在人类酒精依赖的前额叶皮层中,KLF11(TIEG2)的表达作为单胺氧化酶 B 的转录激活物。
The expression of KLF11 (TIEG2), a monoamine oxidase B transcriptional activator in the prefrontal cortex of human alcohol dependence.
机构信息
Department of Psychiatry and Human Behavior , University of Mississippi Medical Center, Jackson, Mississippi.
出版信息
Alcohol Clin Exp Res. 2014 Jan;38(1):144-51. doi: 10.1111/acer.12229. Epub 2013 Aug 5.
BACKGROUND
The biochemical pathways underlying alcohol abuse and dependence are not well understood, although brain cell loss and neurotoxicity have been reported in subjects with alcohol dependence. Monoamine oxidase B (MAO B; an enzyme that catabolizes neurotransmitters such as dopamine) is consistently increased in this psychiatric illness. MAO B has been implicated in the pathogenesis of alcohol dependence and alcohol-induced brain neurotoxicity. Recently, the cell growth inhibitor protein, Kruppel-like factor 11 (KLF11), has been reported to be an MAO transcriptional activator. KLF11 is also known as TIEG2 (transforming growth factor-beta-inducible early gene 2) and mediates apoptotic cell death. This study investigates the protein expression of KLF11 and its relationship with MAO B using human postmortem prefrontal cortex from subjects with alcohol dependence.
METHODS
Twelve subjects with alcohol dependence and the respective psychiatrically normal control subjects were investigated. Expression of KLF11 and MAO B proteins in the prefrontal cortex was measured by Western blot analysis. Correlation studies involving KLF11 and MAO B protein expression were performed. Localization of KLF11 in the human prefrontal cortex was also determined by immunohistochemistry.
RESULTS
Levels of KLF11 protein were significantly increased by 44% (p < 0.03) in the postmortem prefrontal cortex of subjects with alcohol dependence as compared to age- and gender-matched, psychiatrically normal control subjects. Furthermore, KLF11 levels were significantly and positively correlated with both the increased MAO B protein levels and blood alcohol content in alcohol-dependent subjects. In addition, KLF11 protein expression was visualized in both neuronal and glial cells.
CONCLUSIONS
This novel study shows the important role of KLF11, an MAO transcriptional activator, in human alcohol dependence. It further supports that the KLF11-MAO B cell death cascade may contribute to chronic alcohol-induced brain damage. This argues a case for KLF11-MAO B inhibition as a novel therapeutic strategy that may impact this highly prevalent illness.
背景
尽管已有报道称酒精依赖症患者的脑细胞出现了缺失和神经毒性,但人们对导致酒精滥用和依赖的生化途径仍知之甚少。单胺氧化酶 B(MAO B;一种分解神经递质如多巴胺的酶)在这种精神疾病中始终增加。MAO B 已被牵连到酒精依赖症和酒精引起的脑神经毒性的发病机制中。最近,细胞生长抑制剂蛋白,类 Kruppel 因子 11(KLF11),已被报道为 MAO 的转录激活剂。KLF11 也称为 TIEG2(转化生长因子-β诱导的早期基因 2),并介导细胞凋亡。本研究使用来自酒精依赖症患者的人脑前额叶皮质来调查 KLF11 的蛋白质表达及其与 MAO B 的关系。
方法
对 12 名酒精依赖症患者和相应的精神病正常对照组进行了研究。通过 Western blot 分析测量前额叶皮质中的 KLF11 和 MAO B 蛋白的表达。进行了涉及 KLF11 和 MAO B 蛋白表达的相关性研究。还通过免疫组织化学确定了 KLF11 在人前额叶皮质中的定位。
结果
与年龄和性别匹配的精神病正常对照组相比,酒精依赖症患者死后前额皮质中的 KLF11 蛋白水平显着增加了 44%(p <0.03)。此外,KLF11 水平与 MAO B 蛋白水平的增加以及酒精依赖症患者的血液酒精含量呈显着正相关。此外,在神经元和神经胶质细胞中都可以观察到 KLF11 蛋白的表达。
结论
这项新研究表明,MAO 转录激活剂 KLF11 在人类酒精依赖中起重要作用。它进一步支持 KLF11-MAO B 细胞死亡级联可能导致慢性酒精引起的脑损伤。这表明 KLF11-MAO B 抑制可能是一种新的治疗策略,可能对这种高度流行的疾病产生影响。
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