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Unité de recherche
PCRD EU
Numéro de projet
96.0447-3
Titre du projet
Development of novel peptide based radiopharmaceuticals for in vivo receptor associated tumor diagnosis and therapy
Titre du projet anglais
Development of novel peptide based radiopharmaceuticals for in vivo receptor associated tumor diagnosis and therapy

Textes relatifs à ce projet
 AllemandFrançaisItalienAnglais
Mots-clé
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Description succincte
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Références bases de données
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Textes saisis


CatégorieTexte
Mots-clé
(Anglais)
Peptide receptors; neurotensin; bombesin; human cancers; tumor targeting
Autre Numéro de projet
(Anglais)
EU project number: BMH4-CT98-3198
Programme de recherche
(Anglais)
EU-programme: 4. Frame Research Programme - 4.2 Agriculture and agroindustry
Description succincte
(Anglais)
See abstract
Partenaires et organisations internationales
(Anglais)
Coordinator: Forschungszentrum Rossendorf e.V. (D)
Résumé des résultats (Abstract)
(Anglais)
The high expression of neurotensin (NT) receptors in pancreatic cancer and of gastrin-releasing peptide (GRP) receptors in breast and prostate cancers strongly suggests that these tumors may be targeted in vivo with adequate peptide radioligands. In vitro binding properties of novel peptide-based radiopharmaceuticals were evaluated in human GRP and NT receptor-expressing tumors using in vitro receptor autoradiography with either 125I-Tyr3-NT or 125I-Tyr4-bombesin as radioligands.
In GRP-expressing prostate cancers we found excellent binding affinities for the following chelator-linked bombesin analogs: Demotide 1 [(N4-Bzl-NH-diG-[D-Phe6,Leu-NHEt13,des-Met14]-BN(6-14)] and Demotide 2 [(N4-CO-[D-Phe6,Leu-NHEt13,des-Met14]-BN(6-14)] had an IC50 of 2.6 nM ± 0.2 (n = 6) and 9.2 nM ± 2.7 (n = 6) respectively. Also 185/187 Re-PADA-AVA-bombesin(7-14) had an excellent IC50 of 4.9 nM ± 0.3 (n = 2), comparable to natural bombesin (4.5 nM ± 0.2 (n = 21)).
In NT receptor-expressing colon cancers and pancreatic cancers we found excellent affinities for the following stabilized NT radiopharmaceuticals: Demotide 4 [N4-Gly-Arg-y-Arg-Pro-Tyr-Tle-Leu] had an IC50 of 2.9 nM ± 0.4 (n = 4); the stabilized fluorobenzoyl (FB) neurotensin analogs [FB-Arg8y(CH2NH)Arg9]-NT(8-13) and [FB-Arg8y(CH2NH)Arg9-Tle12]-NT(8-13) had IC50's of respectively 0.91 nM ± 0.2 (n = 6) and 4.1 nM ± 0.6 (n = 6). Finally, four different Rhenium-labeled neurotensin analogs had binding affinities of 3.1 nM ± 0.1 (n = 4) [(NaHis)Ac-Lys-(yCH2NH)-Arg-Pro-Tyr-Tle-Leu], 0.77 nM ± 0.2 (n = 4) [(NaHis)Ac-Arg-(N-CH3)-Arg-Pro-Tyr-Tle-Leu], 2.1 nM ± 0.4 (n = 4) [(NaHis)Ac-bArg-Lys-Pro-Tyr-Tle-Leu] and 1.2 nM ± 0.2 (n = 4) [(NaHis)Ac-(N-CH3)-Arg-Lys-Pro-Tyr-Tle-Leu].
These results show that various stabilized peptide radiopharmaceuticals that can be labeled with different isotopes can successfully be developed; with their high binding affinity to human GRP and NT receptors, they are good candidates for in vivo targeting of GRP and NT receptor-positive human tumors.
Références bases de données
(Anglais)
Swiss Database: Euro-DB of the
State Secretariat for Education and Research
Hallwylstrasse 4
CH-3003 Berne, Switzerland
Tel. +41 31 322 74 82
Swiss Project-Number: 96.0447-3