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一种有前途的关节软骨再生新配方:在人类滑膜液细胞中过表达 SOX9 的治疗方法的临床前评估。

A promising novel formulation for articular cartilage regeneration: Preclinical evaluation of a treatment that produces SOX9 overexpression in human synovial fluid cells.

机构信息

Cancerology State Institute, Colima State Health Services, Colima 28000, Mexico.

Centro Hospitalario Union, Villa de Álvarez, Colima 28950, Mexico.

出版信息

Mol Med Rep. 2018 Mar;17(3):3503-3510. doi: 10.3892/mmr.2017.8336. Epub 2017 Dec 20.

Abstract

Osteoarthritis (OA) is a chronic disorder of synovial joints, in which there is progressive softening and disintegration of the articular cartilage. OA is the most common form of arthritis, and is the primary cause of disability and impaired quality of life in the elderly. Despite considerable medical necessity, no treatment has yet been proven to act as a disease‑modifying agent that may halt or reverse the structural progression of OA. The replacement of the joint with a prosthesis appears to be the best option in the advanced stages of the disease. A formulation (BIOF2) for cartilage regeneration has been recently developed. The present study evaluated the effects of BIOF2 on gene expression in human cell cultures, followed by efficacy trials in three OA animal models. Human synovial fluid cells that were exposed to the formulation exhibited increased transcription factor SOX‑9 (SOX9; chondrogenic factor) expression, and decreased mimecan (mineralization inducer) and macrophage‑stimulating protein receptor (osteoclastogenic factor) expression. The intra‑articular application of BIOF2 in the animal models significantly increased cartilage thickness from 12 to 31% at 28 days, compared with articular cartilage treated with saline solution. The articular area and number of chondrocytes additionally increased significantly, maintaining an unaltered chondrocyte/mm2 proportion. Evaluation of the histological architecture additionally displayed a decrease in the grade of articular damage in the groups treated with BIOF2. In conclusion, BIOF2 has proven to be effective for treating OA in animal models, most likely due to SOX9 overexpression in articular cells.

摘要

骨关节炎(OA)是一种慢性滑膜关节疾病,其特征是关节软骨逐渐软化和崩解。OA 是最常见的关节炎类型,也是老年人残疾和生活质量受损的主要原因。尽管有大量的医疗需求,但目前还没有任何治疗方法被证明可以作为一种疾病修饰剂,从而阻止或逆转 OA 的结构进展。在疾病的晚期,用假体置换关节似乎是最好的选择。最近开发了一种用于软骨再生的配方(BIOF2)。本研究评估了 BIOF2 对人细胞培养物中基因表达的影响,随后在三种 OA 动物模型中进行了疗效试验。暴露于该配方的人滑膜液细胞表现出转录因子 SOX-9(SOX9;软骨生成因子)表达增加,而 mimecan(矿化诱导因子)和巨噬细胞刺激蛋白受体(破骨细胞生成因子)表达减少。在动物模型中,BIOF2 的关节内应用在 28 天时将软骨厚度从 12%增加到 31%,与用生理盐水处理的关节软骨相比增加了 31%。关节面积和软骨细胞数量也显著增加,保持不变的软骨细胞/mm2 比例。对组织学结构的评估还显示,BIOF2 治疗组的关节损伤程度评分降低。总之,BIOF2 已被证明在动物模型中对 OA 治疗有效,这可能是由于关节细胞中 SOX9 的过度表达。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3f08/5802147/54dfa5bc6997/MMR-17-03-3503-g00.jpg

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