液质联用法测定吴茱萸碱、吴茱萸次碱、去氢吴茱萸碱在大鼠脑脊液和脑组织中的分布

吴茱萸碱、吴茱萸次碱、去氢吴茱萸碱是吴茱萸中主要的生物碱类成分。为研究吴茱萸主要生物碱成分在大鼠脑脊液中的代谢和在脑组织中的分布,吴茱萸碱、吴茱萸次碱、去氢吴茱萸碱以1:1:1的质量比混合,以15 mg/kg的剂量灌胃给予大鼠。本文建立了同时测定大鼠脑脊液和脑组织中三个生物碱成分的液质联用方法,测定结果显示,三个生物碱成分能快速吸收进入脑脊液并分布到脑组织,并能快速消除。三个成分在脑组织中的分布特点不同,吴茱萸碱在小脑和脑干分布最多,而吴茱萸次碱和去氢吴茱萸碱分别在脑干、小脑和海马分布最多。本研究结果揭示了吴茱萸碱、吴茱萸次碱和去氢吴茱萸碱在脑内分布的差异,为进一步研究中药吴茱萸果实治疗脑病的药效物质基础提供了依据。

吴茱萸主要成分在人结肠腺癌细胞和RAW264.7巨噬细胞共培养模型中的肠道抗炎作用

生物碱是吴茱萸中一类主要活性成分,具有抗肿瘤、抗炎、镇痛和抗菌作用。本文报道吴茱萸中六个主要成分吴茱萸碱、吴茱萸次碱、去氢吴茱萸碱、吴茱萸卡品碱、二氢吴茱萸卡品碱和1-甲基-2-十一烷基-4-(1H)-喹诺酮潜在的抗炎作用。在人结肠腺癌细胞和RAW264.7巨噬细胞共培养体系中,当以2μg/m L脂多糖诱导RAW264.7巨噬细胞产生炎症反应时,吴茱萸碱、吴茱萸次碱和去氢吴茱萸碱明显下调促炎性细胞因子(Il-6,Il-1β和Tnf-α)和炎性介质,诸如环氧化酶-2(Cox-2)和诱导型一氧化氮合酶(iNos)的m RNA表达;与模型组比较,给药组跨上皮电阻增高,紧密连接渗透率降低。总之,受试化合物具有抗炎活性,此结果为进一步研究吴茱萸的抗炎机制奠定了基础。

Crosstalk between CYP2E1 and PPARα substrates and agonists modulate adipose browning and obesity

Although the functions of metabolic enzymes and nuclear receptors in controlling physiological homeostasis have been established, their crosstalk in modulating metabolic disease has not been explored.Genetic ablation of the xenobiotic-metabolizing cytochrome P450 enzyme CYP2 E1 in mice markedly induced adipose browning and increased energy expenditure to improve obesity. CYP2 E1 deficiency activated the expression of hepatic peroxisome proliferator-activated receptor alpha(PPARa) target genes,including fibroblast growth factor(FGF) 21, that upon release from the liver, enhanced adipose browning and energy expenditure to decrease obesity. Nineteen metabolites were increased in Cyp2 e1-null mice as revealed by global untargeted metabolomics, among which four compounds, lysophosphatidylcholine and three polyunsaturated fatty acids were found to be directly metabolized by CYP2 E1 and to serve as PPARa agonists, thus explaining how CYP2 E1 deficiency causes hepatic PPARa activation through increasing cellular levels of endogenous PPARa agonists. Translationally, a CYP2 E1 inhibitor was found to activate the PPARa-FGF21-beige adipose axis and decrease obesity in wild-type mice, but not in liver-specific Pparanull mice. The present results establish a metabolic crosstalk between PPARa and CYP2 E1 that supports the potential for a novel anti-obesity strategy of activating adipose tissue browning by targeting the CYP2 E1 to modulate endogenous metabolites beyond its canonical role in xenobiotic-metabolism.

静脉和灌胃给予大鼠茴香酸对羟基苯乙酯的RP-HPLC法测定和药代动力学研究

茴香酸对羟基苯乙酯(HPA)是中药羌活和宽叶羌活的主要生物活性成分之一。本文建立了一种快速、特异的反相高效液相色谱法(RP-HPLC)用于静脉(20 mg/kg)和灌胃(200 mg)/kg)给予大鼠HPA后其在大鼠血浆的测定和药代动力学研究。血浆样品经乙酸乙酯液液萃取净化后,进样RP-HPLC系统分离和测定。分析型色谱柱为DiamonsilTMODS C18;血浆样品分析的流动相为MeOH-H2O(v/v),静脉给药样品分析时为75:25,灌胃给药样品分析时为70:30;流速为1.0 mL/min,UV检测波长为256 nm。HPA标准曲线线性范围,静脉给药时为0.05-5.0μg/mL(r2=0.9984),灌胃给药时为0.5-10.0μg/mL(r2=0.9995);萃取回收率为82.01%-87.97%,日内和日间精密度为1.71%-3.99%,准确度范围为91.22%-110.5%;HPA在大鼠口服时的绝对生物利用度为48.17%。以上结果表明所建方法适合用于HPA在大鼠血浆中的测定和药代动力学研究。