VEGFR-3基因转染淋巴管内皮祖细胞后可溶性VEGFR-3蛋白的分泌

被引:4
|
作者
敖红
谭玉珍
王海杰
国海东
机构
[1] 复旦大学上海医学院人体解剖与组织胚胎学系
来源
中国实验动物学报 | 2009年 / 17卷 / 04期
关键词
BABL/c小鼠; VEGFR-3; 腺病毒载体; 转染; 淋巴管内皮祖细胞;
D O I
暂无
中图分类号
R73-3 [肿瘤学实验研究];
学科分类号
摘要
目的研究携带BABL/c小鼠VEGFR-3(1-3Ig)基因的重组腺病毒转染淋巴管内皮祖细胞(LEPCs)后,对可溶性VEGFR-3蛋白分泌及其生物学特性的作用。方法采用巢式RT-PCR技术从BABL/c小鼠胎盘组织中扩增VEGFR-3(1-3Ig)的编码基因,并通过重组PCR技术在基因的N端加上人CD33的信号肽。将该基因片段亚克隆入腺病毒表达载体(pDC316-IRES-EGFP),重组质粒经酶切及测序验证后,与包装质粒共转染293细胞以产生重组腺病毒。将构建好的携带有小鼠VEGFR-3(1-3Ig)基因的重组腺病毒转染淋巴管内皮祖细胞,通过ELISA检测转染细胞上清液中可溶性VEGFR-3蛋白的分泌及其对VEGF-C的中和作用。结果成功构建了带有信号肽的BABL/c小鼠VEGFR-3(1-3Ig)基因的腺病毒表达质粒,并获得高滴度的携带有小鼠VEGFR-3(1-3Ig)基因的重组腺病毒,重组腺病毒转染淋巴管内皮祖细胞后,可使转染细胞分泌可溶性VEGFR-3蛋白,该蛋白具有中和VEGF-C的作用。结论成功地制备了携带BABL/c小鼠VEGFR-3(1-3Ig)基因的重组腺病毒,用该病毒转染淋巴管内皮祖细胞可使其分泌可溶性VEGFR-3,该蛋白在体外具有中和VEGF-C的作用,这为临床抑制肿瘤淋巴管新生奠定了基础。
引用
收藏
页码:252 / 257+238 +238
页数:7
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