早期和慢性人髌骨肌腱病的病理肌腱组织学

IF 1.2 Q3 SPORT SCIENCES Translational sports medicine Pub Date : 2022-10-04 eCollection Date: 2022-01-01 DOI:10.1155/2022/2799665
Nikolaj Moelkjaer Malmgaard-Clausen, Michael Kjaer, Stephanie G Dakin
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引用次数: 0

摘要

本初步研究调查了慢性腱病和表现出腱病早期临床症状的个体的组织学组织变化程度。该研究包括8名患者,其中3人健康,没有任何肌腱症状,2人有早期症状(1-2 月),3人有慢性症状(>3 几个月)从他们的髌腱。从受影响的肌腱组织区域获得经皮穿刺活检样本。活检样本用苏木精和曙红染色,并进行多重免疫荧光染色以确定炎症和消退的标志物。来自这个小患者队列的早期和慢性期髌腱活检样本都显示出束间基质(IFM)和内皮区域的扩张,以及细胞和血管的增加。这些组织学观察结果在早期腱病中是中等的,而在慢性腱病中更为明显,并与组织结构的显著破坏有关。早期腱性病变的髌腱表达与成纤维细胞(CD90、CD34)、巨噬细胞(S100A8)和内皮细胞(ICAM1、VCAM1)的活化表型相关的标志物。这些组织还表达与炎症有关的酶(PTGS2、15PGDH)和分解(ALOX12)以及分解前受体ERV1。这些标志物的免疫阳性染色主要位于IFM区域。这些初步发现表明,包括IFM和内皮区扩张在内的轻度至中度结构组织学变化是早期腱病的病理特征,支持炎症和消退过程在早期疾病中很活跃。需要对早期肌腱病的细胞和分子基础进行进一步研究,以制定预防不可逆慢性肌腱疾病发展的治疗策略。
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Pathological Tendon Histology in Early and Chronic Human Patellar Tendinopathy.

The present pilot study investigated the extent of histological tissue changes in both chronic tendinopathy and in individuals that display early clinical signs of tendinopathy. The study included 8 individuals of whom 3 were healthy without any tendon symptoms, 2 had early symptoms (1-2 months), and 3 had chronic symptoms (>3 months) from their patellar tendons. Percutaneous needle biopsy samples were obtained from the affected tendon tissue region. Biopsy samples were stained with Haematoxylin & Eosin, and multiplex immunofluorescence staining was performed for markers of inflammation and resolution. Both early and chronic stage patellar tendon biopsy samples from this small patient cohort exhibited expansion of the interfascicular matrix (IFM) and endotenon regions together with increased cellularity and vascularity. These histological observations were moderate in early tendinopathy, whereas they were more pronounced and associated with marked disruption of tissue architecture in chronic tendinopathy. Early stage tendinopathic patellar tendons expressed markers associated with an activated phenotype of fibroblasts (CD90, CD34), macrophages (S100A8), and endothelial cells (ICAM1, VCAM1). These tissues also expressed enzymes implicated in inflammation (PTGS2, 15PGDH) and resolution (ALOX12) and the proresolving receptor ERV1. Immunopositive staining for these markers was predominantly located in the IFM regions. These preliminary findings suggest that mild to moderate structural histological changes including expansion of IFM and endotenon regions are pathological features of early tendinopathy, and support inflammatory and resolving processes are active in early-stage disease. Further investigation of the cellular and molecular basis of early-stage tendinopathy is required to inform therapeutic strategies that prevent the development of irreversible chronic tendon disease.

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