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采用有限元方法评估伴有肿瘤性骨缺损的胫骨近端骨折风险。

Assessment of fracture risk in proximal tibia with tumorous bone defects by a finite element method.

作者信息

Lin Yulin, Ma Limin, Zhu Ye, Lin Zefeng, Yao Zilong, Zhang Yu, Mao Chuanbin

机构信息

Southern Medical University Graduate School, Baiyun District, Guangzhou, 510515, China.

Department of Orthopedics, Guangdong Key Lab of Orthopaedic Technology and Implant, Guangzhou General Hospital of Guangzhou Military Command, Guangzhou, 510010, China.

出版信息

Microsc Res Tech. 2017 Sep;80(9):975-984. doi: 10.1002/jemt.22899. Epub 2017 May 27.

Abstract

There has not been a satisfying method to predict the fracture risk in tumorous bone lesions. To tackle this challenge, we used a finite element method to assess the fracture risk in the proximal tibia (pT) when the size and location of the tumorous defects are varied in bone. Towards this end, the circular cortical defects, mimicking the tumorous lesions by forming cortical window defects, with a diameter (Ф) of 20, 30, 40, or 50 mm, are structured on the anteromedial, lateral, posterior wall of pT, which is located 5, 15, and 25 mm below articular margin, respectively. We found that under walking conditions, the Von Mises Stress of each defective tibia model was larger than that of the intact tibia model and also showed a positive linear correlation with the sizes of the defects. A notable fracture risk was not observed until the defect was Ф30 mm or larger. When the defect emerged, the anteromedial wall resisted fracture risk more than the rest of wall. Our results show that the size and location of the bone tumors are important factors affecting the fracture risk of pT. Our findings will be beneficial to clinicians when deciding what treatment to use for pT lesions.

摘要

目前还没有一种令人满意的方法来预测骨肿瘤性病变的骨折风险。为应对这一挑战,我们采用有限元方法,在骨中肿瘤性缺损的大小和位置发生变化时,评估胫骨近端(pT)的骨折风险。为此,通过形成皮质窗缺损来模拟肿瘤性病变的圆形皮质缺损,其直径(Ф)为20、30、40或50毫米,分别构建在pT的前内侧、外侧、后壁上,这些位置分别位于关节边缘下方5、15和25毫米处。我们发现,在行走条件下,每个缺损胫骨模型的冯·米塞斯应力均大于完整胫骨模型,并且与缺损大小呈正线性相关。直到缺损达到Ф30毫米或更大时,才观察到明显的骨折风险。当出现缺损时,前内侧壁比其他壁更能抵抗骨折风险。我们的结果表明,骨肿瘤的大小和位置是影响pT骨折风险的重要因素。我们的发现将有助于临床医生决定对pT病变采用何种治疗方法。

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