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人类化 COMT 小鼠的与努力相关的决策:ValMet 多态性的影响及其对人类阴性症状的可能意义。

Effort-related decision making in humanized COMT mice: Effects of ValMet polymorphisms and possible implications for negative symptoms in humans.

机构信息

Behavioral Neuroscience Division, Department of Psychology, University of Connecticut, Storrs, CT, USA; Present address: Dept. of Psychiatry, Yale University, New Haven, CT, USA.

Behavioral Neuroscience Division, Department of Psychology, University of Connecticut, Storrs, CT, USA.

出版信息

Pharmacol Biochem Behav. 2020 Sep;196:172975. doi: 10.1016/j.pbb.2020.172975. Epub 2020 Jun 25.

Abstract

Catechol-o-methyltransferase (COMT) is an enzyme that metabolizes catecholamines, and is crucial for clearance of dopamine (DA) in prefrontal cortex. ValMet polymorphism, which causes a valine (Val) to methionine (Met) substitution at codon 158, is reported to be associated with human psychopathologies in some studies. The Val/Val variant of the enzyme results in higher dopamine metabolism, which results in reduced dopamine transmission. Thus, it is important to investigate the relation between ValMet polymorphisms using rodent models of psychiatric symptoms, including negative symptoms such as motivational dysfunction. In the present study, humanized COMT transgenic mice with two genotype groups (Val/Val (Val) and Met/Met (Met) homozygotes) and wild-type (WT) mice from the S129 background were tested using a touchscreen effort-based choice paradigm. Mice were trained to choose between delivery of a preferred liquid diet that reinforced panel pressing on various fixed ratio (FR) schedules (high-effort alternative), vs. intake of pellets concurrently available in the chamber (low-effort alternative). Panel pressing requirements were controlled by varying the FR levels (FR1, 2, 4, 8, 16) in ascending and descending sequences across weeks of testing. All mice were able to acquire the initial touchscreen operant training, and there was an inverse relationship between the number of reinforcers delivered by panel pressing and pellet intake across different FR levels. There was a significant group x FR level interaction in the ascending limb, with panel presses in the Val group being significantly lower than the WT group in FR1-8, and lower than Met in FR4. These findings indicate that the humanized Val allele in mice modulates FR/pellet-choice performance, as marked by lower levels of panel pressing in the Val group when the ratio requirement was moderately high. These studies may contribute to the understanding of the role of COMT polymorphisms in negative symptoms such as motivational dysfunctions in schizophrenic patients.

摘要

儿茶酚-O-甲基转移酶(COMT)是一种代谢儿茶酚胺的酶,对于前额叶皮层中多巴胺(DA)的清除至关重要。ValMet 多态性导致密码子 158 处的缬氨酸(Val)被蛋氨酸(Met)取代,据报道,在一些研究中与人类精神病理学有关。该酶的 Val/Val 变体导致多巴胺代谢增加,从而导致多巴胺传递减少。因此,使用包括动机功能障碍在内的精神症状的啮齿动物模型来研究 ValMet 多态性之间的关系非常重要。在本研究中,使用具有两种基因型组(Val/Val(Val)和 Met/Met(Met)纯合子)和 S129 背景的野生型(WT)小鼠的人源化 COMT 转基因小鼠,使用触摸屏基于努力的选择范式进行测试。将小鼠训练为在不同固定比率(FR)方案(高努力替代方案)之间选择输送首选液体饮食以强化面板按压,与同时在腔室内提供的颗粒(低努力替代方案)之间进行选择。通过在测试周的升序和降序中改变 FR 水平(FR1、2、4、8、16)来控制面板按压要求。所有小鼠都能够获得初始触摸屏操作性训练,并且在不同 FR 水平下,通过面板按压交付的强化物数量与颗粒摄入量之间存在反比关系。在升序支腿中存在显著的组 x FR 水平相互作用,Val 组的面板按压明显低于 WT 组的 FR1-8,并且低于 FR4 的 Met。这些发现表明,小鼠中的人源化 Val 等位基因调节 FR/颗粒选择性能,正如 Val 组在比率要求适中高时的面板按压水平较低所表明的那样。这些研究可能有助于理解 COMT 多态性在精神分裂症患者的动机功能障碍等阴性症状中的作用。

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