轻度缺氧暴露影响外周血清素摄取和降解海湾蟾蜍鱼,Opsanus β。

John Sebastiani, Allyson Sabatelli, M. McDonald
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引用次数: 2

摘要

先前的研究表明,抑制SERT会抑制5-羟色胺的摄取和降解,从而减弱海湾蟾鱼(Opsanus beta)部分心血管缺氧反射,这表明这些5-羟色胺清除过程可能在缺氧暴露中很重要。因此,本实验的目的是确定轻度缺氧对蟾鱼外周组织5-HT摄取和降解的影响。我们假设缺氧时5-羟色胺的摄取和降解会上调,导致血浆5-羟色胺含量降低,摄取发生在鳃、心脏、肝脏和肾脏。将鱼暴露于正常缺氧(97.6% O2饱和度,155.6 torr)或2分钟、40分钟或24小时轻度缺氧(50% O2饱和度,~ 80 torr)中,注射放射性标记的[3H]5-HT,并采集血液、尿液、胆汁和组织。血浆5 - 40分钟后水平降低40%低氧暴露,通过24小时持续。5 -吉尔是吸收的调节缺氧暴露2分钟后,吉尔和退化是调节在40分钟和24 h。有趣的是,没有改变5 -心脏和降解吸收的心脏缺氧暴露的2分钟内下降了58%和85%在24 h。这些结果表明,5 -间隙调节在缺氧和可能的驱动,在某种程度上,是通过鳃内的机制而不是心脏。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Mild hypoxia exposure impacts peripheral serotonin uptake and degradation in Gulf toadfish, Opsanus beta.
Plasma 5-HT homeostasis is maintained through the combined processes of uptake (via the 5-HT transporter SERT, and others), degradation (via monoamine oxidase, MAO), and excretion. Previous studies have shown that inhibiting SERT, which would inhibit 5-HT uptake and degradation, attenuates parts of the cardiovascular hypoxia reflex in Gulf toadfish (Opsanus beta), suggesting that these 5-HT clearance processes may be important during hypoxia exposure. Therefore, the goal of this experiment was to determine the effects of mild hypoxia on 5-HT uptake and degradation in the peripheral tissues of toadfish. We hypothesized that 5-HT uptake and degradation would be upregulated during hypoxia resulting in lower plasma 5-HT, with uptake occurring in the gill, heart, liver, and kidney. Fish were exposed to normoxia (97.6% O2 saturation, 155.6 torr), or 2-min, 40-min or 24 h mild hypoxia (50% O2 saturation, ∼80 torr), injected with radiolabeled [3H]5-HT and blood, urine, bile and tissues taken. Plasma 5-HT levels were reduced by 40% after 40 min of hypoxia exposure and persisted through 24 h. 5-HT uptake by the gill was upregulated following 2 min of hypoxia exposure, and degradation in the gill was upregulated at 40 min and 24 h. Interestingly, there was no change in 5-HT uptake by the heart and degradation in the heart decreased by 58% within 2 min of hypoxia exposure and by 85% at 24 h. These results suggest that 5-HT clearance is upregulated during hypoxia and is likely driven, in part, by mechanisms within the gill and not the heart.
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