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Targeted delivery of anti-inflammatory therapy to rheumatoid tissue by fusion proteins containing an IL-4-linked synovial targeting peptide

机译:通过包含IL-4连接的滑膜靶向肽的融合蛋白将抗炎药靶向递送至类风湿组织

摘要

We provide first-time evidence that the synovial endothelium-targeting peptide (SyETP) CKSTHDRLC successfully delivers conjugated IL-4 to human rheumatoid synovium transplanted into SCID mice. SyETP, previously isolated by in vivo phage display and shown to preferentially localize to synovial xenografts, was linked by recombinant technology to hIL-4 via an MMP-cleavable sequence. Both IL-4 and the MMP-cleavable sequence were shown to be functional. IL-4-SyETP augmented production of IL-1ra by synoviocytes stimulated with IL-1[beta] in a dose-dependent manner. In vivo imaging confirmed increased retention of SyETP-linked-IL-4 in synovial grafts which was enhanced by increasing number of copies (one to three) in the constructs. Strikingly, SyETP delivered bioactive IL-4 in vivo as demonstrated by increased pSTAT6 in synovial grafts. Thus, this study provides proof of concept for peptide-tissue-specific targeted immunotherapy in rheumatoid arthritis. This technology is potentially applicable to other biological therapies providing enhanced potency to inflammatory sites and reducing systemic toxicity.
机译:我们提供的首次证据表明,滑膜内皮靶向肽(SyETP)CKSTHDRLC成功地将缀合的IL-4传递给移植到SCID小鼠中的类风湿性滑膜。 SyETP,以前是通过体内噬菌体展示分离的,并且显示优先定位于滑膜异种移植物,通过重组技术通过MMP可切割的序列连接到hIL-4。 IL-4和MMP可切割的序列均显示有功能。 IL-4-SyETP通过用IL-1β刺激的滑膜细胞以剂量依赖的方式增加了IL-1ra的产生。体内成像证实滑膜移植物中SyETP连接的IL-4的保留增加,这通过增加构建体中的拷贝数(一至三)来增强。令人惊讶的是,SyETP在体内传递了生物活性的IL-4,如滑膜移植物中pSTAT6的增加所证明的。因此,该研究为类风湿关节炎中针对肽组织的靶向免疫治疗提供了概念验证。该技术可能适用于其他生物疗法,可增强炎症部位的效力并降低全身毒性。

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