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肝脏X受体以区域、年龄和亚型特异性方式差异性地调节中枢髓鞘基因mRNA水平。

Liver X Receptors differentially modulate central myelin gene mRNA levels in a region-, age- and isoform-specific manner.

作者信息

Shackleford Ghjuvan' Ghjacumu, Grenier Julien, Abi Habib Walid, Massaad Charbel, Meffre Delphine

机构信息

Paris Descartes University, INSERM UMR-S 1124, 45 rue des Saints-Pères, 75006 Paris, France.

Paris Descartes University, INSERM UMR-S 1124, 45 rue des Saints-Pères, 75006 Paris, France.

出版信息

J Steroid Biochem Mol Biol. 2017 May;169:61-68. doi: 10.1016/j.jsbmb.2016.02.032. Epub 2016 Mar 3.

DOI:10.1016/j.jsbmb.2016.02.032
PMID:26940358
Abstract

Liver X Receptors (LXRs) α and β are nuclear receptors able to bind oxidative forms of cholesterol. They play important roles in the central nervous system (CNS), through their implication in a large variety of physiological and pathological processes among which modulation of cholesterol homeostasis and inflammation. Besides, we recently revealed their crucial role in myelination and remyelination in the cerebellum. Given the pleiotropic effects of such receptors on CNS functioning, we studied here the influence of LXRs on myelin gene mRNA accumulation in the major myelinated regions of the CNS in vivo. We show that both LXR isoforms differentially affect mRNA amount of myelin genes (PLP and MBP) in highly myelinated structures such as spinal cord, corpus callosum, optic nerve and cerebellum. In the adult, LXR activation by the synthetic agonist TO901317 significantly increases myelin gene mRNA amount in the cerebellum but not in the other regions studied. Invalidation of the sole LXRβ isoform leads to decreased PLP and MBP mRNA levels in all the structures except the spinal cord, while the knock out of both isoforms (LXR dKO) decreases myelin gene mRNA amounts in all the regions tested except the corpus callosum. Interestingly, during myelination process (post-natal day 21), both cerebellum and optic nerve display a decrease in myelin gene mRNA levels in LXR dKO mice. Concomitantly, PLP and MBP mRNA accumulation in the spinal cord is increased. Relative expression level of LXR isoforms could account for the differential modulation of myelin gene expression in the CNS. Altogether our results suggest that, within the CNS, each LXR isoform differentially influences myelin gene mRNA levels in a region- and age-dependant manner, participating in the fine regulation of myelin gene expression.

摘要

肝脏X受体(LXRs)α和β是能够结合氧化形式胆固醇的核受体。它们在中枢神经系统(CNS)中发挥重要作用,涉及多种生理和病理过程,包括调节胆固醇稳态和炎症。此外,我们最近揭示了它们在小脑髓鞘形成和髓鞘再生中的关键作用。鉴于此类受体对中枢神经系统功能的多效性影响,我们在此研究了LXRs对体内中枢神经系统主要髓鞘化区域髓鞘基因mRNA积累的影响。我们发现,两种LXR异构体对脊髓、胼胝体、视神经和小脑等高髓鞘化结构中髓鞘基因(PLP和MBP)的mRNA量有不同影响。在成年个体中,合成激动剂TO901317激活LXR可显著增加小脑中髓鞘基因的mRNA量,但在其他研究区域则无此作用。仅使LXRβ异构体失活会导致除脊髓外所有结构中PLP和MBP的mRNA水平降低,而两种异构体敲除(LXR双敲除,LXR dKO)则会使除胼胝体外所有测试区域的髓鞘基因mRNA量减少。有趣的是,在髓鞘形成过程中(出生后第21天),LXR dKO小鼠的小脑和视神经中髓鞘基因的mRNA水平均下降。与此同时,脊髓中PLP和MBP的mRNA积累增加。LXR异构体的相对表达水平可能解释了中枢神经系统中髓鞘基因表达的差异调节。总之,我们的结果表明,在中枢神经系统内,每种LXR异构体以区域和年龄依赖性方式差异影响髓鞘基因的mRNA水平,参与髓鞘基因表达的精细调节。

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