|
|
Blood, 1 June 2007, Vol. 109, No. 11, pp. 4980-4987.
Prepublished online as a Blood First Edition Paper on February 15, 2007; DOI 10.1182/blood-2006-11-056895.
 Previous Article | Table of Contents | Next Article 
NEOPLASIA
Comparative biodistributions of pretargeted radioimmunoconjugates targeting CD20, CD22, and DR molecules on human B-cell lymphomas
Anastasia Pantelias1,
John M. Pagel1,2,
Nathan Hedin1,
Laura Saganic1,
Shani Wilbur1,
Donald K. Hamlin3,
D. Scott Wilbur3,
Yukang Lin1,
Diane Stone1,
Don Axworthy4,
Ajay K. Gopal1,2, and
Oliver W. Press1,2,5
1 Fred Hutchinson Cancer Research Center, Seattle, WA;
2 Division of Oncology, University of Washington School of Medicine, Seattle, WA;
3 Department of Radiation Oncology, University of Washington, Seattle, WA;
4 Aletheon Pharmaceuticals, Inc, Seattle, WA;
5 Department of Biological Structure, University of Washington, Seattle, WA
Pretargeted radioimmunotherapy (PRIT) using streptavidin (SA)–conjugated antibodies (Abs), followed by clearing agent and radiolabeled biotin is a promising method that can increase the effectiveness of RIT, while decreasing the toxicities associated with directly labeled Abs. Although CD20 has been the traditional target antigen for RIT of non-Hodgkin lymphoma (NHL), studies targeting HLA DR and CD22 have yielded promising results. Targeting all 3 antigens at once may further augment the effect of PRIT. This study compares the targeting of Ramos, Raji, and FL-18 lymphoma xenografts with either anti-CD20 Ab/SA (1F5/SA), anti-HLA DR Ab/SA (Lym-1/SA), anti-CD22 Ab/SA (HD39/SA), or all 3 conjugates in combination, followed 24 hours later by a biotin-N-acetyl-galactosamine clearing agent, and 3 hours after that by 111In-DOTA-biotin. The Ab/SA conjugate yielding the best tumor uptake and tumor-to–normal organ ratios of radioactivity varied depending on the target antigen expression on the cell line used, with 1F5/SA and Lym-1/SA yielding the most promising results overall. Also, the best tumor-to–normal organ ratios of absorbed radioactivity were obtained using single conjugates optimized for target tumor antigen expression rather than the combination therapy. This study highlights the importance of screening the antigenic expression on lymphomas to select the optimal reagent for PRIT.
 CiteULike  Connotea  Del.icio.us  Digg  Reddit  Technorati What's this?
This article has been cited by other articles:
|
|
|
|
 
D. J. Green, J. M. Pagel, E. R. Nemecek, Y. Lin, A. Kenoyer, A. Pantelias, D. K. Hamlin, D. S. Wilbur, D. R. Fisher, J. G. Rajendran, et al.
Pretargeting CD45 enhances the selective delivery of radiation to hematolymphoid tissues in nonhuman primates
Blood,
August 6, 2009;
114(6):
1226 - 1235.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
|
|
J. M. Pagel, N. Orgun, D. K. Hamlin, D. S. Wilbur, T. A. Gooley, A. K. Gopal, S. I. Park, D. J. Green, Y. Lin, and O. W. Press
A comparative analysis of conventional and pretargeted radioimmunotherapy of B-cell lymphomas by targeting CD20, CD22, and HLA-DR singly and in combinations
Blood,
May 14, 2009;
113(20):
4903 - 4913.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
|
|
D. V. Gold, D. M. Goldenberg, H. Karacay, E. A. Rossi, C.-H. Chang, T. M. Cardillo, W. J. McBride, and R. M. Sharkey
A Novel Bispecific, Trivalent Antibody Construct for Targeting Pancreatic Carcinoma
Cancer Res.,
June 15, 2008;
68(12):
4819 - 4826.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
|
|
J. M. Pagel, N. Hedin, L. Drouet, B. L. Wood, A. Pantelias, Y. Lin, D. K. Hamlin, D. S. Wilbur, A. K. Gopal, D. Green, et al.
Eradication of disseminated leukemia in a syngeneic murine leukemia model using pretargeted anti-CD45 radioimmunotherapy
Blood,
February 15, 2008;
111(4):
2261 - 2268.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
|
|
D. J. Green, J. M. Pagel, A. Pantelias, N. Hedin, Y. Lin, D. S. Wilbur, A. Gopal, D. K. Hamlin, and O. W. Press
Pretargeted Radioimmunotherapy for B-Cell Lymphomas
Clin. Cancer Res.,
September 15, 2007;
13(18):
5598s - 5603s.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
