Synthesis and Evaluation of 18 F-Labeled Peptide for Gonadotropin-Releasing Hormone Receptor Imaging
The gonadotropin-releasing hormone (GnRH) receptor is overexpressed in the majority of tumors of the human reproductive system. The purpose of this study was to develop an 18 F-labeled peptide for tumor GnRH receptor imaging. In this study, the GnRH (pGlu 1 -His 2 -Trp 3 -Ser 4 -Tyr 5 -Gly 6 -Leu 7...
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Veröffentlicht in: | Contrast media and molecular imaging 2019-03, Vol.2019, p.1-10 |
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Sprache: | eng |
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Zusammenfassung: | The gonadotropin-releasing hormone (GnRH) receptor is overexpressed in the majority of tumors of the human reproductive system. The purpose of this study was to develop an
18
F-labeled peptide for tumor GnRH receptor imaging. In this study, the GnRH (pGlu
1
-His
2
-Trp
3
-Ser
4
-Tyr
5
-Gly
6
-Leu
7
-Arg
8
-Pro
9
-Gly
10
-NH
2
) peptide analogues FP-
D
-Lys
6
-GnRH (FP = 2-fluoropropanoyl) and NOTA-P-
D
-Lys
6
-GnRH (
P
= ethylene glycol) were designed and synthesized. The IC
50
values of FP-
D
-Lys
6
-GnRH and NOTA-P-
D
-Lys
6
-GnRH were 2.0 nM and 56.2 nM, respectively. 4-Nitrophenyl-2-[
18
F]fluoropropionate was conjugated to the
ε
-amino group of the
D
-lysine side chain of
D
-Lys
6
-GnRH to yield the new tracer [
18
F]FP-
D
-Lys
6
-GnRH with a decay-corrected yield of 8 ± 3% and a specific activity of 20−100 GBq/
µ
mol (
n
=
6
). Cell uptake studies of [
18
F]FP-
D
-Lys
6
-GnRH in GnRH receptor-positive PC-3 cells and GnRH receptor-negative CHO-K1 cells indicated receptor-specific accumulation. Biodistribution and PET studies in nude mice bearing PC-3 xenografted tumors showed that [
18
F]FP-
D
-Lys
6
-GnRH was localized in tumors with a higher uptake than in surrounding muscle and heart tissues. Furthermore, the metabolic stability of [
18
F]FP-
D
-Lys
6
-GnRH was determined in mouse blood and PC-3 tumor homogenates at 1 h after tracer injection. The presented results indicated a potential of the novel tracer [
18
F]FP-
D
-Lys
6
-GnRH for tumor GnRH receptor imaging. |
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ISSN: | 1555-4309 1555-4317 |
DOI: | 10.1155/2019/5635269 |