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首页> 外文期刊>The FASEB Journal >Aquaporin-1 gene deletion reduces breast tumor growth and lung metastasis in tumor-producing MMTV-PyVT mice.
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Aquaporin-1 gene deletion reduces breast tumor growth and lung metastasis in tumor-producing MMTV-PyVT mice.

机译:水通道蛋白-1 基因缺失可减少产瘤 MMTV-PyVT 小鼠的乳腺肿瘤生长和肺转移。

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摘要

Aquaporin 1 (AQP1) is a plasma membrane water-transporting protein expressed strongly in tumor microvascular endothelia. We previously reported impaired angiogenesis in implanted tumors in AQP1-deficient mice and reduced migration of AQP1-deficient endothelial cells in vitro. Here, we investigated the consequences of AQP1 deficiency in mice that spontaneously develop well-differentiated, luminal-type breast adenomas with lung metastases mouse mammary tumor virus-driven polyoma virus middle T oncogene (MMTV-PyVT). AQP1(+/+) MMTV-PyVT mice developed large breast tumors with total tumor mass 3.5 ± 0.5 g and volume 265 ± 36 mm(3) (SE, 11 mice) at age 98 d. Tumor mass (1.6±0.2 g) and volume (131±15 mm(3), 12 mice) were greatly reduced in AQP1(-/-) MMTV-PyVT mice (P<0.005). CD31 immunofluorescence showed abnormal microvascular anatomy in tumors of AQP1(-/-) MMTV-PyVT mice, with reduced vessel density. HIF-1α expression was increased in tumors in AQP1(-/-) MMTV-PyVT mice. The number of lung metastases (5±1/mouse) was much lower than in AQP1(+/+) MMTV-PyVT mice (31±8/mouse, P<0.005). These results implicate AQP1 as an important determinant of tumor angiogenesis and, hence, as a potential drug target for adjuvant therapy of solid tumors.
机译:水通道蛋白 1 (AQP1) 是一种在肿瘤微血管内皮中强烈表达的质膜水转运蛋白。我们之前报道了 AQP1 缺陷小鼠植入肿瘤的血管生成受损和 AQP1 缺陷内皮细胞在体外的迁移减少。在这里,我们研究了自发发展为具有肺转移的分化良好的管腔型乳腺腺瘤 [小鼠乳腺肿瘤病毒驱动的多瘤病毒中间 T 癌基因 (MMTV-PyVT)] 的小鼠 AQP1 缺乏的后果。AQP1(+/+) MMTV-PyVT小鼠在98 d龄时发生腺肿瘤,总肿瘤质量为3.5±0.5g,体积为265±36mm(3)(SE,11只小鼠)。AQP1(-/-) MMTV-PyVT小鼠(P<0.005)的肿瘤质量(1.6±0.2g)和体积(131±15 mm(3),12只小鼠)显著减少。CD31免疫荧光显示AQP1(-/-)MMTV-PyVT小鼠肿瘤的微血管解剖结构异常,血管密度降低。HIF-1α 在 AQP1(-/-) MMTV-PyVT 小鼠肿瘤中的表达增加。肺转移灶数(5±1/小鼠)远低于AQP1(+/+)MMTV-PyVT小鼠(31±8/小鼠,P<0.005)。这些结果表明AQP1是肿瘤血管生成的重要决定因素,因此是实体瘤辅助治疗的潜在药物靶点。

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