| Literature DB >> 32379519 |
Aleksandra Pęcak1,2, Łukasz Skalniak3, Katarzyna Pels1, Mirosław Książek2, Mariusz Madej2, Dobrosława Krzemień1,2,3, Stanisław Malicki2, Benedykt Władyka1, Adam Dubin1, Tad A Holak3, Grzegorz Dubin2.
Abstract
CD44 is a type I transmembrane glycoprotein interacting with a number of extracellular components, including hyaluronic acid (HA). CD44-HA axis is involved in a variety of processes, including adhesion, migration, differentiation, trafficking, and others. CD44 is overexpressed in several cancers where binding of HA induces signal transduction leading to activation of antiapoptotic proteins and factors linked to drug resistance. As such, CD44 has been implicated in cancer growth, progression, and metastasis. It has been convincingly demonstrated that blocking CD44-HA interaction decreases cancer cell survival and metastasis. In this study, using in vitro selection, we have developed DNA aptamers recognizing a HA-binding domain of CD44 with high affinity and specificity. The aptamers bind to CD44 with nanomolar affinities and efficiently inhibit the growth of leukemic cancer cells characterized by high expression of CD44. The selectivity is demonstrated by an irrelevant effect on cells characterized by low CD44 levels. The obtained aptamers broaden the existing landscape of potential approaches to the development of antitumor strategies based on inhibition of the CD44 axis.Entities:
Keywords: CD44; DNA aptamer; cancer; leukemia
Year: 2020 PMID: 32379519 DOI: 10.1089/nat.2019.0833
Source DB: PubMed Journal: Nucleic Acid Ther ISSN: 2159-3337 Impact factor: 5.486