Probing the Anticancer Mechanism of (−)‐Ainsliatrimer A through Diverted Total Synthesis and Bioorthogonal Ligation

Herein, we report an efficient approach for exploring the novel anticancer mechanism of (?)‐ainsliatrimer A, a structurally complex and unique trimeric sesquiterpenoid, through a combined strategy of diverted total synthesis (DTS) and bioorthogonal ligation (TQ ligation), which allowed us to visualize the subcellular localization of this natural product in live cells. Further biochemical studies facilitated by pretarget imaging revealed that PPARγ, a nucleus receptor, was a functional cellular target of ainsliatrimer A. We also confirmed that the anticancer activity of ainsliatrimer A was caused by the activation of PPARγ.     

Inverse screening of Simvastatin kinase targets from glioblastoma druggable kinome

The statin drug Simvastatin is a HMG-CoA reductase inhibitor that has been widely used to lower blood lipid. However, the drug is clinically observed to reposition a significant suppressing potency on glioblastoma (GBM) by unexpectedly targeting diverse kinase pathways involved in GBM tumorigensis. Here, an inverse screening strategy is described to discover potential kinase targets of Simvastatin. Various human protein kinases implicated in GBM are enriched to define a druggable kinome; the binding behavior of Simvastatin to the kinome is profiled systematically via an integrative computational approach, from which most kinases have only low or moderate binding potency to Simvastatin, while only few are identified as promising kinase hits. It is revealed that Simvastatin can potentially interact with certain known targets or key regulators of GBM such as ErbB, c-Src and FGFR signaling pathways, but exhibit low affinity to the well-established GBM target of PI3K/Akt/mTOR pathway. Further assays determine that Simvastatin can inhibit kinase hits EGFR, MET, SRC and HER2 at nanomolar level, which are comparable with those of cognate kinase inhibitors. Structural analyses reveal that the sophisticated T790 M gatekeeper mutation can considerably reduce Simvastatin sensitivity to EGFR by inducing the ligand change between different binding modes.     

In vitro antiproliferative activity of glabridin derivatives and their in silico target identification

Abstract

Novel Mannich base derivatives of glabridin were synthesized and their antiproliferative activity were performed along with our previously reported glabridin-chalcone hybrids molecules (GCHMs) against various human cell lines MDA-MB-231 (breast adenocarcinoma), HEK-293 (embryonic kidney cell line), K562 (leukemia), MCF-7 (breast adenocarcinoma), HeLa (cervix adenocarcinoma), HepG2 (hepatocellular carcinoma) and WRL-68 (hepatic carcinoma). The result showed that the glabridin significantly reduced cell proliferation with IC₅₀ ranges from 3.67 to 58.30?µM against all the tested cell lines. The remarkable reduction in antiproliferative activity 2’,4’-dimethoxyglabridin and GCHMs compounds with phenolic OH groups protected by methoxy (OCH₃) groups suggested that the free OH groups are essential factor for the antiproliferative activity of glabridin and its derivatives. The Mannich base derivatives of glabridin showed moderate activity IC₅₀ (2.20–>95.78?µM). Furthermore, in silico target identification analysis revealed that AKT1, DECR1 and NOS1 are the potential targets for glabridin and their derivatives.     

中高分辨力遥感图像中飞机目标自动识别算法研究

提出了一种中高分辨力的航空航天遥感图像中飞机目标快速自动识别的新算法。在分割和分类过程中充分利用飞机目标的先验知识,提出了一种改进区域分割方法,并应用树分类器对飞机目标进行自动识别。所提出的改进区域分割方法较好地实现了区域分割中阈值的准确自动选取,克服了复杂背景图像中小目标的全局阈值自动分割的失效问题。采用二叉树分类器,通过提取简单的目标几何特征,分层进行种类识别,提高了识别速度,降低了漏检率和虚警率。运用该方法进行了实验。结果表明,识别率达到了100%。     

基于DIGNET网络的数据融合方法

针对数据融合和目标识别的特点,提出了基于DIGNET自组织聚类人工神经网络的数据融合方法。考虑到多传感器系统测量多个参量的特点,用并行的子网络结构代替中间隐层,实现了基于决策层的信息融合目标识别。利用仿真数据对基于DIGNET的数据融合方法进行了实验研究。实验结果表明,该方法具有数据正确分类率高和抗噪能力强等优点,有效地实现了融合识别。将该方法应用于前视红外和可见光双传感器目标跟踪系统的数据融合识别是可行的。     

基于红外/毫米波双模融合的目标识别方法

在数据融合的基础上,以红外/毫米波双模传感器的智能融合结构为模型,将模糊神经网络与D-S证据理论相结合,提出了一种新的目标识别方法.该算法根据红外/毫米波传感器的性能及工作范围,构造模糊变量作为神经网络的输入,根据神经网络的不同输出判别目标的真伪,并利用D-S证据理论进行目标身份识别.仿真结果证明了该算法的可行性.     

不同材料弹体超声速侵彻钢筋混凝土靶的结构破坏对比实验

设计了超声速钻地结构弹,采用203 mm口径的火炮,开展了25 kg量级弹体在1100~1300 m/s速度范围内侵彻钢筋混凝土靶的实验研究,应用数值仿真对弹体侵彻钢筋混凝土靶的过程进行了模拟计算。基于实验和仿真结果,对超声速侵彻条件下两种金属材料弹体的结构响应、质量损失等问题进行了分析。结果表明:在超声速侵彻钢筋混凝土靶的过程中,两种金属材料的弹体结构变形破坏形式主要为头部侵蚀和侧壁磨蚀,头部侵蚀量的大小与弹体壳体材料有关,高强度G50钢材料更适合用于1200 m/s速度量级的超声速侵彻环境。对出现的“径缩”现象作了初步分析,并对今后工程应用的结构弹体设计提出了指导意见。     

激光惯性约束聚变靶制备技术研究进展

在实验室实现聚变反应释放的能量大于点燃聚变反应所需能量的阈值是当今世界ICF研究的主要目标,实现这一目标仍需要深入研究一系列的关键物理问题。在ICF研究中,制靶能力的发展与提升至关重要,靶的质量是实验成功的核心要素之一。本文介绍了国际ICF靶制备工作近年来在新型烧蚀层材料靶丸、新型靶丸支撑技术、优化黑腔材料与构型以及减小燃料填充管直径等方面取得的一系列进展,并结合ICF物理需求,简要阐述了ICF靶的发展趋势。     

载机平台光电转塔目标定位的仿真算法

目标定位是光电转塔典型功能和任务之一,对其定位精度的考量也是转塔作战技术指标之一,针对该问题,从理论和仿真角度进行了分析。分析目标定位中用到的坐标系及其相互转换关系,给出光电转塔视轴反演、有源目标定位、无源目标定位的算法流程,通过仿真实验加以验证,考虑了定位过程中可能的随机误差来源,并分析是否采用均值滤波及其对定位结果的影响,最后通过Monte-Carlo分析计算了定位精度。分析结果表明:1）有源定位比无源定位的精度高,在仿真假设条件下,精度约提高1倍;2）均值滤波后,定位精度有较大提升（约提高15倍）;3）18 km距离时典型无源定位精度在80%置信度条件下约为39.4 m;4）统计直方图反映出80%置信度CEP半径及最大误差距离随载机位置、姿态、转塔视轴等（体现在目标载机距离上）不同参数的变化结果。     

基于粒子滤波的运动目标光电定位仿真研究

运动目标的光电定位不能像静止目标那样简单做均值滤波,鉴于此,引入粒子滤波算法,它不仅可以应用于线性系统,而且还适用于非线性系统。结合光电定位需求,详细推导了计算公式及初值和参数选取公式,对只含测量噪声以及含有测量和运动噪声等的海面运动目标光电无源定位算法进行了仿真计算,验证了算法的有效性,讨论了噪声强度对滤波效果的影响,滤波参数选择对滤波效果的影响,目标运动方式对滤波跟随性的影响,重采样算法对滤波效果的影响等。所得结论为:粒子滤波可用于运动目标光电定位过程,可有效降低定位误差;粒子滤波算法具有较强鲁棒性,适用于噪声较大、目标运动形态变化大等情况。