Functionalized selenium nanoparticles ameliorated acetaminophen-induced hepatotoxicity through synergistically triggering PKCδ/Nrf2 signaling pathway and inhibiting CYP 2E1

Selenium nanoparticles(SeNPs)have been demonstrated potential for use in diseases associated with oxidative stress.Functionalized SeNPs with lower toxicity and higher biocompatibility could bring better therapeutic activity and clinical application value.Herein,this work was conducted to investigate the protective effect of Pleurotus tuber-regium polysaccharide-protein complex funtionnalized SeNPs(PTR-SeNPs)against acetaminophen(APAP)-induced oxidative injure in HepG2 cells and C57BL/6J mouse liver.Further elucidation of the underlying molecular mechanism,in particular their modulation of Nrf2 signaling pathway was also performed.The results showed that PTR-SeNPs could significantly ameliorate APAP-induced oxidative injury as evidenced by a range of biochemical analysis,histopathological examination and immunoblotting study.PTR-SeNPs could hosphorylate and activate PKCδ,depress Keap1,and increase nuclear accumulation of Nrf2,resulting in upregulation of GCLC,GCLM,HO-1 and NQO-1 expression.Besides,PTR-SeNPs suppressed the biotransformation of APAP to generate intracellular ROS through CYP 2E1 inhibition,restoring the mitochondrial morphology.Furthermore,the protective effect of PTR-SeNPs against APAP induced hepatotoxicity was weakened as Nrf2 was depleted in vivo,indicating the pivotal role of Nrf2 signaling pathway in PTR-SeNPs mediated hepatoprotective efficacy.Being a potential hepatic protectant,PTR-SeNPs could serve as a new source of selenium supplement for health-promoting and biomedical applications.

Cytochrome P450 2E1 genetic polymorphism and gastric cancer in Changle,Fujian Province

AIM: Genetic polymorphism in enzymes of carcinogen metabolism has been found to have the influence on the susceptibility to cancer. Cytochrome P450 2E1 ( CYP2 E1) is considered to play an important role in the metabolic activation of procarcinogens such as N-nitroscoamines and Iow molecular weight organic compounds. The purpose of this study is to determine whether CYP450 2Elpolymorphisms are associated with risk s of gastric cancer.METHODS: We conducted a population based case-control study in Changle county, Fujian Province, a high-risk region of gastric cancer in China. Ninety-one incident gastric cancer patients and ninety-four healthy controls were included in our study. Datas including dsmographic characteristcs, diet intake, and alcohol and tobacco consumption of indivduals in our study were completed by a standardized questionnaire. PCR-RFLP revealed three genotypes: heterozygote (C1/C2) and two homozygotes (C1/C1 and C2/C2) in CYP2E1.RESULTS: The frequency of variant genotypes (C1/C2 and C2/C2) in gastric cancer cases and controls was 36.3% and 24.5%, respectively. The rare homozygous C2/C2 genotype was found in 6 indivduals in gastric cancer group(6.6%),whereas there was only one in the control group (1.1%).However, there was no statistically significan difference between the two groups (two-tailed Fisher′s exact test, P =0.066). Indivduals in gastric cancer group were more likely to carry genotype C1/C2 (odds ratio, OR = 1.50) and C2/C2(OR = 7.34) than indivduals in control group (X2 = 4.597, for trend P=0.032). The frequencies of genofypes with the C2allele ( C1/C2 and C2/C2 genotypes) were compared with those of genotypes without C2 allele ( C1/C1 genotype )among indivduals in gastric cancer group and control group according to the pattern of gastric cancer risk factors. The results show that indivduals who exposed to these gastric cancer risk factors and carry the C2 allele seemed to have a higher risk of developing gastric cancer.CONCLUSION: Polymorphism of CYP2E1 gene may have some effct in the development of gastric cancer in Changle county, Fujian Province.

Hepatoprotective effects of S-adenosyl-L-methionine against alcohol-and cytochrome P450 2E1-induced liver injury

S-adenosyl-L-methionine (SAM) acts as a methyl donor for methylation reactions and participates in the synthesis of glutathione. SAM is also a key metabolite that regulates hepatocyte growth, differentiation and death. Hepatic SAM levels are decreased in animal models of alcohol liver injury and in patients with alcohol liver disease or viral cirrhosis. This review describes the protection by SAM against alcohol and cytochrome P450 2E1-dependent cytotoxicity both in vitro and in vivo and evaluates mechanisms for this protection.

Cytochrome P450 2E1 RsaI/PstI and DraI Polymorphisms Are Risk Factors for Lung Cancer in Mongolian and Han Population in Inner Mongolia

Objective： To explore the relationship between cytochrome P450 2E1 （CYP2E1） RsaI/PstI and DraI polymorphism and lung cancer susceptibility in Mongolian and Han population in Inner Mongolia of China. Methods： CYP2E1 RsaI/PstI and DraI polymorphisms were detected by polymerase chain reaction-restriction fragment length polymorphism in 64 lung cancer patients, 150 healthy Mongolian and 150 healthy Han individuals. The distribution of genotype and allele frequencies of CYP2E1 RsaI/PstI and DraI polymorphisms were studied. Results： The risk of lung cancer was increased in individuals with CYP2E1 （cl/cl） and CYP2E1 （DD） with OR values of 2.431 （95%CI=1.082-5.460） and 2.778 （95%CI=1.358-5.683） respectively （P0.05）. When CYP2E1 RsaI/PstI and DraI polymorphisms were combined, the risk of lung cancer was reduced in individuals with CYP2E1 （cl/c2＋c2/c2 and DD＋CC） with OR values of 0.233 （95%CI=0.088-0.615, P0.05）. In smokers, the susceptibility to lung cancer was higher in the individuals with CYP2E1 （c1/c1） and CYP2E1 （DD） than in the individuals with c2 and C allele （P0.05, OR=2.643 and 4.308 respectively）. There was no significant difference in distribution of CYP2E1 genotype frequency between healthy Mongolian, Han population and lung cancer patients, healthy controls in Inner Mongolia. Conclusion： CYP2E1 （c1/c1） and CYP2E1 （DD） are predisposing factors of lung cancer in population in Inner Mongolia. CYP2E1 （c2﹢C） co-mutation may decrease the risk of lung cancer. Smoking exerts synergetic effect with CYP2E1 （c1/c1） and CYP2E1 （DD） on the occurrence of lung cancer.

酒精性肝损伤大鼠细胞色素P450 CYP2E1和细胞色素P450 CYP3A的代谢活性

目的观察酒精性肝损伤对大鼠细胞色素P450CYP3A(CYP3A)和细胞色素P450CYP2E1(CYP2E1)代谢活性的影响。方法采用ig给予白酒制备大鼠酒精性肝损伤模型,检测血清中谷丙转氨酶(GPT)和谷草转氨酶(GOT)活性,采用HE染色法光镜下观测酒精对肝脏损伤程度。大鼠ip给予CYP3A探针药物咪达唑仑10mg·kg-1或ig给予CYP2E1探针药物氯唑沙宗50mg·kg-1后,采用高效液相色谱法测定不同时间点大鼠血浆中咪达唑仑和氯唑沙宗的血药浓度,并应用3P87软件计算其药代动力学参数,以考察CYP2E1和CYP3A的代谢活性的变化。大鼠ig给予氯唑沙宗80mg·kg-1后,热板方法测定大鼠添足次数和添足反射潜伏期。结果酒精性肝损伤可致大鼠肝小叶结构不清,肝索排列紊乱,肝细胞体积增大,呈弥漫性中度水变性,肝窦受压,大部分肝细胞胞浆内见大小不等的脂肪空泡;与正常对照组相比,酒精性肝损伤组大鼠GPT和GOT活性分别增加了16.0%和20.0%(P<0.05,P<0.01)。酒精性肝损伤致大鼠CYP2E1对探针药物氯唑沙宗的代谢活性增强,AUC,t1/2和cmax分别降低了38.0%,30.5%和35.0%(P<0.05);酒精肝损伤组大鼠氯唑沙宗镇痛效果明显降低;酒精性肝损伤致大鼠CYP3A对探针药物咪达唑仑的代谢活性增强,AUC,t1/2和cmax分别降低了122.6%,54.9%和56.9%(P<0.01,P<0.05)。结论酒精性肝损伤可使大鼠CYP2E1和CYP3A代谢活性增强。

注射用丹参总酚酸(冻干)对人CYP450酶和P-糖蛋白体外抑制作用及对大鼠CYP1A2和CYP3A体内诱导作用(英文)

目的探讨注射用丹参总酚酸(冻干)(SLI)对人CYP450酶和P-糖蛋白体外抑制作用以及对大鼠CYP1A2和CYP3A体内诱导作用。方法①应用P450-GloTMCYP450检测试剂盒,通过化学发光法测定SLI和经典抑制剂对细胞色素P4501A2(CYP1A2),CYP2D6,CYP3A4,CYP2C19和CYP2C9的IC50值,通过比较SLI和经典抑制剂对相应细胞色素P450亚型的IC50值来判断SLI对人CYP450酶的体外抑制作用。②Wistar大鼠分别iv给予SLI 3,10和30 mg·kg-1和诱导剂苯巴比妥钠20 mg·kg-1,采用探针底物法,通过比较代谢产物的生成速率来评价SLI对大鼠CYP1A2和CYP3A的诱导作用。③应用ATP酶检测试剂盒,通过化学发光法测定ATP酶活性来评价SLI是否为P-gp的底物或抑制剂。结果①CYP1A2,CYP2C9,CYP2C19,CYP2D6和CYP3A4抑制剂的IC50与SLI对其的IC50进行比较(CYP1A2:0.12μmol·L-1vs 840μmol·L-1;CYP2C9:3.362μmol·L-1vs 704μmol·L-1;CYP2C19:3.236μmol·L-1vs 306μmol·L-1;CYP2D6:0.117μmol·L-1vs 2660μmol·L-1;CYP3A4:0.078μmol·L-1vs 1780μmol·L-1)。②与空白对照组(86.4±6.3)nmol·g-1.min-1相比,SLI 3,10和30 mg·kg-1组CYP1A2活性分别为83.4±6.6,82.5±4.0和(83.4±6.6)nmol·g-1.min-1。与空白对照组(16.1±0.9)nmol·g-1.min-1比较,SLI 3,10和30 mg·kg-1组CYP3A活性分别为15.7±0.6,15.9±0.7和(15.9±1.0)nmol·g-1.min-1,无显著性差异。③以临床血药浓度为依据设计的一系列浓度的SLI 0.0002,0.0006,0.002,0.006,0.017,0.052,0.156和0.468 g.L-1的ATP酶活性分别与空白对照组进行比较(5.8,5.3,5.8,5.5,5.8,5.2,,5.8,5.3,vs 5.75μmol·g-1.min-1),无显著性差异。结论SLI临床给药剂量既不能体外抑制人CYP1A2,CYP2D6,CYP3A4,CYP2C19和CYP2C9酶活性,也不能诱导大鼠CYP1A2和CYP3A,同时也不是P-gp的体外抑制剂或底物。

细胞色素P450 CYP2E1酶构型特征及其表达调控机制的研究进展

细胞色素P450CYP2E1酶参与代谢活化及失活多种前毒物、前致癌物和少数药物。在细胞色素P450超家族中,CYP2E1具有易介导自由基生成引发氧化应激反应的特征。CYP2E1表达水平可能是机体对环境和工业毒物或致癌物敏感程度的重要因素。研究表明,CYP2E1可被多种内、外源性物质所调控,并且CYP2E1的药理和毒理学功能与其以蛋白构型为基础的代谢行为密切相关。本文综述了CYP2E1基因多态性、酶构型特征与其代谢活性间的关系,并分析了其区别于其他细胞色素P450亚型的表达调控机制。

3Gyγ射线照射和丝裂霉素C对大鼠肝脏细胞色素P450含量及其同工酶CYP2B1、CYP2E1活性的影响

为研究3Gyγ射线全身照射和丝裂霉素C(MitomycinC,MMC)对雄性(Sprague-Dawley,SD)大鼠肝脏细胞色素P450含量、CYP2B1、CYP2E1活性的影响,分别给大鼠腹腔注射1mg/kgd的MMC(分1d,连续3d及6d用药三组),3mg/kg的MMC1d,3Gyγ射线全身照射,3Gyγ射线全身照射加1d3mg/kgMMC,另设空白对照和溶剂对照。各组处理结束后24h,处死大鼠取肝脏,制备微粒体,测P450含量、CYP2B1、CYP2E1活性。实验结果表明,给MMC1mg/kgd,1d后P450含量、CYP2B1活性变化无统计学差异(p>0.05),CYP2E1活性明显上升(p<0.01);连续3d或6d后,P450含量、CYP2B1、CYP2E1活性均无明显变化(p>0.05)。给3mg/kg的MMC1d,对P450含量、CYP2B1活性影响无统计学差异(p>0.05),CYP2E1活性上升明显(p<0.01);3Gyγ射线全身照射后,P450含量、CYP2B1活性无明显变化(p>0.05),CYP2E1活性下降(p<0.05);分析发现,3mg/kgMMC与3Gyγ射线之间没有交互作用。结果提示,γ射线可以抑制雄性SD大鼠肝脏CYP2E1活性,MMC对CYP2E1活性有诱导作用,但多次刺激使其耐受,P450含量、CYP2B1活性对γ射线、MMC不敏感。

石膏水煎液对肝微粒体细胞色素P450酶系中CYP1A2和CYP2E1的影响

目的:研究石膏水煎液对肝微粒体细胞色素P450酶CYP1A2和CYP2E1活性的影响,指导临床合理用药。方法:采用双抗体夹心酶联免疫吸附试验(ELISA)对肝脏细胞色素P450酶CYP1A2和CYP2E1进行了初步研究。结果:与空白对照组比较,石膏水煎液对大鼠肝脏中的CYP1A2含量有降低的趋势,对CYP2E1的含量没有显著影响。结论:石膏对大鼠肝微粒体CYP1A2活性有抑制作用,临床上当与经过CYP1A2代谢的药物合用时应适当调整药量。

细胞色素P4502E1(CYP2E1)与胃癌遗传易感性

为探讨细胞色素P4502E1(CYP2E1)基因变化与胃癌易感的关系,采用病例—对照分子流行病学研究方法和多聚酶链反应技术—限制性片段长度多态性(PCR—RFLP),对142例胃癌患者和167例正常对照者CYP2E1基因RsaⅠ酶切位点进行多态性分析。结果显示胃癌患者和正常对照人群在基因型和等位基因频率上均无显著的统计学差异;我国人群CYP2E1 RsaⅠ酶切位点多态性的分布频率与日本人群相近,与欧美人群差异较大。

来氟米特对急性化学性肝损伤小鼠肝Cyt.P450酶含量及CYP2E1 mRNA表达的影响

目的观察来氟米特(Lef)作用前后急性化学性肝损伤小鼠肝微粒体细胞色素P450(Cyt.P450)、细胞色素b5(Cyt.b5)含量及P4502E1(CYP2E1)mRNA表达水平的变化,进一步研究其治疗机制。方法采用CCl4诱导小鼠急性化学性肝损伤模型,检测血清丙氨酸氨基转移酶(ALT)、天冬氨酸氨基转移酶(AST)活性,肝匀浆丙二醛(MDA)、谷胱甘肽(GSH)含量以及肝微粒体细胞色素P450(Cyt.P450)和细胞色素b5(Cyt.b5)含量,RT-PCR法检测小鼠肝脏细胞色素P4502E1(CYP2E1)mRNA表达水平,并作肝组织切片病理观察。结果Lef明显降低CCl4急性肝损伤小鼠血清ALT、AST水平;降低肝匀浆MDA含量;提高GSH含量并提高肝微粒体Cyt.P450、Cyt.b5含量;抑制CYP2E1 mRNA表达;减轻肝脏病理损伤。结论Lef治疗CCl4所致小鼠急性化学性肝损伤,可能与其诱导肝微粒体Cyt.P450表达,抑制CYP2E1 mRNA转录及抗脂质过氧化有关。

柴胡水提液对大鼠肝CYP450酶含量及其亚型CYP3A、CYP2E1和CYP1A2活性的影响

目的:研究柴胡水提物对大鼠细胞色素CYP450酶含量及对亚型CYP3A、CYP2E1和CYP1A2活性的影响。方法:大鼠灌胃给予柴胡水提液7d后取肝脏称重并制备肝微粒体,紫外分光光度法测定肝微粒体细胞色素b5(Cytb5)、P450的含量及CYP3A的活性,高效液相法测定CYP2E1和CYP1A2的活性。结果:与空白对照组比较,柴胡水提液组大鼠肝指数无显著变化,CYP450含量减少但统计学意义(P>0.05),CYP1A2活性极显著降低(P<0.01),CYP2E1活性明显降低(P<0.05)。结论:柴胡水提液降低大鼠肝脏CYP450酶含量并抑制CYP2E1和CYP1A2的活性,由于抑制CYP450酶活性,减少对其他药代谢,提示若柴胡水提液与经CYP2E1和CYP1A2代谢的药物同用,有可能会影响这些药物的临床疗效,临床用药时应慎重考虑。

CYP2E1基因多态和血清硒水平与肺癌关系的研究

目的：探讨CYP2E1基因RsaⅠ多态性单独作用和血清硒水平联合作用时与肺癌危险性的关系。方法：采用成组病例一对照研究方法，选择广州地区原发性肺癌患者58例，对照62例，制定统一调查表进行调查，用PCR检测CYP2E1基因多态性，用GHAFS测定血清硒。结果：CYP2E13种基因型在病例组与对照组的总体分布无统计学意义（X^2=1.578，P=0．454），CYP2E1多态性单独作用时与肺癌危险性关系无统计学意义（P〉0．05）；血清硒水平低（〈0．109mg／L）联合CYP2E1 C1C1基因型时OR为9．86（95％CI=1．13～85．99）。结论：CYP2E1基因单独作用与广州地区肺癌关系不明显，但血清硒水平低与CYP2E1 C1C1基因型之间存在协同作用，使肺癌发生的危险性显著增加。

细胞色素 P450 2E1 的研究进展

ＣＹＰ２Ｅ１在药物和人们经常接触的溶剂与环境污染物的代谢中具有重要作用。本文综述ＣＹＰ２Ｅ１的结构特点、基因、底物和探药以及影响其活性的主要因素。

CYP1A1、CYP2E1基因多态性与癌症易感性的研究进展

人类细胞色素P450(CYP450)在多种内源性及外源性物质的生物代谢中起重要作用。大多数CYP450存在基因多态性,其中CYP1A1、CYP2E1两个基因多态性与癌症的发生密切相关。本文综述了近年来人类细胞色素P4501A1(CYP1A1)和P4502E1(CYP2E1)与癌症易感性之间关系的研究进展。

柴胡总皂苷对小鼠肠道首过效应和肝脏Cyp3a、Cyp2e1的影响

目的:研究柴胡总皂苷对小鼠肠道首过效应(Cyp3a,P-糖蛋白)和肝脏细胞色素氧化酶(Cyp3a,Cyp2e1)的影响。方法:供试物灌胃给小鼠2次/d,连续3 d。实验当日,对乙酰氨基酚(Acetaminophen,APAP;P-gp底物)以50 mg/kg经口投予后60 min断头采血,并摘取肝脏和全段小肠。以分光光度法测定血中APAP浓度;用梯度离心法分离小鼠肝/肠微粒体;以分光光度法检测微粒体中Cyp3a/Cyp2e1活性;以实时荧光定量法测定Cyp3a11/Cyp2e1 mRNA在小鼠肝脏中的表达。结果:血中APAP浓度测定结果和P-糖蛋白偶联的ATP酶活性测定结果显示,柴胡总皂苷各剂量组与对照组之间均无统计学差异(P>0.05);在肝脏和肠道微粒体实验中不论以氨基吡啉还是以红霉素为底物测定Cyp3a,仅有柴胡总皂苷高剂量组(150 mg/kg)的Cyp3a活性显著高于对照组(P<0.05);仅有柴胡总皂苷中剂量组(75 mg/kg)的Cyp2e1活性显著低于对照组(P<0.05);RT-PCR结果显示,仅有柴胡总皂苷高剂量(150 mg/kg)时能够诱导Cyp3a11在肝脏中的表达。结论:柴胡总皂苷对小鼠肝脏和肠道中的Cyp3a具有一定的诱导作用,对肝脏中的Cyp2e1具有一定的抑制作用,对小鼠肠道P-糖蛋白的转运活性无影响。

新生儿基因CYP2E15′端RsaⅠ和PON2311位点多态性与早产的关系

探讨新生儿基因细胞色素P4 5 0 2E1(CYP2E1) 5′端RsaⅠ多态性和对氧磷酶 2 (二乙基对硝基苯磷酸酯酶 2 )基因 311位点 (PON2 311)多态性对早产的影响。采用横断面调查方法 ,使用统一的调查表 ,由安庆市各县医院对入院分娩孕妇及其单胎、活产、早产和对照新生儿进行调查 ,共得到有效样本 194个母亲 -新生儿对。单因素分析结果显示 :CYP2E1野生纯合子基因型 (cut/cut)与突变纯合子基因型 (uncut/uncut) /杂合子基因型 (cut/uncut)比较 ,对早产的影响不具有统计学意义。而PON2Ser311Ser纯合子基因型与Cys311Cys纯合子基因型 /Cys311Ser杂合子基因型比较 ,对早产的影响具有显著的统计学意义。进一步分析CYP2E15′端RsaⅠ位点多态性和PON2 311位点多态性是否存在交互作用 ,结果显示 :CYP2E1野生纯合子基因型和PON2Ser311Ser纯合子基因型这一组合与参照组比较 ,对早产的影响具有显著的统计学意义。基因CYP2E15′端RsaⅠ位点多态性与新生儿早产不相关 ,但基因PON2 311位点多态性与新生儿早产相关 ,且CYP2E15′端RsaⅠ位点多态性和PON2 311位点多态性之间对早产的影响存在交互作用。

免疫性肝损伤中一氧化氮诱生对CYP2E1表达及代谢活性的影响

目的:研究BCG诱发啮齿类免疫性肝损伤过程中NO诱生对CYP2E1表达及代谢活性的影响. 方法:采用尾静脉注射BCG诱发小鼠及大鼠产生免疫性肝损伤,紫外分光光度法测定肝微粒体中CYP450全酶含量, 免疫组化法测定肝组织CYP2E1蛋白表达,HPLC法测定经CYP2E1代谢的探针药物氯唑沙宗血药浓度经时变化. 结果:BCG刺激可致肝组织炎性细胞浸润形成大量肉芽肿, 肝微粒体CYP450全酶含量降低,肝脏CYP2E1蛋白表达下调,CYP2E1代谢底物氯唑沙宗血药浓度-时间曲线右移.选择性iNOS抑制剂氨基胍可逆转BCG所致肝脏CYP450全酶含量降低,增加CYP2E1蛋白表达,增强CYP2E1对探针药物氯唑沙宗的代谢活性. 结论:NO诱生机制参与了BCG免疫性肝损伤中CYP450全酶含量降低,CYP2E1表达下调及代谢活性的下降.

普洱茶(熟茶)茶粉、黑茶茶粉、六堡茶对非酒精性脂肪肝大鼠肝细胞CYP2E1表达的影响

背景:CYP2E1是一种可被乙醇诱导的细胞色素P450酶。在非酒精性脂肪性肝病发病机制的"二次打击"学说中,CYP2E1介导的脂质过氧化发挥重要作用。目的:从改善氧化应激的角度探讨普洱茶(熟茶)茶粉、黑茶茶粉和六堡茶对非酒精性脂肪肝(NAFL)模型大鼠的辅助保护作用。方法:120只Wistar大鼠分为正常对照组、高脂模型组、降脂药物组以及低、中、高剂量(0.5、1.0、2.0 g/kg)普洱茶(熟茶)茶粉、黑茶茶粉、六堡茶组。以高脂饮食诱导NAFL模型,实验组予相应品种、剂量的茶汤灌胃35 d。处死大鼠,测定肝组织抗氧化指标,real time PCR检测肝细胞CYP2E1 mRNA表达,同时观察肝脏组织学表现。结果:适宜剂量的普洱茶(熟茶)茶粉和六堡茶能显著降低高脂模型大鼠的肝组织MDA含量,增高SOD、GSH-Px活性,抑制肝细胞CYP2E1 mRNA表达(P均<0.05)。高剂量六堡茶组肝脏组织学表现为轻度脂肪肝,高剂量普洱茶(熟茶)茶粉组和黑茶茶粉组表现为中度脂肪肝。结论:普洱茶(熟茶)茶粉和六堡茶对NAFL大鼠模型的肝脏抗氧化指标、CYP2E1基因表达和组织学表现具有积极作用,表明两者对NAFLD可发挥辅助保护作用,六堡茶的作用更为明显。