厄洛替尼对肝脏表皮生长因子受体的抑制作用:剂量递减试点试验作为化学预防策略的第一步
Epidermal Growth Factor Receptor Inhibition With Erlotinib in Liver: Dose De-Escalation Pilot Trial as an Initial Step in a Chemoprevention Strategy.
作者信息
Tanabe Kenneth K, Zahrieh David, Strand Carrie A, Hoshida Yujin, Flotte Thomas J, Della'Zanna Gary, Umar Asad, Chavin Kenneth D, Cleary Sean, Kubota Naoto, Llovet Josep M, Patel Tushar, Siegel Christopher, Limburg Paul J
机构信息
Department of Surgery, Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts.
Division of Clinical Trial and Biostatistics, Mayo Clinic, Rochester, New York.
出版信息
Gastro Hep Adv. 2024 Jan 29;3(3):426-439. doi: 10.1016/j.gastha.2024.01.009. eCollection 2024.
BACKGROUND AND AIMS
Effective approaches for prevention of hepatocellular carcinoma (HCC) will have a significant impact on HCC-related mortality. There are strong preclinical data and rationale to support targeting epidermal growth factor receptor (EGFR) for HCC chemoprevention. Small molecule inhibitors of EGFR have been Food and Drug Administration-approved for cancer therapy, which provides an opportunity to repurpose one of these drugs for chemoprevention of HCC. Unfortunately, the frequency of side effects associated with administration of these drugs at oncology doses renders them ineffective for chemoprevention. This clinical trial assesses whether lower doses of one of these inhibitors, erlotinib, still engages EGFR in the liver to block signaling (eg, EGFR phosphorylation). The objective of this clinical trial was determination of a safe and minimum effective dose of erlorinib for which ≥ 50% reduction phospho-EGFR immunohistochemical staining in the liver was observed.
METHODS
Forty six participants were preregistered and 25 participants were registered in this multicenter trial. By dose de-escalation trial design, cohorts of participants received a 7-day course of erlotinib 75 mg/day, 50 mg/day or 25 mg/day with liver tissue acquisition prior to and after erlotinib.
RESULTS
A ≥50% reduction phospho-EGFR immunohistochemical staining in the liver was observed in a minimum of 40% of participants (predetermined threshhold) at each of the dose levels. Erlotinib was very well tolerated with few side effects observed, particularly at the dose of 25 mg/day. Favorable modulation of the Prognostic Liver Signature was observed in participants who received erlotinib.
CONCLUSION
These data support the selection of erlotinib doses as low as 25 mg/day of for a longer intervention to assess for evidence of efficacy as an HCC chemoprevention drug (ClinicalTrials.govNCT02273362).
背景与目的
预防肝细胞癌(HCC)的有效方法将对HCC相关死亡率产生重大影响。有强有力的临床前数据和理论依据支持将表皮生长因子受体(EGFR)作为HCC化学预防的靶点。EGFR的小分子抑制剂已获美国食品药品监督管理局批准用于癌症治疗,这为将其中一种药物重新用于HCC化学预防提供了机会。不幸的是,以肿瘤学剂量使用这些药物时出现副作用的频率使其在化学预防中无效。这项临床试验评估了这些抑制剂之一厄洛替尼的较低剂量是否仍能在肝脏中作用于EGFR以阻断信号传导(如EGFR磷酸化)。该临床试验的目的是确定厄洛替尼的安全最低有效剂量,在此剂量下观察到肝脏中磷酸化EGFR免疫组化染色减少≥50%。
方法
46名参与者进行了预注册,25名参与者登记参加了这项多中心试验。通过剂量递减试验设计,参与者队列接受为期7天的厄洛替尼治疗,剂量分别为75毫克/天、50毫克/天或25毫克/天,并在厄洛替尼治疗前后采集肝组织。
结果
在每个剂量水平上,至少40%的参与者(预定阈值)肝脏中磷酸化EGFR免疫组化染色减少≥50%。厄洛替尼耐受性良好,观察到的副作用很少,尤其是在25毫克/天的剂量下。在接受厄洛替尼治疗的参与者中观察到预后肝脏特征的有利调节。
结论
这些数据支持选择低至25毫克/天的厄洛替尼剂量进行更长时间的干预,以评估其作为HCC化学预防药物的疗效证据(ClinicalTrials.govNCT02273362)。
Zotero 插件