医学
腰椎
椎间盘
解剖
腰动脉
动物模型
尸体痉挛
内分泌学
作者
Long Zhang,Guicheng Du,Bogang Teng,Xueqing Shi,Xuemei He,Na Li,Yu Chen,Ren Xu
标识
DOI:10.1016/j.bbrc.2022.10.022
摘要
Intervertebral disc degeneration (IDD) may be the primary cause of low back pain. Potential therapeutics for IDD must be validated in animal models, and their effectiveness quantified using functional metrics. Needle puncture of intervertebral discs (IVDs) has been used to induce IDD in mice and rats. Due to operational challenges, most animal IDD models are constructed using needle puncture of the caudal IVDs in mice, or by using larger animals, such as rats and rabbits. However, mouse IDD models involving lumbar IVD puncture are preferable because mice are genetically similar to humans and are the most commonly used transgenic animals, and because human IDD commonly affects the lumbar spine. We constructed a needle puncture-based mouse IDD model that relies on vascular anatomy to pinpoint lumbar IVDs. We evaluated the morphological and molecular changes in this model by using radiological, pathological, and immunostaining examinations. In our mechanical injury-induced IDD model, lumbar IVDs were accurately localized by injecting colored perfusates into the common iliac artery and vein, and right iliolumbar vein, which helped to visualize puncture positions, avoid neuromuscular injury, shorten the operation time, and decrease bleeding. Nucleus pulposus cells, defined by Krt19, and the disc height index gradually decreased after the surgery, and the degenerative effects peaked at 1 week. In conclusion, we established a mouse IDD model by performing precise puncture of lumbar IVDs via the ventral anterior approach assisted by vessel position. Our model effectively simulated the effects of IDD, and may serve as an efficient research tool. • We established a mouse intervertebral disc degeneration model by performing precise puncture of lumbar intervertebral discs. • The intervertebral disc degeneration model was processed via the ventral anterior approach which have reduced modeling complications. • We used vascular dye perfusion, and identified the positions of different discs based on the locations of signature vessels for clear localization of the common iliac artery and vein.
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