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跟腱和髌腱病变的细胞与结构变化:一项体内初步研究

Cellular and Structural Changes in Achilles and Patellar Tendinopathies: A Pilot In Vivo Study.

作者信息

Kouroupis Dimitrios, Perucca Orfei Carlotta, Correa Diego, Talò Giuseppe, Libonati Francesca, De Luca Paola, Raffo Vincenzo, Best Thomas M, de Girolamo Laura

机构信息

Department of Orthopedics, UHealth Sports Medicine Institute, Miller School of Medicine, University of Miami, Miami, FL 33146, USA.

Diabetes Research Institute & Cell Transplant Center, Miller School of Medicine, University of Miami, Miami, FL 33136, USA.

出版信息

Biomedicines. 2024 Apr 30;12(5):995. doi: 10.3390/biomedicines12050995.

Abstract

Tendinopathies continue to be a challenge for both patients and the medical teams providing care as no universal clinical practice guidelines have been established. In general, tendinopathies are typically characterized by prolonged, localized, activity-related pain with abnormalities in tissue composition, cellularity, and microstructure that may be observed on imaging or histology. In the lower limb, tendinopathies affecting the Achilles and the patellar tendons are the most common, showing a high incidence in athletic populations. Consistent diagnosis and management have been challenged by a lack of universal consensus on the pathophysiology and clinical presentation. Current management is primarily based on symptom relief and often consists of medications such as non-steroidal anti-inflammatories, injectable therapies, and exercise regimens that typically emphasize progressive eccentric loading of the affected structures. Implementing the knowledge of tendon stem/progenitor cells (TSPCs) and assessing their potential in enhancing tendon repair could fill an important gap in this regard. In the present pilot in vivo study, we have characterized the structural and cellular alterations that occur soon after tendon insult in models of both Achilles and patellar tendinopathy. Upon injury, CD146 TSPCs are recruited from the interfascicular tendon matrix to the vicinity of the paratenon, whereas the observed reduction in M1 macrophage polarization is related to a greater abundance of reparative CD146 TSPCs in situ. The robust TSPCs' immunomodulatory effects on macrophages were also demonstrated in in vitro settings where TSPCs can effectively polarize M1 macrophages towards an anti-inflammatory therapeutic M2 phenotype. Although preliminary, our findings suggest CD146 TSPCs as a key phenotype that could be explored in the development of targeted regenerative therapies for tendinopathies.

摘要

肌腱病对于患者和提供护理的医疗团队来说仍然是一个挑战,因为尚未建立通用的临床实践指南。一般来说,肌腱病的典型特征是长期的、局部的、与活动相关的疼痛,组织成分、细胞数量和微观结构存在异常,这些异常可在影像学或组织学上观察到。在下肢,影响跟腱和髌腱的肌腱病最为常见,在运动员群体中发病率很高。由于对病理生理学和临床表现缺乏普遍共识,一致的诊断和管理面临挑战。目前的治疗主要基于症状缓解,通常包括使用非甾体抗炎药等药物、注射治疗和运动方案,这些方案通常强调对受影响结构进行渐进性离心负荷训练。了解肌腱干/祖细胞(TSPCs)的知识并评估它们在增强肌腱修复方面的潜力可以填补这方面的一个重要空白。在本项体内初步研究中,我们描述了跟腱和髌腱肌腱病模型中肌腱损伤后不久发生的结构和细胞改变。损伤后,CD146 TSPCs从束间肌腱基质募集到腱旁组织附近,而观察到的M1巨噬细胞极化减少与原位修复性CD146 TSPCs数量增加有关。在体外实验中也证明了TSPCs对巨噬细胞具有强大的免疫调节作用,TSPCs可以有效地将M1巨噬细胞极化为抗炎治疗性M2表型。尽管是初步研究,但我们的发现表明CD146 TSPCs是一种关键表型,可用于探索针对肌腱病的靶向再生疗法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/47dc/11117798/93dcbec38f61/biomedicines-12-00995-g001.jpg

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