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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Prevention of pulmonary metastasis from subcutaneous tumors by binary system-based sustained delivery of catalase
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Prevention of pulmonary metastasis from subcutaneous tumors by binary system-based sustained delivery of catalase

机译:通过基于二元系统的过氧化氢酶持续递送预防皮下肿瘤引起的肺转移

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摘要

Catalase delivery can be effective in inhibiting reactive oxygen species (ROS)-mediated acceleration of tumor metastasis. Our previous studies have demonstrated that increasing the plasma half-life of catalase by pegylation (PEG-catalase) significantly increases its potency of inhibiting experimental pulmonary metastasis in mice. In the present study, a biodegradable gelatin hydrogel formulation was used to further increase the circulation time of PEG-catalase. Implantation of In-111-PEG-catalase/hydrogel into subcutaneous tissues maintained the radioactivity in plasma for more than 14 days. Then, the effect of the PEG-catalase/hydrogel on spontaneous pulmonary metastasis of tumor cells was evaluated in mice with subcutaneous tumor of B16-111.6/Luc cells, a murine melanoma cell line stably expressing luciferase. Measuring luciferase activity in the lung revealed that the PEG-catalase/hydrogel significantly (P<0.05) inhibited the pulmonary metastasis compared with PEG-catalase solution. These findings indicate that sustaining catalase activity in the blood circulation achieved by the use of pegylation and gelatin hydrogel can reduce the incidence of tumor cell metastasis.
机译:过氧化氢酶递送可有效抑制活性氧(ROS)介导的肿瘤转移加速。我们以前的研究表明,通过聚乙二醇化(PEG-过氧化氢酶)增加过氧化氢酶的血浆半衰期可显着提高其抑制小鼠实验性肺转移的能力。在本研究中,可生物降解的明胶水凝胶制剂用于进一步增加PEG-过氧化氢酶的循环时间。将In-111-PEG-过氧化氢酶/水凝胶植入皮下组织可使血浆中的放射性保持14天以上。然后,在具有稳定表达荧光素酶的鼠黑素瘤细胞系B16-111.6 / Luc细胞的皮下肿瘤小鼠中评估了PEG-过氧化氢酶/水凝胶对肿瘤细胞自发性肺转移的作用。测量肺中的荧光素酶活性表明,与PEG-过氧化氢酶溶液相比,PEG-过氧化氢酶/水凝胶显着(P <0.05)抑制了肺转移。这些发现表明,通过使用聚乙二醇化和明胶水凝胶实现的血液循环中过氧化氢酶活性的维持可以减少肿瘤细胞转移的发生。

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