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在大鼠脑中,乙酰-L-肉碱治疗可调节参与神经元蜡样脂褐质沉积症的基因表达。

In the rat brain acetyl-L-carnitine treatment modulates the expression of genes involved in neuronal ceroid lipofuscinosis.

作者信息

Traina Giovanna, Bernardi Rodolfo, Cataldo Enrico, Macchi Monica, Durante Mauro, Brunelli Marcello

机构信息

Department of Internal Medicine, University of Perugia, Via San Costanzo, 06126 Perugia, Italy.

出版信息

Mol Neurobiol. 2008 Oct;38(2):146-52. doi: 10.1007/s12035-008-8038-8. Epub 2008 Aug 23.

Abstract

Acetyl-L-carnitine (ALC) is a naturally occurring substance that, when administered at supraphysiological concentration, is neuroprotective. It is a molecule of considerable interest for its clinical application in various neural disorders, including Alzheimer's disease and painful neuropathies. Suppression subtractive hybridization methodology was used for the generation of subtracted cDNA libraries and the subsequent identification of differentially expressed transcripts in the rat brain after ALC treatment. The method generates an equalized representation of differentially expressed genes irrespective of their relative abundance and it is based on the construction of forward and reverse cDNA libraries that allow the identification of the genes which are regulated by ALC. We report that ALC treatment: (1) upregulates lysosomal H(+)/ATPase gene expression and (2) downregulates myelin basic protein gene expression. The expression of these genes is altered in some forms of neuronal ceroid lipofuscinosis (NCL) pathologies. In this case, ALC might rebalance the disorders underlying NCL disease represented by a disturbance in pH homeostasis affecting the acidification of vesicles transported to lysosomal compartment for degradation. This study provides evidence that ALC controls genes involved in these serious neurological pathologies and provides insights into the ways in which ALC might exert its therapeutic benefits.

摘要

乙酰左旋肉碱(ALC)是一种天然存在的物质,当以超生理浓度给药时具有神经保护作用。因其在包括阿尔茨海默病和疼痛性神经病变在内的各种神经疾病中的临床应用而备受关注。抑制性消减杂交方法用于生成消减cDNA文库,并随后鉴定ALC处理后大鼠脑中差异表达的转录本。该方法能够产生差异表达基因的均衡表征,而不考虑其相对丰度,并且基于正向和反向cDNA文库的构建,从而能够鉴定受ALC调控的基因。我们报告ALC处理:(1)上调溶酶体H(+)/ATP酶基因表达,(2)下调髓鞘碱性蛋白基因表达。这些基因的表达在某些形式的神经元蜡样脂褐质沉积症(NCL)病理中发生改变。在这种情况下,ALC可能会重新平衡NCL疾病所潜在的紊乱,这种紊乱表现为pH稳态的干扰,影响转运至溶酶体区室进行降解的囊泡的酸化。本研究提供了证据表明ALC控制参与这些严重神经病理的基因,并深入了解了ALC可能发挥其治疗益处的方式。

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