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骨关节炎的基因治疗:马模型中关节腔内自互补腺相关病毒白细胞介素-1受体拮抗剂递送的药代动力学

Gene Therapy for Osteoarthritis: Pharmacokinetics of Intra-Articular Self-Complementary Adeno-Associated Virus Interleukin-1 Receptor Antagonist Delivery in an Equine Model.

作者信息

Watson Levings Rachael S, Broome Ted A, Smith Andrew D, Rice Brett L, Gibbs Eric P, Myara David A, Hyddmark E Viktoria, Nasri Elham, Zarezadeh Ali, Levings Padraic P, Lu Yuan, White Margaret E, Dacanay E Anthony, Foremny Gregory B, Evans Christopher H, Morton Alison J, Winter Mathew, Dark Michael J, Nickerson David M, Colahan Patrick T, Ghivizzani Steven C

机构信息

1 Department of Orthopedics and Rehabilitation, University of Florida , Gainesville, Florida.

2 Department of Large Animal Clinical Sciences, University of Florida , Gainesville, Florida.

出版信息

Hum Gene Ther Clin Dev. 2018 Jun;29(2):90-100. doi: 10.1089/humc.2017.142.

Abstract

Toward the treatment of osteoarthritis (OA), the authors have been investigating self-complementary adeno-associated virus (scAAV) for intra-articular delivery of therapeutic gene products. As OA frequently affects weight-bearing joints, pharmacokinetic studies of scAAV gene delivery were performed in the joints of the equine forelimb to identify parameters relevant to clinical translation in humans. Using interleukin-1 receptor antagonist (IL-1Ra) as a secreted therapeutic reporter, scAAV vector plasmids containing codon-optimized cDNA for equine IL-1Ra (eqIL-1Ra) were generated, which produced eqIL-1Ra at levels 30- to 50-fold higher than the native sequence. The most efficient cDNA was packaged in AAV2.5 capsid, and following characterization in vitro, the virus was injected into the carpal and metacarpophalangeal joints of horses over a 100-fold dose range. A putative ceiling dose of 5 × 10 viral genomes was identified that elevated the steady-state eqIL-1Ra in the synovial fluids of injected joints by >40-fold over endogenous levels and was sustained for at least 6 months. No adverse effects were seen, and eqIL-1Ra in serum and urine remained at background levels throughout. Using the 5 × 10 viral genome dose of scAAV, and green fluorescent protein as a cytologic marker, the local and systemic distribution of vector and transduced cells following intra-articular injection scAAV.GFP were compared in healthy equine joints and in those with late-stage, naturally occurring OA. In both cases, 99.7% of the vector remained within the injected joint. Strikingly, the pathologies characteristic of OA (synovitis, osteophyte formation, and cartilage erosion) were associated with a substantial increase in transgenic expression relative to tissues in healthy joints. This was most notable in regions of articular cartilage with visible damage, where foci of brilliantly fluorescent chondrocytes were observed. Overall, these data suggest that AAV-mediated gene transfer can provide relatively safe, sustained protein drug delivery to joints of human proportions.

摘要

为了治疗骨关节炎(OA),作者一直在研究用于关节内递送治疗性基因产物的自我互补腺相关病毒(scAAV)。由于OA经常影响负重关节,因此在马前肢关节中进行了scAAV基因递送的药代动力学研究,以确定与人类临床转化相关的参数。使用白细胞介素-1受体拮抗剂(IL-1Ra)作为分泌型治疗报告基因,构建了含有马IL-1Ra(eqIL-1Ra)密码子优化cDNA的scAAV载体质粒,其产生的eqIL-1Ra水平比天然序列高30至50倍。最有效的cDNA被包装在AAV2.5衣壳中,在体外进行表征后,将病毒以100倍的剂量范围注射到马的腕关节和掌指关节中。确定了一个推定的上限剂量为5×10病毒基因组,该剂量使注射关节滑液中的稳态eqIL-1Ra比内源性水平提高了40倍以上,并持续了至少6个月。未观察到不良反应,血清和尿液中的eqIL-1Ra始终保持在背景水平。使用5×10病毒基因组剂量的scAAV,并以绿色荧光蛋白作为细胞标记物,比较了关节内注射scAAV.GFP后载体和转导细胞在健康马关节和晚期自然发生OA的关节中的局部和全身分布。在这两种情况下,99.7%的载体仍留在注射的关节内。令人惊讶的是,与健康关节组织相比,OA的特征性病理变化(滑膜炎、骨赘形成和软骨侵蚀)与转基因表达的大幅增加有关。这在可见损伤的关节软骨区域最为明显,在那里观察到了明亮荧光软骨细胞灶。总体而言,这些数据表明AAV介导的基因转移可以为人体比例的关节提供相对安全、持续的蛋白质药物递送。

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