Ustekinumab for Treatment of Plaque Psoriasis in a Patient With Down Syndrome

Down syndrome (DS) is a chromosomal disorder resulting by triplication of chromosome 21, with an estimated prevalence of 1 per 600 to 1 per 800.¹ This congenital condition is characterized by intellectual disability, ranging from mild to severe, and typical physical features such as hypotonia, epicanthal folds and upward slanting eyes, Brushfield spots, flat nasal bridge, small mouth and ears, large tongue, excess nuchal skin, a single transverse palmar crease, and clinodactyly of the fifth fingers.^2,3 Down syndrome includes an increased risk of congenital heart disease (50%), seizure disorders (2.6% to 8.8%) atlantoaxial or atlantooccipital instability (10% to 30%), leukemia (<1%), deafness (75%), serous otitis media (50% to 70%), gastrointestinal atresias (12%), cataracts (15%), severe refractive errors (50%), and hypothyroidism (15%), among many other physical and psychosocial difficulties. ^1,2 Although main physical and psychosocial features have been well-characterized in DS, correlated skin disorders have been rarely investigated. It is known that DS is associated with accelerated aging and an increased incidence of acne vulgaris, anetoderma, cheilitis, cutis marmorata, elastosis perforans serpiginosa, fissured and geographic tongue, onychomycosis, palmo-plantar hyperkeratosis, pityriasis rubra pilaris, psoriasis, seborrheic dermatitis, syringoma, tinea pedis, alopecia areata, vitiligo, atopic dermatitis, and xerosis.^2,4-9 The high incidence of immune-related disorders of the skin, such as alopecia areata, vitiligo, atopic dermatitis, and psoriasis, seems to be correlated to an immunological imbalance associated with a T-cell dysfunction.^10,11 Evidences regarding the impaired immune response occurring in DS are still controversial: defects in both humoral and cellular immunity might increase the susceptibility to infections and the incidence of malignancies that are commonly observed in individuals affected by DS.^12-13 The incidence of psoriasis in the general population is 1% to 3%,14 whereas it has been reported as 0.5% to 8%^5,6 among patients with DS. Down syndrome-related psoriasis is a challenging condition considering a) the large number of comorbidities, b) the increased risk of malignancies and, c) factually, therapeutic agents are immunosuppressive or organ-specific toxic, or both. It is still debated whether the use of biologics in the treatment of DS-related psoriasis is safe. We report the case of a DS-correlated psoriasis patient treated for a long-term with various biologics, showing a satisfactory safety profile while undergoing treatment, and experiencing an excellent clinical response to uteskinumab after failing anti-TNF α therapies.

We describe the case of a 31-year-old Caucasian patient with DS suffering from plaque type psoriasis since the age of 14. The physical features include epicanthal folds and upward-slanting eyes, flat nasal bridge, small mouth and ears, large tongue, short neck, clinodactyly of the fifth fingers, plantar crease between first and second toes. The patient, showing mild intellectual disability, is socially well-integrated, with a regular job as well as regular social life.