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首页> 外文期刊>Circulation journal >Transient Increase of Cytokines in the Acute Ischemic Tissue is Beneficial to Cell-Based Therapeutic Angiogenesis
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Transient Increase of Cytokines in the Acute Ischemic Tissue is Beneficial to Cell-Based Therapeutic Angiogenesis

机译:急性缺血组织中细胞因子的短暂增加有益于基于细胞的治疗性血管生成

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摘要

Background Implantation of bone marrow cells (BMCs) is a treatment of ischemic disease. It is well known that many inflammatory cytokines are released in ischemic tissue, especially in the acute phase, so in the present study it was investigated if the transient increase of cytokines in the acute ischemic tissue influences cell-based therapeutic angiogenesis.Methods and Results Ischemic limb models were created in C57BL/6 mice as 24 h (acute) or 2 weeks (chronic) after ischemia. BMCs were cultured with total tissue protein, which was extracted from the acute and chronic ischemic muscles. The survival, adhesion, and migration of BMCs were significantly better after culture with 1 mg/ml total tissue protein extracted from the acute ischemic limbs than from the chronic ischemic limbs (p<0.001). For the in-vivo study, 8 x 10~6 BMCs, collected from green fluorescent protein (GFP) transgenic mice, were implanted into the acute or chronic ischemic limbs of the mice. The survival of implanted cells and blood flow were significantly better when BMCs were implanted into the acute ischemic limbs than into the chronic ischemic limbs (p<0.001).Conclusions A transient increase of cytokines in the acute ischemic tissue is beneficial for cell-based therapeutic angiogenesis.
机译:背景技术骨髓细胞(BMC)的植入是缺血性疾病的一种治疗方法。众所周知,缺血组织尤其是急性期释放出许多炎性细胞因子,因此在本研究中,研究了急性缺血组织中细胞因子的瞬时增加是否会影响基于细胞的治疗性血管生成。在缺血后24小时(急性)或2周(慢性),在C57BL / 6小鼠中创建肢体模型。用总组织蛋白培养BMC,该组织蛋白是从急性和慢性缺血性肌肉中提取的。用1 mg / ml从急性缺血性肢体提取的总组织蛋白培养后,BMC的存活,粘附和迁移明显优于从慢性缺血性肢体提取的细菌(p <0.001)。为了进行体内研究,将从绿色荧光蛋白(GFP)转基因小鼠中收集的8 x 10〜6 BMC植入到小鼠的急性或慢性缺血肢体中。当将BMC植入急性缺血肢体中时,植入细胞的存活率和血流显着好于慢性缺血肢体中(p <0.001)。结论急性缺血组织中细胞因子的短暂增加有利于基于细胞的治疗血管生成。

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