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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Hypoxia-Inducible Factor-2{alpha} Regulates GM-CSF-Derived Soluble Vascular Endothelial Growth Factor Receptor 1 Production from Macrophages and Inhibits Tumor Growth and Angiogenesis.
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Hypoxia-Inducible Factor-2{alpha} Regulates GM-CSF-Derived Soluble Vascular Endothelial Growth Factor Receptor 1 Production from Macrophages and Inhibits Tumor Growth and Angiogenesis.

机译:缺氧诱导因子-2 {α}调节巨噬细胞衍生的GM-CSF衍生的可溶性血管内皮生长因子受体1的产生,并抑制肿瘤的生长和血管生成。

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摘要

Macrophage secretion of vascular endothelial growth factor (VEGF) in response to the hypoxic tumor microenvironment contributes to tumor growth, angiogenesis, and metastasis. We have recently demonstrated that macrophages stimulated with GM-CSF at low O(2) secrete high levels of a soluble form of the VEGF receptor 1 (sVEGFR-1), which neutralizes VEGF and inhibits its biological activity. Using small interfering RNA targeting to deplete hypoxia-inducible factor (HIF)-1alpha or HIF-2alpha in murine macrophages, we found that macrophage production of sVEGFR-1 in response to low O(2) was dependent on HIF-2alpha, whereas HIF-1alpha specifically regulated VEGF production. In our current report, we evaluated the growth of B16F10 malignant melanoma in mice with a monocyte/macrophage-selective deletion of HIF-1alpha or HIF-2alpha (HIF-1alpha(flox/flox)- or HIF-2alpha(flox/+)/LysMcre mice). GM-CSF treatment increased intratumoral VEGF and sVEGFR-1 in control mice, an effect that was associated with a decrease in microvessel density. GM-CSF treatment of HIF-1alpha(flox/flox)/LysMcre mice induced sVEGFR-1 but not VEGF, resulting in an overall greater reduction in tumor growth and angiogenesis compared with control mice. In addition, real-time PCR for melanoma-specific genes revealed a significantly reduced presence of lung micrometastases in HIF-1alpha(flox/flox)/LysMcre mice treated with GM-CSF. Conversely, GM-CSF treatment induced VEGF but not sVEGFR-1 in HIF-2alpha(flox/+)/LysMcre mice, and, correspondingly, GM-CSF did not decrease tumor growth, angiogenesis, or lung metastasis in these mice. This study reveals opposing roles for the HIFs in the regulation of angiogenesis by tumor-associated macrophages and suggests that administration of GM-CSF might be an effective means of inducing sVEGFR-1 and inhibiting tumor growth and angiogenesis in patients with melanoma.
机译:缺氧肿瘤微环境中血管内皮生长因子(VEGF)的巨噬细胞分泌有助于肿瘤的生长,血管生成和转移。我们最近已经证明,在低O(2)下用GM-CSF刺激的巨噬细胞会分泌高水平的可溶形式的VEGF受体1(sVEGFR-1),中和VEGF并抑制其生物学活性。使用小型干扰RNA靶向耗竭鼠巨噬细胞中的缺氧诱导因子(HIF)-1alpha或HIF-2alpha,我们发现响应低O(2)的巨噬细胞sVEGFR-1的生产依赖于HIF-2alpha,而HIF -1alpha专门调节VEGF的产生。在我们当前的报告中,我们评估了具有单核细胞/巨噬细胞选择性缺失HIF-1alpha或HIF-2alpha(HIF-1alpha(flox / flox)-或HIF-2alpha(flox / +)的小鼠中B16F10恶性黑色素瘤的生长/ LysMcre小鼠)。 GM-CSF处理可增加对照组小鼠的肿瘤内VEGF和sVEGFR-1,这种作用与微血管密度的降低有关。 GM-CSF对HIF-1alpha(flox / flox)/ LysMcre小鼠的治疗可诱导sVEGFR-1,但不能诱导VEGF,与对照小鼠相比,肿瘤生长和血管生成的总体降低幅度更大。此外,针对黑色素瘤特异性基因的实时PCR显示,在用GM-CSF治疗的HIF-1alpha(flox / flox)/ LysMcre小鼠中,肺微转移的存在显着减少。相反,GM-CSF处理在HIF-2alpha(flox / +)/ LysMcre小鼠中诱导VEGF,但不诱导sVEGFR-1,因此,GM-CSF没有降低这些小鼠的肿瘤生长,血管生成或肺转移。这项研究揭示了HIFs在肿瘤相关巨噬细胞对血管生成的调控中的相反作用,并提示GM-CSF的给药可能是诱导sVEGFR-1并抑制黑素瘤患者肿瘤生长和血管生成的有效手段。

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