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A Cyclic Peptide‐Based Radiotheranostic Agent for Urokinase‐Type Plasminogen Activator in Tumors
Author(s) -
Wang Xingkai,
Dai Dong,
Shen Jieting,
Zhang Siqi,
Ohkubo Takayuki,
Xie Lin,
Zhang Yiding,
Li Guoqing,
Liu Can,
Tian Hao,
Zhang Yingzi,
Zhang MingRong,
Wang Rui,
Hu Kuan
Publication year - 2025
Publication title -
chemistry – a european journal
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.687
H-Index - 242
eISSN - 1521-3765
pISSN - 0947-6539
DOI - 10.1002/chem.202500479
Subject(s) - urokinase receptor , plasminogen activator , urokinase , cancer research , chemistry , peptide , metastasis , extracellular matrix , receptor , activator (genetics) , biology , biochemistry , medicine , cancer , endocrinology
Abstract The plasminogen activator system is critically involved in tumor progression regulation. Aberrant activation of urokinase‐type plasminogen activator (uPA) induces proteolytic degradation of cellular membranes and the extracellular matrix, thereby promoting tumor invasion and metastasis. Consequently, uPA has emerged as a promising diagnostic and therapeutic target. Herein, we designed and evaluated three cyclic peptide‐based radioligands ([⁶⁴Cu]CAP‐1, [⁶⁴Cu]CAP‐2, and [⁶⁴Cu]CAP‐3) as potential PET tracers for uPA visualization in mouse tumor models, assessing their binding ability, specificity, and pharmacokinetic profiles. Among them, [⁶⁴Cu]CAP‐1, featuring a native disulfide bond, emerged as the optimal candidate. This radioligand demonstrated superior tumor uptake and reduced hepatic accumulation compared to the clinically advanced uPAR‐targeted tracer [⁶⁴Cu]DOTA‐AE105, currently in Phase 2 trials. A single administration of [⁶⁴Cu]CAP‐1 (2 mCi/mouse) significantly suppressed tumor growth and prolonged survival in mouse models. These findings position [⁶⁴Cu]CAP‐1 as a potent radiotheranostic agent for uPA‐overexpressing tumors, offering a novel strategy for precision targeting of the uPA/uPAR axis.
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