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Jaspreet Singh Jaggi, Jorge A. Carrasquillo, Surya V. Seshan, Pat Zanzonico, Erik Henke, Andrew Nagel, Jazmin Schwartz, Brad Beattie, Barry J. Kappel, Debjit Chattopadhyay, Jing Xiao, George Sgouros, Steven M. Larson, David A. Scheinberg
Published in Volume 117, Issue 9
J Clin Invest. 2007; 117(9):2422–2430 doi:10.1172/JCI32226
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Figure 2
High-dose IgG administration enhances blood clearance and tumor-to-blood contrast in immuno-PET imaging without affecting the uptake of radiolabeled antibody in the tumor.

(A and B) Organ distribution of 111In activity at 72 hours after injection with 111In-cG250 (A) or 111In-A33 (B). IgG administration (1 g/kg i.p.; administered 24 hours after 111In-antibody) decreased the blood and renal 111In activity without affecting the tumor uptake. Data are mean ± SEM. (C and E) PET images of representative tumor xenograft-bearing mice at the indicated time points following injection with 124I-labeled cG250 (C) or A33 (E) antibody. (D) Excised tumors from mice in C. Enhanced tumor-to-blood contrast was seen in mice that received 1 g/kg human IgG, either 24 hours (C) or 6 hours (E) following 124I-antibody injection. H, heart; T, tumor; B, urinary bladder.