首页> 外文期刊>Clinical and experimental pharmacology & physiology >Effects of vascular endothelial growth factor (VEGF)A and VEGFB gene transfer on vascular reserve in a conscious rabbit hindlimb ischaemia model.
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Effects of vascular endothelial growth factor (VEGF)A and VEGFB gene transfer on vascular reserve in a conscious rabbit hindlimb ischaemia model.

机译:血管内皮生长因子(VEGF)A和VEGFB基因转移对清醒家兔后肢缺血模型中血管储备的影响。

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1. As a result of the ageing population, there are increasing numbers of patients with severe peripheral vascular occlusive disease associated with intermittent claudication (pain on walking) and decreased exercise tolerance. There is a great clinical need for pharmacological treatments that may stimulate collateral blood vessel growth, increase vascularity and improve skeletal muscle function. 2. Therapeutic angiogenesis using growth factors such as vascular endothelial growth factor (VEGF) has been used to improve collateral artery development in myocardial or skeletal muscle ischaemia. The broad aims of the work briefly summarized here were to compare the effects of VEGFA165 and VEGFB167 (500 micro g, i.m., gene transfer) on calf blood pressure ratio and reactive hyperaemia in a chronic rabbit preparation with unilateral limb ischaemia. 3. Unilateral femoral artery ligation caused an immediate deficit (compared with the contralateral limb) of 72% in calf systolic blood pressure. There were improvements 14 days after ligation with VEGFA and VEGFB treatments compared with the vehicle control plasmid treatment, but a deficit remained of some 32%. 4. Reactive hyperaemic responses were significantly attenuated 7 days after ligation in the vehicle and VEGFA treatment groups. On day 14, this loss of vascular reserve was restored in the VEGFA group, but remained in the vehicle group (-30%). In VEGFB-treated animals, there was no deficit in reserve 7-14 days post-ligation. 5. In conclusion, there is considerable value in the serial measurements of calf blood pressure ratio and reactive hyperaemia in the rabbit unilateral hindlimb ischaemia model. Gene transfer of either VEGFA or VEGFB allowed significant improvements in these indices compared with vehicle but, at 14 days post-ligation, large deficits still remained. Studies extending this experimental period are in progress.
机译:1.由于人口老龄化,伴有间歇性lau行(行走时疼痛)和运动耐力下降的严重外周血管闭塞性疾病的患者数量不断增加。临床上对药物治疗的需求很大,可能会刺激侧支血管生长,增加血管分布并改善骨骼肌功能。 2.使用诸如血管内皮生长因子(VEGF)的生长因子的治疗性血管生成已被用于改善心肌或骨骼肌缺血中的侧支动脉发育。本文简要概述的工作的广泛目标是比较VEGFA165和VEGFB167(500微克,即基因转移)对慢性兔单侧肢体缺血的小腿血压比和反应性充血的影响。 3.单侧股动脉结扎导致小腿收缩压立即下降(与对侧肢体相比)为72%。与媒介物对照质粒处理相比,与VEGFA和VEGFB处理连接后14天有改善,但仍存在约32%的缺陷。 4.在媒介物和VEGFA治疗组中,结扎后7天反应性充血反应明显减弱。在第14天,血管储备的这种损失在VEGFA组中得以恢复,但在媒介物组中仍然存在(-30%)。在VEGFB治疗的动物中,结扎后7-14天没有储备不足。 5.总之,在兔单侧后肢缺血模型中,小腿血压比和反应性充血的连续测量具有相当大的价值。与赋形剂相比,VEGFA或VEGFB的基因转移可以使这些指标得到显着改善,但结扎后14天仍存在大量缺陷。延长该实验期的研究正在进行中。

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