4.4 Article

64Cu-Labeled Affibody Molecules for Imaging of HER2 Expressing Tumors

期刊

MOLECULAR IMAGING AND BIOLOGY
卷 12, 期 3, 页码 316-324

出版社

SPRINGER
DOI: 10.1007/s11307-009-0256-6

关键词

Affibody; HER2; PET; Imaging; Cu-64

资金

  1. National Cancer Institute (NCI) [R24 CA93862]
  2. In Vivo Cellular Molecular Imaging Center (ICMIC) [P50 CA114747]
  3. General Electric Global Research

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The development of molecular probes based on novel engineered protein constructs is under active investigation due to the great potential of this generalizable strategy for imaging a variety of tumor targets. In this report, human epidermal growth factor receptor type 2 (HER2)-binding Affibody molecules were radiolabeled with Cu-64 and their imaging ability was further evaluated in tumor mice models to understand the promise and limitations of such probes. The anti-HER2 Affibody molecules in monomeric (Z(HER2:477)) and dimeric [(Z(HER2:477))(2)] forms were site specifically modified with the maleimide-functionalized chelator, 1,4,7,10-tetraazacyclododecane-1,4,7-tris(acetic acid)-10-acetate mono (N-ethylmaleimide amide) (Mal-DOTA). The resulting DOTA-Affibody conjugates were radiolabeled with Cu-64 and evaluated in nude mice bearing subcutaneous SKOV3 tumors. Biodistribution experiments showed that tumor uptake values of Cu-64-DOTA-Z(HER2:477) and Cu-64-DOTA-(Z(HER2:477))(2) were 6.12 +/- 1.44% and 1.46 +/- 0.50% ID/g, respectively, in nude mice (n = 3 each) at 4 h postinjection. Moreover, Cu-64-labeled monomer exhibited significantly higher tumor/blood ratio than that of radiolabeled dimeric counterpart at all time points examined in this study. MicroPET imaging of Cu-64-DOTA-Z(HER2:477) in SKOV3 tumor mice clearly showed good and specific tumor localization. This study demonstrates that Cu-64-labeled Z(HER2:477) is a promising targeted molecular probe for imaging HER2 receptor expression in living mice. Further work is needed to improve the excretion properties, hence dosimetry and imaging efficacy, of the radiometal-based probe.

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