Background/aims: Orexins (OXs) are a newly described family of hypothalamic neuropeptides. Based on the distribution of OX neurons and their receptors in the brain, it has been postulated that they could play a role in the regulation of neuroendocrine function. GH secretion is markedly influenced by nutritional status and body weight. To investigate the role OX-A plays in the neuroregulation of GH secretion we have studied its effect on spontaneous GH secretion as well as GH responses to GHRH and ghrelin in freely moving rats. Finally, we also assessed the effect of OX-A on in vitro GH secretion. Methods: We administered OX-A (10 mg, i.c.v.) or vehicle (10 ml, i.c.v.) to freely moving rats. Spontaneous GH secretion was assessed over 6 h with blood samples taken every 15 min. Results: Administration of OX-A led to a decrease in spontaneous GH secretion in comparison with vehicle-treated rats, as assessed by mean GH levels (means^S.E.M. 4.2^1.7 ng/ml vs 9.4^2.2 ng/ml; P , 0.05), mean GH amplitude (3.6^0.5 ng/ml vs 20.8^5.6 ng/ml; P , 0.01) and area under the curve (848^379 ng/ml per 4 h vs 1957^458 ng/ml per 4 h; P , 0.05). In contrast, OX-A failed to modify in vivo GH responses to GHRH (10 mg/kg, i.v.) although it markedly blunted GH responses to ghrelin (40 mg/kg, i.v.) (mean peak GH levels: 331^71 ng/ml, vehicle, vs 43^11 ng/ml in OX-A-treated rats; P , 0.01). Finally, OX-A infusion (10
The role of mesozooplankton grazers in the development of monospecific algal blooms has often been examined in a scenario in which grazers, depending on their abilities of recognition, select against toxic species and increase grazing pressure on non-toxic species. Here, we present a different ecological scenario in which grazers may select between different strains (toxic and nontoxic) of the same species, which may coexist in similar densities in natural environments prior to bloom initiation. The calanoid copepod Acartia clausi was fed with single and mixed diets of 2 strains of the dinoflagellate Alexandrium minutum, a producer of paralytic shellfish poisoning (PSP) toxins. One strain produced high, and the other low, quantities of PSP toxins. We examined feeding strategies and estimated copepod responses based on their food selection abilities, toxic effects on maintenance physiology and fitness, and benefits produced by a toxin-dilution strategy in a mixed diet. Copepods were found to feed selectively on A. minutum strains. Diet composition had a strong effect on parameters such as food ingestion, mortality, egg hatching, and egg production. The effect on copepod mortality and egg production was greatly reduced when a mixed diet (toxic + non-toxic) was provided to the copepods. However, the negative effects on egg hatching were dose-dependent, and this parameter was not recovered by toxin-dilution mechanisms. We conclude that copepods did not effectively reject the toxic strain and that the effect of A. minutum on mortality and egg production, but not on egg hatching, is reduced by dilution mechanisms. Therefore, we suggest that feeding pressure by grazers does not appear to be an important mechanism that favors toxic over non-toxic strains prior to bloom initiation.
GH secretion is markedly altered in diabetes mellitus (DM) in both rats and humans, albeit in opposite directions. In the rat, diabetes suppresses pulsatile GH secretion, especially high amplitude pulses, and decreases GH responses to secretagogue, depending inversely on severity of metabolic alteration. In the present study, we wanted to address the GH responses to GHRH and low doses of ghrelin in a streptozotocin (STZ) model of diabetes characterized by the delayed onset of the metabolic alterations. We have shown that the administration of high doses of STZ (90 mg/kg in 0.01 M solution of chloride-sodium, ip) to five-day-old pups (n5-STZ) can induce the appearance of a characteristic diabetic syndrome in adult age, the diabetic triad, with elevated plasma glucose levels: polyuria, polydipsia, hyperphagia, and reduced body weight gain. At the age of 3 months, in these n5-STZ male and female rats the GH responses to GHRH (1 microg/kg) and GHRH combined with ghrelin (1+3 microg/kg) had diminished both in punctual times and in the area under the curve (AUC). However, the combined administration of GHRH and ghrelin, being the more potent stimulus, elicited a synergistic GH response. Thus, male and female rats with delayed onset diabetes displayed an altered GH response to GHRH, although the combined administration of GHRH and ghrelin was able to restore the GH secretion with a synergistic effect.
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