Psoriasis affects male and female patients equally. Two-thirds of patients are thought to have mild disease, and one-third of patients are thought to have more severe involvement. Psoriasis is found in practically all racial groups and is thought to affect approximately 2% of the world’s population. Although psoriasis is a global disease, there are some regional variations in prevalence, with rates varying from 0.4% in Asians to 2.6% in the United States and 2.9% in Denmark. In Africa, there is a higher prevalence in East Africans as opposed to West Africans, which may help explain racial differences within the United States. Interestingly, a study of 26,000 South American Native Americans did not document a single case of psoriasis.

Psoriasis may appear at any age, but it most commonly presents between the ages of 15 and 30. An earlier age of onset and family history have been associated with particular HLA class I antigens, most notably HLA-Cw6. Based on this finding, Henseler and Christophers¹ proposed that 2 different forms of psoriasis exist: type I psoriasis, with onset before the age of 40; and type II psoriasis, with age of onset after the age of 40. Both types of psoriasis respond similarly to treatment.

Psoriasis is characterized clinically by red and scaly plaques sharply demarcated from normal skin. Histologically, it is characterized by marked proliferation of keratinocytes, altered epidermal differentiation, and proliferation of endothelial cells accompanied by an influx of a variety of inflammatory cells. The development of a psoriatic lesion is a complex and multicellular process that involves keratinocytes, T cells, dendritic cells, macrophages, mast cells, endothelial cells, and neutrophils. Cytokines and growth factors initiate and sustain inflammation in this process through pathways that involve cells of both the innate and the acquired immune systems. Initial pinhead-sized macular lesions show edema and mononuclear cell infiltrates within the upper dermis. The overlying epidermis becomes spongiotic, and there is a focal loss of the granular layer. As the plaque matures, the epidermis becomes thickened in the center with increasing parakeratosis, capillary elongation, and perivascular infiltration of various types of immune cells. Mature psoriatic lesions contain elongated and uniform rete ridges with thinning of the epidermis overlying the dermal papillae. The tips of the rete ridges may become clubbed with dilated, tortuous capillaries in the dermal papillae. There is typically confluent parakeratosis and hyperkeratosis.⁵ More inflammatory cells are present with CD4+ T cells and dendritic cells in the upper dermis and CD8+ T cells in the epidermis. Neutrophils are commonly seen in psoriatic lesions and form characteristic collections in the spinous layer (spongiform pustules of Kogoj) and in the stratum corneum (Munro microabscesses). Eosinophils are not seen in psoriasis, unless the disease is drug induced.

The role of T cells in psoriasis was first documented in the 1980s, and the last 30 years of scientific and clinical research...