Inhibitory effects of patchouli alcohol on stress-induced diarrhea-predominant irritable bowel syndrome

AIM To elucidate the mechanism of patchouli alcohol(PA) in treatment of rat models of diarrhea-predominant irritable bowel syndrome(IBS-D).METHODS We studied the effects of PA on colonic spontaneous motility using its cumulative log concentration(3 × 10^(-7) mol/L to 1 × 10^(-4)mol/L). We then determined the responses of the proximal and distal colon segments of rats to the folowing stimuli:(1) carbachol(1 × 10^(-9) mol/L to 1 × 10^(-5) mol/L);(2) neurotransmitter antagonists including N~ω-nitro-l-arginine methyl ester hydrochloride(10μmol/L) and(1 R~*, 2 S~*)-4-[2-Iodo-6-(methylamino)-9 Hpurin-9-yl]-2-(phosphonooxy)bicyclo[3.1.0]hexane-1-methanol dihydrogen phosphate ester tetraammonium salt(1 μmol/L);(3) agonist α,β-methyleneadenosine 5′-triphosphate trisodium salt(100 μmol/L); and(4) single KCl doses(120 mmol/L). The effects of blockers against antagonist responses were also assessed by pretreatment with PA(100 μmol/L) for 1 min. Electrical-field stimulation(40 V, 2-30 Hz, 0.5 ms pulse duration, and 10 s) was performed to observe nonadrenergic, noncholinergic neurotransmitter release in IBS-D rat colon. The ATP level of Kreb's solution was also determined.RESULTS PA exerted a concentration-dependent inhibitory effect on the spontaneous contraction of the colonic longitudinal smooth muscle, and the half maximal effective concentration(EC_(50)) was 41.9 μmol/L. In comparison with the KCl-treated IBS-D group, the contractile response(mg contractions) in the PA + KCl-treated IBS-D group(11.87 ± 3.34) was significantly decreased in the peak tension(P < 0.01). Compared with CCh-treated IBS-D rat colon, the cholinergic contractile response of IBS-D rat colonic smooth muscle(EC_(50) = 0.94 μmol/L) was significantly decreased by PA(EC_(50) = 37.43 μmol/L)(P < 0.05). Lack of nitrergic neurotransmitter release in stress-induced IBS-D rats showed contraction effects on colonic smooth muscle. Pretreatment with PA resulted in inhibitory effect on l-NAME-induced(10 μmol/L) contraction(P < 0.05). ATP might not be the main neurotransmitter involved in inhibitory effects of PA in the colonic relaxation of stressinduced IBS-D rats.CONCLUSION PA application may serve as a new therapeutic approach for IBS-D.

Lactoferrin-mediated macrophage targeting delivery and patchouli alcohol-based therapeutic strategy for inflammatory bowel diseases

Inflammatory bowel diseases(IBD)are the incurable chronic recurrent gastrointestinal disorders and currently lack in safe and effective drugs.In this study,patchouli alcohol,a main active compound of traditional Chinese herb patchouli,was developed into biomimetic liposomes for macrophagetargeting delivery for IBD treatment.The developed lactoferrin-modified liposomes(LF-lipo)can specifically bind to LRP-1 expressed on the activated colonic macrophages and achieve cell-targeting anti-inflammatory therapy.LF-lipo reduced the levels of inflammatory cytokines and ROS and suppressed the MAPK/NF-κB pathway.LF-lipo also suppressed the formation of NLRP3 inflammasome and the consequent IL-1βactivation.LF-lipo showed improved therapeutic efficacy in a DSS-induced colitis murine model,evidenced by the reduced disease activity index,the improved colon functions,and the downregulated inflammatory cytokines in the colon.LF-lipo provided an effective and safe macrophagetargeting delivery and therapeutic strategy for addressing the unmet medical need in IBD management.

In Vitro and In Vivo Antibacterial Activity of Patchouli Alcohol from Pogostemon cablin

Objective:To investigate the antibacterial activity of patchouli alcohol(PA)against 127 bacteria strains,including the common bacteria and drug-resistant bacteria strains both in the in vitro and in vivo tests.Methods:For the in vitro trial,the antibacterial property of PA against 107 Gram-positive and 20 Gram-negative bacteria strains was screened by agar double dilution method.For the in vivo trial,specific pathogen free Kunming strain of both male and female white mice,were used to test the protective ability of PA after being injected with the median lethal dose of the tested strains.Results:PA possessed antibacterial activity against all the tested 127 strains.In the in vitro test,PA could inhibit both Gram-negative bacteria(25-768μg/m L)and Gram-positive bacteria(1.5-200μg/m L).Particularly,PA was active against some drug-resistant bacteria like methicillin-resistant Staphylococcus aureus(MRSA).PA also exhibited in vivo anti-MRSA activity in mice via intraperitoneal injection.PA could protect mice entirely infected with MRSA at 100 and 200 mg/kg,while 80% mice injected with MRSA could be protected at a low dose of 50 mg/kg.Conclusion:PA might be a potential antibacterial drug from natural sources and might be worthy to explore its mechanism and application in further study.

Anti-nociceptive Effect of Patchouli Alcohol: Involving Attenuation of Cyclooxygenase 2 and Modulation of Mu-Opioid Receptor

Objective: To explore the anti-nociceptive effect of patchouli alcohol(PA), the essential oil isolated from Pogostemon cablin(Blanco) Bent, and determine the mechanism in molecular levels. Methods: The acetic acid-induced writhing test and formalin-induced plantar injection test in mice were employed to con?rm the effect in vivo. Intracellular calcium ion was imaged to verify PA on mu-opioid receptor(MOR). Cyclooxygenase 2(COX2)and MOR of mouse brain were expressed for determination of PA’s target. Cellular experiments were carried out to find out COX2 and MOR expression induced by PA. Results: PA significantly reduced latency period of visceral pain and writhing induced by acetic acid saline solution(P<0.01) and allodynia after intra-plantar formalin(P<0.01) in mice. PA also up-regulated COX2 mRNA and protein(P<0.05) with a down-regulation of MOR(P<0.05) both in in vivo and in vitro experiments, which devote to the analgesic effect of PA. A decrease in the intracellular calcium level(P<0.05) induced by PA may play an important role in its anti-nociceptive effect.PA showed the characters of enhancing the MOR expression and reducing the intracellular calcium ion similar to opioid effect. Conclusions: Both COX2 and MOR are involved in the mechanism of PA’s anti-nociceptive effect,and the up-regulation of the receptor expression and the inhibition of intracellular calcium are a new perspective to PA’s effect on MOR.

A formal synthesis of (-)-patchouli alcohol from (-)-carvone

Enantiomerically pure 6-acetyl-1,3,3-trimethyl bicyclo[2.2.2]octan-2-one,a key inter- mediate for synthesis of(-)-patchouli alcohol,was facilely synthesized from the adduct of a monome- thylated(-)-carvone 2 and methyl acrylate.

靶向表皮生长因子受体的百秋李醇纳米颗粒抑制非小细胞肺癌裸鼠皮下移植瘤生长的作用及机制

目的探讨靶向表皮生长因子受体(EGFR)的百秋李醇(PA)纳米颗粒对非小细胞肺癌(NSCLC)肿瘤生长的抑制作用及其机制。方法①利用二硬脂酰基磷脂酰乙醇胺-聚乙二醇-EGFR靶向肽AA1(DSPE-PEG-AA1)脂质体负载PA,构建靶向EGFR的PA脂质体纳米颗粒(EGFR-PA-NP)。②将人NSCLC A549细胞(2×106个/只)接种于裸鼠腋下,建立肺癌异种皮下移植瘤裸鼠模型。10只模型裸鼠随机分为PA脂质体纳米颗粒(PA-NP)组和EGFR-PA-NP组(n=5),分别尾静脉注射给予20 mg·kg^(-1)相应药物,24 h后剥取肿瘤、癌旁、肝、肺、心、脑、肾、脾、胃、小肠等组织,液相色谱-质谱(LC-MS)法检测药物在体内的组织分布情况。③20只模型裸鼠随机分为模型组(100μL)、PA组(15 mg·kg^(-1))、PA-NP组(15 mg·kg^(-1))和EGFR-PA-NP组(15 mg·kg^(-1))(n=5),分别尾静脉注射给予相应干预,隔日1次,共28 d。28 d后观察药物对裸鼠皮下移植瘤生长的影响。通过原位末端转移酶标记(TUNEL)检测法检测皮下移植瘤中肿瘤细胞凋亡情况,免疫荧光染色法检测皮下移植瘤中血小板-内皮细胞黏附分子(CD31)表达情况,免疫组化染色法和Western blot法检测皮下移植瘤中蛋白激酶B(Akt)、磷酸化(p)-Akt、哺乳动物雷帕霉素靶蛋白(mTOR)和p-mTOR表达水平。结果①制备的EGFR-PA-NP粒径为(122±6.90)nm、Zeta电位为(-24.28±3.76)mV、包封率为85.24%、载药量为8.09%,符合纳米颗粒特征。②LC-MS法检测药物组织分布结果显示,EGFR-PA-NP组药物在裸鼠瘤体内的富集量是PA-NP组的3倍,显著高于PA-NP组(P<0.05)。③在裸鼠A549皮下移植瘤模型中,PA组、PA-NP组和EGFR-PA-NP组裸鼠瘤体体积明显小于模型组(P<0.05),而EGFR-PA-NP组瘤体体积明显小于PA-NP组(P<0.05)。与PA-NP组相比,EGFR-PA-NP组肿瘤中凋亡细胞数量显著增加(P<0.05),CD31蛋白表达水平显著降低(P<0.05),并且p-Akt、p-mTOR表达水平显著降低(P<0.05)。结论EGFR-PA-NP能够通过促进肿瘤细胞凋亡、抑制肿瘤血管新生发挥抗肺癌作用,其机制与抑制Akt/mTOR通路激活相关。

广藿香醇合酶PcPTS互作蛋白的筛选与鉴定分析

【目的】广藿香[Pogostemon cablin(Blanco)Benth.]是临床常用的芳香化湿药,其质量指标成分广藿香醇具有良好的抗病毒、抗炎症等活性。广藿香醇合酶(Patchouli alcohol synthase,PcPTS)在广藿香醇生物合成途径中起关键作用,但其在蛋白互作层面调控广藿香醇合成的机制尚不清楚。旨在筛选PcPTS的互作蛋白,以揭示PcPTS在广藿香醇生物合成途径中的调控机制和功能。【方法】利用酵母双杂交技术和GST pull-down联合液相色谱-串联质谱(LC-MS/MS)技术筛选可能与PcPTS互作的蛋白,利用MASCOT软件和BLAST分析注释互作蛋白,选取有文献报道参与其他蛋白互作、影响蛋白转运、修饰或降解、参与次生代谢调控的蛋白,利用酵母双杂交技术初步验证它们与PcPTS蛋白的互作关系并对互作蛋白进行生物信息学分析。【结果】通过PCR技术成功克隆了PcPTS的cDNA序列,开放阅读框(ORF)为1659 bp,编码522个氨基酸。构建了广藿香cDNA初级文库和酵母杂交文库,初级和次级文库容量分别为7.6×10^(6) CFU和8.6×10^(6) CFU,初级和次级文库的重组率均为100%,且插入片段平均长度均大于800 bp。构建的诱饵载体pGBKT7-PcPTS对酵母菌株不产生毒性,且无自激活活性。利用酵母双杂交筛选得到阳性克隆并进行测序和BLAST分析,获得17个候选蛋白。成功构建了GST-PcPTS表达载体,诱导表达纯化获得GST-PcPTS诱饵蛋白,利用诱饵蛋白从广藿香总蛋白中捕获互作蛋白,共鉴定出98个候选互作蛋白。从候选蛋白中筛选14个可能与PcPTS互作的蛋白,利用酵母双杂交进行点对点验证,结果发现PcC3H6、PcENO3、PcACR11和PcHAD与PcPTS存在相互作用。生物信息分析表明,四者分别属于CCCH锌指蛋白家族、烯醇化酶蛋白、ACR亚家族和HAD-like超家族。【结论】初步筛选验证获得与PcPTS存在相互作用的4个蛋白PcC3H6、PcENO3、PcACR11和PcHAD,有助于揭示PcPTS在广藿香醇生物合成途径中的作用机制,也为进一步研究广藿香醇的合成调控机制奠定了坚实基础。

广藿香醇下调PD-L1的表达对人胃癌细胞抗肿瘤作用的研究

目的研究广藿香醇能否通过下调人胃癌细胞中关键促癌因子PD-L1的表达进而抑制人胃癌细胞的恶性行为以及下调PD-L1表达的机制。方法使用不同剂量的广藿香醇作用于常规培养的人胃癌细胞SGC-7901和BGC-823,用CCK-8实验、细胞划痕实验和流式细胞技术分别检测不同浓度的广藿香醇对SGC-7901和BGC-823细胞的增殖能力、迁移能力和凋亡能力的影响,用荧光定量PCR法检测SGC-7901和BGC-823细胞中PD-L1、NF-κB的mRNA表达水平的变化,用Western-blot法检测SGC-7901和BGC-823细胞中PD-L1、NF-κB的蛋白表达水平的变化。结果经实时荧光定量PCR法检测人胃正常上皮细胞GSY和胃癌细胞系细胞BGC-823、MGC-803、SGC-7901、MKN-74中mRNAPD-L1、NF-κB mRNA表达水平,最终筛选出BGC823、SGC7901进行后续实验。与对照组比较,0.08、0.1、0.3、0.5 mmol/L药物组中BGC-823、SGC-7901细胞的增殖能力显著降低,且降低幅度随加药浓度升高而增大。经计算SGC-7901的IC_(50)浓度为0.37 mmol/L,BGC-823的IC_(50)浓度为0.27 mmol/L,因此选择浓度为0.3 mmol/L、0.5 mmol/L的广藿香醇进行后续实验。与人胃癌细胞SGC-7901、BGC-823的对照组比较,广藿香醇各加药组细胞的划痕愈合率均有明显下降,差异有统计学意义(P<0.05),并且0.3、0.5 mmol/L的广藿香醇对BGC823细胞的划痕愈合率的影响更为显著。经AnnexinV-FITC/PI双染后,0.3、0.5 mmol/L广藿香醇作用后能明显诱导SGC-7901、BGC-823细胞发生凋亡。加药组(广藿香醇浓度分别为0.3,0.5 mmol/L)作用于SGC-7901、BGC-823细胞24 h后,细胞凋亡率显著高于对照组(P<0.05),并且广藿香醇对SGC-7901、BGC-823细胞的凋亡作用呈剂量依赖,与对照组比较,0.3、0.5 mmol/L加药组的两种胃癌细胞的凋亡率均显著提高(P<0.05)。在SGC-7901中,与对照组比较,广藿香醇各加药组细胞中PD-L1、NF-κB的mRNA均明显下降(P<0.05);在BGC-823中,与对照组比较,广藿香醇各加药组细胞中PD-L1、NF-κB的mRNA均明显下降(P<0.05)。在SGC-7901细胞中,与对照组比较,广藿香醇各加药组细胞中PD-L1、NF-κB的蛋白表达含量均明显下降(P<0.05);在BGC-823细胞中,与对照组比较,广藿香醇各加药组细胞中PD-L1、NF-κB的蛋白表达含量均明显下降(P<0.05)。结论广藿香醇可以通过下调PD-L1的表达抑制胃癌细胞的恶性行为,并且这种作用机制与广藿香醇抑制胃癌细胞中NF-κB的表达有关。

广藿香化学诱变植株SRAP遗传特性及质量研究

目的:研究广藿香化学诱变植株的遗传特性和品质差异。方法:以前期经氟乐灵、亚硝酸钠及亚硫酸钠诱变后筛选出的变异植株为材料,对其基因组DNA进行相关序列扩增多态性(SRAP)分析,并测定其主要有效成分含量。结果:10对SRAP引物扩增的总位点数为235个,其位点数为16~29个,而多态位点数为220个,平均多态性百分比达86.96%;广藿香变异植株的遗传相似系数为0.445~0.938,其变异程度大于不同产地种群间的变异程度;当遗传相似系数为0.55时,变异程度较大的植株N1a、N1b、N1c、S4c、S4d、S6c聚为一类,其他与CK聚为另一类。变异植株主要化学成分百秋李醇及广藿香酮含量与CK差异均有统计学意义(P<0.05),其中变异植株F1、F2a、F4a、F4d、F4e、F6e、F8i、N2c、N2d的广藿香酮明显升高,且高于百秋李醇的含量,由“醇型”广藿香转变为“酮型”广藿香;变异植株F4c、F6d、F8j、N1a、N1b、N1c、S3b、S4c、S4d、S6b、S6c的百秋李醇或广藿香酮含量均显著高于CK。结论:化学诱变是广藿香新品种选育的有效途径,可提高其遗传多态性,影响其有效成分的合成和积累;变异植株F1、F2a、F4a、F4b、F4d、F4e、F6e、F8i、F10d、N2c、N2d、N1a、N1b、N1c、S4c、S4d、S6c具有开发潜能,可为后续研究提供材料。

防暑清热饮的质量控制

为建立防暑清热饮中总多酚和挥发性成分含量的测定方法,通过酒石酸亚铁法测定总多酚的含量,顶空气相色谱法测定薄荷酮、薄荷脑和百秋李醇的含量。结果总多酚、薄荷酮、薄荷脑和百秋李醇线性关系良好(r≥0.9991),平均加样回收率(RSD)分别为103.62%(2.33%)、90.29%(2.81%)、95.36%(3.49%)和90.20%(3.94%)。建立的测定方法简单、灵敏,能够准确测定该制剂中总多酚和挥发性指标成分的含量。

藿香清胃胶囊中百秋李醇含量的测定

为了建立毛细管柱气相色谱法测定藿香清胃胶囊中百秋李醇的含量。样品经正己烷超声提取后采用气相色谱法进行含量测定。色谱柱为DB-5毛细管柱(30 m×0.25 mm×0.25μm);柱温采用程序升温,初始温度为180℃,保持7 min,再以40℃/min的速率升温至280℃,保持5 min;进样口温度为280℃;FID检测器温度为280℃;载气为氮气,色谱柱流量为3.0 mL/min,分流比为5∶1;进样量为1μL。结果显示,百秋李醇在0.2312μg~6.9360μg/mL的浓度范围内与峰面积呈良好线性关系(相关系数r=0.9994);平均回收率为99.35%,RSD=1.16%(n=9)。该方法操作简单方便,灵敏度高,可作为藿香清胃胶囊中百秋李醇含量的检测方法。

分子蒸馏技术用于广藿香油纯化工艺的研究

目的 :建立一种先进的分离纯化广藿香油的技术。方法 :采用分子蒸馏技术对广藿香油进行分离纯化。结果 :得到 4个馏分 ,经GC MS检测 ,馏分Ⅱ和Ⅲ中广藿香醇和广藿香酮 2种有效成分的含量与广藿香原油相比提高了 2 7%～ 4 7%。结论 :用分子蒸馏分离技术能有效地提高广藿香油中广藿香醇和广藿香酮的含量 。

广藿香化学成分的研究

从广藿香的全草及挥发油中分得９种化合物，经理化常数和光诸分析鉴定为广藿香醇（１），广藿香酮（２），木栓酮（３），表木栓醇（４），３，３’，７－三甲氧－４’，５．二羟黄酮（５），３，３’，４’，７－四甲氧－５－羟黄酮（６），齐墩果酸（７），β－谷甾（８），胡萝卜甙（９）。除化合物１，２和５外均为首次从该植物中分离得到。

顶空固相微萃取-气相色谱质谱法定性定量分析广藿香中的挥发性成分

采用顶空固相微萃取-气相色谱质谱法(HS-SPME/GC-MS)定性定量分析广藿香药材中的挥发性成分。以百秋里醇的峰面积为指标,确定HS-SPME最佳的实验条件为:160目药材粉末用无水Na2SO4稀释10倍,称取30mg于15mL萃取瓶中,以250r/min速度搅拌预热(80℃)40min,插入65μm聚二甲基硅烷-二乙烯(PDMS-DVB)涂层的纤维头,在相同搅拌速度下80℃萃取40min,纤维头进入GC进样口在250℃下解吸100s。GC色谱条件:色谱柱为DB-5MS柱;载气流速为1mL/min;柱温的起始温度为90℃,以0.8℃/min升至110℃,保持5min;1.0℃/min升至134℃,保持5min;最后以5.0℃/min升至143℃,保持10min。结果:百秋里醇的平均回收率为91.8%,RSD为3.0%。运用本方法对10份不同产地广藿香中百秋里醇的含量进行测定,并以其为参比对照,测定了广藿香中其它主要挥发性成分的含量。

广藿香醇及广藿香油中广藿香醇在大鼠体内药代动力学比较

目的 建立毛细管气相色谱法测定大鼠血浆中广藿香醇的方法;比较广藿香醇和广藿香油单次静脉注射给药后,广藿香醇在大鼠体内的药代动力学差异。方法 以丁香酚为内标;用毛细管气相色谱法,色谱柱为HP-5MS毛细管气相色谱柱(30 m×0.32 mm×0.25μm);氢火焰离子化检测器;用程序升温法,初始温度80℃,保持1 min;15℃·min-1升温至200℃,保持1min;60℃·min-1升温至290℃,保持1 min。结果 广藿香醇在25～5 000μg·L-1线性关系良好(r=0.9990),定量限为25μg·L-1,检测限为10 μg·L-1,方法精密度(RSD％)小于10％,方法准确度为90％～110％。结论 该法可用于广藿香醇的药代动力学研究;广藿香醇单体与广藿香油中广藿香醇在大鼠体内的主要药代动力学参数(AUC,T1/2β,MRT等)有显著性差异。

广藿香醇的急性毒性研究

目的观察广藿香醇对小鼠的急性毒性,评价其安全性,为新药研发和临床用药提供理论依据。方法采用口服和腹腔注射给药途径,观察小鼠给予不同剂量广藿香醇花生油溶液后的死亡率,Bliss法计算半数致死量。结果广藿香醇花生油溶液的灌胃给药的LD50是4.693 g/kg,95%的置信区间上限是5.498 g/kg,下限是4.038 g/kg;广藿香醇花生油溶液的腹腔注射给药的LD50是3.145 g/kg,95%的置信区间上限是3.675 g/kg,下限是2.663 g/kg。结论广藿香醇的安全性较高,属于低毒药物。

海南广藿香药材中百秋李醇和广藿香酮的含量测定

目的建立海南广藿香药材百秋李醇和广藿香酮的含量测定方法。方法采用气相色谱法同时测定11批海南广藿香药材百秋李醇和广藿香酮含量。结果广藿香药材的质量与生长地点有直接关系。结论该方法快速、稳定可靠,可以用于广藿香药材质量评价。

广藿香醇对β-淀粉样蛋白神经毒性的抑制作用

目的研究雌激素受体卢亚型（estrogen receptor β，ERβ）选择性激动剂广藿香醇（patchouli alcohol，PA）对β-淀粉样蛋白（β-amyloidpe ptide，Aβ）片段神经毒性的体外抑制作用。方法Aβ25-35位氨基酸片段（Aβ25-35）作用于人神经母细胞瘤细胞（SH-SY5Y）之前不同浓度PA预防给药，荧光探针法检测细胞内活性氧（reactive oxygen species，ROS）水平和细胞内钙离子浓度（[Ca^2＋]；），流式细胞术检测细胞凋亡率。结果PA（0．05、0．5、5μg·ml^-1）能够抑制Aβ25-35引起的细胞内ROS水平和[Ca^2＋]；升高，使细胞凋亡减少。结论PA对Aβ25-35的神经毒性具有抑制作用。

气相色谱法测定藿香清胃片中百秋李醇的含量

目的建立藿香清胃片中百秋李醇的GC含量测定方法。方法色谱柱:HP-5柱(30m×0.32mm×0.25μm),以交联5%苯基甲基聚硅氧烷为固定相;柱温采用程序升温:起始150℃,保持23min,8℃/min升至230℃,保持2min;气化温度:280℃;检测器温度:280℃;载气为氮气,流量25mL/min,流速为0.9mL/min;进样量1μL,分流比为5∶1。结果百秋李醇在0.057～1.140mg/mL浓度范围内呈良好的线性关系,r=0.9994;平均回收率为99.38%,RSD=1.82%(n=5)。结论该方法简单、灵敏、重现性好,可作为藿香清胃片的质量控制指标之一。

GC法测定藿香正气水中百秋李醇含量

目的建立藿香正气水中广藿香油指标成分百秋李醇的定量测定方法。方法采用气相色谱法,弹性石英毛细管HP-5色谱柱;氢火焰离子化检测器。结果 GC方法学考察结果表明,百秋李醇在4.4×10-5~1.1×10-3mg范围内线性关系良好（r=0.9996）;平均加样回收率为97.82%,RSD为1.4%。结论该方法准确、灵敏、结果可靠,可作为藿香正气水质量控制方法。