Generation of cytotoxic aptamers specifically targeting fibroblast-like synoviocytes by CSCT-SELEX for treatment of rheumatoid arthritis.

IF 20.3 1区医学 Q1 RHEUMATOLOGY

Annals of the Rheumatic Diseases Pub Date : 2024-09-04 DOI:10.1136/ard-2024-225565

Fang Qiu, Duoli Xie, Hongzhen Chen, Zhuqian Wang, Jie Huang, Chunhao Cao, Yiying Liang, Xu Yang, Dong-Yi He, Xuekun Fu, Aiping Lu, Chao Liang

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引用次数: 0

Abstract

Objectives: Rheumatoid arthritis (RA) is an autoimmune disease characterised by aggressive fibroblast-like synoviocytes (FLSs). Very few RA patients-derived FLSs (RA-FLSs)-specific surface signatures have been identified, and there is currently no approved targeted therapy for RA-FLSs. This study aimed to screen therapeutic aptamers with cell-targeting and cytotoxic properties against RA-FLSs and to uncover the molecular targets and mechanism of action of the screened aptamers.

Methods: We developed a cell-specific and cytotoxic systematic evolution of ligands by exponential enrichment (CSCT-SELEX) method to screen the therapeutic aptamers without prior knowledge of the surface signatures of RA-FLSs. The molecular targets and mechanisms of action of the screened aptamers were determined by pull-down assays and RNA sequencing. The therapeutic efficacy of the screened aptamers was examined in arthritic mouse models.

Results: We obtained an aptamer SAPT8 that selectively recognised and killed RA-FLSs. The molecular target of SAPT8 was nucleolin (NCL), a shuttling protein overexpressed on the surface and involved in the tumor-like transformation of RA-FLSs. Mechanistically, SAPT8 interacted with the surface NCL and was internalised to achieve lysosomal degradation of NCL, leading to the upregulation of proapoptotic p53 and downregulation of antiapoptotic B-cell lymphoma 2 (Bcl-2) in RA-FLSs. When administrated systemically to arthritic mice, SAPT8 accumulated in the inflamed FLSs of joints. SAPT8 monotherapy or its combination with tumour necrosis factor (TNF)-targeted biologics was shown to relieve arthritis in mouse models.

Conclusions: CSCT-SELEX could be a promising strategy for developing cell-targeting and cytotoxic aptamers. SAPT8 aptamer selectively ablates RA-FLSs via modulating NCL-p53/Bcl-2 signalling, representing a potential alternative or complementary therapy for RA.

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通过 CSCT-SELEX 生成特异性靶向成纤维细胞样滑膜细胞的细胞毒性适配体，用于治疗类风湿性关节炎。

目的：类风湿性关节炎（RA）是一种以侵袭性成纤维细胞样滑膜细胞（FLSs）为特征的自身免疫性疾病。目前只发现了极少数 RA 患者衍生的 FLSs（RA-FLSs）特异性表面特征，而且目前还没有针对 RA-FLSs 的获批靶向疗法。本研究旨在筛选针对RA-FLSs具有细胞靶向性和细胞毒性的治疗性适配体，并揭示筛选出的适配体的分子靶点和作用机制：我们开发了一种细胞特异性和细胞毒性配体的指数富集系统进化（CSCT-SELEX）方法，在事先不了解RA-FLSs表面特征的情况下筛选治疗性适配体。筛选出的适配体的分子靶点和作用机制是通过下拉实验和RNA测序确定的。在关节炎小鼠模型中检验了筛选出的适配体的疗效：结果：我们获得了一种能选择性识别并杀死RA-FLS的适配体SAPT8。SAPT8的分子靶点是核仁蛋白（NCL），它是一种表面过度表达的穿梭蛋白，参与了RA-FLSs的肿瘤样转化。从机理上讲，SAPT8 与表面的 NCL 相互作用，并被内化以实现 NCL 的溶酶体降解，从而导致 RA-FLS 中促凋亡的 p53 上调和抗凋亡的 B 细胞淋巴瘤 2（Bcl-2）下调。给关节炎小鼠全身用药时，SAPT8会在关节发炎的FLS中积聚。在小鼠模型中，SAPT8单药治疗或与肿瘤坏死因子（TNF）靶向生物制剂联合治疗均可缓解关节炎：结论：CSCT-SELEX可能是开发细胞靶向和细胞毒性适配体的一种有前途的策略。SAPT8适配体通过调节NCL-p53/Bcl-2信号选择性地消减RA-FLS，是治疗RA的一种潜在替代或补充疗法。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Annals of the Rheumatic Diseases 医学-风湿病学

CiteScore

35.00

自引率

9.90%

发文量

3728

审稿时长

1.4 months

期刊介绍： Annals of the Rheumatic Diseases (ARD) is an international peer-reviewed journal covering all aspects of rheumatology, which includes the full spectrum of musculoskeletal conditions, arthritic disease, and connective tissue disorders. ARD publishes basic, clinical, and translational scientific research, including the most important recommendations for the management of various conditions.

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