Radio-labeled somatostatin analogs have recently gained popularity as agents useful in intraoperative tumor localization, external scintigraphy and in situ radiotherapy. We have synthesized and characterized a series of novel N-terminally extended multiply-tyrosinated somatostatin analogs that possess high binding affinity for somatostatin receptors, exhibit biological activity comparable to the native peptide and retain these characteristics after iodination. These analogs can be radio-iodinated to high specific activities. Following radio-iodination, these analogs exhibit minimal radiolysis and may be clinically useful for tumor localization, scanning and therapy.
Revised: November 10, 2005 |
Published: February 1, 1999
Citation
Woltering E.A., M.S. O'Dorisio, W.A. Murphy, F. Chen, G.J. Drouant, G.D. Espenan, and D.R. Fisher, et al. 1999.Synthesis and characterization of multiply-tyrosinated, multiply-iodinated somatostatin analogs.Journal of Peptide Research 53, no. 2:201-213. PNWD-SA-4658.