首页> 外文期刊>Hypertension: An Official Journal of the American Heart Association >Targeted Delivery of Carbaprostacyclin to Ischemic Hindlimbs Enhances Adaptive Remodeling of the Microvascular NetworkNovelty and Significance
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Targeted Delivery of Carbaprostacyclin to Ischemic Hindlimbs Enhances Adaptive Remodeling of the Microvascular NetworkNovelty and Significance

机译:将碳前列环素靶向递送至缺血性后肢可增强微血管网络的适应性改造的意义和意义

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摘要

Prostacyclin and its stable analogs play an important vascular protective role by promoting angiogenesis, but their role in arteriolar growth is unclear. Here, we examined the effect of prostacyclin stable analog carbaprostacyclin on arteriolar growth in mouse hindlimb ischemia. Using an osmotic-controlled release system to continuously deliver carbaprostacyclin or saline (control) to ischemic mouse hindlimbs for up to 14 days, we found that blood perfusion was significantly better at 7 and 14 days in carbaprostacyclin-treated mice than in saline-treated mice. Microscopic examination of the microvasculature showed more morphological signs of arteriolar formation in carbaprostacyclin- versus saline-treated legs. A double-blind, quantitative microcomputed tomography analysis indicated that carbaprostacyclin-treated legs had markedly increased vascular volume and small- to medium-sized vessel numbers that correspond to decreased vessel separation. A proteome profiler antibody array demonstrated that carbaprostacyclin-treated ischemic muscles secreted significantly higher amounts of acidic fibroblast growth factor and other chemokines. Conditioned media containing those secreted factors promoted smooth muscle cell growth and migration. Additionally, increased acidic fibroblast growth factor protein levels were detected in smooth muscle cells and skeletal myotubes at different time periods after carbaprostacyclin treatment. Furthermore, the selective peroxisome proliferation-activated receptor β/δ antagonist significantly suppressed carbaprostacyclin-induced acidic fibroblast growth factor protein production. Collectively, our data provide the first morphological and molecular evidence that local delivery of carbaprostacyclin promotes vascular growth in hindlimb ischemia, and that peroxisome proliferation-activated receptor β/δ signaling plays a critical role in inducing acidic fibroblast growth factor expression.
机译:前列环素及其稳定的类似物通过促进血管生成发挥重要的血管保护作用,但它们在小动脉生长中的作用尚不清楚。在这里,我们检查了稳定的前列环素类似物碳前列环素对小鼠后肢缺血小动脉生长的影响。使用渗透控制释放系统将碳巴前列环素或生理盐水(对照)连续输送至缺血小鼠后肢长达14天,我们发现碳巴前列环素治疗的小鼠在7天和14天的血流灌注明显优于生理盐水治疗的小鼠。显微检查微脉管系统显示,在碳巴前环素治疗组和生理盐水治疗组的腿中,小动脉形成的形态学迹象更多。双盲,定量微计算机断层扫描分析表明,经前列环素处理的腿明显增加了血管体积,相应的中小血管数也相应减少了血管间隔。蛋白质组分析仪抗体阵列证明,用碳前列环素处理的缺血性肌肉分泌的酸性成纤维细胞生长因子和其他趋化因子的量明显更高。含有那些分泌因子的条件培养基促进了平滑肌细胞的生长和迁移。另外,在碳前列环素治疗后的不同时间段,平滑肌细胞和骨骼肌管中检测到酸性成纤维细胞生长因子蛋白水平升高。此外,选择性过氧化物酶体增殖激活受体β/δ拮抗剂显着抑制了碳环前环素诱导的酸性成纤维细胞生长因子蛋白的产生。总的来说,我们的数据提供了第一个形态学和分子证据,即碳前列环素的局部递送促进后肢缺血中的血管生长,并且过氧化物酶体增殖激活受体β/δ信号传导在诱导酸性成纤维细胞生长因子表达中起关键作用。

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