Magnetic resonance imaging of RRx-001 pharmacodynamics in preclinical tumors

Natarajan Raghunand _, Jan Scicinski, Gerald P. Guntle, Bhumasamudram Jagadish, Eugene A. Mash, Elizabeth Bruckheimer, Bryan Oronsky and Ronald L. Korn

Abstract

ABSTRACT

RRx-001 is an anticancer agent that subjects cancer cells to reactive oxygen/nitrogen species (ROS/RNS) and acts as an epigenetic modifier. We have used a thiol-bearing MRI contrast agent, Gd-LC7-SH, to investigate the pharmacodynamics of RRx-001 in CHP-100 Ewing’s Sarcoma, HT-29 colorectal carcinoma, and PANC-1 pancreatic carcinoma xenografts in SCID mice. Binding of Gd-LC7-SH to the Cys³⁴ residue on plasma albumin prolongs retention in the tumor microenvironment and increases tumor enhancement on MRI. Mice were imaged by MRI and in vivo T1 maps acquired 50 min (T1_{50 min}) after injection of 0.05 mmol/kg Gd-LC7-SH (i.v.) at baseline and 1, 24, and 72 h post-treatment with 10 mg/kg RRx-001 (i.v.). Consistent with an indirect thiol-modifying activity of RRx-001, tumor T1_{50 min} at 1 h post-drug was significantly longer than pre-drug tumor T1_{50 min} in all three tumor models, with the T1_{50 min} remaining significantly longer than baseline through 72 h post-drug in the HT-29 and PANC-1 tumors. The T1_{50 min} of CHP-100 tumors recovered to baseline by 24 h post-drug, suggesting a robust anti-oxidant response to the RRx-001 challenge that was presaged by a marked increase in perfusion at 1 h post-drug measured by DCE-MRI. MRI enhanced with Gd-LC7-SH provides a mechanistically rational biomarker of RRx-001 pharmacodynamics.

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PII: 18455