A New Prostate Carcinoma Binding Peptide (DUP-1) for Tumor Imaging and Therapy

前列腺 体内分布 前列腺癌 内化 癌症研究 病理 医学 化学 体外 癌症 细胞 内科学 生物化学
作者
Sabine Zitzmann,Walter Mier,Arno Schad,Ralf Kinscherf,Vasileios Askoxylakis,Susanne Krämer,Annette Altmann,Michael Eisenhut,Uwe Haberkorn
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:11 (1): 139-146 被引量:74
标识
DOI:10.1158/1078-0432.139.11.1
摘要

Prostate carcinomas belong to the most widespread tumors, and their number is increasing. Imaging modalities used for diagnosis, such as ultrasound, computed tomography, and positron emission tomography, often produce poor results. Radiolabeled peptides with high sensitivity and specificity for prostate cancer would be a desirable tool for tumor diagnosis and treatment.We used phage display and the prostate-specific membrane antigen-negative cell line DU-145 to identify a peptide. The isolated DUP-1 was tested in vitro for its binding specificity, kinetics, and affinity. Internalization of the peptide was evaluated with confocal microscopy. The tumor accumulation in a nude mouse model was analyzed with 131I-labeled DUP-1 in PC-3 and DU-145 prostate tumors as well as in the rat prostate tumor model AT-1.The synthesized peptide showed rapid binding kinetics peaking at 10 minutes. It shows specific binding to prostate carcinoma cells but low binding affinity to nontumor cells. Peptide binding is competed with unlabeled DUP-1, and a time-dependent internalization into DU-145 cells was shown. Biodistribution studies of DUP-1 in nude mice with s.c. transplanted DU-145 and PC-3 tumors showed a tumor accumulation of 5% and 7% injected dose per gram, and bound peptide could not be removed by perfusion. The rat prostate tumor model showed an increase of radioactivity in the prostate tumor up to 300% in comparison with normal prostate tissue.DUP-1 holds promise as a lead peptide structure applicable in the development of new diagnostic tracers or anticancer agents that specifically target prostate carcinoma.
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