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一种用于关节内给药的热响应性生物聚合物。

A thermally responsive biopolymer for intra-articular drug delivery.

作者信息

Betre Helawe, Liu Wenge, Zalutsky Michael R, Chilkoti Ashutosh, Kraus Virginia B, Setton Lori A

机构信息

Department of Biomedical Engineering, 136 Hudson Hall, Box 90821, Duke University, Durham, NC 27708, USA.

出版信息

J Control Release. 2006 Oct 10;115(2):175-82. doi: 10.1016/j.jconrel.2006.07.022. Epub 2006 Jul 26.

Abstract

Intra-articular drug delivery is the preferred standard for targeting pharmacologic treatment directly to joints to reduce undesirable side effects associated with systemic drug delivery. In this study, a biologically based drug delivery vehicle was designed for intra-articular drug delivery using elastin-like polypeptides (ELPs), a biopolymer composed of repeating pentapeptides that undergo a phase transition to form aggregates above their transition temperature. The ELP drug delivery vehicle was designed to aggregate upon intra-articular injection at 37 degrees C, and form a drug 'depot' that could slowly disaggregate and be cleared from the joint space over time. We evaluated the in vivo biodistribution and joint half-life of radiolabeled ELPs, with and without the ability to aggregate, at physiological temperatures encountered after intra-articular injection in a rat knee. Biodistribution studies revealed that the aggregating ELP had a 25-fold longer half-life in the injected joint than a similar molecular weight protein that remained soluble and did not aggregate. These results suggest that the intra-articular joint delivery of ELP-based fusion proteins may be a viable strategy for the prolonged release of disease-modifying protein drugs for osteoarthritis and other arthritides.

摘要

关节内给药是将药物治疗直接靶向关节以减少全身给药相关不良副作用的首选标准方法。在本研究中,设计了一种基于生物学的药物递送载体,用于关节内给药,该载体使用类弹性蛋白多肽(ELP),一种由重复五肽组成的生物聚合物,在其转变温度以上会发生相变形成聚集体。ELP药物递送载体设计为在37℃关节内注射时聚集,并形成药物“贮库”,随着时间的推移,该“贮库”可缓慢解聚并从关节腔清除。我们评估了在大鼠膝关节内注射后生理温度下,有聚集能力和无聚集能力的放射性标记ELP的体内生物分布和关节半衰期。生物分布研究表明,与保持可溶且不聚集的类似分子量蛋白质相比,聚集性ELP在注射关节中的半衰期长25倍。这些结果表明,基于ELP的融合蛋白的关节内递送可能是用于骨关节炎和其他关节炎疾病修饰蛋白药物长效释放的可行策略。

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