The effects of prophylactic tadalafil use on VEGF expression in the rabbit model of steroid-induced femoral head avascular necrosis.

Emre Özmen, Hazal İzol Özmen, Sezen Atasoy, Menduh Dursun, Bilge Bilgiç, Ahmet Salduz
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Abstract

Objective: The purpose of this study was to examine the effect of prophylactic tadalafil use on a steroid-induced femoral head avascular necrosis model in terms of microscopic, imaging, and molecular biological changes.

Methods: Twenty-four New Zealand rabbits were divided into 3 equal groups. Eight rabbits were designated as the control group and did not receive treatment. Rabbits in group 1 (G1) received 0.1 mg/kg Escherichia coli lipopolysaccharide (LPS) intravenously and 40 mg/ kg methylprednisolone sodium succinate (MP) was administered intramuscularly for 3 days consecutively. Rabbits in group 2 (G2) were given 5 mg/kg tadalafil orally for 10 consecutive days. Starting on the eighth day, 0.1 mg/kg LPS was given, and following this 40 mg/kg MP injections were administered for 3 days. All animals were sacrificed 3 weeks after the final MP injection. Magnetic resonance imaging was performed, and bilateral femora were harvested. Half of the femoral head was stored for Vascular Endothelial Growth Factor (VEGF) examination with Western blot analysis. The other half was examined microscopically for the presence of osteonecrosis.

Results: In G1, 15 out of 16 hips (93%) of the 8 rabbits had osteonecrosis compared to 8 out of 12 hips (67%) of 6 rabbits in G2 (P > .05). The VEGF expression in G2 was significantly higher than in the control group and G1 (P < .05 and P < .001, respectively). There was no significant difference in VEGF expression between the control group and G1 (P > .05).

Conclusion: This study has shown us that femoral head osteonecrosis can be reliably induced with LPS and corticosteroid, as described in the literature. Prophylactic tadalafil use did not decrease the occurrence of osteonecrosis significantly. However, it significantly increased VEGF expression in the femoral head independent of the effects of steroids and LPS.

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在激素诱导的兔股骨头缺血性坏死模型中,预防性使用他达拉非对VEGF表达的影响。
目的:本研究的目的是从微观、影像学和分子生物学变化方面检查预防性使用他达拉非对类固醇诱导的股骨头缺血性坏死模型的影响。方法:将24只新西兰兔随机分为3组。8只兔子被指定为对照组,并且不接受治疗。第1组(G1)兔静脉注射0.1mg/kg大肠杆菌脂多糖(LPS),肌肉注射40mg/kg甲基强的松龙琥珀酸钠(MP),连续3天。第2组(G2)的兔子口服5mg/kg他达拉非,连续10天。从第八天开始,给予0.1mg/kg LPS,随后给予40mg/kg MP注射3天。在最后一次MP注射后3周处死所有动物。进行了磁共振成像,并采集了双侧股骨。将一半股骨头储存起来,用蛋白质印迹分析进行血管内皮生长因子(VEGF)检查。另一半用显微镜检查是否存在骨坏死。结果:在G1期,8只兔的16个髋关节中有15个(93%)发生骨坏死,而在G2期,6只兔的12个髋关节(67%)中有8个发生骨坏死(P>.05)。G2期VEGF的表达显著高于对照组和G1期(分别为P<.05和P<.001)。对照组和G1组之间VEGF的表达没有显著差异(P>0.05)。结论:本研究表明,如文献所述,LPS和皮质类固醇可以可靠地诱导股骨头坏死。预防性使用他达拉非并不能显著减少骨坏死的发生。然而,它显著增加了股骨头中VEGF的表达,与类固醇和LPS的作用无关。
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