Synthesis and evaluation of ^(64)Cu-radiolabeled NOTA-cetuximab(^(64)Cu-NOTA-C225) for immuno-PET imaging of EGFR expression

Objective: Epidermal growth factor receptor(EGFR) is overexpressed in a wide variety of solid tumors, serving as a well-characterized target for cancer imaging or therapy. In this study, we aimed to design and synthesize a radiotracer, ^(64) Cu-NOTA-C225, targeting EGFR for tumor positron emission tomography(PET) imaging.Methods: Cetuximab(C225) was conjugated to a bifunctional chelator, p-isothiocyanatobenzyl-1,4,7-triazacyclononane-1,4,7-triacetic acid(NOTA), and further radiolabeled with copper-^(64) for PET imaging. ^(64) CuNOTA-IgG and Cy5.5-C225 were also synthesized as control probes. A431 and A549 mouse models were established for micro-PET and/or near-infrared fluorescence(NIRF) imaging.Results: ^(64) Cu-NOTA-C225 exhibited stability in vivo and in vitro up to 24 h and 50 h post-injection,respectively. A431 tumors with average standard uptake values(SUVs) of 5.61±0.69, 6.68±1.14, 7.80±1.51 at 6, 18 and 36 h post-injection, respectively, which were significantly higher than that of moderate EGFR expressing tumors(A549), with SUVs of 0.89±0.16, 4.70±0.81, 2.01±0.50 at 6, 18 and 36 h post-injection, respectively. The expression levels of A431 and A549 were confirmed by western blotting. Additionally, the tracer uptake in A431 tumors can be blocked by unlabeled cetuximab, suggesting that tracer uptake by tumors was receptor-mediated.Furthermore, NIRF imaging using Cy5.5-C225 showed that the fluorescence intensity in tumors increased with time, with a maximal intensity of 8.17 E+10(p/s/cm^2/sr)/(μW/cm^2) at 48 h post-injection, which is consistent with the paradigm from micro-PET imaging in A431 tumor-bearing mice.Conclusions: The ^(64) Cu-NOTA-C225 PET imaging may be able to specifically and sensitively differentiate tumor models with different EGFR expression levels. It offers potentials as a PET radiotracer for imaging of tracer EGFR-positive tumors.

^(64)Cu标记单链DNA及其体内分布的初步研究

本文探索^(64)Cu标记单链脱氧核糖核酸(Deoxyribo Nucleic Acid,DNA)方法及小鼠体内分布情况。将单链DNA(ssDNA)与螯合剂p-SCN-Bn-NOTA偶联,得到NOTA-ssDNA,加入64Cu孵育一定时间,利用薄层色谱监测反应,NAP-5脱盐柱纯化,得到64Cu-ssDNA。静脉注射进入昆明鼠体内后,研究不同时间点感兴趣器官或脏器的放射性摄取量。NOTA-ssDNA与64Cu反应1 h后,放化标记率为(66.4±2.85)%;纯化后,放化纯度大于95%。体外稳定实验显示,^(64)Cu-ssDNA在PBS(Phosphate Buffer Saline)或小鼠血清中至少能稳定存在6 h。^(64)Cu-ssDNA通过静脉注射到小鼠体内后,在胃肠道有一定的摄取,而肾脏和膀胱出现高放射性摄取量。注射180 min后,膀胱中的放射性摄取量达到了(63.84±5.86)%ID∙g^(−1)。结果表明:64Cu-ssDNA主要通过泌尿系统代谢排出体外。^(64)Cu-ssDNA的成功制备,为基于DNA多面体的PET分子探针的制备解决了关键一步;其体内分布实验为研究^(64)Cu标记DNA多面体的体内生物分布提供了实验对照信息。

特异性靶向高转移骨肉瘤的长循环型PET探针的合成及显像

目的 研究[^(64)Cu]Cu-DOTA-EB-TMTP1对143B骨肉瘤荷瘤小鼠模型的诊断效果。方法 多肽TMTP1(NVVRQ)对高转移性细胞有很好的靶向性,本研究利用^(64)Cu标记DOTA-EB-TMTP1合成[^(64)Cu]Cu-DOTA-EB-TMTP1,然后对143B骨肉瘤肝癌荷瘤小鼠进行microPET/CT显像,研究其对肿瘤的诊断效果。结果 [^(64)Cu]Cu-DOTA-EB-TMTP1的放射性标记产率为(87.3±5.2)%,放化纯度大于95.0%。实验证明经过伊文思蓝(Evans Blue)修饰后的TMTP1,具有更高的肿瘤摄取和更长的血液半衰期,8 h肿瘤摄取值可达(6.50±0.88)%ID/g。结论 对于骨肉瘤的诊断来说,[^(64)Cu]Cu-DOTA-EB-TMTP1可能是更好的PET探针,更有利于肿瘤的诊疗一体化转化应用。

FM4-64和Hoechst染料在活细菌胞膜和拟核标记定位中的条件优化与应用

【目的】为了观察细菌细胞膜和拟核的形态结构,准确对亚细胞进行定位。【方法】本文利用FM4-64和Hoechst两种染料,分别采用不同浓度和不同时间对大肠杆菌活细胞进行染色和荧光共聚焦显微成像,并对7种细菌的活细胞(金黄色葡萄球菌、铜绿假单胞菌、肺炎克雷伯菌、鼠疫耶尔森菌、军团菌、霍乱弧菌和炭疽芽孢杆菌)进行染色观察。【结果】相同观察条件下,不同染料浓度和不同的染色时间影响了细胞膜、拟核的荧光强度;确定了FM4-64染色通用条件(浓度20μg/m L染色1 min)和Hoechst的最佳条件(浓度20μg/m L染色20min)。上述条件下,Hoechst对8种细菌染色效果均较理想,然而FM4-64对细菌染色效果不同,革兰氏阴性菌(大肠杆菌、肺炎克雷伯菌、鼠疫耶尔森菌、霍乱弧菌、铜绿假单胞菌和军团菌)表现较好的细胞膜轮廓,革兰氏阳性菌(炭疽芽孢杆菌和金黄色葡萄球菌)效果较差。【结论】FM4-64和Hoechst两种染料共染8种细菌,对细胞膜和拟核的染色观察,可为原核细胞结构染色提供借鉴,并为大分子的亚细胞定位研究奠定基础。

Alexa-555 WGA和FM4-64在活细菌定位中的比较应用

为了准确定位亚细胞形态,本试验比较应用Alexa-555 WGA和FM4-64两种染料,为研究者合理选择染料提供线索。以大肠杆菌(Escherichia coli)、鲍曼不动杆菌(Acinetobacter baumannii)、金黄色葡萄球菌(Staphylococcus aureus)和炭疽芽孢杆菌(Bacillus anthracis)为对象,使用Hoechst 33342标记拟核,FM4-64标记细胞膜,Alexa-555 WGA标记细胞壁,Perkin Elmer Ultra VIEW Vo X荧光共聚焦显微镜观察成像。FM4-64染料适合于革兰氏阴性菌细胞膜染色,Alexa-555 WGA染料对革兰氏阴性菌和革兰氏阳性菌细胞壁染色效果均较好。Alexa-555 WGA能用于不同类型细菌细胞壁的定位。本研究首次将Alexa-555 WGA染料应用于原核生物,可为细菌的亚细胞定位研究提供借鉴。