VIP enhances TRH‐stimulated prolactin secretion of pituitary tumours

Artigo Revisado por pares

VIP enhances TRH‐stimulated prolactin secretion of pituitary tumours

1984; Wiley; Volume: 177; Issue: 1 Linguagem: Inglês

10.1016/0014-5793(84)80983-7

ISSN

1873-3468

Autores

R. A. Prysor-Jones, J. J. Silverlight, J. S. Jenkins, A. N. Stevens, J.L. Rodrigues, John R. Griffiths,

Tópico(s)

Caveolin-1 and cellular processes

Resumo

Intravenous thyrotrophin releasing hormone (TRH) caused a 6.5‐fold increase in plasma prolactin (PRL) in rats carrying implanted pituitary tumours. Vasoactive intestinal polypeptide (VIP) had no effect, but TRH given after VIP raised TRH stimulated secretion 13‐fold above basal. 31 P NMR spectroscopy showed that VIP caused a decrease in high energy metabolites (depleted phosphocreatine, elevated inorganic phosphate and lowered intracellular pH). TRH alone caused a similar but smaller effect; given after VIP, it caused no detectable depletion. We suggest that the changes in high energy metabolite cencentrations reflect increased cellular energy consumption consistent with a priming process (stage 1) in PRL secretion, followed by hormone release (stage 2). VIP induces stage 1 whereas RTH induced both stages.

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VIP enhances TRH‐stimulated prolactin secretion of pituitary tumours