A Polar Substituent-Containing Acylation Agent for the Radioiodination of Internalizing Monoclonal Antibodies: N-Succinimidyl 4-Guanidinomethyl-3-[131I]iodobenzoate ([131I]SGMIB)

Abstract

The objective of this study was to develop an acylation agent for the radioiodination of monoclonal antibodies that would maximize retention of the label in tumor cells following receptor- or antigen-mediated internalization. The strategy taken was to add a polar substituent to the labeled aromatic ring to impede transport of labeled catabolites across lysosomal and cell membranes after antibody degradation. Preparation of unlabeled N-succinimidyl 4-guanidinomethyl-3-iodobenzoate (SGMIB) was achieved in six steps from 3-iodo-4-methylbenzoic acid. Preparation of 4-guanidinomethyl-3-[¹³¹I]iodobenzoic acid from the silicon precursor, 4-(N¹,N²-bis-tert-butyloxycarbonyl)guanidinomethyl-3-trimethylsilylbenzoic acid proceeded in less than 5% radiochemical yield. A more successful approach was to prepare [¹³¹I]SGMIB directly from the tin precursor, N-succinimidyl 4-(N¹,N²-bis-tert-butyloxycarbonyl)guanidinomethyl-3-trimethylstannylbenzoate, which was achieved in 60−65% radiochemical yield. A rapidly internalizing anti-epidermal growth factor receptor variant III antibody L8A4 was labeled using [¹³¹I]SGMIB in 65% conjugation efficiency and with preservation of immunoreactivity. Paired-label in vitro internalization assays demonstrated that the amount of radioactivity retained in cells after internalization for L8A4 labeled with [¹³¹I]SGMIB was 3−4-fold higher than that for L8A4 labeled with ¹²⁵I using either Iodogen or [¹²⁵I]SIPC. Catabolite assays documented that the increased retention of radioiodine in tumor cells for antibody labeled using [¹³¹I]SGMIB was due to positively charged, low molecular weight species. These results suggest that [¹³¹I]SGMIB warrants further evaluation as a reagent for labeling internalizing antibodies.