1 research outputs found
Strand breakage by decay of DNA-bound <sup>124</sup>I provides a basis for combined PET imaging and Auger endoradiotherapy
<p><b>Purpose</b> DNA ligands labelled with <sup>125</sup>I induce cytotoxic DNA double-strand breaks (DSB), suggesting a potential for Auger endoradiotherapy. Since the 60-day half-life of <sup>125</sup>I is suboptimal for therapy, we have investigated another Auger-emitter <sup>124</sup>I, with shorter half-life (4.18 days), and the additional feature of positron-emission, enabling positron emission tomography (PET) imaging. The purpose of this study was to compare the two radionuclides on the basis of DNA DSB per decay.</p> <p><b>Materials and methods</b> Using a <sup>124</sup>I- (or <sup>125</sup>I)-labelled minor groove binding DNA ligand, we investigated DNA breakage using the plasmid DNA assay. Biodistribution of the conjugate of the labelled ligand with transferrin was investigated in nude mice bearing a K562 human lymphoma xenograft.</p> <p><b>Results</b> The probability of DSB per decay was 0.58 and 0.85 for <sup>124</sup>I and <sup>125</sup>I, respectively, confirming the therapeutic potential of the former. The crystal structure of the ligand DNA complex shows the iodine atom deep within the minor groove, consistent with the high efficiency of induced damage. Biodistribution studies, including PET imaging, showed distinctive results for the conjugate, compared to the free ligand and transferrin, consistent with receptor-mediated delivery of the ligand.</p> <p><b>Conclusions</b> Conjugation of <sup>124</sup>I-labelled DNA ligands to tumor targeting peptides provides a feasible strategy for Auger endoradiotherapy, with the advantage of monitoring tumor targeting by PET imaging.</p