Pharmacology and Therapeutics
Dermatologic toxicities to targeted cancer therapy: shared clinical and histologic adverse skin reactions
Version of Record online: 24 JUL 2013
© 2013 The International Society of Dermatology
International Journal of Dermatology
Volume 53, Issue 3, pages 376–384, March 2014
How to Cite
Curry, J. L., Torres-Cabala, C. A., Kim, K. B., Tetzlaff, M. T., Duvic, M., Tsai, K. Y., Hong, D. S. and Prieto, V. G. (2014), Dermatologic toxicities to targeted cancer therapy: shared clinical and histologic adverse skin reactions. International Journal of Dermatology, 53: 376–384. doi: 10.1111/ijd.12205
- Issue online: 20 FEB 2014
- Version of Record online: 24 JUL 2013
Dermatologic toxicities (DT) to targeted cancer therapy may present as inflammatory dermatoses, keratoses, and as benign and malignant squamous proliferations.
Published reports of DT with cancer therapy with epidermal growth factor receptor (EGFR), tyrosine kinase (TK), MEK, PI3K, AKT, and BRAF inhibitors were reviewed.
DT associated with targeted cancer therapy demonstrated similar reactions and may be grouped as (i) DT as cutaneous inflammation, and (ii) DT as cutaneous epithelial proliferation. EGFR inhibitor, cetuximab, and MEK inhibitors, selumetinib and trametinib, demonstrated papulopustular rash with a suppurative folliculitis in 83%, 93%, and 80% of the patients on therapy, respectively. Common DT with EGFR inhibitors erlotinib and tyrosine kinase inhibitor sorafenib were hand–foot skin reactions in 30–60% of patients on therapy. PI3K inhibitor BKM-120 and AKT inhibitor MK2206 produced maculopapular eruptions seen as dermal hypersensitivity reaction on the skin biopsy. RAF inhibitors vemurafenib and sorafenib were associated with a variety of cutaneous epithelial proliferations (keratosis pilaris, seborrheic keratosis, verruca vulgaris, actinic keratosis, keratoacanthoma, and squamous cell carcinoma.
Various anticancer agents may target similar cellular compounds and/or cell signaling pathways thus share similar clinical and histologic features of DT. The knowledge of the overlap of DT with different types of targeted cancer therapy will assist in evaluation of cutaneous reactions.