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用肽酶增强的细胞毒性美法仑氟芬酰胺靶向侵袭性骨肉瘤。

Targeting aggressive osteosarcoma with a peptidase-enhanced cytotoxic melphalan flufenamide.

作者信息

Byrgazov Konstantin, Anderson Claes, Salzer Benjamin, Bozsaky Eva, Larsson Rolf, Gullbo Joachim, Lehner Manfred, Lehmann Fredrik, Slipicevic Ana, Kager Leo, Fryknäs Mårten, Taschner-Mandl Sabine

机构信息

Oncopeptides AB, Luntmakragatan 46, Stockholm, SE-111 37, Sweden.

Department of Medical Sciences, Division of Cancer Pharmacology and Computational Medicine, Uppsala University, Uppsala, Sweden.

出版信息

Ther Adv Med Oncol. 2020 Jul 29;12:1758835920937891. doi: 10.1177/1758835920937891. eCollection 2020.

Abstract

BACKGROUND

Low survival rates in metastatic high-grade osteosarcoma (HGOS) have remained stagnant for the last three decades. This study aims to investigate the role of aminopeptidase N (ANPEP) in HGOS progression and its targeting with a novel lipophilic peptidase-enhanced cytotoxic compound melphalan flufenamide (melflufen) in HGOS.

METHODS

Meta-analysis of publicly available gene expression datasets was performed to determine the impact of gene expression on metastasis-free survival of HGOS patients. The efficacy of standard-of-care anti-neoplastic drugs and a lipophilic peptidase-enhanced cytotoxic conjugate melflufen was investigated in patient-derived HGOS models and cell lines. The kinetics of apoptosis and necrosis induced by melflufen and doxorubicin were compared. Anti-neoplastic effects of melflufen were investigated .

RESULTS

Elevated expression in diagnostic biopsies of HGOS patients was found to significantly reduce metastasis-free survival. In drug sensitivity assays, melflufen has shown an anti-proliferative effect in HGOS samples and cell lines, including those resistant to methotrexate, etoposide, doxorubicin, and PARP inhibitors. Further, HGOS cells treated with melflufen displayed a rapid induction of apoptosis and this sensitivity correlated with high expression of . In combination treatments, melflufen demonstrated synergy with doxorubicin in killing HGOS cells. Finally, Melflufen displayed anti-tumor growth and anti-metastatic effects .

CONCLUSION

This study may pave the way for use of melflufen as an adjuvant to doxorubicin in improving the therapeutic efficacy for the treatment of metastatic HGOS.

摘要

背景

在过去三十年中,转移性高级别骨肉瘤(HGOS)的低生存率一直停滞不前。本研究旨在探讨氨肽酶N(ANPEP)在HGOS进展中的作用,以及一种新型亲脂性肽酶增强型细胞毒性化合物美法仑氟芬酰胺(melflufen)在HGOS中的靶向作用。

方法

对公开可用的基因表达数据集进行荟萃分析,以确定基因表达对HGOS患者无转移生存期的影响。在患者来源的HGOS模型和细胞系中研究了标准护理抗肿瘤药物和亲脂性肽酶增强型细胞毒性偶联物melflufen的疗效。比较了melflufen和阿霉素诱导的凋亡和坏死动力学。研究了melflufen的抗肿瘤作用。

结果

发现HGOS患者诊断活检中的高表达显著降低无转移生存期。在药物敏感性试验中,melflufen在HGOS样本和细胞系中显示出抗增殖作用,包括对甲氨蝶呤、依托泊苷、阿霉素和PARP抑制剂耐药的样本和细胞系。此外,用melflufen处理的HGOS细胞显示出快速的凋亡诱导,这种敏感性与……的高表达相关。在联合治疗中,melflufen与阿霉素在杀死HGOS细胞方面表现出协同作用。最后,melflufen显示出抗肿瘤生长和抗转移作用。

结论

本研究可能为使用melflufen作为阿霉素的佐剂以提高转移性HGOS的治疗疗效铺平道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b231/7391428/04fe67467aae/10.1177_1758835920937891-fig1.jpg

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