Non-Viral Episomal Vector Mediates Efficient Gene Transfer of the β-Globin Gene into K562 and Human Haematopoietic Progenitor Cells

Author:

Lazaris Vassileios M.1ORCID,Simantirakis Emmanouil2,Stavrou Eleana F.1,Verras Meletios1,Sgourou Argyro3ORCID,Keramida Maria K.4,Vassilopoulos George2,Athanassiadou Aglaia1ORCID

Affiliation:

1. Department of General Biology, Medical School, University of Patras, 26504 Patras, Greece

2. Centre of Basic Research, Biomedical Research Foundation of the Academy of Athens (BRFAA), 11527 Athens, Greece

3. Biology Laboratory, School of Science and Technology, Hellenic Open University, 26335 Patras, Greece

4. IVF and Andrology Labs, IVF Unit, General University Hospital of Patras, 26504 Patras, Greece

Abstract

β-Thalassemia is a subgroup of inherited blood disorders associated with mild to severe anemia with few and limited conventional therapy options. Lately, lentiviral vector-based gene therapy has been successfully applied for disease treatment. However, the current development of non-viral episomal vectors (EV), non-integrating and non-coding for viral proteins, may be helpful in generating valid alternatives to viral vectors. We constructed a non-viral, episomal vector pEPβ-globin for the physiological β-globin gene based on two human chromosomal elements: the scaffold or matrix attachment region (S/MAR), allowing for long nuclear retention and non-integration and the β-globin replication initiation region (IR), allowing for enhancement of replication and establishment. After nucleofections into K562 cells with a transfection efficiency of 24.62 ± 7.7%, the vector induces stable transfection and is detected in long-term cultures as a non-integrating, circular episome expressing the β-globin gene efficiently. Transfections into CD34+ cells demonstrate an average efficiency of 15.57 ± 11.64%. In the colony-forming cell assay, fluorescent colonies are 92.21%, which is comparable to those transfected with vector pEP-IR at 92.68%. Additionally, fluorescent colonies produce β-globin mRNA at a physiologically 3-fold higher level than the corresponding non-transfected cells. Vector pEPβ-globin provides the basis for the development of therapeutic EV for gene therapy of β-thalassemias.

Funder

Greek Secretariat for Research and Technology

Publisher

MDPI AG

Subject

Genetics (clinical),Genetics

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