An Efficient One-step Methyl Esterification of Carboxylic Acid and Deacetylation of Alcohol under BF_3·OEt_2-MeOH

An efficient one-step methyl esterification of carboxylic acid and deacetylation of alcohol under BF3O·Et2-MeOH was developed.

THE EFFECTS OF MAGNETIC FIELD ON GRAFT COPOLYMERIZATION OF METHYL METHACRYLATE ONTO POLYVINYL ALCOHOL IN THE PRESENCE OF BENZOPHENONE DURING UV IRRADIATION

The effects of magnetic field on the graft ratio and stereoregularity of grafts of PVA-g-MMA in the presence ofbenzophenone during UV irradiation are discussed. By means of IR, it was found that the graft ratio was increased with the increment of magnetic field strength. Furthermore, application of relative weak magnetic field of 0.4 Tesla had been shown to substantially enhance the stereo-regularity of graft copolymer. The maximum stereo-regularity appeared when the graft ratio approached to 85% with the magnetic field of 1.2 Tesla (T). The resistance to moisture and heat resistance of the grafted copolymer in the presence of magnetic field were also improved.

Alcohol promotes renal fibrosis by activating Nox-mediated DNA methylation of Smad7

OBJECTIVE Alcohol is mainly metabolized through liver and excreted by kidney in the body.Kidney damage has been considered as the secondary to liver injury and kidney dysfunction is common in hospitalized patients with severe alcoholic hepatitis.Both acute and chronic alcoholism accumulation can compromise kidney function,although alcoholic kidney disease has drawn much more attention recently,the methodology for establishing the in vivo and in vitro alcoholic renal fibrosis models are still lacking,and the underlying mechanisms are to be determined.METHODS and RESULTS Mice were feed with a liquid diet containing alcohol for 4 weeks,8 weeks and 12 weeks respectively,results of Masson′ s Trichrome staining showed that kidney fibrosis peaked in 8-week model group,which consistent with the results of albumin assay,Western blot,immunostaining and real-time PCR of collagen I and α-SMA.In vitro study also confirmed that ethanol upregulated the level of fibrotic index.es,including collagen I and α-SMA,in tubular epithelial cells(HK2 cells).Additionally,both in vivo and in vitro studies showed that Smad7 was decreased and Smad3 was highly activated.Then we further detected the underlying mechanisms by which alcohol induced the imbalance of Smad7 and Smad3.Results of Genome-wide methylation sequencing found DNA methylation of Smad7 in the alcoholic fibrosis kidney,which may be mainly mediated by DNA methyltransferase 1(DNMT1),because knock.down of DNMT1,but not DNMT2 and 3,largely restored Smad7 level in ethanol-treated HK2 cells.Con.sequently,we found that NADPH Oxidases(nox)-mediated oxidative stress is the major force upregu.lating DNMT1,since knockdown of Nox2 and 4 could both decrease DNMT1 while rebalancing Smad7/Smad3 axis,and thereby relieved ethanol-induced fibrotic response in HK2 cells.More importantly,intraperitoneal injection of apocynin,an inhibitor of NADPH oxidoreductase,attenuated renal fibrosis in alcoholic kidney fibrosis mouse model.CONCLUSION By establishing the novel in vivo and in vitro models,we found that through activating oxidative stress-induced DNA methylation of Smad7,alcohol induces renal fibrosis by breaking the balance between Smad7 and Smad3.Elimination of Nox-mediated oxidative stress may be a potential therapy for treatment of long-term alcohol abuse-induced kidney fibrosis.

CAFs促进ADH1B甲基化对卵巢癌细胞增殖及侵袭的影响

目的 探讨肿瘤相关成纤维细胞(CAFs)分泌的IL-6对卵巢癌细胞增殖及侵袭的影响及机制。方法 收取新鲜离体上皮性卵巢癌及正常卵巢上皮组织,分离纯化获得CAFs及正常卵巢成纤维细胞(NFs);蛋白质印迹和免疫荧光实验检测上皮细胞和成纤维细胞标志物α-平滑肌动蛋白(α-SMA)、上皮型钙黏附素(E-cadherin)表达;收集CAFs和NFs培养上清液与卵巢癌SKOV3细胞建立间接共培养体系,细胞分为SKOV3单独培养(SKOV3)组、SKOV3与NFs上清液(NFs)组及SKOV3与CAFs上清液(CAFs)组;细胞免疫组化检测SKOV3细胞共CAFs及NFs上清液培养后乙醇脱氢酶1B(ADH1B)表达;甲基化特异性PCR (MSP)、逆转录实时荧光定量PCR(RT-qPCR)、酶联免疫吸附试验(ELISA)及蛋白质印迹实验分别检测甲基化抑制剂5-氮杂-2′-脱氧胞苷(5-Aza-dC)干预前后各组细胞ADH1B mRNA表达及甲基化状态、信号转导和激活因子3(STAT3)蛋白磷酸化水平;细胞计数试剂盒8(CCK-8)法及Transwell实验分别检测IL-6抑制剂LMT-286及重组IL-6 (rhIL-6)对细胞增殖及侵袭能力的影响。结果 肿瘤成纤维细胞中高表达α-SMA,极低表达E-cadherin;相比较SKOV3组及NFs组,CAFs组ADH1B mRNA及蛋白表达明显下调,同时CAFs组细胞上清液中IL-6水平较SKOV3组及NFs组明显升高;5-Aza-dC作用后,ADH1B甲基化部分逆转;三组细胞ADH1B mRNA和蛋白表达均增加,CAFs组STAT3磷酸化水平下降;LMT-286及rhIL-6干预均仅抑制或促进CAFs组细胞增殖和侵袭,而SKOV3组和NFs组无明显改变。结论 CAFs通过IL-6/STAT3信号通路增强ADH1B甲基化促进卵巢癌细胞增殖和侵袭。

有色冶炼污酸治理中硫化氢气体制取工艺的选择研究

以某公司污酸治理升级改造项目所需的硫化氢气体制取工艺选择为实例,对Na_(2)S/NaHS酸解法、氢气与硫磺合成法制取硫化氢工艺,以及甲醇裂解、天然气蒸气转化制氢方案进行综合对比分析。综合多种影响因素研究选取了甲醇-硫磺合成硫化氢工艺治理污酸废水。

碱催化p-QMs的1,6-共轭加成合成二芳基甲基(硫)醚

在摩尔分数为20%的氢氧化钠的催化作用下,实现了对亚甲基苯醌(p-QMs)与醇(或硫酚)的溶剂解反应,即p-QMs的1,6-共轭加成反应,以37%~95%的产率制备了一系列二芳基甲基(硫)醚类化合物。结果表明,该反应具有操作简便、反应条件温和高效、官能团耐受性良好等特点;该方法易于放大,能以80%的产率得到二芳基甲基乙基醚,为后期的潜在应用与转化提供了可能。

甲基嘧啶磷的绿色合成研究

以嘧啶醇和碳酸钾水溶液在有机溶剂中反应减压脱水,生成嘧啶醇钾盐与甲基氯化物进行缩合反应,经过滤、减压浓缩得到甲基嘧啶磷。优化的反应条件为:以甲苯为溶剂,n(嘧啶醇)∶n(碳酸钾)=1.0∶2.0,嘧啶醇钾盐含水量<0.1%,反应温度30~40℃,反应时间6 h。优化条件下,甲基嘧啶磷纯度98.5%,收率92.6%,该工艺转化率高、收率高、三废少,符合绿色环保生产理念,具有工业化应用前景。

顺-3-己烯酸甲酯还原制备叶醇的工艺研究

以顺-3-己烯酸甲酯为原料,探究不同反应体系对叶醇合成收率的影响。并优化了以顺-3-己烯酸甲酯、乙醇、氯化钙为原料的还原体系工艺条件,得到的最优反应条件为:顺-3-己烯酸甲酯用量为38.4g,m(95%乙醇):m(顺-3-己烯酸甲酯)=6;n(CaCl_(2)):n(顺-3-己烯酸甲酯)=0.8;n(NaBH_(4)):n(顺-3-己烯酸甲酯)=1.2,反应温度20℃,反应1h,叶醇收率为80.92%,并在此基础上扩大到公斤级反应,最终得到叶醇收率为80%以上,具有广阔的工业化应用前景。

Adipose tissue-liver axis in alcoholic liver disease

Alcoholic liver disease(ALD) remains an important health problem worldwide. The disease spectrum is featured by early steatosis, steatohepatitis(steatosis with inflammatory cells infiltration and necrosis), with some individuals ultimately progressing to fibrosis/cirrhosis. Although the disease progression is well characterized, no effective therapies are currently available for the treatment in humans. The mechanisms underlying the initiation and progression of ALD are multifactorial and complex. Emerging evidence supports that adipose tissue dysfunction contributes to the pathogenesis of ALD. In the first part of this review, we discuss the mechanisms whereby chronic alcohol exposure contributed to adipose tissue dysfunction, including cell death, inflammation and insulin resistance. It has been long known that aberrant hepatic methionine metabolism is a major metabolic abnormality induced by chronic alcohol exposure and plays an etiological role in the pathogenesis of ALD. The recent studies in our group documented the similar metabolic effect of chronic alcohol drinking on methionine in adipose tissue. In the second part of this review, we also briefly discuss the recent research progress in the field with a focus on how abnormal methionine metabolism in adipose tissue contributes to adipose tissue dysfunction and liver damage.

Alcohol,nutrition and liver cancer:Role of Toll-like receptor signaling

This article reviews the evidence that ties the development of hepatocellular carcinoma (HCC) to the natural immune pro-inflammatory response to chronic liver disease, with a focus on the role of Toll-like receptor (TLR) signaling as the mechanism of liver stem cell/progenitor transformation to HCC. Two exemplary models of this phenomenon are reviewed in detail. One model applies chronic ethanol/lipopolysaccharide feeding to the activated TLR4 signaling pathway. The other applies chronic feeding of a carcinogenic drug, in which TLR2 and 4 signaling pathways are activated. In the drug-induced model, two major methyl donors, S-adenosylmethionine and betaine, prevent the upregulation of the TLR signaling pathways and abrogate the stem cell/progenitor proliferation response when fed with the carcinogenic drug. This observation supports a nutritional approach to liver cancer prevention and treatment. The observation that upregulation of the TLR signaling pathways leads to liver tumor formation gives evidence to the popular concept that the chronic pro-inflammatory response is an important mechanism of liver oncogenesis. It provides a nutritional approach, which could prevent HCC from developing in many chronic liver diseases.

Aberrant post-translational protein modifications in the pathogenesis of alcohol-induced liver injury

It is likely that the majority of proteins will undergo post-translational modification, be it enzymatic or non-enzymatic. These modified protein(s) regulate activity, localization and interaction with other cellular molecules thereby maintaining cellular hemostasis. Alcohol exposure significantly alters several of these post-translational modifications leading to impairments of many essential physiological processes. Here, we present new insights into novel modifications following ethanol exposure and their role in the initiation and progression of liver injury. This critical review condenses the proceedings of a symposium at the European Society for the Biomedical Research on Alcoholism Meeting held September 12-15, 2015, in Valencia, Spain.

改性聚乙烯醇协同硅酸盐水泥制高强防水石膏

以脱硫石膏为基料,以液碱活化聚甲基氢硅氧烷(PMHS)催化改性聚乙烯醇(PVA)防水剂协同硅酸盐水泥研发高强防水石膏。探究了改性PVA防水剂、硅酸盐水泥对脱硫石膏标准试块表面吸水率、力学性能和软化系数的影响;通过红外光谱确定改性疏水剂、硅酸盐水泥单独及协同研发强防水石膏的连接形式;通过热重仪分析不同掺加剂对石膏热稳定性的影响;研究表明,改性PVA防水剂协同硅酸盐水泥制高强防水石膏的最佳配比为:防水剂120 g、硅酸盐水泥150 g,此时表面吸水率9.35%,绝干抗压强度22.54 MPa、软化系数67.57%,同时有效提高了纸面石膏板的热稳定性。

Prolonged feeding with guanidinoacetate, a methyl group consumer, exacerbates ethanol-induced liver injury

AIM To investigate the hypothesis that exposure to guanidinoacetate(GAA, a potent methyl-group consumer) either alone or combined with ethanol intake for a prolonged period of time would cause more advanced liver pathology thus identifying methylation defects as the initiator and stimulator for progressive liver damage.METHODS Adult male Wistar rats were fed the control or ethanolLieber De Carli diet in the absence or presence of GAA supplementation. At the end of 6 wk of the feeding regimen, various biochemical and histological analyses were conducted. RESULTS Contrary to our expectations, we observed that GAA treatment alone resulted in a histologically normal liver without evidence of hepatosteatosis despite persistence of some abnormal biochemical parameters. This protection could result from the generation of creatine from the ingested GAA. Ethanol treatment for 6 wk exhibited changes in liver methionine metabolism and persistence of histological and biochemical defects as reported before. Further, when the rats were fed the GAA-supplemented ethanol diet, similar histological and biochemical changes as observed after 2 wk of combined treatment, including inflammation, macroand micro-vesicular steatosis and a marked decrease in the methylation index were noted. In addition, rats on the combined treatment exhibited increased liver toxicity and even early fibrotic changes in a subset of animals in this group. The worsening liver pathology could be related to the profound reduction in the hepatic methylation index, an increased accumulation of GAA and the inability of creatine generated to exert its hepato-protective effects in the setting of ethanol.CONCLUSION To conclude, prolonged exposure to a methyl consumer superimposed on chronic ethanol consumption causes persistent and pronounced liver damage.

甲醇作为甲基化试剂催化体系研究进展

甲醇是最小的含有碳氢氧的饱和有机分子,广泛应用于能源、化工以及有机合成等领域。通过氢转移的方法,将甲醇作为甲基化试剂,与胺、醇/酮以及烃类化合物耦合转化制备高值化的甲基化产品,是一项非常有意义的研究工作。氢转移反应过程的机理主要包括:甲醇的催化脱氢制甲醛;甲醛与底物脱水获得不饱和键;不饱和键原位加氢获得最终的产物。总结了近年来甲醇作为甲基化试剂,通过氢转移的方法制备甲基化胺、醇/酮以及烃类化合物催化体系的发展,并重点介绍了基于贵金属与非贵金属的均相和多相反应体系。鉴于反应过程中甲醇催化脱氢和不饱和键加氢对反应活性和选择性的影响这一科学问题,通过配位结构/金属载体的相互作用的调控有可能制备高催化性能均相/多相催化反应体系,且多相非贵金属催化体系具有较好的工业化应用前景。

羧酸离子液体/氧气催化氧化芳甲醇

在组合体系“1-乙基-3-甲基咪唑乙酸盐([EMIm][OAc])/O_(2)”作用下,以芳甲醇为原料,经氧化反应,合成了系列芳甲醛(酮)类化合物。通过对条件进行优化,得到适宜反应条件为:芳甲醇与1-乙基-3-甲基咪唑乙酸盐物质的量比为1∶1、O_(2)压力为0.20MPa、温度为130℃、时间为12h。在此条件下,实现了苯甲醛的克级规模制备,得到20种芳甲醛(酮),产率为62%~96%。提出了[EMIm][OAc]通过阴离子作用于苯甲醇,经O_(2)氧化,脱水得到苯甲醛的反应机理。

高脂饮食诱导的小鼠NAFLD模型肝组织中m6A甲基化修饰表达谱分析

目的·利用微阵列芯片技术检测高脂饮食诱导的小鼠非酒精性脂肪性肝病(non-alcoholic fatty liver disease,NAFLD)模型中肝组织mRNA的m6A甲基化修饰和基因表达的变化。方法·以6~8周龄雄性C57BL/6J小鼠为实验动物,高脂饲料喂养16周诱导建立NAFLD模型(高脂组,n=10);另设基础组(n=10)为对照,给予含10%脂肪的基础饲料喂养。苏木精-伊红(hematoxylin-eosin,H-E)染色评估小鼠肝组织病理改变,判断NAFLD模型是否构建成功。运用甲基化RNA免疫共沉淀技术(methylated RNA immunoprecipitation,MeRIP)和微阵列测序技术(microarray表达谱分析)检测2组小鼠肝组织中mRNA的m6A甲基化和表达水平变化。结果·基础组小鼠肝脏呈鲜红色,少见脂肪沉积;高脂组小鼠肝脏边界黄润,H-E染色可见肝细胞中脂滴弥漫浸润且相互融合,提示高脂饲料诱导的NAFLD模型构建成功。MeRIP-微阵列芯片检测结果显示,与基础组相比,高脂组小鼠肝脏中共有320个基因m6A甲基化修饰水平变化显著(P<0.05且变化倍数>1.5),其中有108个上调基因和212个下调基因。将组间m6A甲基化水平差异显著的基因与mRNA差异表达基因取交集,发现有163个基因m6A甲基化水平和mRNA表达水平均差异显著。结论·高脂饮食诱导的小鼠NAFLD模型中肝组织mRNA的m6A修饰变化显著,且该变化与mRNA的基因表达有关。

一种水中臭味物质测定的可行性方案

研究了吹扫捕集/气相色谱-质谱法检测水中的臭味物质的可行性方法。与国标方法(GB/T 32470-2016)相比较,本方法可以大大的降低了对臭味物质的检测的成本,而且对土臭素、2-甲基异莰醇可以满足检测要求,更容易在各检测实验室普及使用。本方法土臭素、2-甲基异莰醇的方法检出限分别为0.26 ng/L、0.47 ng/L,土臭素的加标回收率在87.9%~96.8%,2-甲基异莰醇的加标回收率在86.0%~101.0%。

丁烯水合反应器床层压差的研究进展

正丁烯直接水合法合成SBA是甲乙酮生产工艺中的重要环节,直接水合法与传统的硫酸间接水合法相比具有流程短、占地省、投资少、三废排放量小、选择性好等优点。在以强酸性阳离子交换树脂为催化剂进行正丁烯水合反应工艺研究过程中,观察到随着反应时间增加,水合反应床层压差升高并伴有床层压力震荡产生。本文分析了丁烯水合反应运行过程中床层压差升高的原因,提出了降低反应器压差的方法,有效的保证了水合反应装置的正常平稳运行。

(S)-4-苄氧基取代苯丙胺醇衍生物的制备

采用以L-N-Boc酪氨酸甲酯为原料,经苄基保护4位酚羟基、LiAlH4还原甲酯、脱苄基保护、醚化反应、脱Boc保护基等反应,合成了中间体3和(S)-4-苄氧基取代苯丙胺醇衍生物3个。实验过程中得到的中间体3和(S)-4-苄氧基取代苯丙胺醇衍生物分别为(S)-3-(4-羟基苯基)-2-叔丁氧甲酰氨基-1-丙醇、(S)-3-(4-苄氧苯基)-2-氨基-1-丙醇、(S)-3-[4-(3,4-二氟苄氧苯基)]-2-氨基-1-丙醇和(S)-3-[4-(2,6-二氟苄氧苯基)]-2-氨基-1-丙醇,所得化合物的化学结构经质谱和核磁共振氢谱确证。本合成路线具有操作简单、收率高的特点,其中中间体3可用于氨基醇类衍生物的合成,而(S)-4-苄氧基取代苯丙胺醇衍生物的合成提供了基础化合物和合成方法参考,以发现和研制新的活性药物。

乙醇酸甲酯选择性氧化制备乙醛酸甲酯研究进展

乙醛酸甲酯在有机合成和化工生产中应用广泛,传统的制备方法存在成本高、效率低、易造成环境污染等缺点.乙醇酸甲酯是煤基合成气经草酸二甲酯加氢制乙二醇工艺的中间产物且可高选择性控制合成,以其为原料选择性氧化制备乙醛酸甲酯具有较好的工业应用前景,但目前为止,研究较为有限.本文综述了乙醛酸甲酯的应用、传统制备方法及乙醇酸甲酯氧化法的研究现状,也总结了相关醇类(如乙醇)选择性氧化制醛酮的研究进展.