重视增龄的肝脏衰老

病毒性肝炎、酒精性肝病、非酒精性脂肪性肝病和自身免疫性肝病的发病率持续增高，使得肝硬化在我国的发病率居高不下。对于终未期肝硬化患者，各种治疗仍局限于危及生命的并发症的对症治疗，如消化道出血、肝肾综合征和肝性脑病等，这些治疗虽然对延长患者的生存时间有很大的帮助，但这些患者的生活质量仍非常低。然而，与这些患者生活质量息息相关的心肺功能异常因症状隐匿而得不到应有的关注。虽然肝移植有望能从根本上解决问题，但受种种条件的制约，广泛开展仍较困难。同时，肝移植前对心肺功能的评估对手术及预后亦非常重要。

肝脏衰老与胆道疾病

胆道疾病与肝脏解剖、生理功能、病理机制和治疗方法都存在密切联系,本文从肝胆系统在功能及结构上的紧密相连性,探讨肝脏的衰老对胆道疾病的发生产生影响。

膳食核苷酸长期喂养对SD大鼠肝增龄性纤维增生的作用和机制

目的:探讨长期喂养膳食核苷酸(NTs)对SD大鼠由增龄引起的肝纤维增生的保护作用和机制。方法:初断乳雄性大鼠随机分为老年对照组、0.01%和0.64%NTs干预组,每组6只,喂养24～26月后进行实验;另取8只12月龄对照组SD大鼠作为中年对照组。采用miRNA基因芯片对各组肝脏的miRNA表达变化,同时用qRT-PCR检测了相关靶基因的表达水平,并对肝脏中羟脯氨酸水平进行测定。结果:NTs可显著调控肝组织内11个miRNA的表达。其中miR-182基因显著上调,其降低靶基因Thbs-2的表达,降低细胞外基质纤维化;miR-328a*基因显著下调,降低Pdgf-b基因的表达,降低与肝纤维化形成有关的重要细胞因子的分泌,减轻肝星状细胞的增殖。与此同时,NTs长期干预可一定程度降低增龄引起的肝脏中羟脯氨酸水平上升。结论:NTs长期干预可缓解由增龄引起的肝纤维增生。

大黄蛰虫丸调控ROS介导的PI3K/Akt/FoxO4信号通路改善大鼠肝脏衰老的作用和机制

近年来的研究显示,非酒精性脂肪性肝病、肝硬化以及肝癌等常见肝病的发生和发展都与肝脏衰老(liver aging,LA)有关。基于此,为了探究传统经方——大黄蛰虫丸(Dahuang Zhechong Pills,DHZCP)多靶点地改善LA的作用和机制,笔者将24只大鼠随机均分为4组,即正常组、衰老模型组(模型组)、衰老模型+DHZCP组(DHZCP组)和衰老模型+维生素E(vitamin E,VE)组(VE组)。通过D-半乳糖(D-galactose,D-gal)连续腹腔注射建立大鼠LA模型。对于LA模型鼠,采用衰老表型和体质量来评估其一般情况;采用肝细胞衰老病理学特征、肝功能指标、肝脏磷酸化组蛋白H2A变异体(phosphorylated histone family 2A variant,γ-H2AX)染色特征、肝脏细胞周期阻滞蛋白(P21、P53、P16)表达水平以及肝脏衰老相关分泌表型(senescence-associated secretory phenotypes,SASP)因子蛋白表达水平来评估其LA;采用肝脏活性氧产物(reactive oxygen species,ROS)表达特征以及肝组织磷脂酰肌醇-3激酶(phosphatidylinositol-3 kinase,PI3K)/蛋白激酶B(protein kinase B,Akt)/叉头盒蛋白O4(forkhead box protein O4,FoxO4)信号通路关键信号分子蛋白表达水平来评估ROS介导的PI3K/Akt/FoxO4信号通路活性。结果显示,经DHZCP或VE干预12周后,对于DHZCP组和VE组大鼠,其特征性衰老表型和体质量,肝细胞衰老病理学特征和肝功能指标,肝脏ROS相对表达量,肝组织磷酸化PI3K(phosphorylated PI3K,p-PI3K)、磷酸化Akt(phosphorylated Akt,p-Akt)、FoxO4等关键信号分子的蛋白表达水平,肝脏γ-H2AX染色的特征以及肝组织P16、P21、P53和白细胞介素-6(interleukin-6,IL-6)、肿瘤坏死因子-α(tumor necrosis factor-α,TNF-α)的蛋白表达水平均得到相应改善,且两者的作用相似。总之,借助D-gal诱导的LA模型鼠,该研究阐明,DHZCP在体内能多靶点地改善LA,其作用和机制与调控肝组织ROS介导的PI3K/Akt/FoxO4信号通路活性有关。这些发现为DHZCP治疗衰老相关肝病提供了新的药理学证据。

Characterization of Natural Killer Cells in the Liver of Young Mice

OBJECTIVE To determine the quantity and quality of liver NK cells from young and adult mice and compare their characteristics. METHODS C57BL/6 mice were used at 2 weeks （young） and 8 weeks （adult） of age. The percentage and absolute number of NK cells in the liver and spleen were analyzed. The cytotoxicity of NK cells in the liver and spleen against various targets were detected by a 4 h ^51Cr-release method. FACScan was used to analyze the expression of CD69, Mac-l1 Ly49C/I and CD94 on the NK cells. Perforin mRNA levels were analyzed by the reverse transcription polymerase chain reaction （RT-PCR）. RESUTLS The percentages of NK cells in the liver of young and adult mice were similar （11.9%＋1.7% vs. 9.9%＋1.6%, P〉0.05）, but the absolute number per liver weight was higher in the young animals （11.6＋2.5×10^5/g vs. 3.4＋0.8×10^5/g, P〈0.05）. The level of NK cytotoxicity was extremely high in the liver of young compared to adult mice （71.0%＋5.5% vs. 23.8%＋4.4%, P〈0.05）, but this difference was not observed in the spleen. Phenotypes of the liver NK cells from young and adult mice were completely different from each other. The liver NK cells from young mice were CD69^high Mac-1^low Ly49C/ I^low, whereas NK cells from older mice displayed inverse antigen levels （CD- 69^low Mac-1^high Ly49C/I^high）. The expression levels of other NK cell-related markers were similar in both groups.The perforin mRNA level in the liver lymphocytes from young mice was consistently greater compared to adult mice. CONCLUSION From 2 to 8 weeks C57BU6 mice liver NK cells undergo age-associated changes. At 2 weeks of age the liver NK cells showed a high level of NK cytotoxicity and a unique phenotype which was not apparent at 8 weeks of age.