UNIV OF TX SOUTHWESTERN COMPREHENSIVE MED SICKLE CELL CT
Project Number1U54HL070588-01
Contact PI/Project LeaderBUCHANAN, GEORGE R
Awardee OrganizationUT SOUTHWESTERN MEDICAL CENTER
Description
Abstract Text
In recent years, treatments for Sickle Cell Disease (SCD) have significantly decreased the
frequency and duration of sickle cell crises and significantly lengthened the life expectancy of
patients. These improvements have been due to clinical, genetic and molecular advances that
have revealed basic aspects of the pathophysiology of SCD. In spite of these advances, SCD
remains associated with significant mortality and morbidity. The large body of data for
autologous stem cell bone marrow transplantation has shown it to be effective for a minority
of patients with SCD, but early mortality, the availability of suitable donors and factors involved
in patient selection remain limiting factors. As an alternative, genetic correction of SCD offers
hope as a potential curative approach for the majority of patients. Recent progress in the
development of mouse models of hemoglobin disorders and in lentivirus-based vector design
have provided strong rationale and impetus for preclinical implementation of gene therapy
approaches for SCD. In this proposal, we address three important challenges to the successful
genetic correction of SCD. First, we develop lentivirus-based vectors for the transduction of
human gamma-globin genes. These vectors include regulatory elements that are critical for high-level single copy gene expression and are evaluated both in transgenic mice and model cell lines. Second, we evaluate their transduction efficiency into bone marrow-derived hematopoietic stem cells from SCD patients. And third, we evaluate these transduced cells in vivo using a
human/mouse xenograft model of bone marrow transplantation. The preclinical data obtained
from these experiments will serve as the rational basis for the implementation of future clinical
gene therapy protocols aimed at the genetic correction of SCD.
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