ANTITUMOR ACTIVITY OF CIGB-300, A PEPTIDE CK2 INHIBITOR, IN BREAST CANCER MODELS

GOTTARDO, MARÍA FLORENCIA; CAPOBIANCO, CARLA SABRINA; SIDABRA, JOHANNA ELENA; YASSER PERERA; SILVIO PEREA; ALONSO, DANIEL; FARINA, HERNAN GABRIEL

Chicago

Congreso; AACR Annual Meeting 2018; 2018

AACR

CK2 is a serine-threonine kinase that has been involved in growth, proliferation and cell apoptosis. CK2 has a constitutive expression and it has more than 300 substrates. In recent years, CK2 became an interesting target for anticancer therapies. Inhibition of CK2 showed antitumor activity in different types of cancer. Because breast cancer is one of the main tumor types in which CK2 is overexpressed, we focus on the effect of CK2 inhibition as a modulator of key features of breast cancer cell biology. The aim of the present study was to evaluate the role of inhibition of CK2 by CIGB-300 in murine and human mammary carcinoma cell lines. For this purpose, we evaluated the action of CIGB-300 on viability, apoptosis, cell cycle, clonogenic capacity and migration using three different breast tumor cell lines, MCF7 (positive for estrogen, progesterone and HER2-neu receptors), MDA MB 231 (representative of triple negative tumors) and F3II, a murine mammary carcinoma. As compared the potential of CK2 inhibition in these models we included another chemical inhibitor of the enzyme, CX-4945. Our results showed that CIGB-300 reduced the viability of MDA MB 231 (IC50=120 μM) and MCF-7 (IC50=140 μM) (p