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Development of a CLDN18.2-targeting immuno-PET probe for non-invasive imaging in gastrointestinal tumors

摘要Claudin18.2(CLDN18.2)is a tight junction protein that is overexpressed in a variety of solid tumors such as gastrointestinal cancer and oesophageal cancer.It has been identified as a promising target and a potential biomarker to diagnose tumor,evaluate efficacy,and determine patient prognosis.TST001 is a recombinant humanized CLDN18.2 antibody that selectively binds to the extracellular loop of human Claudin18.2.In this study,we constructed a solid target radionuclide zirconium-89(89Zr)labled-TST001 to detect the expression of in the human stomach cancer BGC823CLDN18.2 cell lines.The[89Zr]Zr-des-ferrioxamine(DFO)-TST001 showed high radiochemical purity(RCP,>99%)and specific activity(24.15±1.34 GBq/μmol),and was stable in 5%human serum albumin,and phosphate buffer saline(>85%RCP at 96 h).The EC50 values of TST001 and DFO-TST001 were as high as 0.413±0.055 and 0.361±0.058 nM(P>0.05),respectively.The radiotracer had a significantly higher average standard uptake values in CLDN18.2-positive tumors than in CLDN18.2-negative tumors(1.11±0.02 vs.0.49±0.03,P=0.0016)2 days post injection(p.i.).BGC823CLDN18.2 mice models showed high tumor/muscle ratios 96 h p.i.with[89Zr]Zr-DFO-TST001 was much higher than those of the other imaging groups.Immunohistochemistry results showed that BGC823CLDN18.2 tumors were highly positive(+++)for CLDN18.2,while those in the BGC823 group did not express CLDN18.2(-).The results of ex vivo biodistribution studies showed that there was a higher distribution in the BGC823CLDN18.2 tumor bearing mice(2.05±0.16%ID/g)than BGC823 mice(0.69±0.02%ID/g)and blocking group(0.72±0.02%ID/g).A dosimetry estimation study showed that the effective dose of[89Zr]Zr-DFO-TST001 was 0.0705 mSv/MBq,which is within the range of acceptable doses for nuclear medicine research.Taken together,these re-sults suggest that Good Manufacturing Practices produced by this immuno-positron emission tomog-raphy probe can detect CLDN18.2-overexpressing tumors.

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作者 Yan Chen [1] Xingguo Hou [2] Dapeng Li [1] Jin Ding [2] Jiayue Liu [2] Zilei Wang [3] Fei Teng [4] Hongjun Li [4] Fan Zhang [4] Yi Gu [4] Steven Yu [4] Xueming Qian [4] Zhi Yang [5] Hua Zhu [5] 学术成果认领
作者单位 Guizhou University Medicine College,Guiyang,550025,China;The Ministry of Education Key Laboratory of Carcinogenesis and Translational Research;NMPA Key Laboratory for Research and Evaluation of Radiopharmaceuticals,Department of Nuclear Medicine,Peking University Cancer Hospital & Institute,Beijing,100142,China [1] The Ministry of Education Key Laboratory of Carcinogenesis and Translational Research;NMPA Key Laboratory for Research and Evaluation of Radiopharmaceuticals,Department of Nuclear Medicine,Peking University Cancer Hospital & Institute,Beijing,100142,China [2] The Ministry of Education Key Laboratory of Carcinogenesis and Translational Research;NMPA Key Laboratory for Research and Evaluation of Radiopharmaceuticals,Department of Nuclear Medicine,Peking University Cancer Hospital & Institute,Beijing,100142,China;Department of Biochemistry and Molecular Biology,School of Basic Medical Sciences,Southwest Medical University,Luzhou,Sichuan,646000,China [3] Suzhou Transcenta Therapeutics Co.,Ltd,Suzhou,Jiangsu,215127,China [4] Guizhou University Medicine College,Guiyang,550025,China;The Ministry of Education Key Laboratory of Carcinogenesis and Translational Research;NMPA Key Laboratory for Research and Evaluation of Radiopharmaceuticals,Department of Nuclear Medicine,Peking University Cancer Hospital & Institute,Beijing,100142,China;Institute of Biomedical Engineering,Peking University Shenzhen Graduate School,Shenzhen,Guangdong,518055,China [5]
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发布时间 2023-06-30(万方平台首次上网日期,不代表论文的发表时间)
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药物分析学报(英文版)

药物分析学报(英文版)

2023年13卷4期

367-375页

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