18β-glycyrrhetinic acid inhibits proliferation of gastric cancer cells through regulating the miR-345-5p/TGM2 signaling pathway

BACKGROUND Gastric cancer(GC)is a common gastrointestinal malignancy worldwide.Based on cancer-related mortality,the current prevention and treatment strategies for GC still show poor clinical results.Therefore,it is important to find effective drug treatment targets.AIM To explore the molecular mechanism of 18β-glycyrrhetinic acid(18β-GRA)regulating the miR-345-5p/TGM2 signaling pathway to inhibit the proliferation of GC cells.METHODS CCK-8 assay was used to determine the effect of 18β-GRA on the survival rate of GES-1 cells and AGS and HGC-27 cells.Cell cycle and apoptosis were detected by flow cytometry,cell migration was detected by a wound healing assay,the effect of 18β-GRA on subcutaneous tumor growth in BALB/c nude mice was investigated,and the cell autophagy level was determined by MDC staining.TMT proteomic analysis was used to detect the differentially expressed autophagy-related proteins in GC cells after 18β-GRA intervention,and then the protein-protein interaction was predicted using STRING(https://string-db.org/).MicroRNAs(miRNAs)transcriptome analysis was used to detect the miRNA differential expression profile,and use miRBase(https://www.mirbase/)and TargetScan(https://www.targetscan.org/)to predict the miRNA and complementary binding sites.Quantitative real-time polymerase chain reaction was used to detect the expression level of miRNA in 18β-GRA treated cells,and western blot was used to detect the expression of autophagy related proteins.Finally,the effect of miR-345-5p on GC cells was verified by mir-345-5p overexpression.RESULTS 18β-GRA could inhibit GC cells viability,promote cell apoptosis,block cell cycle,reduce cell wound healing ability,and inhibit the GC cells growth in vivo.MDC staining results showed that 18β-GRA could promote autophagy in GC cells.By TMT proteomic analysis and miRNAs transcriptome analysis,it was concluded that 18β-GRA could down-regulate TGM2 expression and up-regulate miR-345-5p expression in GC cells.Subsequently,we verified that TGM2 is the target of miR-345-5p,and that overexpression of miR-345-5p significantly inhibited the protein expression level of TGM2.Western blot showed that the expression of autophagy-related proteins of TGM2 and p62 was significantly reduced,and LC3II,ULK1 and AMPK expression was significantly increased in GC cells treated with 18β-GRA.Overexpression of miR-345-5p not only inhibited the expression of TGM2,but also inhibited the proliferation of GC cells by promoting cell apoptosis and arresting cell cycle.CONCLUSION 18β-GRA inhibits the proliferation of GC cells and promotes autophagy by regulating the miR-345-5p/TGM2 signaling pathway.

18β- glycyrrhetinic acid inhibits apoptosis of renal tubular epithelial cells via enhancing level of BMP-7 epigenetically through targeting HDAC2

Cisplatin （CP） , a highly effective and widely used chemotherapeutic agent, has a major limitation for its nephrotoxicity. We recently identified a novel strategy for attenuating its nephrotoxicity in chemotherapy by an ef- fective adjuvant via epigenetic modification through targeting Histone deacetylase 2 （HDAC2）. Glycyrrhizic acid （GA） ,a major active component of Licorice, was described here for its new application. Molecular docking and Surface Plasmon resonance （SPR） assay firstly reported that 18βGA, GA metabolite in vivo, could directly bind to HDAC2 and prevent HDAC2 activation. The effects and mechanisms of GA and its major metabolite 18βGA were assessed in CP-induced acute kidney injury （AKI） in C57BL/6 mice, and in CP-treated HK-2 and mTEC cells lines. Terminal deoxynucleotidyl transferase dUTP nick end labeling （TUNEL） and flow cytometry （FCM） results confirmed that GA and 18βGA could inhibit apoptosis of renal tubular epithelial cells induced by CP in vivo and in vitro. Western blot and immunofluorescence results demonstrated that the expression of bone morphogenetic protein- 7 （BMP-7） , a protective molecule in renal inflammation, was clearly induced by 18βGA in AKI models while siR- NA BMP-7 could reduce the inhibitory effect of 18βGA on apoptosis. Results of current study indicated that 18βGA inhibited apoptosis of renal tubular epithelial cells via enhancing level of BMP-7 epigenetically through targeting HDAC2, therefore protecting against CP-induced AKI. These available evidence, which led to an improved under- standing of molecular recognition, suggested that 18βGA could serve as a potential clinical adjuvant in chemothera-

PDB-18C6对TI(Ⅰ),An(Ⅲ),Cu(Ⅱ)的吸附及从α轰击的金靶中分离^(199)TI

本文研究了用冠醚树脂二苯并-18-冠-6甲醛聚合物(简称PDB-18C6)对T1(Ⅰ),Au(Ⅲ),Cu(Ⅱ)的吸附行为。实验表明,在盐酸溶液中冠醚树脂的吸附效率顺序为Au(Ⅲ)>T1(Ⅰ)>Cu(Ⅱ)。用高氯酸和乙二醇乙醚淋洗T1(Ⅰ),Au(Ⅲ),它们的回收率一般在82-98.9％和98-100％。还在1.2m回旋加速器的外靶装置上,用25-27MeV的α粒子轰击金靶,累计束流强度为27μA·h,经处理分离后得到仅含0.50％^(200)T1的较高纯度的^(199)T1。

磷钨系杂多酸复合TiO_2纳米粒子的制备及光催化特性

用溶胶-凝胶法制备了磷钨系杂多酸复合的TiO2纳米粒子。利用透射电子显微镜、紫外-可见吸收光谱和傅立叶转换红外光谱对杂多酸复合TiO2纳米粒子的形貌、结构和粒径进行了表征。结果表明制备的复合TiO2纳米粒子为近球形,粒径为12～15nm,表现出量子尺寸效应,杂多酸阴离子保持原有的Keggin结构;并且对复合TiO2纳米粒子的结构进行了理论探讨。还对杂多酸复合TiO2纳米粒子的光催化活性进行了研究,表明复合的TiO2纳米粒子具有更高的光催化活性。

柴油机尾气中的碱性无机污染物引起Cu-SAPO-18脱硝催化剂的化学失活（英文）

选择性催化还原NO_x (NH_3-SCR)已是柴油机尾气处理系统中有效的NO_x减排技术.铜基分子筛催化剂作为潜在的NH_3-SCR催化剂已被广泛研究,其中具有AEI结构的Cu-SAPO-18分子筛表现出优异的脱硝活性和水热稳定性,成为柴油机尾气后处理系统潜在的替代品.然而在实际的后处理应用中,生物柴油污染物、发动机润滑剂和燃料添加剂中的一些无机组分(K, Na, S, P, Ca和Mg等)可逐渐聚集在催化剂表面,导致催化剂孔道堵塞和活性位点丢失,最终导致SCR催化剂失活.由于碱金属和碱土金属在柴油衍生物中含量较高,因而其对SCR催化剂的影响引起了人们更多的关注.本文采用浸渍法制备了掺杂不同含量碱性无机污染物(K, Na, Ca和Mg)的Cu-SAPO-18催化剂,以阐明这些污染物对Cu-SAPO-18结构、酸性位点和铜物种的影响.XRD和氮吸附实验结果表明,低含量污染物的掺入造成催化剂孔道堵塞和比表面积下降,而高含量污染物引入导致催化剂部分结构被破坏,其中高含量Na的引入造成催化剂结构破坏最为严重.H_2-TPR和EPR结果表明,污染物引入Cu-SAPO-18后,催化剂的Cu^(2+)数目减少,这是由于Cu^(2+)被K^+, Na^+, Ca^(2+)和Mg^(2+)取代造成的.被取代的Cu^(2+)由于无法位于离子交换位点上会在煅烧过程中转变成CuO和CuAl_2O_4, CuO的产生会造成催化剂孔道堵塞甚至部分骨架结构坍塌.另外,NH_3-TPD结果表明,与新鲜催化剂相比,被污染的Cu-SAPO-18催化剂总酸性位点减少,这是由于H^+和Cu^(2+)被K^+, Na^+, Ca^(2+)和Mg^(2+)取代造成Br?nsted酸和Lewis酸减少造成的.催化剂比表面积的降低、Cu^(2+)数目以及酸含量的减少最终造成催化剂失活,且催化剂失活程度随无机污染物含量的增加而增大.但不同无机组分造成催化剂的失活程度不同,其中K, Na, Ca和Mg造成Cu-SAPO-18催化剂失活程度为K> Na> Ca> Mg.此外, K, Na, Ca和Mg造成Cu-SAPO-18催化剂比表面积、Cu^(2+)含量以及酸含量的减少程度分别为Na> K> Ca> Mg, Na> K> Mg> Ca和K> Na> Ca> Mg.其中酸含量下降程度与催化剂失活程度一致,表明在某种程度上,酸含量对催化剂NH_3-SCR活性的影响高于催化剂结构和Cu^(2+)对活性的影响.最后,我们还通过NH3-SCR动力学测试研究了K, Na, Ca和Mg对Cu-SAPO-18催化NH_3-SCR反应机理的影响,结果显示新鲜催化剂和被污染催化剂具有相近的活化能,表明无机污染物对Cu-SAPO-18催化NH3-SCR反应机理没有影响.

维甲酸受体反应蛋白2活化NLRP3炎症小体在慢性阻塞性肺疾病炎性损伤中的作用机制研究

目的:探究维甲酸受体反应蛋白2(RARRES2)是否通过调控核苷酸结合寡聚化结构域样受体蛋白3(NLRP3)炎症小体及下游炎症因子的表达来调控慢性阻塞性肺疾病(COPD)小鼠的的炎性损伤。方法:通过烟熏法构建COPD小鼠模型,选取C57BL/6J野生型雌性成年小鼠32只,体重18~22 g,随机分为4组(n=8):空白对照小鼠组(control组)、COPD小鼠组(COPD组)、注射阴性对照siRNA的COPD小鼠组(COPD+NC组)及注射RARRES2-siRNA加COPD小鼠组(COPD+siRNA组),COPD+NC组和COPD+siRNA组每4 d注射一次对应siRNA。HE染色和免疫组织化学染色观察肺组织病理学变化,湿干重比评估各组肺水肿程度,血气分析计算氧合指数评估各组肺功能情况。Western blot和免疫组织化学染色检测RARRES2、NLRP3、caspase-1、白细胞介素1β(IL-1β)和IL-18表达水平。ELISA检测支气管肺泡灌洗液和血浆中IL-1β和IL-18水平,比较肺部炎性损伤程度。结果:与control组相比,COPD组小鼠肺湿干重比、肺功能损伤程度、RARRES2、NLRP3、caspase-1、IL-1β和IL-18表达水平均显著上升(P<0.05)。与COPD组相比,COPD+NC组小鼠肺干湿重比、肺功能损伤程度、RARRES2、NLRP3、caspase-1、IL-1β和IL-18表达水平的差异无统计学意义(P>0.05);COPD+siRNA组小鼠肺干湿重比、肺功能损伤程度、RARRES2、NLRP3、caspase-1、IL-1β和IL-18表达水平显著下降(P<0.05)。结论:RARRES2可通过活化NLRP3炎症小体从而上调IL-1β和IL-18表达,提示其可能参与了小鼠COPD炎性损伤的发生和发展。

基于溶胶-凝胶技术的磷钨杂多酸化学修饰电极的组装及其电催化

将 Dawson型磷钨杂多酸盐 K6 P2 W1 8O6 2 · 1 0 H2 O( P2 W1 8)掺杂到溶胶 -凝胶中 ,滴涂在碳糊电极表面 ,制备成化学修饰电极 .并对该化学修饰电极的电化学行为 ,包括溶液 p H值的影响和电极稳定性等进行了详细的研究 .结果表明 ,此电极既保持了该杂多酸的电化学活性和电催化性能 ,又具有良好的稳定性和灵敏度 .实验发现 ,在 0 .5mol/L H2 SO4溶液中 ,掺杂在溶胶 -凝胶膜中的 P2 W1 8的第 3、第 4个还原峰对 NO- 2 离子具有很好的电催化活性 ,且催化电流同 NO- 2 浓度呈线性关系 .同时 ,P2 W1 8的第 3、第 4个还原峰对分子氧也具有很好的电催化活性 .

五环三萜类单体诱导人乳腺癌细胞凋亡的研究

目的:探讨熊果酸、齐墩果酸和18β-甘草次酸对人乳腺癌细胞(MCF-7)诱导凋亡的作用,并探讨凋亡发生与细胞内Ca2+浓度变化的关系。方法:选用不同浓度梯度的熊果酸、齐墩果酸和18β-甘草次酸分别处理MCF-7细胞24h,用MTT比色法测定细胞增殖能力,用末端脱氧核苷酸转移酶介导dUTP末端标记法和an-nexin V流式细胞仪法检测细胞凋亡率,用Fura-2荧光负载方法测定细胞内Ca2+浓度。结果:熊果酸、齐墩果酸和18β-甘草次酸的半增殖抑制浓度(IC50)分别为36.18、88.36和234.33μmol/L;20μmol/L和30μmol/L熊果酸、75μmol/L和100μmol/L齐墩果酸及100μmol/L和150μmol/L18β-甘草次酸使细胞凋亡率显著升高(P<0.01和P<0.05);20μmol/L熊果酸、75μmol/L齐墩果酸和150μmol/L18β-甘草次酸处理组的细胞内Ca2+浓度明显高于对照组(P<0.05)。结论:熊果酸、齐墩果酸和18β-甘草次酸均具有诱导MCF-7细胞凋亡而抑制其增殖的作用;其诱导凋亡可能依赖于细胞内Ca2+水平上调。

毛白杨亚油酸去饱和酶基因的克隆与表达模式分析

以毛白杨为材料,利用现有的杨树基因组EST序列库资源,通过同源序列搜索,经过多次拼接合并获得了理论的杨树亚油酸去饱和酶cDNA序列全长,通过RT-PCR手段首次克隆得到了毛白杨PtFAD3基因编码序列cDNA(GenBank登录号:DQ354393),该cDNA全长1 199 bp,开放阅读框编码383个氨基酸。通过RT-PCR半定量研究表明PtFAD3在叶片中的表达量最高,茎和根中的表达量依次降低;用低温、干旱、NaCl、ABA分别处理毛白杨组培苗,叶片中的PtFAD3表达量在逆境初期24 h之内没发生变化。该研究为毛白杨脂肪酸去饱和酶的研究以及植物脂肪酸基因工程提供了基础。

2-^(18)F-氟丁酸作为PET/CT显像剂可行性的初步研究

目的:设计合成^(18)F标记的新型短链脂肪酸代谢型显像剂2-^(18)F-氟丁酸(2-^(18)F-FBA),对其作为肿瘤PET/CT显像剂进行初步研究。方法:前体2-溴丁酸甲酯通过^(18)F-亲核取代反应实现放射性标记,中间体2-^(18)F-氟丁酸甲酯经高效液相色谱法分离纯化,收集时间在16~18 min的中间体,20 mL纯水稀释后过C18柱,并用10 mL纯水冲洗,吹干,此时中间体被吸附,使用1 mL NaOH溶液水解,得到2-^(18)F-FBA。目测产品的澄清度,测定pH值,检测放射化学纯度和稳定性。经美国癌症研究所健康小鼠尾静脉注射2-^(18)F-FBA(0.2 mL,7 MBq),检测2-^(18)F-FBA在正常小鼠体内的生物学分布。S180肉瘤荷瘤小鼠行micro-PET/CT显像,并进行图像分析和计算SUV max。各组织器官不同时间点生物学分布的比较采用Student t检验。结果:2-^(18)F-FBA的合成时间约为40 min,放射化学产率为(40±5)%(经时间校正),放射化学纯度>98%。产品溶液澄清无颗粒,pH值为7.2,体内外的稳定性良好。体内生物学分布的结果显示,注射2-^(18)F-FBA 5 min后,小鼠肝脏、心脏以及肺的放射性摄取较高,脑组织在各个时间点摄取均较低,代谢60 min后各脏器放射性摄取趋于稳定,骨骼的放射性摄取率随时间的延长均较低,但5 min与30、90 min比较,差异均无统计学意义(t=1.532、1.104,均P>0.05)。S180肉瘤荷瘤小鼠micro-PET/CT图像显示,注射2-^(18)F-FBA 30 min后肿瘤处放射性摄取较高,而此时周围组织脏器摄取较低,60 min后肿瘤摄取达到最大值,SUV max=1.90±0.03,但肝脏以及肠道等腹腔脏器亦有放射性摄取。结论:2-^(18)F-FBA的合成操作简便,合成时间短,放射化学产率较高,是一种具有潜在应用价值的新型脂肪酸代谢型显像剂。

Indole Alkaloids from the Roots of Ervatamia hainanensis

Two new indole alkaloids, named ibogamine-18-carboxylic acid, 3, 4-didehydro-7, 8-dioxo-methyl ester 1, ibogamine-18-carboxylic acid, 16, 17-didehydro-9, 17-dihydro-9-hydroxy （2-oxopropyl）-methyl ester 2, were isolated from Ervatamia hainanensis. Their structures were elucidated on the basis of spectroscopic methods.

软枣猕猴桃叶化学成分研究

从中药软枣猕猴桃Ainidia arguta(Sieb et Zucc)Planth ex Miguel的叶正丁醇提取物中分离并鉴定了2种结晶性成分,经理化常数测定及光谱分析,证明为β—谷甾醇(β—Sitosterol)和2α3α,24—三羟基—12—烯—28—乌苏酸(2α,3α,24—trihydroxyurs—12—en—28—oicacid)均为首次从该植物中分得。

Two new triterpenes from Duchesnea indica

Two new triterpenes, 2α,3β-dihydroxyurs- 12-en- 18,19-epoxy-28-oic acid （1） and 18,19-seco, 2α, 2α-dihydroxyl-19-oxo-urs- 11,13（18）-dien-28-oic acid （2） were isolated from the herbaceous part of Duchesnea indica. Their structures were elucidated by spectroscopic analysis, including 2D NMR technique. The isolated compounds exhibited moderate cytotoxic activities against HeLa and L929 cell lines.

Study of Gallium Plating of Metal Electrodes

Conditions of gallium plating of metal electrodes were studied in the paper. It was found that stability of gallium cover depends on the material and is increasing in the raw: stainless steel 08Х18Н12Т < Steel 1, Steel 2, Steel 3, Steel 45 < Ni < Cd < Cu. Phase composition of the electrode surface layer obtained after gallium plating was studied. It was found that gallium with nickel form Ga36Ni64(Ga Ni2) compound and gallium with copper form CuGa2compound. Different acids were used for electrode leaching: H2SO4;HNO3;H3PO4;HCI. It was shown that only hydrochloric acid is suit-able for gallium plating of the electrodes.

红簕钩中1个新的齐墩果烷型降三萜

目的 研究红簕钩Rubus pirifolicus的化学成分。方法 采用大孔树脂、硅胶、ODS、Sephadex LH-20以及半制备HPLC等方法进行分离纯化,根据波谱数据并结合文献对化合物结构进行鉴定。结果 从红簕钩醋酸乙酯部位中分离得到16个化合物,分别鉴定为梨叶悬钩子酸A(1)、acanthochlamic acid(2)、2α,3β-dihydroxyolean-13(18)-en-28-oic acid(3)、3-表-2-氧代-坡模醇酸(4)、2α,3α,19α,22α-tetrahydroxyurs-12-en-28-oicacid(5)、23-O-galloylarjungenin(6)、2α,3α,19α,24-四羟基齐墩果-12-烯-28-羧酸(7)、bellericageninB(8)、roburgenicacid(9)、2β,3β,19α-三羟基齐墩果-12-烯-23,28-二羧酸(10)、2α,3β,23-trihydroxylup-20(29)-en-28-oicacid28-O-β-D-glucopyranoside(11)、熊果酸(12)、山楂酸(13)、科罗索酸(14)、坡模酸(15)、齐墩果酸(16)。结论 化合物1为新化合物,命名为梨叶悬钩子酸A,化合物2~3、5~6、8~10为首次从悬钩子属中分离得到,所有化合物均为首次从该植物中分离得到。

Development of a highly-specific ^(18)F-labeled irreversible positron emission tomography tracer for monoacylglycerol lipase mapping

As a serine hydrolase,monoacylglycerol lipase(MAGL) is principally responsible for the metabolism of 2-arachidonoylglycerol(2-AG) in the central nervous system(CNS),leading to the formation of arachidonic acid(AA).Dysfunction of MAGL has been associated with multiple CNS disorders and symptoms,including neuroinflammation,cognitive impairment,epileptogenesis,nociception and neurodegenerative diseases.Inhibition of MAGL provides a promising therapeutic direction for the treatment of these conditions,and a MAGL positron emission tomography(PET) probe would greatly facilitate preclinical and clinical development of MAGL inhibitors.Herein,we design and synthesize a small library of fluoropyridyl-containing MAGL inhibitor candidates.Pharmacological evaluation of these candidates by activity-based protein profiling identified 14 as a lead compound,which was then radiolabeled with fluorine-18 via a facile SNAr reaction to form 2-[^(18)F]fluoropyridine scaffold.Good blood-brain barrier permeability and high in vivo specific binding was demonstrated for radioligand [^(18)F]14(also named as [^(18)F]MAGL-1902).This work may serve as a roadmap for clinical translation and further design of potent 18F-labeled MAGL PET tracers.