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Optimization of a rat lumbar IVD degeneration model for low back pain

变性(医学) 医学 椎间盘 腰痛 H&E染色 腰椎 组织学 病理 免疫组织化学 外科 替代医学
作者
Juliane D. Glaeser,Wafa Tawackoli,Derek G. Ju,Jae Hyuk Yang,Linda E.A. Kanim,Khosrowdad Salehi,Victoria Yu,Evan Saidara,Jean‐Phillipe Vit,Zhanna Khnkoyan,Zachary NaPier,Laura S. Stone,Hyun W. Bae,Dmitriy Sheyn
出处
期刊:JOR spine [Wiley]
卷期号:3 (2) 被引量:30
标识
DOI:10.1002/jsp2.1092
摘要

Abstract Introduction Intervertebral disc (IVD) degeneration is often associated with low back pain and radiating leg pain. The purpose of this study is to develop a reproducible and standardized preclinical model of painful lumbar IVD degeneration by evaluation of structural and behavioral changes in response to IVD injury with increasing needle sizes. This model can be used to develop new therapies for IVD degeneration. Methods Forty‐five female Sprague Dawley rats underwent anterior lumbar disc needle puncture at levels L4‐5 and L5‐6 under fluoroscopic guidance. Animals were randomly assigned to four different experimental groups: needle sizes of 18 Gauge (G), 21G, 23G, and sham control. To monitor the progression of IVD degeneration and pain, the following methods were employed: μMRI, qRT‐PCR, histology, and biobehavioral analysis. Results T1‐ and T2‐weighted μMRI analysis showed a correlation between the degree of IVD degeneration and needle diameter, with the most severe degeneration in the 18G group. mRNA expression of markers for IVD degeneration markers were dysregulated in the 18G and 21G groups, while pro‐nociceptive markers were increased in the 18G group only. Hematoxylin and Eosin (H&E) and Alcian Blue/Picrosirius Red staining confirmed the most pronounced IVD degeneration in the 18G group. Randall‐Selitto and von Frey tests showed increased hindpaw sensitivity in the 18G group. Conclusion Our findings demonstrate that anterior disc injury with an 18G needle creates severe IVD degeneration and mechanical hypersensitivity, while the 21G needle results in moderate degeneration with no increased pain sensitivity. Therefore, needle sizes should be selected depending on the desired phenotype for the pre‐clinical model.
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