Samson Willis K, Keown Cynthia, Samson Charles K, Samson Henry W, Lane Brian, Baker Jennifer R, Taylor Meghan M
Department of Pharmacological and Physiological Science, Saint Louis University School of Medicine, St Louis, MO 63104, USA.
Endocrine. 2003 Feb-Mar;20(1-2):59-66. doi: 10.1385/ENDO:20:1-2:59.
The RF-amide peptides (RFRPs), including prolactin (PRL)-releasing peptide-31 (PrRP-31) and RFRP-1, have been reported to stimulate stress hormone secretion by either direct pituitary or indirect hypothalamic actions. We examined the possible direct effects of these peptides on PRL and adrenocorticotropin (adrenocorticotropic hormone [ACTH]) release from dispersed anterior pituitary cells in culture and on PRL and ACTH secretion following intracerebroventricular (i.c.v.) administration in vivo. Neither peptide significantly altered PRL or ACTH release from cultured pituitary cells (male rat donors). Central administration of 1.0 and 3.0 nmol of PrRP-31, but only the higher dose of RFRP-1, significantly elevated serum corticosterone levels in conscious male rats. The effect of PrRP-31 was not blocked by pretreatment (i.v.) with the corticotropin-releasing hormone (CRH) antagonist, alpha-helical CRH 9-41; however, pretreatment of the animals (i.v.) with an antiserum to CRH significantly lowered the hypothalamic-pituitary- adrenal axis response to central administration of PrRP-31. On the other hand, the release of PRL was significantly elevated by 3.0 nmol of RFRP-1, but not PrRP-31, in similarly treated, conscious male rats. Pretreatment with the catecholamine synthesis inhibitor, alpha-methyl-para-tyrosine, prevented the stimulation of PRL secretion observed following central administration of RFRP-1. RFRP-1 similarly did not alter PRL secretion in rats pretreated with the dopamine, D(2) receptor blocker, domperidone. These results suggest that the RF-amide peptides are not true neuroendocrine regulators of stress hormone secretion in the rat but, instead, act centrally to alter the release of neuroendocrine factors that do act in the pituitary gland to control PRL and ACTH release. In the case of RFRP-1, stimulation of PRL secretion is potentially owing to an action of the peptide to inhibit dopamine release into the median eminence. The corticosterone secretion observed following central administration of PrRP-31 does not appear, based on our current results, to be solely owing to an action of the peptide on CRH-producing neurons but, instead, may be a result of the ability of PrRP-31 to increase as well the exposure of the corticotrophs in vivo to other ACTH secretagogues, such as oxytocin or vasopressin.
包括催乳素(PRL)释放肽-31(PrRP-31)和RFRP-1在内的RF酰胺肽,据报道可通过直接作用于垂体或间接作用于下丘脑来刺激应激激素的分泌。我们研究了这些肽对培养的分散垂体前叶细胞中PRL和促肾上腺皮质激素(促肾上腺皮质激素[ACTH])释放的可能直接影响,以及在体内脑室内(i.c.v.)给药后对PRL和ACTH分泌的影响。两种肽均未显著改变培养的垂体细胞(雄性大鼠供体)中PRL或ACTH的释放。向清醒雄性大鼠脑室内注射1.0和3.0 nmol的PrRP-31,但仅较高剂量的RFRP-1可显著提高血清皮质酮水平。PrRP-31的作用未被促肾上腺皮质激素释放激素(CRH)拮抗剂α-螺旋CRH 9-41静脉预处理所阻断;然而,用抗CRH抗血清对动物进行静脉预处理可显著降低下丘脑-垂体-肾上腺轴对脑室内注射PrRP-31的反应。另一方面,在同样处理的清醒雄性大鼠中,3.0 nmol的RFRP-1可显著提高PRL的释放,但PrRP-31则不能。用儿茶酚胺合成抑制剂α-甲基-对-酪氨酸预处理可阻止脑室内注射RFRP-1后观察到的PRL分泌刺激。在多巴胺D2受体阻滞剂多潘立酮预处理的大鼠中,RFRP-1同样未改变PRL的分泌。这些结果表明,RF酰胺肽不是大鼠应激激素分泌的真正神经内分泌调节因子,而是通过中枢作用改变神经内分泌因子的释放,这些因子确实在垂体中起作用以控制PRL和ACTH的释放。就RFRP-1而言,PRL分泌的刺激可能是由于该肽抑制多巴胺释放到正中隆起中的作用。根据我们目前的结果,脑室内注射PrRP-31后观察到的皮质酮分泌似乎并非仅仅由于该肽对产生CRH的神经元的作用,而是可能是PrRP-31增加体内促肾上腺皮质激素细胞对其他ACTH促分泌剂(如催产素或血管加压素)暴露的能力的结果。
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