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一项评估晚期癌症患者中 eIF-4E 反义寡核苷酸 LY2275796 的剂量递增、药代动力学和药效学的 I 期研究。

A phase 1 dose escalation, pharmacokinetic, and pharmacodynamic evaluation of eIF-4E antisense oligonucleotide LY2275796 in patients with advanced cancer.

机构信息

Clinical Center for Targeted Therapy, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA.

出版信息

Clin Cancer Res. 2011 Oct 15;17(20):6582-91. doi: 10.1158/1078-0432.CCR-11-0430. Epub 2011 Aug 10.

DOI:10.1158/1078-0432.CCR-11-0430
PMID:21831956
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5036398/
Abstract

PURPOSE

The antisense oligonucleotide LY2275796 blocks expression of cap-binding protein eukaryotic initiation factor 4E (eIF-4E), an mRNA translation regulator upregulated in tumors. This phase I study sought an appropriate LY2275796 dose in patients with advanced tumors.

EXPERIMENTAL DESIGN

A 3-day loading dose, then weekly maintenance doses, were given to 1 to 3 patient cohorts, beginning with 100 mg and escalating. Plasma samples were collected to determine LY2275796 concentrations and tumor biopsies to quantify eIF-4E mRNA/protein.

RESULTS

Thirty patients with stage 4 disease received 1 or more LY2275796 dose. A dose-limiting toxicity was observed at 1,200 mg, with 1,000 mg the maximum-tolerated dose. Across all dose levels, most patients (87%) had only grade 1 to 2 toxicities. LY2275796 pharmacokinetics supported the dosing regimen. Comparison of pre- and postdose biopsies showed eIF-4E decreased in most patients. Fifteen patients had progressive disease, and 7 patients achieved stable disease (minimum of 6 weeks) as best response, with 2 patients on therapy for more than 3 months (one with melanoma, one with cystadenocarcinoma of the head/neck).

CONCLUSIONS

LY2275796 was well tolerated up to 1,000 mg. Because tumor eIF-4E expression was decreased, but no tumor response observed, LY2275796 should be studied combined with other treatment modalities.

摘要

目的

反义寡核苷酸 LY2275796 阻断帽结合蛋白真核起始因子 4E(eIF-4E)的表达,eIF-4E 是肿瘤中上调的 mRNA 翻译调节剂。这项 I 期研究旨在确定晚期肿瘤患者中 LY2275796 的合适剂量。

实验设计

1 至 3 个患者队列接受为期 3 天的负荷剂量,然后每周维持剂量,起始剂量为 100mg,并逐步递增。采集血浆样本以确定 LY2275796 浓度,并对肿瘤活检以定量测定 eIF-4E mRNA/蛋白。

结果

30 名患有 4 期疾病的患者接受了 1 次或多次 LY2275796 剂量。在 1200mg 时观察到剂量限制毒性,最大耐受剂量为 1000mg。在所有剂量水平下,大多数患者(87%)仅出现 1 至 2 级毒性。LY2275796 的药代动力学支持该给药方案。比较治疗前后的活检显示,大多数患者的 eIF-4E 水平降低。15 名患者出现疾病进展,7 名患者达到最佳反应的稳定疾病(最少 6 周),其中 2 名患者的治疗时间超过 3 个月(1 名患有黑色素瘤,1 名患有头颈部囊腺癌)。

结论

LY2275796 的耐受性良好,最高剂量可达 1000mg。由于肿瘤 eIF-4E 表达减少,但未观察到肿瘤反应,因此 LY2275796 应与其他治疗方式联合研究。

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