Investigations on the Usefulness of CEACAMs as Potential Imaging Targets for Molecular Imaging Purposes | Zendy

Markus Heine | Zendy; Peter Nollau | Zendy; Christoph Maßlo | Zendy; Peter Nielsen | Zendy; Barbara Freund | Zendy; Oliver T. Bruns | Zendy; Rudolph Reimer | Zendy; Heinrich Hohenberg | Zendy; Kersten Peldschus | Zendy; Harald Ittrich | Zendy; Udo Schumacher | Zendy

AI Assistant Blog Pricing

Home ZAIA Blog

Open Access

Investigations on the Usefulness of CEACAMs as Potential Imaging Targets for Molecular Imaging Purposes

Author(s) -

Markus Heine,

Peter Nollau,

Christoph Maßlo,

Peter Nielsen,

Barbara Freund,

Oliver T. Bruns,

Rudolph Reimer,

Heinrich Hohenberg,

Kersten Peldschus,

Harald Ittrich,

Udo Schumacher

Publication year - 2011

Publication title -

plos one

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.99

H-Index - 332

ISSN - 1932-6203

DOI - 10.1371/journal.pone.0028030

Subject(s) - molecular imaging , medicine , computational biology , biology , genetics , in vivo

Members of the carcinoembryonic antigen cell adhesion molecules (CEACAMs) family are the prototype of tumour markers. Classically they are used as serum markers, however, CEACAMs could serve as targets for molecular imaging as well. In order to test the anti CEACAM monoclonal antibody T84.1 for imaging purposes, CEACAM expression was analysed using this antibody. Twelve human cancer cell lines from different entities were screened for their CEACAM expression using qPCR, Western Blot and FACS analysis. In addition, CEACAM expression was analyzed in primary tumour xenografts of these cells. Nine of 12 tumour cell lines expressed CEACAM mRNA and protein when grown in vitro . Pancreatic and colon cancer cell lines showed the highest expression levels with good correlation of mRNA and protein level. However, when grown in vivo , the CEACAM expression was generally downregulated except for the melanoma cell lines. As the CEACAM expression showed pronounced expression in FemX-1 primary tumours, this model system was used for further experiments. As the accessibility of the antibody after i.v. application is critical for its use in molecular imaging, the binding of the T84.1 monoclonal antibody was assessed after i.v. injection into SCID mice harbouring a FemX-1 primary tumour. When applied i.v., the CEACAM specific T84.1 antibody bound to tumour cells in the vicinity of blood vessels. This binding pattern was particularly pronounced in the periphery of the tumour xenograft, however, some antibody binding was also observed in the central areas of the tumour around blood vessels. Still, a general penetration of the tumour by i.v. application of the anti CEACAM antibody could not be achieved despite homogenous CEACAM expression of all melanoma cells when analysed in tissue sections. This lack of penetration is probably due to the increased interstitial fluid pressure in tumours caused by the absence of functional lymphatic vessels.

The content you want is available to Zendy users.

Already have an account? Click here to sign in.

Having issues? You can contact us here

Accelerating Research