Treating Cutaneous Immune-Related Adverse Events from Immune Checkpoint Blockade

Immune checkpoint inhibitors (ICPis) have revolutionized outcomes in various advanced malignancies. Therapeutic restoration of a robust T-cell response against malignant cells is also at the root of distinct cutaneous immune-related adverse events (cirAEs). As approved indications for ICPis increase and interdisciplinary collaboration with oncology grows, identifying the most common skin toxicities from ICPis, particularly on melanin-rich skin,¹ and understanding treatment strategies are increasingly crucial for dermatologists. This brief review highlights common cirAEs and summarizes the latest evidence for interventions.

Around one-third of patients on ICPi monotherapy and threequarters of patients on combination regimens experience cirAEs, which are graded by Common Terminology Criteria for Adverse Events² (Table 1). Morbilliform dermatoses, pruritus, lichenoid eruptions (Figure 1), psoriasiform dermatitis (Figure 2), and bullous pemphigoid (Figure 3) are frequently seen with immune checkpoint blockade.³ The current treatment recommendations, summarized in Table 1, are based on level III-IV evidence of retrospective descriptive studies and expert consensus.4-6 Although topical and systemic corticosteroids are the mainstay, refractory cases warrant oral retinoids and targeted biologics based on clinical or histopathologic morphology.^5-6 Growing evidence proposes that immunotherapies shift cytokine axes systemically, clinically manifesting as cirAEs.⁷ More data about ICPi antitumor efficacy with concomitant targeted cytokine blockade are needed.