Eric H. Kowalski scite author profile

Prurigo nodualris (PN) is a chronic condition with highly pruritic, hyperkeratotic papules or nodules arising in the setting of chronic pruritus. While PN may serve as a phenotypic presentation of several underlying conditions such as atopic dermatitis, chronic kidney disease-related pruritus, and neurological diseases, it represents a distinct clinical entity that may persist despite the removal of the underlying cause, if one is identified. Neuronal proliferation, eosinophils, mast cells, and small-fiber neuropathy play a role in the production of pruritus in PN, although the exact mechanism has not yet been established. Identifying an underlying cause, if present, is essential to prevent recurrence of PN. Due to often present comorbidities, treatment is typically multimodal with utilization of topical and systemic therapies. We performed a PubMed/MEDLINE search for PN and present a review of recent developments in the treatment of PN. Treatment typically relies on the use of topical or intralesional steroids, though more severe or recalcitrant cases often necessitate the use of phototherapy or systemic immunosuppressives. Thalidomide and lenalidomide can both be used in severe cases; however, their toxicity profile makes them less favorable. Opioid receptor antagonists and neurokinin-1 receptor antagonists represent two novel families of therapeutic agents which may effectively treat PN with a lower toxicity profile than thalidomide or lenalidomide.

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Iatrogenic calcinosis cutis secondary to calcium chloride successfully treated with topical sodium thiosulfate

Abbott

Kowalski

Klein

et al. 2020

JAAD Case Reports

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Epidermal expression of eotaxins and thymic stromal lymphopoietin in eosinophil rich dermatoses

et al. 2019

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From bench to bedside: evolving therapeutic targets in autoimmune blistering disease

Kridin

Kowalski

Kneiber

et al. 2019

Acad Dermatol Venereol

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Autoimmune blistering diseases comprise a group of heterogenous conditions characterized by the loss of tolerance and subsequent development of autoantibodies targeting epidermal and subepidermal adhesion proteins. Blisters and erosions form on the skin and mucous membranes leading to significant morbidity and mortality. Traditional therapies rely on systemic immunosuppression. Advancements in our understanding of the pathophysiology of pemphigus and pemphigoid have led to the development of molecules which target specific pathways involved in induction and perpetuation of disease. In this review, we outline the novel therapeutic strategies including B‐cell depletion, T‐regulatory cell repletion, cell signalling inhibitors and small molecular inhibitors, inhibitory monoclonal antibodies, as well as complement inhibition. We additionally review their current level of clinical evidence. We lastly review therapeutics targets gleaned from the experimental epidermolysis bullosa acquisita mouse model. These emerging treatments offer an exciting progression from basic science discoveries that have the potential to transform the treatment paradigm in autoimmune blistering diseases.

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Pemphigus subtype: a confounder in determining the association of oral involvement with post‐rituximab relapses

Kneiber

Kowalski

Kridin

et al. 2019

Dermatologic Therapy

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Reductive cleavage versus hydrogenation of allyl aryl ethers and allylic esters using sodium borohydride/catalytic ruthenium(III) in various aqueous solvent mixtures

Babler

White

Kowalski

et al. 2011

Tetrahedron Letters

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Eric H. Kowalski

Epidermolysis bullosa acquisita: A comprehensive review

Serum and blister fluid levels of cytokines and chemokines in pemphigus and bullous pemphigoid

<p>Treatment-resistant prurigo nodularis: challenges and solutions</p>

Iatrogenic calcinosis cutis secondary to calcium chloride successfully treated with topical sodium thiosulfate

Epidermal expression of eotaxins and thymic stromal lymphopoietin in eosinophil rich dermatoses

From bench to bedside: evolving therapeutic targets in autoimmune blistering disease

Pemphigus subtype: a confounder in determining the association of oral involvement with post‐rituximab relapses

Reductive cleavage versus hydrogenation of allyl aryl ethers and allylic esters using sodium borohydride/catalytic ruthenium(III) in various aqueous solvent mixtures

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