WATERTOWN, MA – April 21, 2015 – Blend Therapeutics, Inc., a biopharmaceutical company discovering and developing two distinct classes of targeted anti-cancer medicines to advance the treatment of patients with solid tumor cancers, presented preclinical data today on its lead Pentarin™ program, BTP-277, showing specific and potent targeting of tumor cells expressing the somatostatin receptor, which is known to be over expressed in small cell lung cancer (SCLC) and neuroendocrine cancer tumor cells. BTP-277 is the first in a series of proprietary drug candidates from Blend’s Pentarin™ platform, which creates miniaturized biologic drug conjugates (mBDCs) incorporated in polymeric nanoparticles that offer the potential for highly effective penetration and distribution of targeted anti-cancer treatment deep into the tumor tissue. The results were presented in a poster entitled “Pentarins: Improved tumor targeting through nanoparticle encapsulation of miniaturized biologic drug conjugates” at the American Association for Cancer Research (AACR) Annual Meeting in Philadelphia, Penn.
BTP-277’s biologic targeting ligand is designed to specifically and selectively target cancers that over-express the somatostatin receptor. The targeting ligand is conjugated to a potent cytotoxic payload through an optimized chemical linker to create miniaturized biologic drug conjugates (mBDCs), which are incorporated in nanoparticles to create the Pentarin, BTP-277. Synergistic anticancer activity occurs based on the unique approach of the Pentarin: the nanoparticle enables high therapeutic concentration of mBDCs in the tumor; the small size of mBDCs allows for effective penetration deep into the tumor tissue; and ligand’s targeting ability allows for specific binding to tumor cells and selective intracellular payload delivery.