肝细胞癌和实体瘤肝转移的福斯特沙星-布拉帕胺（Fostrox）单药 1a/1b 期研究。

IF 4.2 3区医学 Q2 ONCOLOGY

Journal of Hepatocellular Carcinoma Pub Date : 2024-10-24 eCollection Date: 2024-01-01 DOI:10.2147/JHC.S481410

Ruth Plummer, Alastair Greystoke, Gregory Naylor, Debashis Sarker, A N M Kaiser Anam, Hans Prenen, Laure-Anne Teuwen, Eric Van Cutsem, Jeroen Dekervel, Beate Haugk, Thomas Ness, Sujata Bhoi, Malene Jensen, Tom Morris, Pia Baumann, Niclas Sjögren, Karin Tunblad, Hans Wallberg, Fredrik Öberg, Thomas R Jeffry Evans

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引用次数: 0

摘要

目的：评估福斯特罗沙他滨-布拉帕胺（fostrox，MIV-818）的安全性、初步疗效、药代动力学和药效动力学：在一项开放标签、单臂、首次人体1a/1b期研究中，对肝细胞癌（HCC）、肝内胆管癌或实体瘤肝转移患者进行了Fostrox单药治疗。第一阶段（1a）包括患者体内/患者间剂量递增（3毫克至70毫克），每日1次，最多5天；第二阶段（1b）包括剂量递增（40毫克至70毫克），每日1次，最多5天，21天为一个周期。安全性和耐受性由安全审查委员会评估，疗效每6周通过CT或MRI（采用RECIST 1.1和mRECIST）进行评估：19名患者接受了福斯特罗克斯治疗。最常见的不良反应（AEs）是血液学反应和谷草转氨酶升高。53%的患者出现了3级治疗相关不良反应（TRAE），其中最常见的是一过性中性粒细胞减少症和血小板减少症。未观察到 5 级 AE。福斯特罗克斯的2期推荐剂量为40毫克，每天5天，21天为一个周期。初步疗效显示，肝脏的临床获益率为53%，10名患者的最佳反应为病情稳定（SD）。与血浆相比，特罗沙西他滨及其代谢物在肝脏中的暴露量更高，这证实了福斯特罗克斯对肝脏的靶向作用。以托沙他滨为主要分析物的福斯特罗克斯全身暴露量普遍较低。活组织检查显示，药物诱导的DNA损伤具有肿瘤选择性：结论：对肝脏肿瘤患者进行的福斯特罗克斯1a/1b期单药治疗研究显示，福斯特罗克斯在肝脏中具有肿瘤选择性作用，而且40毫克QD、5天、21天为一个周期是安全和可耐受的。在晚期 HCC 患者中的安全性和初步疗效支持了 fostrox 与其他作用方式联合治疗 HCC 的临床开发。

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A Phase 1a/1b Study of Fostroxacitabine Bralpamide (Fostrox) Monotherapy in Hepatocellular Carcinoma and Solid Tumor Liver Metastases.

Purpose: To evaluate safety, preliminary efficacy, pharmacokinetics, and pharmacodynamics, of fostroxacitabine bralpamide (fostrox, MIV-818), a novel oral troxacitabine nucleotide prodrug designed to direct exposure to the liver, while minimizing systemic toxicity.

Patients and methods: Fostrox monotherapy was administered in an open-label, single-arm, first-in-human, phase 1a/1b study, in patients with hepatocellular carcinoma (HCC), intrahepatic cholangiocarcinoma, or solid tumor liver metastases. The first part (1a) consisted of intra/inter-patient escalating doses (3 mg to 70 mg) QD for up to 5 days, and the second part (1b), doses of 40 mg QD for 5 days, in 21-day cycles. Safety and tolerability were evaluated by the Safety Review Committee, and efficacy was assessed every 6 weeks with CT or MRI using RECIST 1.1 and mRECIST.

Results: Nineteen patients were treated with fostrox. Most common adverse events (AEs) were hematological and increased AST. Grade 3 treatment related AEs (TRAE) were seen in 53% of the patients, with transient neutropenia and thrombocytopenia as the most common. No grade 5 AE was observed. Recommended Phase 2 dose of fostrox was 40 mg QD for 5 days in 21-day cycles. Preliminary efficacy showed a clinical benefit rate in the liver of 53% and stable disease (SD) as best response in 10 patients. Liver targeting with fostrox was confirmed with higher exposure of troxacitabine and its metabolites in liver compared to plasma. Systemic exposure of fostrox was generally low with troxacitabine as main analyte. Biopsies demonstrated tumor-selective, drug-induced DNA damage.

Conclusion: The phase 1a/1b monotherapy study of fostrox, in patients with liver tumors, showed a tumor selective effect in the liver and that 40 mg QD for 5 days in 21-day cycles is safe and tolerable. Safety and preliminary efficacy in patients with advanced HCC supports clinical development of fostrox in combination with other modes of action in HCC.

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来源期刊

Journal of Hepatocellular Carcinoma ONCOLOGY-

CiteScore

0.50

自引率

2.40%

发文量

108

审稿时长

16 weeks