Pre-clinical studies of EC2629, a highly potent folate- receptor-targeted DNA crosslinking agent

Author:

Reddy Joseph A.,Nelson Melissa,Dircksen Christina,Vetzel Marilynn,Johnson Theresa,Cross Vicky,Westrick Elaine,Qi LongWu,Hahn Spencer,Santhapuram Hari Krishna,Parham Garth,Wang Kevin,Vaughn Jeremy F.,Felten Albert,Pugh Michael,Lu June,Klein Patrick,Vlahov Iontcho R.,Leamon Christopher P.

Abstract

AbstractFolate receptor (FR)-targeted small molecule drug conjugates (SMDCs) have shown promising results in early stage clinical trials with microtubule destabilizing agents, such as vintafolide and EC1456. In our effort to develop FR-targeted SMDCs with varying mechanisms of action, we synthesized EC2629, a folate conjugate of a DNA crosslinking agent based on a novel DNA-alkylating moiety. This agent was found to be extremely potent with an in vitro IC50 ~ 100× lower than folate SMDCs constructed with various microtubule inhibitors. EC2629 treatment of nude mice bearing FR-positive KB human xenografts led to cures in 100% of the test animals with very low dose levels (300 nmol/kg) following a convenient once a week schedule. The observed activity was not accompanied by any noticeable weight loss (up to 20 weeks post end of dosing). Complete responses were also observed against FR-positive paclitaxel (KB-PR) and cisplatin (KB-CR) resistant models. When evaluated against FR-positive patient derived xenograft (PDX) models of ovarian (ST070), endometrial (ST040) and triple negative breast cancers (ST502, ST738), EC2629 showed significantly greater anti-tumor activity compared to their corresponding standard of care treatments. Taken together, these studies thus demonstrated that EC2629, with its distinct DNA reacting mechanism, may be useful in treating FR-positive tumors, including those that are classified as drug resistant.

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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