The novel use of mu-opioid receptor antagonism for the treatment of refractory pruritus in Kyrle’s disease☆☆☆

Abstract

Dear Editor, Kyrle’s disease (KD) is an acquired perforating dermatosis commonly associated with underlying systemic diseases, particularly chronic renal disease; in fact, KD occurs in approximately 10% of patients with end stage renal disease (ESRD) who require hemodialysis (Joseph et al., 1996). This disease is more prevalent in women, with a female-to-male ratio of up to 6:1; and has no racial predilection. Cutaneous manifestations of KD typically present as intensely pruritic, hyperkeratotic papules with central keratotic plugs commonly localized on the extensor surfaces of the lower extremities. Patients will often times exhibit the Koebner phenomenon, whereby skin lesions develop at sites of trauma and, thus, are exacerbated by scratching. The pruritus seen in this population greatly impacts quality of life, contributing to poor sleep, anxiety, and depression (Pisoni et al., 2006). As the number of patients on hemodialysis worldwide continues to grow, so does the demand for effective management of Kyrle’s disease. To date, there have been no controlled studies or guidelines put into place regarding the treatment of KD. Currently, therapeutic recommendations exist on the basis of small case studies, where underlying disease management and pruritus alleviation is the main focus. While the optimal treatment for KD remains unclear, current therapies reported in the literature include phototherapy, topical or intralesional corticosteroids, antihistamines, isotretinoin, immunosuppressive agents, and various destructive therapies. This article highlights an alternative therapeutic option for this increasingly prevalent disease. We describe the case of a 64-year-old male patient with dialysis-dependent ESRD who presented with a seven-month history of intractable pruritus and numerous hyperkeratotic papules with white compact cores on the extensor surfaces of his lower extremities (Fig. 1A). Despite adequate management of his underlying disease, as well as the use of topical triamcinolone and oral gabapentin, the patient reported that his lesions had progressively worsened. He rated his pruritus as a 10/10 and ‘‘unbearable, especially at night.” A skin-biopsy specimen revealed epidermal acanthosis and papillomatosis with deposits of elastic fibers and degraded collagen in the papillary dermis, consistent with KD. Subsequently, intranasal butorphanol, a medication with kappa-agonist and mu-antagonist activity, was prescribed once daily (1 mg spray per nostril) to address the patient’s pruritus; the previously used topical and oral agents were discontinued.