Synthesis, in silico and biodistribution studies of a novel 47Sc-radiolabeled α-amino acid ester derivative attached to pyrazine and tetrazole rings for tumor targeted radiotherapy

Author:

Gizawy Mohamed A.1ORCID,Shamsel-Din Hesham A.1,El-Tahawy Mohsen M. T.2,Ibrahim Ayman A.3

Affiliation:

1. Labeled Compounds Department, Hot Labs Center , Egyptian Atomic Energy Authority , P.O. Box 13759 , Cairo , Egypt

2. Chemistry Department, Faculty of Science , Damanhour University , P.O. Box 22511 , Damanhour , Egypt

3. Drug Radiation Research Department , National Center for Radiation Research and Technology (NCRRT), Egyptian Atomic Energy Authority , Cairo , Egypt

Abstract

Abstract Recently, tumor-targeted radionuclide therapy has gained much recognition for the treatment of metastasized cancer. There is a growing interest in using the theranostic radionuclide 47Sc, owing to its excellent chemical and nuclear properties. However, the available chelating agents require a relatively high temperature for their radiolabeling, which could denature biomolecules. The aim of the present study is to synthesize a dipeptide agent that forms a thermodynamically more stable complex with 47Sc at room temperature. A novel α-amino acid ester derivative attached to pyrazine and tetrazole heterocyclic rings has been prepared by the azide coupling method. Different spectroscopic methods (FT-IR, 1H NMR, and mass spectra) were used for characterization of the target compound. The newly synthesized dipeptide was radiolabeled with 47Sc, and a high radiochemical yield of 98.5 ± 1.5 % and in vitro serum stability up to 72 h were attained at room temperature within 20 min. The quantum chemical calculations at B3PW91/6-31G(d) level were employed to establish the molecular structure of the dipeptide and its complexation with 47Sc. The selectivity of 47Sc-dipeptide toward localization in tumor cells was performed by molecular docking on different receptors in addition to in vivo biodistribution on solid tumor-bearing mice. A high T/NT ratio of 8.16 was obtained after 4 h p.i, suggesting that this complex could be used as a potential cancer theranostic agent.

Publisher

Walter de Gruyter GmbH

Reference43 articles.

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