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Horm Metab Res 1975; 7(4): 334-337
DOI: 10.1055/s-0028-1093725
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© Georg Thieme Verlag KG Stuttgart · New York

The Relation of Hepatic In Vitro Inactivation of Corticosteroids to the Circadian Rhythm of Plasma Corticosterone[*]

S. F. Marotta , L. G. Hiles , D. M. Lanuza , U.  Boonayathap [**]
  • Research Resources Center and the Department of General Nursing, University of Illinois at the Medical Center, Chicago, Illinois, U.S.A.
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Publikationsdatum:
23. Dezember 2008 (online)

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Abstract

Plasma corticosterone levels and the in vitro capacity of the liver to reduce the Δ43-ketone group of corticosterone were ascertained at 4 hr intervals in male rats maintained on a normal lighting schedule (12L:12D). The rates of Δ43-ketone reduction, as well as wet liver weight, were highest during the early portion (08.00 hr) of the light period when liver protein and plasma corticosterone concentrations were low. Shortly (2000 hr) after the beginning of the dark period plasma corticosterone reached peak levels, while hepatic inactivation of corticosterone was markedly depressed. This inverse relationship suggests that the rhythmicity in the capacity of the liver to inactivate corticosterone may contribute to the circadian periodicity of plasma corticosterone.

Key words

Circadian Plasma Corticosterone - Hepatic Steroid Inactivation

1 Supported in part by internal grants of the University of Illinois and by the Office of Naval Research contract NR 201-020

1 Supported in part by internal grants of the University of Illinois and by the Office of Naval Research contract NR 201-020

2 Present address: Department of Physiology, Faculty of Medicine, Chiang Mai University, Chiang Mai, Thailand

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