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Partial correction of murine hereditary growth disorder by germ-line incorporation of a new gene

Nature volume 311pages 65–67 (1984)Cite this article

Abstract

The dwarf little (lit) mouse is a model for the human hereditary disorder, isolated growth hormone (GH) deficiency type I1. In these animals, dwarfism results from an autosomal recessively inherited gene mutation. The GH gene is present2 but production of GH mRNA is deficient3, resulting in reduced serum GH and concomitantly decreased serum somatomedin4–6. Growth retardation is evident by 15 days of age and adult animals reach approximately one-half normal size1. Mutant mice of both sexes also exhibit a delayed onset of puberty, with males having a high degree of infertility1. As administration of GH restores growth7, we reasoned that growth failure in the mutant mice might be corrected by providing them with sufficient GH by gene therapy. Here we demonstrate that although the rat and human GH genes alone do not restore growth in transgenic mutants, a metallothionein–rat growth hormone fusion gene (MT–rGH) does. Moreover, the fertility of transgenic mutant males is improved; however, female fertility is impaired.

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Author notes

  1. Richard D. Palmiter: Howard Hughes Medical Institute, Department of Biochemistry, University of Washington, Seattle, Washington 98195, USA

Authors and Affiliations

  1. Laboratory of Reproductive Physiology, School of Veterinary Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, 19104, USA

    Robert E. Hammer, Richard D. Palmiter & Ralph L. Brinster

Authors
  1. Robert E. Hammer
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  2. Richard D. Palmiter
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  3. Ralph L. Brinster
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Hammer, R., Palmiter, R. & Brinster, R. Partial correction of murine hereditary growth disorder by germ-line incorporation of a new gene. Nature 311, 65–67 (1984). https://doi.org/10.1038/311065a0

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