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In Situ Modulation of Dendritic Cells by Injectable Thermosensitive Hydrogels for Cancer Vaccines in Mice

机译:注射热敏性水凝胶对小鼠癌症疫苗的树突状细胞的原位调节

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Attempts to develop cell-based cancer vaccines have shown limited efficacy, partly because transplanted dendritic cells (DCs) do not survive long enough to reach the lymph nodes. The development of biomaterials capable of modulating DCs in situ to enhance antigen uptake and presentation has emerged as a novel method toward developing more efficient cancer vaccines. Here, we propose a two-step hybrid strategy to produce a more robust cell-based cancer vaccine in situ. First, a significant number of DCs are recruited to an injectable thermosensitive mPEG-PLGA hydrogel through sustained release of chemoattractants, in particular, granulocyte-macrophage colony-stimulating factor (GM- CSF). Then, these resident DCs can be loaded with cancer antigens through the use of viral or nonviral vectors. We demonstrate that GM-CSF-releasing mPEG-PLGA hydrogels successfully recruit and house DCs and macrophages, allowing the subsequent introduction of antigens by vectors to activate the resident cells, thus, initiating antigen presentation and triggering immune response. Moreover, this two-step hybrid strategy generates a high level of tumor-specific immunity, as demonstrated in both prophylactic and therapeutic models of murine melanoma. This injectable thermosensitive hydrogel shows great promise as an adjuvant for cancer vaccines, potentially providing a new approach for cell therapies through in situ modulation of cells.
机译:尝试开发基于细胞的癌症疫苗的效果有限,部分原因是移植的树突状细胞(DC)存活时间不足以到达淋巴结。能够原位调节DC以增强抗原摄取和呈递的生物材料的开发已经作为开发更有效的癌症疫苗的新方法而出现。在这里,我们提出了两步混合策略,以在现场生产出更强大的基于细胞的癌症疫苗。首先,通过持续释放趋化剂,特别是粒细胞-巨噬细胞集落刺激因子(GM-CSF),将大量DC募集到可注射的热敏性mPEG-PLGA水凝胶中。然后,可以通过使用病毒或非病毒载体将这些常驻DC载有癌症抗原。我们证明,释放GM-CSF的mPEG-PLGA水凝胶成功募集并容纳了DC和巨噬细胞,从而允许随后通过载体引入抗原以激活驻留细胞,从而启动抗原呈递并触发免疫反应。而且,如鼠类黑色素瘤的预防和治疗模型所证明的,这种两步混合策略可产生高水平的肿瘤特异性免疫。这种可注射的热敏性水凝胶有望作为癌症疫苗的佐剂,有望通过原位调节细胞为细胞疗法提供一种新方法。

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