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生长激素释放肽六元瑞林重复给药和持续输注对清醒雄性大鼠的影响。

Effects of repeated doses and continuous infusions of the growth hormone-releasing peptide hexarelin in conscious male rats.

作者信息

Conley L K, Gaillard R C, Giustina A, Brogan R S, Wehrenberg W B

机构信息

Department of Biology, Carroll College, Waukesha, Wisconsin 53186, USA.

出版信息

J Endocrinol. 1998 Sep;158(3):367-75. doi: 10.1677/joe.0.1580367.

Abstract

We have previously shown that hexarelin, a novel GH-releasing peptide (GHRP), is able to elicit GH release when administered i.v., s.c. or by mouth and that it is a more potent GH secretagogue than GHRP-6. In the current study, we investigated the effects of hexarelin administered as repeated doses at 2 h intervals or as a continuous 6, 30 or 174 h infusion to conscious male rats. In the first experiment, adult male Sprague-Dawley rats were prepared with dual indwelling jugular catheters. On the day of experimentation, these animals received three 25 micrograms/kg i.v. boluses of hexarelin at 2 h intervals with blood sampling at 5, 10, 15, 30, 60, 90 and 120 min after each dose. The mean peak GH response and the mean area under the GH response curve (AUC) for the 30 min after each administration were calculated and are reported as the mean +/- S.E.M. For both the peak and AUC results there was a significant (P < 0.05) difference in the GH response noted between the first (peak 301 +/- 37 ng/ml; AUC 5585 +/- 700 ng/ml per 30 min) and second (peak 149 +/- 47 ng/ml; AUC 3056 +/- 908 ng/ml per 30 min) injections of hexarelin, but not between the first and third (peak 214 +/- 49 ng/ml; AUC 3862 +/- 844 ng/ml per 30 min). In a second series of experiments, adult male Sprague-Dawley rats received continuous infusions (100 micrograms/h) of hexarelin or saline (1 ml/h) for 6, 30 or 174 h. Blood samples were collected every 20 min for the duration of the 6 h infusion and for the last 6 h of the two longer hexarelin infusions. Plasma GH concentrations peaked within 40 min of the initiation of infusion, but soon returned to basal levels. Mean plasma GH concentrations did not differ between any of the treatment groups, nor did any of the parameters of pulsatile hormone release analyzed. No significant differences in plasma corticosterone concentrations were noted between any of the treatment groups. On the other hand, while neither the 6 h (941 +/- 70 ng/ml) nor the 30 h (954 +/- 70 ng/ml) hexarelin infusions resulted in a significant increase in the plasma IGF-I concentrations over those noted in the saline controls (935 +/- 65 ng/ml), a 174 h hexarelin infusion did elicit a significant increase (1289 +/- 42 ng/ml; P < 0.05). Thus it appears that, while continuous exposure to hexarelin does not disrupt normal GH cycling, it may (after up to 174 h of exposure) alter other components of the growth axis. In addition, since the character of pulsatile GH release remained unaltered in response to the hexarelin infusion, it appears that this GHRP may not act by suppression of functional somatostatin tone as has been suggested previously.

摘要

我们之前已经表明,六元瑞林是一种新型生长激素释放肽(GHRP),静脉注射、皮下注射或口服时均能促使生长激素释放,且它是比GHRP-6更强效的生长激素促分泌素。在本研究中,我们调查了以2小时间隔重复给药或连续输注6、30或174小时的六元瑞林对清醒雄性大鼠的影响。在第一个实验中,成年雄性斯普拉格-道利大鼠植入双留置颈静脉导管。在实验当天,这些动物每隔2小时静脉注射三次25微克/千克的六元瑞林,并在每次给药后5、10、15、30、60、90和120分钟采集血样。计算每次给药后30分钟的平均峰值生长激素反应以及生长激素反应曲线下的平均面积(AUC),并以平均值±标准误报告。对于峰值和AUC结果,首次注射六元瑞林(峰值301±37纳克/毫升;AUC 5585±700纳克/毫升每30分钟)和第二次注射(峰值149±47纳克/毫升;AUC 3056±908纳克/毫升每30分钟)之间的生长激素反应存在显著差异(P<0.05),但首次和第三次注射(峰值214±49纳克/毫升;AUC 3862±844纳克/毫升每30分钟)之间无显著差异。在第二系列实验中,成年雄性斯普拉格-道利大鼠接受六元瑞林或生理盐水(1毫升/小时)连续输注(100微克/小时)6、30或174小时。在6小时输注期间以及两个较长时间的六元瑞林输注的最后6小时,每20分钟采集一次血样。血浆生长激素浓度在输注开始后40分钟内达到峰值,但很快恢复到基础水平。各治疗组之间的平均血浆生长激素浓度无差异,所分析的任何脉冲式激素释放参数也无差异。各治疗组之间的血浆皮质酮浓度无显著差异。另一方面,虽然6小时(941±70纳克/毫升)和30小时(954±70纳克/毫升)的六元瑞林输注均未使血浆胰岛素样生长因子-I浓度比生理盐水对照组(935±65纳克/毫升)显著升高,但174小时的六元瑞林输注确实引起了显著升高(1289±42纳克/毫升;P<0.05)。因此,虽然持续接触六元瑞林不会扰乱正常的生长激素循环,但它可能(在接触长达174小时后)改变生长轴的其他成分。此外由于六元瑞林输注后脉冲式生长激素释放的特征未改变,似乎这种GHRP可能不像之前所认为的那样通过抑制功能性生长抑素张力起作用。

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