载药蛋白质/聚苯硼酸复合纳米微球制备及其释药性能研究

蛋白质纳米颗粒具有良好的生物相容性和生物降解性,易于进行额外的表面修饰,用作药物输送系统提高了生物利用度,减少了药物分子的毒副作用.本工作在利用苯硼酸基团与再生桑蚕丝蛋白(RSF)上相关侧基之间具有路易斯酸-碱配对反应的基础上,通过3-丙烯酰胺苯硼酸(APBA)在RSF水溶液中原位聚合,使RSF分子链重排形成微球并在表面负载抗炎中药,制备了载药丝蛋白/聚苯硼酸纳米微球.此尺寸分布均匀的微球直径约为550～600nm,表面光滑且在水中的分散性能良好;对乔松素、杜鹃素和地奥司明三种药物的负载率分别为7.8%,11.9%和13.4%,包封率分别为75.0%,89.1%和93.7%.载药微球控制释放约7d,且缓释行为具有pH响应性.丝蛋白/聚苯硼酸纳米微球与主体药物协同作用提高了自由基清除速度和清除效率,优于直接给药组.与此同时,将RSF改换为牛血清白蛋白或明胶蛋白,采用此方法也能制成尺寸分别为260和100nm的白蛋白/聚苯硼酸微球或明胶蛋白/聚苯硼酸微球.由此,三种不同尺寸、电性和药物释放速率的蛋白质/聚苯硼酸纳米微球有望适应多种静脉注射和皮下或腹腔注射药物传输的需求.     

5-氟尿嘧啶/壳聚糖载药纳米微球的制备及性能

以三聚磷酸钠为交联剂,采用离子交联法制备了5-氟尿嘧啶/壳聚糖纳米微球,评价其性能、体外释药性能及对人肺癌细胞GLC-82的体外杀伤效应,并通过Zeta电位和红外光谱分析载药纳米微球形成机理.结果表明,所制备的5-Fu/CS纳米微球平均包封率为32.3%,平均载药量为25.6%,平均粒径为253nm,平均zeta电势为+8.38mV,成球性及分散性良好.CS载药纳米微球具有缓释性能,体外释药行为符合双向动力学规律.在体外作用72h,CS载药纳米微球对人肺癌细胞GLC-82的杀伤率达66.6%,杀伤效果明显优于5-Fu对照组.     

抗癌载药体系Fe_3O_4@ZIF-8@PA的合成及药物释放

采用溶剂热法合成磁性Fe_3O_4纳米粒子,并以此为基底设计制备了一种具有pH响应核壳结构的磁性纳米复合材料Fe_3O_4@ZIF-8@PA.该材料的比饱和磁化强度可达35.46 A·m2/g,具有良好的磁性.Fe_3O_4纳米粒子呈球型结构,分散性良好.与基底相比,复合微球的粒径尺寸明显增大,但依然符合载体材料的理想尺寸且分布均匀.此外,载体具有多孔结构,表面积较大,载药效率和载药量分别高达96.4%和144.6 mg/g.在pH为7.4和5.0的条件下对载药纳米粒子进行了药物释放研究.24 h内,粒子在2种pH下累计释放量分别为39.8%和78.6%.通过药物缓释验证了载体的pH响应性能.在实验中引入了对癌细胞具有杀伤作用的植酸,使合成的载体具有一定的抗癌作用.同时采用四甲基偶氮唑盐(MTT)法对人骨肉瘤细胞(MG-63)进行了体外分析实验,证实材料与抗癌药物阿霉素(DOX)之间存在着一定的协同抗癌效果.     

可降解聚乙交酯-丙交酯缓释微球用于甲状旁腺相关肽的持续释放

采用水包油包水(W1/O/W2)复乳溶剂挥发法制备了包载甲状旁腺激素相关肽(PTHrP)的聚乙交酯-丙交酯(PLGA)微球,通过核磁,红外,GPC,扫描电子显微镜等观察PLGA载药微球的结构,表明载药微球具有良好的球形结构,其平均粒径约为8μm.而体外模拟释放表明,此PLGA载药微球能实现PTHrP1-34长达25天的持续释放.并通过MTT法、碱性磷酸酶活性测定等检测负载PTHrP1-34的PLGA微球缓释系统对小鼠成骨细胞MC3T3-E1增殖及分化的影响,结果表明PTHrP1-34浓度为1×10-9mol/L时对MC3T3-E1增殖促进效应最大,且随着药物作用时间的延长,缓释系统促进细胞增殖、分化的作用越明显.     

Fe_3O_4磁性纳米粒子的PEG修饰剂的合成与性能

采用共沉淀法制备了用柠檬酸包覆的Fe3O4磁性纳米粒子,为提高其生物环境适应性和生物应用,利用聚乙二醇二胺(NH2-PEG-NH2)通过碳二亚胺化学法进一步修饰,得到具有良好性能的磁性纳米粒子修饰剂,并分别用场发射扫描电子显微镜(SEM)、洛伦兹透射电子显微镜(TEM)、马尔文激光粒度仪、X-射线粉末衍射仪(XRD)、傅里叶变换红外光谱(FTIR)、综合热分析仪(TG/DTA)、振动样品磁强计(VSM)对磁性纳米粒子的表面形态、化学结构、晶体结构、热稳定性和磁性能进行了表征.在此基础上用合成的磁性纳米粒子修饰剂对盐酸阿霉素(DOX·HCl)进行了修饰,研究了修饰剂的载药和释药行为.结果表明,所制备的修饰剂近乎球形,尺寸相对均匀,粒径在15 nm左右,饱和磁化强度为68 A·m2/kg,在磁靶向药物运输中可以达到良好的磁响应性能.在水中的载药量达到83%,在p H=7.4和p H=5.0下,磁性纳米粒子载药盐酸阿霉素释放均是一个缓慢的过程,具有明显的缓释效果,此外,由于不同p H值下,DOX中的氨基质子化程度存在差异,在较低的p H值下质子化的氨基互相排斥,这更有利于DOX的释放,累计释药率在72 h后分别为65.8%(p H=7.4)与73.6%(p H=5.0).研究表明该磁性纳米粒子具有很好的载药能力及缓释效果.     

2,4-D/CMC-g-AM/SA/FK微球的制备及其缓释性能

以丙烯酰胺(AM)为单体,制备了羧甲基纤维素钠接枝丙烯酰胺共聚物(CMC-g-AM)。以2,4-二氯苯氧乙酸(2,4-D)为模型药物,以羽毛蛋白(FK)为共混改性剂,采用挤压法制备了CMC-g-AM/海藻酸钠(SA)/羽毛蛋白载药微球。利用红外光谱、光学显微镜、激光粒度仪分别对接枝共聚物的结构、载药微球的形貌以及粒径分布进行了表征,并探讨了不同的接枝共聚物、羽毛蛋白用量、交联剂浓度和交联时间对缓释微球的载药量和缓释性能影响。结果表明,当CMC-g-AM的合成单体比AM:CMC为3:1,羽毛蛋白用量为30%,交联剂浓度为0.7 mol·L-1,交联时间为1 h,载药微球的载药量较高,为16.7%。复合微球平均粒径为1.6 mm。载药微球具有良好的缓释性能,释药曲线符合Higuchi动力学方程。     

壳交联pH响应型PLGA载药微球的制备与研究

首先采用一次乳化法制备出PLGA[聚(乳酸-羟基乙酸)]纳米微球,并通过静电吸附将阳离子聚合物壳聚糖修饰到PLGA微球表面,然后以香草醛为交联剂对壳聚糖进行化学交联,得到一种壳交联的p H响应型纳米微球(PCV),微球粒径为(277.60±38.01)nm,表面电位为(21.60±4.51)m V.微球稳定性评价结果显示微球在24 h内粒径变化较小;流式细胞仪检测显示细胞对PCV微球的摄取量比未经修饰的PLGA微球的摄取量高;空白微球细胞毒性实验表明在空白微球浓度小于80μg/m L时细胞的存活率达93.24%.以多西他赛(DTX)为模型药物进行包载,该纳米微球DTX的载药率为7.48%,包封率为34.98%;体外药物释放实验显示,该微球在p H=5.0环境下孵育90 h的药物积累释放率达58.66%,而在p H=7.4的环境下的药物积累释放率为50.63%;此外,载DTX微球毒性试验结果表明该载药微球对A549肺癌细胞有较强的杀伤作用,其IC50值可达0.0009μg/m L.     

玉米醇溶蛋白/壳聚糖复合纳米微球的制备及性能研究

以生物相容性的玉米醇溶蛋白(Zein)和壳聚糖(Chitosan)为原料,利用溶剂-非溶剂相分离法成功制备了玉米醇溶蛋白/壳聚糖复合纳米微球(NSZ/CS),运用FT-IR、SEM和TEM等对复合纳米微球进行了表征。采用罗丹明B(RB)为模型药物分子,研究了复合纳米微球的药物释放性能。与玉米醇溶蛋白纳米微球(NSZ)相比,复合纳米微球NSZ/CS对RB和Dox·HCl的包封率显著上升,分别可达83.5%和75.3%。NSZ/CS对RB的累积释放量也大幅度提高。在模拟人工胃液和人工肠液中,NSZ/CS对RB释放36 h后,累积释放量分别为85.2%和95.4%。进一步将NSZ/CS用于负载抗癌药物盐酸阿霉素(Dox·HCl),发现Dox@NSZ/CS在p H=7.4的磷酸缓冲液(PBS)中的累积释放量达91.0%。复合纳米微球NSZ/CS有望作为水溶性药物载体应用于生物医药领域。     

羧甲基壳聚糖/有机累托石纳米复合材料及其药物缓释性能研究

利用简单的溶液插层法制备了羧甲基壳聚糖/有机累托石纳米复合材料,其中累托石(REC)用十六烷基三甲基溴化铵进行改性.用X-射线衍射(XRD)、红外光谱(FTIR)和扫描电镜(SEM)表征了该纳米复合材料的微观结构和形态,实验表明羧甲基壳聚糖插层进入了累托石层间,增大了累托石的层间距,并且累托石均匀地分布在羧甲基壳聚糖基体中.以牛血清蛋白(BSA)为药物模型,研究了纳米复合材料与海藻酸钠形成的微球的药物缓释性能.结果显示,该微球对药物的包封率及缓释性能与纯羧甲基壳聚糖微球相比都有较大改善,包封率从56%提高到86%,药物缓释时间从24 h上升到72 h.并且纳米复合材料/海藻酸钠微球的释药具有pH响应性,在pH为1.2的条件下释药慢,而在pH为7.4时释药快,可用于小肠或结肠定位缓释系统.因此,羧甲基壳聚糖/有机累托石纳米复合材料很有潜力作为药物载体.     

线性麦芽糊精聚合物功能化Fe3O4纳米复合物药物载体的合成和应用

采用共沉淀法制备得到了线性麦芽糊精聚合物功能化的Fe₃O₄磁性纳米粒子(LM-SP-MNPs),通过傅里叶变换红外光谱、透射电子显微镜、热重分析等技术对其结构、形貌进行了表征。 其粒径大小为(12±2) nm。 选取抗癌药物盐酸阿霉素(DOX)作为模型药物,运用荧光光谱法研究了LM-SP-MNPs的载药性能和释放行为,探讨了pH值对LM-SP-MNPs药物释放性能的影响。 最适pH条件下,LM-SP-MNPs对盐酸阿霉素的最大吸附量约为357.1 mg/g,吸附等温线符合Freundlich等温吸附模型。 LM-SP-MNPs与盐酸阿霉素的复合物(DOX@LM-SP-MNPs),在37 ℃的条件下药物在酸性条件下的释放效率大于中性条件。 pH=5.3时,盐酸阿霉素在7 h内的累积释放率为26.9%。 此外,细胞毒性试验表明,LM-SP-MNPs具有良好的生物相容性,而DOX@LM-SP-MNPs和肝癌细胞共培养后可以明显杀死HepG2肝癌细胞。     

二氧化碳和丙烯直接合成甲基丙烯酸的NiPMo/TiO2催化剂的研究

用溶胶-凝胶法以磷钼酸(MPA)的镍盐溶液水解钛酸四丁酯制备了NiPMo/TiO2催化剂.使用ICP、 XRD、 TG-DTA、 IR、 TPD-MS和微反应技术研究了催化剂的化学组成、热稳定性、化学吸附性质和催化反应性能.杂多钼酸盐与TiO2通过O2-在TiO2表面发生了键合.在623 K下,杂多阴离子仍保持原有的Keggin结构.CO2在Lewis酸位Ni(Ⅱ)和Lewis碱位Ni-O-Mo的桥氧协同作用下生成CO2卧式吸附态Ni(Ⅱ)←O-(CO)←(O--Ni).丙烯有多种吸附态在催化剂上吸附.在563 K、 1 MPa和空速1500 h-1的反应条件下,丙烯的摩尔转化率为3.2%,产物MAA选择性为95%.     

Toward new camptothecins. Part 6: Synthesis of crucial ketones and their use in Friedländer reaction

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.     

CoFe2O4自形成磁性液体场致结构化对磁化的影响

The Langevin paramagnetic theory can’t describe the relation between magnetization of ferrofluids and applied magnetic field. The structuralization of ferrofluids, which is considered the main influence factor of the magnetization, is regarded. The part of magnetization works is deposited when the structure is forming. This action influences the magnetization of ferrofluids directly or indirectly. On the base of the “compressing” model, the Langevin function that usually describes the magnetization of ferrofluid is modified, and a well-fitted curve is obtained. An equation of the relation between the equivalent volume fraction after being “compressed” and the intensity of magnetic field is discovered, which approximately describes the process of magnetization. The relation between the approximate initial susceptibility and the volume fraction can be obtained from modified formula.     

Highly regioselective Buchwald–Hartwig amination at C-2 of 2,4-dichloropyridine enabling a novel approach to 2,4-bisanilinopyridine (BAPyd) libraries

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.     

KMnO4-mediated oxidative CN bond cleavage of tertiary amines: Synthesis of amides and sulfonamides

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.     

Chemistry of heterocyclic compounds at the A. E. Favorsky Irkutsk Institute of Chemistry, Siberian Branch of the Russian Academy of Sciences, over 50 years (Review)

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.     

Sulfur-directed metal-free and regiospecific methyl C(sp3)–H imidation of thioanisoles

Regiospecific and direct imidation of the methyl C(sp³)–H bond of thioanisoles is realized under mild and metal-free conditions with N-fluorobis(benzenesulfonyl)imide as an oxidant and nitrogen source. Proposed mechanism suggests that thionium ion intermediates and a Pummerer-type reaction are involved. The imidation has advantages such as high step-economy, excellent functionality tolerance, and regiospecificity, giving structurally diverse imidation products.     

Selective syntheses of 2H-1,3-oxazines and 1H-pyrrol-3(2H)-ones via temperature-dependent Rh(II)-carbenoid-mediated 2H-azirine-ring expansion

The Rh(II)-catalyzed reaction of 2-carbonyl-substituted 2H-azirines with ethyl 2-cyano-2-diazoacetate or 2-diazo-3,3,3-trifluoropropionate provides an easy access to 2H-1,3-oxazines and 1H-pyrrol-3(2H)-ones. These compounds can be selectively prepared from the same starting material using temperature as the only varied parameter. The 2-azabuta-1,3-diene intermediate, a common precursor for both heterocyclic products, isomerizes into 2H-1,3-oxazine under kinetic control, while 1H-pyrrol-3(2H)-one is the sole product of the reaction at elevated temperatures. According to DFT-calculations a one-atom oxazine ring contraction involving ring-opening to a 2-azabuta-1,3-diene intermediate, followed by a 1,5- and 1,2-prototropic shift leads to the consecutive formation of imidoylketene and azomethine ylide, which then further undergo cyclization to the pyrrole derivative.     

Synthesis of 1-benzyloxypyrazin-2(1H)-one derivatives

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.