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按需从酶响应型可注射水凝胶中释放选择性 MMP-13 抑制剂可防止骨关节炎中软骨的退行性进展。

On-demand release of a selective MMP-13 blocker from an enzyme-responsive injectable hydrogel protects cartilage from degenerative progression in osteoarthritis.

机构信息

Chemical Biology Unit, Institute of Nano Science and Technology, Knowledge City, Sector-81, Mohali-140306, Punjab, India.

Division of Endocrinology and Centre for Research in ASTHI, CSIR-Central Drug Research Institute, Lucknow-226031, Uttar Pradesh, India.

出版信息

J Mater Chem B. 2024 Jun 5;12(22):5325-5338. doi: 10.1039/d3tb02871b.

DOI:10.1039/d3tb02871b
PMID:38669084
Abstract

In osteoarthritis (OA), the degradation of cartilage is primarily driven by matrix metalloprotease-13 (MMP-13). Hence, the inhibition of MMP-13 has emerged as an attractive target for OA treatment. Among the various approaches that are being explored for MMP-13 regulation, blocking of the enzyme with specific binding molecules appears to be a more promising strategy for preventing cartilage degeneration. To enhance effectiveness and ensure patient compliance, it is preferable for the binding molecule to exhibit sustained activity when administered directly into the joint. Herein, we present an enzyme-responsive hydrogel that was designed to exhibit on-demand, the sustained release of BI-4394, a potent and highly selective MMP-13 blocker. The stable and compatible hydrogel was prepared using triglycerol monostearate. The efficacy of the hydrogel to prevent cartilage damage was assessed in a rat model of OA induced by anterior cruciate ligament transection (ACLT). The results revealed that in comparison to the rats administrated weekly with intra-articular BI-4394, the hydrogel implanted rats had reduced levels of inflammation and bone erosion. In comparison to untreated control, the cartilage in animals administered with BI-4394/hydrogel exhibited significant levels of collagen-2 and aggrecan along with reduced MMP-13. Overall, this study confirmed the potential of BI-4394 delivery using an enzyme-responsive hydrogel as a promising treatment option to treat the early stages of OA by preventing further cartilage degradation.

摘要

在骨关节炎(OA)中,软骨的降解主要由基质金属蛋白酶-13(MMP-13)驱动。因此,抑制 MMP-13 已成为 OA 治疗的一个有吸引力的靶点。在探索 MMP-13 调节的各种方法中,用特异性结合分子阻断酶似乎是预防软骨退化的更有前途的策略。为了提高疗效和确保患者的依从性,当直接施用于关节时,结合分子最好表现出持续的活性。在此,我们提出了一种酶响应水凝胶,旨在按需持续释放 BI-4394,这是一种有效的、高度选择性的 MMP-13 抑制剂。该稳定且相容的水凝胶是使用三甘油脂单硬脂酸酯制备的。通过前交叉韧带切断术(ACLT)诱导的 OA 大鼠模型评估了水凝胶预防软骨损伤的功效。结果表明,与每周关节内给予 BI-4394 的大鼠相比,植入水凝胶的大鼠炎症和骨侵蚀水平降低。与未治疗的对照组相比,给予 BI-4394/水凝胶的动物的软骨中胶原-2 和聚集蛋白聚糖的水平显著升高,同时 MMP-13 水平降低。总体而言,这项研究证实了使用酶响应水凝胶递送 BI-4394 作为一种有前途的治疗选择的潜力,通过防止进一步的软骨降解来治疗 OA 的早期阶段。

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