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人血管内皮细胞的胆碱磷脂代谢产物因环氧化酶抑制、生长因子缺乏以及癌细胞分泌的旁分泌因子而发生改变。

Choline phospholipid metabolites of human vascular endothelial cells altered by cyclooxygenase inhibition, growth factor depletion, and paracrine factors secreted by cancer cells.

作者信息

Mori Noriko, Natarajan Kshama, Chacko V P, Artemov Dmitri, Bhujwalla Zaver M

机构信息

Johns Hopkins University, Baltimore, MD, USA.

出版信息

Mol Imaging. 2003 Apr;2(2):124-30. doi: 10.1162/15353500200303127.

Abstract

Magnetic resonance studies have previously shown that solid tumors and cancer cells in culture typically exhibit high phosphocholine and total choline. Treatment of cancer cells with the anti-inflammatory agent, indomethacin (INDO), reverted the phenotype of choline phospholipid metabolites in cancer cells towards a less malignant phenotype. Since endothelial cells form a key component of tumor vasculature, in this study, we used MR spectroscopy to characterize the phenotype of choline phospholipid metabolites in human umbilical vein endothelial cells (HUVECs). We determined the effect of growth factors, the anti-inflammatory agent INDO, and conditioned media obtained from a malignant cell line, on choline phospholipid metabolites. Growth factor depletion or treatment with INDO induced similar changes in the choline phospholipid metabolites of HUVECs. Treatment with conditioned medium obtained from MDA-MB-231 cancer cells induced changes similar to the presence of growth factor supplements. These results suggest that cancer cells secrete growth factors and/or other molecules that influence the choline phospholipid metabolism of HUVECs. The ability of INDO to alter choline phospholipid metabolism in the presence of growth factor supplements suggests that the inflammatory response pathways of HUVECs may play a role in cancer cell-HUVEC interaction and in the response of HUVECs to growth factors.

摘要

磁共振研究先前已表明,培养中的实体瘤和癌细胞通常表现出高磷酸胆碱和总胆碱水平。用抗炎药吲哚美辛(INDO)处理癌细胞,可使癌细胞中胆碱磷脂代谢物的表型向恶性程度较低的表型转变。由于内皮细胞是肿瘤血管系统的关键组成部分,在本研究中,我们使用磁共振波谱来表征人脐静脉内皮细胞(HUVECs)中胆碱磷脂代谢物的表型。我们确定了生长因子、抗炎药INDO以及从恶性细胞系获得的条件培养基对胆碱磷脂代谢物的影响。生长因子缺乏或用INDO处理会在HUVECs的胆碱磷脂代谢物中诱导相似的变化。用从MDA-MB-231癌细胞获得的条件培养基处理会诱导出与存在生长因子补充剂时相似的变化。这些结果表明,癌细胞分泌生长因子和/或其他影响HUVECs胆碱磷脂代谢的分子。在存在生长因子补充剂的情况下,INDO改变胆碱磷脂代谢的能力表明,HUVECs的炎症反应途径可能在癌细胞与HUVECs的相互作用以及HUVECs对生长因子的反应中起作用。

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