Two cases of severe childhood-onset psoriasis successfully treated with risankizumab in patients with Down syndrome and morbid obesity

Abstract

Dear Editors, Down syndrome (DS) is a congenital chromosomal disorder resulting from the complete or partial trisomy of chromosome 21. It occurs in around one in every 700 live births and represents one of the most common chromosomal abnormalities. Beyond its characteristic developmental delay, DS is also associated with an increased risk of autoimmune disorders, such as autoimmune thyroid disease, celiac disease, and type 1 diabetes mellitus. Furthermore, several studies have reported that individuals with DS may exhibit a higher prevalence of cutaneous immune-mediated diseases, such as atopic dermatitis, alopecia areata, vitiligo, and psoriasis compared to the general population [1]. According to a systematic review of previous studies in 2022, the prevalence of psoriasis in populations with DS was reported to be 4.8% [1]. While the association between DS and psoriasis has yet to be fully elucidated, both conditions are thought to involve overlapping immunological dysregulation. In this report, we present two cases of severe childhood-onset psoriasis vulgaris in individuals with DS complicated by morbid obesity, whose cutaneous symptoms were markedly improved with risankizumab (RZB), an IL-23 inhibitor.Patient 1 is a 32-year-old male with DS who developed skin lesions at around the age of nine and was diagnosed with psoriasis at 11 years old. He received topical therapy for this condition. Due to a worsening of cutaneous symptoms, cyclosporine was administered from the age of 19 to 25. At the age of 26, the treatment was switched to apremilast, resulting in clinical stabilization. However, he became resistant to apremilast at the age of 30, leading to his referral to our department. On clinical examination, scaly infiltrated erythematous plaques were observed on the trunk and extremities including the palms and soles (Figure 1a). He was considered to have psoriasis vulgaris complicated by palmoplantar psoriasis. The psoriasis area and severity index (PASI) score was calculated as 17.1. He had a body mass index (BMI) of 38.2, indicating morbid obesity. Laboratory investigations revealed mildly elevated liver enzymes: aspartate aminotransferase (AST) at 47 U/L and alanine aminotransferase (ALT) at 94 U/L. Abdominal computed tomography (CT) demonstrated fatty liver. Treatment with RZB was initiated, and the erythematous plaques including sole and palm lesions had resolved with residual post-inflammatory pigmentation at 16 weeks after starting the biologic (Figure 1b). The patient has been undergoing treatment for two and a half years and has not yet developed any adverse events.Patient 2 is a 28-year-old female with DS who was diagnosed with psoriasis at around the age of nine due to the development of skin lesions on her scalp. Topical therapy was initially used. Due to exacerbation of cutaneous symptoms, apremilast was started at the age of 21, leading to disease stabilization. However, the disease flared up again at around the age of 27, prompting a switch to biologic treatment. Clinical examination revealed hyperkeratotic erythematous plaques distributed on the trunk and extremities (Figure 1c). She was considered to have psoriasis vulgaris. The PASI score was 39.3. BMI was 38, indicating morbid obesity. Serum AST and ALT levels were 32 U/L and 63 U/L, respectively, and fatty liver was identified on abdominal CT. The hemoglobin A1c level was elevated at 7.5%, consistent with diabetes mellitus. RZB was started, and after 16 weeks, the erythematous plaques had resolved, leaving residual postinflammatory pigmentation (Figure 1d). RZB is still being used for nine months without any adverse events.In both cases, psoriasis developed during childhood at around the age of nine. This is earlier than the typical age of onset for psoriasis vulgaris. Similar to psoriasis, in patients with DS, T helper type 1 (Th1) and Th17 subsets are enriched among nonregulatory CD4 + T cells, and the production of interferon-gamma (IFN-γ) from T cells and plasma levels of IL-17 and IL-22 are significantly higher compared to healthy controls [2]. Moreover, the trisomy of chromosome 21 is known to enhance sensitivity to IFN-γ, with the supernumerary copies of chromosome 21 conferring increased responsiveness to IFN-γ signaling [2]. Collectively, the abnormal immune dysregulation in DS similar to that in psoriasis may cause the early onset of the disease in our cases.There are no guidelines for choosing biologics in cases of psoriasis complicated by DS.Considering the immunologic abnormalities in DS as described above, any biologics can be considered for such patients. Although anti-TNF-α antibodies have been frequently used in the literature, a recent report presented cases of psoriasis complicated by DS successfully treated with ustekinumab, secukinumab, ixekizumab, or risankizumab [3]. Similarly, risankizumab exerted its effect sufficiently in our cases.However, more research is needed to decide which biologics are suitable for psoriasis patients with DS.In addition, interestingly, both of our cases showed severe obesity. They had been prone to obesity since childhood, and marked obesity became apparent several years after the onset of psoriasis. Both children and adults with DS have been reported to exhibit a higher prevalence of obesity compared to the general population [4]. Obesity has been recognized as a risk factor for the development of psoriasis and is further associated with increased severity of cutaneous symptoms, the development of joint manifestations, and reduced response to biologics. Furthermore, obesity increases the production of IFN-γ within adipose tissue, which induce differentiation of macrophages toward the pro-inflammatory M1 phenotype and contributes to the sustained production of inflammatory cytokines [5]. In addition, IFN-γ impairs adipocyte function and promotes the development of insulin resistance. In light of the above, DS is characterized by chronic systemic inflammation, and when compounded by obesityrelated adipose tissue inflammation, it may augment the risk of psoriasis development and promote increased severity. Thus, obesity due to DS may also contribute to the early development and repeated exacerbation of psoriasis, as well as to the complications of metabolic comorbidities, such as fatty liver and/or diabetes mellitus, in our cases.In conclusion, we present clinically intriguing cases that provide insights into the potential interplay among DS, psoriasis, and obesity, suggesting that systemic inflammation may influence each of these conditions.