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慢性产后单胺氧化酶抑制影响幼鼠的亲和行为。

Chronic postnatal monoamine oxidase inhibition affects affiliative behavior in rat pupso.

作者信息

Blazevic Sofia, Merkler Mirna, Persic Dora, Hranilovic Dubravka

机构信息

University of Zagreb, Faculty of Science, Department of Biology, Rooseveltov trg 6, HR-10 000 Zagreb, Croatia.

University of Zagreb, Faculty of Science, Department of Biology, Rooseveltov trg 6, HR-10 000 Zagreb, Croatia.

出版信息

Pharmacol Biochem Behav. 2017 Feb;153:60-68. doi: 10.1016/j.pbb.2016.12.008. Epub 2016 Dec 15.

Abstract

Monoamine neurotransmitters serotonin (5-HT), dopamine (DA), and noradrenaline (NA) act as important modulators of mammalian brain development and represent neurobiological substrates of affiliative behavior reflected in rat pups as a tendency to huddle or produce ultrasonic vocalizations (USV) when separated from the nest. Monoamines are metabolized through oxidative deamination catalyzed by the mitochondrial enzyme monoamine oxidase (MAO). In this study, we examined the consequences of postnatal MAO inhibition on affiliative behavior in rat pups. Pups received daily injections of either an irreversible non-selective MAO inhibitor tranylcypromine (TCP) or saline, from post-natal day (PND) 1 to PND 22. Quantitative and qualitative components of USV were analyzed on PNDs 10, 13 and 16 in order to determine the level of separation-induced anxiety and the modality of vocal communication. In comparison to control pups, TCP-treated pups displayed higher cortical 5-HT, DA and NA levels, higher peripheral 5-HT concentration, lower body mass throughout the pre-weaning period, higher isolation-induced drop in body temperature, and reduced total number of calls. Furthermore, they produced lower pitched calls of longer average duration without a preferable waveform. Our results demonstrate that chronic MAO inhibition by TCP primarily affects 5-HT concentrations, but also raises central catecholamine levels. They further indicate that disturbed monoaminergic homeostasis during early postnatal development leads to decreased weight-gain, compromised thermoregulation, and altered affiliative behavior in pre-weaning pups as reflected in reduced separation anxiety and inadequate vocal communication. Finally, they suggest a need for thorough examination of the potential effects of TCP and other monoamine inhibitors on the developing human brain.

摘要

单胺神经递质5-羟色胺(5-HT)、多巴胺(DA)和去甲肾上腺素(NA)是哺乳动物大脑发育的重要调节因子,也是依恋行为的神经生物学基础,在大鼠幼崽身上表现为与巢穴分离时挤成一团或发出超声波叫声(USV)的倾向。单胺通过线粒体酶单胺氧化酶(MAO)催化的氧化脱氨作用进行代谢。在本研究中,我们检测了出生后抑制MAO对大鼠幼崽依恋行为的影响。从出生后第1天(PND 1)到PND 22,幼崽每天注射不可逆的非选择性MAO抑制剂反苯环丙胺(TCP)或生理盐水。在PND 10、13和16分析USV的定量和定性成分,以确定分离诱导的焦虑水平和声音交流方式。与对照幼崽相比,接受TCP治疗的幼崽在断奶前整个时期皮质5-HT、DA和NA水平更高,外周5-HT浓度更高,体重更低,隔离诱导的体温下降更高,叫声总数减少。此外,它们发出的叫声音调更低,平均持续时间更长,且没有偏好的波形。我们的结果表明,TCP慢性抑制MAO主要影响5-HT浓度,但也会提高中枢儿茶酚胺水平。结果还表明,出生后早期发育过程中,单胺能稳态紊乱会导致断奶前幼崽体重增加减少、体温调节受损以及依恋行为改变,表现为分离焦虑减轻和声音交流不足。最后,研究结果表明需要全面检查TCP和其他单胺抑制剂对发育中的人类大脑的潜在影响。

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