芬维 A 酯(NSC 374551)治疗复发性小细胞肺癌的Ⅱ期临床试验。
Phase II trial of fenretinide (NSC 374551) in patients with recurrent small cell lung cancer.
机构信息
Division of Hematology/Oncology, Department of Internal Medicine, Weill Cornell Medical College, 525 East 68th Street, J-321, New York, NY 10021, USA.
出版信息
Invest New Drugs. 2009 Dec;27(6):571-8. doi: 10.1007/s10637-009-9228-6. Epub 2009 Feb 19.
BACKGROUND
Alterations in retinoid signaling appear to be involved in the pathogenesis of small cell lung cancer (SCLC). Fenretinide [N-(4-hydroxyphenyl)retinamide], a synthetic retinoid, inhibits the growth of SCLC cells in vitro via the induction of apoptosis. Since these data suggested that SCLC is the adult solid tumor that is most susceptible to fenretinide, a trial to evaluate the clinical activity of fenretinide in patients with SCLC was considered the definitive test of its clinical potential in adult oncology.
METHODS
Patients with progressive SCLC after one or two prior chemotherapy regimens and a performance status of 0-2 were eligible for the study. Patients with stable, treated brain metastases were eligible. Fenretinide 900 mg/m(2) twice daily was administered orally on days 1-7 of each 21-day cycle. Blood and saliva were collected pre-treatment and on day 7 of cycle 1 to measure fenretinide and retinol levels by high-pressure liquid chromatography (HPLC).
RESULTS
Nineteen patients were enrolled. Fifteen patients had one prior chemotherapy regimen and four patients had two prior regimens. The median time from diagnosis to enrollment was 10 months. A median of two cycles of fenretinide was administered. There were no objective responses, but four of 17 evaluable patients (24%) had stable disease after 2-17 cycles. The median time to treatment failure was 5.7 weeks overall, while the four patients with stable disease demonstrated treatment failure at 11, 13, 19, and 52 weeks. Median survival was 25 weeks, with one patient alive 22 months after the start of treatment. The 1-year survival rate was 29%. Toxicity included mild, reversible visual changes (haziness, altered night vision), grade 1-3 nausea/vomiting, and grade 1-2 diarrhea. The mean day 7 plasma fenretinide level was 2.90 +/- 1.66 μg/ml (7.40 +/- 4.25 muM; n = 14). The mean pre-treatment and day 7 plasma retinol levels were 0.47 +/- 0.16 μg/ml and 0.05 +/- 0.07 μg/ml (n = 8), respectively. The mean day 7 salivary fenretinide level was 0.08 +/- 0.18 μg/ml, with no correlation between salivary and plasma drug levels.
CONCLUSIONS
Fenretinide is well tolerated in patients with SCLC and stabilization of disease was noted in 24% of patients with this aggressive disease. However, after the first stage of enrollment, the response rate did not meet criteria to proceed with full trial accrual. Plasma concentrations of fenretinide that induce cytotoxicity in vitro in SCLC cell lines are clinically achievable, but there were no objective responses. Non-invasive drug monitoring using saliva underestimates systemic exposure.
背景
视黄酸信号的改变似乎参与了小细胞肺癌(SCLC)的发病机制。芬维 A 胺[N-(4-羟基苯基)视黄酰胺],一种合成的视黄酸,通过诱导细胞凋亡抑制 SCLC 细胞在体外的生长。由于这些数据表明 SCLC 是最易受芬维 A 胺影响的成人实体肿瘤,因此评估芬维 A 胺在 SCLC 患者中的临床活性被认为是其在成人肿瘤学中临床潜力的决定性试验。
方法
在接受过一次或两次化疗方案且体能状态为 0-2 的进展性 SCLC 患者有资格参加这项研究。有稳定、治疗过的脑转移的患者也有资格参加。患者每天口服两次,每次 900mg/m2,每日剂量为 1800mg/m2,于第 1-7 天,每个 21 天周期进行治疗。在第 1 周期的第 7 天,收集治疗前和治疗前的血液和唾液样本,采用高效液相色谱法(HPLC)检测芬维 A 胺和视黄醇水平。
结果
共纳入 19 名患者。15 名患者接受了一次化疗方案,4 名患者接受了两次化疗方案。从诊断到入组的中位时间为 10 个月。中位芬维 A 胺治疗周期数为 2 个周期。没有客观缓解,但 17 名可评价患者中有 4 名(24%)在 2-17 个周期后疾病稳定。总的中位无进展生存期为 5.7 周,而 4 名疾病稳定的患者在 11、13、19 和 52 周时出现疾病进展。中位总生存期为 25 周,1 名患者在开始治疗后 22 个月时仍存活。1 年生存率为 29%。毒性包括轻微、可逆的视觉改变(模糊、夜间视力改变)、1-3 级恶心/呕吐和 1-2 级腹泻。第 7 天平均血浆芬维 A 胺水平为 2.90±1.66μg/ml(7.40±4.25μM;n=14)。第 7 天治疗前和血浆视黄醇水平分别为 0.47±0.16μg/ml 和 0.05±0.07μg/ml(n=8)。第 7 天唾液芬维 A 胺的平均水平为 0.08±0.18μg/ml,唾液和血浆药物水平之间无相关性。
结论
芬维 A 胺在 SCLC 患者中耐受性良好,在这种侵袭性疾病中,24%的患者疾病稳定。然而,在第一阶段入组后,缓解率未达到进行全面试验入组的标准。在 SCLC 细胞系中体外诱导细胞毒性的芬维 A 胺血浆浓度是可达到的,但没有客观缓解。使用唾液进行非侵入性药物监测低估了全身暴露。
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