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L-MTP-PE与唑来膦酸联合治疗骨肉瘤:临床转化积极治疗组合的临床前证据

L-MTP-PE and zoledronic acid combination in osteosarcoma: preclinical evidence of positive therapeutic combination for clinical transfer.

作者信息

Biteau Kevin, Guiho Romain, Chatelais Mathias, Taurelle Julien, Chesneau Julie, Corradini Nadège, Heymann Dominique, Redini Françoise

机构信息

INSERM, UMR-957, Equipe Ligue Contre le Cancer 2012Nantes, F-44035, France; Université de Nantes, Faculté de Médecine, Laboratoire De Physiopathologie De La Résorption Osseuse Et Thérapie Des Tumeurs Osseuses PrimitivesNantes, F-44035, France.

INSERM, UMR-957, Equipe Ligue Contre le Cancer 2012Nantes, F-44035, France; Université de Nantes, Faculté de Médecine, Laboratoire De Physiopathologie De La Résorption Osseuse Et Thérapie Des Tumeurs Osseuses PrimitivesNantes, F-44035, France; Pediatric Oncology Unit, Hôpital Mère-EnfantNantes, F-44035, France.

出版信息

Am J Cancer Res. 2016 Feb 15;6(3):677-89. eCollection 2016.

Abstract

Osteosarcoma, the most frequent malignant primary bone tumor in pediatric patients is characterized by osteolysis promoting tumor growth. Lung metastasis is the major bad prognosis factor of this disease. Zoledronic Acid (ZA), a potent inhibitor of bone resorption is currently evaluated in phase III randomized studies in Europe for the treatment of osteosarcoma and Ewing sarcoma. The beneficial effect of the liposomal form of Muramyl-TriPeptide-Phosphatidyl Ethanolamine (L-mifamurtide, MEPACT®), an activator of macrophage populations has been demonstrated to eradicate lung metastatic foci in osteosarcoma. The objective of this study was to evaluate the potential therapeutic benefit and the safety of the ZA and L-mifamurtide combination in preclinical models of osteosarcoma, as a prerequisite before translation to patients. The effects of ZA (100 μg/kg) and L-mifamurtide (1 mg/kg) were investigated in vivo in xenogeneic and syngeneic mice models of osteosarcoma, at clinical (tumor proliferation, spontaneous lung metastases development), radiological (bone microarchitecture by microCT analysis), biological and histological levels. No interference between the two drugs could be observed on ZA-induced bone protection and on L-mifamurtide-induced inhibition of lung metastasis development. Unexpectedly, ZA and L-mifamurtide association induced an additional and in some cases synergistic inhibition of primary tumor progression. L-mifamurtide has no effect on tumor proliferation in vitro or in vivo, and macrophage population was not affected at the tumor site whatever the treatment. This study evidenced for the first time a significant inhibition of primary osteosarcoma progression when both drugs are combined. This result constitutes a first proof-of-principle for clinical application in osteosarcoma patients.

摘要

骨肉瘤是儿科患者中最常见的原发性恶性骨肿瘤,其特征是促进肿瘤生长的骨溶解。肺转移是该疾病的主要不良预后因素。唑来膦酸(ZA)是一种有效的骨吸收抑制剂,目前正在欧洲进行III期随机研究,用于治疗骨肉瘤和尤文肉瘤。脂质体形式的胞壁酰三肽磷脂酰乙醇胺(L-米伐木肽,MEPACT®)作为巨噬细胞群体的激活剂,其有益作用已被证明可消除骨肉瘤中的肺转移灶。本研究的目的是在骨肉瘤临床前模型中评估ZA和L-米伐木肽联合应用的潜在治疗益处和安全性,作为转化至患者前的前提条件。在骨肉瘤的异种和同基因小鼠模型中,在临床(肿瘤增殖、自发性肺转移发展)、放射学(通过microCT分析骨微结构)、生物学和组织学水平上研究了ZA(100μg/kg)和L-米伐木肽(1mg/kg)的体内作用。在ZA诱导的骨保护和L-米伐木肽诱导的肺转移发展抑制方面,未观察到两种药物之间的相互干扰。出乎意料的是,ZA和L-米伐木肽联合使用可额外且在某些情况下协同抑制原发性肿瘤进展。L-米伐木肽在体外或体内对肿瘤增殖均无影响,无论采用何种治疗,肿瘤部位的巨噬细胞群体均未受到影响。本研究首次证明,两种药物联合使用时可显著抑制原发性骨肉瘤进展。这一结果构成了在骨肉瘤患者中临床应用的首个原理验证。

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