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脆性X智力低下1(FMR1)基因的前突变影响母体锌含量、母乳以及围产期大脑生物能量学和支架构建。

Premutation in the Fragile X Mental Retardation 1 (FMR1) Gene Affects Maternal Zn-milk and Perinatal Brain Bioenergetics and Scaffolding.

作者信息

Napoli Eleonora, Ross-Inta Catherine, Song Gyu, Wong Sarah, Hagerman Randi, Gane Louise W, Smilowitz Jennifer T, Tassone Flora, Giulivi Cecilia

机构信息

Department of Molecular Biosciences, School of Veterinary Medicine Davis, CA, USA.

Medical Investigations of Neurodevelopmental Disorders Institute, University of California, DavisDavis, CA, USA; Department of Pediatrics, University of California Davis Medical CenterSacramento, CA, USA.

出版信息

Front Neurosci. 2016 Apr 19;10:159. doi: 10.3389/fnins.2016.00159. eCollection 2016.

Abstract

Fragile X premutation alleles have 55-200 CGG repeats in the 5' UTR of the FMR1 gene. Altered zinc (Zn) homeostasis has been reported in fibroblasts from >60 years old premutation carriers, in which Zn supplementation significantly restored Zn-dependent mitochondrial protein import/processing and function. Given that mitochondria play a critical role in synaptic transmission, brain function, and cognition, we tested FMRP protein expression, brain bioenergetics, and expression of the Zn-dependent synaptic scaffolding protein SH3 and multiple ankyrin repeat domains 3 (Shank3) in a knock-in (KI) premutation mouse model with 180 CGG repeats. Mitochondrial outcomes correlated with FMRP protein expression (but not FMR1 gene expression) in KI mice and human fibroblasts from carriers of the pre- and full-mutation. Significant deficits in brain bioenergetics, Zn levels, and Shank3 protein expression were observed in the Zn-rich regions KI hippocampus and cerebellum at PND21, with some of these effects lasting into adulthood (PND210). A strong genotype × age interaction was observed for most of the outcomes tested in hippocampus and cerebellum, whereas in cortex, age played a major role. Given that the most significant effects were observed at the end of the lactation period, we hypothesized that KI milk might have a role at compounding the deleterious effects on the FMR1 genetic background. A higher gene expression of ZnT4 and ZnT6, Zn transporters abundant in brain and lactating mammary glands, was observed in the latter tissue of KI dams. A cross-fostering experiment allowed improving cortex bioenergetics in KI pups nursing on WT milk. Conversely, WT pups nursing on KI milk showed deficits in hippocampus and cerebellum bioenergetics. A highly significant milk type × genotype interaction was observed for all three-brain regions, being cortex the most influenced. Finally, lower milk-Zn levels were recorded in milk from lactating women carrying the premutation as well as other Zn-related outcomes (Zn-dependent alkaline phosphatase activity and lactose biosynthesis-whose limiting step is the Zn-dependent β-1,4-galactosyltransferase). In premutation carriers, altered Zn homeostasis, brain bioenergetics and Shank3 levels could be compounded by Zn-deficient milk, increasing the risk of developing emotional and neurological/cognitive problems and/or FXTAS later in life.

摘要

脆性X前突变等位基因在FMR1基因的5'非翻译区有55 - 200个CGG重复序列。据报道,60岁以上前突变携带者的成纤维细胞中锌(Zn)稳态发生改变,补充锌可显著恢复锌依赖性线粒体蛋白的导入/加工及功能。鉴于线粒体在突触传递、脑功能和认知中起关键作用,我们在一个具有180个CGG重复序列的敲入(KI)前突变小鼠模型中检测了脆性X智力低下蛋白(FMRP)的表达、脑生物能量代谢以及锌依赖性突触支架蛋白SH3和多个锚蛋白重复结构域3(Shank3)的表达。线粒体相关结果与KI小鼠以及前突变和全突变携带者的人类成纤维细胞中的FMRP蛋白表达(而非FMR1基因表达)相关。在出生后第21天(PND21),在富含锌的KI海马体和小脑中观察到脑生物能量代谢、锌水平和Shank3蛋白表达存在显著缺陷,其中一些影响持续到成年期(PND210)。在海马体和小脑中测试的大多数结果都观察到了强烈的基因型×年龄相互作用,而在皮质中,年龄起主要作用。鉴于在哺乳期结束时观察到最显著的影响,我们推测KI母鼠的乳汁可能在加重对FMR1基因背景的有害影响方面起作用。在KI母鼠的乳腺组织中观察到锌转运蛋白ZnT4和ZnT6(在脑和哺乳期乳腺中大量存在)的基因表达较高。一项交叉寄养实验使食用野生型(WT)乳汁的KI幼崽的皮质生物能量代谢得到改善。相反,食用KI乳汁的WT幼崽在海马体和小脑中的生物能量代谢出现缺陷。在所有三个脑区都观察到了极显著的乳汁类型×基因型相互作用,其中皮质受影响最大。最后,携带前突变的哺乳期妇女的乳汁中锌水平较低,以及其他与锌相关的结果(锌依赖性碱性磷酸酶活性和乳糖生物合成,其限速步骤是锌依赖性β-1,4-半乳糖基转移酶)。在前突变携带者中,锌稳态、脑生物能量代谢和Shank3水平的改变可能因缺锌乳汁而加剧,增加了在生命后期出现情绪和神经/认知问题及/或脆性X相关震颤共济失调综合征(FXTAS)的风险。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bc17/4835505/c1c7a99651bf/fnins-10-00159-g0001.jpg

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