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Cu-1,4,7,10-Tetraazacyclododecane-,,,-tetraacetic acid-E(E{E[c(RGDyK)]}) peptide

作者信息

Cheng Kenneth T.

机构信息

National Center for Biotechnology Information, NLM, NIH, Bethesda, MD,

出版信息


DOI:
PMID:20641736
Abstract

Cu-1,4,7,10-Tetraazacyclododecane-,,,-tetraacetic acid-E(E{E[c(RGDyK)}) peptide (Cu-DOTA-RGD octamer) is an integrin-targeted molecular imaging agent developed for positron emission tomography (PET) imaging of tumor vasculature, tumor angiogenesis, and osteoclasts (1). Cu is a positron emitter with a half-life () of 12.7 h. Cellular survival, invasion, and migration control embryonic development, angiogenesis, tumor metastasis, and other physiological processes (2, 3). Among the molecules that regulate angiogenesis are integrins, which comprise a superfamily of cell adhesion proteins that form heterodimeric receptors for extracellular matrix (ECM) molecules (4, 5). These transmembrane glycoproteins consist of two noncovalently associated subunits, α and β (18 α- and 8 β-subunits in mammals), which are assembled into at least 24 α/β pairs. Several integrins, such as integrin αβ, have affinity for the arginine-glycine-aspartic acid (RGD) tripeptide motif, which is found in many ECM proteins. Expression of integrin αβ receptors on endothelial cells is stimulated by angiogenic factors and environments. The integrin αβ receptor is generally not found in normal tissue but it is strongly expressed in vessels with increased angiogenesis, such as tumor vasculature. It is significantly upregulated in certain types of tumor cells and in almost all tumor vasculature. Molecular imaging probes carrying the RGD motif that binds to the integrin αβ can be used to image tumor vasculature and evaluate angiogenic response to tumor therapy (6, 7). Various RGD peptides in both linear and cyclic forms have been developed for binding to integrin αβ (8). It has been hypothesized that cyclic RGD peptides (RGDfK or RGDyK) may have a faster rate of receptor binding or a slower rate of dissociation from the integrin αβ than linear single-RGD peptides (9). Chen et al. (10) evaluated a cyclic RGD D-Tyr analog peptide [c(RGDyK)] labeled with Cu or F in nude mice bearing breast tumors. They used DOTA for c(RGDyK) conjugation with Cu, and Cu-DOTA-c(RGDyK) showed prolonged tumor radioactivity retention but persistent liver radioactivity. Wu et al. (9) suggested that a multimeric RGD peptide with more than two repeating cyclic RGD units would further enhance the affinity of the receptor−ligand interactions through the phenomenon of polyvalency. They also suggested that the increase in molecular size might prolong circulation time and reduce tumor washout rate. Consequently, Wu et al. (9) developed a tetrameric RGD D-Phe analog peptide, Cu-DOTA-E{E[c(RGDfK)}, and they showed that this PET radioligand appeared to have high integrin avidity and favorable biokinetics in nude mice bearing human gliomas. Using the same approach, Li et al. (1) synthesized and evaluated both Cu-DOTA-RGD tetramer and Cu-DOTA-RGD octamer.

摘要

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