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基于纳米颗粒的肌腱靶向药物传递系统的开发,以药理学方式调节肌腱愈合。

Development of a nanoparticle-based tendon-targeting drug delivery system to pharmacologically modulate tendon healing.

机构信息

Department of Biomedical Engineering, University of Rochester, Rochester, NY 14623, USA.

Center for Musculoskeletal Research, University of Rochester Medical Center, Rochester, NY 14642, USA.

出版信息

Sci Adv. 2024 Jun 21;10(25):eadn2332. doi: 10.1126/sciadv.adn2332. Epub 2024 Jun 19.

Abstract

Satisfactory healing following acute tendon injury is marred by fibrosis. Despite the high frequency of tendon injuries and poor outcomes, there are no pharmacological therapies in use to enhance the healing process. Moreover, systemic treatments demonstrate poor tendon homing, limiting the beneficial effects of potential tendon therapeutics. To address this unmet need, we leveraged our existing tendon healing spatial transcriptomics dataset and identified an area enriched for expression of (TRAP) and subsequently demonstrated robust TRAP activity in the healing tendon. This unexpected finding allowed us to refine and apply our existing TRAP binding peptide (TBP) functionalized nanoparticle (NP) drug delivery system (DDS) to facilitate improved delivery of systemic treatments to the healing tendon. To demonstrate the translational potential of this DDS, we delivered niclosamide (NEN), an inhibitor. While systemic delivery of free NEN did not alter healing, TBP-NP enhanced both functional and mechanical recovery, demonstrating the translational potential of this approach to enhance the tendon healing process.

摘要

尽管肌腱损伤的频率很高,且预后不佳,但目前尚无用于增强愈合过程的药理学治疗方法。此外,全身治疗对肌腱的归巢作用不佳,限制了潜在肌腱治疗药物的有益效果。为了满足这一未满足的需求,我们利用现有的肌腱愈合空间转录组学数据集,鉴定出一个富含表达的区域(TRAP),并随后在愈合的肌腱中证实了强大的 TRAP 活性。这一意外的发现使我们能够改进和应用我们现有的 TRAP 结合肽(TBP)功能化纳米颗粒(NP)药物递送系统(DDS),以促进全身治疗药物更有效地递送到愈合的肌腱。为了证明这种 DDS 的转化潜力,我们递送了尼氯硝唑(NEN),一种 抑制剂。虽然游离 NEN 的全身递送并未改变愈合,但 TBP-NP 增强了功能和机械恢复,证明了这种方法增强肌腱愈合过程的转化潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dca4/11186494/b2c56ef44792/sciadv.adn2332-f1.jpg

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