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氟西汀治疗会影响一种海洋硬骨鱼的氮废物排泄和渗透压调节。

Fluoxetine treatment affects nitrogen waste excretion and osmoregulation in a marine teleost fish.

作者信息

Morando Michael B, Medeiros Lea R, McDonald M Danielle

出版信息

Aquat Toxicol. 2009 Jul 26;93(4):253-60. doi: 10.1016/j.aquatox.2009.03.011. Epub 2009 Apr 18.

Abstract

Measurable quantities of the selective serotonin reuptake inhibitor (SSRI), fluoxetine, have been found in surface waters and more recently in the tissues of fish. This highly prescribed pharmaceutical inhibits the reuptake of the monoamine, serotonin (5-HT; 5-hydroxytryptamine), causing a local amplification of 5-HT concentrations. Serotonin is involved in the regulation of many physiological processes in teleost fish including branchial nitrogen excretion and intestinal osmoregulation. Since the gill and intestine are directly exposed to the environment, environmental exposure to fluoxetine has the potential of affecting both these mechanisms. In the present study, we test the potential sensitivity of these processes to fluoxetine by implanting gulf toadfish, Opsanus beta, intraperitoneally with different concentrations of fluoxetine (0 (control), 25, 50, 75 and 100 microgg(-1)). Fluoxetine treatments of 25 and 50 microgg(-1) were sub-lethal and were used in subsequent experiments. Fish treated with both 25 and 50 microgg(-1) fluoxetine had significantly higher circulating levels of 5-HT than control fish, suggesting that any 5-HT sensitive physiological process could potentially be affected by these two fluoxetine doses. However, only fish treated with 25 microgg(-1) fluoxetine showed a significant increase in urea excretion. A similar increase was not measured in fish treated with 50 microgg(-1) fluoxetine, likely because of their high circulating levels of cortisol which inhibits urea excretion in toadfish. Intestinal fluid absorption appeared to be stimulated in fish treated with 25 microgg(-1) fluoxetine but inhibited in 50 microgg(-1) treated fish. Despite these differing responses, both doses of fluoxetine resulted in lowered plasma osmolality values, which was expected based on the stimulation of fluid absorption in the 25 microgg(-1) fluoxetine-treated fish but is surprising with the 50 microgg(-1) treated fish. In the case of the latter, the corresponding stress response invoked by this level of fluoxetine may have resulted in an additional osmoregulatory response which accounts for the lowered plasma osmolality. Our findings suggest that branchial urea excretion and intestinal osmoregulation are responsive to the SSRI, fluoxetine, and further investigation is needed to determine the sensitivity of these processes to chronic waterborne fluoxetine contamination.

摘要

在地表水中已检测到可测量量的选择性5-羟色胺再摄取抑制剂(SSRI)氟西汀,最近在鱼类组织中也发现了它。这种被大量开处方的药物会抑制单胺5-羟色胺(5-HT;5-羟色胺)的再摄取,导致5-HT浓度局部升高。5-羟色胺参与硬骨鱼许多生理过程的调节,包括鳃部氮排泄和肠道渗透调节。由于鳃和肠道直接暴露于环境中,环境中氟西汀的暴露有可能影响这两种机制。在本研究中,我们通过向海湾蟾鱼(Opsanus beta)腹腔注射不同浓度的氟西汀(0(对照)、25、50、75和100微克/克)来测试这些过程对氟西汀的潜在敏感性。25和50微克/克的氟西汀处理剂量为亚致死剂量,并用于后续实验。用25和50微克/克氟西汀处理的鱼,其循环中的5-羟色胺水平显著高于对照鱼,这表明任何对5-羟色胺敏感的生理过程都可能受到这两种氟西汀剂量的影响。然而,只有用25微克/克氟西汀处理的鱼尿素排泄显著增加。用50微克/克氟西汀处理的鱼未检测到类似的增加,可能是因为它们循环中的皮质醇水平较高,抑制了蟾鱼的尿素排泄。用25微克/克氟西汀处理的鱼肠道液体吸收似乎受到刺激,但用50微克/克处理的鱼则受到抑制。尽管有这些不同的反应,但两种剂量的氟西汀都导致血浆渗透压值降低,基于对用25微克/克氟西汀处理的鱼液体吸收的刺激,这是预期的,但在用50微克/克处理的鱼中却令人惊讶。对于后者,这种水平的氟西汀引发的相应应激反应可能导致了额外的渗透调节反应,这解释了血浆渗透压的降低。我们的研究结果表明,鳃部尿素排泄和肠道渗透调节对SSRI氟西汀有反应,需要进一步研究以确定这些过程对慢性水体氟西汀污染的敏感性。

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