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用改性过氧化锌纳米粒子诱导耐受原性树突状细胞来调节类风湿关节炎的免疫策略。

Immune-regulating strategy against rheumatoid arthritis by inducing tolerogenic dendritic cells with modified zinc peroxide nanoparticles.

机构信息

Department of Orthopaedic Surgery, Shanghai Ninth People's Hospital, Shanghai Jiao Tong University School of Medicine, 639 Zhizaoju Road, Shanghai, 200011, People's Republic of China.

Shanghai Key Laboratory of Orthopaedic Implants, Shanghai Ninth People's Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai, People's Republic of China.

出版信息

J Nanobiotechnology. 2022 Jul 14;20(1):323. doi: 10.1186/s12951-022-01536-0.

Abstract

In hypoxic dendritic cells (DCs), a low level of Zn can induce the activation of immunogenic DCs (igDCs), thereby triggering an active T-cell response to propel the immune progression of rheumatoid arthritis (RA). This finding indicates the crucial roles of zinc and oxygen homeostasis in DCs during the pathogenesis of RA. However, very few studies have focused on the modulation of zinc and oxygen homeostasis in DCs during RA treatment. Proposed herein is a DC-targeting immune-regulating strategy to induce igDCs into tolerogenic DCs (tDCs) and inhibit subsequent T-cell activation, referred to as ZnO/Catalase@liposome-Mannose nanoparticles (ZnCM NPs). ZnCM NPs displayed targeted intracellular delivery of Zn and O towards igDCs in a pH-responsive manner. After inactivating OTUB1 deubiquitination, the ZnCM NPs promoted CCL5 degradation via NF-κB signalling, thereby inducing the igDC-tDC transition to further inhibit CD4 T-cell homeostasis. In collagen-induced arthritis (CIA) mice, this nanoimmunoplatform showed significant accumulation in the spleen, where immature DCs (imDCs) differentiated into igDCs. Splenic tDCs were induced to alleviate ankle swelling, improve walking posture and safely inhibit ankle/spleen inflammation. Our work pioneers the combination of DC-targeting nanoplatforms with RA treatments and highlights the significance of zinc and oxygen homeostasis for the immunoregulation of RA by inducing tDCs with modified ZnO NPs, which provides novel insight into ion homeostasis regulation for the treatment of immune diseases with a larger variety of distinct metal or nonmetal ions.

摘要

在低氧状态下的树突状细胞(DCs)中,低水平的锌可以诱导免疫原性 DCs(igDCs)的激活,从而引发主动的 T 细胞反应,推动类风湿关节炎(RA)的免疫进展。这一发现表明锌和氧平衡在 RA 发病机制中对 DCs 的重要作用。然而,很少有研究关注 RA 治疗过程中 DC 中锌和氧平衡的调节。本文提出了一种针对 DC 的免疫调节策略,通过将 igDC 诱导为耐受性 DC(tDC)并抑制随后的 T 细胞激活,即 ZnO/Catalase@liposome-Mannose 纳米颗粒(ZnCM NPs)。ZnCM NPs 以 pH 响应的方式靶向向 igDC 细胞内递呈锌和氧。在抑制 OTUB1 去泛素化后,ZnCM NPs 通过 NF-κB 信号通路促进 CCL5 的降解,从而诱导 igDC-tDC 转化,进一步抑制 CD4 T 细胞稳态。在胶原诱导性关节炎(CIA)小鼠中,这种纳米免疫平台在脾脏中表现出明显的积累,不成熟的 DC(imDCs)分化为 igDCs。诱导脾脏中的 tDCs 以减轻踝关节肿胀,改善行走姿势,并安全抑制踝关节/脾脏炎症。我们的工作开创了 DC 靶向纳米平台与 RA 治疗相结合的先河,并强调了锌和氧平衡通过用修饰的 ZnO NPs 诱导 tDCs 在 RA 的免疫调节中的重要性,这为使用各种不同的金属或非金属离子治疗免疫性疾病的离子平衡调节提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/01ac/9281050/e9d4b2fd6ef7/12951_2022_1536_Fig1_HTML.jpg

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