Science and Research

Type 2 responses determine skin rash during recombinant interleukin-2 therapy

The skin is the organ most often affected by adverse drug reactions. Although these cutaneous adverse drug reactions (CADRs) often are mild, they represent a major burden for patients. One of the drugs inducing CADRs is aldesleukin, a recombinant interleukin-2 (recIL-2) originally approved to treat malignant melanoma and metastatic renal cell carcinoma which frequently led to skin rashes when applied in high doses for anti-cancer therapy. Skin rashes and other side effects, together with poor efficacy led to a drawback of the therapeutic, but modified recIL-2 molecules are on the rise to treat both cancer and inflammatory diseases such as autoimmunity. Still, pathophysiological mechanisms of recIL-2-induced skin rashes are not understood. In the study reported here, a hypothetical literature-based immune-related adverse outcome pathway (irAOP) was developed to identify possible key cells and molecules in recIL-2-induced skin rash. Using this approach, a hypothesis was formed that the induced immune response predominantly is Type 2-driven by T-helper and innate lymphoid cells, leading to the occurrence of cutaneous side effects during recIL-2 therapy. This paper further discusses mechanisms beyond the proposed irAOP which might add to the pathology but currently are less-studied. Together, this hypothetic irAOP forms a basis to clarify possible cellular and molecular interactions leading to recIL-2-induced skin rash. This might be used to adapt existing or develop new test systems to help predict and prevent cutaneous side effects in future IL-2-based or similar therapies.

  • Sommer, C.
  • Neuhaus, V.
  • Gogesch, P.
  • Flandre, T.
  • Dehmel, S.
  • Sewald, K.

Keywords

  • Humans
  • *Interleukin-2/adverse effects/administration & dosage/immunology/analogs &
  • derivatives
  • *Exanthema/chemically induced/immunology
  • *Recombinant Proteins/adverse effects/administration & dosage/immunology
  • Drug Eruptions/diagnosis/immunology/etiology/therapy
  • Melanoma/drug therapy/immunology
  • Skin/pathology/immunology/drug effects
  • Immunity, Innate/drug effects
  • Animals
  • Carcinoma, Renal Cell/drug therapy/immunology
  • Kidney Neoplasms/drug therapy/immunology
  • IL-2 therapy
  • Immunotherapy
  • adverse outcome pathway
  • cutaneous adverse drug reactions
  • imSAVAR
  • type 2 immunity
Publication details
DOI: 10.1080/1547691x.2024.2343359
Journal: J Immunotoxicol
Pages: S48-s59 
Number: sup1
Work Type: Review
Location: BREATH
Disease Area: LC
Partner / Member: ITEM
Access-Number: 39655497

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