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Originally published In Press as doi:10.1074/jbc.M506026200 on October 18, 2005

J. Biol. Chem., Vol. 281, Issue 1, 341-347, January 6, 2006
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Evidence That the 11 {beta}-Hydroxysteroid Dehydrogenase (11 {beta}-HSD1) Is Regulated by Pentose Pathway Flux

STUDIES IN RAT ADIPOCYTES AND MICROSOMES*

Kenneth L. McCormick1, Xudong Wang, and Gail J. Mick

From the Department of Pediatrics, Division of Endocrinology, University of Alabama at Birmingham, Birmingham, Alabama 35233

11 {beta}-hydroxysteroid dehydrogenase type 1 (11 {beta}-HSD1) catalyzes the interconversion of biologically inactive 11 keto derivatives (cortisone, 11-dehydrocorticosterone) to active glucocorticoids (cortisol, corticosterone) in fat, liver, and other tissues. It is located in the intraluminal compartment of the endoplasmic reticulum. Inasmuch as an oxo-reductase requires NADPH, we reasoned that 11 {beta}-HSD1 would be metabolically interconnected with the cytosolic pentose pathway because this pathway is the primary producer of reduced cellular pyridine nucleotides. To test this theory, 11 {beta}-HSD1 activity and pentose pathway were simultaneously measured in isolated intact rodent adipocytes. Established inhibitors of NAPDH production via the pentose pathway (dehydroandrostenedione or norepinephrine) inhibited 11 {beta}-HSD1 oxo-reductase while decreasing cellular NADPH content. Conversely these compounds slightly augmented the reverse, or dehydrogenase, reaction of 11 {beta}-HSD1. Importantly, using isolated intact microsomes, the inhibitors did not directly alter the tandem microsomal 11 {beta}-HSD1 and hexose-6-phosphate dehydrogenase enzyme unit. Metabolites of 11 {beta}-HSD1 (corticosterone or 11-dehydrocorticosterone) inhibited or increased pentose flux, respectively, demonstrating metabolic interconnectivity. Using isolated intact liver or fat microsomes, glucose-6 phosphate stimulated 11 {beta}-HSD1 oxo-reductase, and this effect was blocked by selective inhibitors of glucose-6-phosphate transport. In summary, we have demonstrated a metabolic interconnection between pentose pathway and 11 {beta}-HSD1 oxo-reductase activities that is dependent on cytosolic NADPH production. These observations link cytosolic carbohydrate flux with paracrine glucocorticoid formation. The clinical relevance of these findings may be germane to the regulation of paracrine glucocorticoid formation in disturbed nutritional states such as obesity.

Received for publication, June 2, 2005 , and in revised form, September 16, 2005.

* The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked "advertisement" in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.

1 To whom correspondence should be addressed: Dept. of Pediatrics, University of Alabama at Birmingham, ACC 608, 1600 7th Ave. South, Birmingham, AL 35233. Tel.: 205-939-5260; Fax: 205-939-9821; E-mail: kmccormick{at}peds.uab.edu.


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