Preclinical comparison of (111)In-labeled DTPA- or DOTA-bombesin analogs for receptor-targeted scintigraphy and radionuclide therapy

Wouter A P Breeman; Marion de Jong; Jack L Erion; Joseph E Bugaj; Ananth Srinivasan; Bert F Bernard; Dik J Kwekkeboom; Theo J Visser; Eric P Krenning

Preclinical comparison of (111)In-labeled DTPA- or DOTA-bombesin analogs for receptor-targeted scintigraphy and radionuclide therapy

J Nucl Med. 2002 Dec;43(12):1650-6.

Authors

Wouter A P Breeman¹, Marion de Jong, Jack L Erion, Joseph E Bugaj, Ananth Srinivasan, Bert F Bernard, Dik J Kwekkeboom, Theo J Visser, Eric P Krenning

Affiliation

¹ Department of Nuclear Medicine, Erasmus University Medical Center Rotterdam, Rotterdam, The Netherlands. breeman@nuge.azr.nl

PMID: 12468515

Abstract

The 14-amino-acid peptide bombesin (BN) has a high affinity for the gastrin-releasing peptide (GRP) receptor that is expressed by a variety of tumors. Recently, high densities of GRP receptors were identified by in vitro receptor autoradiography in human prostate and breast carcinomas using [(125)I-Tyr(4)]BN as radioligand. Radiometal-labeled diethylenetriaminepentaacetic acid (DTPA)-BN derivatives are potentially useful radioligands for receptor-targeted scintigraphy and radiotherapy of GRP receptor-expressing tumors.

Methods: [DTPA-Pro(1),Tyr(4)]BN (A), [DOTA-Pro(1),Tyr(4)]BN (B), [DTPA-epsilon-Lys(3),Tyr(4)]BN (C), and [DOTA-epsilon-Lys(3),Tyr(4)]BN (D) (where DOTA is dodecanetetraacetic acid) were synthesized and studied for competition with binding of [(125)I-Tyr(4)]BN to the GRP receptor. The (111)In-labeled BN analogs were studied in vitro for binding and internalization by GRP receptor-expressing CA20948 and AR42J pancreatic tumor cells as well as in vivo for tissue distribution in rats. Specific tissue binding was tested by coinjection of 0.1 mg [Tyr(4)]BN.

Results: All BN analogs competitively inhibited the binding of [(125)I-Tyr(4)]BN to the GRP receptor with 50% inhibitory concentration values in the range of 2-9 nmol/L. All (111)In-labeled analogs showed high and specific time- and temperature-dependent binding and internalization by CA20948 and AR42J cells. In in vivo studies, high and specific binding was found in GRP receptor-positive tissues such as pancreas (0.90, 1.2, 0.54, and 0.79 percentage injected dose per gram for A-D, respectively). In a rat model, the AR42J tumor could clearly be visualized by scintigraphy using [(111)In-DTPA-Pro(1),Tyr(4)]BN as the radioligand. Although [(111)In-DOTA-Pro(1),Tyr(4)]BN showed the highest uptake of radioactivity in GRP receptor-positive tissues as well as higher target-to-blood ratios, [(111)In-DTPA-Pro(1),Tyr(4)]BN was easier to handle and is more practical to use. Therefore, we decided to start phase I studies with this DTPA-conjugated radioligand.

Conclusion: [(111)In-DTPA-Pro(1),Tyr(4)]BN is a promising radioligand for scintigraphy of GRP receptor-expressing tumors. We are currently performing a phase I study on patients with invasive prostate carcinoma.

Publication types

Comparative Study

MeSH terms

Amino Acid Sequence
Animals
Bombesin / analogs & derivatives*
Indium Radioisotopes* / therapeutic use
Male
Molecular Sequence Data
Pentetic Acid*
Radiopharmaceuticals*
Rats
Receptors, Bombesin / analysis*
Tissue Distribution

Substances

DTPA-Pro(1),Tyr(4)bombesin
Indium Radioisotopes
Radiopharmaceuticals
Receptors, Bombesin
Pentetic Acid
Bombesin