (cAMP) has emerged as one of the master regulators of cell adhesion in endothelium and, more recently, also in epithelial cells as well as in cardiomyocytes. A broad spectrum of experimental models from vascular physiology and cell biology applied by different generations of researchers provided evidence that not only cadherins of endothelial adherens junctions (AJ) but also desmosomal contacts in keratinocytes and the cardiomyocyte intercalated discs are central targets in this scenario. The molecular mechanisms involve protein kinase A‐ and exchange protein directly activated by cAMP‐mediated regulation of Rho family GTPases and S665 phosphorylation of the AJ and desmosome adaptor protein plakoglobin. In line with this, phosphodiesterase 4 inhibitors such as apremilast have been proposed as a therapeutic strategy to stabilize cadherin‐mediated adhesion in pemphigus and may also be effective to treat other disorders where cadherin‐mediated binding is compromised.

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“…Both genders are equally affected, having no apparent differences in the rate of occurrence as per skin type or race. Current management includes topical and systemic glucocorticoids, topical calcineurin inhibitors, antioxidants, and narrowband ultraviolet B phototherapy used to promote re-pigmentation; they all have varying degrees of success and adverse effects associated [9,10]. Hence, alternative and more efficacious therapies with better safety profiles for prolonged use are needed to treat vitiligo.…”

Section: Introductionmentioning

confidence: 99%

Apremilast Add-On Benefits Over Conventional Drugs (ABCD) in Unstable Non-segmental Vitiligo: A 12-Week Single-Center Randomized Controlled Trial

Sharma¹,

Bhardwaj²,

Dwivedi³

et al. 2023

Cureus

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BackgroundApremilast is an oral phosphodiesterase-4 enzyme inhibitor that modulates the immune system by increasing intracellular cyclic adenosine monophosphate levels and inhibiting inflammatory cytokines synthesis. We aimed to compare the efficacy and safety of add-on apremilast in combination therapy with standard treatment in patients with unstable, non-segmental vitiligo. MethodsThe study was a 12-week randomized, controlled, parallel-group, open-labeled trial. The control group received standard treatment (n=15), and the intervention group received 30 mg apremilast twice daily in addition to standard treatment (n= 16). Time to the first sign of re-pigmentation, halt in progression, and change in vitiligo area scoring index (VASI) score is the primary outcomes. Normality was assessed, and appropriate parametric and nonparametric tests were undertaken. ResultsThirty-seven participants were randomized into two groups, and analysis was done on thirty-one participants. Over the treatment duration of 12 weeks, the median time to observe the first sign of repigmentation was four weeks in the add-on apremilast group compared to seven weeks in the control group (p=0.018). The halt in progression was observed more in the add-on Apremilast group (93.75%) compared to the control group (66.66%) (p=0.08). The VASI score decreased by 1.24 in the add-on apremilast group and 0.05 in the control group (p= 0.754). Parameters including body surface area, dermatology life quality index, and body mass index reduced significantly, while the visual analog scale increased significantly in the addon apremilast group. However, results were comparable between groups. ConclusionsTreatment with add-on apremilast accelerated clinical improvement. It also reduced disease progression and improved the disease index among participants. However, add-on apremilast had a lower tolerability profile than the control group.

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Evolving utility of apremilast in dermatological disorders for off-label indications

Cited by 6 publications

References 70 publications

Advances in the Study of PDE4 Inhibitors in Dermatological Disorders

Advances in the Study of PDE4 Inhibitors in Dermatological Disorders

cAMP: A master regulator of cadherin‐mediated binding in endothelium, epithelium and myocardium

Apremilast Add-On Benefits Over Conventional Drugs (ABCD) in Unstable Non-segmental Vitiligo: A 12-Week Single-Center Randomized Controlled Trial

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