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Bio-polymeric transferrin-targeted temozolomide nanoparticles in gel for synergistic post-surgical GBM therapy

机译:凝胶中的生物聚合物转铁蛋白靶向替莫唑胺纳米颗粒用于协同术后 GBM 治疗

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摘要

Spatiotemporal targeting of anti-glioma drugs remains a pressing issue in glioblastoma (GBM) treatment. We challenge this issue by developing a minimally invasive in situ implantable hydrogel implant comprising transferrin-targeted temozolomide–miltefosine nanovesicles in the surgically resected GBM cavity (tumour bed). Injection of the “nanovesicle in hydrogel system” in orthotopic GBM-bearing mice improved drug penetration into the peri-cavitary region (∼4.5 mm in depth) with the potential to act as a bridge therapy in the immediate postoperative period, before the initiation of adjuvant radiotherapy. The controlled and sustained release of temozolomide over a month in the surgical cavity eradicated the microscopic GBM cells present within the tumour bed, thereby augmenting the efficacy of adjuvant therapy. The drug (temozolomide and miltefosine) combination was tolerable and efficiently inhibited tumour growth, causing significant prolongation of the survival of tumour-bearing mice compared to that with the free drug. Direct implantation at the target site in the brain resulted in spatiotemporal anti-glioma activity with minimal extracranial and systemic distribution. Nanovesicle in flexible hydrogel systems can be used as potential platforms for the post-surgical management of GBM before initiating adjuvant radiation therapy.
机译:时空定位anti-glioma药物在胶质母细胞瘤(GBM)仍是一个紧迫的问题治疗。一种微创原位植入水凝胶植入物包括transferrin-targetedtemozolomide-miltefosine nanovesicles在肿瘤手术切除GBM腔(床)。在水凝胶注入“nanovesicle系统”在原位GBM-bearing改善药物的小鼠渗透到peri-cavitary地区(4.5∼毫米深度)和潜在的作为桥治疗术后立即期间,辅助启动之前放射治疗。释放temozolomide超过一个月外科腔根除微观“绿带运动”肿瘤细胞呈现在床上,从而增加辅助治疗的功效。(的药物和miltefosine)的组合是有效地抑制肿瘤所接受增长,导致重要的延伸生存tumour-bearing小鼠相比免费药物。目标站点在大脑中导致时空anti-glioma活动以最少的颅外和系统分布。Nanovesicle水凝胶系统可以灵活用作术后潜在的平台GBM之前启动辅助管理放射治疗。

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