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大孔载锶干凝胶支架对去卵巢大鼠临界尺寸干骺端骨折缺损处新骨形成的影响。

Effects of macroporous, strontium loaded xerogel-scaffolds on new bone formation in critical-size metaphyseal fracture defects in ovariectomized rats.

作者信息

Ray Seemun, Thormann Ulrich, Sommer Ursula, Khassawna Thaqif El, Hundgeburth Marvin, Henß Anja, Rohnke Marcus, Lips Katrin S, Heiss Christian, Heinemann Sascha, Hanke Thomas, Dürselen Lutz, Schnettler Reinhard, Alt Volker

机构信息

Laboratory of Experimental Trauma Surgery, Justus-Liebig-University, Giessen, Germany.

Laboratory of Experimental Trauma Surgery, Justus-Liebig-University, Giessen, Germany; Department of Trauma Surgery, University Hospital Giessen-Marburg GmbH, Campus Giessen, Germany.

出版信息

Injury. 2016 Jan;47 Suppl 1:S52-61. doi: 10.1016/S0020-1383(16)30013-4.

Abstract

New bone formation was studied in a metaphyseal fracture-defect in ovariectomized rats stimulated by a plain and a strontium-enriched macroporous silica/collagen scaffold (ScB30 and ScB30Sr20) and a compact silica/collagen xerogel (B30). 45 female Sprague-Dawley rats were randomly assigned to three different treatment groups: (1) ScB30 (n=15), (2) ScB30Sr20 (n=15), and (3) B30 (n=15). 12 weeks after bilateral ovariectomy and multi-deficient diet, a 4 mm wedge-shaped fracture-defect was created at the metaphyseal area of the left femur. A 7-hole T-shaped plate at the lateral aspect of the femur stabilized the bone and the defect was filled with ScB30, ScB30Sr20 or B30 subsequently. After six weeks, histomorphometrical analysis revealed a statistically significant higher bone volume/tissue volume ratio in the ScB30Sr20 group compared to ScB30 (p=0.043) and B30 (p=0.0001) indicating an improved formation of new bone by the strontium-enriched macroporous silica/collagen scaffold. Furthermore, immunohistochemical results showed increased expression of BMP2 and OPG and a decreased RANKL expression in the ScB30Sr20 group. This was further confirmed with the gene expression analysis where an increase in prominent bone formation markers (ALP, OCN, Runx2, Col1a1 and Col10a1) was seen. No material remnants were found in the scaffold group indicating an almost complete degradation process of the biomaterials. This is confirmed by ToF-SIMS analysis that did not detect any strontium in the ScB30Sr20 group neither in the defect nor in the surrounding tissue. Taken together, this study shows the stimulating effects of strontium through increased bone formation by up regulation of osteoanabolic markers. This work also indicates the importance of material porosity, geometry and biodegradability in bone healing.

摘要

研究了普通和富锶大孔二氧化硅/胶原蛋白支架(ScB30和ScB30Sr20)以及致密二氧化硅/胶原蛋白干凝胶(B30)对去卵巢大鼠干骺端骨折缺损处新骨形成的影响。45只雌性Sprague-Dawley大鼠随机分为三个不同的治疗组:(1)ScB30组(n = 15),(2)ScB30Sr20组(n = 15),(3)B30组(n = 15)。双侧卵巢切除并给予多缺乏饮食12周后,在左股骨干骺端区域制造一个4毫米的楔形骨折缺损。股骨外侧的一块7孔T形钢板固定骨骼,随后缺损处分别用ScB30、ScB30Sr20或B30填充。六周后,组织形态计量学分析显示,与ScB30组(p = 0.043)和B30组(p = 0.0001)相比,ScB30Sr20组的骨体积/组织体积比具有统计学意义的显著升高,表明富锶大孔二氧化硅/胶原蛋白支架促进了新骨形成。此外,免疫组化结果显示ScB30Sr20组中BMP2和OPG表达增加,RANKL表达降低。基因表达分析进一步证实了这一点,其中可见显著的骨形成标志物(ALP、OCN、Runx2、Col1a1和Col10a1)增加。支架组未发现材料残留,表明生物材料几乎完全降解。飞行时间二次离子质谱分析证实了这一点,该分析在ScB30Sr20组的缺损处和周围组织中均未检测到任何锶。综上所述,本研究表明锶通过上调骨合成代谢标志物增加骨形成具有刺激作用。这项工作还表明了材料孔隙率、几何形状和生物降解性在骨愈合中的重要性。

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