首页> 外文期刊>American Journal of Physiology >Hypoxic signaling: Some organs are more equal than others. Focus on 'Differential HIF and NOS responses to acute anemia: Defining organ-specific hemoglobin thresholds for tissue hypoxia'
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Hypoxic signaling: Some organs are more equal than others. Focus on 'Differential HIF and NOS responses to acute anemia: Defining organ-specific hemoglobin thresholds for tissue hypoxia'

机译:低氧信号:某些器官比其他器官更平等。专注于“对急性贫血的HIF和NOS不同反应:定义组织缺氧的器官特异性血红蛋白阈值”

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Understanding vascular growth and maturation in developing tumors has important implications for tumor progression, spread, and ultimately host survival. Modulating the signaling of endothelial G protein-coupled receptors (GPCRs) in blood and lymphatic vessels can enhance or limit tumor progression. Sphingosine 1-phosphate receptor 1 (S1PR1) is a GPCR for circulating lysophospholipid S1P that is highly expressed in blood and lymphatic vessels. Using the S1PR1- enhanced green fluorescent protein (eGFP) mouse model in combination with intravital imaging and pharmacologic modulation of S1PR1 signaling, we show that boundary conditions of high and low S1PR1 signaling retard tumor progression by enhancing or destabilizing neovasculature integrity, respectively. In contrast, midrange S1PR1 signaling, achieved by receptor antagonist titration, promotes abundant growth of small, organized vessels and thereby enhances tumor progression. Furthermore, in vivo S1PR1 antagonism supports lung colonization by circulating tumor cells. Regulation of endothelial S1PR1 dynamically controls vascular integrity and maturation and thus modulates angiogenesis, tumor growth, and hematogenous metastasis.
机译:了解正在发展的肿瘤中的血管生长和成熟对肿瘤的进展,扩散以及最终的宿主存活具有重要意义。调节血液和淋巴管中内皮G蛋白偶联受体(GPCR)的信号传导可以增强或限制肿瘤的进展。鞘氨醇1-磷酸受体1(S1PR1)是用于循环溶血磷脂S1P的GPCR,溶血磷脂S1P在血液和淋巴管中高度表达。使用S1PR1增强的绿色荧光蛋白(eGFP)小鼠模型与活体成像和S1PR1信号的药理学调节相结合,我们显示高和低S1PR1信号的边界条件分别通过增强或破坏新脉管系统完整性来延迟肿瘤进展。相反,通过受体拮抗剂滴定实现的中端S1PR1信号传导促进小而有组织的血管的大量生长,从而增强了肿瘤的进展。此外,体内S1PR1拮抗作用通过循环肿瘤细胞支持肺部定植。内皮S1PR1的调节动态控制血管完整性和成熟度,从而调节血管生成,肿瘤生长和血源性转移。

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