Milosavljevic Snezana, Piroli Maria V, Sandago Emma J, Piroli Gerardo G, Smith Holland H, Beggiato Sarah, Frizzell Norma, Pocivavsek Ana
Department of Pharmacology, Physiology and Neuroscience, University of South Carolina School of Medicine, Building 1, D26, 6311 Garners Ferry Rd, Columbia, SC, 29209, USA.
Department of Life Sciences and Biotechnology, University of Ferrara, Ferrara, Italy.
Biol Sex Differ. 2025 Apr 2;16(1):22. doi: 10.1186/s13293-025-00703-w.
Disruptions in brain development can impact behavioral traits and increase the risk of neurodevelopmental conditions such as autism spectrum disorder, attention-deficit/hyperactivity disorder (ADHD), schizophrenia, and bipolar disorder, often in sex-specific ways. Dysregulation of the kynurenine pathway (KP) of tryptophan metabolism has been implicated in cognitive and neurodevelopmental disorders. Increased brain kynurenic acid (KYNA), a neuroactive metabolite implicated in cognition and sleep homeostasis, and variations in the Kmo gene, which encodes kynurenine 3-monooxygenase (KMO), have been identified in these patients. We hypothesize that parental Kmo genetics influence KP biochemistry, sleep behavior and brain energy demands, contributing to impairments in cognition and sleep in offspring through the influence of parental genotype and genetic nurture mechanisms.
A mouse model of partial Kmo deficiency, Kmo heterozygous (HET-Kmo), was used to examine brain KMO activity, KYNA levels, and sleep behavior in HET-Kmo compared to wild-type control (WT-Control) mice. Brain mitochondrial respiration was assessed, and KP metabolites and corticosterone levels were measured in breast milk. Behavioral assessments were conducted on wild-type offspring from two parental groups: (i) WT-Control from WT-Control parents, (ii) wild-type Kmo (WT-Kmo) from Kmo heterozygous parents (HET-Kmo). All mice were C57Bl/6J background strain. Adult female and male offspring underwent behavioral testing for learning, memory, anxiety-like behavior and sleep-wake patterns.
HET-Kmo mice exhibited reduced brain KMO activity, increased KYNA levels, and disrupted sleep architecture and electroencephalogram (EEG) power spectra. Mitochondrial respiration (Complex I and Complex II activity) and electron transport chain protein levels were impaired in the hippocampus of HET-Kmo females. Breast milk from HET-Kmo mothers increased kynurenine exposure during lactation but corticosterone levels were unchanged. Compared to WT-Control offspring, WT-Kmo females showed impaired spatial learning, heightened anxiety, reduced sleep and abnormal EEG spectral power. WT-Kmo males had deficits in reversal learning but no sleep disturbances or anxiety-like behaviors.
These findings suggest that Kmo deficiency impacts KP biochemistry, sleep behavior, and brain mitochondrial function. Even though WT-Kmo inherit identical genetic material as WT-Control, their development might be shaped by the parent's physiology, behavior, or metabolic state influenced by their Kmo genotype, leading to phenotypic sex-specific differences in offspring.
大脑发育的紊乱会影响行为特征,并增加患神经发育疾病的风险,如自闭症谱系障碍、注意力缺陷多动障碍(ADHD)、精神分裂症和双相情感障碍,且这些影响通常具有性别特异性。色氨酸代谢的犬尿氨酸途径(KP)失调与认知和神经发育障碍有关。在这些患者中已发现,具有神经活性的代谢物犬尿喹啉酸(KYNA)在大脑中的水平升高,以及编码犬尿氨酸3-单加氧酶(KMO)的Kmo基因存在变异。我们推测,亲本的Kmo基因会影响KP生物化学、睡眠行为和大脑能量需求,通过亲本基因型和遗传养育机制的影响,导致后代出现认知和睡眠障碍。
使用部分Kmo缺陷的小鼠模型,即Kmo杂合子(HET-Kmo),与野生型对照(WT-Control)小鼠相比,检测HET-Kmo小鼠的大脑KMO活性、KYNA水平和睡眠行为。评估大脑线粒体呼吸,并测量母乳中的KP代谢物和皮质酮水平。对来自两个亲本组的野生型后代进行行为评估:(i)来自WT-Control亲本的WT-Control,(ii)来自Kmo杂合亲本(HET-Kmo)的野生型Kmo(WT-Kmo)。所有小鼠均为C57Bl/6J背景品系。成年雌性和雄性后代接受了学习、记忆、焦虑样行为和睡眠-觉醒模式的行为测试。
HET-Kmo小鼠的大脑KMO活性降低,KYNA水平升高,睡眠结构和脑电图(EEG)功率谱紊乱。HET-Kmo雌性小鼠海马体中的线粒体呼吸(复合体I和复合体II活性)以及电子传递链蛋白水平受损。HET-Kmo母亲的母乳在哺乳期增加了犬尿氨酸的暴露,但皮质酮水平未变。与WT-Control后代相比,WT-Kmo雌性小鼠表现出空间学习能力受损、焦虑加剧、睡眠减少和EEG频谱功率异常。WT-Kmo雄性小鼠在逆向学习方面存在缺陷,但没有睡眠障碍或焦虑样行为。
这些发现表明,Kmo缺陷会影响KP生物化学、睡眠行为和大脑线粒体功能。尽管WT-Kmo与WT-Control继承了相同的遗传物质,但它们的发育可能受到亲本Kmo基因型影响的生理、行为或代谢状态的塑造,导致后代出现表型性别特异性差异。
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