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各种组织工程骨关节炎模型的开发与特性研究。

Development and characterization of various osteoarthritis models for tissue engineering.

机构信息

KU-KIST Graduate School of Converging Science and Technology, Korea University, Seoul, Korea.

Center for Biomaterials, Korea Institute of Science and Technology, Seoul, Republic of Korea.

出版信息

PLoS One. 2018 Mar 13;13(3):e0194288. doi: 10.1371/journal.pone.0194288. eCollection 2018.

Abstract

Osteoarthritis (OA) is characterized by a progressive loss of articular cartilage, subchondral bone sclerosis and synovial inflammation and is the most common chronic condition worldwide today. However, most treatments have focused on pain relief and OA symptoms. For these reasons, many ongoing studies are currently trying to develop efficient and successful therapies based on its pathology. Animal models that mimic the histopathology and symptoms of OA have a critical role in OA research and make it possible to investigate both secondary osteoarthritic changes due to a precedent event such as traumatic injury and naturally occurring changes for the development of therapeutics which can be tested in preclinical and clinical OA trials. We induced OA in various animal models including rats, rabbits and guinea pigs by chemical, surgical and naturally occurring methods. In particular, the Dunkin-Hartley guinea pig is very attractive as an OA animal model because OA slowly progresses which is similar to human primary OA. Thus, this animal model mimics the pathophysiological process and environment of human primary OA. Besides the spontaneous OA model, anterior cruciate ligament transection (ACLT) with medial meniscectomy and bilateral ovariectomy (OVX) as well as a chemical technique using sodium monoiodoacetate (MIA) were used to induce OA. We found that ACLT in the rat model induced OA changes in the histology and micro-CT image compared to OVX. The osteoarthritic change significantly increased following ACLT surgery in the rabbit model. Furthermore, we identified that OA pathogenic changes occurred in a time-dependent manner in spontaneous Dunkin-Hartley guinea pigs. The MIA injection model is a rapid and minimally invasive method for inducing OA in animal models, whereas the spontaneous OA model has a slow and gradual progression of OA similar to human primary OA. We observed that histological OA change was extraordinarily increased at 9 ½ months in the spontaneous OA model, and thus, the grade was similar with that of the MIA model. Therefore, this study reports on OA pathology using various animal models as well as the spontaneous results naturally occurring in an OA animal model which had developed cartilage lesions and progressive osteoarthritic changes.

摘要

骨关节炎(OA)的特征是关节软骨进行性丧失、软骨下骨硬化和滑膜炎症,是当今全球最常见的慢性疾病。然而,大多数治疗方法都集中在缓解疼痛和 OA 症状上。基于这些原因,许多正在进行的研究目前正试图根据 OA 的病理学开发有效的治疗方法。模拟 OA 组织病理学和症状的动物模型在 OA 研究中具有重要作用,使我们能够研究由于创伤等先前事件引起的继发性骨关节炎变化,以及自然发生的变化,从而开发出可在临床前和临床 OA 试验中进行测试的治疗方法。我们通过化学、手术和自然发生的方法在各种动物模型中诱导 OA,包括大鼠、兔子和豚鼠。特别是,Dunkin-Hartley 豚鼠作为 OA 动物模型非常有吸引力,因为 OA 进展缓慢,类似于人类原发性 OA。因此,这种动物模型模拟了人类原发性 OA 的病理生理过程和环境。除了自发性 OA 模型,前交叉韧带切断(ACLT)伴内侧半月板切除术和双侧卵巢切除术(OVX)以及使用单碘乙酸钠(MIA)的化学技术也被用于诱导 OA。我们发现,与 OVX 相比,大鼠模型中的 ACLT 诱导了组织学和 micro-CT 图像的 OA 变化。兔模型中的 ACLT 手术后,骨关节炎变化显著增加。此外,我们确定 OA 发病变化在自发性 Dunkin-Hartley 豚鼠中呈时间依赖性发生。MIA 注射模型是一种在动物模型中快速且微创的诱导 OA 的方法,而自发性 OA 模型具有类似于人类原发性 OA 的缓慢而渐进的 OA 进展。我们观察到,在自发性 OA 模型中,9 个半月时 OA 组织学变化显著增加,因此其等级与 MIA 模型相似。因此,本研究报告了使用各种动物模型以及在发生软骨损伤和进行性骨关节炎变化的 OA 动物模型中自然发生的自发性结果的 OA 病理学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b169/5849317/c211d300abcc/pone.0194288.g001.jpg

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