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载脂蛋白E:复原力基因。

Apolipoprotein E: the resilience gene.

作者信息

James Lisa M, Engdahl Brian E, Georgopoulos Apostolos P

机构信息

Department of Veterans Affairs Health Care System, Brain Sciences Center (11B), Minneapolis VAHCS, One Veterans Drive, Minneapolis, MN, 55417, USA.

Department of Neuroscience, University of Minnesota Medical School, Minneapolis, MN, 55455, USA.

出版信息

Exp Brain Res. 2017 Jun;235(6):1853-1859. doi: 10.1007/s00221-017-4941-4. Epub 2017 Mar 15.

Abstract

The apolipoprotein E (apoE) gene has been implicated in various conditions, most notably Alzheimer's disease and coronary artery disease. A predisposing role of the apoE4 isoform and a protective role of apoE2 isoform in those diseases have been documented. Here we investigated the role of apoE in resilience to trauma. Three hundred and forty-three US veterans were genotyped for apoE and were assessed for their lifetime trauma exposure (trauma score, T) and severity of posttraumatic stress disorder symptoms (PCL). The ratio PCL/T indicates sensitivity to trauma; hence, its inverse indicates resilience, R, to trauma. We found a significantly higher resilience in participants with apoE genotype containing the E2 allele (E2/2, E2/3) as compared to participants with the E4 allele (E4/4, E4/3). In addition, when the categorical apoE genotype was reexpressed as the number of cysteine residues per apoE mole (CysR/mole), a highly significant positive association was found between resilience and CysR/mole, such that resilience was systematically higher as the number of CysR/mole increased, from zero CysR/mole in E4/4 to four CysR/mole in E2/2. These findings demonstrate the protective role of the CysR/mole apoE in resilience to trauma: the more CysR/mole, the higher the resilience. Thus, they are in accord with other findings pointing to a generally protective role of increasing number of CysR/mole (from E4/4 to E2/2) in other diseases. However, unlike other conditions (e.g., Alzheimer's disease and coronary artery disease), resilience to trauma is not a disease but an adaptive response to trauma. Therefore, the effects of apoE seem to be more pervasive along the CysR/mole continuum, most probably reflecting underlying effects on brain synchronicity and its variability that we have documented previously (Leuthold et al., Exp Brain Res 226:525-536, 2013).

摘要

载脂蛋白E(apoE)基因与多种疾病有关,最显著的是阿尔茨海默病和冠状动脉疾病。apoE4异构体的易患作用以及apoE2异构体在这些疾病中的保护作用已得到证实。在此,我们研究了apoE在创伤恢复力中的作用。对343名美国退伍军人进行了apoE基因分型,并评估了他们一生的创伤暴露情况(创伤评分,T)和创伤后应激障碍症状的严重程度(PCL)。PCL/T比值表示对创伤的敏感性;因此,其倒数表示对创伤的恢复力,R。我们发现,与携带E4等位基因(E4/4、E4/3)的参与者相比,携带E2等位基因的apoE基因型(E2/2、E2/3)的参与者具有显著更高的恢复力。此外,当将分类的apoE基因型重新表示为每摩尔apoE的半胱氨酸残基数量(CysR/摩尔)时,发现恢复力与CysR/摩尔之间存在高度显著的正相关,即随着CysR/摩尔数量的增加,恢复力系统性地升高,从E4/4中的零个CysR/摩尔到E2/2中的四个CysR/摩尔。这些发现证明了CysR/摩尔apoE在创伤恢复力中的保护作用:CysR/摩尔越多,恢复力越高。因此,它们与其他研究结果一致,这些结果表明在其他疾病中,CysR/摩尔数量增加(从E4/4到E2/2)通常具有保护作用。然而,与其他疾病(如阿尔茨海默病和冠状动脉疾病)不同,对创伤的恢复力不是一种疾病,而是对创伤的适应性反应。因此,apoE的影响似乎在CysR/摩尔连续体上更为普遍,很可能反映了我们之前记录的对大脑同步性及其变异性的潜在影响(Leuthold等人,《实验脑研究》226:525 - 536,2013)。

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