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碘124标记的抗前列腺干细胞抗原工程化抗体片段在携带LAPC-9肿瘤的严重联合免疫缺陷小鼠中的正电子发射断层扫描成像

Positron emission tomographic imaging of iodine 124 anti-prostate stem cell antigen-engineered antibody fragments in LAPC-9 tumor-bearing severe combined immunodeficiency mice.

作者信息

Fonge Humphrey, Leyton Jeffrey V

机构信息

Department of Pharmaceutical Sciences, University of Toronto, Toronto, ON, Canada.

出版信息

Mol Imaging. 2013 May;12(3):191-202.

Abstract

The humanized antibody (hu1G8) has been shown to localize to prostate stem cell antigen (PSCA) and image PSCA-positive xenografts. We previously constructed hu1G8 anti-PSCA antibody fragments and tested them for tumor targeting and the ability to image prostate cancer at early and late time points postinjection by positron emission tomography (PET). We now then compare the PET imaging and the radioactivity accumulation properties in prostate cancer tumors and nontarget tissues to determine the superior 124I-labeled hu1G8 antibody format. 124I-labeled diabody, minibody, scFv-Fc, scFv-Fc double mutant (DM), and parental IgG were administered into severe combined immunodeficiency (SCID) mice bearing LAPC-9 xenografts and followed by whole-body PET imaging of mice at preselected time points. Regions of interest were manually drawn around tumor and nontarget tissues and evaluated for radioactivity accumulation. The 124I-hu1G8 IgG has its best time point for tumor high-contrast imaging at 168 hours postinjection. The 124I-hu1G8 minibody at 44 hours postinjection results in superior tumor high-contrast imaging compared to the other antibody formats. The 124I-hu1G8 minibody at 44 hours postinjection also has comparable percent tumor radioactivity compared to 124I-hu1G8 IgG at 168 hours postinjection. The 124I-hu1G8 minibody is the best engineered hu1G8 antibody format for imaging prostate cancer.

摘要

人源化抗体(hu1G8)已被证明可定位于前列腺干细胞抗原(PSCA),并对PSCA阳性异种移植瘤进行成像。我们之前构建了hu1G8抗PSCA抗体片段,并通过正电子发射断层扫描(PET)在注射后的早期和晚期时间点测试了它们的肿瘤靶向性以及对前列腺癌成像的能力。然后,我们比较了PET成像以及前列腺癌肿瘤和非靶组织中的放射性积累特性,以确定124I标记的hu1G8抗体的最佳形式。将124I标记的双体、微型抗体、单链抗体片段-免疫球蛋白融合蛋白(scFv-Fc)、scFv-Fc双突变体(DM)和亲本IgG注射到携带LAPC-9异种移植瘤的严重联合免疫缺陷(SCID)小鼠体内,并在预先选定的时间点对小鼠进行全身PET成像。在肿瘤和非靶组织周围手动绘制感兴趣区域,并评估放射性积累情况。124I-hu1G8 IgG在注射后168小时具有肿瘤高对比度成像的最佳时间点。与其他抗体形式相比,注射后44小时的124I-hu1G8微型抗体可实现更优的肿瘤高对比度成像。与注射后168小时的124I-hu1G8 IgG相比,注射后44小时的124I-hu1G8微型抗体在肿瘤中的放射性百分比也相当。124I-hu1G8微型抗体是用于前列腺癌成像的最佳工程化hu1G8抗体形式。

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