A 57-year-old woman underwent complete excision of a spitzoid melanoma of the left calf in 2021 (Breslow thickness, 0.88 mm); re-excision on 11 March 2021 demonstrated no residual tumor. In July 2025, she noted a progressively enlarging mass in the left inguinal region. Ultrasonography revealed a suspicious lymph node measuring 3.4 × 2.0 cm, and core needle biopsy confirmed metastatic melanoma with S100 and SOX10 positivity and a BRAF V600E mutation. Magnetic resonance imaging of the brain and contrast-enhanced computed tomography of the chest and abdomen showed no evidence of distant metastases. After completion of staging, the recurrence was classified as pT1bN2bM0, corresponding to the American Joint Committee on Cancer stage IIIB.

The patient received neoadjuvant ipilimumab (80 mg) plus nivolumab (240 mg) on 12 August 2025 and 2 September 2025. Left inguinal lymphadenectomy on 23 September 2025 demonstrated persistent melanoma in six of seven lymph nodes (pN3b), but restaging magnetic resonance imaging of the brain and computed tomography of the chest and abdomen on 3 October 2025 remained negative for distant disease.

On 10 October 2025 (59 days after the first dose), routine laboratory evaluation revealed markedly decreased adrenocorticotropic hormone and serum cortisol levels, consistent with secondary adrenal insufficiency. Clinically, the patient reported fatigue, hypotension, and tachycardia up to 110 beats per minute. Immune-related hypophysitis was diagnosed. Because hydrocortisone was temporarily unavailable, physiologic replacement with prednisolone (5 mg in the morning and 2.5 mg at midday) was initiated on 13 October 2025 with prompt symptomatic improvement and was converted to hydrocortisone (20 mg in the morning and 10 mg at midday; total 30 mg per day) on 28 October 2025.

Given the absence of a major pathological response and the presence of a BRAF V600E mutation, adjuvant therapy with dabrafenib and trametinib was planned. Initiation of that protocol was delayed by a dental infection treated with clindamycin on 20 October 2025, during which hydrocortisone was increased to 40 mg in the morning, 20 mg at midday, and 10 mg in the evening as stress dosing. Notably, outpatient laboratory testing on 24 October 2025- prior to targeted therapy- had already documented severe hepatitis in the treating records.

Finally, Dabrafenib and trametinib were initiated on 28 October 2025. The patient developed fever up to 39.2°C and was admitted on 6 November 2025 for progressive liver injury. On admission, aspartate aminotransferase (AST) and alanine aminotransferase (ALT) were 2307 U/L and 2171 U/L, respectively; total bilirubin was 3.6 mg/dl; and the international normalized ratio (INR) was 1.37. Intravenous methylprednisolone (32 mg per day) was started. Transaminases peaked at 3580 U/L (AST) and 2992 U/L (ALT), prompting escalation on 9 November 2025 to methylprednisolone 65 mg intravenously (approximately 1 mg per kilogram per day). Blood cultures remained repeatedly negative and C-Reactive Protein (CRP) levels were unremarkable; therefore, antibiotic therapy was not initiated. Under high-dose corticosteroids, transaminases decreased, whereas total bilirubin peaked later at 12.3 mg/dl on 20 November 2025.

Corticosteroids were subsequently tapered and transitioned to oral prednisolone from 29 November 2025. The patient was discharged on 3 December 2025 on prednisolone 37.5 mg per day with a slow gradual dose reduction; prednisolone was discontinued on 27 February 2026 without relapse. At follow-up on 21 January 2026, ALT was 39 U/L, gamma- glutamyl transferase (yGT) was 62 U/L, and S100 was 0.164 µg/L. Dabrafenib and trametinib remained paused, with re-initiation planned after hepatology reassessment. The clinical course is summarized in Table 1.

Table 1: Chronological timeline of the case.