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原位化疗不完全共聚物降解。

Incomplete copolymer degradation of in situ chemotherapy.

机构信息

Department of Neurosurgery, Hospices Civils de Lyon, Hospital for Neurology and Neurosurgery Pierre Wertheimer, Lyon, France.

Brain and Spine Institute, INSERM U1127, CNRS 7225, Paris, France.

出版信息

J Mater Sci Mater Med. 2018 Feb 17;29(3):25. doi: 10.1007/s10856-018-6032-x.

Abstract

In situ carmustine wafers containing 1,3-bis(2-chloroethyl)-1-nitrosourea (BCNU) are commonly used for the treatment of recurrent glioblastoma to overcome the brain-blood barrier. In theory, this chemotherapy diffuses into the adjacent parenchyma and the excipient degrades in maximum 8 weeks but no clinical data confirms this evolution, because patients are rarely operated again. A 75-year-old patient was operated twice for recurrent glioblastoma, and a carmustine wafer was implanted during the second surgery. Eleven months later, a third surgery was performed, revealing unexpected incomplete degradation of the wafer. 1H-Nuclear Magnetic Resonance was performed to compare this wafer to pure BCNU and to an unused copolymer wafer. In the used wafer, peaks corresponding to hydrophobic units of the excipient were no longer noticeable, whereas peaks of the hydrophilic units and traces of BCNU were still present. These surprising results could be related to the formation of a hydrophobic membrane around the wafer, thus interfering with the expected diffusion and degradation processes. The clinical benefit of carmustine wafers in addition to the standard radio-chemotherapy remains limited, and in vivo behavior of this treatment is not completely elucidated yet. We found that the wafer may remain after several months. Alternative strategies to deal with the blood-brain barrier, such as drug-loaded liposomes or ultrasound-opening, must be explored to offer larger drug diffusion or allow repetitive delivery.

摘要

卡莫司汀植入剂含有 1,3-双(2-氯乙基)-1-亚硝基脲(BCNU),常用于治疗复发性胶质母细胞瘤以克服血脑屏障。理论上,这种化疗药物会扩散到相邻的实质组织中,赋形剂在 8 周内最大程度降解,但没有临床数据证实这种演变,因为患者很少再次接受手术。一名 75 岁的患者因复发性胶质母细胞瘤接受了两次手术,第二次手术中植入了卡莫司汀植入剂。11 个月后,进行了第三次手术,结果显示出乎意料的是,植入剂并未完全降解。对该植入剂进行 1H 核磁共振分析,与纯 BCNU 和未使用的共聚物植入剂进行比较。在使用过的植入剂中,赋形剂的疏水单元的峰不再明显,而亲水单元的峰和 BCNU 的痕迹仍然存在。这些令人惊讶的结果可能与植入剂周围形成的疏水膜有关,从而干扰了预期的扩散和降解过程。除了标准的放化疗之外,卡莫司汀植入剂的临床获益仍然有限,并且这种治疗方法的体内行为尚未完全阐明。我们发现,植入剂可能会在几个月后仍然存在。必须探索其他策略来解决血脑屏障问题,如载药脂质体或超声开放,以提供更大的药物扩散或允许重复给药。

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