Long-Term Transfer and Expression of the Human β-Globin Gene in a Mouse Transplant Model

Author:

Raftopoulos Harry1,Ward Maureen1,Leboulch Philippe1,Bank Arthur1

Affiliation:

1. From Columbia University, College of Physicians and Surgeons, the Department of Genetics and Development, the Department of Medicine, New York, New York; Massachusetts Institute of Technology, Harvard-MIT, the Division of Health Sciences and Technology, Cambridge, MA; and Harvard Medical School, Brigham and Women's Hospital, Hematology-Oncology Division, Boston, MA.

Abstract

AbstractSomatic gene therapy of hemoglobinopathies depends initially on the demonstration of safe, efficient gene transfer and long-term, high-level expression of the transferred human β-globin gene in animal models. We have used a β-globin gene/β-locus control region retroviral vector containing several modifications to optimize gene transfer and expression in a mouse transplant model. In this report we show that transplantation of β-globin–transduced hematopoietic cells into lethally irradiated mice leads to the continued presence of the gene up to 8 months posttransplantation. The transferred human β-globin gene is detected in 3 of 5 mice surviving long term (>4 months) transplanted with bone marrow cells transduced with high-titer virus. Southern blotting confirms the presence of the unrearranged 5.1-kb human β-globin gene-containing provirus in 2 of these mice. In addition, long-term expression of the transferred gene is seen in 2 mice at levels of 5% and 20% that of endogenous murine β-globin at 6 and 8 months posttransplantation. We further document stem cell transduction by the successful transfer and high-level expression of the human β-globin gene from mice transduced 9 months earlier into irradiated secondary recipient mice. These results demonstrate high-level, long-term somatic human β-globin gene transfer into the hematopoietic stem cells of an animal for the first time, and suggest the potential feasibility of a retroviral gene therapy approach to sickle cell disease and the β thalassemias.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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