Int J Mol Sci：ATPS mAb标记Zr-89，可用于肿瘤血管生成的免疫-PET成像

2020-04-23 网络网络

本研究中，我们合成了一种Zr-89标记的抗腺苷三磷酸合酶单克隆抗体（ATPS mAb），用于免疫-positron发射断层扫描（PET），并评估了其在血管生成成像中的可行性。

本研究中，我们合成了一种Zr-89标记的抗腺苷三磷酸合酶单克隆抗体（ATPS mAb），用于免疫-positron发射断层扫描（PET），并评估了其在血管生成成像中的可行性。

对Zr-89 ATPS mAb在体外处理癌细胞株后的细胞摄取量进行了测定，并对其在小鼠体内4、24和48 h时的生物分布进行了评估。在Zr-89 ATPS mAb给药后的4，24，48和96 h获得PET图像。使用抗CD31免疫荧光染色分析肿瘤血管生成。

结果显示，在MDA-MB-231乳腺癌细胞中，Zr-89 ATPS mAb的细胞摄取量随着时间的推移而增加，但在PC3前列腺癌细胞中没有增加。MDA-MB-231细胞在24 h时对Zr-89 ATPS mAb的肿瘤吸收率为9.4±0.9% ID/g，PC3细胞为3.8±0.6% ID/g（p = 0.004）。Zr-89 ATPS mAb在MDA-MB-231异种移植细胞中的吸收被冷ATPS mAb给药所抑制（4.4±0.5% ID/g，p = 0.011）。在MDA-MB-231肿瘤中，Zr-89 ATPS mAb的摄取可以通过PET可视化，长达96 h。相比之下，在PC3异种移植模型中，没有明显的肿瘤吸收通过PET检测到明显的肿瘤吸收。CD31阳性的肿瘤血管在MDA-MB-231肿瘤中大量存在，而在PC3肿瘤中几乎没有检测到。

总之，ATPS mAb成功标记了Zr-89，可用于肿瘤血管生成的免疫-PET成像。

原始出处：

Bok-Nam Park, Ga-Hee Kim, et al., Zr-89 Immuno-PET Targeting Ectopic ATP Synthase Enables In-Vivo Imaging of Tumor Angiogenesis. Int J Mol Sci. 2019 Aug; 20(16): 3928. doi: 10.3390/ijms20163928

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2020-06-08 feather89

#PE#

62 0
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2020-11-11 肉我只吃一口

#肿瘤血管生成#

73 0
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2021-02-22 meichuangyi

#肿瘤血管#

75 0
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2020-09-06 ms1260584454294838

#PET成像#

70 0
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2020-12-15 snf701207

#mAb#

55 0
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2020-04-25 ms7514935887898259

#PET#

45 0
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2020-04-25 listen320

#ATP#

80 0

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Int J Mol Sci：ATPS mAb标记Zr-89，可用于肿瘤血管生成的免疫-PET成像

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