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本文引用的文献

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Electrospun nanofibrous materials for tissue engineering and drug delivery.用于组织工程和药物递送的电纺纳米纤维材料。
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The current state of scaffolds for musculoskeletal regenerative applications.用于肌肉骨骼再生应用的支架的现状。
Nat Rev Rheumatol. 2015 Apr;11(4):213-22. doi: 10.1038/nrrheum.2015.27. Epub 2015 Mar 17.
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Comparative effectiveness of pharmacologic interventions for knee osteoarthritis: a systematic review and network meta-analysis.药物干预治疗膝骨关节炎的疗效比较:系统评价和网络荟萃分析。
Ann Intern Med. 2015 Jan 6;162(1):46-54. doi: 10.7326/M14-1231.
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Strategic design and fabrication of engineered scaffolds for articular cartilage repair.用于关节软骨修复的工程支架的策略性设计与制造
J Funct Biomater. 2012 Nov 14;3(4):799-838. doi: 10.3390/jfb3040799.
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Emerging pathways and promising agents with possible disease modifying effect in osteoarthritis treatment.在骨关节炎治疗中具有潜在疾病修饰作用的新兴途径和有前途的药物。
Curr Drug Targets. 2014 Jun;15(6):635-61. doi: 10.2174/1389450115666140306153115.
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Drug delivery systems for intra-articular treatment of osteoarthritis.用于骨关节炎关节内治疗的药物输送系统。
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Interleukin-1 beta and tumor necrosis factor alpha inhibit migration activity of chondrogenic progenitor cells from non-fibrillated osteoarthritic cartilage.白细胞介素-1β和肿瘤坏死因子-α抑制非纤维性骨关节炎软骨来源的软骨祖细胞的迁移活性。
Arthritis Res Ther. 2013;15(5):R119. doi: 10.1186/ar4299.
8
Short-chain fatty acid-modified hexosamine for tissue-engineering osteoarthritic cartilage.短链脂肪酸修饰的己糖胺用于组织工程化骨关节炎软骨。
Tissue Eng Part A. 2013 Sep;19(17-18):2035-44. doi: 10.1089/ten.TEA.2012.0317. Epub 2013 Jun 8.
9
Differential response of chondrocytes and chondrogenic-induced mesenchymal stem cells to C1-OH tributanoylated N-acetylhexosamines.软骨细胞和诱导性软骨形成间充质干细胞对 C1-OH 三丁酸酰化 N-乙酰己糖胺的差异反应。
PLoS One. 2013;8(3):e58899. doi: 10.1371/journal.pone.0058899. Epub 2013 Mar 14.
10
Functional articular cartilage repair: here, near, or is the best approach not yet clear?功能性关节软骨修复:此处、附近,还是最佳方法尚不清楚?
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具有抗炎三丁酰化N-乙酰-d-葡萄糖胺的电纺微纤维支架促进软骨再生。

Electrospun Microfiber Scaffolds with Anti-Inflammatory Tributanoylated N-Acetyl-d-Glucosamine Promote Cartilage Regeneration.

作者信息

Kim Chaekyu, Shores Lucas, Guo Qiongyu, Aly Ahmed, Jeon Ok Hee, Kim Do Hun, Bernstein Nicholas, Bhattacharya Rahul, Chae Jemin Jeremy, Yarema Kevin J, Elisseeff Jennifer H

机构信息

Translational Tissue Engineering Center, Wilmer Eye Institute and the Department of Biomedical Engineering, Johns Hopkins University , Baltimore, Maryland.

出版信息

Tissue Eng Part A. 2016 Apr;22(7-8):689-97. doi: 10.1089/ten.TEA.2015.0469.

DOI:10.1089/ten.TEA.2015.0469
PMID:27019285
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4841077/
Abstract

Tissue-engineering strategies offer promising tools for repairing cartilage damage; however, these strategies suffer from limitations under pathological conditions. As a model disease for these types of nonideal systems, the inflammatory environment in an osteoarthritic (OA) joint limits the efficacy of engineered therapeutics by disrupting joint homeostasis and reducing its capacity for regeneration. In this work, we investigated a sugar-based drug candidate, a tributanoylated N-acetyl-d-glucosamine analogue, called 3,4,6-O-Bu3GlcNAc, that is known to reduce nuclear factor kappa-light-chain-enhancer of activated B cells (NF-κB) signaling in osteoarthritis. 3,4,6-O-Bu3GlcNAc not only inhibited NFκB signaling but also exerted chondrogenic and anti-inflammatory effects on chondrocytes isolated from patients with osteoarthritis. 3,4,6-O-Bu3GlcNAc also increased the expression of extracellular matrix proteins and induced cartilage tissue production in three-dimensional in vitro hydrogel culture systems. To translate these chondrogenic and anti-inflammatory properties to tissue regeneration in osteoarthritis, we implanted 3,4,6-O-Bu3GlcNAc-loaded poly(lactic-co-glycolic acid) microfiber scaffolds into rats. The drug-laden scaffolds were biocompatible, and when seeded with human OA chondrocytes, similarly promoted cartilage tissue formation. 3,4,6-O-Bu3GlcNAc combined with the appropriate structural environment could be a promising therapeutic approach for osteoarthritis.

摘要

组织工程策略为修复软骨损伤提供了有前景的工具;然而,这些策略在病理条件下存在局限性。作为这些非理想系统类型的模型疾病,骨关节炎(OA)关节中的炎症环境通过破坏关节稳态并降低其再生能力,限制了工程治疗方法的疗效。在这项工作中,我们研究了一种基于糖的候选药物,一种三丁酰化的N-乙酰-d-葡萄糖胺类似物,称为3,4,6-O-三丁酰基葡糖胺(3,4,6-O-Bu3GlcNAc),已知其可减少骨关节炎中活化B细胞的核因子κB(NF-κB)信号传导。3,4,6-O-Bu3GlcNAc不仅抑制NFκB信号传导,还对从骨关节炎患者分离的软骨细胞发挥软骨生成和抗炎作用。3,4,6-O-Bu3GlcNAc还增加了细胞外基质蛋白的表达,并在三维体外水凝胶培养系统中诱导了软骨组织的产生。为了将这些软骨生成和抗炎特性转化为骨关节炎的组织再生,我们将负载3,4,6-O-Bu3GlcNAc的聚(乳酸-共-乙醇酸)微纤维支架植入大鼠体内。载药支架具有生物相容性,当接种人OA软骨细胞时,同样促进了软骨组织的形成。3,4,6-O-Bu3GlcNAc与合适的结构环境相结合可能是一种有前景的骨关节炎治疗方法。