Holcmann Martin, Sibilia Maria
Institute of Cancer Research; Department of Medicine I; Medical University of Vienna; Comprehensive Cancer Center ; Vienna, Austria.
Mol Cell Oncol. 2015 Jun 1;2(4):e1004969. doi: 10.1080/23723556.2015.1004969. eCollection 2015 Oct-Dec.
The epidermal growth factor receptor (EGFR) is a receptor tyrosine kinase that is frequently mutated or overexpressed in a large number of tumors such as carcinomas or glioblastoma. Inhibitors of EGFR activation have been successfully established for the therapy of some cancers and are more and more frequently being used as first or later line therapies. Although the side effects induced by inhibitors of EGFR are less severe than those observed with classic cytotoxic chemotherapy and can usually be handled by out-patient care, they may still be a cause for dose reduction or discontinuation of treatment that can reduce the effectiveness of antitumor therapy. The mechanisms underlying these cutaneous side effects are only partly understood. Important questions, such as the reasons for the correlation between the intensity of the side effects and the efficiency of treatment with EGFR inhibitors, remain to be answered. Optimized adjuvant strategies to accompany anti-EGFR therapy need to be found for optimal therapeutic application and improved quality of life of patients. Here, we summarize current literature on the molecular and cellular mechanisms underlying the cutaneous side effects induced by EGFR inhibitors and provide evidence that keratinocytes are probably the optimal targets for adjuvant therapy aimed at alleviating skin toxicities.
表皮生长因子受体(EGFR)是一种受体酪氨酸激酶,在大量肿瘤(如癌或胶质母细胞瘤)中经常发生突变或过度表达。EGFR激活抑制剂已成功用于某些癌症的治疗,并且越来越频繁地被用作一线或二线治疗。尽管EGFR抑制剂引起的副作用不如经典细胞毒性化疗严重,通常可通过门诊护理处理,但它们仍可能导致剂量减少或治疗中断,从而降低抗肿瘤治疗的效果。这些皮肤副作用的潜在机制仅得到部分理解。一些重要问题,如副作用强度与EGFR抑制剂治疗效果之间相关性的原因,仍有待解答。需要找到优化的辅助策略来配合抗EGFR治疗,以实现最佳治疗应用并改善患者生活质量。在此,我们总结了关于EGFR抑制剂引起的皮肤副作用的分子和细胞机制的现有文献,并提供证据表明角质形成细胞可能是旨在减轻皮肤毒性的辅助治疗的最佳靶点。
