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1.
用TRP技术研究了以全硅MCM-41(Si-MCM-41)和HNO3交换的全硅MCM-41(H-MCM-41)为载体制备的Ni-Mo、Co-Mo和Ni-W加氢脱硫(HDS)催化剂的还原性能,并以0.8(wt)%二苯并噻吩(DBT)的十氢萘溶液为模型化合物,在高压固定床反应器上考察了上述催化剂的加氢脱硫(HDS)反应性能。结果表明,Si-MCM-41经稀HNO3交换后,所担载的Ni-Mo和Ni-W催化剂还原性能、HDS活性和加氢活性有显著变化,但对Co-Mo催化剂影响不大。这说明在Ni-Mo/H-MCM-41和Ni-W/H-MCM-41中可能存在氢溢流现象,DBT的HDS活性与载体表面酸性和氢溢流有关。  相似文献   

2.
在固定床高压微反装置上,考察了预硫化型NiMoS/γ-Al2O3催化剂上二苯并噻吩(DBT)加氢脱硫(HDS)反应和喹啉加氢脱氮(HDN)反应之间的相互影响.结果表明,喹啉对DBT的HDS反应具有强烈的抑制作用,其中对加氢路径比氢解路径的抑制作用更强,这是由喹啉及其HDN反应的中间产物与DBT在活性位上的竞争吸附造成的.在300和340℃时,喹啉对DBT的HDS反应中氢解路径的抑制程度与其HDN中间产物的相对含量紧密相关.而DBT能够提高喹啉的脱氮能力,这源于其HDS产物H2S.H2S促进了催化剂表面硫阴离子空穴向B酸位的转化,从而提高了喹啉HDN中间产物分子的C(sp3)-N键的断裂能力.HDN活性相的保持不需要过多的硫原子.  相似文献   

3.
研究了4-甲基二苯并噻吩(4-MDBT)和二苯并噻吩(DBT)在CoMo/γ-Al2O3上的加氢脱硫反应产物分布及其可能的反应网络,通过反应压力和温度对产物分布影响的研究,揭示了加氢脱硫反应的可能机理。研究发现4-MDBT在CoMo/γ-Al2O3上的加氢脱硫反应主要通过直接氢解路径和加氢路径进行,且两者反应速率相当;DBT在 CoMo/γ-Al2O3上的加氢脱硫反应主要通过直接氢解路径进行。4-MDBT分子位于4位的甲基阻碍其在催化剂表面通过硫原子的端连吸附,从而降低了其直接氢解脱硫路径的反应速率,因而也降低了其总的加氢脱硫转化率。反应压力降低,DBT和4-MDBT加氢脱硫反应中加氢路径反应速率明显下降,而其对氢解路径影响较小,但效果却与加氢路径相反,反应压力对4-MDBT转化率的影响大于DBT。反应温度对DBT和4-MDBT加氢脱硫反应中加氢路径和氢解路径都有明显影响,但是对DBT加氢脱硫反应中氢解路径的影响小于加氢路径,而对4-MDBT加氢脱硫反应中氢解路径的影响稍高于加氢路径,4-MDBT分子中甲基的供电子作用有利于相连苯环的加氢反应。  相似文献   

4.
工业NiW/Al2O3催化剂上二苯并噻吩的加氢脱硫动力学   总被引:6,自引:2,他引:4  
以二苯并噻吩(DBT)为含硫模型化合物, 在高压滴流床反应装置中,考察了工业NiW/Al2O3催化剂(RN-10)的加氢脱硫(HDS)动力学规律,研究了氢分压(1.5 MPa~4.5 MPa)、氢油体积比(150~700)、液体质量空速(15 h-1~60 h-1)、反应温度(280 ℃~380 ℃)等对DBT的HDS反应结果的影响。结果表明,当氢分压和氢油体积比较大时,两者变化对DBT的转化率基本无影响;温度对DBT的转化率影响较大,提高温度可有效提高DBT的转化率,随着温度的升高,DBT转化率的增加逐渐变缓。采用2级平推流反应动力学模型对不同温度实验数据进行了拟合,求得了不同温度的表观反应速率常数,模型的相关系数>0.989。活化能计算结果表明,RN-10催化剂在高反应温度区(>330 ℃)的DBT的HDS活化能明显低于较低温度时的活化能,分别为13.4 kJ/mol和121.4 kJ/mol。对于RN-10催化剂,不可单纯地通过提高反应温度来大幅度提高HDS转化率。  相似文献   

5.
以MCM-41为载体,以镍(Ni)为助剂,制备了Ni含量不同的WP/MCM-41催化剂。采用XRD、BET、SEM和XPS对催化剂进行了表征;以二苯并噻吩(DBT)为模型化合物,通过高压微反装置考察催化剂的加氢脱硫(HDS)活性。结果表明,Ni的加入促进了活性组分WP的生长并使其晶相尺寸略有增加,一定含量的Ni有利于提高催化剂的比表面积。Ni对WP/MCM-41催化剂二苯并噻吩HDS反应具有促进作用。少量Ni的加入有利于WP活性相的生成并增加了活性位的数量;加入过量的Ni,在催化剂中形成了具有一定活性的类似Ni-W-P结构的物种,减少了活性组分WP所占的比例,从而使催化剂DBT的 HDS活性降低。其中,Ni的质量分数为1%的催化剂(cat-Ni-1)具有相对较高活性,其DBT 脱硫率和转化率分别为76.78%和72.16%,比不加Ni的催化剂分别提高了30.04%和21.62%。二苯并噻吩在WP/MCM-41催化剂上以加氢脱硫途径为主,Ni的加入对提高加氢脱硫途径选择性起到了促进作用,且加氢脱硫选择性随Ni含量的增加而提高。  相似文献   

6.
采用程序升温氮化法制备了Mo2N/SiO2,在此基础上负载Ni盐,制备了Ni-Mo2N/SiO2复合纳米催化剂,并考察了催化剂对四氢萘加氢的催化活性.结果表明,与Ni2Mo3N/SiO2及Ni/SiO2催化剂相比,Ni-Mo2N/SiO2复合催化剂具有较高的催化活性.采用"分离床"方法研究了Ni和Mo2N对四氢萘加氢活性的影响.通过X射线粉末衍射、透射电镜、氢吸附、元素分析和比表面积测定等技术对Ni-Mo2N/SiO2催化剂进行了表征.结果表明,与Ni/SiO2催化剂相比,Ni-Mo2N/SiO2复合催化剂中Ni的分散度并未提高;催化活性的提高归因于Ni与Mo2N在四氢萘加氢中的协同作用.氮化物的引入增加了芳烃吸附活性位的数目.提出了四氢萘在Ni-Mo2N/SiO2催化剂上的可能加氢机理.  相似文献   

7.
在固定床高压微反装置上考察了预硫化型NiMoS/γ-Al2O3催化剂上二苯并噻吩(DBT)加氢脱硫(HDS)反应和吲哚加氢脱氮(HDN)反应之间的相互影响。结果表明,吲哚对DBT的加氢脱硫反应具有抑制作用,其中对加氢路径(HYD)比对氢解路径(DDS)的抑制作用强,温度升高后,吲哚的抑制作用减弱。吲哚对DBT加氢脱硫反应的抑制作用源于吲哚及其HDN反应的中间产物在活性位上的竞争吸附。DBT和原位生成的H2S促进了催化剂表面硫阴离子空穴(CUS)向B酸位的转化,从而提高1,2-二氢吲哚(HIN)分子中C(sp3)—N键的断裂能力,使得吲哚的转化率和产物中邻乙基苯胺(OEA)的相对含量增大。HDN活性相的形成虽然需要硫原子的参与,但是活性相的保持并不需要大量的硫原子,较高含量硫化物存在时加氢活性位减少,不利于脱氮反应。  相似文献   

8.
HY/MCM-41/γ-Al2O3负载的硫化态Ni-Mo-P催化剂上萘的加氢   总被引:1,自引:0,他引:1  
 采用水热法合成了不同SiO2/Al2O3比的MCM-41介孔分子筛. 并分别以HY/MCM-41/γ-Al2O3, HY/γ-Al2O3和γ-Al2O3为载体,用浸渍法制备了Mo-Ni-P催化剂. 以萘为模型化合物,考察了硫化态Mo-Ni-P催化剂的加氢活性. 结果表明,不同载体负载的催化剂催化活性均随着活性组分负载量的增大而提高,其中掺杂大比表面MCM-41的HY/MCM-41/γ-Al2O3所负载的催化剂催化活性提高幅度最大. 由于MCM-41与HY分子筛在酸性和孔结构上存在互补性,因而催化剂对萘加氢存在协同作用. 提出了萘加氢的反应机理,认为反应网络包括两个平行路径: 一是萘加氢生成四氢萘后发生异构化或开环反应; 二是萘加氢生成四氢萘后进一步加氢生成十氢萘,继而发生异构化或开环反应.  相似文献   

9.
以三苯基膦(PPh3)为磷源,以三正辛胺(TOA)为液相反应体系,采用溶剂热法制备了负载型Ni-P(x)/MCM-41催化剂(x为初始P/Ni物质的量比),并用X射线衍射(XRD)、N2吸附比表面积测定(BET)、CO吸附、X射线光电子能谱(XPS)和TEM对催化剂进行了结构表征。以含质量分数1%二苯并噻吩(DBT)的十氢萘溶液为原料,在连续固定床反应装置上,研究了初始P/Ni物质的量比对加氢脱硫(HDS)性能的影响。结果表明,在初始P/Ni物质的量比为0.5时,生成的磷化镍物相为以Ni12P5为主,含有少量Ni2P的混合相;初始P/Ni物质的量比大于0.5时,可得到纯Ni_2P相,且随着P/Ni物质的量比的提高,Ni2P晶粒粒径减小,分散度提高。在反应温度613 K,压力3.0 MPa,H_2/oil体积比500,质量空速2.0 h-1时,Ni-P(6)/MCM-41和Ni-P(10)/MCM-41催化剂的DBT转化率接近100%。  相似文献   

10.
郭锐  马骏  杨锡尧 《分子催化》2002,16(1):19-24
通过氧吸附量、噻吩吸附热及反应速率常数的测定,研究了MoO3/MCM-41、MoO3-CoO(NiO)/MCM-41系列催化剂,发现,对于MoO3/MCM-41催化剂,当MoO3的质量分数(以MCM-41为底数,即MCM-41=1g时,MoO3含量为0.15g,下同)从15%增加到20%时,其噻吩的加氢硫(HDS)活性增大,至25%时活性下降,所对应的氧吸附量(mL/g催化剂)也是先增大后减少,并且两者有很好的线性对应关系,而且噻吩吸附热则基本保持不变,采用不同的MoO3-CoO(NiO)浸渍顺序制备的MoO3-CoO(NiO)/MCM-41催化剂中,先浸渍CoO(NiO)再浸渍MoO3的催化剂,其噻吩HDS活性明显优于对其它浸渍顺序制备的催化剂,同时催化剂的氧吸附量和噻吩吸附热也最大。  相似文献   

11.
In the context of the preparation of camptothecin and luotonin A analogs, the synthesis of some key keto-precursors and their use in Friedländer condensation are described. This paper also focuses on the stability of these keto intermediates and emphasizes the major differences between indolizinones and pyrroloquinazolinones series. Noteworthy is also the report of some original structures isolated as by-products of some experiments.  相似文献   

12.
KMnO4-mediated oxidative CN bond cleavage of tertiary amines producing secondary amine was introduced, which was trapped by electrophiles (acyl chloride and sulfonyl chloride) to form amides and sulfonamides. The reaction could take place at mild condition, tolerating a wide range of function groups and affording products in moderate to excellent yields.  相似文献   

13.
The review contains a concise historical account and information on the most significant researches undertaken by the staff at the A. E. Favorsky Irkutsk Institute of Chemistry, Siberian Branch of the Russian Academy of Sciences on the Chemistry of Heterocyclic Compounds. Dedicated to Academician of the Russian Academy of Sciences B. A. Trofimov on his 70th jubilee. Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 10, pp. 1443–1502, October, 2008.  相似文献   

14.
Different approaches for the synthesis of 1-benzyloxypyrazin-2(1H)-one derivatives from simple amino acids have been investigated. A library of 33 precursors for the preparation of N-hydroxy pyrazinones was obtained in moderate to good yields.  相似文献   

15.
The highly regioselective Buchwald–Hartwig amination at C-2 of the cheap and readily accessible reagent, 2,4-dichloropyridine with a range of anilines and heterocyclic amines is described. This new methodology is robust and provides a facile access to 4-chloro-N-phenylpyridin-2-amines on 0.25 mol scale. These intermediates undergo a further Buchwald–Hartwig amination at higher temperature to enable rapid exploration of the chemical space at C-4 and to provide a library of 2,4-bisaminopyridines.  相似文献   

16.
A new and simple synthesis of novel N-protected methyl 5-substituted-4-hydroxypyrrole-3-carboxylates, which exist in equilibrium with their 4-oxo tautomers, has been developed in two steps starting from N-protected α-amino acids. The key intermediates are enaminones, which can also be isolated, characterized, and used for the construction of other functionalized heterocycles, before they spontaneously decompose to pyrrole products. 4-Hydroxypyrroles are prone to partial aerial oxidation but can be efficiently alkylated or reduced to stable polysubstituted pyrrolidine derivatives.  相似文献   

17.
The chemoselectivity in the intramolecular CH insertion of various diazosulfonamides has been experimentally studied. The results reveal that the aliphatic 1,4-, 1,5-, or 1,6-C(sp3)?H insertions of diazosulfonamides are not accessible, while the aromatic 1,5-C(sp2)?H insertion can be realized specifically by adjusting the diazo-adjacent group. In addition, the general chemoselectivities in the intramolecular CH insertions of diazosulfonyl compounds are summarized. Generally, diazosulfones undergo both aromatic 1,5-C(sp2)?H and aliphatic 1,5- and 1,6-C(sp3)?H insertions, while diazosulfonates undergo aliphatic 1,5- and 1,6-C(sp3)?H insertions. However, diazosulfonamides only undergo aromatic 1,5-C(sp2)?H insertion.  相似文献   

18.
19.
An efficient approach to the synthesis of highly congested di, penta and hexacyclic pyrazoles as well as imidazole fragment containing novel heterocyclic molecule has been developed through a carbanion induced transformation of suitably functionalized 2H-pyran-2-ones, benzo[h]chromene and thiochromeno[4,3-b]pyrans. Due to the presence of fluorescence, we report their prime application metal sensor as off/on switching in ferric ions.  相似文献   

20.
Quercetin, the polyphenolic compound, which has the highest daily intake, is well known for its protective effects against aging diseases and has received a lot of attention for this reason. Both quercetin 3-O-β-d-glucuronide and quercetin 3′-O-β-d-glucuronide are human metabolites, which, together with their regioisomers, are required for biological as well as physical chemistry studies. We present here a novel synthetic route based on the sequential and selective protections of the hydroxyl functions of quercetin allowing selective glycosylation, followed by TEMPO-mediated oxidation to the glucuronide. This methodology enabled us to synthesize the five O-β-d-glucosides and four O-β-d-glucuronides of quercetin, including the major human metabolite, quercetin 3-O-β-d-glucuronide.  相似文献   

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