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Endothelial cells enhance tumor cell invasion through a crosstalk mediated by CXC chemokine signaling.内皮细胞通过CXC趋化因子信号介导的相互作用增强肿瘤细胞的侵袭。
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In vitro wounding: effects of hypoxia and transforming growth factor beta1 on proliferation, migration and myofibroblastic differentiation in an endothelial cell-fibroblast co-culture model.体外创伤:缺氧和转化生长因子β1对内皮细胞-成纤维细胞共培养模型中细胞增殖、迁移及肌成纤维细胞分化的影响
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4
Adenoviral transfer of rho family proteins to lung cancer cells ameliorates cell proliferation and motility and increases apoptotic change.将rho家族蛋白通过腺病毒载体导入肺癌细胞可改善细胞增殖和运动能力,并增加凋亡变化。
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Physiological roles of PKB/Akt isoforms in development and disease.蛋白激酶B/Akt亚型在发育和疾病中的生理作用。
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Akt1 in endothelial cell and angiogenesis.内皮细胞中的Akt1与血管生成
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Akt1/蛋白激酶Bα参与肿瘤条件培养基诱导的内皮细胞体外迁移和存活

Involvement of Akt1/protein kinase Balpha in tumor conditioned medium-induced endothelial cell migration and survival in vitro.

作者信息

Tu Ming Li, Wang Han Qin, Chen Long Ju, Lu Jin Chang, Jiang Fei, Liang Jiang Hong, Xu Da Guo, Li Dong Sheng

机构信息

Department of Respiratory Medicine, Yunyang Medical College, Taihe Hospital, Hubei, China.

出版信息

J Cancer Res Clin Oncol. 2009 Nov;135(11):1543-50. doi: 10.1007/s00432-009-0601-9. Epub 2009 Jun 2.

DOI:10.1007/s00432-009-0601-9
PMID:19488783
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12160271/
Abstract

PURPOSE

Endothelial cell migration and survival might be called "major angiogenic responses". Tumor conditioned medium (CM) has been widely used to stimulate endothelial cells to form capillary-like structures in angiogenesis models in vitro. However, the molecular events triggered by tumor CM are not fully understood. Here, we examined the effects of the CM from human lung carcinoma cell lines A549 and SPC-A-1 on cultures of primary human umbilical veins endothelial cells (HUVECs).

METHODS

After treatment of HUVECs with the CM, cell migration was assessed by wound-healing assay, cell viability was evaluated by XTT assay, and apoptosis and cell death of HUVECs was analyzed by flow cytometry. Phosphorylation of Akt was assessed by Western blotting. To dissect the direct role of Akt, small interfering RNA (siRNA) against Akt1 was used.

RESULTS

Both A549 and SPC-A-1 CM significantly stimulated cell migration. However, only A549 CM promoted cell viability and inhibited low serum-induced apoptosis and cell death of HUVECs, but SPC-A-1-CM showed no effects on survival of HUVECs. Meanwhile, A549 CM was found to be able to induce much more phosphorylation of Akt compared to SPC-A-1 CM treated group. The inhibitor of PI3K (wortmaninn) or Akt1 siRNA blocked A549 CM-induced migration and survival of HUVECs.

CONCLUSION

These results indicated that the angiogenic effects of A549 CM are largely mediated through activation of the PI3K-Akt in endothelial cells, and that the Akt1 is crucial in this process, which may provide a therapeutic target for decreasing tumor angiogenesis.

摘要

目的

内皮细胞迁移和存活可被称为“主要的血管生成反应”。肿瘤条件培养基(CM)已被广泛用于在体外血管生成模型中刺激内皮细胞形成毛细血管样结构。然而,肿瘤CM引发的分子事件尚未完全了解。在此,我们研究了人肺癌细胞系A549和SPC-A-1的CM对原代人脐静脉内皮细胞(HUVECs)培养物的影响。

方法

用CM处理HUVECs后,通过伤口愈合试验评估细胞迁移,通过XTT试验评估细胞活力,并通过流式细胞术分析HUVECs的凋亡和细胞死亡。通过蛋白质印迹法评估Akt的磷酸化。为了剖析Akt的直接作用,使用了针对Akt1的小干扰RNA(siRNA)。

结果

A549和SPC-A-1的CM均显著刺激细胞迁移。然而,只有A549的CM促进细胞活力并抑制低血清诱导的HUVECs凋亡和细胞死亡,而SPC-A-1的CM对HUVECs的存活没有影响。同时,发现与SPC-A-1 CM处理组相比,A549的CM能够诱导更多的Akt磷酸化。PI3K抑制剂(渥曼青霉素)或Akt1 siRNA可阻断A549的CM诱导的HUVECs迁移和存活。

结论

这些结果表明,A549的CM的血管生成作用很大程度上是通过激活内皮细胞中的PI3K-Akt介导的,并且Akt1在这一过程中至关重要,这可能为减少肿瘤血管生成提供一个治疗靶点。