Scientific publications

A pan-tumor-siRNA aptamer chimera to block nonsense-mediated mRNA decay inflames and suppresses tumor progression. Scientific Publication

Jul 20, 2020 | Magazine: Molecular Therapy Nucleic Acids

Daniel Meraviglia-Crivelli 1 2, Helena Villanueva 1 2, Ashwathi Puravankara Menon 1 2, Angelina Zheleva 1 2, Beatriz Moreno 1, María Villalba-Esparza 1 2 3, Fernando Pastor 1 2


Abstract

Immune-checkpoint blockade (ICB) therapy has changed the clinical outcome of many types of aggressive tumors, but there still remain many cancer patients that do not respond to these treatments. There is an unmet need to develop a feasible clinical therapeutic platform to increase the rate of response to ICB. Here we use a previously described clinically tested aptamer (AS1411) conjugated with SMG1 RNAi (AS1411-SMG1 aptamer-linked siRNA chimeras [AsiCs]) to inhibit the nonsense-mediated RNA decay pathway inducing tumor inflammation and improving response to ICB. The aptamer AS1411 shows binding to numerous mouse and human tumor cell lines tested. AS1411 induces tumor cytotoxicity in long incubation times, which allows for the use of the aptamer as a carrier to target the RNAi inhibition to the tumor. The AS1411-SMG1 AsiCs induce a strong antitumor response in local and systemic treatment in different types of tumors. Finally, AS1411-SMG1 AsiCs are well tolerated with no detected side effects.

CITATION Mol Ther Nucleic Acids. 2022 Jul 20:29:413-425. doi: 10.1016/j.omtn.2022.07.017. eCollection 2022 Sep 13.

Our authors

Helena Villanueva Ruiz
Dr. Angelina Zheleva
Investigadora del Programa de Terapias Moleculares del Cima Universidad de Navarra
Dr. Beatriz Moreno Bruna
Investigador Adscrito a Proyecto Plataforma de Aptámeros y Química Médica