Open Access
Synthesis and preclinical evaluation of DOTAGA-conjugated PSMA ligands for functional imaging and endoradiotherapy of prostate cancer
Martina Weineisen
1
,
Jakub Šimeček
1
,
Margret Schottelius
1
,
Markus Schwaiger
2
,
Hans Jürgen Wester
1
Тип публикации: Journal Article
Дата публикации: 2014-11-25
scimago Q1
wos Q2
БС2
SJR: 0.940
CiteScore: 5.0
Impact factor: 3.0
ISSN: 2191219X
PubMed ID:
26116124
Radiology, Nuclear Medicine and imaging
Краткое описание
Due to its high expression in prostate cancer, PSMA (prostate-specific membrane antigen) represents an ideal target for both diagnostic imaging and endoradiotherapeutic approaches. Based on a previously published highly specific PSMA ligand ([68Ga]DOTA-FFK(Sub-KuE)), we developed a corresponding metabolically stable 1,4,7,10-tetraazacyclododececane,1-(glutaric acid)-4,7,10-triacetic acid (DOTAGA) construct for theranostic treatment of prostate cancer. All ligands were synthesized by a combined solid phase and solution phase synthesis strategy. The affinity of the natgallium and lutetium complexes to PSMA and the internalization efficiency of the radiotracers were determined on PSMA-expressing LNCaP cells. The 68Ga- and 177Lu-labelled ligands were further investigated for lipophilicity, binding specificity, metabolic stability, as well as biodistribution and μPET in LNCaP-tumour-bearing mice. Radiochemical yields for 68Ga (3 nmol, 5.0 M NaCl/2.7 M HEPES (approximately 5/1), pH 3.5 to 4.5, 5 min, 95°C) and 177Lu labelling (0.7 nmol, 0.1 M NH4OAc, pH 5.5, 30 min, 95°C) were almost quantitative, resulting in specific activities of 250 to 300 GBq/μmol for the 68Ga analogues and 38 GBq/μmol for 177Lu complexes. Due to metabolic instability of l-amino acid spacers, d-amino acids were implemented resulting in a metabolically stable DOTAGA ligand. Compared to the DOTA ligand, the DOTAGA derivatives showed higher hydrophilicity (logP = -3.6 ± 0.1 and -3.9 ± 0.1 for 68Ga and 177Lu, respectively) and improved affinity to PSMA resulting in an about twofold increased specific internalization of the 68Ga- and 177Lu-labelled DOTAGA analogue. Especially, [68Ga]DOTAGA-ffk(Sub-KuE) exhibits favourable pharmacokinetics, low unspecific uptake and high tumour accumulation in LNCaP-tumour-bearing mice. The pair of diagnostic/therapeutic PSMA-ligands [68Ga/177Lu]DOTAGA-ffk(Sub-KuE) possess remarkable potential for the management of prostate cancer.
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Weineisen M. et al. Synthesis and preclinical evaluation of DOTAGA-conjugated PSMA ligands for functional imaging and endoradiotherapy of prostate cancer // EJNMMI Research. 2014. Vol. 4. No. 1. 63
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Weineisen M., Šimeček J., Schottelius M., Schwaiger M., Wester H. J. Synthesis and preclinical evaluation of DOTAGA-conjugated PSMA ligands for functional imaging and endoradiotherapy of prostate cancer // EJNMMI Research. 2014. Vol. 4. No. 1. 63
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TY - JOUR
DO - 10.1186/s13550-014-0063-1
UR - https://doi.org/10.1186/s13550-014-0063-1
TI - Synthesis and preclinical evaluation of DOTAGA-conjugated PSMA ligands for functional imaging and endoradiotherapy of prostate cancer
T2 - EJNMMI Research
AU - Weineisen, Martina
AU - Šimeček, Jakub
AU - Schottelius, Margret
AU - Schwaiger, Markus
AU - Wester, Hans Jürgen
PY - 2014
DA - 2014/11/25
PB - Springer Nature
IS - 1
VL - 4
PMID - 26116124
SN - 2191-219X
ER -
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@article{2014_Weineisen,
author = {Martina Weineisen and Jakub Šimeček and Margret Schottelius and Markus Schwaiger and Hans Jürgen Wester},
title = {Synthesis and preclinical evaluation of DOTAGA-conjugated PSMA ligands for functional imaging and endoradiotherapy of prostate cancer},
journal = {EJNMMI Research},
year = {2014},
volume = {4},
publisher = {Springer Nature},
month = {nov},
url = {https://doi.org/10.1186/s13550-014-0063-1},
number = {1},
pages = {63},
doi = {10.1186/s13550-014-0063-1}
}