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大鼠脉络丛转录组与神经保护相关的发育变化。

Developmental changes in the transcriptome of the rat choroid plexus in relation to neuroprotection.

机构信息

Inserm U1028, Lyon Neuroscience Research Center, Neurooncology & Neuroinflammation Team, Lyon-1 University, Lyon F-69000, France.

出版信息

Fluids Barriers CNS. 2013 Aug 1;10(1):25. doi: 10.1186/2045-8118-10-25.

Abstract

BACKGROUND

The choroid plexuses are the interface between the blood and the cerebrospinal fluid (CSF) contained within the ventricular spaces of the central nervous system. The tight junctions linking adjacent cells of the choroidal epithelium create a physical barrier to paracellular movement of molecules. Multispecific efflux transporters as well as drug-metabolizing and antioxidant enzymes functioning in these cells contribute to a metabolic barrier. These barrier properties reflect a neuroprotective function of the choroid plexus. The choroid plexuses develop early during embryogenesis and provide pivotal control of the internal environment throughout development when the brain is especially vulnerable to toxic insults. Perinatal injuries like hypoxia and trauma, and exposure to drugs or toxic xenobiotics can have serious consequences on neurogenesis and long-term development. The present study describes the developmental expression pattern of genes involved in the neuroprotective functions of the blood-CSF barrier.

METHODS

The transcriptome of rat lateral ventricular choroid plexuses isolated from fifteen-day-old embryos, nineteen-day old fetuses, two-day old pups, and adults was analyzed by a combination of Affymetrix microarrays, Illumina RNA-Sequencing, and quantitative RT-PCR.

RESULTS

Genes coding for proteins involved in junction formation are expressed early during development. Overall perinatal expression levels of genes involved in drug metabolism and antioxidant mechanisms are similar to, or higher than levels measured in adults. A similar developmental pattern was observed for multispecific efflux transporter genes of the Abc and Slc superfamilies. Expression of all these genes was more variable in choroid plexus from fifteen-day-old embryos. A large panel of transcription factors involved in the xenobiotic- or cell stress-mediated induction of detoxifying enzymes and transporters is also expressed throughout development.

CONCLUSIONS

This transcriptomic analysis suggests relatively well-established neuroprotective mechanisms at the blood-CSF barrier throughout development of the rat. The expression of many transcription factors early in development raises the possibility of additional protection for the vulnerable developing brain, should the fetus or newborn be exposed to drugs or other xenobiotics.

摘要

背景

脉络丛是血-脑脊髓液(CSF)在中枢神经系统脑室空间内的界面。脉络丛上皮细胞相邻细胞之间的紧密连接形成了分子经旁细胞运动的物理屏障。多特异性外排转运体以及在这些细胞中发挥作用的药物代谢和抗氧化酶有助于形成代谢屏障。这些屏障特性反映了脉络丛的神经保护功能。脉络丛在胚胎发生早期发育,并在大脑特别容易受到毒性损伤的发育过程中提供对内部环境的关键控制。围产期缺氧和创伤等损伤以及暴露于药物或有毒异生物质会对神经发生和长期发育产生严重后果。本研究描述了参与血脑屏障神经保护功能的基因的发育表达模式。

方法

通过 Affymetrix 微阵列、Illumina RNA-Seq 和定量 RT-PCR 的组合,分析了来自 15 日龄胚胎、19 日龄胎儿、2 日龄幼仔和成年大鼠侧脑室脉络丛的转录组。

结果

编码参与连接形成的蛋白质的基因在发育早期表达。药物代谢和抗氧化机制相关基因的整体围产期表达水平与成年时相当或高于成年时的水平。多特异性外排转运体基因的 ABC 和 Slc 超家族也表现出类似的发育模式。15 日龄胚胎脉络丛中这些基因的表达更为多变。大量参与细胞应激或细胞应激介导的解毒酶和转运体诱导的转录因子也在整个发育过程中表达。

结论

这种转录组分析表明,在大鼠的整个发育过程中,血脑屏障具有相对成熟的神经保护机制。许多转录因子在发育早期的表达为发育中的脆弱大脑提供了额外保护的可能性,如果胎儿或新生儿暴露于药物或其他异生物质。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fcd7/3737068/bac330e7a2e2/2045-8118-10-25-1.jpg

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