Central vasopressin receptors are upregulated by deoxycorticosterone acetate.

Brain Res

Department of Physiology, University of Alabama, Birmingham 35294.

Published: September 1991

AI Article Synopsis

  • The study investigated how deoxycorticosterone acetate (DOCA) treatment affects vasopressin (AVP) receptor regulation in both rats and cultured neurons.
  • DOCA-NaCl treatment led to a significant increase in the number of AVP receptors within 3 to 14 days, while receptor affinity remained unchanged, and no differences were noted after long-term hypertension.
  • The findings indicate that the increase in AVP receptors may be a direct effect of DOCA on neuronal cells, distinguishing it from other steroid treatments that did not influence AVP binding.

Article Abstract

Studies were performed to characterize the regulation of central vasopressin (AVP) receptors in deoxycorticosterone acetate (DOCA)-NaCl-treated and control rats, and in DOCA-treated primary neuronal enriched cell cultures. Uninephrectomized rats were given NaCl to drink and implanted subcutaneously with a silastic implant containing 200 mg/kg DOCA. [3H]AVP binding to a diencephalic block of tissue was examined. Whereas DOCA-NaCl treatment did not affect the affinity of [3H]AVP binding, the total number of AVP receptors was increased between 3 and 14 days following DOCA-NaCl administration. No differences in the number of binding sites were present in the established (35-56 days after DOCA-NaCl administration) stages of hypertension. To determine whether the increase in [3H]AVP binding was a direct effect of DOCA on neurons or related to the hormonal, volume or other physiologic changes that DOCA-NaCl treatment causes in the whole animal, [3H]AVP binding was examined in neurons grown in culture that was treated with DOCA. Scatchard analysis demonstrated that DOCA treatment (compared to control) produced an increase in the number but no change in the affinity of the AVP binding sites in primary neuron-enriched cultures. Treatment of cultured neurons with other steroids (estrogen, corticosterone, or aldosterone), did not change the kinetics of [3H]AVP binding, suggesting that the effects of DOCA on the AVP receptor were specific for this steroid. These data indicate that, in comparison to control rats, DOCA-NaCl hypertensive rats, have an enhanced number of AVP receptors in the diencephalon, perhaps as a direct result of an interaction between DOCA and AVP receptors.(ABSTRACT TRUNCATED AT 250 WORDS)

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Source
http://dx.doi.org/10.1016/0006-8993(91)90280-9DOI Listing

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