Synthesis,Growth and Spectroscopic Studies of Piperazinium Paranitrophenolate Monohydrate Crystals

A new piperazinium 4-nitro phenolate monohydrate single crystal(PNP)was grown by employing the solution growth technique piperazine and 4-nitrophenol,were the source material used for the growth,acetonitrile is used as solvent.The grown crystal was characterized by Single X-ray analysis and it shows that piperazinium 4-nitrophenol monohydrate crystallizes in the monoclinic space group P2 1/c,with cell parameters a=10.902 5(4),b=6.226 1(3),c=14.031 8(5),and z=4.The lattice parameters of the substances were also determined by using powder diffraction methods.The functional groups are identified by using FTIR spectral analysis.The absorbance of title compound were analyzed using UV-Vis spectra.The thermo analytical properties of the crystal were studied using TG,DTA.

双哌嗪盐类化合物电子轰击离子化质谱研究（STUDY ON BIS—PIPERAZINIUM SALTS（M2＋2Br-2HCI） BY ELECTRON IMPACT IONIZATION MASS SPECTROMETRY）

Electron impact ionization mass spectra of six new synthetic bis-piperazinium salts (M2+ 2Br-2HC1) with anti-tumor activities were obtained. Although the M+ ions and double charge ions M2+ were notobserved in E1 mass spectra, some strange ions such as [M-2]+ ions,[M-R]+ ions , [M-R-l]+ ions, [M-2R]+ ions and even [RX]+ ions presented in EIMS by decreasing the electron energy. These phenomena may be explained as R+ rearrangement and intermolecular reaction occurring in the condensed phase. We tried to describe the main routes of fragmentation and high sensitive mass spectra of the fragments oaboutthese compounds.

突触前α7烟碱受体对海马神经元兴奋性突触传递的调控(英文)

采用盲法膜片钳技术观察突触前烟碱受体(nicotinic acetylcholine receptors,nAChRs)对海马脑片CA1区锥体神经元兴奋性突触传递的调控作用。结果显示,nAChRs激动剂碘化二甲基苯基哌嗪(dimethylphenyl-piperazini-um iodide,DMPP)不能在CA1区锥体神经元上诱发出烟碱电流。DMPP对CA1区锥体神经元自发兴奋性突触后电流(spontaneous excitatory postsynaptic current,sEPSC)具有明显的增频和增幅作用,并呈现明显的浓度依赖关系。DMPP对微小兴奋性突触后电流(miniature excitatory postsynaptic Current,mEPSC)具有增频作用,但不具有增幅作用。上述DMPP增强突触传递的作用不能被nAChRs拮抗剂美加明、六烃季铵和双氢-B-刺桐丁所阻断,但可被α-银环蛇毒素阻断。上述结果提示,海马脑片CA1区锥体神经元兴奋性突触前nAChRs含有对α-银环蛇毒素敏感的α7亚单位,其激活可增强海马CA1区锥体神经元突触前递质谷氨酸的释放,从而对兴奋性突触传递发挥调控作用。

1，1－二烷基－4－（3－溴丙酰基）－哌嗪溴化物的合成及生物活性研究

设计合成了七种新的１，１－二烷基－４－（３－溴丙酰基）哌嗪季铵盐溴化物，通过ＩＲ，￣１ＨＮＭＲ和元素分析证实其结构。初步生物活性试验结果表明，Ⅵａ，Ⅵｃ和Ⅵｅ～ｇ有明显的镇痛活性，Ⅵｅ～ｇ还有较好的抗氧化ＳＯＤ活性，但未发现有抗肿瘤作用。

双哌嗪双季铵盐类衍生物的快原子轰击质谱和电子轰击离子化质谱研究(英文)

〕双派嗪双季铵盐类化合物（Ｍ２＋ ２Ｂｒ－ ２ＨＣｌ）具有良好的抗肿瘤，镇痛和抗氧化作用。本文对三个１，１０－双（Ｎ－取代哌嗪）癸烷双季铵盐新化合物进行了质谱及其裂解规律的研究。从快原子轰击质谱（ＦＡＢＭＳ）得到了［Ｍ＋ Ｘ］＋ 峰，［Ｍ－ Ｈ］＋ 峰和［Ｍ－ Ｒ＋ Ｈ］＋ 峰。此［Ｍ－ Ｈ］＋ 峰可由Ｒ＋ 重排而来。从电子轰击离子化质谱（ＥＩＭＳ）得到了主要碎片峰，特征峰ｍ ／ｚ９９，ｍ ／ｚ１１３，ｍ ／ｚ２８１，ｍ ／ｚ３１１，等也可由类霍夫曼（Ｈｏｆｆｍ ａｎｎ）降解形成。

Design,Synthesis and Antitumor Activity of Fluoroquinolone C3 Heterocyclic Bis-oxadiazole Methylsulfide Derivatives Derived from Levofloxacin

To discover an efficient route for the shift from an antibacterial fluoroquinolone to an antitumor one based on the mechanistic similarities between targeting topoisomerases and the eukaryotic ones,two series of the title compounds,C3 bis-oxadiazole methylsulfides 6a―6h and corresponding dimethylpiperazinium iodides 7a―7h derived from levofloxacin 1 were designed and synthesized.Their in vitro antiproliferative activities against Chinese hamster ovary cell line（CHO）,murine leukemia cell line（L1210） and human leukocytoma cell line（HL60） were evaluated by MTT assay,and inhibitory effect on DNA topoisomerase IIα was also measured by means of densitometric assay.

基于N,N'-二(3-吗啉基丙基)哌嗪三核阳离子酸性离子液体的合成及其催化作用

合成出了两种基于N,N'-二(3-吗啉基丙基)哌嗪[(mp)2pi]的三核阳离子型酸性离子液体——N,N'-二(3-吗啉基丙基)哌嗪四(三氟甲烷磺酸)盐{[(Hmp)2h2pi](OTf)4}和N,N'-二(3-吗啉基丙基)哌嗪四(硫酸氢)盐{[(Hmp)2h2pi](HSO4)4}。选取含相同内核的吗啉和哌嗪单、双阳离子的离子液体以及传统工业酸催化剂硫酸作为对照,在环己酮与苯甲醛之间的交叉Aldol反应中考察了4种酸性离子液体及硫酸的催化活性,实验结果表明,具有三核阳离子的酸性离子液体的催化活性比包含部分相同结构的单、双阳离子的离子液体及硫酸的强。其中,[(Hmp)2h2pi](OTf)4)的催化活性最强,在反应温度100℃,n(环烷酮)∶n(芳醛)=1∶1.2,催化剂用量x([(Hmp)2h2pi](OTf)4)=30%n(酮)时最高产率可达89%。催化剂重复使用6次后仍然具有一定的催化活性。

哌嗪为阳离子的新型离子液体

制备了两种哌嗪为阳离子的新型化合物,甲酸哌嗪与二甲酸哌嗪,应用红外光谱、核磁共振氢谱和元素分析对所制备的化合物进行了表征。并且通过化合物熔点、电导率等性质的测定发现此两种化合物具有离子液体的特征。

一锅法制备1-(2,3-二氯苯基)哌嗪盐酸盐

1-(2,3-二氯苯基)哌嗪盐酸盐是重要的医药中间体。以二乙醇胺为起始原料,无溶剂条件下经氯代反应制得β,β′-二氯代二乙基胺盐酸盐,不经分离直接滴加2,3-二氯苯胺和相转移催化剂,经环合反应合成目标化合物1-(2,3-二氯苯基)哌嗪盐酸盐。产率48.3%,纯度95.7%。讨论了各步反应的影响因素。产物经红外光谱、核磁共振氢谱分析验证与目标化合物的结构一致。该方法经济环保,省时,易操作。

1-烷基-1-苄基-4-(3-氯-2-羟基)丙基哌嗪季铵盐的合成及生物活性

设计合成了７个１烷基１苄基４（３氯２羟基）丙基哌嗪季铵盐（Ｉａ～ｇ）。生物活性试验结果表明，苄基苯环上连有强吸电子取代基时，可使抗炎和镇痛活性明显增强；季铵盐中的负离子对生物活性有一定的影响。在２０ｍｇ·ｋｇ－１的剂量下，Ｉｄ和Ｉｅ的抗炎活性和Ｉｅ的镇痛活性明显。

Synthesis, Spectroscopic Properties and Crystal Structure of (C_4N_2H_(12))_2Zr(C_2O_4)_4·H_2O

The title compound (C4N2H12)2Zr(C2O4)4稨2O 1 was synthesized by the reaction of ZrOCl28H2O, H2C2O42H2O and piperazinium in aqueous solution. Single-crystal X-ray analysis has revealed that compound 1 (C16H26N4O17Zr, Mr = 637.63) crystallizes in the monoclinic system, space group P21/c with a = 9.0425(3), b = 13.3844(3), c = 19.1191(5) ? ?= 98.365(1)o, V = 2289.34(11) ?, Z = 4, Dc = 1.850 g/cm3, F(000) = 1304, ?= 0.577 mm-1, the final R = 0.0240 and wR = 0.0628 for 4386 observed reflections with I > 2s(I). X-ray crystal-structure analysis suggests that compound 1 consists of [Zr(C2O4)4]4- anion and two protonated piperazinium cations. The anions are linked through hydrogen bonds of piperazinium. FT-IR and Raman spectra clearly show the existence of oxalate groups in the crystal lattice.

微波辐射下N-芳基哌嗪盐酸盐的合成

取代苯胺与N,N'-双(2-氯乙基)胺盐酸盐在二乙二醇单甲醚溶剂中,微波辐射下一步合成了10种N-芳基取代哌嗪盐酸盐,反应在3～4 min内完成,产率36.9%～75.4%。结果表明,苯胺芳环上的取代基对N-芳基哌嗪化反应有着可合理预测的电子效应及位阻效应。与常规加热法相比,微波辐射法具有反应时间短、产率高、操作简便和环境友好等特点。所有产物的分子结构用IR、1HNMR和MS进行了表征。

8-苯基-8-氮杂-5-氮杂鎓-螺旋环[4,5]癸烷卤化物盐的合成及其工艺优化

以二乙醇胺和氯化亚砜为原料,经三步合成8-苯基-8-氮杂-5-氮杂鎓-螺旋环[4,5]癸烷卤化物盐。首先,二乙醇胺经SOCl2氯代得到双(2-氯乙基)胺盐酸盐,产率88.0%;接下来与苯胺亲核取代产生N-苯基哌嗪盐酸盐,产率78.0%;最后与1,4-二溴丁烷以十六烷基三甲基溴化铵为催化剂,合成目标产物,8-苯基-8-氮杂-5-氮杂鎓-螺旋环[4,5]癸烷卤化物盐。重点对第三步反应的工艺条件进行了优化。结果表明:在以K2CO3为缚酸剂,十六烷基三甲基溴化铵为相转移催化剂时,n(N-苯基哌嗪盐酸盐)∶n(1,4-二溴丁烷)=1∶1,反应温度为80℃,反应时间7h时,粗产物产率高达94.8%。经乙醇和乙腈混合液中重结晶得到浅黄色晶体,分离产率86.4%。所有合成产物的分子结构都经红外光谱,1 H和13 C核磁共振光谱进行了表征。

1-(3-氯-2-甲基苯基)哌嗪盐酸盐的合成研究

目的:研究1-(3-氯-2-甲基苯基)哌嗪盐酸盐的最佳合成工艺。方法:以二乙醇胺为起始原料,经SOCl2氯代合成β,β′-二氯代二乙基胺盐酸盐,然后在碳酸钠的作用下与3-氯-2-甲基苯胺经环合反应合成目标化合物,并通过正交实验筛选最佳工艺条件。结果:通过正交实验筛选得到1-(3-氯-2-甲基苯基)哌嗪盐酸盐的最佳合成工艺条件,其结构经1HNMR及IR表征,产率为63.2%。结论:该目标化合物的合成路线简单易操作,且得到较高的产率适合工业生产。

Synthesis and Crystal Structure of (C_6N_3H_(18))_2Ti_4O_4(C_2O_4)_7·4H_2O

The title compound (C6N3H18)2Ti4O4(C2O4)74H2O 1 (C13H22N3O18Ti2, Mr = 604.14) was synthesized by the reaction of Ti(SO4)2, H2C2O42H2O and N-(2-ammonioethyl)- piperazinium (AEPP) in aqueous solution. The single-crystal X-ray analysis has revealed that 1 crystallizes in the triclinic system, space group Pi with a = 9.1437(6), b = 11.4991(10), c = 11.6975(8) ? a = 96.2915(18), ?= 107.998(3), ? = 104.276(4), V = 1110.35(14) ?, Z = 2, Dc = 1.807 g/cm3, F(000) = 618, ?= 0.815 mm-1, the final R = 0.0463 and wR = 0.1264 for 3718 observed reflections with I > 2s(I). X-ray crystal-structure analysis suggests that compound 1 consists of [Ti4O4(C2O4)7]6- anion and two protonated N-(2-ammonioethyl)piperazinium cations. The anions are linked into an infinite chain through Ti4O4(C2O4)8 by sharing the oxalates as bridging ligands.

氟喹诺酮C-3杂环化合物的设计、合成与抗肿瘤活性研究：环丙沙星双-噁二唑甲硫醚衍生物(英文)

为进一步探究发现抗肿瘤氟喹诺酮候选化合物的有效策略,用噁二唑杂环作为环丙沙星的羧基电子等排体得中间体C-3噁二唑硫醇(5),与噁二唑氯甲烷(6a–6h)缩合形成双-噁二唑甲硫醚(7a–7h),再与碘甲烷成哌嗪季铵盐(8a–8h),其结构经元素分析和光谱数据确证,评价了体外对CHO、HL60和L1210 3种肿瘤细胞的生长抑制活性。初步的药理结果表明,哌嗪季铵盐(8)的活性高于相应游离碱(7)的活性。

新型环磷酰胺前药:环磷酰胺哌嗪季铵盐的构效关系(英文)

作为对环磷酰胺结构改造新思路的延续, 本文以化合物9i为先导物设计并合成了三个系列环磷酰胺哌嗪季铵盐类衍生物(10, 11和13)。通过体内抗肿瘤活性试验, 其构效关系表明: 1)环磷酰胺螺环哌嗪季铵盐(10)的构象和N-3位的取代基对活性影响极大2)不同类型的环磷酰胺非螺环哌嗪季铵盐(11)显示出其抗肿瘤活性的差异 3) 选择合适的季铵盐部分, 化合物1,2-苯并异恶唑磷酰哌嗪季铵盐(13)有可能具有抗肿瘤活性。此研究结果将有助于进一步设计和改造各种氮芥类抗肿瘤药物。