Effective Technical Protocol for Producing a Mono-Iodoacetate-Induced Temporomandibular Joint Osteoarthritis in a Rat Model.

IF 2.7 4区医学 Q3 CELL & TISSUE ENGINEERING

Tissue engineering. Part C, Methods Pub Date : 2023-09-01 Epub Date: 2023-07-26 DOI:10.1089/ten.TEC.2023.0066

So-Yeon Yun, Yerin Kim, Hyunjeong Kim, Bu-Kyu Lee

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Abstract

An animal model of osteoarthritis (OA) induced by monosodium iodoacetate (MIA) can be effectively adjusted based on the concentration of MIA to control the onset, progression, and severity of OA as required. The rat temporomandibular joint osteoarthritis (TMJOA) model using MIA is a useful tool for studying the effectiveness of disease-modifying OA drugs in TMJOA research. However, the intricate and complex anatomy of the rat TMJ often poses challenges in achieving consistent TMJOA induction during experiments. In the previous article, a reference point was established by drawing parallel lines based on the line connecting the external ear and the zygomatic arch. However, this is not suitable for the anatomical characteristics of the rat. We used the zygomatic arch as a reference, which is a technical protocol that considers it. In our protocol, we designated a point ∼1 mm away from the point where the zygomatic arch bends toward the ear as the injection site. To ensure precise injection of MIA and increase the likelihood of inducing OA, it is recommended to insert the needle at a 45° angle so that the needle tip contacts the joint projection. To confirm TMJOA induction, we identified changes in the condyle using in vivo microcomputed tomography (CT) in a rat model of MIA-induced OA and measured the degree of pain-related inflammation using head withdrawal threshold (HWT) measurements. Micro-CT scanning revealed typical OA-like lesions, including degenerative changes and subchondral bone remodeling induced by MIA in the TMJ. Pain, a major clinical feature of OA, showed an appropriate response corresponding to the structural changes shown in micro-CT scanning. In addition, the MIA concentration suitable for long-term observation of lesions was determined through ex vivo micro-CT imaging and HWT measurements. The 8 mg concentration exhibited a significant difference compared with others, confirming the sustained presence of lesions, particularly through changes in subchondral bone over an extended period. Consequently, we have successfully established a reliable rat TMJOA induction model and identified the MIA concentration suitable for long-term observation of subchondral bone research, which will greatly contribute to the study of TMJOA-an incurable disease lacking specific treatment options. The Clinical Trial Registration number is 2021-12-208.

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在大鼠模型中产生碘乙酸单酯诱导的颞下颌关节骨关节炎的有效技术方案。

碘乙酸单钠（MIA）诱导的骨关节炎（OA）动物模型可以根据MIA的浓度进行有效调整，以根据需要控制OA的发作、进展和严重程度。使用MIA的大鼠颞下颌关节骨性关节炎（TMJOA）模型是研究TMJOA研究中疾病修饰OA药物有效性的有用工具。然而，大鼠颞下颌关节复杂而复杂的解剖结构往往对在实验中实现一致的TMJOA诱导提出挑战。在上一篇文章中，通过在连接外耳和颧骨弓的线的基础上绘制平行线来建立参考点。然而，这不适合大鼠的解剖特征。我们使用颧骨弓作为参考，这是一个考虑它的技术协议。在我们的协议中，我们指定了一个点～1 距离作为注射部位的颧骨弓向耳朵弯曲的点1mm。为了确保精确注射MIA并增加诱发OA的可能性，建议以45°角插入针头，使针尖接触关节突起。为了证实TMJOA的诱导，我们在MIA诱导的OA大鼠模型中使用体内微计算机断层扫描（CT）确定了髁突的变化，并使用头部退缩阈值（HWT）测量测量了疼痛相关炎症的程度。显微CT扫描显示典型的OA样病变，包括TMJ中MIA诱导的退行性变化和软骨下骨重塑。疼痛是OA的一个主要临床特征，在微CT扫描中显示出与结构变化相对应的适当反应。此外，通过离体显微CT成像和HWT测量确定了适合长期观察病变的MIA浓度。8 mg浓度与其他浓度相比表现出显著差异，证实了病变的持续存在，特别是通过软骨下骨的长期变化。因此，我们成功地建立了可靠的大鼠TMJOA诱导模型，并确定了适合软骨下骨研究长期观察的MIA浓度，这将大大有助于TMJOA的研究，TMJOA是一种缺乏特定治疗选择的不治之症。临床试验注册号为2021-12-208。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Tissue engineering. Part C, Methods Medicine-Medicine (miscellaneous)

CiteScore

5.10

自引率

3.30%

发文量

136

期刊介绍： Tissue Engineering is the preeminent, biomedical journal advancing the field with cutting-edge research and applications that repair or regenerate portions or whole tissues. This multidisciplinary journal brings together the principles of engineering and life sciences in the creation of artificial tissues and regenerative medicine. Tissue Engineering is divided into three parts, providing a central forum for groundbreaking scientific research and developments of clinical applications from leading experts in the field that will enable the functional replacement of tissues. Tissue Engineering Methods (Part C) presents innovative tools and assays in scaffold development, stem cells and biologically active molecules to advance the field and to support clinical translation. Part C publishes monthly.