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  Vol. 270 No. 19, November 17, 1993 TABLE OF CONTENTS
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Progress Toward Human Gene Therapy

Manal A. Morsy, MD, PhD; Kohnosuke Mitani, PhD; Paula Clemens, MD; C. Thomas Caskey, MD

JAMA. 1993;270(19):2338-2345.

Since this article does not have an abstract, we have provided the first 150 words of the full text PDF and any section headings.

THE TECHNOLOGY of gene transfer has evolved over nearly 50 years since studies of DNA-mediated bacterial transformation reported by Avery et al in 1944.1 These earliest gene transfer experiments explored "the chemical nature of the substance inducing transformation of pneumococcal types."1 More than two decades later, mammalian cells were transformed with SV40 and polyoma papovavirus DNA by calcium phosphate—mediated cellular uptake.2-4 In 1971, the first workshop on gene therapy was held.5 Recombinant DNA technology provided the first approaches for cell transfer of disease-related genes (ie, β-globin [hemoglobinopathies] and hypoxanthine guanine phosphoribosyltransferase [Lesch-Nyhan syndrome]).6-10 The Human Genome Project, with its high rate of heritable disease and cancer gene discoveries, fuels the opportunities for gene transfer therapy.

Replication-defective viral vectors are essential vehicles for gene transfer. Safe viral vectors were developed in the laboratories of Mulligan, Verma, Miller, and Gilboa based on the basic research on the life . . . [Full Text PDF of this Article]


Author Affiliations

From Baylor College of Medicine (Drs Morsy, Mitani, Clemens, and Caskey) and the Howard Hughes Medical Institute (Dr Caskey), Houston, Tex.


Footnotes

Reprint requests to the Institute for Molecular Genetics, Baylor College of Medicine, One Baylor Plaza, Houston, TX 77030 (Dr Caskey).



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