Cancers (Oct 2021)

Selection of a Nuclease-Resistant RNA Aptamer Targeting CD19

  • Carla L. Esposito,
  • Katrien Van Roosbroeck,
  • Gianluca Santamaria,
  • Deborah Rotoli,
  • Annamaria Sandomenico,
  • William G. Wierda,
  • Alessandra Ferrajoli,
  • Menotti Ruvo,
  • George A. Calin,
  • Vittorio de Franciscis,
  • Silvia Catuogno

DOI
https://doi.org/10.3390/cancers13205220
Journal volume & issue
Vol. 13, no. 20
p. 5220

Abstract

Read online

The transmembrane glycoprotein cluster of differentiation 19 (CD19) is a B cell–specific surface marker, expressed on the majority of neoplastic B cells, and has recently emerged as a very attractive biomarker and therapeutic target for B-cell malignancies. The development of safe and effective ligands for CD19 has become an important need for the development of targeted conventional and immunotherapies. In this regard, aptamers represent a very interesting class of molecules. Additionally referred to as ‘chemical antibodies’, they show many advantages as therapeutics, including low toxicity and immunogenicity. Here, we isolated a nuclease-resistant RNA aptamer binding to the human CD19 glycoprotein. In order to develop an aptamer also useful as a carrier for secondary reagents, we adopted a cell-based SELEX (Systematic Evolution of Ligands by EXponential Enrichment) protocol adapted to isolate aptamers able to internalise upon binding to their cell surface target. We describe a 2′-fluoro pyrimidine modified aptamer, named B85.T2, which specifically binds to CD19 and shows an exquisite stability in human serum. The aptamer showed an estimated dissociation constant (KD) of 49.9 ± 13 nM on purified human recombinant CD19 (rhCD19) glycoprotein, a good binding activity on human B-cell chronic lymphocytic leukaemia cells expressing CD19, and also an effective and rapid cell internalisation, thus representing a promising molecule for CD19 targeting, as well as for the development of new B-cell malignancy-targeted therapies.

Keywords