聚谷氨酸发酵过程中ATR-FTIR光谱信号的分数阶基线校正

采用衰减全反射傅里叶变换红外光谱法（ATR-FTIR）,结合多元校正模型对γ-聚谷氨酸（γ-PGA）发酵过程中两种主要底物葡萄糖和谷氨酸钠的浓度进行间接测量,为优化发酵系统控制提供重要的反馈信息。光谱测量中经常出现的基线漂移会严重影响后续多元校正模型的性能,需要采用基线校正算法对光谱进行预处理。现有流行的基线校正算法多数是基于Whittaker Smoother（WS）平滑算法,这些算法均采用整数阶微分对拟合基线进行约束,表达能力有限。针对现有基线校正算法中的整数阶微分自适应性差的问题,利用更加灵活的分数阶微分对基线进行约束,提出了一种基于分数阶的基线校正算法,实现对整数阶基线校正的扩展。总共进行了5个批次的γ-PGA发酵实验,并对不同批次和全部批次的ATR-FTIR光谱数据分别进行了分数阶基线校正,模型的预测精度均得到不同程度的提升。实验结果表明,只有在批次2时,基于整数阶的基线校正效果最好;其他批次的基线校正效果最好时的阶次均为分数阶。这也表明了分数阶微分（包含整数阶微分）对基线的约束更加合理。同时发现全部批次的整体基线校正效果远远差于单一批次的效果,原因可能是各批次发酵光谱的基线是不同的,对不同的批次需要选用不同的阶次以获得最佳的基线校正。此外,γ-PGA发酵样品的ATR-FTIR光谱测量是以蒸馏水为背景,会在3 100~3 600 cm-1波数范围内出现负水峰,形成有害的干扰信号;分数阶基线校正后的光谱表明,分数阶基线校正算法将负的水峰当作基线,在一定程度上进行了消除。综上分析,分数阶基线校正算法不仅扩展了传统整数阶基线校正算法的应用范围,也为消除ATR光谱中负的水峰提供了新的解决思路。     

Inhibitor Development against p7 Channel in Hepatitis C Virus

Hepatitis C Virus (HCV) is the key cause of chronic and severe liver diseases. The recent direct-acting antiviral agents have shown the clinical success on HCV-related diseases, but the rapid HCV mutations of the virus highlight the sustaining necessity to develop new drugs. p7, the viroporin protein from HCV, has been sought after as a potential anti-HCV drug target. Several classes of compounds, such as amantadine and rimantadine have been testified for p7 inhibition. However, the efficacies of these compounds are not high. Here, we screened some novel p7 inhibitors with amantadine scaffold for the inhibitor development. The dissociation constant (Kd) of 42 ARD-series compounds were determined by nuclear magnetic resonance (NMR) titrations. The efficacies of the two best inhibitors, ARD87 and ARD112, were further confirmed using viral production assay. The binding mode analysis and binding stability for the strongest inhibitor were deciphered by molecular dynamics (MD) simulation. These ARD-series compounds together with 49 previously published compounds were further analyzed by molecular docking. Key pharmacophores were identified among the structure-similar compounds. Our studies suggest that different functional groups are highly correlated with the efficacy for inhibiting p7 of HCV, in which hydrophobic interactions are the dominant forces for the inhibition potency. Our findings provide guiding principles for designing higher affinity inhibitors of p7 as potential anti-HCV drug candidates.     

On Extension of 1-Lipschitz Mappings between Two Unit Spheres of lp(Γ) Type Spaces (1

FANG Xi Nian 《数学研究与评论》2009,29(4)

Application of differential pulse stripping voltammetry and chemometrics for the determination of three antibiotic drugs in food samples

A reliable method for simultaneous determination of three antibiotic drugs(levofloxacin,gatifloxacin and lomefloxacin) by differential pulse stripping voltammetry(DPSV) in Britton-Robinson buffer(pH 7.96) was presented.The method is based on adsorptive accumulation of the antibacterial drugs on a hanging mercury dropping electrode(HMDE),followed by the reduction of the adsorptive species by the technique of DPSV.Optimal conditions,the deposition time of 80 s,the deposition potential of—1250 mV,and the scan rate of 25 mV/s,were obtained.The linear concentration ranges of 0.010-0.080μg/mL were obtained for all these three antibiotic drugs,while the detection limits were 2.38,3.20 and 1.60ng/mL for levofloxacin,gatifloxacin and lomefloxacin,respectively.In this work,chemometrics methods,such as classical least squares(CLS),partial least squares(PLS), principle component regression(PCR) and radial basis function-artificial neural networks(RBF-ANN),were used to quantitatively resolve the overlapping signals.It was found that PCR gave the best results with total relative prediction error(RPE_T) of 7.71%.The proposed method was applied to determine these three drugs in several commercial food samples with spiked method and yielded satisfactory recoveries.     

含4-氨基哌啶片段的6,7-二甲氧基喹啉衍生物的合成及抗肿瘤活性

以2-氨基-4,5-二甲氧基苯甲酸（2）和环酮（环戊酮、环己酮）为原料,在三氯氧磷作用下“一锅法”合成6,7-二甲氧基喹啉中间体（3）,再与4-氨基哌啶或4-异丙基-1-氨基环己烷（4）发生Buchwald-Hartwig偶联反应,得到含有4-氨基哌啶或4-异丙基-1-氨基环己烷片段的6,7-二甲氧基喹啉衍生物（1a～1f）,产物及中间体结构通过¹H NMR、¹³C NMR、MS及元素分析进行表征。初步抗肿瘤活性测试表明,所合成化合物对HepG2、MCF-7、PC3和HeLa均有明显的抑制活性,尤其是化合物1b展现出较强的MCF-7抑制活性(IC₅₀ =11.2μmol/L),甚至强于当前乳腺癌的一线治疗药物4-羟基他莫昔芬(IC₅₀ =15.1μmol/L);此外,标题化合物对正常的乳腺上皮细胞MCF-10A没有毒性。     

3,5-二叔丁基甲苯的气相色谱法分析

用气相色谱法定量测定了反应混合物中的３,５－二叔丁基甲苯。方法简便、快速,完成一次分析仅需１０ｍｉｎ,校正曲线在１．１～９．２μｇ间呈现良好的线性关系（ｒ＝０．９９９０,ｎ＝８）。     

具有优异甲醇催化氧化性能的Pt/MoO3-WO3/CNTs催化剂

以聚二烯丙基二甲基胺盐酸盐(PDDA)为连接剂,采用原位自组装方式将MoO3和WO3负载到碳纳米管(CNTs)上,然后通过乙二醇还原法负载Pt纳米颗粒,得到Pt纳米颗粒均匀分布的Pt/MoO3-WO3/CNTs催化剂.当氧化物总量控制在10 wt%,MoO3与WO3摩尔比为1:0.5时,Pt/MoO3-WO3/CNTs催化剂催化甲醇氧化活性最高,甲醇氧化峰电流If高达835 A/gPt.WO3和MoO3的加入提高了催化剂的甲醇氧化活性、抗CO中毒能力和稳定性,使得Pt/MoO3-WO3/CNTs催化剂表现出优异的甲醇电催化氧化性能.     

Novel graphene oxide/bentonite composite for uranium(VI) adsorption from aqueous solution

A novel graphene oxide/bentonite composite (GO/bentonite) was synthesized and then characterized through powder X-ray diffraction, fourier transform infrared spectroscopy, thermogravimetric analysis, scanning electron microscopy, and energy dispersive spectroscopy. Adsorption achieved equilibrium within 10 min. Moreover, U(VI) adsorption on GO/bentonite was highly dependent on solution pH and independent of ionic strength. These characteristics suggested that inner-sphere surface complexes of U(VI) formed on GO/bentonite. The adsorption of U(VI) from aqueous solution on GO/bentonite was fitted to the pseudo-second-order and Freundlich isotherm models. The maximum sorption capacity of GO/bentonite was 234.19 mg g^?1 under neutral pH at 303 K. GO/bentonite is a potentially powerful adsorbent for the efficient removal of U(VI) from aqueous solutions.