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免疫 PET 显像及抗 CEA scFv 三聚体与其单体型对照在荷人胃癌裸鼠体内的药代动力学研究。

Immuno-PET Imaging and Pharmacokinetics of an Anti-CEA scFv-based Trimerbody and Its Monomeric Counterpart in Human Gastric Carcinoma-Bearing Mice.

机构信息

Radiochemistry and Nuclear Imaging Group , CIC biomaGUNE , 20014 San Sebastián , Guipúzcoa , Spain.

Molecular Immunology Unit , Hospital Universitario Puerta de Hierro Majadahonda , Manuel de Falla 1, 28222 Majadahonda, Madrid , Spain.

出版信息

Mol Pharm. 2019 Mar 4;16(3):1025-1035. doi: 10.1021/acs.molpharmaceut.8b01006. Epub 2019 Feb 18.

DOI:10.1021/acs.molpharmaceut.8b01006
PMID:30726099
Abstract

Monoclonal antibodies (mAbs) are currently used as therapeutic agents in different types of cancer. However, mAbs and antibody fragments developed so far show suboptimal properties in terms of circulation time and tumor penetration/retention. Here, we report the radiolabeling, pharmacokinetic evaluation, and determination of tumor targeting capacity of the previously validated anti-CEA MFE23-scFv-based N-terminal trimerbody (MFE23-trimerbody), and the results are compared to those obtained for the monomeric MFE23-scFv. Dissection and gamma-counting studies performed with the I-labeled protein scaffolds in normal mice showed slower blood clearance for the trimerbody, and accumulation in the kidneys, the spleen, and the liver for both species. These, together with a progressive uptake in the small intestine, confirm a combined elimination scheme with hepatobiliary and urinary excretion. Positron emission tomography studies performed in a xenograft mouse model of human gastric adenocarcinoma, generated by subcutaneous administration of CEA-positive human MKN45 cells, showed higher tumor accumulation and tumor-to-muscle (T/M) ratios for I-labeled MFE23-trimerbody than for MFE23-scFv. Specific uptake was not detected with PET imaging in CEA negative xenografts as indicated by low T/M ratios. Our data suggest that engineered intermediate-sized trivalent antibody fragments could be promising candidates for targeted therapy and imaging of CEA-positive tumors.

摘要

单克隆抗体(mAbs)目前被用作治疗不同类型癌症的药物。然而,迄今为止开发的 mAbs 和抗体片段在循环时间和肿瘤穿透/保留方面表现出不理想的特性。在这里,我们报告了先前经过验证的抗 CEA MFE23-scFv 为基础的 N 端三聚体(MFE23-trimerbody)的放射性标记、药代动力学评估和肿瘤靶向能力的测定,结果与单体 MFE23-scFv 的结果进行了比较。在正常小鼠中用 I 标记的蛋白质支架进行的剖析和伽马计数研究表明,三聚体的血液清除速度较慢,在肾脏、脾脏和肝脏中均有积累。这些与从小肠逐渐吸收一起,证实了具有肝胆和尿液排泄的联合消除方案。在皮下注射 CEA 阳性人 MKN45 细胞生成的人胃腺癌异种移植小鼠模型中进行的正电子发射断层扫描研究表明,I 标记的 MFE23-trimerbody 比 MFE23-scFv 具有更高的肿瘤积累和肿瘤与肌肉(T/M)比值。如 T/M 比值较低所示,PET 成像未检测到 CEA 阴性异种移植物中的特异性摄取。我们的数据表明,工程化的中等大小的三价抗体片段可能是 CEA 阳性肿瘤靶向治疗和成像的有前途的候选物。

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