大脉冲能量单层CVD石墨烯被动调Q掺镱双包层光纤激光器

基于单层化学气相沉积(CVD)石墨烯可饱和吸收体的大脉冲能量被动调Q双包层光纤激光器.采用三明治结构,将CVD法生长的单层石墨烯通过聚甲基丙烯酸甲酯(PMMA)从铜箔上转移到光纤端面,制备成PMMA/石墨烯调Q器.采用全光纤线性腔结构,掺镱双包层光纤和PMMA/单层石墨烯分别作为增益介质和被动调Q器件,大功率975nm半导体激光器作为泵浦源,大比例(95%)功率耦合输出,成功实现了中心波长为1 063.6nm大脉冲能量的稳定调Q光纤激光器.调Q脉冲序列重复频率在9.7~26.46kHz连续可调,当泵浦功率为756.1mW时,最大输出功率为46mW,最小脉宽为4.5μs,并且获得的最大单脉冲能量为1.7μJ.实验结果表明,单层CVD石墨烯性能优异,将有望在双包层光纤激光器中实现更大平均功率、单脉冲能量的激光输出.

鲨鱼软骨多糖中硫酸角质素分离方法研究

探索简单有效的分离和检测鲨鱼软骨多糖中硫酸角质素组分的方法。使用乙醇分级沉淀法分离多糖中硫酸角质素,使用硫酸-咔唑法测定糖醛酸含量,Mono Q HPLC法测定硫酸角质素含量。:硫酸角质素从多糖中分离的条件:氯化钠浓度为2.0%,乙醇浓度小于56%时;氯化钠浓度为1.5%,乙醇浓度小于58%时;氯化钠浓度为1.0%,乙醇浓度小于60%时。使用乙醇分级沉淀法可实现鲨鱼软骨多糖中硫酸角质素组分的分离,Mono Q HPLC法可简单快速检测多糖中硫酸角质素组分。

血吸虫肠相关循环抗原组分CAA和CCA的纯化与特异检测

目的：探讨血吸虫肠相关循环抗原ＣＡＡ与ＣＣＡ诊断靶微粒特异性的差别，并试探获取其纯化制品用于定量检测的标准系列。方法：对两组分进行了亲和层析及阴离子交换剂高效液相纯化分离，并应用单抗检测系统进行同相和异相交互测试。结果：Ｍｏｎｏ－Ｑ－ＨＰＬＣ（高效液相层析）梯度洗脱分离ＡＷＡｊ－ＴＣＡ可溶组分，可获得一个带阳离子活性的非结合ＣＣＡ－１洗脱峰及３个大小不等的、带阳离子活性的ＣＣＡ－２、ＣＣＡ－３及ＣＣＡ－４非结合洗脱峰，以及一个带阴离子活性ＣＡＡ－１洗脱峰。ＣＡＡ活性峰在峰谱上与ＣＣＡ－３有部分重叠。与单抗亲和层析纯品的活性对比测定显示ＣＣＡ－１与ＣＣＡ－２为该组分的主要构成，但ＣＣＡ－２及ＣＡＡ－１在本实验条件下均有微量的相互杂染。同相和异相双位点ＥＬＩＳＡ的４种组合交互检测，展示ＣＣＡ只能在捕获与检测抗体同为抗ＣＣＡ单抗的一种组合中被检出，而另３种组合只能测出ＣＡＡ组分。结论：血吸虫肠相关ＣＣＡ组分为一兼含两性电荷的分子混合体；而ＣＡＡ分子上具有一个可被抗ＣＣＡ单抗识别的活性表位位点，从而可能影响纯化分离和特异检测。

Isolation and specific detection of two major schistosoma gut-associated circulating antigens

Objectives To investigate the nature of the common epitopes of Schistosoma japonicum (S. japonicum) circulating anodic (CAA) and circulating cathodic antigen (CCA) and to try to obtain sufficient purified material to set up a standard series for quantitative determinations.Methods Isolation of the two worm fractions from a trichloroacetic acid (TCA) soluble preparation of S. japonicum adult worm antigen (AWAj-TCA) via Mono-Q anion exchange chromatography was performed and analysis of specific reactivity of the eluted fractions was done by antigen-capture Enzyme Linked Immuno Sorbent Assay (ELISA) specific for CAA or CCA with reference to affinity purified preparations of S. mansoni CAA and CCA. Results When an ionic strength gradient was used, CCA was eluted in two major peaks, an unbound fraction CCA-1, and a major bound fraction, CCA-2. Two additional minor peaks, CCA-3 and CCA-4, were eluted at higher ionic strengths. CAA was only detected in the bound fraction, partly overlapping with CCA-3. In the CCA-1 and CCA-2 fractions, reactivity was only found in the antigen-capture ELISA using anti-CCA McAbs both for capture and detection. The CAA fraction was predominantly found to be positive in the antigen-capture ELISA using anti-CAA McAbs both for capture and detection. However, in ELISA using combined anti-CCA and anti-CAA McAbs for capture and detection, this fraction showed some reactivity.Conclusion The two CCA fractions contain molecules which bear at least two CCA-epitopes; the CAA fraction contains molecules which contain at least two CAA-epitopes, and one CCA-epitope.

用分析色谱方法检测核酸疫苗中超螺旋构象质粒的比例

为建立阴离子分析色谱法用于检测核酸疫苗中各种构象的质粒所占的比例.以中高压层析系统(如AKTA Purifier)和Mono Q FPLC分析柱为基础建立分析平台,通过软件计算各层析峰的面积从而得到各种构象(特别是超螺旋构象)的质粒所占的比例.检测过程可以在30 min内完成,样品中各种组分分离完整,层析峰面积计算有效,检测结果客观准确.该方法克服了传统方法人为因素影响大的缺点,达到了较高的精度.不但能够用于核酸疫苗半成品和成品的质控,还能够应用于疫苗工艺开发和生产过程的控制,为工艺优化和生产环节的质控提供依据.