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热敏水凝胶作为 CTLA-4 检查点阻断抗体的持续药物递送系统。

Thermosensitive hydrogels as sustained drug delivery system for CTLA-4 checkpoint blocking antibodies.

机构信息

Department of Radiology, Division Translational Nanobiomaterials and Imaging, Leiden University Medical Center, Leiden, the Netherlands; Percuros B.V., Zernikedreef 8, 2333 CL Leiden, the Netherlands.

Department of Immunohematology and Bloodtransfusion, Leiden University Medical Center, Leiden, the Netherlands.

出版信息

J Control Release. 2020 Jul 10;323:1-11. doi: 10.1016/j.jconrel.2020.03.050. Epub 2020 Apr 2.

DOI:10.1016/j.jconrel.2020.03.050
PMID:32247805
Abstract

Thermosensitive poloxamer 407 (P407) hydrogels were evaluated as slow release system for optimizing CTLA-4 therapy. Slow release reduces systemic antibody levels and potentially mitigates the side effects of CTLA-4 therapy. The 25% P407 hydrogel is injectable at room temperature and depots are established quickly after subcutaneous injection. Scanning electron microscopy revealed the porous structure of the hydrogel, average pore surface was 1335 μm. Release studies were optimized using the human IgG antibody. IgG was easily incorporated in the hydrogel by simple mixing and no antibodies were lost during preparation. In vitro, hydrogels showed low burst release within the first 24 h. Total IgG load was gradually released within 120 h. In vitro cytotoxicity assays showed that P407 is not cytotoxic and induces no immune activation by itself. In vivo, P407 hydrogels significantly reduced serum IgG levels, were biocompatible and were broken down 1 week after injection. Finally, local hydrogel delivery of anti-CTLA-4 antibodies near established tumors effectively slowed down tumor growth, whilst significantly reduced serum anti-CTLA-4 levels. Altogether, P407 hydrogels represent promising delivery systems for the optimization of CTLA-4 blocking therapy.

摘要

温敏性泊洛沙姆 407(P407)水凝胶被评估为优化 CTLA-4 治疗的缓释系统。缓释可以降低系统抗体水平,并可能减轻 CTLA-4 治疗的副作用。25%的 P407 水凝胶在室温下可注射,在皮下注射后迅速形成储库。扫描电子显微镜显示水凝胶具有多孔结构,平均孔径表面为 1335μm。使用人 IgG 抗体优化了释放研究。通过简单混合,IgG 很容易掺入水凝胶中,在制备过程中不会损失任何抗体。体外研究表明,水凝胶在最初的 24 小时内呈现出较低的突释。总 IgG 负荷在 120 小时内逐渐释放。体外细胞毒性试验表明,P407 本身无细胞毒性,也不会引起免疫激活。在体内,P407 水凝胶可显著降低血清 IgG 水平,具有生物相容性,并在注射后 1 周内被分解。最后,在已建立的肿瘤附近局部水凝胶递送抗 CTLA-4 抗体,有效地减缓了肿瘤生长,同时显著降低了血清抗 CTLA-4 水平。总之,P407 水凝胶是优化 CTLA-4 阻断治疗的有前途的递药系统。

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