In vitro and in vivo comparison of DTPA- and DOTA-conjugated antiferritin monoclonal antibody for imaging and therapy of pancreatic cancer

Sabbah, Emmanuelle N.; Kadouche, Jean; Ellison, David; Finucane, Ciara; Decaudin, Didier; Mather, Stephen J.

doi:10.1016/j.nucmedbio.2007.01.004

« Previous Next »Nuclear Medicine and Biology
Volume 34, Issue 3 , Pages 293-304, April 2007

In vitro and in vivo comparison of DTPA- and DOTA-conjugated antiferritin monoclonal antibody for imaging and therapy of pancreatic cancer

Emmanuelle N. Sabbah
- M.A.T., Génocampus 1, 5 rue Henri Desbrvères, 91030 Evry cedex, France
- Nuclear Medicine Research Laboratory, St Bartholomew's Hospital, EC1A 7BE London, United Kingdom
- Corresponding author. Nuclear Medicine Research Laboratory, St Bartholomew's Hospital, London EC1A 7BE, United Kingdom. Tel.: + 44 0 207 601 71 51; fax +44 0 207 601 71 43.
Jean Kadouche
- M.A.T., Génocampus 1, 5 rue Henri Desbrvères, 91030 Evry cedex, France
David Ellison
- Nuclear Medicine Research Laboratory, St Bartholomew's Hospital, EC1A 7BE London, United Kingdom
Ciara Finucane
- Nuclear Medicine Research Laboratory, St Bartholomew's Hospital, EC1A 7BE London, United Kingdom
Didier Decaudin
- Institut Curie, Clinical Haematology, 75005 Paris, France
Stephen J. Mather
- Nuclear Medicine Research Laboratory, St Bartholomew's Hospital, EC1A 7BE London, United Kingdom

Received 24 November 2006; received in revised form 26 December 2006; accepted 5 January 2007.

Abstract

Pancreatic cancer has a very poor prognosis with a less than 5% survival rate at 5 years. Neither external beam radiation nor chemotherapy, alone or in combination, have given encouraging results so far. A possible solution might come from the use of targeted therapy such as radioimmunotherapy. We present here the results obtained from the preclinical development of a new monoclonal antiferritin antibody (Ab), AMB8LK. Ferritin is overexpressed in pancreatic cancer and could thus be used as a target for the delivery of radioactivity at the tumour sites. The AMB8LK Ab was conjugated to three chelating agents: the 2-(4-isothiocyanatobenzyl)-diethylenetriamine pentaacetic acid (PSCN-Bz-DTPA), the (R)-2-amino-3-(4-isothiocyanatophenyl)propyl]-trans-(S,S)-cyclohexane-1,2-diamine-pentaacetic acid (p5CN-Bz-CHX-Aʺ-DTPA) and the 2-(4-isothiocyanatobenzyl)-1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid (pSCN-Bz-DOTA). Radiolabelling of the three immunoconjugates with indium 111 and yttrium 90 as well as in vitro stability and immunoreactivity against pure ferritin and cells expressing ferritin were analysed. In vivo biodistribution studies were conducted on normal and on human pancreatic adenocarcinoma CAPAN-1 tumour bearing mice. These experiments demonstrated good radiolabelling (>95%), stability and immunoreactivity of the three compounds. In the biodistribution studies, differences between the three immunoconjugates were apparent in the rate of blood clearance and in tumour, liver and bone uptake. A very good pancreatic adenocarcinoma tumour targeting was observed especially with the Bz-DTPA-AMB8LK: 20% of the injected dose of the indium-labelled compound 3 days after injection; 15% of the injected dose 5 days after that of the yttrium-labelled Ab. Altogether, these results in animal models suggest that ⁹⁰Y-Bz-DTPA-AMB8LK is a good candidate for further therapeutic efficacy studies.

Keywords: Ferritin, Monoclonal antibody, Bifunctional ligand, Pancreatic cancer, Biodistribution