Two cases of Stevens-Johnson syndrome presenting severe ocular complications associated with immune checkpoint inhibitor

Abstract

Dear Editor, Immune checkpoint inhibitors (ICIs) have emerged as promising treatment options for various malignancies. However, their use is often associated with severe immune-related adverse events (irAEs), including Stevens-Johnson Syndrome (SJS) and toxic epidermal necrolysis (TEN), affecting approximately 1-2% of ICI-treated patients. 1 Although ophthalmic irAEs have been reported in around 1% of cases, the clinical manifestations of severe ophthalmic irAEs associated with SJS/TEN remain poorly understood. 1,2 Here, we present two cases experiencing irAE-SJS with severe ocular complications, evaluated using the SJS ophthalmologic severity score. 3 A 69-year-old man with stage IV renal cell carcinoma developed mild eyelid erythema and conjunctival hyperemia a few days after initiating nivolumab and ipilimumab in July 201X.After completing three courses of immunotherapy, he was referred to our department in September 201X, because his condition worsened, presenting with tense facial bullae and mucosal erosions on the cheek with a positive Nikolsky sign (Figure 1a,b).Ophthalmological examinations revealed conjunctival hyperemia, edema, pseudomembrane formation, and discharge (Figure 1c). Histopathological examination of a skin biopsy obtained from the forehead, where the erosive erythema with a positive Nikolsky sign was observed (Figure 1b), revealed a lichenoid reaction, intraepidermal and subepidermal bullae, and perivascular infiltration of lymphocytes, histiocytes, and eosinophils (Figure 1d). Direct immunofluorescence (DIF) tests of the basement membrane zone and intercellular space were negative (data not shown), and his blood tested negative for anti-desmograin 1 and 3 and anti-BP180 antibodies. Based on these findings, we ruled out autoimmune blistering diseases. The patient was concomitantly taking amlodipine and doxazosin, which tested negative in a druginduced lymphocyte stimulation test (DLST) while on oral prednisolone (PSL) at a dose of 20mg/day. Testing for infections such as Mycoplasma and herpes simplex virus (HSV) was not performed. Thus, we diagnosed the condition as an irAE-SJS. After immediate discontinuation of ICI therapy and concomitant drugs. He was treated with systemic corticosteroids (PSL 1 mg/kg/day), ophthalmic pseudomembrane debridement, antibiotics, immunosuppressive eye drops, and subconjunctival dexamethasone injections. Despite significant improvement in the skin rash, ocular symptoms persisted. Ophthalmologic severity scoring revealed severe epithelial defects, loss of palisades of Vogt, neovascularization, and hyperemia (grade 3) (Figure 1m). 3 Despite maintaining PSL at 10 mg/day, the patient experienced significant visual loss 6 months after discontinuing immunotherapy. During treatment for the irAE-SJS, he was at high risk of rupture of an abdominal aortic aneurysm, and steroid pulse therapy was considered a critical risk factor for elevated blood pressure; its rupture caused sudden death.A 64-year-old man with a history of esophagogastric junction cancer developed irAEdermatomyositis after completing seven courses of combination therapy with oxaliplatin, tegafur-gimeracil-oteracil potassium (TS-1), and nivolumab in April 202Y. He discontinued ICI therapy and underwent steroid pulse therapy, followed by oral PSL at 40 mg/day with sulfamethoxazole-trimethoprim (SMT-TMP) in May 202Y. Despite discontinuing ICI therapy and receiving PSL at 30 mg/day, he developed fever, conjunctival hyperemia, oral erosions, and a diffuse erythematous rash with a positive Nikolsky sign approximately on June 20, 202Y (Figure 1f-j). A skin biopsy taken from the back revealed epidermal necrosis, subepidermal bullae, interface dermatitis, and infiltration of lymphocytes and histiocytes into the dermal papillae and perivascular areas (Figure 1h). DIF tests of the basement membrane zone and intercellular space were negative (data not shown). Several concomitant medications, including SMT-TMP and metformin hydrochloride, which were potential causative agents, were immediately discontinued. All drugs tested negative in DLSTs while on PSL at a dose of 5mg/day. His blood tested negative for anti-desmograin 1 and 3 and anti-BP180 antibodies. Cytomegalovirus, HSV-1, and HSV-2 antigens were negative. We diagnosed the condition as an irAE-SJS, and the patient was treated with steroid pulse therapy on June 22, 202Y, followed by systemic corticosteroids (PSL 1 mg/kg/day), ophthalmic pseudomembrane debridement, and antibiotic and immunosuppressive eye drops.Although the skin rash improved significantly, ocular symptoms persisted. Ophthalmologic severity scoring revealed severe epithelial defects, superficial punctate keratopathy (SPK), and hyperemia (grade 3) (Figure 1k-m). 3 The patient experienced significant visual loss in September 202Y.In Case 1, the total ophthalmologic severity score for SJS was 19, with symblepharon formation leading to hand motion vision. Case 2 had a score of 17, with residual dry eye and SPK in the left eye causing significant visual loss. Despite the rapid improvement in the skin rash with standard treatments for irAE-SJS, ocular symptoms persisted for > 6 months, resulting in severe corneal damage and visual loss. This prolonged ocular involvement may be attributable to the sustained effects of ICI therapy, even after discontinuation. 4 According to the SJS/TEN treatment algorithm, steroid pulse therapy is recommended for patients with severe ocular involvement, specifically for those with an ocular score ≥ 2. 5 Furthermore, in patients with SJS who develop corneal damage, immediate administration of steroid pulse therapy in addition to high-dose systemic steroids (PSL at 1 mg/kg/day) should be considered because it may help prevent future visual loss. 5 Because of complications (unruptured abdominal aortic aneurysm), steroid pulse therapy could not be administered in Case 1. In contrast, although steroid pulse therapy was appropriately initiated two days after the onset of irAE-SJS in Case 2, ocular involvement progressed.Typical SJS is a severe skin and mucous membrane disorder characterized by erythema, erosions, and blisters. Histological findings of SJS include full-thickness epidermal necrosis with subepidermal blister formation. 3,5 On the other hand, skin and mucosal symptoms associated with irAEs during ICI therapy are often diverse. To differentiate these symptoms from SJS, it is essential to consider autoimmune blistering disorders such as bullous pemphigoid, pemphigus vulgaris, and paraneoplastic pemphigus. We described two cases in which patients undergoing ICI therapy developed erythema and erosions on the skin, along with ocular symptoms and oral mucosal erosions. After excluding autoimmune blistering diseases, we diagnosed these conditions as irAE-SJS.In conclusion, close collaboration between dermatologists and ophthalmologists is essential to optimize the management and prognosis of ocular complications associated with ICI therapy. Note: Blurring has been applied to the iris in Figure 1f to protect patient identity.