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人类骨关节炎关节的滑膜保持其软骨生成潜力,与年龄无关。

The Synovium of Human Osteoarthritic Joints Retains Its Chondrogenic Potential Irrespective of Age.

机构信息

Department of Osteoporosis, Inselspital Bern University Hospital, Bern, Switzerland.

Department of Orthopaedic Surgery, Inselspital Bern University Hospital, Bern, Switzerland.

出版信息

Tissue Eng Part A. 2022 Mar;28(5-6):283-295. doi: 10.1089/ten.TEA.2021.0105. Epub 2021 Dec 27.

Abstract

The autologous synovium is a potential tissue source for local induction of chondrogenesis by tissue engineering approaches to repair articular cartilage defects that occur in osteoarthritis. It was the aim of the present study to ascertain whether the aging of human osteoarthritic patients compromises the chondrogenic potential of their knee-joint synovium and the structural and metabolic stability of the transformed tissue. The patients were allocated to one of the following two age categories: 54-65 years and 66-86 years ( = 7-11 donors per time point and experimental group; total number of donors: 64). Synovial biopsies were induced to undergo chondrogenesis by exposure to bone morphogenetic protein-2 (BMP-2) alone, transforming growth factor-β1 (TGF-β1) alone, or a combination of the two growth factors, for up to 6 weeks. The differentiated explants were evaluated morphologically and morphometrically for the volume fraction of metachromasia (sulfated proteoglycans), immunohistochemically for type-II collagen, and for the gene expression levels of anabolic chondrogenic markers as well as catabolic factors by a real-time polymerase chain reaction analysis. Quantitative metachromasia revealed that chondrogenic differentiation of human synovial explants was induced to the greatest degree by either BMP-2 alone or the BMP-2/TGF-β1 combination, that is, to a comparable level with each of the two stimulation protocols and within both age categories. The BMP-2/TGF-β1combination protocol resulted in chondrocytes of a physiological size for normal human articular cartilage, unlike the BMP-2-alone stimulation that resulted in cell sizes of terminal hypertrophy. The stable gene expression levels of the anabolic chondrogenic markers confirmed the superiority of these two stimulation protocols and demonstrated the hyaline-like qualities of the generated cartilage matrix. The gene expression levels of the catabolic markers remained extremely low. The data also confirmed the usefulness of experimental studies with bovine synovial tissue as a paradigm for human synovial investigations. Our data reveal the chondrogenic potential of the human knee-joint synovium of osteoarthritic patients to be uncompromised by aging and catabolic processes. The potential of synovium-based clinical engineering (repair) of cartilage tissue using autologous synovium may thus not be reduced by the age of the human patient. Impact statement Our data reveal that in younger and older age groups alike, synovial explants from osteoarthritic joints can be equally well induced to undergo chondrogenesis ; that is, the chondrogenic potential of the human synovium is not compromised by aging. These findings imply that the autologous synovium represents an adequate tissue source for the repair of articular cartilage in clinical practice by tissue engineering approaches in human patients suffering from osteoarthritis, independent of the patient's age.

摘要

自体滑膜是一种潜在的组织来源,可以通过组织工程方法局部诱导软骨生成,从而修复骨关节炎中发生的关节软骨缺损。本研究旨在确定人类骨关节炎患者的衰老是否会影响其膝关节滑膜的软骨生成潜力以及转化组织的结构和代谢稳定性。将患者分配到以下两个年龄组之一:54-65 岁和 66-86 岁(每个时间点和实验组有 7-11 个供体;供体总数:64 个)。滑膜活检通过单独暴露于骨形态发生蛋白-2(BMP-2)、转化生长因子-β1(TGF-β1)或两种生长因子的组合来诱导软骨生成,时间长达 6 周。通过实时聚合酶链反应分析评估分化的外植体的体积分数(硫酸软骨素)、Ⅱ型胶原的免疫组织化学以及合成代谢软骨生成标记物和分解代谢因子的基因表达水平。定量变色表明,人类滑膜外植体的软骨生成分化程度最大,无论是单独使用 BMP-2 还是 BMP-2/TGF-β1 联合使用,都与两种刺激方案中的每一种以及两个年龄组中的每一种相当。BMP-2/TGF-β1 联合方案导致的软骨细胞大小与正常人类关节软骨的生理大小相似,而单独使用 BMP-2 刺激则导致终末肥大的细胞大小。合成代谢软骨生成标记物的稳定基因表达水平证实了这两种刺激方案的优越性,并证明了所产生的软骨基质的透明样特性。分解代谢标记物的基因表达水平仍然极低。这些数据还证实了使用牛滑膜组织进行实验研究作为人类滑膜研究范例的有用性。我们的数据表明,骨关节炎患者膝关节滑膜的软骨生成潜力不受衰老和分解代谢过程的影响。因此,使用自体滑膜进行基于滑膜的临床工程(修复)软骨组织的潜力不会因患者年龄的增长而降低。

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