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Treatment of osteoarthritis using a helper-dependent adenoviral vector retargeted to chondrocytes

机译:使用靶向软骨细胞的辅助依赖性腺病毒载体治疗骨关节炎

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摘要

Osteoarthritis (OA) is a joint disease characterized by degeneration of the articular cartilage, subchondral bone remodeling, and secondary inflammation. It is among the top three causes of chronic disability, and currently there are no treatment options to prevent disease progression. The localized nature of OA makes it an ideal candidate for gene and cell therapy. However, gene and cell therapy of OA is impeded by inefficient gene transduction of chondrocytes. In this study, we developed a broadly applicable system that retargets cell surface receptors by conjugating antibodies to the capsid of helper-dependent adenoviral vectors (HDVs). Specifically, we applied this system to retarget chondrocytes by conjugating an HDV to an α-10 integrin monoclonal antibody (a10mab). We show that a10mab-conjugated HDV (a10mabHDV)-infected chondrocytes efficiently in vitro and in vivo while detargeting other cell types. The therapeutic index of an intra-articular injection of 10mabHDV-expressing proteoglycan 4 (PRG4) into a murine model of post-traumatic OA was 10-fold higher than with standard HDV. Moreover, we show that PRG4 overexpression from articular, superficial zone chondrocytes is effective for chondroprotection in postinjury OA and that α-10 integrin is an effective protein for chondrocyte targeting.
机译:骨关节炎(OA)是一种关节疾病,其特征在于关节软骨变性,软骨下骨重塑和继发性炎症。它是慢性残疾的三大原因之一,目前没有预防疾病进展的治疗选择。 OA的局部性质使其成为基因和细胞疗法的理想候选者。然而,软骨细胞的低效率基因转导阻碍了OA的基因和细胞治疗。在这项研究中,我们开发了一种可广泛应用的系统,该系统通过将抗体与辅助依赖型腺病毒载体(HDV)衣壳缀合来重新靶向细胞表面受体。具体来说,我们通过将HDV与α-10整联蛋白单克隆抗体(a10mab)结合,将这一系统应用于软骨细胞的再靶向。我们显示a10mab缀合的HDV(a10mabHDV)感染的软骨细胞有效地在体外和体内,同时使其他细胞类型脱靶。向创伤后OA的小鼠模型中关节内注射表达10mabHDV的蛋白聚糖4(PRG4)的治疗指数比标准HDV高10倍。此外,我们表明,从关节,浅表区软骨细胞过度表达PRG4对于损伤后OA中的软骨保护有效,而α-10整联蛋白是针对软骨细胞的有效蛋白质。

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