Jatoi Aminah, Rowland Kendrith, Sloan Jeff A, Gross Howard M, Fishkin Paul A, Kahanic Stephen P, Novotny Paul J, Schaefer Paul L, Johnson David B, Tschetter Loren K, Loprinzi Charles L
Department of Oncology, Mayo Clinic and Mayo Foundation, Rochester, Minnesota 55905, USA.
Cancer. 2008 Aug 15;113(4):847-53. doi: 10.1002/cncr.23621.
Epidermal growth factor receptor (EGFR) inhibitors are effective cancer therapies, but they are reported to cause a rash in >50% of patients. In the current study, the authors examined the use of tetracycline for rash prevention.
This placebo-controlled, double-blinded trial enrolled patients who were starting cancer treatment with an EGFR inhibitor. Patients could not have had a rash at the time of enrollment. All patients were randomly assigned to receive either tetracycline at a dose of 500 mg orally twice a day for 28 days versus a placebo. Patients were monitored for rash (through monthly physician assessment and weekly patient-reported questionnaires), quality of life (using the SKINDEX-16, a skin-specific quality of life index), and adverse events. Monitoring occurred during the 4-week intervention and then for an additional 4 weeks. The primary objective of the current study was to compare the incidence of rash between the study arms, and the enrollment of 30 patients per arm provided a 90% probability of detecting a 40% difference in incidence with a P value of .05 (2-sided).
A total of 61 evaluable patients were enrolled. The 2 treatment arms were well balanced with regard to baseline characteristics, dropout rates, and rates of discontinuation of the EGFR inhibitor. The incidence of rash was found to be comparable across treatment arms. Physicians reported that 16 patients treated with tetracycline (70%) and 22 patients treated with placebo (76%) developed a rash (P = .61). Tetracycline appears to have lessened the rash severity, although the high dropout rates invite caution when interpreting these findings. By Week 4, physician-reported grade 2 rash (using the National Cancer Institute's Common Terminology Criteria for Adverse Events [version 3.0]) occurred in 17% of tetracycline-treated patients (n = 4 patients) and in 55% of placebo-exposed patients (n = 16 patients) (P = .04). Patients treated with tetracycline reported better scores, as per the SKINDEX-16, on certain quality-of-life parameters such as skin burning or stinging, skin irritation, and being bothered by the persistence/recurrence of a skin condition. Adverse events were found to be comparable across treatment arms.
In the current study, tetracycline was not found to prevent EGFR inhibitor-induced rashes and therefore cannot be clinically recommended for this purpose. However, preliminary observations of diminished rash severity and improved quality of life suggest this antibiotic merits further study.
表皮生长因子受体(EGFR)抑制剂是有效的癌症治疗药物,但据报道,超过50%的患者会出现皮疹。在本研究中,作者研究了四环素在预防皮疹方面的应用。
这项安慰剂对照、双盲试验纳入了开始使用EGFR抑制剂进行癌症治疗的患者。入组时患者不能有皮疹。所有患者被随机分配接受以下两种治疗之一:每日口服两次500mg四环素,共28天,或接受安慰剂。对患者进行皮疹监测(通过每月的医生评估和每周患者报告的问卷)、生活质量评估(使用SKINDEX-16,一种皮肤特异性生活质量指数)以及不良事件监测。监测在4周的干预期间进行,然后再持续4周。本研究的主要目的是比较研究组之间皮疹的发生率,每组纳入30名患者可提供90%的概率检测到发生率有40%的差异,P值为0.05(双侧)。
共纳入61例可评估患者。两个治疗组在基线特征、脱落率和EGFR抑制剂停药率方面平衡良好。发现各治疗组皮疹发生率相当。医生报告,接受四环素治疗的16例患者(70%)和接受安慰剂治疗的22例患者(76%)出现了皮疹(P = 0.61)。四环素似乎减轻了皮疹的严重程度,不过在解释这些结果时,高脱落率需谨慎考虑。到第4周时,医生报告的2级皮疹(使用美国国立癌症研究所的不良事件通用术语标准[第3.0版])在接受四环素治疗的患者中发生率为17%(n = 4例患者),在接受安慰剂治疗的患者中发生率为55%(n = 16例患者)(P = 0.04)。根据SKINDEX-16,接受四环素治疗的患者在某些生活质量参数上得分更高,如皮肤灼痛或刺痛、皮肤刺激以及因皮肤状况持续/复发而感到困扰。发现各治疗组不良事件相当。
在本研究中,未发现四环素可预防EGFR抑制剂引起的皮疹,因此临床上不推荐为此目的使用。然而,关于皮疹严重程度减轻和生活质量改善的初步观察表明,这种抗生素值得进一步研究。