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首页> 外文期刊>Journal of vascular and interventional radiology: JVIR >Challenging the surgical rodent hindlimb ischemia model with the miniinterventional technique.
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Challenging the surgical rodent hindlimb ischemia model with the miniinterventional technique.

机译:用微型介入技术挑战鼠类后肢缺血模型。

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摘要

PURPOSE: To develop an interventional hindlimb ischemic model and compare its angiogenic effect versus surgical ligation (SL) and excision of the femoral artery in rats treated with transplantation of bone marrow mononuclear cells (MNCs) as an angiogenic stimulator. MATERIALS AND METHODS: Forty-eight Lewis rats randomly received interventional embolization (IE) with hydrogel wire or SL and excision of the right femoral artery. Rodents were intraarterially transplanted with 1.5 x 10(7) MNCs in 500 muL medium from 24 isogenic donor rats. Functional and structural recovery was evaluated by laser Doppler imaging (LDI), cytokine/chemokine assay, and histologic staining. RESULTS: In vivo microscopic images showed significantly dilated vasa vasorum around the embolized segment of the right femoral artery at 3 days compared with disorganized tissue structure in the SL group. However, the LDI index was significantly higher in the SL group at 3 days compared with the IE group. LDI did not significantly differ between the two groups at 2 weeks after transplantation. Cytokine assay showed higher levels of interleukin (IL)-1alpha and IL-18 in the SL group; the IE group had higher levels of interferon-gamma, IL-6, IL-13, and granulocyte colony-stimulating factor. Histologic examination demonstrated inflammatory infiltration near the incision within nerve fibers with dilated capillaries, showing nerve degeneration in the SL group. At 2 weeks, histologic analysis demonstrated massive scarring under the skin spreading into the musculature in the SL group. CONCLUSIONS: A minimally invasive hindlimb ischemia model has been successfully developed that preserves tissue integrity and minimizes inflammation and confounding factors in the early stages of angiogenesis and arteriogenesis.
机译:目的:建立一种干预性后肢缺血模型,并比较其在以骨髓单个核细胞(MNC)作为血管生成刺激物移植治疗的大鼠中的手术结扎(SL)和股动脉切除的血管生成作用。材料与方法:48只Lewis大鼠随机接受水凝胶丝或SL介入性栓塞(IE)并切除右股动脉。将啮齿类动物用1.5 x 10(7)MNC动脉移植到来自24只等基因供体大鼠的500μL培养基中。通过激光多普勒成像(LDI),细胞因子/趋化因子测定和组织学染色评估功能和结构恢复。结果:与SL组相比,在体内显微图像显示,第3天右股动脉栓塞段周围的vasa血管明显扩张。但是,SL组在3天时的LDI指数明显高于IE组。两组在移植后2周时的LDI无明显差异。细胞因子检测显示SL组的白介素(IL)-1alpha和IL-18含量较高; IE组的干扰素-γ,IL-6,IL-13和粒细胞集落刺激因子水平较高。组织学检查显示,神经纤维内切口附近有炎性浸润,毛细血管扩张,显示SL组神经变性。在第2周,组织学分析显示SL组皮肤下的大量瘢痕扩散到肌肉组织中。结论:成功开发了一种微创后肢缺血模型,该模型可在血管生成和动脉生成的早期阶段保持组织完整性并使炎症和混杂因素降至最低。

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