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Bromocriptine-induced dissociation of hyperglycemia and prolactin response to restraint

2001; Elsevier BV; Volume: 68; Issue: 2 Linguagem: Inglês

10.1016/s0091-3057(00)00453-6

1873-5177

Antonio Ribeiro-de-Oliveira, Rachel Menezes Guerra, Rodrigo Bastos Fóscolo, Umeko Marubayashi, Adelina M. Reis, Cândido Celso Coimbra,

Adipose Tissue and Metabolism

The present study investigated the effects of immobilization (restraint stress) on rat chronically treated with a D2 receptor agonist (bromocriptine, 0.4 mg/100 g body weight, injected daily intraperitoneally (ip) for 2 weeks) on plasma glucose, prolactin, and insulin levels. During restraint, the plasma prolactin of vehicle-treated (VEH) rats increased rapidly, reaching a peak at 10 min (57.9±8.1 ng/ml, P<.01). In contrast, restraint failed to induce any significant change in the plasma prolactin levels of bromocriptine-treated (BR) rats. The hyperglycemic response to immobilization was 97% higher (P<.05) in BR rats than in VEH rats. Our data demonstrate that prolactin secretion and hyperglycemia in response to restraint can be dissociated by chronic treatment with BR, which also increased the hyperglycemic response to immobilization probably due to central D2 dopaminergic activity.