68Ga-Complex Lipophilicity and the Targeting Property of a Urea-Based PSMA Inhibitor for PET Imaging
Matthias Eder
1
,
Martin Schäfer
2
,
Ulrike Bauder-Wüst
2
,
William Edmund Hull
2
,
Carmen Wängler
3
,
WE Haefeli
4
,
Uwe Haberkorn
4
,
Michael Eisenhut
5
3
Department of Nuclear Medicine, University Hospital Munich, Munich, Germany
|
5
Imaging and Radiooncology
Publication type: Journal Article
Publication date: 2012-03-13
scimago Q1
wos Q1
SJR: 1.035
CiteScore: 7.5
Impact factor: 3.9
ISSN: 10431802, 15204812
PubMed ID:
22369515
Organic Chemistry
Pharmacology
Pharmaceutical Science
Biotechnology
Bioengineering
Biomedical Engineering
Abstract
Urea-based inhibitors of the prostate-specific membrane antigen (PSMA) represent low-molecular-weight pepidomimetics showing the ability to image PSMA-expressing prostate tumors. The highly efficient, acyclic Ga(III) chelator N,N'-bis [2-hydroxy-5-(carboxyethyl)benzyl] ethylenediamine-N,N'- diacetic acid (HBED-CC) was introduced as a lipophilic side chain into the hydrophilic pharmacophore Glu-NH-CO-NH-Lys which was found favorable to interact with the PSMA "active binding site". This report describes the syntheses, in vitro binding analyses, and biodistribution data of the radiogallium labeled PSMA inhibitor Glu-NH-CO-NH-Lys(Ahx)-HBED-CC in comparison to the corresponding DOTA conjugate. The binding properties were analyzed using competitive cell binding and enzyme-based assays followed by internalization experiments. Compared to the DOTA-conjugate, the HBED-CC derivative showed reduced unspecific binding and considerable higher specific internalization in LNCaP cells. The (68)Ga complex of the HBED-CC ligand exhibited higher specificity for PSMA expressing tumor cells resulting in improved in vivo properties. (68)Ga labeled Glu-NH-CO-NH-Lys(Ahx)-HBED-CC showed fast blood and organ clearances, low liver accumulation, and high specific uptake in PSMA expressing organs and tumor. It could be demonstrated that the PET-imaging property of a urea-based PSMA inhibitor could significantly be improved with HBED-CC.
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Eder M. et al. 68Ga-Complex Lipophilicity and the Targeting Property of a Urea-Based PSMA Inhibitor for PET Imaging // Bioconjugate Chemistry. 2012. Vol. 23. No. 4. pp. 688-697.
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Eder M., Schäfer M., Bauder-Wüst U., Hull W. E., Wängler C., Haefeli W., Haberkorn U., Eisenhut M. 68Ga-Complex Lipophilicity and the Targeting Property of a Urea-Based PSMA Inhibitor for PET Imaging // Bioconjugate Chemistry. 2012. Vol. 23. No. 4. pp. 688-697.
Cite this
RIS
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TY - JOUR
DO - 10.1021/bc200279b
UR - https://doi.org/10.1021/bc200279b
TI - 68Ga-Complex Lipophilicity and the Targeting Property of a Urea-Based PSMA Inhibitor for PET Imaging
T2 - Bioconjugate Chemistry
AU - Eder, Matthias
AU - Schäfer, Martin
AU - Bauder-Wüst, Ulrike
AU - Hull, William Edmund
AU - Wängler, Carmen
AU - Haefeli, WE
AU - Haberkorn, Uwe
AU - Eisenhut, Michael
PY - 2012
DA - 2012/03/13
PB - American Chemical Society (ACS)
SP - 688-697
IS - 4
VL - 23
PMID - 22369515
SN - 1043-1802
SN - 1520-4812
ER -
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@article{2012_Eder,
author = {Matthias Eder and Martin Schäfer and Ulrike Bauder-Wüst and William Edmund Hull and Carmen Wängler and WE Haefeli and Uwe Haberkorn and Michael Eisenhut},
title = {68Ga-Complex Lipophilicity and the Targeting Property of a Urea-Based PSMA Inhibitor for PET Imaging},
journal = {Bioconjugate Chemistry},
year = {2012},
volume = {23},
publisher = {American Chemical Society (ACS)},
month = {mar},
url = {https://doi.org/10.1021/bc200279b},
number = {4},
pages = {688--697},
doi = {10.1021/bc200279b}
}
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Eder, Matthias, et al. “68Ga-Complex Lipophilicity and the Targeting Property of a Urea-Based PSMA Inhibitor for PET Imaging.” Bioconjugate Chemistry, vol. 23, no. 4, Mar. 2012, pp. 688-697. https://doi.org/10.1021/bc200279b.