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Differential expression and HIV-1 regulation of μ-opioid receptor splice variants across human central nervous system cell types

机译:μ-ApiOID受体接头变体对人体中枢神经系统细胞类型的差异表达和HIV-1调节

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摘要

The μ-opioid receptor (MOR) is known to undergo extensive alternative splicing as numerous splice variants of MOR have been identified. However, the functional significance of MOR variants, as well as how splice variants other than MOR-1 might differentially regulate HIV-1 pathogenesis in the CNS, or elsewhere, has been largely ignored. Our findings suggest that there are specific differences in the MOR variant expression profile among CNS cell types, and that the expression levels of these variants are differentially regulated by HIV-1. While MOR-1A mRNA was detected in astroglia, microglia and neurons, MOR-1 and MOR-1X were only found in astroglia. Expression of the various forms of MOR along with the chimeric G protein qi5 in HEK-293T cells resulted in differences in calcium/NFAT signaling with morphine treatment, suggesting that MOR variant expression might underlie functional differences in MOR-effector coupling and intracellular signaling across different cell types. Furthermore, the data suggest that the expression of MOR-1 and other MOR variants may also be differentially regulated in the brains of HIV infected subjects with varying levels of neurocognitive impairment. Overall, the results reveal an unexpected finding, that MOR-1 may not be the predominant form of MOR expressed by some CNS cell types and that other splice variants of MOR-1, with possible differing functions, may contribute to the diversity of MOR-related processes in the CNS.
机译:已知μ-ApiOID受体(Mor)经历广泛的替代剪接,因为已经鉴定了Mor的许多剪接变体。然而,MOR变体的功能意义,以及MOR-1以外的剪接变体如何差异地调节CNS中的HIV-1发病机制,在很大程度上被忽略了。我们的研究结果表明,CNS细胞类型中的MOR变体表达谱存在特异性差异,并且这些变体的表达水平通过HIV-1差异调节。虽然Mor-1a mRNA在星形虎胶,但Mor-1和Mor-1X中仅在星形虎胶质菌属中发现。在HEK-293T细胞中表达各种形式的MOR以及嵌合G蛋白质QI5,导致钙/ NFAT信号与吗啡治疗的差异,表明MOR变异表达可能在不同的偶联和细胞内信号传导下呈现功能差异细胞类型。此外,数据表明,MOR-1和其他MOR变体的表达也可以在HIV感染受试者的大脑中差异调节,具有不同水平的神经认知障碍。总体而言,结果揭示了意外发现,Mor-1可能不是一些CNS细胞类型表达的主要形式,并且MOR-1的其他剪接变体具有可能不同的功能,可能有助于MOR-的多样性CNS中的相关过程。

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