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Preliminary biological evaluation of 18F-AlF-NOTA-MAL-Cys-Annexin V as a novel apoptosis imaging agent

机译:新型细胞凋亡显像剂18F-AlF-NOTA-MAL-Cys-Annexin V的初步生物学评估

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摘要

A novel annexin V derivative (Cys-Annexin V) with a single cysteine residue at its C-terminal has been successfully labeled site-specifically with NOTA-maleimide aluminum [18F]fluoride complexation and evaluated it as a novel apoptosis agent in vitro and in vivo. The total synthesis time of 18F-AlF-NOTA-MAL-Cys-Annexin V from [18F]fluoride was about 65 min. The tracer was stable in vitro and it was excreted through renal in normal mice. The rate of the tracer bound to erythrocytes with exposed phosphatidylserine was 89.36±0.61% and this binding could be blocked by unlabeled Cys-Annexin V. In rats treated with cycloheximide, there were 6.23±0.23 times (n=4) increase in hepatic uptake of the tracer as compared to normal rats at 1h p.i. The uptake of the tracer in liver also could be blocked by co-injection of unlabeled Cys-Annexin V. These results indicated the favorable characterizations such as convenient synthesis and specific apoptotic cells targeting of18F-AlF-NOTA-MAL- Cys-Annexin V were suitable for its further investigation in clinical apoptosis imaging.
机译:一种新型的膜联蛋白V衍生物(Cys-Annexin V)在其C端具有一个半胱氨酸残基,已成功地通过NOTA-马来酰亚胺铝[ 18 F]氟化物络合位点进行了特异性标记,并将其评估为体外和体内的新型凋亡剂。 [sup> 18 F]氟化物合成 18 F-AlF-NOTA-MAL-Cys-Annexin V的总时间约为65分钟。示踪剂在体外稳定,在正常小鼠中通过肾脏排泄。示踪剂与暴露于磷脂酰丝氨酸的红细胞结合的比率为89.36±0.61%,这种结合可以被未标记的Cys-Annexin V阻断。在用环己酰亚胺治疗的大鼠中,肝脏摄取量增加了6.23±0.23倍(n = 4)。 pi 1h时示踪剂与正常大鼠的比较共注射未标记的Cys-Annexin V也可以阻止肝脏中示踪剂的摄取。这些结果表明了 18 F-AlF-靶向的方便合成和特异性凋亡细胞的良好特性。 NOTA-MAL-半胱氨酸-Annexin V适合在临床细胞凋亡成像中进行进一步研究。

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