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Molecular Endocrinology Vol. 2, No. 1 85-89
doi:10.1210/mend-2-1-85
Copyright © 1988 by the Endocrine Society.
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*Substance via MeSH
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*Genes and Gene Therapy

Abnormalities of the Human Growth Hormone Gene and Protooncogenes in Some Human Pituitary Adenomas

Hoi Sang U, Patricia Kelley and Wen-Hwa Lee

Division of Neurologic Surgery, University of California, School of Medicine San Diego, California 92103
Department of Pathology, University of California, School of Medicine San Diego, California 92103
Veterans Administration Medical Center San Diego, California 92161

Address requests for reprints to: Division of Neurologic Surgery, University of California School of Medicine, H-893, 225 Dickinson Street, San Diego, California 92103.

Abstract

Hypersecretion of human GH (hGH) or PRL by human pituitary adenomas is not under normal homeostatic control despite normal receptor function mediating the regulatory effects of hypothalamic peptides for these trophic hormones. This implies that the defects underlying hormonal hypersecretion may not reside at the plasma membrane of the adenoma cell; instead, dysregulation may resideat the hormone gene level. To investigate this, genomic DNA derived from a prolactinoma and a hGH-secreting adenoma were digested with the restriction endonuclease EcoRI and the methylationsensitive restriction endonuclease Hpall and hybridized with the 32P-labeled genomic hGH (2.6 kilobase) probe. Our data revealed hypomethylation of genes of the hGH family (hGH and chorionic somatomammotropin) in the absence of gross abnormalities such as gene translocation. In a similar analysis using a 32P-labeled probe consisting of the EcoRI-BamHI (500 base pair) fragment in the 5'-flanking region upstream of the first exon of the hGH gene, hypomethylation of this specific site of the hGH genes was observed. These results are consistent with the concept that hypomethylation of genes is involved in gene expression.

At the same time, protooncogene abnormalities in these adenomas were investigated to delineate any genetic basis for their neoplastic growth. Genomic DNA of adenomas were subjected to Southern blotting analysis using a panel of protooncogene probes. Amplification of the v-fos gene was observed in one prolactinoma. The significance of this observation is discussed.

FOOTNOTES

Supported by research grants from the Veterans Administration and the UCSD Academic Senate, and a Teachers Investigator Development Award from the NIH (to H.S.U.).

Received for publication May 28, 1987. Accepted for publication October 25, 1987.




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